2003
DOI: 10.1101/gad.260003
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A novel regulation mechanism of DNA repair by damage-induced and RAD23-dependent stabilization of xeroderma pigmentosum group C protein

Abstract: Primary DNA damage sensing in mammalian global genome nucleotide excision repair (GG-NER) is performed by the xeroderma pigmentosum group C (XPC)/HR23B protein complex. HR23B and HR23A are human homologs of the yeast ubiquitin-domain repair factor RAD23, the function of which is unknown. Knockout mice revealed that mHR23A and mHR23B have a fully redundant role in NER, and a partially redundant function in embryonic development. Inactivation of both genes causes embryonic lethality, but appeared still compatibl… Show more

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Cited by 232 publications
(233 citation statements)
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“…XPC protein itself possesses DNA-binding activity, whereas the ubiquitin-binding Rad23B and the calcium-binding centrin-2 protect the initiator complex from degradation and stimulate its activity in DNA repair [28,30]. In double-mutant mouse cells lacking Rad23B as well as the functionally redundant Rad23A ortholog, XPC protein is completely degraded by proteasomal activity [31].…”
Section: Initiation Of Ggr Activity By the Xpc Complexmentioning
confidence: 99%
“…XPC protein itself possesses DNA-binding activity, whereas the ubiquitin-binding Rad23B and the calcium-binding centrin-2 protect the initiator complex from degradation and stimulate its activity in DNA repair [28,30]. In double-mutant mouse cells lacking Rad23B as well as the functionally redundant Rad23A ortholog, XPC protein is completely degraded by proteasomal activity [31].…”
Section: Initiation Of Ggr Activity By the Xpc Complexmentioning
confidence: 99%
“…Rad23-family proteins can block extension of ubiquitin chains (Ortolan et al, 2000;Chen et al, 2001), and hHR23 proteins can block proteasome degradation of certain substrates (Hiyama et al, 1999;Raasi and Pickart, 2003). MEFs derived from targeted deletion of the mouse orthologs of hHR23 (mHR23A and B) demonstrated defects in xeroderma pigmentosa group-C (XP-C) protein stabilization, consistent with a role for mHR23 proteins in stabilizing specific proteasome substrates (Ng et al, 2003).…”
Section: Introductionmentioning
confidence: 98%
“…The basic hypothesis in the field of NER is that the mammalian DNA repair apparatus recognizes structural distortions and thermodynamic destabilization in the DNA duplex caused by the lesions, followed by a verification step that detects the presence of a chemically modified nucleobase and the excision of a fragment 24-32 nucleotides long that contains the damaged base. [3][4][5][6][7][8][9][10][11] It is now established that the first and rate-determining step in NER is the recognition of the bulky lesions by the XPC/HR23B protein heterodimer complex. 12 Since the NER machinery processes a diverse array of bulky lesions with different efficiencies, the conformational features that invoke NER are of great interest.…”
Section: Introductionmentioning
confidence: 99%