Caspase inhibitors improve survival in sepsis: a critical role of the lymphocyte

Hotchkiss, Richard S.; Chang, Kathy; Swanson, Paul E.; Tinsley, Kevin W.; Hui, Jia; Klender, Paula M.; Xanthoudakis, Steven; Roy, Sophie; Black, Cheryl; Grimm, Erich L.; Aspiotis, Renée; Han, Yongxin; Nicholson, Donald W.; Karl, Irene E.

doi:10.1038/82741

Cited by 494 publications

(494 citation statements)

References 29 publications

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“…In this respect Hotchkiss et al [52] observed early on that when administered one hour after experimental sepsis, the pan-caspase inhibitor N-benzyloxycarbonyl-Val-Ala-Asp(O-methyl) fluoromethyl ketone (z-VAD) significantly reduced apoptosis in the thymus and spleen, and z-VAD administration (6mg/kg) immediately following and 24 hours after sepsis resulted in 100% survival as compared to 40% observed in controls. Inhibition of caspase-3 by injection of M-791 also markedly improved survival in septic mice, reducing thymocyte and splenocyte apoptosis [53] while the adoptive transfer of apoptosis-resistant T cells also markedly enhanced the survival rate of the septic animals [53]. Studies with C3H/HeJ (endotoxin-tolerant) and C3H/HeJ-FasL gld (endotoxin-tolerant/FasL-deficient) mice showed that the Fas/FasL pathway was a mediator of apoptosis in B220 + B cells of the Peyer's patches as well as CD4 + and CD8 + T cells of the intestinal intraepithelial lymphocyte (IEL) population or splenic CD4 + T cells during sepsis [19][20][21].…”

Section: Inhibiting Apoptosis Improves Septic Survival -Therapeutic Omentioning

confidence: 90%

Role of programmed cell death in the immunopathogenesis of sepsis

Perl

Chung

Swan

et al. 2007

Drug Discovery Today: Disease Mechanisms

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Apoptosis is an important mechanism during the immunopathogenesis of sepsis. Early programmed cell death of lymphocytes substantially impairs innate and adaptive immunity reducing the capacity to ward off the invading pathogen. Apoptosis of parenchymal cells (e.g. in the lung, liver and gut) may also promote organ failure and death. Several experimental therapeutic strategies have now been developed to beneficially influence these mechanisms; however, their potential clinical benefit is yet to be evaluated.

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Section: Inhibiting Apoptosis Improves Septic Survival -Therapeutic Omentioning

confidence: 90%

Role of programmed cell death in the immunopathogenesis of sepsis

Perl

Chung

Swan

et al. 2007

Drug Discovery Today: Disease Mechanisms

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“…58 In heart failure, cardiomyocytes show autophagic rather than apoptotic cell death. 59 One of the few diseases in which caspase inhibitors may yield convincing preclinical effects is septic shock, 60 which involves the contribution of caspases, not only as cellular demolition enzymes but also for the biosynthesis of proinflammatory cytokines. Thus, although caspase inhibition can successfully prevent the phenotypic manifestation of apoptosis, it often does not prevent cell death, which is likely to be executed through different mechanisms (including apoptosis-like cell death, autophagy and necrosis) 5,23,24,34,61 and perhaps through phagocytic recognition and destruction.…”

Section: Comments and Examplesmentioning

confidence: 99%

Redundant cell death mechanisms as relics and backups

Golstein

Kroemer

2005

Cell Death Differ

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Here we review recent observations indicating the existence of redundant cell death mechanisms. We speculate that this redundancy reflects a particular evolutionary history for cellular demise. Autophagic or apoptotic elements might have been added to a primordial death mechanism, initially improving cell dismantling and later acquiring the ability to act themselves as death effectors. The resulting redundancy of cell death mechanisms has pathophysiological implications.

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“…Caspase inhibitors have also shown some benefit in murine models of sepsis (Ref. 150). However, the targeted blockade of apoptosis to lymphocytes, and not to cell populations that harbour EBOV, is a formidable hurdle that must be overcome before this therapeutic strategy can be fully realised.…”

Section: Inhibition Of Apoptosis Of Bystander Lymphocytesmentioning

confidence: 99%

Ebola virus: new insights into disease aetiopathology and possible therapeutic interventions

Geisbert

Hensley

2004

Expert Rev. Mol. Med.

110

105

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Ebola virus (EBOV) gained public notoriety in the last decade largely as a consequence of the highly publicised isolation of a new EBOV species in a suburb of Washington, DC, in 1989, together with the dramatic clinical presentation of EBOV infection and high case-fatality rate in Africa (near 90% in some outbreaks), and the unusual and striking morphology of the virus. Furthermore, there are no vaccines or effective therapies currently available. Progress in understanding the origins of the pathophysiological changes that make EBOV infections of humans so devastating has been slow, primarily because these viruses require special containment for safe research. However, an increasing understanding of the mechanisms of EBOV pathogenesis, facilitated by the development of new tools to elucidate critical regulatory elements in the viral life cycle, is providing new targets that can be exploited for therapeutic interventions. Notably, identifying factors triggering the haemorrhagic complications that characterise EBOV infections led to the development of a strategy to modulate coagulopathy; this therapeutic modality successfully mitigated the effects of EBOV haemorrhagic fever in nonhuman primates. This review summarises our current understanding of EBOV pathogenesis and discusses various approaches to therapeutic intervention based on our current understanding of how EBOV produces a lethal infection.

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Caspase inhibitors improve survival in sepsis: a critical role of the lymphocyte

Cited by 494 publications

References 29 publications

Role of programmed cell death in the immunopathogenesis of sepsis

Role of programmed cell death in the immunopathogenesis of sepsis

Redundant cell death mechanisms as relics and backups

Ebola virus: new insights into disease aetiopathology and possible therapeutic interventions

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