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由ATP结合和水解差异调节的不同MutS DNA结合模式。

Distinct MutS DNA-binding modes that are differentially modulated by ATP binding and hydrolysis.

作者信息

Blackwell L J, Bjornson K P, Allen D J, Modrich P

机构信息

Department of Biochemistry, Duke University Medical Center, Durham, North Carolina 27710, USA.

出版信息

J Biol Chem. 2001 Sep 7;276(36):34339-47. doi: 10.1074/jbc.M104256200. Epub 2001 Jul 13.

Abstract

The role of MutS ATPase in mismatch repair is controversial. To clarify further the function of this activity, we have examined adenine nucleotide effects on interactions of Escherichia coli MutS with homoduplex and heteroduplex DNAs. In contrast to previous results with human MutS alpha, we find that a physical block at one end of a linear heteroduplex is sufficient to support stable MutS complex formation in the presence of ATP.Mg(2+). Surface plasmon resonance analysis at low ionic strength indicates that the lifetime of MutS complexes with heteroduplex DNA depends on the nature of the nucleotide present when MutS binds. Whereas complexes prepared in the absence of nucleotide or in the presence of ADP undergo rapid dissociation upon challenge with ATP x Mg(2+), complexes produced in the presence of ATP x Mg(2+), adenosine 5'-(beta,gamma-imino)triphosphate (AMPPNP) x Mg(2+), or ATP (no Mg(2+)) are resistant to dissociation upon ATP challenge. AMPPNP x Mg(2+) and ATP (no Mg(2+)) reduce MutS affinity for heteroduplex but have little effect on homoduplex affinity, resulting in abolition of specificity for mispaired DNA at physiological salt concentrations. Conversely, the highest mismatch specificity is observed in the absence of nucleotide or in the presence of ADP. ADP has only a limited effect on heteroduplex affinity but reduces MutS affinity for homoduplex DNA.

摘要

MutS 腺苷三磷酸酶在错配修复中的作用存在争议。为了进一步阐明该活性的功能,我们研究了腺嘌呤核苷酸对大肠杆菌 MutS 与同型双链和异型双链 DNA 相互作用的影响。与之前关于人 MutSα 的结果相反,我们发现线性异型双链一端的物理阻断足以在存在 ATP·Mg²⁺ 时支持稳定的 MutS 复合物形成。低离子强度下的表面等离子体共振分析表明,MutS 与异型双链 DNA 复合物的寿命取决于 MutS 结合时存在的核苷酸的性质。在不存在核苷酸或存在 ADP 的情况下制备的复合物在受到 ATP·Mg²⁺ 挑战时会迅速解离,而在存在 ATP·Mg²⁺、腺苷 5′-(β,γ-亚氨基)三磷酸 (AMPPNP)·Mg²⁺ 或 ATP(无 Mg²⁺)时产生的复合物在受到 ATP 挑战时对解离具有抗性。AMPPNP·Mg²⁺ 和 ATP(无 Mg²⁺)降低了 MutS 对异型双链的亲和力,但对同型双链亲和力影响很小,导致在生理盐浓度下对错配 DNA 的特异性丧失。相反,在不存在核苷酸或存在 ADP 的情况下观察到最高的错配特异性。ADP 对异型双链亲和力的影响有限,但降低了 MutS 对同型双链 DNA 的亲和力。

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