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The arginine finger of the Bloom syndrome protein: its structural organization and its role in energy coupling

机译:Bloom综合征蛋白的精氨酸指:其结构组织及其在能量耦合中的作用

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摘要

RecQ family helicases are essential in maintaining chromosomal DNA stability and integrity. Despite extensive studies, the mechanisms of these enzymes are still poorly understood. Crystal structures of many helicases reveal a highly conserved arginine residue located near the gamma-phosphate of ATP. This residue is widely recognized as an arginine finger, and may sense ATP binding and hydrolysis, and transmit conformational changes. We investigated the existence and role of the arginine finger in the Bloom syndrome protein (BLM), a RecQ family helicase, in ATP hydrolysis and energy coupling. Our studies by combination of structural modelling, site-directed mutagenesis and biochemical and biophysical approaches, demonstrate that mutations of residues interacting with the -phosphate of ATP or surrounding the ATP-binding sites result in severe impairment in the ATPase activity of BLM. These mutations also impair BLMs DNA-unwinding activities, but do not affect its ATP and DNA-binding abilities. These data allow us to identify R982 as the residue that functions as a BLM arginine finger. Our findings further indicate how the arginine finger is precisely positioned by the conserved motifs with respect to the gamma-phosphate.
机译:RecQ家族解旋酶对于维持染色体DNA的稳定性和完整性至关重要。尽管进行了广泛的研究,但对这些酶的机制仍知之甚少。许多解旋酶的晶体结构揭示了位于ATPγ-磷酸附近的高度保守的精氨酸残基。该残基被广泛认为是精氨酸指,可以感知ATP结合和水解,并传递构象变化。我们调查了布卢姆综合症蛋白(BLM),RecQ家族解旋酶中的精氨酸手指在ATP水解和能量耦合中的存在和作用。我们通过结构建模,定点诱变以及生化和生物物理方法相结合的研究表明,与ATP的-磷酸相互作用或围绕ATP结合位点的残基突变会严重损害BLM的ATPase活性。这些突变也损害了BLM的DNA解链活性,但不影响其ATP和DNA结合能力。这些数据使我们能够将R982鉴定为具有BLM精氨酸指功能的残基。我们的发现进一步表明,相对于γ-磷酸,保守的基序如何精确地定位精氨酸手指。

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