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The XPD helicase: XPanDing archaeal XPD structures to get a grip on human DNA repair

  • Stefanie C. Wolski , Jochen Kuper and Caroline Kisker
Published/Copyright: May 19, 2010
Biological Chemistry
From the journal Volume 391 Issue 7

Abstract

Xeroderma pigmentosum complementation group D protein (XPD) is an iron-sulfur cluster containing 5′-3′ helicase and, in humans, part of the transcription factor TFIIH. TFIIH is involved in nucleotide excision repair as well as in transcription initiation. Recently, three different groups have reported the structures of archaeal XPDs. All structures revealed a four-domain organization with two RecA-like domains, an Arch domain and an iron-sulfur cluster domain. It was possible to rationalize several of the mutations in the human XPD gene that lead to one of the three severe diseases xeroderma pigmentosum, Cockayne syndrome and trichothiodystrophy. The different structures are compared and disease-related mutations are discussed.


Corresponding author

Received: 2010-1-20
Accepted: 2010-3-22
Published Online: 2010-05-19
Published in Print: 2010-07-01

©2010 by Walter de Gruyter Berlin New York

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