Calpains Mediate P53 Activation and Neuronal Death Evoked by DNA Damage

Overview

Journal J Biol Chem

Specialty Biochemistry

Date 2003 May 2

PMID 12721303

Citations 35

Authors

Mary Sedarous

Elizabeth Keramaris

Michael OHare

Edon Melloni

Ruth S Slack

John S Elce

Peter A Greer

David S Park

Affiliations

Soon will be listed here.

Abstract

DNA damage is an initiator of neuronal death implicated in neuropathological conditions such as stroke. Previous evidence has shown that apoptotic death of embryonic cortical neurons treated with the DNA damaging agent camptothecin is dependent upon the tumor suppressor p53, an upstream death mediator, and more distal death effectors such as caspases. We show here that the calcium-regulated cysteine proteases, calpains, are activated during DNA damage induced by camptothecin treatment. Moreover, calpain deficiency, calpastatin expression, or pharmacological calpain inhibitors prevent the death of embryonic cortical neurons, indicating the important role of calpain in DNA damage-induced death. Calpain inhibition also significantly reduced and delayed the induction of p53. Consistent with the actions of calpains upstream of p53 and the proximal nature of p53 death signaling, calpain inhibition inhibited cytochrome c release and DEVD-AFC cleavage activity. Taken together, our results indicate that calpains are a key mediator of p53 induction and consequent caspase-dependent neuronal death due to DNA damage.

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