Your search keyword '"Godin, Chantal"' showing total 2 results

1. The Fanconi Anemia Group C Protein Interacts with Uncoordinated 5A and Delays Apoptosis.

Author

Huang, FengFei, Ben Aissa, Manel, Magron, Audrey, Huard, Caroline C., Godin, Chantal, Lévesque, Georges, and Carreau, Madeleine

Subjects

FANCONI'S anemia, PROTEIN-protein interactions, APOPTOSIS, CARRIER proteins, CELL death

Abstract

The Fanconi anemia group C protein (FANCC) is one of the several proteins that comprise the Fanconi anemia (FA) network involved in genomic surveillance. FANCC is mainly cytoplasmic and has many functions, including apoptosis suppression through caspase-mediated proteolytic processing. Here, we examined the role of FANCC proteolytic fragments by identifying their binding partners. We performed a yeast two-hybrid screen with caspase-mediated FANCC cleavage products and identified the dependence receptor uncoordinated-5A (UNC5A) protein. Here, we show that FANCC physically interacts with UNC5A, a pro-apoptotic dependence receptor. FANCC interaction occurs through the UNC5A intracellular domain, specifically via its death domain. FANCC modulates cell sensitivity to UNC5A-mediated apoptosis; we observed reduced UNC5A-mediated apoptosis in the presence of FANCC and increased apoptosis in FANCC-depleted cells. Our results show that FANCC interferes with UNC5A's functions in apoptosis and suggest that FANCC may participate in developmental processes through association with the dependence receptor UNC5A. [ABSTRACT FROM AUTHOR]

Published

2014

2. Regulation of the Fanconi Anemia Group C Protein through Proteolytic Modification.

Author

Brodeur, Isabelle, Goulet, Isabelle, Tremblay, Cédric S., Charbonneau, Chantal, Delisle, Marie-Chantal, Godin, Chantal, Huard, Caroline, Khandjian, Edward W., Buchwald, Manuel, Lévesque, Georges, and Carreau, Madeleine

Subjects

*FANCONI'S anemia, *PROTEIN C, *PROTEOLYTIC enzymes, *BIOCHEMISTRY, *BIOLOGY, *CHEMISTRY

Abstract

The function of the Fanconi anemia group C protein (FANCC) is still unknown, though many studies point to a role in damage response signaling. Unlike other known FA proteins, FANCC is mainly localized to the cytoplasm and is thought to act as a messenger of cellular damage rather than an effector of repair. FANCC has been shown to interact with several cytoplasmic and nuclear proteins and to delay the onset of apoptosis through redox regulation of GSTP1. We investigated the fate and function of FANCC during apoptosis. Here we show that FANCC undergoes proteolytic modification by a caspase into a predominant 47-kDa ubiquitinated protein fragment. Lack of proteolytic modification at the putative cleavage site delays apoptosis but does not affect MMC complementation. These results suggest that FANCC function is regulated through proteolytic processing. [ABSTRACT FROM AUTHOR]

Published

2004