Nanotoxicology: an emerging discipline evolving from studies of ultrafine particles.Although humans have been exposed to airborne nanosized particles (NSPs; < 100 nm) throughout their evolutionary stages, such exposure has increased dramatically over the last century due to anthropogenic an·thro·po·gen·ic adj. 1. Of or relating to anthropogenesis. 2. Caused by humans: anthropogenic degradation of the environment. sources. The rapidly developing field of nanotechnology is likely to become yet another source through inhalation, ingestion ingestion /in·ges·tion/ (-chun) the taking of food, drugs, etc., into the body by mouth. in·ges·tion n. 1. The act of taking food and drink into the body by the mouth. 2. , skin uptake, and injection of engineered nanomaterials. Information about safety and potential hazards is urgently needed. Results of older biokinetic studies with NSPs and newer epidemiologic and toxicologic studies with airborne ultrafine particles can be viewed as the basis for the expanding field of nanotoxicology, which can be defined as safety evaluation of engineered nanostructures and nanodevices. Collectively, some emerging concepts of nanotoxicology can be identified from the results of these studies. When inhaled, specific sizes of NSPs are efficiently deposited by diffusional mechanisms in all regions of the respiratory tract respiratory tract n. The air passages from the nose to the pulmonary alveoli, including the pharynx, larynx, trachea, and bronchi. Respiratory tract . The small size facilitates uptake into cells and transcytosis across epithelial and endothelial cells Endothelial cells The cells lining the inner walls of the blood vessels. Mentioned in: Von Willebrand Disease into the blood and lymph circulation to reach potentially sensitive target sites such as bone marrow, lymph nodes Lymph nodes Small, bean-shaped masses of tissue scattered along the lymphatic system that act as filters and immune monitors, removing fluids, bacteria, or cancer cells that travel through the lymph system. , spleen, and heart. Access to the central nervous system and ganglia ganglia /gan·glia/ (gang´gle-ah) plural of ganglion. via translocation translocation /trans·lo·ca·tion/ (trans?lo-ka´shun) the attachment of a fragment of one chromosome to a nonhomologous chromosome. Abbreviated t. along axons and dendrites of neurons has also been observed. NSPs penetrating the skin distribute via uptake into lymphatic lymphatic /lym·phat·ic/ (lim-fat´ik) 1. pertaining to lymph or to a lymphatic vessel. 2. a lymphatic vessel. lym·phat·ic adj. channels. Endocytosis endocytosis (ĕn'dōsītō`səs), in biology, process by which substances are taken into the cell. When the cell membrane comes into contact with a suitable food, a portion of the cell cytoplasm surges forward to meet and surround and biokinetics are largely dependent on NSP (1) (Network Service Provider) An organization that provides a high-speed Internet backbone to ISPs and other service providers. Sprint, MCI and UUNET are examples of NSPs. See Internet backbones. surface chemistry (coating) and in vivo in vivo /in vi·vo/ (ve´vo) [L.] within the living body. in vi·vo adj. Within a living organism. in vivo adv. surface modifications. The greater surface area per mass compared with larger-sized particles of the same chemistry renders NSPs more active biologically. This activity includes a potential for inflammatory and pro-oxidant, but also antioxidant antioxidant, substance that prevents or slows the breakdown of another substance by oxygen. Synthetic and natural antioxidants are used to slow the deterioration of gasoline and rubber, and such antioxidants as vitamin C (ascorbic acid), butylated hydroxytoluene , activity, which can explain early findings showing mixed results in terms of toxicity of NSPs to environmentally relevant species. Evidence of mitochondrial mitochondrial pertaining to mitochondria. mitochondrial RNAs a unique set of tRNAs, mRNAs, rRNAs, transcribed from mitochondrial DNA by a mitochondrial-specific RNA polymerase, that account for about 4% of the total cell RNA that distribution and oxidative stress oxidative stress, n an imbalance of the prooxidant antioxidant ratio in which too few antioxidants are produced or ingested or too many oxidizing agents are produced. response after NSP endocytosis points to a need for basic research on their interactions with subcellular sub·cel·lu·lar adj. 1. Situated or occurring within a cell: subcellular organelles. 2. Smaller in size than ordinary cells: subcellular organisms. 3. structures. Additional considerations for assessing safety of engineered NSPs include careful selections of appropriate and relevant doses/concentrations, the likelihood of increased effects in a compromised organism, and also the benefits of possible desirable effects. An interdisciplinary team interdisciplinary team, n a group that consists of specialists from several fields combining skills and resources to present guidance and information. approach (e.g., toxicology, materials science, medicine, molecular biology molecular biology, scientific study of the molecular basis of life processes, including cellular respiration, excretion, and reproduction. The term molecular biology was coined in 1938 by Warren Weaver, then director of the natural sciences program at the Rockefeller , and bioinformatics, to name a few) is mandatory for nanotoxicology research to arrive at an appropriate risk assessment. Key words." biokinetics, central nervous system, engineered nanomaterials, environmental health, human health, nanosized particles, respiratory tract, risk assessment, skin, ultrafine particles. doi. 10.1289/ehp.7339 available via http://dx.doi.org/[Online 22 March 2005] ********** Exposures to airborne nanosized particles (NSPs; < 100 nm) have been experienced by humans throughout their evolutionary stages, but it is only with the advent of the industrial revolution that such exposures have increased dramatically because of anthropogenic sources such as internal combustion engines, power plants, and many other sources of thermo-degradation. The rapidly developing field of nanotechnology is likely to become yet another source for human exposures to NSPs--engineered nanoparticles (NPs)--by different routes: inhalation (respiratory tract), ingestion [gastrointestinal (GI) tract], dermal dermal /der·mal/ (der´mal) pertaining to the dermis or to the skin. der·mal or der·mic adj. Of or relating to the skin or dermis. (skin), and injection (blood circulation). Table 1 summarizes some of the natural and anthropogenic sources of NSPs, the latter divided into unintentional and intentional sources. Biologically based or naturally occurring molecules that are found inside organisms since the beginning of life can serve as model nanosized materials. For example, biogenic biogenic /bi·o·gen·ic/ (-jen´ik) having origins in biological processes. biogenic having the property of originating in a biological process. magnetite magnetite (măg`nətīt), lustrous black, magnetic mineral, Fe3O4. It occurs in crystals of the cubic system, in masses, and as a loose sand. is a naturally occurring NSP that occurs in many species ranging from bacteria to protozoa to animals (Blakemore 1975; Kirschvink et al. 2001). Biogenic magnetite has even been found in brains of humans (Dunn et al. 1995; Kirschvink et al. 1992; Schultheiss-Grassi et al. 1999) and has been associated with neurodegenerative diseases neurodegenerative diseases diseases characterized by neurodegeneration. Lesions are microscopic only but in chronic disease with massive involvement there may be grossly visible atrophy of affected nervous tissue. (Dobson 2001; Hautot et al. 2003). A biologic model of coated nanomaterials can be found in ferritin ferritin /fer·ri·tin/ (-i-tin) the iron-apoferritin complex, one of the chief forms in which iron is stored in the body. fer·ri·tin n. , which is an approximately 12-nm-large iron storage protein that contains 5- to 7-nm-sized hydrous hydrous containing water. ferric oxide phosphate inside a protective protein shell (Donlin et al. 1998). Nanosized materials, including fullerenes, occur naturally from combustion processes such as forest fires and volcanoes. Obvious differences between unintentional and intentional anthropogenic NSPs are the polydispersed and chemically complex nature (elemental, soluble, and volatile carbon compounds; soluble and poorly soluble inorganics; Cyrys et al. 2003; Hughes et al. 1998) of the former, in contrast to the monodisperse A collection of objects are called monodisperse if they have the same size - i.e. their size distribution is effectively a delta function. A sample of objects with a broader size distribution is called polydisperse. In practice, exactly monodisperse collections rarely exist. and precise chemically engineered characteristics and solid form of the latter, generated in gas or liquid phase [National Nanotechnology Initiative The National Nanotechnology Initiative is an American federal nanoscale science, engineering, and technology research and development program. Initiative participants (cited below) state that its four goals are to NSPs are variably called ultrafine particles (UFPs) by toxicologists [U.S. Environmental Protection Agency Environmental Protection Agency (EPA), independent agency of the U.S. government, with headquarters in Washington, D.C. It was established in 1970 to reduce and control air and water pollution, noise pollution, and radiation and to ensure the safe handling and (EPA EPA eicosapentaenoic acid. EPA abbr. eicosapentaenoic acid EPA, n.pr See acid, eicosapentaenoic. EPA, n. ) 2004], Aitken mode and nucleation nu·cle·a·tion n. 1. The beginning of chemical or physical changes at discrete points in a system, such as the formation of crystals in a liquid. 2. The formation of cell nuclei. mode particles by atmospheric scientists [Kulmala 2004; National Research Council (NRC NRC abbr. 1. National Research Council 2. Nuclear Regulatory Commission Noun 1. NRC - an independent federal agency created in 1974 to license and regulate nuclear power plants ) 1983], and engineered nanostructured materials by materials scientists (NNI 2004). Figure 1 depicts the range of sizes of airborne ambient particulate matter, including the nucleation-mode, Aitken-mode, accumulation-mode, and coarse-mode particles. Ambient particles < 0.1 [micro]m, defined as UFPs in the toxicologic literature, consist of transient nuclei or Aitken nuclei (NRC 1983). More recently, even smaller particles in the nucleation mode with peak diameters around 4 nm have been observed (McMurry and Woo 2002). The distinction between NSPs generated by internal combustion engines and NPs becomes further clouded by the finding of nanotubes in diesel exhaust (Evelyn et al. 2003). The use of the term "nano" in this review reflects only particle size and not chemical composition. For the purposes of this review, we use the following terms: "Nanosized particle" (NSP) includes all engineered and ambient nanosized spherical particles < 100 nm. "Engineered nanoparticle" (NP) includes only spherical NSPs specifically engineered in the laboratory; other engineered nanosized structures will be labeled according to their shape, for example, nanotubes, nanofibers, nanowires, nanorings, and so on. "Ultrafine particle" (UFP UFP United Federation of Planets (Star Trek) UFP Union des Forces Progressistes (French: Union of the Forces Progressists, Quebec provincial party) UFP URL Filtering Protocol ) includes ambient and laboratory-generated NSPs that are not produced in a controlled, engineered way. [FIGURE 1 OMITTED] Table 2 shows the tremendous differences in particle number concentrations and particle surface areas for particles of the four ambient modes, assuming an airborne concentration of 10 [micro]g/[m.sup.3] of unit density particles of each size. The extraordinarily high number concentrations of NSPs per given mass will likely be of toxicologic significance when these particles interact with cells and subcellular components. Likewise, their increased surface area per unit mass can be toxicologically important if other characteristics such as surface chemistry and bulk chemistry are the same. Although the mass of UFPs in ambient air is very low, approaching only 0.5-2 [micro]g/[m.sup.3] at background levels (Hughes et al. 1998), it can increase several-fold during high pollution episodes or on highways (Brand et al. 1991; Shi et al. 2001; Zhu et al. 2002). Physicochemical physicochemical /phys·i·co·chem·i·cal/ (fiz?i-ko-kem´ik-il) pertaining to both physics and chemistry. phys·i·co·chem·i·cal adj. 1. Relating to both physical and chemical properties. characteristics as determinants of biologic activity. The small size and corresponding large specific surface area of solid NSPs (Table 2) confer specific properties to them, for example, making them desirable as catalysts for chemical reactions. The importance of surface area becomes evident when considering that surface atoms or molecules play a dominant role in determining bulk properties (Amato 1989); the ratio of surface to total atoms or molecules increases exponentially with decreasing particle size (Figure 2). Increased surface reactivity predicts that NSPs exhibit greater biologic activity per given mass compared with larger particles, should they be taken up into living organisms and provided they are solid rather than solute solute /so·lute/ (sol´ut) the substance dissolved in solvent to form a solution. sol·ute n. particles. This increased biologic activity can be either positive and desirable (e.g., antioxidant activity, carrier capacity for therapeutics, penetration of cellular barriers for drug delivery) or negative and undesirable (e.g., toxicity, induction of oxidative stress or of cellular dysfunction), or a mix of both. Not only may adverse effects be induced, but interactions of NSPs with cells and subcellular structures and their biokinetics are likely to be very different from those of larger-sized particles. For example, more than 60 years ago virologists described the translocation of 30- to 50-nm-sized virus particles along axons and dendrites of neurons and across epithelia ep·i·the·li·a n. A plural of epithelium. (Howe and Bodian 1940), whereas first reports about increased inflammatory activity and epithelial translocation of manmade 20- and 30-nm solid particles appeared only more recently (Ferin et al. 1990; Oberdorster et al. 1990). [FIGURE 2 OMITTED] The characteristic biokinetic behaviors of NPs are attractive qualities for promising applications in medicine as diagnostic and therapeutic devices and as tools to investigate and understand molecular processes and structures in living cells (Akerman et al. 2002; Foley et al. 2002; Kreuter 2001; Li et al. 2003). For example, targeted drug delivery Scientists began to study targeted drug delivery, because the traditional drug delivery system had many disadvantages, such as high toxic effect and high minimum effective dose. In traditional drug delivery system, after the patient takes some drugs, the drugs will be all over his body to tissues that are difficult to reach [e.g., central nervous system (CNS See Continuous net settlement. CNS See continuous net settlement (CNS). )], NPs for the fight against cancer, intravascular intravascular /in·tra·vas·cu·lar/ (in?trah-vas´ku-lar) within a vessel. in·tra·vas·cu·lar adj. Within one or more blood vessels. nanosensor and nanorobotic devices, and diagnostic and imaging procedures are presently under development. The discipline of nanomedicine--defined as medical application of nanotechnology and related research--has arisen to design, test, and optimize these applications so that they can eventually be used routinely by physicians (Freitas 1999). However, in apparent stark contrast to the many efforts aimed at exploiting desirable properties of NPs for improving human health are the limited attempts to evaluate potential undesirable effects of NPs when administered intentionally for medicinal purposes, or after unintentional exposure during manufacture or processing for industrial applications. The same properties that make NPs so attractive for development in nanomedicine and for specific industrial processes could also prove deleterious when NPs interact with cells. Thus, evaluating the safety of NPs should be of highest priority given their expected worldwide distribution for industrial applications and the likelihood of human exposure, directly or through release into the environment (air, water, soil). Nanotoxicology--an emerging discipline that can be defined as "science of engineered nanodevices and nanostructures that deals with their effects in living organisms"--is gaining increased attention. Nanotoxicology research not only will provide data for safety evaluation of engineered nanostructures and devices but also will help to advance the field of nanomedicine by providing information about their undesirable properties and means to avoid them. Human exposure to nanosized materials. In addition to natural and anthropogenic sources of UFPs in the ambient air, certain workplace conditions also generate NSPs that can reach much higher exposure concentrations, up to several hundred micrograms per cubic meter, than is typically found at ambient levels. In contrast to airborne UFP exposures occurring via inhalation at the workplace and from ambient air, not much is known about levels of exposure via different routes for NPs, whether it is by direct human exposure or indirectly through contamination of the environment. For example, are there or will there be significant exposures to airborne singlet engineered carbon nanotubes or [C.sub.60] fullerenes? First measurements at a model workplace gave only very low concentrations, < 50 [micro]g/[m.sup.3], and these were most likely in the form of aggregates (Maynard et al. 2004). However, even very low concentrations of nanosized materials in the air represent very high particle number concentrations, as is well known from measurements of ambient UFPs (Hughes et al. 1998). For example, a low concentration of 10 [micro]g/[m.sup.3] of unit density 20-nm particles translates into > 1 x [10.sup.6] particles/[cm.sup.3] (Table 2). Inhalation may be the major route of exposure for NPs, yet ingestion and dermal exposures also need to be considered during manufacture, use, and disposal of engineered nanomaterials, and specific biomedical bi·o·med·i·cal adj. 1. Of or relating to biomedicine. 2. Of, relating to, or involving biological, medical, and physical sciences. applications for diagnostic and therapeutic purposes will require intravenous, subcutaneous, or intramuscular intramuscular /in·tra·mus·cu·lar/ (-mus´ku-ler) within the muscular substance. in·tra·mus·cu·lar adj. Abbr. IM Within a muscle. administration (Table 1). It can be assumed, however, that the toxicology of NPs can build on the experience and data already present in the toxicology literature of ambient UFPs. [Additional details provided in Supplemental Material available online (http://ehp.niehs.nih.gov/members/ 2005/7339/supplemental.pdf).] Manufactured nanomaterials in the environment. Manufactured nanomaterials are likely to enter the environment for several reasons. Some are and others will be produced by the ton, and some of any material produced in such mass quantities is likely to reach the environment from manufacturing effluent or from spillage during shipping and handling. They are being used in personal-care products such as cosmetics and sunscreens and can therefore enter the environment on a continual basis from washing off of consumer products (Daughton and Ternes 1999). They are being used in electronics, tires, fuel cells, and many other products, and it is unknown whether some of these materials may leak out or be worn off over the period of use. They are also being used in disposable materials such as filters and electronics and may therefore reach the environment through landfills and other methods of disposal. Scientists have also found ways of using nanomaterials in remediation. Although many of these are still in testing stages (Chitose et al. 2003; Jaques and Kim 2000; Joo et al. 2004; Nagaveni et al. 2004; Nghiem et al. 2004; Tungittiplakorn et al. 2004), dozens of sites have already been injected with various nanomaterials, including nano-iron (Mach 2004). Testing to determine the safety of these NPs used for remediation to environmentally relevant species has not yet been done. Although most people are concerned with effects on large wildlife, the basis of many food chains depends on the benthic ben·thos n. 1. The collection of organisms living on or in sea or lake bottoms. 2. The bottom of a sea or lake. [Greek. and soil flora and fauna, which could be dramatically affected by such NP injections. In addition, as noted by Lecoanet et al. (2004), nanosized materials may not migrate through soils at rapid enough rates to be valuable in remediation. Future laboratory and field trials will help clarify the line between remediation and contamination [Supplemental Material available online (http://ehp.niehs.nih. gov/members/2005/7339/supplemental.pdf)]. Toxicology of Airborne UFPs In recent years, interest in potential effects of exposure to airborne UFPs has increased considerably, and studies have shown that they can contribute to adverse health effects in the respiratory tract as well as in extrapulmonary organs. Results on direct effects of ambient and model UFPs have been reported from epidemiologic studies and controlled clinical studies in humans, inhalation/instillation studies in rodents, or in vitro in vitro /in vi·tro/ (in ve´tro) [L.] within a glass; observable in a test tube; in an artificial environment. in vi·tro adj. In an artificial environment outside a living organism. cell culture systems. For example, several epidemiologic studies have found associations of ambient UFPs with adverse respiratory and cardiovascular effects resulting in morbidity and mortality Morbidity and Mortality can refer to:
n. Abbr. COPD A chronic lung disease, such as asthma or emphysema, in which breathing becomes slowed or forced. , in addition, effects on the cardiovascular system cardiovascular system: see circulatory system. cardiovascular system System of vessels that convey blood to and from tissues throughout the body, bringing nutrients and oxygen and removing wastes and carbon dioxide. , including blood markers of coagulation coagulation (kōăg'y  lā`shən), the collecting into a mass of minute particles of a solid dispersed throughout a liquid (a sol), usually followed by the precipitation or and systemic inflammation and pulmonary
diffusion capacity, were observed after controlled exposures to
carbonaceous car·bo·na·ceous adj. Consisting of, containing, relating to, or yielding carbon. carbonaceous Adjective of, resembling, or containing carbon Adj. 1. UFPs (Anderson et al. 1990; Brown et al. 2002; Chalupa
A chalupa is a kind of tostada platter in Mexican cuisine. et al. 2004; Henneberger et al., 2005; Jaques and Kim 2000; Pekkanen et al. 2002; Pietropaoli et al. 2004; Wichmann et al. 2000). Studies in animals using laboratory-generated model UFPs or ambient UFPs showed that UFPs consistently induced mild yet significant pulmonary inflammatory responses as well as effects in extrapulmonary organs. Animal inhalation studies included the use of different susceptibility models in rodents, with analysis of lung lavage lavage /la·vage/ (lah-vahzh´) 1. the irrigation or washing out of an organ, as of the stomach or bowel. 2. to wash out, or irrigate. lav·age n. parameters and lung histopathology his·to·pa·thol·o·gy n. The science concerned with the cytologic and histologic structure of abnormal or diseased tissue. Histopathology The study of diseased tissues at a minute (microscopic) level. , effects on the blood coagulation cascade, and translocation studies to extrapulmonary tissues (Elder et al. 2000, 2002, 2004; Ferin et al. 1991; Ferin and Oberdorster 1992; Kreyling et al. 2002; Li et al. 1999; Nemmar et al. 1999, 2002a, 2002b, 2003; Oberdorster et al. 1992a, 1995, 2000, 2002, 2004; Semmler et al. 2004; Zhou et al. 2003). In vitro studies using different cell systems showed varying degrees of proinflammatory- and oxidative-stress--related cellular responses after dosing with laboratory-generated or filter-collected ambient UFPs (Brown et al. 2000, 2001; Li et al. 2003). Collectively, the in vitro results have identified oxidative-stress--related changes of gene expression and cell signaling pathways as underlying mechanisms of UFP effects, as well as a role of transition metals and certain organic compounds on combustion-generated UFPs (Figure 3). These can alter cell signaling pathways, including [Ca.sup.2+] signaling and cytokine Cytokine Any of a group of soluble proteins that are released by a cell to send messages which are delivered to the same cell (autocrine), an adjacent cell (paracrine), or a distant cell (endocrine). signaling (e.g., interleukin-8) (Donaldson et al. 2002; Donaldson and Stone 2003). Effects were on a mass basis greater for model UFPs than for fine particles, whereas effects for ambient UFP cellular responses were sometimes greater and sometimes less than those of fine and coarse particles. The interpretation of the in vitro studies is oftentimes difficult because particles of different chemical compositions were used, target cells were different, and duration, end points, and generally high dose levels also differed. Results from high doses in particular should be viewed with caution if they are orders of magnitude higher than predicted from relevant ambient exposures (see "Exposure dose-response considerations," below). [Supplemental Material available online (http://ehp.niehs.nih.gov/members/ 2005/7339/supplemental.pdf).] [FIGURE 3 OMITTED] Concepts of Nanotoxicology Laboratory rodent studies. With respect to potential health effects of NSPs, two examples should serve to illustrate a) that NSPs have a higher inflammatory potential per given mass than do larger particles, provided they are chemically the same, and b) that NSPs generated under certain occupational conditions can elicit severe acute lung injury. The first example involves studies with ultrafine and fine titanium dioxide (Ti[O.sub.2]) particles, which showed that ultrafine anatase an·a·tase n. A rare blue or light yellow to brown crystalline mineral, the rarest of three forms of titanium dioxide, TiO2, used as a pigment, especially in paint. Ti[O.sub.2] (20 nm), when instilled intratracheally into rats and mice, induced a much greater pulmonary-inflammatory neutrophil neutrophil /neu·tro·phil/ (noo´tro-fil) 1. a granular leukocyte having a nucleus with three to five lobes connected by threads of chromatin, and cytoplasm containing very fine granules; cf. heterophil. 2. response (determined by lung lavage 24 hr after dosing) than did fine anatase Ti[O.sub.2] (250 nm) when both types of particles were instilled at the same mass dose (Figure 4A,C). However, when the instilled dose was expressed as particle surface area, it became obvious that the neutrophil response in the lung for both ultra-fine and fine Ti[O.sub.2] fitted the same dose-response curve dose-response curve A graphic representation of the effects that varous doses of an agent–eg, ionizing radiation or a chemotherapeutic agent, have on a given parameter–eg, cell viability, mutation frequency, DNA damage, tumor growth or metastasis or (Figure 4B,D), suggesting that particle surface area for particles of different sizes but of the same chemistry, such as Ti[O.sub.2], is a better dosemetric than is particle mass or particle number (Oberdorster G 2000). Moreover, normalizing the particle surface dose to lung weight shows excellent agreement of the inflammatory response in both rats and mice [Figure S-2 in Supplemental Material available online (http://ehp.niehs.nih.gov/ members/2005/7339/supplemental.pdf)]. The better fit of dose-response relationships by expressing the dose as surface area rather than mass when describing toxicologic effects of inhaled solid particles of different sizes has been pointed out repeatedly, especially when particles of different size ranges--nano to fine--were studied (Brown et al. 2001; Donaldson et al. 1998, 2002; Driscoll 1996; Oberdorster and Yu 1990; Oberdorster et al. 1992a; Tran et al. 1998, 2000) [Supplemental Material available online (http://ehp.niehs.nih. gov/members/2005/7339/supplemental.pdf)]. [FIGURE 4 OMITTED] Particle chemistry, and specifically surface chemistry, plays a decisive role in addition to particle size, as shown in the second example: exposure of rats to polytetrafluoroethylene polytetrafluoroethylene a synthetic material commonly used as a nonstick lining in domestic cooking utensils (frypans); abbreviated PTFE; called also Teflon. Overheating produces toxic fumes that cause an acute hemorrhagic pneumonitis and death in small caged birds, which are (PTFE PTFE polytetrafluoroethylene. ) fume fume Occupational medicine A solid suspension resulting from condensation of the products of combustion. See Inhalant Vox populi verbTo be in the midst of a mental mini-meltdown. . PTFE fume (generated by heating PTFE) has long been known to be of high acute toxicity acute toxicity Pharmacology Illness caused by a single exposure to a toxic substance to birds and mammals, including humans (Cavagna et al. 1961; Coleman et al. 1968; Griffith et al. 1973; Nuttall et al. 1964; Waritz and Kwon 1968). Analysis of these fumes fumes odorous gases and other volatile materials; inhalation of irritating fumes causes coughing and, if sufficiently severe, irreversible pulmonary edema. revealed the nanosized nature of the particles generated by heating PTFE to about 480[degrees]C, with a count median diameter (CMD CMD cerebromacular degeneration. ) of 18 nm. They were highly toxic highly toxic Occupational medicine adjective Referring to a chemical that 1. Has a median lethal dose–LD50 of ≤ 50 mg/kg when administered orally to 200-300 g albino rats 2. to rats, causing severe acute lung injury with high mortality within 4 hr after a 15-min inhalation exposure to 50 [micro]g/[m.sup.3] (Oberdorster et al. 1995). This short exposure resulted in an estimated deposited dose in the alveolar alveolar /al·ve·o·lar/ (al-ve´o-lar) [L. alveolaris ] pertaining to an alveolus. al·ve·o·lar adj. Relating to an alveolus. regions of only approximately 60 ng. In humans, acute lung injury, known as polymer fume fever polymer fume fever n. A condition marked by fever, pain in the chest, and cough caused by the inhalation of fumes given off by the plastic polytetrafluorethylene when heated. , can result from exposures to PTFE fumes (Auclair et al. 1983; Goldstein et al. 1987; Lee et al. 1997; Williams et al. 1974; Woo et al. 2001). Additional rat studies showed that the gas phase alone was not acutely toxic and that aging of the PTFE fume particles for 3 min increased their particle size to > 100 nm because of accumulation, which resulted in a loss of toxicity (Johnston et al. 2000). However, it is most likely that changes in particle surface chemistry during the aging period contributed to this loss of toxicity, and that this is not just an effect of the accumulated larger particle size [Supplemental Material available online (http://ehp.niehs.nih.gov/ members/2005/7339/supplemental.pdf)]. These examples seem to represent the extremes of NSPs in terms of pulmonary toxicity, one (Ti[O.sub.2]) being rather benign yet still inducing significantly greater inflammatory effects on a mass basis than fine particles of the same chemical makeup, the other (PTFE fumes) inducing very high acute toxicity, possibly related to reactive groups on the large surface per unit mass. Engineered nanomaterials can have very different shapes, for example, spheres, fibers, tubes, rings, and planes. Toxicologic studies of spherical and fibrous particles have well established that natural (e.g., asbestos) and manmade (e.g., biopersistent vitreous vitreous /vit·re·ous/ (vit´re-us) 1. glasslike or hyaline. 2. vitreous body. primary persistent hyperplastic vitreous ) fibers are associated with increased risks of pulmonary fibrosis Pulmonary Fibrosis Definition Pulmonary fibrosis is scarring in the lungs. Description Pulmonary fibrosis develops when the alveoli, tiny air sacs that transfer oxygen to the blood, become damaged and inflamed. and cancer after prolonged exposures [Greim et al. 2001; International Agency for Research on Cancer The International Agency for Research on Cancer (IARC, or CIRC in its French acronym) is an intergovernmental agency forming part of the World Health Organisation of the United Nations. Its main offices are in Lyon, France. (IARC) 2002]. Critical parameters are the three Ds: dose, dimension, and durability of the fibers. Fibers are defined as elongated e·lon·gate tr. & intr.v. e·lon·gat·ed, e·lon·gat·ing, e·lon·gates To make or grow longer. adj. or elongated 1. Made longer; extended. 2. Having more length than width; slender. structures with a diameter-to-length ratio (aspect ratio) of 1:3 or greater and with a length of > 5 [micro]m and diameter [less than or equal to] 3 [micro]m [World Health Organization (WHO) 1985]. Carbon nanotubes have aspect ratios of up to [greater than or equal to] 100, and length can exceed 5 [micro]m with diameters ranging from 0.7 to 1.5 nm for single-walled nanotubes, and 2 to 50 nm for multiwalled nanotubes. Results from three studies using intratracheal dosing of carbon nanotubes in rodents indicate significant acute inflammatory pulmonary effects that either subsided in rats (Warheit et al. 2004) or were more persistent in mice (Lam et al. 2004; Shvedova et al. 2004b). Administered doses were very high, ranging from 1 to 5 mg/kg in rats; in mice doses ranged from 3.3 to 16.6 mg/kg (Lam et al. 2004) or somewhat lower, from 0.3 to 1.3 mg/kg (Shvedova et al. 2004a). Granuloma granuloma /gran·u·lo·ma/ (gran?u-lo´mah) pl. granulomas, granulo´mata an imprecise term for (1) any small nodular delimited aggregation of mononuclear inflammatory cells, or (2) such a collection of modified macrophages formation as a normal foreign body response of the lung to high doses of a persistent particulate material was a consistent finding in these studies. Metal impurities (e.g., iron) from the nanotube A carbon molecule that resembles a cylinder made out of chicken wire one to two nanometers in diameter by any number of millimeters in length. Accidentally discovered by a Japanese researcher at NEC in 1990 while making Buckyballs, they have potential use in many applications. generation process may also have contributed to the observed effects. Although these in vivo first studies revealed high acute effects, including mortality, this was explained by the large doses of the instilled highly aggregated nanotubes that caused death by obstructing the airways and should not be considered a nanotube effect per se (Warheit et al. 2004). In vitro studies with carbon nanotubes also reported significant effects. Dosing keratinocytes Keratinocytes Cells found in the epidermis. The keratinocytes at the outer surface of the epidermis are dead and form a tough protective layer. The cells underneath divide to replenish the supply. and bronchial bronchial /bron·chi·al/ (brong´ke-al) pertaining to or affecting one or more bronchi. bron·chi·al adj. Relating to the bronchi, the bronchial tubes, or the bronchioles. epithelial cells Epithelial cells Cells that form a thin surface coating on the outside of a body structure. Mentioned in: Corneal Transplantation in vitro with single-walled carbon nanotubes (SWNTs) resulted in oxidative stress, as evidenced by the formation of free radicals, accumulation of peroxidative products, and depletion of cell antioxidants Antioxidants Substances that reduce the damage of the highly reactive free radicals that are the byproducts of the cells. Mentioned in: Aging, Nutritional Supplements antioxidants, n. (Shvedova et al. 2004a, 2004b). Multiwalled carbon nanotubes (MWNTs) showed proinflammatory effects and were internalized in keratinocytes (Monteiro-Riviere et al. 2005). Again, the relatively high doses applied in these studies need to be considered when discussing the relevancy of these findings for in vivo exposures. A most recent study in macrophages Macrophages White blood cells whose job is to destroy invading microorganisms. Listeria monocytogenes avoids being killed and can multiply within the macrophage. comparing SWNTs and MWNTs with [C.sub.60] fullerenes found a cytotoxicity ranking on a mass basis in the order SWNT SWNT Single-Walled Nanotube > MWNT MWNT Multi-Walled Nanotube > [C.sub.60]. Profound cytotoxicity (mitochondrial function, cell morphology, phagocytic phag·o·cyt·ic adj. 1. Of or relating to phagocytes. 2. Of, relating to, or characterized by phagocytosis. phagocytic emanating from or pertaining to phagocytes. function) was seen for SWNTs, even at a low concentration of 0.38 [micro]g/[cm.sup.2]. The possible contribution of metal impurities of the nanotubes still needs to be assessed. Therefore, whether the generally recognized principles of fiber toxicology apply to these nanofiber structures needs still to be determined (Huczko et al. 2001). Future studies should be designed to investigate both effects and also the fate of nanotubes after deposition in the respiratory tract, preferentially by inhalation using well-dispersed (singlet) airborne nanotubes. In order to design the studies using appropriate dosing, it is necessary to assess the likelihood and degree of human exposure. It is of utmost importance to characterize human exposures in terms of the physicochemical nature, the aggregation state, and concentration (number, mass, surface area) of engineered nanomaterials and perform animal and in vitro studies accordingly. If using direct instillation into the lower respiratory tract Noun 1. lower respiratory tract - the bronchi and lungs lung - either of two saclike respiratory organs in the chest of vertebrates; serves to remove carbon dioxide and provide oxygen to the blood , a large range of doses, which include expected realistic exposures of appropriately prepared samples, needs to be considered [Supplemental Material available online (http://ehp.niehs.nih.gov/members/2005/ 7339/supplemental.pdf)]. Ecotoxicologic studies. Studies have been carried out to date on only a few species that have been accepted by regulatory agencies as models for defining ecotoxicologic effects. Tests with uncoated, water-soluble, colloidal colloidal of the nature of a colloid. colloidal bath a bath containing gelatin, bran, starch or similar substances, to relieve skin irritation and pruritus. fullerenes (n[C.sub.60]) show that the 48-hr L[C.sub.50] (median lethal concentration) in Daphnia magna is 800 ppb (Oberdorster E 2004b), using standard U.S. EPA protocols (U.S. EPA 1994). In largemouth bass largemouth bass see micropterus salmoides. (Micropterus salmoides Micropterus salmoides finfish in family Centrarchidae. Called also largemouth bass. See Table 23. ), although no mortality was seen, lipid peroxidation in the brain and glutathione glutathione: see coenzyme. depletion in the gill were observed after exposure to 0.5 ppm n[C.sub.60] for 48 hr (Oberdorster E 2004a). There are several hypotheses as to how lipid damage may have occurred in the brain, including direct redox redox (rē`dŏks): see oxidation and reduction. activity by fullerenes reaching the brain via circulation or axonal axonal pertaining to or arising from an axon. axonal degeneration an axon dies and cannot be replaced if its cell body is destroyed. translocation (see also "Disposition of NSPs in the respiratory tract," below) and dissolving into the lipid-rich brain tissue; oxyradical production by microglia microglia /mi·crog·lia/ (mi-krog´le-ah) small nonneural cells forming part of the supporting structure of the central nervous system. They are migratory and act as phagocytes to waste products of nerve tissue. , or reactive fullerene fullerene, any of a class of carbon molecules in which the carbon atoms are arranged into 12 pentagonal faces and 2 or more hexagonal faces to form a hollow sphere, cylinder, or similar figure. metabolites Metabolites Substances produced by metabolism or by a metabolic process. Mentioned in: Interactions may be produced by cytochrome cytochrome (sī`təkrōm'), protein containing heme (see coenzyme) that participates in the phase of biochemical respiration called oxidative phosphorylation. P450 metabolism. Initial follow-up studies using suppressive sup·pres·sive adj. Tending or serving to suppress. Adj. 1. suppressive - tending to suppress; "the government used suppressive measures to control the protest" subtractive sub·trac·tive adj. 1. Producing or involving subtraction. 2. Of or being a color produced by light passing through or reflecting off a colorant, such as a filter or pigment, that absorbs certain wavelengths and transmits or hybridization hybridization /hy·brid·iza·tion/ (hi?brid-i-za´shun) 1. crossbreeding; the act or process of producing hybrids. 2. molecular hybridization 3. of pooled control fish versus pooled 0.5-ppm-exposed fish liver mRNA were also performed. Proteins related to immune responses and tissue repair were up-regulated, and several proteins related to homeostatic homeostatic pertaining to homeostasis. control and immune control were down-regulated. A cytochrome P450 (CYP CYP In currencies, this is the abbreviation for the Cyprus Pound. Notes: The currency market, also known as the Foreign Exchange market, is the largest financial market in the world, with a daily average volume of over US $1 trillion. 2K4) involved in lipid metabolism was up-regulated ]Supplemental Material available online (http://ehp.niehs.nih. gov/members/2005/7339/supplemental.pdf)]. In addition to these biochemical and molecular-level changes in fish, bactericidal bactericidal /bac·te·ri·ci·dal/ (bak-ter?i-si´d'l) destructive to bacteria. Bactericidal An agent that destroys bacteria (e.g. properties of fullerenes have also been reported and are being explored as potential new antimicrobial agents (Yamakoshi et al. 2003). Engineered nanomaterials used as antimicrobials may shift microbial microbial pertaining to or emanating from a microbe. microbial digestion the breakdown of organic material, especially feedstuffs, by microbial organisms. communities if they are released into the environment via effluents. As we know from anthropogenic endocrine-disrupting compounds, interference of signaling between nitrogen-fixing bacteria and their plant hosts could be extremely harmful both ecologically and economically in terms of crop production (Fox et al. 2001). Aqueous fullerenes and coated SWNTs are stable in salt solutions (Cheng et al. 2004; Warheit et al. 2004), cell culture media (Lu et al. 2004; Sayes et al. 2004), reconstituted hard water, and MilliQ water (Dieckmann et al. 2003; Oberdorster E 2004a, 2004b). NSPs will tend to sorb onto sediment and soil particles and be immobilized because of their high surface area:mass ratio (Lecoanet and Wiesner 2004). Biologic transport would occur from ingested sediments, and one would expect movement of nanomaterials through the food chain (Figure 5). [FIGURE 5 OMITTED] To make engineered nanomaterials more biocompatible biocompatible /bio·com·pat·i·ble/ (-kom-pat´i-b'l) being harmonious with life; not having toxic or injurious effects on biological function. , both surface coatings and covalent co·va·lent adj. Of or relating to a chemical bond characterized by one or more pairs of shared electrons. surface modifications have been incorporated. Some studies have shown that both the surface coating and the covalent modifications can be weathered either by exposure to the oxygen in air or by ultraviolet (UV) irradiation for 1-4 hr (Derfus et al. 2004; Rancan et al. 2002). Therefore, although coatings and surface modifications may be critically important in drug-delivery devices, the likelihood of weathering under environmental conditions makes it important to study toxicity under UV and air exposure conditions. Even coatings used in drug delivery of NPs may not be bio-persistent or could be metabolized to expose the core NP material [Supplemental Material available online (http://ehp.niehs.nih.gov/ members/2005/7339/supplemental.pdf)]. Reactive oxygen species reactive oxygen species, n molecules and ions of oxygen that have an unpaired electron, thus rendering them extremely reactive. Many cellular structures are susceptible to attack by ROS contributing to cancer, heart disease, and cerebrovascular disease. mechanisms of NSP toxicity. Both in vivo and in vitro, NSPs of various chemistries have been shown to create reactive oxygen species (ROS ROS, n.pr See reactive oxygen species. ). ROS production has been found in NPs as diverse as [C.sub.60] fullerenes, SWNTs, quantum dots, and UFPs, especially under concomitant exposure to light, UV, or transition metals (Brown et al. 2000, 2001; Derfus et al. 2004; Joo et al. 2004; Li et al. 2003; Nagaveni et al. 2004; Oberdorster E 2004a; Rancan et al. 2002; Sayes et al. 2004; Shvedova et al. 2004a, 2004b; Wilson et al. 2002; Yamakoshi et al. 2003). It has been demonstrated that NSPs of various sizes and various chemical compositions preferentially mobilize to mitochondria (de Lorenzo 1970; Foley et al. 2002; Gopinath et al. 1978; Li et al. 2003; Rodoslav et al. 2003). Because mitochondria are redox active organdies, there is a likelihood of altering ROS production and thereby overloading or interfering with antioxidant defenses (Figure 3). Figure 6 diagrams some of the antioxidant defense systems that occur in animals, and possible areas where NSPs may create oxyradicals. The [C.sub.60] fullerene is shown as a model NP producing superoxide superoxide /su·per·ox·ide/ (-ok´sid) any compound containing the highly reactive and extremely toxic oxygen radical O2-, a common intermediate in numerous biological oxidations. su·per·ox·ide n. , as has been shown by Yamakoshi et al. (2003). The exact mechanism by which each of these diverse NPs cause ROS is not yet fully understood, but suggested mechanisms include a) photo excitation of fullerenes and SWNTs, causing intersystem crossing to create free electrons; b) metabolism of NPs to create redox active intermediates, especially if metabolism is via cytochrome P450s; and c) inflammation responses in vivo that may cause oxyradical release by macrophages. Other mechanisms will likely emerge as studies on NP toxicity continue. [FIGURE 6 OMITTED] The small size and respective large specific surface area of NPs, like those of ambient airborne UFPs, give them unique properties with respect to a potential to cause adverse effects. Certainly, as shown in studies with UFPs, chemical composition and other particle parameters are additional important effect modifiers. Results from these studies will therefore serve as a basis for future studies in the field of nanotoxicology, for example, the propensity of NSPs to translocate trans·lo·cate v. 1. To change from one place or one position to another; to displace. 2. To transfer a chromosomal segment to a new position; to cause to undergo translocation. across cell layers and along neuronal pathways (see "Disposition of NSPs in the respiratory tract" below). Exposure dose-response considerations. A careful evaluation of exposure-dose-response relationships is critical to the toxicologic assessment of NSPs. This includes not only questions about the dosemetric--mass, number, or surface of the particles, as discussed above--but most important, also the relevance of dose levels. For example, it is tempting, and a continual practice, to dose primary cells or cell lines in vitro with very high doses without any consideration or discussion of realistic in vivo exposures; for instance, 100 [micro]g NSPs/mL culture medium--labeled as a low dose--is extremely high and is unlikely to be encountered in vivo. Likewise, intratracheal instillations of several hundred micrograms into a rat does not resemble a relevant in vivo inhalation exposure; both dose and dose rate cause high bolus bolus /bo·lus/ (bo´lus) 1. a rounded mass of food or pharmaceutical preparation ready to swallow, or such a mass passing through the gastrointestinal tract. 2. a concentrated mass of pharmaceutical preparation, e. dose artifacts artifacts see specimen artifacts. . Although such studies may be used in a first proof-of-principle approach, it is mandatory to follow up and validate results using orders of magnitude lower concentrations resembling realistic in vivo exposures, including worst-case scenarios. The 500-year-old phrase "the dose makes the poison" can also be paraphrased as "the dose makes the mechanism." The mechanistic pathways that operate at low realistic doses are likely to be different from those operating at very high doses when the cell's or organism's defenses are overwhelmed. Therefore, in vivo and in vitro studies will provide useful data on the toxicity and mode of action of NSPs only if justifiable concentrations/doses are considered when designing such studies. This approach is particularly important for the proper identification of the dose-response curve. When data are generated only at high concentrations/doses, it is difficult to determine whether the dose-response curve in question is best described by a linear (no threshold), supralinear, threshold, or hormetic model (Figure 7). Study designs should include doses that most closely reflect the expected exposure levels. A critical gap that urgently needs to be filled in this context is the complete lack of data for human or environmental exposure levels of NSPs. Furthermore, some knowledge about the biokinetics of NSPs is required in order to estimate appropriate doses. [FIGURE 7 OMITTED] Do specific NPs reach certain target sites? If so, what are the doses, dose rates, and their persistence? Further, although it may be tempting to extrapolate extrapolate - extrapolation from in vitro results to an in vivo risk assessment, it is important to keep in mind that in vitro tests are most useful in providing information on mechanistic processes and in elucidating mechanisms/mode of actions suggested by studies in whole animals. A combination of in vitro and in vivo studies with relevant dose levels will be most useful in identifying the potential hazards of NPs, and a thorough discussion and justification of selected dose levels should be mandatory. Portals of Entry and Target Tissues Most of the toxicity research on NSPs in vivo has been carried out in mammalian systems, with a focus on respiratory system respiratory system: see respiration. respiratory system Organ system involved in respiration. In humans, the diaphragm and, to a lesser extent, the muscles between the ribs generate a pumping action, moving air in and out of the lungs through a exposures for testing the hypothesis that airborne UFPs cause significant health effects. With respect to NPs, other exposure routes, such as skin and GI tract, also need to be considered as potential portals of entry. Portal-of-entry-specific defense mechanisms protect the mammalian organism from harmful materials. However, these defenses may not always be as effective for NSPs, as is discussed below. Respiratory Tract In order to appreciate what dose the organism receives when airborne particles are inhaled, information about their deposition as well as their subsequent fate is needed. Here we focus on the fate of inhaled nanosized materials both within the respiratory tract itself and translocated out of the respiratory tract. There are significant differences between NSPs and larger particles regarding their behavior during deposition and clearance in the respiratory tract [Supplemental Material available online (http://ehp.niehs.nih.gov/members/2005/ 7339/supplemental.pdf)]. Efficient deposition of inhaled NSPs. The main mechanism for deposition of inhaled NSPs in the respiratory tract is diffusion due to displacement when they collide with air molecules. Other deposition mechanisms of importance for larger particles, such as inertial impaction, gravitational grav·i·ta·tion n. 1. Physics a. The natural phenomenon of attraction between physical objects with mass or energy. b. The act or process of moving under the influence of this attraction. 2. settling, and interception, do not contribute to NSP deposition, and electrostatic precipitation occurs only in cases where NSPs carry significant electric charges. Figure 8 shows the fractional deposition of inhaled particles in the nasopharyngeal nasopharyngeal pertaining to the nasal and pharyngeal cavities. nasopharyngeal meatus see nasopharyngeal meatus. nasopharyngeal spasm see reverse sneeze. , tracheobronchial tracheobronchial /tra·cheo·bron·chi·al/ (-brong´ke-al) pertaining to the trachea and bronchi. tra·che·o·bron·chi·al adj. Of or relating to the trachea and the bronchi. , and alveolar regions of the human respiratory tract under conditions of nose breathing during rest, based on a predictive mathematical model (International Commission on Radiological Protection The International Commission on Radiological Protection (ICRP) is an advisory body providing recommendations and guidance on radiation protection; It was founded in 1928 by the International Society of Radiology (ISR) and was then called the ‘International X-ray and Radium 1994). These predictions apply to particles that are inhaled as singlet particles of a given size and not as aggregates; the latter obviously will have larger particle size and different deposition site. In each of the three regions of the respiratory tract, significant amounts of a certain size of NSPs (1-100 nm) are deposited. For example, 90% of inhaled 1-nm particles are deposited in the nasopharyngeal compartment, only approximately 10% in the tracheobronchial region, and essentially none in the alveolar region. On the other hand, 5-nm particles show about equal deposition of approximately 30% of the inhaled particles in all three regions; 20-nm particles have the highest deposition efficiency in the alveolar region (~ 50%), whereas in tracheobronchial and nasopharyngeal regions this particle size deposits with approximately 15% efficiency. These different deposition efficiencies should have consequences for potential effects induced by inhaled NSPs of different sizes as well as for their disposition to extrapulmonary organs, as discussed further below. [FIGURE 8 OMITTED] Disposition of NSPs in the respiratory tract. In the preceding section we summarized data demonstrating that inhaled NSPs of different sizes can target all three regions of the respiratory tract. Several defense mechanisms exist throughout the respiratory tract aimed at keeping the mucosal surfaces free from cell debris and particles deposited by inhalation. Several reviews describe the well-known classic clearance mechanisms and pathways for deposited particles (Kreyling and Scheuch 2000; Schlesinger et al. 1997; U.S. EPA 2004), so here we only briefly mention those mechanisms and point out specific differences that exist with respect to inhaled NSPs [Supplemental Material available online (http://ehp.niehs.nih.gov/members/2005/ 7339/supplemental.pdf)]. Once deposited, NSPs--in contrast to larger-sized particles--appear to translocate readily to extrapulmonary sites and reach other target organs by different transfer routes and mechanisms. One involves transcytosis across epithelia of the respiratory tract into the interstitium and access to the blood circulation directly or via lymphatics Lymphatics Channels that are conduits for lymph. Mentioned in: Colon Cancer, Rectal Cancer , resulting in distribution throughout the body. The other is a not generally recognized mechanism that appears to be distinct for NSPs and that involves their uptake by sensory nerve sensory nerve n. An afferent nerve conveying impulses that are processed by the central nervous system to become part of the organism's perception of itself and of its environment. endings embedded in airway epithelia, followed by axonal translocation to ganglionic ganglionic /gan·gli·on·ic/ (-on´ik) pertaining to a ganglion. gan·gli·on·ic adj. Relating to a ganglion; ganglial. ganglionic pertaining to a ganglion. and CNS structures. Classical clearance pathways. The clearance of deposited particles in the respiratory tract is basically due to two processes (Table 3): a) physical translocation of particles by different mechanisms and b) chemical clearance processes. Leaching refers to loss of elements from a particle matrix (e.g., loss of sodium from asbestos fibers due to dissolution in intra- or extracellular milieu). Chemical dissolution is directed at biosoluble particles or components of particles that are either lipid soluble or soluble in intracellular and extracellular fluids. Solutes and soluble components can then undergo absorption and diffusion or binding to proteins and other subcellular structures and may be eventually cleared into blood and lymphatic circulation. Chemical clearance for biosoluble materials can happen at any location within the three regions of the respiratory tract, although to different degrees, depending on local extracellular and intracellular conditions (pH). In contrast, a number of diverse processes involving physical translocation of inhaled particles exist in the respiratory tract and are different in the three regions. Figure 9 summarizes these clearance processes for solid particles. As discussed further below, some of them show significant particle-size-dependent differences, making them uniquely effective for a certain particle size but very inefficient for other sizes. [FIGURE 9 OMITTED] The most prevalent mechanism for solid particle clearance in the alveolar region is mediated by alveolar macrophages, through phagocytosis phagocytosis: see endocytosis. Phagocytosis A mechanism by which single cells of the animal kingdom, such as smaller protozoa, engulf and carry particles into the cytoplasm. of deposited particles. The success of macrophage-particle encounter appears to be facilitated by chemotactic che·mo·tac·tic adj. Of or relating to chemotaxis. attraction of alveolar macrophages to the site of particle deposition (Warheit et al. 1988). The chemotactic signal is most likely complement protein 5a (C5a), derived from activation of the complement cascade complement cascade Immunology A complex, multimolecular biologic system with ± 25 different proteins that self-assemble on cell surfaces, functioning in concert with the specific immune systems to mediate host reactions and anti-microbial defense; the coup from serum proteins present on the alveolar surface (Warheit et al. 1986; Warheit and Hartsky 1993). This is followed by gradual movement of the macrophages with internalized particles toward the mucociliary escalator. The retention half-time of solid particles in the alveolar region based on this clearance mechanism is about 70 days in rats and up to 700 days in humans. The efficacy of this clearance mechanism depends highly on the efficiency of alveolar macrophages to "sense" deposited particles, move to the site of their deposition, and then phagocytize phag·o·cy·tize v. To ingest by phagocytosis; phagocytose. phagocytize phagocytose. them. This process of phagocytosis of deposited particles takes place within a few hours, so by 6-12 hr after deposition essentially all of the particles are phagocytized by alveolar macrophages, to be cleared subsequently by the slow alveolar clearance mentioned above. However, it appears that there are significant particle-size-dependent differences in the cascade of events leading to effective alveolar macrophage-mediated clearance. Figure 10 displays results of several studies in which rats were exposed to different-sized particles (for the 3- and 10-[micro]m particles, 10-[micro]g and 40-[micro]g polystyrene beads, respectively, were instilled intratracheally) (Kreyling et al. 2002; Oberdorster et al. 1992b, 2000; Semmler et al. 2004). Twenty-four hours later, the lungs of the animals were lavaged repeatedly, retrieving about 80% of the total macrophages as determined in earlier lavage experiments (Ferin et al. 1991). As shown in Figure 10, approximately 80% of 0.5-, 3-, and 10-[micro]m particles could be retrieved with the macrophages, whereas only approximately 20% of nanosized 15-20-nm and 80-nm particles could be lavaged with the macrophages. In effect, approximately 80% of the UFPs were retained in the lavaged lung after exhaustive lavage, whereas approximately 20% of the larger particles > 0.5 [micro]m remained in the lavaged lung. This indicates that NSPs either were in epithelial cells or had further translocated to the interstitium [Supplemental Material available online (http://ehp.niehs.nih. gov/members/2005/7339/supplemental.pdf)]. [FIGURE 10 OMITTED] Epithelial translocation. Because of the apparent inefficiency of alveolar macrophage phagocytosis of NSPs, one might expect that these particles interact instead with epithelial cells. Indeed, results from several studies show that NSPs deposited in the respiratory tract readily gain access to epithelial and interstitial sites. This was also shown in studies with ultrafine PTFE fumes: shortly after a 15-min exposure, the fluorine-containing particles could be found in interstitial and submucosal submucosal /sub·mu·co·sal/ (-mu-ko´sal) 1. pertaining to the submucosa. 2. beneath a mucous membrane. sites of the conducting airways as well as in the interstitium of the lung periphery close to the pleura pleura (pl  r`ə), membranous lining of the upper body cavity and covering for the lungs. (Oberdorster G 2000). Such interstitial translocation represents a shift
in target site away from the alveolar space to the interstitium,
potentially causing direct particle-induced effects there.In a study evaluating the pulmonary inflammatory response of Ti[O.sub.2] particles, ranging from NP Ti[O.sub.2] to pigment-grade Ti[O.sub.2] (12-250 nm), a surprising finding was that, 24 hr after intratracheal instillation of different doses, higher doses induced a lower effect (Oberdorster et al. 1992a). This was explained by the additional finding that at the higher doses (expressed as particle surface area) of the nanosized Ti[O.sub.2], [greater than or equal to] 50% had reached the pulmonary interstitium, causing a shift of the inflammatory cell response from the alveolar space to the interstitium [Supplemental Material available online (http://ehp.niehs.nih. gov/members/2005/7339/supplemental.pdf)]. The smaller particle size of 12 and 20 nm versus 220 and 250 nm also means that the administered particle number was more than three orders of magnitude higher for the NSPs, a factor that seems to be an important determinant for particle translocation across the alveolar epithelium, as are the delivered total dose and the dose rate (Ferin et al. 1992). Because interstitial translocation of fine particles across the alveolar epithelium is more prominent in larger species (dogs, nonhuman primates) than in rodents (Kreyling and Scheuch 2000; Nikula et al. 1997), it is reasonable to assume that the high translocation of NSPs observed in rats occurs in humans as well [Supplemental Material available online (http://ehp.niehs.nih. gov/members/2005/7339/supplemental.pdf)]. Translocation to the circulatory system. Once the particles have reached pulmonary interstitial sites, uptake into the blood circulation, in addition to lymphatic pathways, can occur; again, this pathway is dependent on particle size, favoring NSPs. Berry et al. (1977) were the first to describe translocation of NSPs across the alveolar epithelium using intratracheal instillations of 30-nm gold particles in rats. Within 30 min postexposure, they found large amounts of these particles in platelets of pulmonary capillaries; the researchers suggested that this is an elimination pathway for inhaled particles that is significant for transporting the smallest air pollutant particles--in particular, particles of tobacco smoke--to distant organs. They also hypothesized that this "might predispose pre·dis·pose v. To make susceptible, as to a disease. to platelet aggregation with formation of microthrombi atheromatous ath·er·o·ma n. pl. ath·er·o·mas or ath·er·o·ma·ta A deposit or degenerative accumulation of lipid-containing plaques on the innermost layer of the wall of an artery. plaques" (Berry et al. 1977). Since then, a number of studies with different particle types have confirmed the existence of this translocation pathway, as summarized in Table 4. Collectively, these studies indicate that particle size and surface chemistry (coating), and possibly charge, govern translocation across epithelial and endothelial endothelial /en·do·the·li·al/ (-the´le-al) pertaining to or made up of endothelium. Endothelial A layer of cells that lines the inside of certain body cavities, for example, blood vessels. cell layers. In particular, the studies summarized by Mehta et al. (2004) and those performed by Heckel et al. (2004) using intravenous administration of albumin-coated gold nanoparticles in rodents demonstrated receptor-mediated transcytosis (albumin-binding proteins) via caveolae (Figure 11). These 50-100 nm vesicles, first described by Simionescu et al. (1975), form from indentations of the plasmalemma plasmalemma /plas·ma·lem·ma/ (-lem´ah) 1. plasma membrane. 2. a thin peripheral layer of the ectoplasm in a fertilized egg. plas·ma·lem·ma n. See cell membrane. and are coated with the caveolin-1 protein. Albumin, as the most abundant protein in plasma and interstitium, appears to facilitate NP endocytosis, as does lecithin lecithin Any of a class of phospholipids (also called phosphatidyl cholines) important in cell structure and metabolism. They are composed of phosphate, choline, glycerol (as the ester), and two fatty acids. Various fatty acids pairs distinguish the various lecithins. , a phospholipid phospholipid (fŏs'fōlĭp`ĭd), lipid that in its simplest form is composed of glycerol bonded to two fatty acids and a phosphate group. : even 240-nm polystyrene particles translocated across the alveolo-capillary barrier when coated with lecithin, whereas uncoated particles did not (Kato et al. 2003). The presence of both albumin and phospholipids in alveolar epithelial lining fluid may, therefore, be important constituents for facilitated epithelial cell uptake of NSPs after deposition in the alveolar space. [FIGURE 11 OMITTED] Rejman et al. (2004) reviewed a number of different endocytic pathways for internalization Internalization A decision by a brokerage to fill an order with the firm's own inventory of stock. Notes: When a brokerage receives an order they have numerous choices as to how it should be filled. of a variety of substances, including phagocytosis, macropinocytosis, clathrin-mediated endocytosis, and caveolae-mediated endocytosis. They found in nonphagocytic cells in vitro that internalization via clathrin-coated pits prevailed for latex microspheres < 200 nm, whereas with increasing size up to 500 nm, caveolae became the predominant pathway. However, as shown in Table 4, surface coating of NSPs with albumin clearly causes even the smallest particles to be internalized via caveolae. The presence of caveolae on cells differs: they are abundant in lung capillaries and alveolar type l cells but not in brain capillaries (Gumbleton 2001). In the lung, during inspiratory in·spi·ra·to·ry adj. Of, relating to, or used for the drawing in of air. inspiratory pertaining to or used in the inspiration of air into the lungs. expansion and expiratory ex·pi·ra·to·ry adj. Of, relating to, or involving the expiration of air from the lungs. expiratory relating to or employed in the expiration of air from the lungs. contraction of the alveolar walls, caveolae with openings around 40 nm disappear and reappear, forming vesicles that are thought to function as transport pathways across the cells for macromolecules Macromolecules A large molecule composed of thousands of atoms. Mentioned in: Gene Therapy macromolecules (Patton 1996). Knowledge from virology virology, study of viruses and their role in disease. Many viruses, such as animal RNA viruses and viruses that infect bacteria, or bacteriophages, have become useful laboratory tools in genetic studies and in work on the cellular metabolic control of gene expression about cell entry of biologic NSPs (viruses) via clathrin-coated pits and caveolae mechanisms should also be considered (Smith and Helenius 2004) and can shed light on the mechanism by which engineered NPs may enter cells and interact with subcellular structures. Evidence in humans for the translocation of inhaled NSPs into the blood circulation is ambiguous, with one study showing rapid appearance in the blood and significant accumulation of label in the liver of humans inhaling [sup.99]Tc-labeled 20-nm carbon particles (Nemmar et al. 2002a), whereas another study using the same labeled particles reported no such accumulation (Brown et al. 2002). Taking into consideration all of the evidence from animal and human studies for alveolar translocation of NSPs, it is likely that this pathway also exists in humans; however, the extent of extrapulmonary translocation is highly dependent on particle surface characteristics/chemistry, in addition to particle size. Translocation to the blood circulation could provide a mechanism for a direct particle effect on the cardiovascular system as an explanation for epidemiologic findings of cardiovascular effects associated with inhaled ambient UFPs (Pekkanen et al. 2002; Wichmann et al. 2000) and for results of clinical studies showing vascular responses to inhaled elemental carbon UFPs (Pietropaoli et al. 2004). In addition to direct alveolar translocation of NSPs, cardiovascular effects may also be the corollary of a sequence of events starting with particle-induced alveolar inflammation initiating a systemic acute phase response acute phase response n. A group of physiologic changes that occur shortly after the onset of an infection or other inflammatory process and include an increase in the blood level of various proteins, especially C-reactive protein, fever, and other with changes in blood coagulability coagulability /co·ag·u·la·bil·i·ty/ (ko-ag?u-lah-bil´it-e) the capability of forming or of being formed into clots. coagulability the state of being capable of forming or of being formed into clots. and resulting in cardiovascular effects (Seaton et al. 1995). Once NSPs have translocated to the blood circulation, they can he distributed throughout the body. The liver is the major distribution site via uptake by Kupffer cells, followed by the spleen as another organ of the reticulo-endothelial system, although coating with polyethylene glycol (PEG) almost completely prevents hepatic and splenic splenic /splen·ic/ (splen´ik) pertaining to the spleen. splen·ic adj. Of, in, near, or relating to the spleen. splenic pertaining to the spleen. localization Customizing software and documentation for a particular country. It includes the translation of menus and messages into the native spoken language as well as changes in the user interface to accommodate different alphabets and culture. See internationalization and l10n. so that other organs can be targeted (Akerman et al. 2002). Distribution to heart, kidney, and immune-modulating organs (spleen, bone marrow) has been reported. For example, several types of NPs, ranging from 10 to 240 nm, localized to a significant degree in bone marrow after intravenous injection into mice (Table 5). Such target specificity may be extremely valuable for drug delivery; for example, drug delivery to the CNS via blood-borne NPs requires NP surface modifications in order to facilitate translocation across the tight blood-brain barrier via specific receptors (e.g., apolipoprotein apolipoprotein /apo·lipo·pro·tein/ (ap?o-lip?o-pro´ten) any of the protein constituents of lipoproteins, grouped by function in four classes, A, B, C, and E. ap·o·lip·o·pro·tein n. coating for LDL-receptor-mediated endocytosis in brain capillaries) (Kreuter 2001, 2004; Kreuter et al. 2002). Such highly desirable properties of NPs must be carefully weighed against potential adverse cellular responses of targeted NP drug delivery, and a rigorous toxicologic assessment is mandatory [Supplemental Material available online (http://ehp.niehs.nih.gov/members/ 2005/7339/supplemental.pdf)]. Neuronal uptake and translocation. A translocation pathway for solid particles in the respiratory tract involving neuronal axons is apparently specific for NSPs. Respective studies are summarized in Table 6. This pathway was described > 60 years ago, yet it has received little or no attention from toxicologists. This pathway, shown in Figure 9 for the nasal and tracheobronchial regions, comprises sensory nerve endings of the olfactory olfactory /ol·fac·to·ry/ (ol-fak´ter-e) pertaining to the sense of smell. ol·fac·to·ry adj. Of, relating to, or contributing to the sense of smell. and the trigeminus tri·gem·i·nus n. See trigeminal nerve. nerves and an intricate network of sensory nerve endings in the tracheobronchial region. These early studies concerned a large series of studies with 30-nm polio virus intranasally instilled into chimpanzees and rhesus monkeys (Bodian and Howe 1941a, 1941b; Howe and Bodian 1940). Their studies revealed that the olfactory nerve and olfactory bulbs are, indeed, portals of entry to the CNS for intranasally instilled nanosized polio virus particles, which could subsequently be recovered from the olfactory bulbs. The close proximity of nasal olfactory mucosa and olfactory bulb requires only a short distance to be covered by neuronal transport (Figure 12). Bodian and Howe (1941b) determined the transport velocity of the virus in the axoplasm of axons to be 2.4 mm/hr, which is very well in agreement with neuronal transport velocities measured later by Adams and Bray (1983) for solid particles (up to 500 nm) directly microinjected into giant axons of crabs, and by de Lorenzo (1970) for silver-coated colloidal gold (50 nm) in squirrel monkeys. [FIGURE 12 OMITTED] The de Lorenzo (1970) study demonstrated in squirrel monkeys that intranasally instilled silver-coated colloidal gold particles (50 nm) translocated anterogradely in the axons of the olfactory nerves to the olfactory bulbs. The 50-nm gold particles even crossed synapses in the olfactory glomerulus glomerulus /glo·mer·u·lus/ (glo-mer´u-lus) pl. glomer´uli [L.] a small tuft or cluster, as of blood vessels or nerve fibers; often used alone to designate one of the renal glomeruli. to reach mitral cell dendrites within 1 hr after intranasal in·tra·na·sal adj. Within the nose. instillation. An interesting finding in this study--and important for potential adverse effects--was that the NSPs in the olfactory bulb were no longer freely distributed in the cytoplasm cytoplasm: see protoplasm. cytoplasm Portion of a eukaryotic cell outside the nucleus. The cytoplasm contains all the organelles (see eukaryote). but were preferentially located in mitochondria (see also "Reactive oxygen species mechanisms of NSP toxicity," above). Newer studies indicated that this translocation pathway is also operational for inhaled NSPs. Inhalation of elemental [sup.13]C UFPs (CMD = 35 nm) resulted in a significant increase of [sup.13]C in the olfactory bulb on day 1, which increased further throughout day 7 post-exposure (Oberd6rster et al. 2004). Results of another inhalation study with solid nanosized (CMD = 30 nm) manganese oxide (Mn[O.sub.2]) particles in rats showed after a 12-day exposure a more than 3.5-fold significant increase of Mn in the olfactory bulb, compared with only a doubling of Mn in the lung. When one nostril nostril /nos·tril/ (nos´tril) either of the nares. nos·tril n. A naris. nostril either of the two apertures (nares) of the nose that lead into the nasal cavity. was occluded during a 6-hr exposure, Mn accumulation in the olfactory bulb was restricted to the side of the open nostril only (Figure 13) (Feikert et al. 2004). This result contrasts with 15-day inhalation of larger-sized Mn[O.sub.2] particles in rats (1.3 and 18 [micro]m mass median aerodynamic diameter) where no significant increases in olfactory Mn was found (Fechter et al. 2002). This was to be expected given that the individual axons of the fila olfactoria (forming the olfactory nerve) are only 100-200 nm in diameter (de Lorenzo 1957; Plattig 1989). [FIGURE 13 OMITTED] Collectively, these studies point out that the olfactory nerve pathway should also be considered a portal of entry portal of entry, n the area in which a microorganism enters the body. They may be cuts, lesions, injection sites, or natural body orifices. to the CNS for humans under conditions of environmental and occupational exposures to airborne NSPs. However, there are important differences between rodents and humans. The olfactory mucosa of the human nose comprises only 5% of the total nasal mucosal surface as opposed to 50% in rats--which in addition are obligatory nose breathers (Table 7). One can argue that the olfactory route may therefore be an important transfer route to the CNS for inhaled NSPs in animals with a well-developed olfaction system, yet at the same time its importance for humans with a more rudimentary olfactory system can be questioned. However, estimates using a predictive particle deposition model and data from Table 7 show that concentrations of 20-nm translocated particles in the human olfactory bulb can, indeed, be 1.6-10 times greater than in rats [Supplemental Material available online (http://ehp.niehs.nih.gov/members/2005/ 7339/supplemental.pdf)]. Translocation into deeper brain structures may possibly occur as well, as shown in rats for soluble Mn (Gianutsos et al. 1997), but requires further confirmatory studies with respect to solid NSPs. Further evidence for movement of NSPs along axons and dendrites in humans is provided by knowledge accumulated by virologists who have long understood the movement of human meningitis virus through olfactory and trigeminal trigeminal /tri·gem·i·nal/ (tri-jem´i-n'l) 1. triple. 2. pertaining to the trigeminal (fifth cranial) nerve. 3. pertaining to trigeminy. tri·gem·i·nal adj. neurons and, similarly, herpes virus movement up and down the trigeminal neuron to trigger outbreaks of herpes cold sores in humans (Kennedy and Chaudhuri 2002; Terasaki et al. 1997). There are additional neuronal translocation pathways for solid NSPs via the trigeminus nerve and tracheobronchial sensory nerves (Table 6). A study by Hunter and Dey (1998) in rats demonstrated the translocation of intranasally instilled rhodamine-labeled microspheres (20-200 nm) to the trigeminal ganglion inside the cranium cranium: see skull. via uptake into the ophthalmic and maxillary max·il·lar·y adj. Of or relating to a jaw or jawbone, especially the upper one. n. A maxillar; a jawbone. maxillary (mak´siler´ē), adj branches of the trigeminus nerve that supplies sensory nerve endings throughout the nasal mucosa. In another study, Hunter and Undem (1999) instilled the same microparticles intratracheally into guinea pigs; they found neuronal translocation of these solid microparticles to the ganglion ganglion: see nervous system. ganglion Aggregate of nerve-cell bodies outside the central nervous system (CNS). The spinal ganglion contains the nerve-cell bodies of the nerve fibres that carry impulses toward the CNS (afferent neurons in dorsal nodosum in the neck area that is networked into the vagal vagal /va·gal/ (va´gal) pertaining to the vagus nerve. va·gal adj. Of or relating to the vagus nerve. vagal pertaining to the vagus nerve. system. This finding may be relevant for ambient UFPs because it can be hypothesized that cardiovascular effects associated with ambient particles in epidemiologic studies (Utell et al. 2002) are in part due to direct effects of translocated UFPs on the autonomic nervous system autonomic nervous system: see nervous system. autonomic nervous system Part of the nervous system that is not under conscious control and that regulates the internal organs. It includes the sympathetic, parasympathetic, and enteric nervous systems. via sensory nerves in the respiratory tract. In the context of potential CNS effects of air pollution, including ambient UFPs, two recent studies with exposures of mice to concentrated ambient fine particles and UFPs should be mentioned. Campbell et al. (2005) and Veronesi et al. (in press) found significant increases of tumor necrosis factor-[alpha] or decreases in dopaminergic neurons, supporting the hypothesis of ambient PM causing neurodegenerative disease. A study by Calderon-Garciduenas et al. (2002) may also point to an interesting link between air pollution and CNS effects: these authors described significant inflammatory or neurodegenerative changes in the olfactory mucosa, olfactory bulb, and cortical and subcortical subcortical /sub·cor·ti·cal/ (-kor´ti-k'l) beneath a cortex, such as the cerebral cortex. brain structures in dogs from a heavily polluted area in Mexico City, whereas these changes were not seen in dogs from a less-polluted rural control city. However, whether direct effects of airborne UFPs are the cause of these effects remains to be determined. Although the existence of neuronal translocation of NSPs has been well established, size alone is only one particle parameter governing this process. Surface characteristics of NSPs (chemistry, charge, shape, aggregation) are essential determinants as well, and it should not be assumed that all NSPs, when inhaled, will be distributed by the mechanism described here. It should be kept in mind, however, that the unique biokinetic behavior of NSPs--cellular endocytosis, transcytosis, neuronal and circulatory translocation and distribution--which makes them desirable for medical therapeutic or diagnostic applications--may be associated with potential toxicity. For example, NP-facilitated drug delivery to the CNS raises the question of the fate of NPs after their translocation to specific cell types or to subcellular structures in the brain. For example, does mitochondrial localization induce oxidative stress? How persistent is the coating or the core of the NPs? A respective safety evaluation is key [Supplemental Material available online (http://ehp.niehs.nih.gov/members/ 2005/7339/supplemental.pdf)]. Exposure via GI Tract and Skin NSPs cleared from the respiratory tract via the mucociliary escalator can subsequently be ingested into the GI tract. Alternatively, nanomaterials can be ingested directly, for example, if contained in food or water or if used in cosmetics or as drugs or drug delivery devices. Only a few studies have investigated the uptake and disposition of nanomaterials by the GI tract, and most have shown that NSPs pass through the GI tract and are eliminated rapidly. In rats dosed orally with radiolabeled functionalized [C.sub.60] fullerenes, water solubilized using PEG and albumin (18 kBq in 100 [micro]L), 98% were cleared in the feces within 48 hr, whereas the rest was eliminated via urine, indicating some uptake into the blood circulation (Yamago et al. 1995). In contrast, in this same study, 90% of the same radiolabeled fullerenes administered intravenously (9.6 kBq in ~50 [micro]L or 14-18 kBq in 215 [micro]L) were retained after 1 week, with most (73-80%, depending on time course) found in the liver. Studies by Kreyling and colleagues (Kreyling et al. 2002; Semmler et al. 2004) using ultrafine [sup.192]Ir did not show significant uptake in the GI tract, whereas earlier studies with larger Ti[O.sub.2] particles (150-500 nm) found uptake into the blood and movement to the liver (Bockmann et al. 2000; Jani et al. 1994). Likely there are differences in GI tract uptake dependent on both particle surface chemistry and particle size. Indeed, after oral dosing in rats, Jani et al. (1990) found a particlesize--dependent uptake of polystyrene particles (ranging from 50 to 3,000 nm) by the GI mucosa. This uptake (6.6% of the administered 50 nm, 5.8% of the 100 nm NSP, 0.8% of 1 [micro]m particles, and 0% for 3 [micro]m particles) was mainly via the Peyer's patches with translocation into the mesenteric mesenteric /mes·en·ter·ic/ (-ter´ik) pertaining to the mesentery. mesenteric pertaining to or emanating from the mesentery. lymph and then to systemic organs (i.e., liver, spleen, blood, bone marrow, and kidney). A potentially important uptake route is through dermal exposure. The epidermis, consisting of the outer horny layer (stratum corneum), the prickle cell layer prickle cell layer n. The layer of polyhedral cells in the epidermis. Also called spinous layer. (stratum spinosum), and basal cell layer (stratum basale), forms a very tight protective layer for the underlying dermis dermis: see skin. (Figure 14). The dermis has a rich supply of blood and tissue macrophages, lymph vessels, dendritic cells (Langerhans, also in stratum spinosum of epidermis), and five different types of sensory nerve endings. Broken skin represents a readily available portal of entry even for larger (0.5-7 [micro]m) particles, as evidenced by reports about accumulation of large amounts of soil particles in inguinal lymph nodes of people who often run or walk barefoot; this can be associated with elephantiatic lymphedema (podoconiosis; Corachan et al. 1988; Blundell et al. 1989). Tinkle tin·kle v. tin·kled, tin·kling, tin·kles v.intr. 1. To make light metallic sounds, as those of a small bell. 2. Informal To urinate. v.tr. 1. et al. (2003) hypothesized that unbroken skin when flexed--as in wrist movements--would make the epidermis permeable for NSPs. They demonstrated in a proof-of-concept experiment that, indeed, flexing the skin, but not flat skin, resulted in penetration of even 1 [micro]m fluorescent beads to the dermis. The follow-up question about access of particles in the dermis to the circulation is answered by the aforementioned reports of podoconiosis, that is, uptake into the lymphatic system and regional lymph nodes. Subsequent translocation of NSPs beyond lymph nodes to the blood circulation is likely to occur as well, as shown in studies with small asbestos fibers (Oberdorster et al. 1988). [FIGURE 14 OMITTED] Newer studies by Kim et al. (2004) in mice and pigs with intradermally in·tra·der·mal adj. Within or between the layers of the skin: an intradermal injection. in injected near-infrared quantum dots confirmed that NPs, once in the dermis, will localize lo·cal·ize v. lo·cal·ized, lo·cal·iz·ing, lo·cal·iz·es v.tr. 1. To make local: decentralize and localize political authority. 2. to regional lymph nodes, which makes these particles very useful for in viva imaging. Likely transport mechanisms to the lymph nodes are skin macrophages and dendritic dendritic /den·drit·ic/ (den-drit´ik) 1. branched like a tree. 2. pertaining to or possessing dendrites. den·drit·ic adj. Relating to the dendrites of nerve cells. (Langerhans) cells (Ohl et al. 2004; Sato et al. 1998); this raises a question about potential modulation of immune responses, after interaction of these NP-containing macrophages and dendritic cells with T lymphocytes. For example, Chen et al. (1998) were able to raise antibodies in mice specific for [C.sub.60] after intraperitoneal injections of [C.sub.60] conjugated conjugated adj. Conjugate. estrogens, conjugated Warning - Hazardous drug! C.E.S. to thyroglobulin thyroglobulin /thy·ro·glob·u·lin/ (thi?ro-glob´u-lin) an iodine-containing glycoprotein of high molecular weight, occurring in the colloid of the follicles of the thyroid gland; the iodinated tyrosine moieties of thyroglobulin form the and serum albumin. Clearly, research is needed to determine whether and under what conditions NPs can be recognized by the immune system, following any route of uptake into the organism. Another question relates to the potential of sensory skin nerves to take up and translocate NPs. Given that this mechanism has been demonstrated for the nasal and tracheobronchial regions of the respiratory tract, how likely is this to occur in the dermis layer of the skin with its dense supply of different types of sensory nerves? It may be conceivable, considering data on neuronal uptake and translocation of NSPs after intramuscular injection. For example, nanosized ferritin and iron-dextran, after injection into the tongue of mice, labeled the neurons of the hypoglossal hypoglossal /hy·po·glos·sal/ (hi´po-glos´al) sublingual. hy·po·glos·sal adj. 1. Of or relating to the area under the tongue. 2. Of or relating to the hypoglossal nerve. nuclei, and injection of both of these NSPs into facial muscles of mice also resulted in synaptic synaptic /syn·ap·tic/ (si-nap´tik) 1. pertaining to or affecting a synapse. 2. pertaining to synapsis. syn·ap·tic adj. Of or relating to synapsis or a synapse. uptake; cationized ferritin was also detected in cell bodies of facial neurons, indicating that electrical charge is of importance for incorporation into axons and axonal transport (Arvidson 1994; Malmgren et al. 1978; Olsson and Kristensson 1981). Other studies using intramuscular injection of ferritin (~112 nm), irondextran (11 or 21 nm), and gold protein (20-25 nm) NSPs also showed rapid penetration through the basal lamina into the synaptic clef clef, in music: see musical notation. clef (French; “key” ) Musical notation symbol at the beginning of a staff to indicate the pitch of the notes on the staff. of the neuromuscular junction, but this was restricted to only the smaller nanoparticles, implying that there may be a size-dependent penetration of the basal lamina with a threshold somewhere between 10 and 20 nm (Oldfors and Fardeau 1983). Neuronal transport of NSPs along sensory skin nerves is well established for herpes virus. After passing through the skin--especially broken skin--the viruses are transported retrogradely along dendrites of sensory neurons to the dorsal root ganglion dorsal root ganglion n. See spinal ganglion. , where they remain dormant until a stress situation triggers anterograde anterograde /an·tero·grade/ (an´ter-o-grad?) extending or moving anteriorly. an·ter·o·grade adj. Moving forward. anterograde extending or moving forward. translocation along the dendrites back to the skin (Kennedy and Chaudhuri 2002; Terasaki et al. 1997). Future studies need to determine whether and to what degree such translocation along sensory skin neurons also occurs with NPs penetrating the epidermis. Risk Assessment The lack of toxicology data on engineered NPs does not allow for adequate risk assessment. Because of this, some may even believe that engineered NPs are so risky that they call for a precautionary halt in NP-related research. However, the precautionary principle should not be used to stop research related to nanotechnology and NPs. Instead, we should strive for a sound balance between further development of nanotechnology and the necessary research to identify potential hazards in order to develop a scientifically defensible database for the purpose of risk assessment. To be able to do this, a basic knowledge about mammalian and ecotoxicologic profiles of NPs is necessary, rather than attempting to assess NP risks based on some popular science fiction literature. Most important, sufficient resources should be allocated by governmental agencies and industries to be able to perform a scientifically based risk assessment and then establish justifiable procedures for risk management. The data needed for this risk assessment should be determined a priori so that limited resources can be used efficiently to develop useful and well-planned studies. At this point, governmental regulation is not possible, given the lack of needed information on which to base such regulations. However, academia, industry, and regulatory governmental agencies should seriously consider the view that NPs have new and unique biologic properties and that the potential risks of NPs are not the same as those of the bulk material of the same chemistry. Assigning a unique identifier to nanosized materials would indicate that the toxicology profile of the material in question may not be the same as the bulk material. Toxicologic tests and the resulting database would provide information for material safety data sheets for NPs as well as a basis for potential NP risk assessments and risk management. Obviously, this approach may not be appropriate for all NPs, for example, when embedded in a matrix, and the feasibility of this proposed strategy needs to be thoroughly discussed and considered. For discussing this, and for developing and deciding upon a reasonable battery of tests for toxicologic profiling, it would be very useful to convene international multidisciplinary workshops of experts from industry, academia, and regulatory agencies (including material scientists, chemists, chemical engineers, toxicologists, physicians, regulators, statisticians, and others) to establish an NP classification scheme and testing guidelines. A muhidisciplinary and multinational collaborative team approach is critical. Respective efforts have been initiated nationally by the American National Standards Institute See ANSI. (body, standard) American National Standards Institute - (ANSI) The private, non-profit organisation (501(c)3) responsible for approving US standards in many areas, including computers and communications. ANSI is a member of ISO. (ANSI (American National Standards Institute, New York, www.ansi.org) A membership organization founded in 1918 that coordinates the development of U.S. voluntary national standards in both the private and public sectors. It is the U.S. member body to ISO and IEC. 2004) and internationally by the International Council on Nanotechnology (ICON 2004) as well as the International Organization for Standardization International Organization for Standardization (ISO) Organization for determining standards in most technical and nontechnical fields. Founded in Geneva in 1947, its membership includes more than 100 countries. (Geneva Geneva, canton and city, Switzerland Geneva (jənē`və), Fr. Genève, canton (1990 pop. 373,019), 109 sq mi (282 sq km), SW Switzerland, surrounding the southwest tip of the Lake of Geneva. , Switzerland). Because many regulatory agencies do not consider a nanotechnologically manufactured substance different from the conventional substance, the manufacture and use of nanotechnology products are currently not specifically regulated. Typically, nanosized substances are treated as variations of the technical material or existing formulation and thus do not require a separate registration. A main reason for producing a nanosize form of a registered substance, however, is that conversion of a substance to a nanoparticle imparts new properties to the substance (e.g., enhanced mechanical, electrical, optical, catalytic, biologic activity). Thus, as stated above, although the toxicology of the base material may be well defined, the toxicity of the nanosize form of the substance may be dramatically different from its parent form. As a result, new toxicology data on the nanosize form of a substance is likely to result in a different hazard assessment for the NPs. Figure 15 shows a risk assessment/risk management paradigm that points out different steps and data required for this process. [FIGURE 15 OMITTED] As described in the preceding sections, the difference in toxicologic profile of NPs compared with its parent form is due to not only its intrinsic chemical properties but also to a large degree to its differing kinetics in vivo. Although larger particles may not enter the CNS, the potential exists for inhaled NSPs to be translocated to the CNS via the axons of sensory neurons in the upper respiratory tract. Furthermore, although the toxicity per unit mass of a particular substance may vary depending on the nano versus larger form, it will be important to take into account not only new biologic activities but also potential new target organs and routes of exposure. To what degree does the nanoform of a substance have enhanced dermal penetration, or increased systemic uptake via the lung or GI tract? What determines how many nanoparticles that enter the systemic circulation will distribute throughout the body, reach the bone marrow, cross the blood-brain barrier, cross the placenta to affect the developing offspring, or sequester sequester v. to keep separate or apart. In so-called "high-profile" criminal prosecutions (involving major crimes, events, or persons given wide publicity) the jury is sometimes "sequestered" in a hotel without access to news media, the general public or their effectively in the liver? Do nanoparticles released into the environment affect species that are important in food chain dynamics? What are the long-term consequences of exposure to nanoparticles? Changes in toxicity profile and new target organs can be expected, and it will then be necessary to establish new risk assessments for nanoparticles in addition to the bulk material. Currently there exists a paucity of data to effectively address these questions, but it will be important to determine whether there exist common modes of action/behavior of NPs to establish baseline assumptions for use in risk assessments. The use of nanotechnology products will likely increase dramatically over the next decade. In fact, nanomaterials are already being used in applications ranging from burn and wound dressings to dental-bonding agents to sunscreens and cosmetics to fuel cells, tires, optics, clothing, and electronics. Although currently there exists little public awareness of nanotechnology in everyday life (e.g., stain-flee clothing), it would be prudent to examine and address environmental and human health concerns before the widespread adoption of nanotechnology. Both the societal benefits and potential risks of nanotechnology should be evaluated and clearly communicated to the general public and regulators. This type of open communication and risk/benefit evaluation will avoid the pitfalls encountered with genetically modified organisms recently experienced in the field of biotechnology. In that instance, the benefits of the emerging field of biotechnology were not communicated effectively before the introduction of the technology. As the public's awareness of this new technology grew, regulators and producers of biotechnology failed to effectively acknowledge public concerns that genetically modified organisms could adversely affect ecosystem balance. As a result, the public support of genetically modified organisms, particularly in the European Union, is low. For nanomaterial producers, it will be important to demonstrate that what they may perceive as a new and potentially harmless form of a familiar material has, indeed, an acceptable risk profile. If such proactive steps are not taken, nanomaterials may be regarded as dangerous by the public and regulators, which could lead to inappropriate categorization and unnecessarily burdensome regulations. Such action (or inaction on the side of producers), in turn, could result in significant barriers to commercialization and the widespread acceptance of otherwise useful nanotechnology materials. Summary and Outlook Research on ambient UFPs has laid the foundation for the emerging field of nanotoxicology, with the goal of studying the biokinetics and the potential of engineered nanomaterials (particles, tubes, shells, quantum dots, etc.) to cause adverse effects. Major differences between ambient UFPs and NPs are the polydisperse nature of the former versus the monodisperse size of the latter, and particle morphology, oftentimes a branched structure from combustion particles versus spherical form of NPs, although other shapes (tubes, wires, rings, planes) are also manufactured. In addition, combustion-derived volatile organic compounds and inorganic constituents (e.g., metals, nitrates, sulfates) of different solubilities on UFPs predict differences in the toxicologic profile between UFPs and NPs. However, as far as the insoluble particle is concerned, concepts of NSPs kinetics, including cell interactions, will most likely be the same for UFPs and NPs (Figure 16). [FIGURE 16 OMITTED] The introduction of nanostructured materials for biomedical and electronics applications opens tremendous opportunities for biomedical applications as therapeutic and diagnostic tools as well as in the fields of engineering Engineering is a collective term to describe the application of scientific theory in the design, creation, and maintenance of technology. According to 1992 NSF data, the largest fields of engineering are Civil, Electrical / Electronic, Industrial and Mechanical Engineering (by number of , electronics, optics, consumer products, alternative energy, soil/water remediation, and others. However, very little is yet known about their potential to cause adverse effects or humoral immune responses once they are introduced into the organism--unintentionally or intentionally. Nanomedicine products will be well tested before introduction into the marketplace. However, for the manufacturers of most current nanotechnology products, regulations requiring nanomaterial-specific data on toxicity before introduction into the marketplace are an evolving area and presently under discussion (Bergeson and Auerbach 2004; Foresight and Governance Project 2003). During a product's life cycle (manufacture, use, disposal), it is probable that nanomaterials will enter the environment, and currently there is no unified plan to examine ecotoxicologic effects of NPs. In addition, the stability of coatings and covalent surface modifications need to be determined both in ecologic settings and in vivo. [Supplemental Material available online (http://ehp.niehs.nih.gov/members/ 2005/7339/supplemental.pdf).] Results of older biokinetic studies and some new toxicology studies with NSPs (mostly ambient UFPs) can be viewed as the basis for the expanding field of nanotoxicology. These studies showed that the greater surface area per mass renders NSPs more active biologically than larger-sized particles of the same chemistry, and that particle surface area and number appear to be better predictors for NSPs-induced inflammatory and oxidative stress responses. The following emerging concepts of nanotoxicology can be identified from these studies: The biokinetics of NSPs are different from larger particles. When inhaled, they are efficiently deposited in all regions of the respiratory tract; they evade specific defense mechanisms; and they can translocate out of the respiratory tract via different pathways and mechanisms (endocytosis and transcytosis). When in contact with skin, there is evidence of penetration to the dermis followed by translocation via lymph to regional lymph nodes. A possible uptake into sensory nerves needs to be investigated. When ingested, systemic uptake via lymph into the organism can occur, but most are excreted via feces. When in blood circulation, they can distribute throughout the organism, and they are taken up into liver, spleen, bone marrow, heart, and other organs. In general, translocation rates are largely unknown; they are probably very low but are likely to change in a compromised/ diseased state. The biologic activity and biokinetics are dependent on many parameters: size, shape, chemistry, crystallinity, surface properties (area, porosity, charge, surface modifications, weathering of coating), agglomeration ag·glom·er·a·tion n. 1. The act or process of gathering into a mass. 2. A confused or jumbled mass: state, biopersistence, and dose. These parameters are likely to modify responses and cell interactions, such as a greater inflammatory potential than larger particles per given mass, translocation across epithelia from portal of entry to other organs, translocation along axons and dendrites of neurons, induction of oxidative stress, pro-oxidant and antioxidant activity of NSPs in environmentally relevant species, binding to proteins and receptors, and localization in mitochondria. The principles of cellular and organismal interactions discussed in this article should be applicable for both ambient UFPs and NPs, even if the latter are coated with a biocompatible material. Knowledge about the biopersistence of this coating is as essential as is knowledge about the bioavailability bioavailability /bio·avail·a·bil·i·ty/ (bi?o-ah-val?ah-bil´i-te) the degree to which a drug or other substance becomes available to the target tissue after administration. bi·o·a·vail·a·bil·i·ty n. of the core material that could have intrinsic toxic properties, for example, semiconductor metal compounds in sub-10-nm quantum dots consisting of cadmium and lead compounds. The very small size of these materials makes them available to the same translocation processes described here for polydisperse NSPs, possibly even in a more efficient way because of their uniform size. When studying biologic/toxicologic effects, new processes of interactions with subcellular structures (e.g., microtubuli, mitochondria) will likely be discovered. The diversity of engineered nanomaterials and of the potential effects represents major challenges and research needs for nanotoxicology, including also the need for assessing human exposure during manufacture and use. The goal to exploit positive aspects of engineered nanomaterials and avoid potential toxic effects can best be achieved through a multidisciplinary team effort involving researchers in toxicology, materials science, medicine, molecular biology, bioinformatics, and their subspecialties. CORRECTION The authors found additional information on GI tract uptake of NSPs that was not in the original manuscript published online. This information has been included here in "Exposure via GI Tract and Skin." We thank J. Havalack for excellent assistance in preparing the manuscript. This work was supported in part by the U.S. Environmental Protection Agency (EPA) STAR Program grant R827354, National Institute of Environmental Health Sciences The National Institute of Environmental Health Sciences (NIEHS) is one of 27 Institutes and Centers of the National Institutes of Health (NIH),which is a component of the Department of Health and Human Services (DHHS). The Director of the NIEHS is Dr. David A. Schwartz. grant ESO ESO European Southern Observatory ESO Educación Secundaria Obligatoria (Spain: compulsory secondary education) ESO European Organisation for Astronomical Research in the Southern Hemisphere ESO Edmonton Symphony Orchestra 1247, U.S. Department of Defense MURI MURI Multidisciplinary University Research Initiative grant FA9550-04-1-430, and the National Science Foundation (SGER SGER Small Grant for Electronic Research (National Science Foundation) ) BES-0427262. 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Atmos Environ 36:4323-4335. Gunter Oberdorster, (1) Eva Oberdorster, (2) and Jan Oberdorster (3) (1) Department of Environmental Medicine, University of Rochester The University of Rochester (UR) is a private, coeducational and nonsectarian research university located in Rochester, New York. The university is one of 62 elected members of the Association of American Universities. , Rochester, New York This article is about the city of Rochester in Monroe County. For the town in Ulster County, see Rochester, Ulster County, New York. Rochester, once known as The Flour City, and more recently as The Flower City or , USA; (2) Department of Biology, Southern Methodist University Southern Methodist University, at Dallas, Tex.; United Methodist; coeducational; chartered 1911. The school's facilities include laboratories for electron microscopy and stable isotopes, a museum of paleontology, and a graduate research center. , Dallas, Texas, USA; (3) Toxicology Department, Bayer CropScience, Research Triangle Park Research Triangle Park, research, business, medical, and educational complex situated in central North Carolina. It has an area of 6,900 acres (2,795 hectares) and is 8 × 2 mi (13 × 3 km) in size. Named for the triangle formed by Duke Univ. , North Carolina, USA Address correspondence to G. Oberdorster, University of Rochester, Department of Environmental Medicine, 575 Elmwood Ave., MRBx Building, Box 850, Rochester, NY 14642 USA. Telephone: (585) 275-3804. Fax: (585) 256-2631. E-mail: Gunter_Oberdorster@ urmc.rochester.edu Supplemental Material is available online at http://ehp.niehs.nih.gov/members/2005/7339/ supplemental.pdf
Table 1. UFPs/NPs (< 100 nm), natural and anthropogenic sources.
Anthropogenic
Natural Unintentional
Gas-to-particle conversions Internal combustion engines
Forest fires Power plants
Volcanoes (hot lava) Incinerators
Viruses Jet engines
Biogenic magnetite: magnetotactic Metal fumes (smelting,
bacteria protoctists, mollusks, welding, etc.)
arthropods, fish, birds Polymer fumes
human brain, meteorite (?) Other fumes
Ferritin (12.5 nm) Heated surfaces
Microparticles (< 100 nm, Frying, broiling, grilling
activated cells) Electric motors
Anthropogenic
Natural Intentional (NPs)
Gas-to-particle conversions Controlled size and shape, designed
Forest fires for functionality
Volcanoes (hot lava) Metals, semiconductors, metal
Viruses oxides, carbon, polymers
Biogenic magnetite: magnetotactic Nanospheres, -wires, -needles,
bacteria protoctists, mollusks, -tubes, -shells, -rings,
arthropods, fish, birds -platelets
human brain, meteorite (?) Untreated, coated (nanotechnology
Ferritin (12.5 nm) applied to many products:
Microparticles (< 100 nm, cosmetics, medical, fabrics,
activated cells) electronics, optics, displays,
etc.)
Table 2. Particle number and particle surface area per 10
[micro]g/[m.sup.3] airborne particles.
Particle surface
Particle Particle area ([micro][m.sup.2]/
diameter ([micro]m) no. ([cm.sup.-3]) [cm.sup.3])
5 153,000,000 12,000
20 2,400,000 3,016
250 1,200 240
5,000 0.15 12
Table 3. Clearance mechanisms for inhaled solid
particles in the respiratory tract.
Physical clearance processes (translocation)
Mucociliary movement (nasal, tracheobronchial)
Macrophage phagocytosis (tracheobronchial, alveolar)
Epithelial endocytosis (nasal, tracheobronchial, alveolar)
Interstitial translocation (tracheobronchial, alveolar)
Lymphatic drainage (tracheobronchial)
Blood circulation (tracheobronchial, alveolar)
Sensory neurons (nasal, tracheobronchial)
Chemical clearance processes (a)
Dissolution
Leaching
Protein binding
(a) Nasal, tracheobronchial, and alveolar regions.
Table 4. Particle size and surface chemistry-related
alveolar-capillary translocation.
Particle size (nm) Type Translocation
5-20 Gold, albumin coated Yes
8 Gold, albumin coated Yes
8 Gold, albumin coated Yes
18 Iridium Yes (a)
30 Gold Yes
35 Carbon Yes
60 Polystyrene (b) Yes
60 Polystyrene ?
80 Iridium Yes (a)
240 Polystyrene, lecithin Yes
240 Polystyrene, uncoated No
400 Polystyrene No
Particle size (nm) Localization/effect Reference
5-20 Via caveolae Mehta et al. 2004
8 Via "vesicles" Konig et al. 1993
8 Via caveolae Heckel et al. 2004
18 Extrapulmonary organs Kreyling et al. 2002
30 Platelet? Berry et al. 1977
35 Liver Oberdorster et al. 2002
60 Thrombus, early Nemmar et al. 2002b
Silva et al., in press
60 No thrombus Nemmar et al. 2002b
80 Extrapulmonary organs Kreyling et al. 2002
240 Monocytes Kato et al. 2003
240 Kato et al. 2003
400 Thrombus, late Nemmar et al. 2003
?, Unknown.
(a) Minimal. (b) Indirect evidence.
Table 5. Translocation of NSPs in the blood circulation to bone
marrow in mice.
Particle size Type Finding
-10 nm PEG quantum dots Fast appearance of quantum
dots in liver, spleen,
lymph nodes, and bone
marrow (mouse)
<220 nm Metallo-fullerene Highest accumulation in
bone marrow after liver;
continued increase in bone
marrow but decrease in
liver (mouse)
90-250 nm HSA-coated polylactic Significant accumulation in
acid nanoparticles bone marrow, second to
liver (rat)
240 nm Polystyrene Rapid passage through
(nonbiodegradable) endothelium in bone marrow,
polylisohexylcyonacrylate uptake by phagocytizing
(biodegradable) cells in tissue (mouse)
Particle size Reference
-10 nm Ballou et al. 2004
<220 nm Cagle et al. 1999
90-250 nm Bazile et al. 1992
240 nm Gibaud et al. 1996,
1998, 1994
HSA, human serum albumin.
Table 6. Studies of neuronal translocation of UFPs from respiratory
tract.
Reference Study
Bodian and Howe 1941 Olfactory axonal transport of polio virus (30
nm) after intranasal instillation in
chimpanzee; transport velocity, 2.4 mm/hr
de Lorenzo 1970 Olfactory axonal transport of 50 nm silver-
coated gold after intranasal instillation
in squirrel monkey; transport velocity, 2.5
mm/hr
Hunter and Dey 1998 Retrograde tracing of trigeminal neurons from
nasal epithelium with microspheres
Hunter and Undem 1999 Rhodamine-labeled microspheres (20-200 nm)
translocation via sensory nerves of
TB region to ganglion nodosum in hamster
after intratracheal instillation
Oberdorster et al. 2004 [sup.13]C particles (CMD - 36 nm) in
olfactory bulb after whole-body inhalation
exposure in rats
TB, tracheobronchial.
Table 7. Rat versus human nasal and olfactory parameters.
Measure Rat Human
Breathing mode Obligatory nose Nasal/oronasal
Area of nasal mucosa ~16 [cm.sup.3] ~105 [cm.sup.2]
Area of olfactory mucosa ~8 [cm.sup.3] (50) ~5.25 [cm.sup.2] (5)
(% total mucosa)
Percent nasal airflow going ~15 ~10
to olfactory mucosa
Weight of olfactory bulb ~85 ng ~168 ng
Based on Keyhani et al. (1997), Kimbell et al. (1997),
and Turetsky et al. (2003).
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