解旋酶
ATP酶
突变
遗传学
RNA解旋酶A
生物
化学
细胞生物学
生物化学
酶
基因
核糖核酸
作者
Martin Borch Jensen,Christopher Dunn,Guido Keijzers,Tomasz Kulikowicz,Lene Juel Rasmussen,Deborah L. Croteau,Vilhelm A. Bohr
出处
期刊:Aging
[Impact Journals LLC]
日期:2012-12-04
卷期号:4 (11): 790-802
被引量:11
标识
DOI:10.18632/aging.100506
摘要
RECQL4 is one of five members of the human RecQ helicase family, and is implicated in three syndromes displaying accelerating aging, developmental abnormalities and a predisposition to cancer. In this study, we purified three variants of RECQL4 carrying previously reported patient mutations. These three mutant proteins were analyzed for the known biochemical activities of RECQL4: DNA binding, unwinding of duplex DNA, ATP hydrolysis and annealing of simplex DNA. Further, the mutant proteins were evaluated for stability and recruitment to sites of laser-induced DNA damage. One mutant was helicase-dead, had marginal ATPase activity and may be structurally compromised, while the other two showed greatly reduced helicase and ATPase activities. The remaining biochemical activities and ability to recruit to damage sites were not significantly impaired for any of the mutants. Our findings demonstrate a consistent pattern of functional deficiency and provide further support for a helicase-dependent cellular function of RECQL4 in addition to its N-terminus-dependent role in initiation of replication, a function that may underlie the phenotype of RECQL4-linked disease.
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