Abstract

The release of cytochrome c from mitochondria is a critical step in the major pathway of caspase activation and apoptosis affecting mammalian cells. However, mitochondrial outer membrane permeabilization (MOMP) appears to commit cells to die regardless of whether or not caspases are activated downstream of MOMP. Although this caspase-independent death (CICD) was first described almost 10 years ago, and has been well characterized, there is little consensus as to how it occurs. This proposal is based on our studies that identify conditions under which cells can be protected from CICD but not apoptosis. Using an unbiased screen, we identified GAPDH as being capable of rescuing cells subjected to conditions for CICD, and further, found that this protection acts downstream of MOMP. That is, cells release cytochrome c and subsequently """"""""heal"""""""" their mitochondria and sustain clonogenic growth. Additional studies led us to another protein capable of protecting mammalian cells from CICD: the C. elegans Bcl-2 family member CED9, which does not protect mammalian cells from apoptosis, but effectively preserved clonogenic survival in the presence of caspase inhibitors. The protection from CICD afforded by GAPDH or CED9 involves elements of the autophagic survival pathway, as well as aspects of mitochondrial dynamics. The current proposal seeks to dissect how CICD occurs, and how protection from CICD works. Our specific goals are to answer the following questions: 1. How do cells survive the process that normally leads to CICD? Here, we will investigate the cellular changes that occur during CICD, especially those relating to mitochondrial number and function, and how these are affected by GAPDH and CED9 to promote cell survival. Studies in this aim will identify key events in this process and place them into the context of physiologically relevant events in cell death and survival. 2. How does autophagy contribute to protection from CICD? Autophagy plays critical roles in survival of stressed cells. We will explore how GAPDH enhances autophagy to remove damaged mitochondria, and how this contributes to protection from CICD. 3. How do mitochondrial dynamics contribute to protection from CICD? Mitochondrial fusion is an essential cellular function, and is impaired following MOMP. Both GAPDH and CED9 prevent mitochondrial fragmentation following MOMP, and therefore the role of mitochondrial dynamics in restoring a full mitochondrial cohort and protection from CICD will be explored. Overall, we will test the idea that cells can survive MOMP if a) caspases are not activated, b) metabolic energy is sustained, c) damaged mitochondria are removed by autophagy, and d) a """"""""seed"""""""" pool of intact mitochondria that have either not undergone MOMP or have repaired their outer membranes can repopulate the cell via mitochondrial dynamics. Our studies employ a number of novel approaches and concepts, all of which are directed at answering these questions. Successful completion of the proposed work will reveal fundamental new processes in the control of cell life and death.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project (R01)
Project #
5R01AI040646-15
Application #
7989136
Study Section
Cancer Molecular Pathobiology Study Section (CAMP)
Program Officer
Leitner, Wolfgang W
Project Start
1997-05-01
Project End
2012-11-30
Budget Start
2010-12-01
Budget End
2011-11-30
Support Year
15
Fiscal Year
2011
Total Cost
$370,479
Indirect Cost

  Institution

Name
St. Jude Children's Research Hospital
Department
Type
DUNS #
067717892
City
Memphis
State
TN
Country
United States
Zip Code
38105

  Publications

Mitchell, Gabriel; Cheng, Mandy I; Chen, Chen et al. (2018) Listeria monocytogenes triggers noncanonical autophagy upon phagocytosis, but avoids subsequent growth-restricting xenophagy. Proc Natl Acad Sci U S A 115:E210-E217
Cunha, Larissa D; Yang, Mao; Carter, Robert et al. (2018) LC3-Associated Phagocytosis in Myeloid Cells Promotes Tumor Immune Tolerance. Cell 175:429-441.e16
Moretti, Julien; Roy, Soumit; Bozec, Dominique et al. (2017) STING Senses Microbial Viability to Orchestrate Stress-Mediated Autophagy of the Endoplasmic Reticulum. Cell 171:809-823.e13
Heckmann, Bradlee L; Boada-Romero, Emilio; Cunha, Larissa D et al. (2017) LC3-Associated Phagocytosis and Inflammation. J Mol Biol 429:3561-3576
Galluzzi, Lorenzo; Baehrecke, Eric H; Ballabio, Andrea et al. (2017) Molecular definitions of autophagy and related processes. EMBO J 36:1811-1836
Park, Sunmin; Buck, Michael D; Desai, Chandni et al. (2016) Autophagy Genes Enhance Murine Gammaherpesvirus 68 Reactivation from Latency by Preventing Virus-Induced Systemic Inflammation. Cell Host Microbe 19:91-101
Lu, Qun; Yokoyama, Christine C; Williams, Jesse W et al. (2016) Homeostatic Control of Innate Lung Inflammation by Vici Syndrome Gene Epg5 and Additional Autophagy Genes Promotes Influenza Pathogenesis. Cell Host Microbe 19:102-13
Joo, Joung Hyuck; Wang, Bo; Frankel, Elisa et al. (2016) The Noncanonical Role of ULK/ATG1 in ER-to-Golgi Trafficking Is Essential for Cellular Homeostasis. Mol Cell 62:491-506
Goodall, Megan L; Fitzwalter, Brent E; Zahedi, Shadi et al. (2016) The Autophagy Machinery Controls Cell Death Switching between Apoptosis and Necroptosis. Dev Cell 37:337-349
Green, D R; Oguin, T H; Martinez, J (2016) The clearance of dying cells: table for two. Cell Death Differ 23:915-26

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