Roles of the Bloom's syndrome helicase in the maintenance of genome stability | Zendy

Csanád Z. Bachrati | Zendy; Chit Fang Cheok | Zendy; KokLung Chan | Zendy; Christine Ralf | Zendy; Leonard Wu | Zendy; Ian D. Hickson | Zendy

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Roles of the Bloom's syndrome helicase in the maintenance of genome stability

Author(s) -

Csanád Z. Bachrati,

Chit Fang Cheok,

KokLung Chan,

Christine Ralf,

Leonard Wu,

Ian D. Hickson

Publication year - 2005

Publication title -

biochemical society transactions

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 2.562

H-Index - 144

eISSN - 1470-8752

pISSN - 0300-5127

DOI - 10.1042/bst20051456

Subject(s) - bloom syndrome , helicase , bloom , genome , biology , genetics , computational biology , gene , ecology , rna

The RecQ family of DNA helicases is highly conserved in evolution from bacteria to humans. Of the five known human RecQ family members, three (BLM, WRN and RECQ4, which cause Bloom's syndrome, Werner's syndrome and Rothmund-Thomson syndrome respectively) are mutated in distinct clinical disorders associated with cancer predisposition and/or premature aging. BLM forms part of a multienzyme complex including topoisomerase IIIalpha, replication protein A and a newly identified factor called BLAP75. Together, these proteins play a role in the resolution of DNA structures that arise during the process of homologous recombination repair. In the absence of BLM, cells show genomic instability and a high incidence of sister-chromatid exchanges. In addition to a DNA structure-specific helicase activity, BLM also catalyses Holliday-junction branch migration and the annealing of complementary single-stranded DNA molecules

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