Prevention of immune cell apoptosis as potential therapeutic strategy for severe infections.Some 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. cell types whose numbers are normally controlled through programmed cell death pro·grammed cell death n. See apoptosis. programmed cell death proposed system of cell death, often including poly(ADP)-ribosylation, ensures that a cell will not survive if it is so badly damaged that its recovery would harm the are subject to markedly increased destruction during some severe infections. Lymphocytes, in particular, undergo massive and apparently unregulated apoptosis in human patients and laboratory animals with sepsis, potentially playing a major role in the severe immunosuppression immunosuppression Suppression of immunity with drugs, usually to prevent rejection of an organ transplant. Its aim is to allow the recipient to accept the organ permanently with no unpleasant side effects. that characterizes the terminal phase of fatal illness. Extensive lymphocyte apoptosis has also occurred in humans and animals infected with several exotic agents, including Bacillus anthracis Bacillus anthracis Infectious disease A gram-positive organism which causes often fatal infections when its endospores–resistant to heat, drying, UV light, gamma radiation, and many disinfectants–enter the body and cause septicemia Military medicine , the cause of anthrax; Yersinia pestis Yersinia pes·tis n. A bacterium that causes plague and is transmitted from rats to humans by the rat flea Xenopsylla cheopis. Also called Pasteurella pestis. , the cause of plague; and Ebola virus Ebola virus (ēbō`lə), a member of a family (Filovirus) of viruses that cause hemorrhagic fevers. The virus, named for the region in Congo (Kinshasa) where it was first identified in 1976, emerged from the rain forest, where it survives in . Prevention of lymphocyte apoptosis, through either genetic modification of the host or treatment with specific inhibitors, markedly improves survival in murine murine /mu·rine/ (mur´en) pertaining to, derived from, or characteristic of mice or rats. mu·rine adj. sepsis models. These findings suggest that interventions aimed at reducing the extent of immune cell apoptosis could improve outcomes for a variety of severe human infections, including those caused by emerging pathogens and bioterrorism agents. ********** Despite success in controlling many infectious diseases, efforts to defend against the wide range of microbes that threaten human health continue to be challenged by the unexpected emergence of novel pathogens and possible use of a variety of virulent agents as biological weapons. A defensive strategy based solely on developing new vaccines and antimicrobial and antiviral drugs Antiviral Drugs Definition Antiviral drugs are medicines that cure or control virus infections. Purpose Antivirals are used to treat infections caused by viruses. , each specific for only 1 or a few agents, is unlikely to be successful in dealing with potential microbial microbial pertaining to or emanating from a microbe. microbial digestion the breakdown of organic material, especially feedstuffs, by microbial organisms. threats and will be exceedingly expensive. An alternative approach attempts to identify mechanisms shared by most or all severe infections that could be targets for pharmacologic intervention. Such generic therapies could supplement agent-specific treatment by increasing resistance to infection, potentially improving outcomes for patients in a variety of disease states. One physiologic process that characterizes some severe infections is a massive loss of lymphocytes, dendritic cells, gastrointestial epithelial cells Epithelial cells Cells that form a thin surface coating on the outside of a body structure. Mentioned in: Corneal Transplantation , and other cell types through apoptosis, or programmed cell death. This process is an apparent acceleration or dysregulation of the same process by which these cell populations are regulated during normal health (1,2). By impairing the development of adaptive immune responses needed for recovery, the apoptotic destruction of lymphocytes and dendritic cells could have a particularly adverse effect on disease outcome. Fortunately, because programmed cell death is an orderly biochemical process triggered by specific stimuli and executed by a limited range of enzymes, it could be inhibited through pharmacologic countermeasures, offering a novel approach to therapy. We begin this article by summarizing evidence that a massive apoptotic loss of lymphocytes takes place in humans during the course of septic shock and describing similar findings in animal models of sepsis. Data are then presented that indicate that a marked die-off of lymphocytes also occurs in Ebola hemorrhagic fever Noun 1. Ebola hemorrhagic fever - a severe and often fatal disease in humans and nonhuman primates (monkeys and chimpanzees) caused by the Ebola virus; characterized by high fever and severe internal bleeding; can be spread from person to person; is largely limited to , anthrax, and plague, which suggests that unregulated apoptosis of these cells is a component of many, and perhaps all, severe infectious processes and may contribute to high case fatality rates by impairing adaptive immune function. After describing encouraging results obtained in proof-of-concept tests of antiapoptotic interventions in lethal murine models of sepsis, we note some potential limitations of such therapy that could slow its introduction into the therapeutic regimen. Whatever the potential role of such strategies, improved understanding of the causes, time course, and extent of programmed cell death will aid management of patients with severe infections. Mechanism and Regulation of Apoptosis Apoptosis, or programmed cell death, is the method by which tissue remodeling remodeling /re·mod·el·ing/ (re-mod´el-ing) reorganization or renovation of an old structure. bone remodeling takes place during normal growth and development and the physiologic mechanism by which labile cell populations such as gastrointestinal epithelial cells, lymphocytes, dendritic cells, and neutrophils neutrophils (ner·ō·trōˑ·filz), n.pl white blood cells with cytoplasmic granules that consume harmful bacteria, fungi, and other foreign materials. are regulated. Apoptosis is of particular importance for the immune system as the means by which self-recognizing lymphocytes are deleted and expanded lymphocyte populations are reduced at the conclusion of an acute immune response (3). This closely regulated, energy-requiring process can be initiated through 2 different mechanisms, each based on the successive activation of preexisting pre·ex·ist or pre-ex·ist v. pre·ex·ist·ed, pre·ex·ist·ing, pre·ex·ists v.tr. To exist before (something); precede: Dinosaurs preexisted humans. v.intr. but dormant cysteine-aspartate proteases, or caspases (Figure 1). [FIGURE 1 OMITTED] As its name implies, the intrinsic apoptotic pathway begins within the cell, when toxic alterations bring about a decrease in 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 transmembrane transmembrane /trans·mem·brane/ (trans-mem´bran) extending across a membrane, usually referring to a protein subunit that is exposed on both sides of a cell membrane. trans·mem·brane adj. potential, leading to the opening of mitochondrial membrane pores and the release of cytochrome C and other substances into the cytoplasm cytoplasm: see protoplasm. cytoplasm Portion of a eukaryotic cell outside the nucleus. The cytoplasm contains all the organelles (see eukaryote). . The extrinsic pathway, by contrast, is triggered by extracellular events through the binding to cell surface receptors of tumor necrosis factor tumor necrosis factor n. Abbr. TNF A protein that is produced in the presence of an endotoxin, especially by monocytes and macrophages, is able to attack and destroy tumor cells, and exacerbates chronic inflammatory diseases. (TNF TNF abbr. tumor necrosis factor TNF, n an abbreviation for tumor necrosis f ) superfamily superfamily /su·per·fam·i·ly/ (soo´per-fam?i-le) 1. a taxonomic category between an order and a family. 2. death ligands, including TNF-[alpha] and Fas ligand. Although the intrinsic pathway involves early activation of caspase-9, and the extrinsic pathway is mediated through caspase-8, both lead to activation of the "executioner" caspase-3 and a variety of proteases and endonucleases. Once begun, apoptosis may be described as an orderly disassembly dis·as·sem·ble v. dis·as·sem·bled, dis·as·sem·bling, dis·as·sem·bles v.tr. To take apart: disassemble a toaster. v.intr. 1. of the cell from within. Chromosomal DNA DNA: see nucleic acid. DNA or deoxyribonucleic acid One of two types of nucleic acid (the other is RNA); a complex organic compound found in all living cells and many viruses. It is the chemical substance of genes. is cleaved cleaved (klevd) split or separated, as by cutting. into oligonucleosomal segments, the nucleus is divided into discrete subunits, and the cell itself is partitioned into multiple membrane-bound fragments whose outer surfaces are marked by large numbers of phosphatidylserine molecules, leading to their rapid uptake by phagocytes. Because all multicellular organisms use programmed cell death to maintain and modify their tissues, this process does not evoke an inflammatory response, and its end products actually serve as antiinflammatory stimuli. Apoptosis thus differs markedly from necrosis, the chaotic breakdown resulting from trauma and other types of damage, in its morphologic and immunologic features (Table 1). Necrosis is characterized by the early loss of outer membrane function, rapid 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, swelling and disintegration, and release of cell contents into surrounding tissues, which evoke an intense inflammatory response. A large number of cell-surface and cytoplasmic proteins participate in the detection and processing of signals that tip the balance toward or away from programmed cell death. These include members of the Bcl-2 protein family, which have both proapoptotic and antiapoptotic activity (Bcl-2 is antiapoptotic), and other inhibitors (Figure 1). Despite these elaborate control mechanisms, innate or acquired defects in the control of apoptosis may lead to a variety of disease states. For example, excessive inhibition of apoptosis is an underlying mechanism of cancer, while an inappropriate increase is seen in some neurodegenerative diseases and other conditions. Lymphocyte Apoptosis in Sepsis During normal health, the immediate fate of each lymphocyte is determined through continuous summation of a stream ofproapoptotic and antiapoptotic signals that arrive from its external environment and from its internal cytoplasmic milieu. A shift toward initiation of apoptosis should therefore be expected during the early phase of sepsis, when bacteria or their byproducts stimulate macrophages Macrophages White blood cells whose job is to destroy invading microorganisms. Listeria monocytogenes avoids being killed and can multiply within the macrophage. to release proapoptotic substances such as TNF-[alpha], nitric oxide, and glucocorticoids Glucocorticoids Any of a group of hormones (like cortisone) that influence many body functions and are widely used in medicine, such as for treatment of rheumatoid arthritis inflammation. . As the disease develops, accumulating products of lymphocyte apoptosis can act as antiinflammatory stimuli, which contribute to the immunosuppression commonly observed as sepsis progresses to septic shock, and which can lead to a state of immune paralysis before death (2,3). Numerous studies have demonstrated a massive apoptotic loss of lymphocytes during sepsis. A prospective investigation in adult patients compared spleens obtained either intraoperatively or within 6 hours after death from sepsis or trauma and found that those from sepsis patients showed a marked decrease in B cells and CD4 T cells CD4 T cells Helper T cells, see there (Figure 2) (1). The degree of 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. B-cell depletion corresponded with the duration of sepsis. Active caspase-9 was present in splenic lymphocytes with apoptotic features, suggesting a mitochondrial-mediated pathway of cell death, although evidence indicates that apoptotic cell death in patients with sepsis can also proceed by the death receptor pathway (4). In most patients, loss of cells from the spleen corresponded with a premortem decrease in circulating lymphocytes. [FIGURE 2 OMITTED] These findings were closely paralleled in another postmortem postmortem /post·mor·tem/ (post-mort´im) performed or occurring after death. post·mor·tem adj. Relating to or occurring during the period after death. n. See autopsy. study, which showed that B and T cells and dendritic cells were markedly depleted in lymphoid lymphoid /lym·phoid/ (lim´foid) resembling or pertaining to lymph or tissue of the lymphoid system. lym·phoid adj. Of or relating to lymph or the lymphatic tissue where lymphocytes are formed. organs of children dying of sepsis and that >3% of cells exhibited histologic signs of apopotosis (5). Approximately 15% of patients had prolonged lymphopenia during their terminal course. This report suggested a possible stimulus for apoptosis, in the form of persistent hypoprolactinemia, because prolactin prolactin /pro·lac·tin/ (-lak´tin) a hormone of the anterior pituitary that stimulates and sustains lactation in postpartum mammals, and shows luteotropic activity in certain mammals. pro·lac·tin n. up-regulates expression of the antiapoptotic protein Bcl-2. A third study also noted a profound loss of B and T cells in the spleens of neonates who died of sepsis and chorioamnionitis. Another study compared premortem blood counts in patients with septic shock, sepsis without shock, or nonseptic critical illness and found that increased lymphocyte apoptosis began early in septic shock, and that severe lymphopenia was predictive of a fatal outcome (6,7). Extensive loss of lymphocytes through programmed cell death has also been demonstrated in animal models of lethal sepsis induced either by normal intestinal flora or by specific gram-negative bacteria. Studies using cecal cecal /ce·cal/ (se´k'l) 1. ending in a blind passage. 2. pertaining to the cecum. ce·cal adj. Of, relating to, or having the characteristics of the cecum. ligation ligation /li·ga·tion/ (li-ga´shun) the application of a ligature. tubal ligation sterilization of the female by constricting, severing, or crushing the uterine tubes. and perforation per·fo·ra·tion n. 1. The act of perforating or the state of being perforated. 2. An abnormal opening in a hollow organ or viscus, as one made by rupture or injury. Perforation A hole. (CLP 1. CLP - Cornell List Processor. 2. CLP - Constraint Logic Programming. ) in mice have shown profound lymphocyte apoptosis in multiple organs, including the thymus thymus Pyramid-shaped lymphoid organ (see lymphoid tissue) between the breastbone and the heart. Starting at puberty, it shrinks slowly. It has no lymphatic vessels draining into it and does not filter lymph; instead, stem cells in its outer cortex develop into and spleen (8). Massive lymphoid apoptosis in the spleen and lymph nodes was also observed in baboons that developed fatal septic shock after injection of Escherichia coli (9). Lymphocyte Apoptosis in Ebola Hemorrhagic Fever In addition to occurring during common forms of sepsis, a marked increase in lymphocyte apoptosis has been observed in such exotic illnesses as Ebola hemorrhagic fever. When transferred to humans from an unidentified animal reservoir, Ebola virus replicates rapidly in macrophages and dendritic cells, causing intense inflammation, high viremia viremia /vi·re·mia/ (vi-re´me-ah) the presence of viruses in the blood. vi·re·mi·a n. The presence of viruses in the bloodstream. , and spread of infection to multiple organs, with fever, 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 abnormalities, and shock (10). Case fatality rates have
reached 90% in outbreaks in central Africa.Limited data from patients and more extensive data from laboratory animals indicate that massive lymphocyte apoptosis occurs during Ebola hemorrhagic fever and may contribute to the high death rate. Thus, the few patients who survive infection develop antibodies to the virus during the second week of illness, while fatally infected persons apparently undergo terminal immunosuppression similar to that seen with septic shock (11,12). A small study of blood samples from patients in Gabon showed that fatal cases of Ebola hemorrhagic fever were characterized by extensive 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. apoptosis, particularly ofT cells, beginning at least 5 days before death, with a decrease and eventual disappearance of Bcl-2 mRNA expression (11). In survivors, by contrast, Bcl-2 mRNA was identified in circulating cells during T-cell activation. Importantly, a similar loss of Bcl-2 has been reported in circulating lymphocytes of patients with sepsis (4). Because of the difficulty of performing clinical research under the conditions of an Ebola outbreak, the pathogenesis of lethal infection has been elucidated principally through intensive studies in nonhuman primates, which develop uniformly lethal illness resembling fatal hemorrhagic fever in humans. Lymphocytes in these animals remain free of viral infection but nevertheless undergo extensive apoptosis, with early development of lymphopenia and depletion of circulating natural killer cells natural killer cells, n.pl lymphocytes that are part of innate immunity that kill foreign substances and abnormal tissues. Decreased number or activi-ty has been linked to a number of diseases, including AIDS, cancer, chronic fatigue syndrome, and CD4+ and CD8+ lymphocytes (13). Massive lymphocyte apoptosis is also observed histologically in lymph nodes, spleen, and other lymphoid tissues, beginning by day 3 postinfection. A model of Ebola virus infection in mice has demonstrated extensive lymphocytolysis in lymph nodes, spleen, and thymus, with histologic features suggestive of apoptosis (14). Lymphocyte apoptosis has also been demonstrated in vitro in cultures of Ebola virus--infected peripheral blood mononuclear mononuclear /mono·nu·cle·ar/ (-noo´kle-er) 1. having but one nucleus. 2. a cell having a single nucleus, especially a monocyte of the blood or tissues. mon·o·nu·cle·ar adj. cells, which suggests that infected monocytes monocytes, n.pl the largest of the white blood cells. They have one nucleus and a large amount of grayish-blue cytoplasm. Develop into macrophages and both consume foreign material and alert T cells to its presence. release substances that induce apoptosis in neighboring lymphocytes (15). Lymphocyte Apoptosis in Anthrax In inhalational anthrax, spores of Bacillus anthracis are carried by pulmonary macrophages to mediastinal mediastinal /me·di·as·ti·nal/ (-as-ti´n'l) of or pertaining to the mediastinum. mediastinal of or pertaining to the mediastinum. lymph nodes, where their replication results in local tissue injury, bacteremia bacteremia: see septicemia. bacteremia Presence of bacteria in the blood. Short-term bacteremia follows dental or surgical procedures, especially if local infection or very high-risk surgery releases bacteria from isolated sites. , shock, and death (16). The ability of the organism to cause rapidly overwhelming infection suggests that, as in the case of Ebola hemorrhagic fever, immunosuppression plays a role in lethal illness. Few data are available from human cases to assess whether accelerated lymphocyte apoptosis contributes to this process, but a review of autopsy findings from 41 known cases of inhalational anthrax in a 1979 outbreak in Sverdlorsk, Russia, showed massive lymphocytolysis in mediastinal lymph nodes and spleens that was morphologically consistent with apoptosis (17). Experimental evidence shows that lethal toxin (LT), an important virulence factor encoded by B. anthracis, interferes with intracellular signaling and can induce apoptosis. Ultrastructural analysis and terminal deoxynucleotidyl (TUNEL TUNEL Terminal Deoxynucleotidyl Transferase Mediated dUTP Nick End Labeling ) staining of LT-treated human monocyte--lerived dendritic cells found activation of apoptotic pathways (18). The same authors demonstrated that bone marrow dendritic cells from C57BL/6 and BALB/c mice differed in susceptibility to LT: cells derived from C57BL/6 mice underwent apoptosis and LT caused necrosis of equivalent cells from BALB/c mice. Lymphocyte Apoptosis in Plague The gram-negative bacillus bacillus (bəsĭl`əs), any rod-shaped bacterium or, more particularly, a rod-shaped bacterium of the genus Bacillus. Some bacterium in the genus cause disease, for example B. Yersinia pestis causes 2 principal forms of illness in humans, a localized infection of lymph nodes (bubonic plague) and a highly lethal septicemia septicemia (sĕptĭsē`mēə), invasion of the bloodstream by virulent bacteria that multiply and discharge their toxic products. The disorder, which is serious and sometimes fatal, is commonly known as blood poisoning. that is a particularly fulminant ful·mi·nant adj. Occurring suddenly, rapidly, and with great severity or intensity, usually of pain. ful form of septic shock (19). The striking virulence of Y. pestis in humans is attributable to a collection of outer membrane proteins (Yops) that cause immune suppression and trigger apoptosis (20). Patients dying of plague would therefore be expected to demonstrate increased lymphocyte apoptosis, but data to support this hypothesis are lacking. However, laboratory studies using a murine model of intranasal in·tra·na·sal adj. Within the nose. Y. pestis infection have provided evidence of increased lymphocyte apoptosis in the spleen by 36 hours after infection (21) (R Hotchkiss, V. Miller, unpub, data). YopH protein inhibits T cell activation by blocking early phosphorylation phosphorylation, chemical process in which a phosphate group is added to an organic molecule. In living cells phosphorylation is associated with respiration, which takes place in the cell's mitochondria, and photosynthesis, which takes place in the chloroplasts. events necessary for signal transduction through the antigen receptor (22). In tests with primary T cells or Jurkat T leukemia cells, the extended presence of YopH led to apoptosis through a mitochondria-dependent pathway, as indicated by mitochondrial breakdown, caspase activation, DNA fragmentation, and annexin V binding. Cell death could be blocked through coexpression of Bcl-[x.sub.L], an antiapoptotic protein in the Bcl-2 family, or by treatment with caspase inhibitors. Evidence of induction of apoptosis was also found in a plague model in rats, in which increased numbers of caspase-positive cells were noted in lymph nodes 36 hours after infection, most prominently in nodes containing the greatest number of bacteria, which suggests Yop-mediated apoptosis (23). However, the apoptotic cells could not be identified because of extensive tissue destruction. Multifocal multifocal /mul·ti·fo·cal/ (mul?te-fo´k'l) arising from or pertaining to many foci. mul·ti·fo·cal adj. Relating to or arising from many foci. lymphocytolysis was also observed in the white pulp of the spleen, with resultant loss of periarteriolar lymphoid sheath--associated lymphocytes. Experimental Inhibition of Apoptosis Efforts to prevent excessive lymphocyte apoptosis during severe infection have focused either on modification of the signal processing system to create an inherent bias against the triggering of cell death pathways or on inhibition of caspase activity to block their execution. Proof-of-concept experiments with murine sepsis models have shown that both approaches can improve survival. Several studies have shown that transgenic mice overexpressing the antiapoptotic protein Bcl-2 were completely protected against lymphocyte apoptosis in T cells and partially protected in B cells after CLP and showed an increase in survival (24,25). The exact protective mechanisms, however, are unclear. The authors of 1 report argued that the beneficial effect of Bcl-2 did not depend on prevention of lymphocyte apoptosis because adoptive transfer of myeloid myeloid /my·eloid/ (mi´e-loid) 1. medullary; pertaining to, derived from, or resembling bone marrow or the spinal cord. 2. having the appearance of myelocytes, but not derived from bone marrow. cells overexpressing Bcl-2 also resulted in improved survival after CLP of Rag-l-/- mice, which lack mature T and B cells (25). This finding suggests that protection resulted from the release of cytoprotective or antiinflammatory molecules from Bcl-2-overexpressing cells, from an increase in neutrophils at sites of infection, or both. Despite these findings, recent studies that showed a lower death rate after CLP in transgenic mice expressing the antiapoptotic protein Akt in T cells have added further support to the concept that prevention of lymphocyte apoptosis is an independent survival factor in sepsis (26). In addition to these reports that used the CLP model, preliminary studies have shown that Bcl-2 overexpression prevents lymphocyte apoptosis in mice infected with Y. pestis (R. Hotchkiss, unpub, data). Bcl-2 transgenic mice that overexpressed Bcl-2 in T and B lymphocytes had a marked decrease in apoptosis at 72 hours after Y. pestis infection compared with wild-type animals (Figure 3). These findings provide hope that apoptotic cell death in plague may be preventable by a Bcl-2-based therapy. [FIGURE 3 OMITTED] Pharmacologic interventions have also been used to prevent initiation of lymphocyte apoptosis in murine models of sepsis (Table 2). One approach has aimed to block initial triggering of the extrinsic pathway by preventing cellular synthesis of Fas or FasL or by administering an inhibitor of Fas-FasL binding. Both techniques have shown benefit in murine CLP studies. Preliminary studies by Chung et al. demonstrated that mice genetically deficient in FasL showed better survival after CLP than their wild-type counterparts (34), and a survival benefit was also observed when mice were treated with siRNA to block intracellular synthesis of Fas (28). Markedly improved survival was also observed when a Fas receptor fusion protein was injected subcutaneously 12 hours after CLP to act as a decoy DECOY. A pond used for the breeding and maintenance of water-fowl. 11 Mod. 74, 130; S. C. 3 Salk. 9; Holt, 14 11 East, 571. for FasL binding. Detailed studies have shown that this intervention restores normal immune function, improves cardiac output, and lowers the serum level of the antiinflammatory 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). interleukin-10 (27). Another strategy aims to influence intracellular signaling networks in a direction opposing the initiation of programmed cell death. A recent publication by the Hotckhiss group showed that this could be achieved by exploiting the normal CD40 regulatory pathway through which lymphocytes are stimulated in an antiapoptotic direction to produce clonal expansion and functional maturation (30). Mice treated with a monoclonal antibody that binds to and stimulates the CD40 receptor showed up-regulation of the antiapoptotic protein Bcl-[x.sub.L], an absence of apoptosis of B cells, a decrease in loss of T cells, and a resistance to CLP (29). Efforts have also been made to alter intracellular signaling by introducing active portions of Bcl-[x.sub.L] fused to carrier peptides to facilitate its transport into cells. In a murine CLP model, treatment resulted in a decrease in lymphocyte apoptosis, but the effect was less marked than that observed in transgenic animals constitutively expressing the same protein (30). Another approach has used the licensed HIV HIV (Human Immunodeficiency Virus), either of two closely related retroviruses that invade T-helper lymphocytes and are responsible for AIDS. There are two types of HIV: HIV-1 and HIV-2. HIV-1 is responsible for the vast majority of AIDS in the United States. protease inhibitors nelfinavir nelfinavir /nel·fin·a·vir/ (nel-fin´ah-vir) an HIV protease inhibitor that causes formation of immature, noninfectious viral particles; used as the mesylate salt in the treatment of HIV infection. and ritonavir ritonavir /ri·to·na·vir/ (ri-to´nah-vir) an HIV protease inhibitor used in treatment of HIV infection and AIDS. ri·ton·a·vir n. , which in addition to blocking the cleavage of HIV propeptides have direct antiapoptotic effects (31). The latter were initially assumed to result from caspase inhibition, but further studies showed that these drugs prevent initiation of the intrinsic apoptotic pathway by stabilizing the mitochondrial membrane potential. Oral administration of nelfinavir and ritonavir to mice, beginning either before or 4 hours after CLP, resulted in decreased lymphocyte apoptosis and improved survival (31). Because both drugs are licensed for use in humans, this approach could potentially be evaluated in sepsis patients. Efforts to prevent completion of the programmed cell death process by blocking executioner caspases have also been reported. Studies with the broad-spectrum caspase inhibitor zVAD showed decreased apoptosis and improved survival in a mouse CLP model (32). Similarly, a selective caspase-3 inhibitor decreased blood bacterial counts and improved survival in mice with sepsis (33). Treatment of septic Rag 1-/- mice with caspase inhibitors failed to improve survival, which suggests that the beneficial effect required the presence of lymphocytes. Potential Limitations of Antiapoptotic Therapy Although the proof-of-concept studies described above have shown promising results, deliberate inhibition of apoptosis during severe infections might have unexpected and undesired consequences. One potential adverse effect of antiapoptotic therapy involves its effects on pathogen replication. Some intracellular agents, such as poxviruses, actively inhibit apoptosis of their host cells so as to permit their own continued replication. Theoretically, pharmacologic inhibition of apoptosis in those situations could actually worsen the clinical outcome by providing an advantage to the pathogen. It may therefore be essential to identify the causative agent of infection before initiating antiapoptotic therapy. An alternative approach that may offer several advantages is targeted delivery of antiapoptotic molecules. Similar to current immune-based therapies, apoptosis inhibitors could be directed to specific classes of immune cells, for example by conjugating them to antibodies to CD4 or CD20, thus avoiding adverse consequences (35). Other potential limitations of antiapoptotic therapy relate to possible undesired effects of the use of caspase inhibitors. First, because only a small amount of activated caspase-3 is sufficient to initiate genomic DNA breakdown and lead to apoptotic cell death, a high degree of inhibition would be needed to achieve therapeutic effectiveness (36). This requirement presents a therapeutic challenge because of the need for persistent and nearly complete caspase blockade. In addition, there is increasing recognition that caspases have numerous functions in addition to their roles as mediators of programmed cell death. One subset of caspases is critical for regulation of inflammation by processing proinflammatory cytokines Cytokines Chemicals made by the cells that act on other cells to stimulate or inhibit their function. Cytokines that stimulate growth are called "growth factors. such as interleukin-1[beta]; others are essential for lymphocyte activation, proliferation, and protective immunity (37,38). Patients with defects in caspase-8, for example, are immunodeficient and have recurring infections (39). Blocking caspases might therefore have some beneficial effects in decreasing lymphocyte apoptosis in sepsis, but these could be counterbalanced by adverse effects on the ability of the patient to mount an effective immune response. Finally, that inhibition of caspases might induce hyperacute TNF-induced shock in certain situations has been recently reported (40). In view of the possible deleterious effects of using caspase inhibitors to treat sepsis, therapy directed at a temporary inhibition of specific caspases, such as caspase-3 or caspase-12, timed to either the hyperinflammatory phase or the hypoinflammatory phase of sepsis, might be the most effective approach. Conclusions A massive loss of lymphocytes and other cells through apoptosis is a proven component of the physiologic changes that occur over the course of septic shock. This process appears also to occur in a variety of other severe infections, including anthrax, plague, and Ebola hemorrhagic fever, which are of major concern for biodefense. A variety of proof-of-concept studies with murine sepsis models have demonstrated that extensive apoptosis worsens disease outcome because its prevention through genetic modification or pharmacologic intervention improves survival. Research is needed to assess the possible contribution of lymphocyte apoptosis to immune impairment in other disease processes, including a variety of newly emerging infections. By helping to bolster immune function, the development of antiapoptotic therapies could mitigate the consequences of infection by a wide variety of pathogenic agents. References (1.) Hotchkiss RS, Tinsley KW, Swanson PE, Schmieg RE Jr, Hui JJ, Chang KC, et al. Sepsis-induced apoptosis causes progressive profound depletion of B and CD4+ T lymphocytes in humans. J Immunol. 2001;166:6952-63. (2.) Hotchkiss RS, Karl IE. The pathophysiology pathophysiology /patho·phys·i·ol·o·gy/ (-fiz?e-ol´ah-je) the physiology of disordered function. path·o·phys·i·ol·o·gy n. 1. and treatment of sepsis. N Engl J Med. 2003;348:138-50. (3.) Wesche DE, Lomas-Neira JL, Perl M, Chung CS, Ayala A. Leukocyte leukocyte (l `kəsīt'): see blood. leukocyte or white blood cell or white corpuscle apoptosis and its significance in sepsis and shock. J Leukoc Biol. 2005;78:325-37. (4.) Hotchkiss RS, Osmon SB, Chang KC, Wagner TH, Coopersmith CM, Karl IE. Accelerated lymphocyte death in sepsis occurs by both the death receptor and mitochondrial pathways. J Immunol. 2005;174:5110-8. (5.) Felmet KA, Hall MW, Clark RS, Jaffe R, Carcillo JA. Prolonged lymphopenia, lymphoid depletion, and hypoprolactinemia in children with nosocomial nosocomial /noso·co·mi·al/ (nos?o-ko´me-il) pertaining to or originating in a hospital. nos·o·co·mi·al adj. 1. Of or relating to a hospital. 2. sepsis and multiple organ failure. J Immunol. 2005;174:3765-72. (6.) Toti P, de Felice C, Occhini R, Schuerfeld K, Stumpo M, Epistolato MC, et al. Spleen depletion in neonatal sepsis and chorioamnionitis. Am J Clin Pathol. 2004;122:765-71. (7.) Le Tulzo Y, Pangault C, Gacouin A, Guilloux V, Tribut O, Amiot L, et al. Early circulating lymphocyte apoptosis in human septic shock is associated with poor outcome. Shock. 2002; 18:487-94. (8.) Hotchkiss RS, Swanson PE, Cobb JP, Jacobson A, Buchman TG, Karl IE. Apoptosis in lymphoid and parenchymal pa·ren·chy·ma n. 1. Anatomy The tissue characteristic of an organ, as distinguished from associated connective or supporting tissues. 2. cells during sepsis: findings in normal and T- and B-cell-deficient mice. Crit Care Med. 1997;25:1298-307. (9.) Efron PA, Tinsley K, Minnich D J, Monterroso V, Wagner J, Lainee P, et al. Increased lymphoid tissue apoptosis in baboons with bacteremic shock. Shock. 2004;21:566-71. (10.) Mahanty S, Bray M. Pathogenesis of filoviral haemorrhagic fevers. Lancet Infect Dis. 2004;4:487-98. (11.) Baize baize n. An often bright-green cotton or woolen material napped to imitate felt and used chiefly as a cover for gaming tables. [French baies, from pl. S, Leroy EM, Georges-Courbot MC, Capron M, Lansoud-Soukate J, Debre P, et al. Defective humoral hu·mor·al adj. 1. Relating to body fluids, especially serum. 2. Relating to or arising from any of the bodily humors. Humoral Pertaining to or derived from a body fluid. responses and extensive intravascular apoptosis are associated with fatal outcome in Ebola virus-infected patients. Nat Meal. 1999;5:423-6. (12.) Sanchez A, Lukwiya M, Bausch D, Mahanty S, Sanchez AJ, Wagoner KD, et al. Analysis of human peripheral blood samples from fatal and nonfatal cases of Ebola (Sudan) hemorrhagic fever: cellular responses, virus load, and nitric oxide levels. J Virol. 2004;78:10370-7. (13.) Reed DS, Hensley LE, Geisbert JB, Jahrling PB, Geisbert TW. Depletion of peripheral blood T lymphocytes and NK cells during the course of Ebola hemorrhagic fever in cynomolgus macaques. Viral Immunol. 2004;17:390-400. (14.) Gibb TR, Bray M, Geisbert TW, Steele KE, Kell WM, Davis KJ, et al. Pathogenesis of experimental Ebola Zaire virus infection in BALB/c mice. J Comp Pathol. 2001;125:233-42. (15.) Geisbert TW, Hensley LE, Gibb TR, Steele KE, Jaax NK, Jahrling PB. Apoptosis induced in vitro and in vivo during infection by Ebola and Marburg viruses. Lab Invest. 2000;80:171-86. (16.) Inglesby TV, O'Toole T, Henderson DA, Bartlett JG, Aseher MS, Eitzen E, et al. Anthrax as a biological weapon, 2002: updated recommendations for management. JAMA JAMA abbr. Journal of the American Medical Association . 2002;287:2236-52. (17.) Grinberg LM, Abramova FA, Yampolskaya OV, Walker DH, Smith JH. Quantitative pathology of inhalational anthrax I: quantitative microscopic findings. Mod Pathol. 2001;14:482-95. (18.) Alileche A, Serfass ER, Muehlbauer SM, Poreelli SA, Brojatsch J. Anthrax lethal toxin-mediated killing of human and murine dendritic cells impairs the adaptive immune response. PLoS Pathog. 2005;1:e19. (19.) Inglesby TV, Dennis DT, Henderson DA, Bartlett JG, Ascher MS, Eitzen E, et al. Plague as a biological weapon: medical and public health management. Working Group on Civilian Biodefense. JAMA. 2000;283:2281-90. (20.) Viboud GI, Bliska JB. Yersinia Yersinia A genus of bacteria in the Enterobacteriaceae family. The bacteria appear as gram-negative rods and share many physiological properties with related Escherichia coli. Of the 11 species of Yersinia, Y. pestis, Y. enterocolitica, and Y. outer proteins: role in modulation of host cell signaling responses and pathogenesis. Annu Rev Microbiol. 2005;59:69-89. (21.) Lathem WW, Crosby SD, Miller VL, Goldman WE. Progression of primary pneumonic plague: a mouse model of infection, pathology, and bacterial transcriptional activity. Proc Natl Acad Sci U S A. 2005;102:17786-91. (22.) Alonso A, Bottini N, Bruckner S, Rahmouni S, Williams S, Schoenberger SP, et al. Lek Lek (lĕk), northern arm of the Rhine River, 40 mi (64 km) long, branching from the Neder Rijn (Lower Rhine), central Netherlands, and flowing W into the Nieuwe Maas (New Meuse) River. It is navigable for its entire length. dephosphorylation at Tyr-394 and inhibition of T cell antigen receptor signaling by Yersinia phosphatase phosphatase /phos·pha·tase/ (-tas) any of a group of enzymes that catalyze the hydrolytic cleavage of inorganic phosphate from esters. phos·pha·tase n. YopH. J Biol Chem. 2004;279:4922-8. (23.) Sebbane F, Gardner D, Long D, Gowen BB, Hinnebusch BJ. Kinetics of disease progression and host response in a rat model of bubonic plague. Am J Pathol. 2005;166:1427-39. (24.) Hotchkiss RS, Swanson PE, Knudson CM, Chang KC, Cobb JP, Osborne DF, et al. Overexpression of Bcl-2 in transgenic mice decreases apoptosis and improves survival in sepsis. J Immunol. 1999;162:4148-56. (25.) Iwata A, Stevenson VM, Minard A, Tasch M, Tupper J, Lagasse E, et al. Over-expression of Bcl-2 provides protection in septic mice by a trans effect. J Immunol. 2003;171:3136-41. (26.) Bommhardt U, Chang KC, Swanson PE, Wagner TH, Tinsley KW, Karl IE, et al. Akt decreases lymphocyte apoptosis and improves survival in sepsis. J Immunol. 2004;172:7583-91. (27.) Chung CS, Yang S, Song GY, Lomas J, Wang P, Simms HH, et al. Inhibition of Fas signaling prevents hepatic injury and improves organ blood flow during sepsis. Surgery. 2001; 130:339-45. (28.) Wesche-Soldato DE, Chung CS, Lomas-Neira J, Doughty dough·ty adj. dough·ti·er, dough·ti·est Marked by stouthearted courage; brave. [Middle English, from Old English dohtig; see dheugh- in Indo-European roots. LA, Gregory SH, Ayala A. In vivo delivery of caspase-8 or Fas siRNA improves the survival of septic mice. Blood. 2005;106:2295-301. (29.) Schwulst SJ, Grayson MH, Dipasco PJ, Davis CG, Brahmbhatt TS, Ferguson TA, et al. Agonistic agonistic /ag·o·nis·tic/ (ag?o-nis´tik) pertaining to a struggle or competition; as an agonistic muscle, counteracted by an antagonistic muscle. monoclonal antibody against CD40 receptor decreases lymphocyte apoptosis and improves survival in sepsis. J Immunol. 2006;177:557-65. (30.) Hotchkiss RS, McConnell KW, Bullok K, Davis CC4 Chang KC, Schwulst SJ, et al. TAT-BH4 and TAT-Bcl-xL peptides protect against sepsis-induced lymphocyte apoptosis in vivo. J Immunol. 2006; 176:5471-7. (31.) Weaver JG, Tarze A, Moffat TC, Lebras M, Deniaud A, Brenner C, et al. Inhibition of adenine nucleotide translocator Adenine nucleotide translocator is a mitochondrial protein. See also
(32.) Hotchkiss RS, Tinsley KW, Swanson PE, Chang KC, Cobb JP, Buchman TG, et al. Prevention of lymphocyte cell death in sepsis improves survival in mice. Proc Natl Acad Sci U S A. 1999;96:14541-6. (33.) Hotchkiss RS, Chang KC, Swanson PE, Tinsley KW, Hut JJ, Klender P, et al. Caspase inhibitors improve survival in sepsis: a critical role of the lymphocyte. Nat Immunol. 2000; 1:496-501. (34.) Chung CS, Xu YX, Wang W, Chaudry IH, Ayala A. Is Fas ligand or endotoxin Endotoxin A biologically active substance produced by bacteria and consisting of lipopolysaccharide, a complex macromolecule containing a polysaccharide covalently linked to a unique lipid structure, termed lipid A. responsible for mucosal lymphocyte apoptosis in sepsis? Arch Surg. 1998;133:1213-20. (35.) Hoogenboom HR. Selecting and screening recombinant antibody libraries. Nat Biotechnol. 2005;23:1105-16. (36.) Methot N, Huang J, Coulombe N, Vaillancourt JP, Rasper rasp v. rasped, rasp·ing, rasps v.tr. 1. To file or scrape with a coarse file having sharp projections. 2. To utter in a grating voice. 3. D, Tam J, et al. Differential efficacy of caspase inhibitors on apoptosis markers during sepsis in rats and implication for fractional inhibition requirements for therapeutics. J Exp Med. 2004; 199:199-207. (37.) Martinon F, Tschopp J. inflammatory caspases: linking an intracellular innate immune system
(38.) Perfettini JL, Kroemer G. Caspase activation is not death. Nat Immunol. 2003;4:308-10. (39.) Chun HJ, Zheng L, Ahmad M, Wang J, Speirs CK, Siegel RM, et al. Pleiotropic defects in lymphocyte activation caused by caspase-8 mutations lead to human immunodeficiency. Nature. 2002;419:395-9. (40.) Cauwels A, Janssen B, Waeytens A, Cuvelier C, Brouckaert P. Caspase inhibition causes hyperacute tumor necrosis factor-induced shock via oxidative stress and phospholipase A2. Nat Immunol. 2003;4:387-93. Janie Parrino, * Richard S. Hotchkiss, ([dagger]) and Mike Bray * * National Institutes of Health, Bethesda, Maryland, USA; and ([dagger]) Washington University School of Medicine Washington University School of Medicine, located in St. Louis, Missouri, is one of the most competitive and highly regarded medical schools and biomedical research institutes in the United States. , Saint Louis, Missouri, USA Dr Parrino is a clinical fellow in allergy and immunology at the National Institute of Allergy and Infectious Diseases. Her research interests include protocols focusing on new vaccines, emerging infectious diseases, and biodefense. Address for correspondence: Mike Bray, Biodefense Clinical Research Branch, National Institute of Allergy and Infectious Diseases, National Institutes of Health, 6700A Rockledge Dr, Rm 5128, Bethesda, MD 20892, USA; email: mbray@niaid.nih.gov
Table 1. Distinguishing features of apoptosis and necrosis
Feature Apoptosis Necrosis
General Genetically programmed, Accidental cell death
description orderly process of cell caused by acute injury or
death other exogenous effect
Membrane Preserved until late in Early loss results in cell
integrity cell breakdown process and organelle swelling and
rupture
Chromosomal Cleavage at nucleosomes Random fragmentation
DNA produces ladder pattern on produces smear pattern
an agarose gel
Inflammatory None; products have Release of intracellular
response antiinflammatory effect contents causes acute
inflammatory response
Table 2. Therapeutic approaches for prevention of lymphocyte apoptosis
in murine models of sepsis
Strategy Intervention Reference
Prevent triggering of Blockade of Fas ligand by using (27)
extrinsic pathway Fas fusion protein
Prevent triggering of Prevent Fas expression by using (28)
extrinsic pathway siRNA
Prevent initiation Anti-CD40 agonist antibodies (29)
Prevent initiation Treatment with Bcl-2 agonist (30)
peptides
Prevent triggering of Antiretroviral protease (31)
intrinsic pathway inhibitors
Prevent execution phase Anticaspase-8 siRNA (28)
Prevent execution phase Treatment with caspase (32, 33)
inhibitors
|
|
||||||||||||||||
Printer friendly
Cite/link
Email
Feedback
Reader Opinion