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The Exonuclease TREX1 is in the SET Complex and Acts in Concert with NM23-H1 to Degrade DNA During Granzyme A-mediated Cell Death

Overview
Journal Mol Cell
Publisher Cell Press
Specialty Cell Biology
Date 2006 Jul 5
PMID 16818237
Citations 133
Authors
Dipanjan Chowdhury
Paul J Beresford
Pengcheng Zhu
Dong Zhang
Jung-Suk Sung
Bruce Demple
Fred W Perrino
Judy Lieberman
Affiliations
Soon will be listed here.
Abstract

Granzyme A (GzmA) activates a caspase-independent cell death pathway with morphological features of apoptosis. Single-stranded DNA damage is initiated when the endonuclease NM23-H1 becomes activated to nick DNA after granzyme A cleaves its inhibitor, SET. SET and NM23-H1 reside in an endoplasmic reticulum-associated complex (the SET complex) that translocates to the nucleus in response to superoxide generation by granzyme A. We now find the 3'-to-5' exonuclease TREX1, but not its close homolog TREX2, in the SET complex. TREX1 binds to SET and colocalizes and translocates with the SET complex. NM23-H1 and TREX1 work in concert to degrade DNA. Silencing NM23-H1 or TREX1 inhibits DNA damage and death of cells treated with perforin (PFN) and granzyme A, but not of cells treated with perforin and granzyme B (GzmB). After granzyme A activates NM23-H1 to make single-stranded nicks, TREX1 removes nucleotides from the nicked 3' end to reduce the possibility of repair by rejoining the nicked ends.

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