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Calpain-dependent cleavage of cain/cabin1 activates calcineurin to mediate calcium-triggered cell death

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Abstract
Cain/cabin1 is an endogenous inhibitor of calcineurin (Cn), a calcium-dependent serine/threonine phosphatase involved in various cellular functions including apoptosis. We show here that during apoptosis cain/cabin1 is cleaved by calpain at the carboxyl terminus to generate a cleavage product with a molecular mass of 32 kDa as a necessary step leading to Cn-mediated cell death. Mouse cain/cabin1 was identified from a thymus cDNA library by an in vitro substrate-screening assay with calpain. Exposure of Jurkat cells to the calcium ionophore, A23187, induced cain/cabin1 cleavage and cell death, accompanied by activation of calpain and Cn. The calpain inhibitors, calpeptin and zLLY, suppressed both A23187-induced cain/cabin1 cleavage and Cn activation, indicating that Cn activation and cain/cabin1 cleavage are calpain-dependent. Expression of cain/cabin1 or a catalytically inactive Cn mutant [CnAbeta(2)(1-401/H160N)] and treatment with FK506 reduced A23187-induced cell death. In vitro calpain cleavage and immunoprecipitation assays with deletion mutants of cain/cabin1 showed that cleavage occurred in the Cn-binding domain of cain/cabin1, indicating that the cleavage at its C terminus by calpain prevented cain/cabin1 from binding to Cn. In addition, in vitro binding assays showed that cain/cabin1 bound to the Cn B-binding domain of Cn A. Taken together, these results indicate that calpain cleaves the calcineurin-binding domain of cain/cabin1 to activate Cn and elicit calcium-triggered cell death.
Author(s)
Kim, MJJo, DGHong, GSKim, BJLai, MCho, DHKim, KWBandyopadhyay, AHong, YMKim, Do HanCho, Chung HeeLiu, JOSnyder, SHJung, Yong Keun
Issued Date
2002-07
Type
Article
DOI
10.1073/pnas.152336999
URI
https://scholar.gist.ac.kr/handle/local/18457
Publisher
National Academy of Sciences
Citation
Proceedings of the National Academy of Sciences of the United States of America, v.99, no.15, pp.9870 - 9875
ISSN
0027-8424
Appears in Collections:
Department of Life Sciences > 1. Journal Articles
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