Your search keyword '"Hawkins, Christine J."' showing total 9 results

1. Caspase-2 is resistant to inhibition by inhibitor of apoptosis proteins (IAPs) and can activate caspase-7.

Author

Ho PK, Jabbour AM, Ekert PG, and Hawkins CJ

Subjects

Animals, Caspase 2, Caspase 7, Caspase Inhibitors, Enzyme Activation, Inhibitor of Apoptosis Proteins, Mammals, Recombinant Proteins metabolism, Saccharomyces cerevisiae genetics, Saccharomyces cerevisiae metabolism, Signal Transduction, Apoptosis physiology, Caspases metabolism, Proteins metabolism

Abstract

Caspases are a family of cysteine proteases with roles in cytokine maturation or apoptosis. Caspase-2 was the first pro-apoptotic caspase identified, but its functions in apoptotic signal transduction are still being elucidated. This study examined the regulation of the activity of caspase-2 using recombinant proteins and a yeast-based system. Our data suggest that for human caspase-2 to be active its large and small subunits must be separated. For maximal activity its prodomain must also be removed. Consistent with its proposed identity as an upstream caspase, caspase-2 could provoke the activation of caspase-7. Caspase-2 was not subject to inhibition by members of the IAP family of apoptosis inhibitors.

Published

2005

2. Hsp72 inhibits apoptosis upstream of the mitochondria and not through interactions with Apaf-1.

Author

Steel R, Doherty JP, Buzzard K, Clemons N, Hawkins CJ, and Anderson RL

Subjects

Animals, Apoptotic Protease-Activating Factor 1, Blotting, Western, Caspase 3, Caspases metabolism, Cell Nucleus metabolism, Cell Proliferation, Cells, Cultured, Cytochromes c metabolism, Cytosol metabolism, Dose-Response Relationship, Drug, Electrophoresis, Polyacrylamide Gel, Enzyme Activation, Etoposide pharmacology, Fibroblasts metabolism, Fluorescent Dyes pharmacology, HSP72 Heat-Shock Proteins, Intracellular Membranes metabolism, Mice, Mice, Inbred BALB C, Microscopy, Fluorescence, Recombinant Proteins chemistry, Rhodamines pharmacology, Salts pharmacology, Temperature, Time Factors, Tumor Necrosis Factor-alpha metabolism, Ultraviolet Rays, Apoptosis, Heat-Shock Proteins physiology, Mitochondria metabolism, Proteins metabolism

Abstract

Hsp72 protects cells against apoptosis in response to various stresses. By simultaneously measuring cytochrome c localization and nuclear morphology in mouse embryo fibroblasts, we have shown that Hsp72 blocks cytochrome c release from mitochondria in response to cytotoxic stress and that permeabilization of the outer mitochondrial membrane is the critical point in deciding the fate of the cell. Hsp72 did not inhibit apoptosis in mouse embryo fibroblasts once cytochrome c had been released from the mitochondria. Recent reports have claimed that Hsp72 can prevent caspase activation by inhibiting the oligomerization of Apaf-1 in the presence of cytochrome c and dATP. We now show that this apparent function of recombinant Hsp72 is due to the presence of salt in the Hsp72 preparation and that the same response can be achieved by the addition of heat-denatured Hsp72 in the same high salt buffer or by the high salt buffer alone. Hsp72 expressed in a range of different cell lines had no inhibitory effect on cytochrome c-stimulated caspase activity of cytosolic extracts. We conclude that the protective effect of Hsp72 occurs upstream of the mitochondria and not through the inhibition of the apoptosome.

Published

2004

3. Apaf-1 and caspase-9 accelerate apoptosis, but do not determine whether factor-deprived or drug-treated cells die.

Author

Ekert PG, Read SH, Silke J, Marsden VS, Kaufmann H, Hawkins CJ, Gerl R, Kumar S, and Vaux DL

Subjects

Animals, Apoptotic Protease-Activating Factor 1, Caspase 9, Caspases deficiency, Caspases genetics, Cell Line, Cell Survival drug effects, Cytochromes c analysis, Flow Cytometry, Gene Deletion, Interleukin-3 pharmacology, Mice, Mice, Knockout, Proteins genetics, Tumor Cells, Cultured, Apoptosis physiology, Caspases physiology, Cell Survival physiology, Proteins physiology

Abstract

Apoptosis after growth factor withdrawal or drug treatment is associated with mitochondrial cytochrome c release and activation of Apaf-1 and caspase-9. To determine whether loss of Apaf-1, caspase-2, and caspase-9 prevented death of factor-starved cells, allowing them to proliferate when growth factor was returned, we generated IL-3-dependent myeloid lines from gene-deleted mice. Long after growth factor removal, cells lacking Apaf-1, caspase-9 or both caspase-9 and caspase-2 appeared healthy, retained intact plasma membranes, and did not expose phosphatidylserine. However, release of cytochrome c still occurred, and they failed to form clones when IL-3 was restored. Cells lacking caspase-2 alone had no survival advantage. Therefore, Apaf-1, caspase-2, and caspase-9 are not required for programmed cell death of factor-dependent cells, but merely affect its rate. In contrast, transfection with Bcl-2 provided long-term, clonogenic protection, and could act independently of the apoptosome. Unlike expression of Bcl-2, loss of Apaf-1, caspase-2, or caspase-9 would therefore be unlikely to enhance the survival of cancer cells.

Published

2004

4. The anti-apoptotic activity of XIAP is retained upon mutation of both the caspase 3- and caspase 9-interacting sites.

Author

Silke J, Hawkins CJ, Ekert PG, Chew J, Day CL, Pakusch M, Verhagen AM, and Vaux DL

Subjects

Apoptosis Regulatory Proteins, Binding Sites genetics, Carrier Proteins metabolism, Caspase 3, Caspase 9, Cells, Cultured, Humans, Intracellular Signaling Peptides and Proteins, Mitochondrial Proteins metabolism, Mutagenesis physiology, Point Mutation, X-Linked Inhibitor of Apoptosis Protein, Zinc Fingers genetics, Apoptosis physiology, Caspases metabolism, Proteins genetics, Proteins metabolism

Abstract

The X-linked mammalian inhibitor of apoptosis protein (XIAP) has been shown to bind several partners. These partners include caspase 3, caspase 9, DIABLO/Smac, HtrA2/Omi, TAB1, the bone morphogenetic protein receptor, and a presumptive E2 ubiquitin-conjugating enzyme. In addition, we show here that XIAP can bind to itself. To determine which of these interactions are required for it to inhibit apoptosis, we generated point mutant XIAP proteins and correlated their ability to bind other proteins with their ability to inhibit apoptosis. partial differential RING point mutants of XIAP were as competent as their full-length counterparts in inhibiting apoptosis, although impaired in their ability to oligomerize with full-length XIAP. Triple point mutants, unable to bind caspase 9, caspase 3, and DIABLO/HtrA2/Omi, were completely ineffectual in inhibiting apoptosis. However, point mutants that had lost the ability to inhibit caspase 9 and caspase 3 but retained the ability to inhibit DIABLO were still able to inhibit apoptosis, demonstrating that IAP antagonism is required for apoptosis to proceed following UV irradiation.

Published

2002

5. A Cloning Method to Identify Caspases and Their Regulators in Yeast: Identification of Drosophila IAP1 as an Inhibitor of the Drosophila Caspase DCP-1

Author

Hawkins, Christine J., Wang, Susan L., and Hay, Bruce A.

Published

1999

6. Cloning and Expression of Apoptosis Inhibitory Protein Homologs that Function to Inhibit Apoptosis and/or Bind Tumor Necrosis Factor Receptor-Associated Factors

Author

Uren, Anthony G., Pakusch, Miha, Hawkins, Christine J., Puls, Kirsten L., and Vaux, David L.

Published

1996

7. Apoptosis Is Triggered When Prosurvival Bcl-2 Proteins Cannot Restrain Bax

Author

Fletcher, Jamie I., Meusburger, Sarina, Hawkins, Christine J., Riglar, David T., Lee, Erinna F., Fairlie, W. Douglas, Huang, David C. S., and Adams, Jerry M.

Published

2008

8. DIABLO Promotes Apoptosis by Removing MIHA/XIAP from Processed Caspase 9.

Author

Ekert, Paul G., Silke, John, Hawkins, Christine J., Verhagen, Anne M., and Vaux, David L.

Subjects

*PROTEINS, *PHYSIOLOGICAL effects of ultraviolet radiation, *CHEMICAL inhibitors, APOPTOSIS prevention

Abstract

Shows that after ultraviolet radiation, MIHA, an inhibitor of apoptosis protein (IAP), prevented apoptosis by inhibiting caspase 9 and caspase 3 activation. Effect of MIHA on serum withdrawal-induced apoptosis; MIHA binding to endogenous, processed caspase 3; MIHA function downstream of mitochondrial cytochrome c and release of the mammalian protein, DIABLO.

Published

2001

9. TWEAK-FN 14 signaling induces lysosomal degradation of a clAP1-TRAF2 complex to sensitize tumor cells to TNFα.

Author

Vince, James E., Chau, Diep, Callus, Bernard, Wong, W. Wei-Lynn, Hawkins, Christine J., Schneider, Pascal, McKinlay, Mark, Benetatos, Christopher A., Condon, Stephen M., Chunduru, Srinivas K., Yeoh, George, Brink, Robert, Vaux, David L., and Silke, John

Subjects

*APOPTOSIS, *CELL death, *CANCER cells, *TUMOR necrosis factors, *PROTEINS

Abstract

Synthetic inhibitor of apoptosis (IAP) antagonists induce degradation of IAP proteins such as cellular IAP1 (cIAP1), activate nuclear factor κB (NF-κB) signaling, and sensitize cells to tumor necrosis factor α (TNFα). The physiological relevance of these discoveries to cIAP1 function remains undetermined. We show that upon ligand binding, the TNF superfamily receptor FN14 recruits a cIAP1-Tnf receptor-associated factor 2 (TRAF2) complex. Unlike IAP antagonists that cause rapid proteasomal degradation of cIAP1, signaling by FN14 promotes the lysosomal degradation of cIAP1-TRAF2 in a cIAP1-dependent manner. TNF-like weak inducer of apoptosis (TWEAK)/FN14 signaling nevertheless promotes the same noncanonical NF-κB signaling elicited by IAP antagonists and, in sensitive cells, the same autocrine TNFα-induced death occurs. TWEAK-induced loss of the cIAP1-TRAF2 complex sensitizes immortalized and minimally passaged tumor cells to TNFα-induced death, whereas primary cells remain resistant. Conversely, cIAP1-TRAF2 complex over-expression limits FN14 signaling and protects tumor cells from TWEAK-induced TNFα sensitization. Lysosomal degradation of cIAP1-TRAF2 by TWEAK/FN14 therefore critically alters the balance of life/death signals emanating from TNF-R1 in immortalized cells. [ABSTRACT FROM AUTHOR]

Published

2008