The PBDEs: An Emerging Environmental Challenge and Another Reason for Breast-Milk Monitoring Programs.

Levels of the polybrominated diphenyl ethers Polybrominated diphenyl ethers or PBDE, are a flame retardant sub-family of the brominated flame retardant group. They have been used in a wide array of household products, including fabrics, furniture, and electronics. (PBDEs), a class of widely used flame retardants, appear to be rising rapidly in human tissues, as evidenced by studies of human breast milk. The case of the PBDEs illustrates the value of breast-milk monitoring programs in identifying important emerging pollutants, and highlights why such monitoring programs are needed in the United States. A review of the use, occurrence, and toxicity of PBDEs indicates many parallels between some PBDEs, PCBs, and other polyhalogenated persistent organic pollutants, and suggests that the PBDEs may be a significant environmental challenge in the future. Key words: breast-milk monitoring programs, flame retardants, persistent organic pollutants, polybrominated diphenyl ethers, polychlorinated biphenyls polychlorinated biphenyls, (pol´ēklôr´

nā´tid bīfē´n , polychlorinated diphenyl diphenyl /di·phen·yl/ (di-fen´il) a toxic compound comprising two linked benzene rings, used as a fungistat in containers for shipping citrus fruits.

di·phen·yl
n.
See biphenyl. ethers, structure-activity relationships, toxicity. Environ Health Perspect 108:387-392 (2000). [Online 15 March 1999] http://ehpnet1.niehs.nih.gov/docs/2000/108p387-392hooper/abstract.html

A family of brominated flame retardants called the polybrominated diphenyl ethers (PBDEs) has been increasing exponentially over the past 25 years as contaminants in breast milk samples from Sweden; their levels have doubled every 5 years (Figure 1) (1). PBDEs are now found as residues in sediments, wildlife (marine mammals marine mammals

mammals inhabiting the sea; generally taken to include the cetaceans (whales, porpoise, dolphin), the sirenians (sea-cows, including manatees and dugong) and the pinnipeds (the carnivores of the group, seals, sealions, walruses). , fish, and bird eggs) and humans (milk, serum, and adipose tissue adipose tissue (ăd`əpōs'): see connective tissue.

adipose tissue
or fatty tissue

Connective tissue consisting mainly of fat cells, specialized to synthesize and contain large globules of fat, within a ). Lipophilic lipophilic,
adj/n the ability to dissolve or attach to lipids.

lipophilic (lipōfil´ik),
adj 1. showing a marked attraction to, or solubility in, lipids.
2. and metabolically resistant, the PBDEs share many of the properties that make them long-lived, bioaccumulating, environmental pollutants environmental pollutants,
n.pl the substances and conditions, including noise, that adversely affect the health and well-being of the people within a community. with the organochlorine or·gan·o·chlo·rine
n.
Any of various hydrocarbon pesticides, such as DDT, that contain chlorine. pesticides (e.g., DDT DDT or 2,2-bis(p-chlorophenyl)-1,1,1,-trichloroethane, chlorinated hydrocarbon compound used as an insecticide. First introduced during the 1940s, it killed insects that spread disease and feed on crops. ), polychlorinated biphenyls (PCBs), and polychlorinated dibenzo-p-dioxins and furans. The increasing levels of PBDEs in breast milk illustrate how breast-milk monitoring programs (BMMPs) can act as warning systems and alert us to new forms of persistent organic pollutants (POPs).

[Figure 1 ILLUSTRATION OMITTED]

Once alerted, new questions arise. What are the PBDEs? Where do they come from? What concerns should we have over their presence in the environment or in breast milk?

Briefly, PBDEs are flame-retardant additives in high-impact plastics, foams, and textiles (5-30% of these products by weight) (2). They are structurally related to the PCBs (Figure 2) and, like PCBs, are produced commercially as mixtures. However, PBDE PBDE Polybrominated Diphenyl Ether
PBDE Pentabromodiphenyl Ether (flame retardant additive in plastics)
PBDE Parallel Block-Decodable Encoder mixtures contain fewer congeners than commercial PCB PCB: see polychlorinated biphenyl.

PCB
in full polychlorinated biphenyl

Any of a class of highly stable organic compounds prepared by the reaction of chlorine with biphenyl, a two-ring compound. mixtures and enter the environment in a different way. PCBs, in general, enter the environment directly from point sources (e.g., broken capacitors) as a complete commercial dielectric mixture. PBDE mixtures, in contrast, are noncovalently bound additives in plastics and textiles that are selectively released over the products' lifetimes. What little is known of PBDE toxicology resembles that of the PCBs. Some of the persistent and bioaccumulative PBDE congeners seem likely to cause cancer and thyroid and/or neurodevelopmental toxicity, based on the available PBDE toxicology data and on structure-activity relationships with PCBs, polychlorinated diphenyl ethers (PCDEs), and other compounds.

[Figure 2 ILLUSTRATION OMITTED]

At present, residue levels of PBDEs in biota biota /bi·o·ta/ (bi-o´tah) all the living organisms of a particular area; the combined flora and fauna of a region.

bi·o·ta
n.
The flora and fauna of a region. are lower than (1/10-1/100th) levels of PCBs. However, the exponential increase in PBDEs found recently in breast milk may be a harbinger of things to come: PBDEs may be the PCBs of the future. PBDEs are an excellent example of why BMMPs are needed in the United States.

Polyhalogenated POPs

Polyhalogenated POPs are a superfamily superfamily /su·per·fam·i·ly/ (soo´per-fam?i-le)
1. a taxonomic category between an order and a family.

2. of compounds with long 2- to 10-year half-lives [e.g., 2,3,7,8-tetrachlorodibenzo-p-dioxin (TCDD) has a half-life of 7.5 years] (3-6). Members of this superfamily include the PCDD/PCDFs, PCBs, PCDEs, and polychlorinated naphthalenes (PCNs), as well as the polybrominated biphenyls polybrominated biphenyls

see biphenyl. (PBBs) and PBDEs (International Union of Pure and Applied Chemistry International Union of Pure and Applied Chemistry (IUPAC), an international organization est. 1919 to advance the chemical sciences and contribute to the application of chemistry to the service of humanity. no. 209) (Table 1). Each subfamily subfamily /sub·fam·i·ly/ (sub´fam-i-le) a taxonomic division between a family and a tribe.

sub·fam·i·ly
n.
A taxonomic category ranking between a family and a genus. consists of many congeners (Table 1) that share the subfamily's chemical backbone but with different numbers and positions of halogen substituents (Figure 2). Not all of the congeners in each subfamily are classified as POPs, i.e., are stable and persistent. For example, only 17 of the 210 PCDDs/PCDFs persist in humans. The polyhalogenated POP superfamily also contains approximately 20 of the organochlorine pesticides.

Table 1. PBDEs and other polyhalogenated POPs.

                               Properties

                       Congeners         Use
Chemical class,        in class      (functional
specific congeners        (n)         property)

PCDDs/PCDFs             75/135     Contaminants
  TCDD
PCBs                       209     Dielectrics
  Co-planar PCB                      (thermally
  Mono-ortho-PCB                     stable)
  Hexa-(PCB-153)(a)
PBBs                       209     Flame retardant
  Hexa-(PBB-153)(a)                  (releases Br)
  Deca-BB(c)
PCDEs                      209      Contaminants
  Penta-(PCDE-99)
  Hexa-(PCDE-153)
PBDEs                      209      Flame retardant
  Tetra-(PBDE-47)(a)                 (releases Br)
  Penta-(PBDE-99)(a)
  Hexa-(PBDE-153)(a)
  Deca-BDE(c)

                                      Properties

                         Commercial
                           mixtures       Half-life,   Half-life,
Chemical class,         (no. congeners      rodent       human
specific congeners       in product)        (days)      (years)

PCDDs/PCDFs            NA                    1-60         2-10
  TCDD                                      10-30         8
PCBs                   e.g., Aroclor         6-28         2-6
  Co-planar PCB        1254, 1260            7-9
  Mono-ortho-PCB       (> 40)
  Hexa-(PCB-153)(a)                        431-478
PBBs                   e.g., Firemaster    160-480        8-11
  Hexa-(PBB-153)(a)      BP-6 (> 30)(b)                   4-97
  Deca-BB(c)
PCDEs                  NA
  Penta-(PCDE-99)                            6
  Hexa-(PCDE-153)
PBDEs
  Tetra-(PBDE-47)(a)                        20-30
  Penta-(PBDE-99)(a)   Penta- (~ 10)        25-47
  Hexa-(PBDE-153)(a)                        45-120
  Deca-BDE(c)          Octa-
                       Deca- (< 10)         < 1(e)

                          Properties             Toxicity

                            Human            Ah      Cancer,
Chemical class,          body burden,     receptor    animal
specific congeners     pg/g lipid,(TEQ)   activity   or human

PCDDs/PCDFs            (20)                 +/+        +/+
  TCDD                 3-5 (3-5)            +          +
PCBs                   1,500,000 (20)       +          +
  Co-planar PCB                             +
  Mono-ortho-PCB                            +
  Hexa-(PCB-153)(a)                         -
PBBs                   [is less than or     +          +
                         equal to]
                         50,000
  Hexa-(PBB-153)(a)
  Deca-BB(c)                                -
PCDEs                                       +
  Penta-(PCDE-99)      2,000-8,000
  Hexa-(PCDE-153)      2,000-8,000          +
PBDEs                  1,000-100,000        +
  Tetra-(PBDE-47)(a)   Tetra-hexa           +
  Penta-(PBDE-99)(a)                        +(d)
  Hexa-(PBDE-153)(a)                        +(d)
  Deca-BDE(c)
                                                       +/-

                                  Toxicity

Chemical class,           Neuro-
specific congeners     developmental   Thyroid

PCDDs/PCDFs                 +/+          +/+
  TCDD                      +            +
PCBs                        +            +
  Co-planar PCB
  Mono-ortho-PCB            +            +
  Hexa-(PCB-153)(a)         +
PBBs                                     +
  Hexa-(PBB-153)(a)
  Deca-BB(c)
PCDEs                       +            +
  Penta-(PCDE-99)
  Hexa-(PCDE-153)
PBDEs                       +            +
  Tetra-(PBDE-47)(a)        +            +
  Penta-(PBDE-99)(a)        +            +
  Hexa-(PBDE-153)(a)
  Deca-BDE(c)                            +
                                         +

Abbreviations: Ah, aryl ar·yl
n.
An organic radical derived from an aromatic compound by the removal of one hydrogen atom. hydrocarbon; NA, not applicable; TEQ TEQ Toxicity Equivalent
TEQ Time Domain Equalizer
TEQ Teacher Education Quarterly
TEQ Terra Est Quaestuosa (web-based game, Spanish: Lland is Profitable)
TEQ The Evil Quakkers (gaming clan) , toxic equivalency. +, positive study; -, negative study; +/-; marginally positive. Cells left blank indicate no data.

(a) Examples of major congeners commonly found in human tissues.

(b) Monsanto Corporation, St. Louis, MO.

(c) Most-produced congener congener /con·ge·ner/ (kon´je-ner) something closely related to another thing, as a member of the same genus, a muscle having the same function as another, or a chemical compound closely related to another in composition and exerting of class.

(d) Commercial grade penta-BDE was positive (primarily contains PBDE-47, -99, and -153).

(d) The short half-life of deca-BDE is likely due to a very low (~ 0.3%) rate of absorption. However, adipose tissue bromine bromine (brō`mēn, –mĭn) [Gr.,=stench], volatile, liquid chemical element; symbol Br; at. no. 35; at. wt. 79.904; m.p. –7.2°C;; b.p. 58.78°C;; sp. gr. of liquid 3.12 at 20°C;; density of vapor 7. levels in rats fed deca-BDE remained unchanged for 90 days after cessation of exposure [reviewed in (2)], indicating a long terminal half-life.

POPs have three chemical characteristics that make them intrinsically hazardous: they are stable (persistent), they are fat-seeking, and they have the potential to act as endocrine disruptors. The stability and lipophilicity of POPs causes them to biomagnify up the food chain, increasing in concentration at each successively higher trophic level. Once polyhalogenated POPs are released into the environment, they invariably in·var·i·a·ble
adj.
Not changing or subject to change; constant.

in·vari·a·bil find their way into the mother, where they pass transplacentally to the developing fetus or through the breast milk to the nursing infant. Some POPs can bind to receptors and act in a hormonelike manner to cause biologic effects at low doses. For example, the 2,3,7,8-substituted PCDDs/PCDFs, PCNs, and coplanar co·pla·nar
adj.
Lying or occurring in the same plane. Used of points, lines, or figures.

copla·nar PCBs bind as ligands to a cytoplasmic cytoplasmic

pertaining to or included in cytoplasm.

cytoplasmic inclusions
include secretory inclusions (enzymes, acids, proteins, mucosubstances), nutritive inclusions (glycogen, lipids), pigment granules (melanin, lipofuscin, hormone-receptor-like molecule called the aryl hydrocarbon (Ah) receptor. This Ah receptor ligand-bound complex migrates from the cytoplasm cytoplasm: see protoplasm.

cytoplasm

Portion of a eukaryotic cell outside the nucleus. The cytoplasm contains all the organelles (see eukaryote). into the nucleus and alters the expression of genes coding for different metabolizing enzymes (e.g., cytochrome P450s). Other POPs such as the PBDEs have the potential to bind to to contract; as, to bind one's self to a wife s>.

See also: Bind the Ah or other receptors and act via hormonelike mechanisms.

Recent studies indicate that a number of polychlorinated POPs are endocrine disruptors. Several have estrogen-like activities, whereas others, the dioxin-like POPs, have antiestrogenic activities (7-10). Health effects as diverse as shortened duration of lactation lactation

Production of milk by female mammals after giving birth. The milk is discharged by the mammary glands in the breasts. Hormones triggered by delivery of the placenta and by nursing stimulate milk production. in mothers (11) and neurodevelopmental cognitive-motor deficits and intellectual impairment in children (12-17) have been attributed to polyhalogenated POPs. For PCDDs/PCDFs, contaminant contaminant /con·tam·i·nant/ (kon-tam´in-int) something that causes contamination.

contaminant

something that causes contamination. levels in breast milk (18-21) and human health effects (19,22-24) have recently been reviewed. For TCDD, there are a plethora of health effects (7,25), ranging from chloracne chloracne /chlor·ac·ne/ (klor-ak´ne) an acneiform eruption due to exposure to chlorine compounds.

chlor·ac·ne
n. to cancer (19) and altered sex ratio (26).

POPs have shorter half-lives in rodents than in humans (e.g., TCDD half-life in rodents is 10-20 days and in humans is 5-10 years). After corrections are made for species differences in residence times, human exposures to TCDD are closer to the dose levels that produce effects in animal studies (27).

Ironically, it is the fetus and the nursing infant that receive significant exposures or the greatest body burdens of environmental POPs. As evidence of fetal exposures, the infant at birth has levels of TCDD that are up to 25% of maternal levels (28-31), and in utero in utero (in u´ter-o) [L.] within the uterus.

in u·ter·o
adj.
In the uterus.

in utero adv. exposures to background levels of some POPs are associated with adverse effects [e.g., cognitive-motor deficits (12,13,15-17)]. Breast-fed breast·feed or breast-feed
v. breast-fed , breast-feed·ing, breast-feeds

v.tr.
To feed (a baby) mother's milk from the breast; suckle.

v.intr.
To breastfeed a baby. infants are effectively at the top of the food chain. Their daily intake of TCDD, for example, is typically 50-fold higher than that of adults, on a body weight basis (32-34), and they absorb 90% of the ingested TCDD (35).

This level of uptake of polyhalogenated POPs by the fetus and the nursing infant raises concerns about the potential for adverse health outcomes. POP body burdens may adversely affect reproduction in the mother or adversely affect the development of the fetus, infant, or child, exposed either in utero and/or via breast-feeding breast-feeding /breast-feed·ing/ (brest´fed?ing) nursing; the feeding of an infant at the mother's breast. (11-17,25,26). Prenatal, and not lactational, exposures appear to be important sources of some of the adverse health effects of POPs seen in infants [e.g., cognitive-motor deficits from PCBs (12)]. There is also evidence that breast-fed infants, even at the highest background exposures, fare better than nonbreast-fed infants with comparable exposure in cognitive and motor development (15,36). Thus, breast-feeding continues to be considered beneficial to the infant, although careful studies of longer term outcomes (e.g., cancer) from ingesting contaminants in breast milk have not been conducted. Thus, at present, POP contaminants in breast milk are useful as markers of maternal body burdens as well as lactational and in utero exposures.

BMMPs

Breast-milk monitoring is a convenient non-invasive means of estimating body burdens of polyhalogenated POPs in the mother, fetus, and breast-fed infant or child. POPs enter humans chiefly as contaminants in animal-derived food (fish, poultry, beef, eggs, and dairy products). Once ingested, POPs 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 in body lipids, where they equilibrate e·quil·i·brate
v. e·quil·i·brat·ed, e·quil·i·brat·ing, e·quil·i·brates

v.intr.
To be in or bring about equilibrium.

v.tr.
To maintain in or bring into equilibrium. at roughly similar levels on a fat-weight basis between adipose tissue, serum, and breast milk. POP contaminants in breast milk increase with maternal age maternal age,
n the age of the mother at the period of conception. [e.g., TCDD (18,37,38)] and decrease with the number and duration of lactation periods (e.g., TCDD levels in breast milk decrease roughly 25% after each successive breast-fed child) (18,39,40).

BMMPs have many uses. They provide data on baseline body burdens for women during the perinatal period and, with the use of breast milk consumption data, provide estimates of POP levels in infants and children. BMMPs identify hot spots of POP contamination, and congener patterns can help to identify the sources of the POP contaminants. BMMPs identify at-risk populations of mothers, infants, and children for follow-up health outcome studies. Using time-trend data, BMMPs can also identify new POPs of emerging concern, and can assess the effectiveness of regulatory strategies to limit exposures to POPs (e.g., pollution prevention or hazardous waste management). Thus, time-trend data from the Swedish BMMP BMMP Business Management Modernization Program (US DoD)
BMMP Biomimetic Materials Processing
BMMP Benign Mucous Membrane Pemphigoid
BMMP Bluebonnet Military Motor Pool (of Texas)
BMMP Basic Major Medical Plan , as reported by Noren et al. (Figure 1), identified PBDEs as a growing concern. The Swedish data also demonstrated a 70% decrease in PCDD/PCDF/PCB body burdens over the past 25 years (1), presumably pre·sum·a·ble
adj.
That can be presumed or taken for granted; reasonable as a supposition: presumable causes of the disaster. as a result of effective regulatory actions.

Breast milk and adipose tissue, like sediments in rivers or lakes, act as storehouses of POPs. POP levels in breast milk, as with sediments, reflect past environmental conditions. BMMP data complement monitoring data from air, water, soil, or food.

BMMPs have operated in several countries (Sweden, Germany, The Netherlands, and New Zealand) over the last 20-30 years, and have helped to identify PCBs and PBDEs as important human contaminants. Standardized collection and analytical protocols (41) now exist for analyzing many POPs in breast milk. Currently, there is no systematic monitoring of breast milk contamination in the United States, and little is known of PBDE breast milk levels or body burdens in the United States.

PBDEs

As with other POPs, PBDEs are transferred via breast milk from the mother to the offspring. Evidence of this transfer comes from pilot whales. Juvenile pilot whales, which subsist sub·sist
v. sub·sist·ed, sub·sist·ing, sub·sists

v.intr.
1.
a. To exist; be.

b. To remain or continue in existence.

2. primarily on mother's milk, had 2- to 3-fold higher levels of 19 PBDE congeners (tetra- to hexa-BDE: 3 vs. 1 ppm) than adults (42).

Identity, use, and production. The PBDEs are structurally similar to the PCBs and PBBs (Figure 2), with the same nomenclature and number (209) of congeners. Since the 1960s, PBDEs have been added as flame-retardants to thermoplastics (e.g., high-impact polystyrene) that are used in electrical appliances, TV sets, computer circuit boards and casings, and building materials. PBDEs are also found in foams and upholstery in home and business furnishings; in interiors in cars, buses, trucks, and airplanes; and in rug and drapery textiles (2,43). Some manufacturers have begun to reduce PBDE levels in products (e.g., computer monitors) to earn the Swedish TCO (1) (Total Cost of Ownership) The cost of using a computer. It includes the cost of the hardware, software and upgrades as well as the cost of the inhouse staff and/or consultants that provide training and technical support. See ROI. 99 environmental label.

Three major commercial mixtures of PBDEs are produced: deca-BDEs (mostly deca-BDE with some nona- and octa-BDE congeners), octa-BDEs (mostly hepta- and octa-BDE congeners), and penta-BDEs (mostly penta- and tetra-BDE congeners). Fully brominated deca-BDE is the major product, accounting for 75% of the PBDE production. The commercial PBDEs generally contain fewer ([is less than] 10) congeners than do commercial PCB mixtures (e.g., roughly 80 congeners in the Aroclor 1254 or 1260 mixtures). Worldwide PBDE production is estimated at roughly 80 million pounds per year (2). In the: United States, commercial penta-, octa-, and deca-BDE were each produced or imported at greater than one million pounds per year in 1990, 1994, and 1998 (44).

Environmental fate. PBDEs are likely to be more susceptible to environmental degradation than PCBs because bromine is a better "leaving group" than chlorine; i.e., the carbon-bromine bond is weaker than the carbon-chlorine bond. Thus, whereas PCBs were used as thermally resistant dielectrics, PBDEs are used as flame retardants because they are somewhat thermally labile labile /la·bile/ (la´bil)
1. gliding; moving from point to point over the surface; unstable; fluctuating.

2. chemically unstable.

la·bile
adj.
1. , and break down with heat to release bromine radicals that quench quench,
v to cool a hot object rapidly by plunging it into water or oil.

quench

to put out, extinguish, or suppress; to cool (as hot metal) by immersing in water. the radical cascade of the combustion and fire-spreading processes.

The environmental fates of the PBDEs are not well documented. Most of the analytical methods used at present detect only the lower molecular weight (MW) ([is less than] 800 MW) tetra- to hepta-BDE congeners, and the fates of the higher MW (octa- to deca-BDE) congeners and the major commercial mixture (deca-BDE) are unclear.

The fate of deca-BDE in the environment needs further study. Even though the deca-BDE has lower bioaccumulative potential (43) and lower biologic activity (45) than the lower PBDE congeners, it is still a source of public health concern. Away from sunlight, deca-BDE likely persists in soils and sediments. In sunlight, the deca-BDE readily degrades to the lower brominated congeners (e.g., tetra- to hexa-BDEs) (43,46,47), which themselves readily bioaccumulate [the tetra-and penta-BDE bioaccumulate almost as well as the PCBs (48,49)]. Currently, it is unclear what proportion of the tetra- to hexa-BDEs in the environment are breakdown products of the deca-BDE congener and what proportion comes from the commercial penta-BDE mixtures.

Tissue levels: humans. Although PBDEs have been measured in humans, animals, and environmental samples for some years (2), the exponential increase of tetra- to hexa-BDEs in Swedish breast milk has galvanized gal·va·nize
tr.v. gal·va·nized, gal·va·niz·ing, gal·va·niz·es
1. To stimulate or shock with an electric current.

2. interest. In the Noren study (Figure 1), milk samples were pooled from native Swedes living in the Stockholm region, with the proportion of primiparae (55-65%) and the average age of donors kept reasonably constant (1). Numbers of mothers in the pools varied from 75 to 116 during 1972-1985 and from 20 to 40 during 1990-1997 (50). 2,2',4,4'-tetra-BDE was the major congener (60-70%), and it was present at approximately 2.3 ng/g lipid in 1997 (1,51). Another recent Swedish breast milk study found wide interindividual variability in PBDEs levels from 39 first-time mothers (1.1-28.2 ng/g fat), with mean levels similar to those reported in the pooled samples in the Noren study (52).

The predominant congeners in human tissues are the three ortho-para-(2,4-) substituted congeners: 2,2',4,4'-tetra-BDE (PBDE-47); 2,2',4,4',5-penta-BDE (PBDE-99); and 2,2',4,4',5,5'-hexa-BDE (PBDE-153). These were present in recent human adipose tissue samples from Sweden at levels ranging from 0.3 to 98.2 ng/g lipid (53,54). Similar levels of the tetra- to hexa-BDEs were found in adipose tissue samples from Spain (55), Israel (56), and' the United States (57). This raises the possibility that exponential increases in PBDEs are occurring worldwide. In the few studies that have measured deca-BDE in environmental samples, deca-BDE is less prevalent in biota than the lower brominated congeners. PBDE congener patterns in humans may provide information on the nature or pathway of the PBDE exposures, much in the manner of the DDE (Dynamic Data Exchange) A message protocol in Windows that allows application programs to request and exchange data between them automatically.

DDE - Dynamic Data Exchange :DDT ratio. Low tetra:deca BDE See Borland Database Engine. ratios suggest direct, recent, or occupational exposures to the parent product. Higher ratios may indicate an environmental pathway, where exposures stem from PBDEs that have leached from commercial products and that have been degraded in the environment.

Deca-BDE levels in human samples may be more likely to arise from direct exposures. For example, whereas breast milk samples had high tetra:deca-BDE ratios, serum samples from dismantlers at an electronics-recycling plant had low tetra:deca-BDE ratios (58). The levels of five PBDE congeners, including deca-BDE, in the serum taken from the dismantlers were significantly higher than levels in samples taken from clerks in the same plant or from a control group of hospital cleaners. Thus, deca-BDE, even with its high MW, is bioavailable.

Tissue levels: animals. PBDE levels have been measured in marine and terrestrial life. These analyses have primarily been conducted on samples taken from the North Atlantic Ocean North Atlantic Ocean

The northern part of the Atlantic Ocean, extending northward from the equator to the Arctic Ocean. and from Northern Europe. The predominant congeners are the tetra- to hexa-BDEs. Levels of PBDEs on a nanogram nanogram /nano·gram/ (ng) (nan?o-gram) one billionth (10-9) of a gram.

nan·o·gram
n. Abbr. ng
One billionth (10^-9) of a gram. per gram lipid basis include: cod liver (3-170), herring (100), trout (100-170), eel (14,000-17,000), pike (27,000), guillemot guillemot (gĭl`əmŏt'), northern sea bird, genus Cephas, of the auk family. The black guillemot, or trystie, Cephus grylle, is about 13 in. egg (2,000), osprey osprey (ŏs`prē), common name for a bird of prey related to the hawk and the New World vulture and found near water in most parts of the world. (0.16-19,000), cormorant liver (28,000), seal blubber (2.6-1,470), sperm whale (79-136), pilot whale (843-3,160), reindeer (0.5), and moose (1.7) (2,53,59,60-65).

Current levels of PCBs or DDTs are considerably higher (10- to 500-fold) than PBDE levels. For example, levels of PCBs or DDTs (in nanogram per gram lipid) in Northern Europe were roughly 10-fold higher than PBDEs in herring, 300- to 400-fold higher in grey seals, and approximately 40-fold higher in osprey (63). However, if the trends in contaminant levels in human milk (Figure 1) and the environment continue, PBDEs will replace PCBs/DDTs as the major environmental POP over the next 15-30 years.

Little is known of environmental levels of PBDEs in the United States. PBDE levels (di- to hepta-BDE) in whole homogenates of Lake Ontario trout were between 200 and 300 pg/g lipid (66). Recent PBDE levels in the muscle tissue of other Great Lakes fish averaged 3,000 ng/g lipid (the sum of six prominent congeners) (67).

Toxicology. PBDEs have some structural similarities to the PCBs and PBBs, the DDT family, the herbicide nitrofen, the PCDDs/PCDFs, and thyroxine ([T.sub.4]) (Figure 2), and they appear to share some toxicologic properties as well. The available data suggest that the lower (tetra- to hexa-) PBDE congeners are likely to be carcinogens Carcinogens
Substances in the environment that cause cancer, presumably by inducing mutations, with prolonged exposure.

Mentioned in: Colon Cancer, Rectal Cancer , endocrine disruptors, and/or neurodevelopmental toxicants.

Deca-BDE, the major commercial product, is expected to be one of the least active congeners because of its poorer 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. . Likely due to its high MW, deca-BDE is poorly absorbed by 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. (approximately 0.3%) and is rapidly eliminated in rodents (half-life [is less than] 1 day) (68). This contrasts with the lower brominated congeners, which are almost completely absorbed and have half-lives in rodents that are comparable to or longer than TCDD (20-30 days for a tetra-BDE or 45-119 days for two hexa-BDEs in rats) (69,70). Activities of several enzymes induced by a commercial penta-BDE mixture in rats remained significantly elevated for 30-60 days after the last exposure, again suggesting long half-lives for the lower brominated congeners (45,71). Because the half-lives of these congeners in rodents are comparable to that of TCDD (69), the lower PBDEs are also likely to persist in humans.

Among commercial PBDE mixtures, those containing lower congeners are stronger inducers of liver enzymes in rats [i.e., penta-BDE [is greater than] octa-BDE [is greater than] deca-BDE (45,71)]. This is similar to the relative activities of the structurally related PBBs, where the lower congeners are generally more active. For the PBDEs, the greater activities of the lower congeners may be due to their greater bioavailability or to their higher affinities for receptor proteins.

Cancer. Human data on PBDE carcinogenicity carcinogenicity /car·ci·no·ge·nic·i·ty/ (kahr?si-no-je-nis´i-te) the ability or tendency to produce cancer.

carcinogenicity

the ability or tendency to produce cancer. are limited. One study cited an association between adipose tissue levels of PBDE-47 and the risk of non-Hodgkin lymphoma (NHL NHL Non-Hodgkin's lymphoma, see there ) among Swedish hospital patients (54). Other studies cited similar associations for PCB levels and the risk of NHL (72), and for PBB PBB: see polybrominated biphenyl. levels and the risk of lymphoma and breast cancer (73, 74).

In animals, only the fully brominated and poorly absorbed (0.3%) deca-BDE has been tested for carcinogenicity in long-term studies (68,75). In mice, results from the National Toxicology Program National Toxicology Program Environment A program that conducts toxicologic tests on substances frequently found at the EPA's National Priorities List sites, which have the greatest potential for human exposure bioassay Bioassay

A method for the quantitation of the effects on a biological system by its exposure to a substance, as well as the quantitation of the concentration of a substance by some observable effect on a biological system. (68) were marginally positive. Deca-BDE produced statistically significant increases in hepatocellular adenomas and carcinomas (combined) in male mice, but the increases were within the range of historical controls. Marginal increases in thyroid gland follicular cell adenomas or carcinomas (combined) were observed for male and female mice. PCBs and dioxin-like compounds disrupt thyroid hormone balance.

Stronger effects of deca-BDE were seen in rats, with significant dose-related increases in liver neoplastic neoplastic /neo·plas·tic/ (ne?o-plas´tik)
1. pertaining to a neoplasm.

2. pertaining to neoplasia.

neoplastic

pertaining to neoplasia or a neoplasm. nodules Nodules
A small mass of tissue in the form of a protuberance or a knot that is solid and can be detected by touch.

Mentioned in: Leprosy (adenomas) in both males and females. An earlier bioassay in rats, using fewer animals and much lower doses of deca-BDE, found no statistically significant increases in tumors (75), as might be expected. Liver tumors were the primary tumors observed in rodent cancer bioassays of PCBs and PBBs, which are structurally related to the PBDEs.

Evidence for Ah receptor mechanism. Although PBDEs have not been tested for their ability to bind to the Ah receptor, mechanistic studies indicate that some PBDE congeners exhibit significant Ah receptormediated (e.g., dioxin-like) effects, with penta-DBE activity greater than tetra-DBE activity. In rats for example, commercial-grade penta-BDE was a more powerful inducer inducer /in·duc·er/ (in-dldbomacs´er) a molecule that causes a cell or organism to accelerate synthesis of an enzyme or sequence of enzymes in response to a developmental signal.

in·duc·er
n. of ethoxyresorufin-o-deethylase (EROD EROD Education Resource Organizations Directory
EROD Ethoxyresorufin-O-deethylation
EROD Early Return of Dependents
EROD Electronic Record of Deposit (pending tranfer) ) activity, a standard assay for dioxin-like compounds, than commercial PCBs (Aroclor 1254). The penta-BDE mixture was active at lower levels (3 mg/kg) than the model inducers, 3-methylcholanthrene, or most PCB mixtures (69). In mice, commercial penta-BDE induced EROD activities and suppressed the immune response, which are consistent with Ah receptor-mediated effects (76).

PBDE-47, the major congener in human and marine tissues, also induced EROD activities in rats (6 mg/kg for 2 weeks), albeit less powerfully than PCBs (Aroclor 1254) (77). The tetra-BDE has less dioxin-like activity than the commercial penta-BDE product [comparing the results of yon Meyerinck et al. (69) and Hallgren and Darnerud (77)].

Ah receptor-mediated activities of PBDEs also have been investigated using the rat hepatoma hepatoma /hep·a·to·ma/ (hep?ah-to´mah)
1. a tumor of the liver.

2. hepatocellular carcinoma (malignant h.).

hep·a·to·ma
n. pl. cell line H-4-II E. A commercial formulation of penta-BDE induced EROD levels in the H-4-II E cells with an estimated potency of one-millionth that of TCDD (78). In a study of 17 specific PBDE congeners, 7 congeners acted as Ah-recep-tor agonists and 9 congeners acted as antagonists when co-treated with TCDD (79). The potencies of the agonists were comparable to the potencies of some mono-ortho PCBs (79).

The PCDEs similarly induce EROD, also with penta activity greater than tetra activity (80,81). These observations agree with molecular modeling predictions of the interactions between PCDEs and the Ah receptor, where chlorines in the ortho positions are predicted to enhance binding to the receptor of the more highly chlorinated chlorinated /chlo·ri·nat·ed/ (klor´i-nat?ed) treated or charged with chlorine.

chlorinated

charged with chlorine.

chlorinated acids
some, e.g. PCDEs (82). Thus, the enzyme induction data and modeling predictions for the PCDEs support the Ah receptor-mediated activity of the PBDEs.

Additional evidence for PBDE dioxin-like activity comes from the induction of EROD by coadministration of tetra-BDE and PCBs (Aroclor 1254). The effects of PBDE and PCBs were additive, suggesting that the two POP families operate through similar mechanisms (77).

Genotoxicity Genotoxic substances are a type of carcinogen, specifically those capable of causing genetic mutation and of contributing to the development of tumors. This includes both certain chemical compounds and certain types of radiation. . The genotoxicity profiles of PBDEs and PCBs are similar. As with the commercial PCB mixtures, the deca-, octa-, and penta-BDE commercial mixtures were not mutagenic mutagenic

inducing genetic mutation. in Salmonella typhimurium (2,68,83). As with two technical mixtures of PCBs, two PBDE technical mixtures of mono- or di-BDEs induced genetic recombination in two mammalian cell lines, whereas the tetra-BDE mixture was positive in one cell line (84). In recent metabolic studies of [[sup.14]C]PBDE-47 in rats and mice, tetra-BDE was covalently bound to macromolecules Macromolecules
A large molecule composed of thousands of atoms.

Mentioned in: Gene Therapy

macromolecules in various tissues, with evidence for a reactive epoxide epoxide /epox·ide/ (e-pok´sid) an organic compound containing a reactive group resulting from the union of an oxygen atom with two other atoms, usually carbon, that are themselves joined together. intermediate (70).

Endocrine effects. The lower PBDEs disrupt thyroid hormone balance. In rats, commercial-grade penta-BDE (2, 10, or 200 mg/kg/day for 90 days) reduced thyroid hormone levels and increased incidences of thyroid hyperplasia, with effects at all dose levels (83). In mice, the penta-BDE also significantly reduced [T.sub.4] levels 8 days after a single exposure and at the lowest dose tested (0.8 mg/kg) (76). PBDE-47, the major congener in human and animal tissues, reduced thyroid hormone levels in female rats at a dose of 18 mg/kg (77). The effects of tetra-BDE in reducing levels of thyroid hormones were additive with coadministered PCBs (Aroclor 1254) or chlorinated paraffins (77).

Higher PBDE congeners also have the potential to disrupt thyroid hormone balance. Deca-BDE produced statistically significant increases in the incidences of thyroid hyperplasia and marginal increases in the incidences of tumors of the thyroid among male and female mice in 2-year feeding studies (68). Commercial octa-BDE administered to rats for 90 days resulted in thyroid changes (2). Also, 4 of 35 production workers in a deca-BDE and deca-BB manufacturing plant manifested clinical hypothyroidism hypothyroidism: see thyroid gland. , with one case reportedly exposed only to deca-BDE. No cases of thyroid dysfunction were observed among 89 age- and sex-matched unexposed workers (85).

Studies of the structurally related PCDEs offer some supporting evidence that PBDEs disrupt thyroid hormone balance. Three specific congeners (2',3,4,6'-tetra-CDE; 2,2',4,5,6'-penta-CDE; and 2,2',4,4',5,5'-hexa-CDE) administered to pregnant rats resulted in reductions of [T.sub.4] levels in dams and in offspring exposed in utero (86).

The mechanism of PBDE-induced thyroid hormone disruption is unclear. PBDEs may induce UDP-glucuronosyltransferases, which increases the rate of [T.sub.4] conjugation conjugation, in genetics
conjugation, in genetics: see recombination.

conjugation, in grammar
conjugation: see inflection. and excretion. Alternatively, PBDEs or their hydroxy hy·drox·y
adj.
Containing the hydroxyl group.

[From hydroxyl.]

hydroxy

Containing the hydroxyl group (OH).

Adj. 1. metabolites Metabolites
Substances produced by metabolism or by a metabolic process.

Mentioned in: Interactions may mimic [T.sub.4] or [T.sub.3] because these hormones are hydroxy-halogenated diphenyl ethers (Figure 2). This mechanism is supported by observations from metabolic studies of tetra-BDE, in which hydroxy-tetra-BDE metabolites were found (70). Hydroxy-PBDEs (as with hydroxy-PCBs) may reduce [T.sub.4] levels by competing with [T.sub.4] for the thyroid hormone transport protein, transthyretin (86).

Developmental toxicity. Neurodevelopmental toxicity has been reported for a tetra-BDE congener, PBDE-47, and a penta-BDE congener, PBDE-99, the major congeners in human tissues. PBDE-47 (0.7 mg) and PBDE-99 (10.5 mg) administered to mice on postnatal postnatal /post·na·tal/ (-na´t'l) occurring after birth, with reference to the newborn.

post·na·tal
adj.
Of or occurring after birth, especially in the period immediately after birth. day 10 resulted in permanent aberrations in motor behavior that worsened with age. Neonatal exposure to PBDE 99 also reduced learning and memory in adult mice (87). Similar effects occurred in mice that were neonatally exposed to some of the ortho-substituted PCBs and coplanar PCBs (87).

Commercial formulations of penta-, octa-, and deca-BDEs give equivocal results in developmental studies. Although increases in embryo mortality and delayed skeletal formation were observed, these effects were accompanied by maternal toxicity in all of the studies except one (with octa-BDE) (2,43).

Structurally related compounds, including PCDEs, nitrofen, and PCB/PBBs, cause developmental effects. A penta- and a tetra-CDE decreased the number of litters born, the perinatal growth, and pup survival in mice when administered from gestational days 6-15 (88). Nitrodiphenyl ethers, including the herbicide nitrofen (2,4-dichlorophenyl-4'-nitrophenyl ether) caused pronounced perinatal and postnatal toxicity, which are believed to be thyroid hormone-mediated outcomes [reviewed by Rosiak et al. (88)]. Moreover, PCBs and PBBs are well recognized as developmental toxicants (89). In mechanistic and structure-activity studies, the di- to penta-CDE congeners showed greater activity than ortho-PCBs in perturbing [Ca.sup.2+] neuronal homeostasis homeostasis

Any self-regulating process by which a biological or mechanical system maintains stability while adjusting to changing conditions. Systems in dynamic equilibrium reach a balance in which internal change continuously compensates for external change in a feedback and other effects associated with ortho-PCB neurobehavioral toxicity (90).

Conclusion

The observation of rising levels of PBDEs in Swedish breast milk illustrates how BMMPs can serve to warn us of new or unrec-ognized POPs. The BMMP time-trend data have spurred research in the last year on the occurrence and toxicity of PBDEs. Monitoring programs are needed to determine PBDE levels in U.S. populations. In addition, BMMPs are needed in the United States to fill data gaps for other POPs, especially for PCDDs/PCDFs and PCBs. No BMMPs exist to monitor PBDE levels or time trends in the United States.

PBDE toxicology is incomplete. Ecologic, neurodevelopment, and thyroid function studies and 2-year rodent cancer bioassays are needed for some congeners, including PBDE-47 and the commercial formulations of penta- and octa-BDEs. Even in the absence of further studies, however, it seems clear that less toxic alternatives to persistent PBDE flame retardants are desirable, given the suggestive parallels between PBDE and PCB toxicology.

Several studies found that prenatal, and not lactational, exposures to polyhalogenated POPs were critical for childhood cognitive-motor deficits. If this is true, the health of the fetus and the infant can be protected only by limiting in utero exposures to POPs, which can be accomplished only by limiting the mother's exposures. Given the proclivity pro·cliv·i·ty
n. pl. pro·cliv·i·ties
A natural propensity or inclination; predisposition. See Synonyms at predilection.

[Latin pr of POP compounds to persist, seek out fat, and biomagnify up the food chain, it is hard to see how the mother's exposures can be limited except by broad preventative strategies (e.g., replacing POPs with biodegradable or environmentally friendly alternatives) (34). Concentrations of POPs in breast milk serve as markers for in utero and lactational exposures. In conjunction with BMMPs, these markers will allow us to assess POP body burdens and monitor the progress of our preventative strategies.

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PGH Proyecto Genoma Humano (Spanish)
PGH Philadelphia General Hospital
PGH Palace of the Golden Horses
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(40.) Albers JMC JMC Joint Military Commission
JMC Jefferson Medical College
JMC Jax Money Crew (computer gaming)
JMC Joint Munitions Command (US Army; Rock Island Arsenal, Rock Island IL)
JMC James Madison College , Kreis IA, Liem AKD AKD Alpha Kappa Delta (Sociology National Honor Society)
AKD Alkyl Ketene Dimer
AKD Automatic Key Distribution
AKD Aqeel Karim Dhedi (Securities; Pakistan)
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(44.) Memorandum from U.S. EPA EPA eicosapentaenoic acid.

EPA
abbr.
eicosapentaenoic acid

EPA,
n.pr See acid, eicosapentaenoic.

EPA,
n. Office of Pollution Prevention and Toxics to T. McDonald, California Environmental Protection Agency The California Environmental Protection Agency (Cal/EPA) was created in 1991 by Governor Pete Wilson, through an executive order.^[1] The agency combined six board, departments, and offices into one cabinet-level office:^[2]

. TSCA TSCA Toxic Substances Control Act of 1976 (15 USC)
TSCA Traditional Small Craft Association (Mystic, CT, USA)
TSCA Tibetan Spaniel Club of America
TSCA Traditional Siamese Cat Association inventory update rule information, 16 September 1999.

(45.) Carlson GP. Induction of xenobiotic xen·o·bi·ot·ic
adj.
Foreign to the body or to living organisms. Used of chemical compounds.

n.
A xenobiotic chemical.

xenobiotic

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hex·ane
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n.
The increase in the concentration of a substance, especially a contaminant, in an organism or in the food chain over time. kinetics of brominated flame retardants (polybrominated diphenyl ethers)in blue mussels (Mytilus edulis). Environ Toxicol Chem 18(6):1218-1224 (1999).

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(64.) Pijnenburg AM, Everts Everts may refer to:

To turn inside out (see wiktionary)
Stefan Everts, motocross racer
Everts Township, Minnesota
Eversion (kinesiology)

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(65.) de Boer J, Wester PG, Klamer HJC HJC Hillsborough Justice Campaign (UK)
HJC Hwa Chong Junior College (Singapore)
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(68.) NTP (Network Time Protocol) A TCP/IP protocol used to synchronize the real time clock in computers, network devices and other electronic equipment that is time sensitive. It is also used to maintain the correct time in NTP-based wall and desk clocks. . Toxicology and Carcinogenesis car·ci·no·gen·e·sis
n.
The production of cancer.

carcinogenesis

production of cancer.

biological carcinogenesis
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Compared with case-control study, nested case-control study can reduce 'recall bias' and temporal ambiguity, and compared with of non-Hodgkin lymphoma and serum organochlorine residues. Lancet 350(9073):240-244 (1997).

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de-
pref.
1. Do or make the opposite of; reverse: decomposition.

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(79.) Meerts IATM IATM International Association of Tour Managers Ltd.
IATM Intel Advanced Thermal Manager
IATM It's All Too Much (Beatles song) , Luijks EAC EAC an abbreviation used in studies of complement, in which E represents erythrocyte, A antibody, and C complement. , Marsh G, Jakobsson E, Bergman A, Brouwer A. Polybrominated diphenyl ethers (PBDEs) as Ah-receptor agonists and antagonists. Organohalogen Compounds 37:147-150 (1998).

(80.) Howie L, Dickerson R, Davis D, Safe S. Immunosuppressive Immunosuppressive
Any agent that suppresses the immune response of an individual.

Mentioned in: Antirheumatic Drugs, Graft-vs.-Host Disease, Immunosuppressant Drugs

immunosuppressive

1. pertaining to or inducing immunosuppression.

2. and monooxygenase induction activities of polychlorinated diphenyl ether congeners in C57BL/6N mice: quantitative structure-activity relationships. Toxicol Appl Pharmacol 105(2):254-263 (1990).

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(83.) 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 . [TSCA Section] 8(e) TRIAGE triage

Division of patients for priority of care, usually into three categories: those who will not survive even with treatment; those who will survive without treatment; and those whose survival depends on treatment. Chemical Studies Database. Available: http://www.epa.gov/docs/8e_triag/[cited 5 May 1999]. [8(e) report numbers 04780A, 04856A, and 05420A.]

(84.) Helleday T, Tuominen KL, Bergman A, Jenssen D. Brominated flame retardants induce intragenic recombination recombination, process of "shuffling" of genes by which new combinations can be generated. In recombination through sexual reproduction, the offspring's complete set of genes differs from that of either parent, being rather a combination of genes from both parents. in mammalian cells. Mutat Res 439(2):137-147 (1999).

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(87.) Eriksson P, Jakobsson E, Fredriksson A. Developmental neurotoxicity neurotoxicity /neu·ro·tox·ic·i·ty/ (noor?o-tok-sis´it-e) the quality of exerting a destructive or poisonous effect upon nerve tissue. of brominated flame-retardants, polybrominated cliphenyl ethers and tetrabromo-bisphenol A. Organohalogen Compounds 35:375-377 (1998).

(88.) Rosiak K, Li MH, Degitz SJ, Skalla DW, Chu I, Francis BM. Maternal and developmental toxicity of polychlorinated diphenyl ethers (PCDEs)in Swiss-Webster mice and Sprague-Dawley rats. Toxicology 121(3):191-204 (1997).

(89.) Office of Environmental Health Hazard Assessment, California Environmental Protection Agency. Proposition 65 [Safe Drinking Water and Toxic Enforcement Act of 1986] Information. Proposition 65 List. Available http://www.oehha.ca.gov/prop65/[cited 6 August 1999].

(90.) Kodavanti PR, Ward TR, McKinney JD, Waller CL, Tilson HA. Increased [[sup.3]H]phorbol phorbol /phor·bol/ (for´bol) a polycyclic alcohol occurring in croton oil; it is the parent compound of the phorbol esters.

phorbol ester ester binding in rat cerebellar cerebellar /cer·e·bel·lar/ (ser?e-bel´ar) pertaining to the cerebellum.

Cerebellar
Involving the part of the brain (cerebellum), which controls walking, balance, and coordination. granule cells and inhibition of [sup.45][Ca.sup.2+] sequestration sequestration

In law, a writ authorizing a law-enforcement official to take into custody the property of a defendant in order to enforce a judgment or to preserve the property until a judgment is rendered. in rat cerebellum cerebellum (sĕr'əbĕl`əm), portion of the brain that coordinates movements of voluntary (skeletal) muscles. It contains about half of the brain's neurons, but these particular nerve cells are so small that the cerebellum accounts for by polychlorinated diphenyl ether congeners and analogs: structure-activity relationships. Toxicol Appl Pharmacol 138(2):251-61 (1996).

Address correspondence to K. Hooper, Hazardous Materials Laboratory, California Environmental Protection Agency, 2151 Berkeley Way, Berkeley, CA 94707 USA. Telephone: (510) 540-3499. Fax: (510) 540-2305. E-mail: kim_hooper@hotmail.com

The views expressed are those of the authors and do not necessarily represent those of the California Environmental Protection Agency or the state of California.

Received 21 September 1999; accepted 12 November 1999.

Kim Hooper(1) and Thomas A. McDonald(2)

(1) Hazardous Materials Laboratory, California Environmental Protection Agency, Berkeley, California, USA;

(2) Office of Environmental Health Hazard Assessment, California Environmental Protection Agency, Oakland, California, USA

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Author:	McDonald, Thomas A.
Publication:	Environmental Health Perspectives
Date:	May 1, 2000
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