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During apoptosis mitochondrial outer membrane permeabilization (MOMP) is often a point-of-no-return; death can proceed even if caspase activation is disrupted. cell types regardless of caspase activity. Importantly the presence of intact mitochondria correlated with cellular recovery following MOMP provided that caspase activity was blocked. Such intact mitochondria underwent MOMP in response to treatment of cells with the Bcl-2 antagonist ABT-737 suggesting that the resistance of these mitochondria to MOMP lies at the point of Bax or Bak activation. Thus iMOMP provides a critical source of intact mitochondria that permits cellular survival following MOMP. Introduction In response to most stimuli engagement of apoptosis involves mitochondrial outer membrane permeabilization (MOMP) which in turn leads to widespread activation of executioner caspases. The proteolytic activity of these caspases causes the physiological hallmarks of apoptosis including DNA fragmentation nuclear condensation phosphatidylserine externalization and plasma membrane blebbing (Taylor et al. 2008 While caspase activation is the defining characteristic of apoptosis cells that undergo MOMP but are prevented from activating executioner caspases by chemical Rabbit Polyclonal to SAA4.inhibitors or by genetic ablation of Apaf-1 or caspase-9 will nonetheless die (Amarante-Mendes et al. 1998 Haraguchi et al. 2000 McCarthy et al. 1997 Xiang et al. 1996 MOMP-dependent caspase-independent cell death (CICD) may be due to loss of mitochondrial function caused by MOMP and/or by release of mitochondrial proteins that can NVP-BVU972 kill a cell in a caspase-independent manner (Tait and Green 2008 Examples of the latter include AIF Omi/HtrA2 and Endonuclease G although their roles in mediating CICD remain controversial (Li et al. 2001 Susin et al. 1999 Suzuki et al. 2001 That CICD is dependent on MOMP is evidenced by observations that expression of anti-apoptotic Bcl-2 proteins (Haraguchi et al. 2000 or lack of the NVP-BVU972 pro-apoptotic Bcl-2 effectors Bax and Bak (Lum et al. 2005 prevents cell death. These findings have led to the view that MOMP represents a point-of-no-return for cell death. However this is not always the case. For example post-mitotic sympathetic neurons deprived of neurotrophic factor undergo MOMP but remain viable provided caspase activity is inhibited and growth factor is replenished (Deshmukh et al. 2000 Martinou et al. 1999 Recently we found that proliferating cells can also recover following MOMP. By employing a retroviral based cDNA screen for inhibitors of CICD we identified glyceraldehyde-3-phosphate dehydrogenase (GAPDH) as being able to promote cellular survival following MOMP and allow clonogenic outgrowth (Colell et al. 2007 This protective effect of GAPDH was dependent upon its well-defined glycolytic role and a novel role in stimulating mitophagy in part through up-regulation of Atg12. The ability of cells to recover from MOMP has a variety of clinical implications including implications for oncogenesis. For example tumor cell lines often display reduced caspase activity owing to a lack of Apaf-1 expression apoptosome activity or caspase expression (Devarajan et al. 2002 Ferreira et al. 2001 Soengas et al. 2001 Wolf et al. 2001 Alternatively some tumors over-express inhibitor of apoptosis proteins (IAPs) that can directly inhibit caspase function (Krajewska et al. 2003 Tamm et al. 2000 Moreover expression of a dominant negative form of caspase-9 (which prevents caspase activation following MOMP) has been shown to enhance survival and proliferation of transformed cells (Schmitt et al. 2002 These studies suggest that tumor cells have developed means of inhibiting caspase activity downstream of MOMP. The ability of tumor cells to recover and proliferate NVP-BVU972 after MOMP would facilitate tumor cell survival and chemotherapeutic resistance. How mitochondrial repopulation occurs during cellular recovery from MOMP is unknown. Mitochondrial function is critical for survival following MOMP since only cells that maintain ??m are able to survive (Colell et al. 2007 Deshmukh et al. 2000 however in order to recover from MOMP and proliferate cells must either generate or already possess a source of healthy.

This entry was posted in MET Receptor and tagged NVP-BVU972, Rabbit Polyclonal to SAA4. onFebruary 1, 2017.

http://www.techbizstrategy.com/2017/02/01/during-apoptosis-mitochondrial-outer-membrane-permeabilization-momp-is-often-a-point-of-no-return/