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Identification of one of the apurinic/apyrimidinic lyase active sites of topoisomerase V by structural and functional studies

机译:通过结构和功能研究鉴定拓扑异构酶V的嘌呤/嘧啶二烯酸裂解酶活性位点之一

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摘要

Topoisomerase V (Topo-V) is the only member of a novel topoisomerase subtype. Topo-V is unique because it is a bifunctional enzyme carrying both topoisomerase and DNA repair lyase activities within the same protein. Previous studies had shown that the topoisomerase domain spans the N-terminus of the protein and is followed by 12 tandem helix-hairpin-helix [(HhH)(2)] domains. There are at least two DNA repair lyase active sites for apurinic/apyrimidinic (AP) site processing, one within the N-terminal region and the second within the C-terminal domain of Topo-V, but their exact locations and characteristics are unknown. In the present study, the N-terminal 78-kDa fragment of Topo-V (Topo-78), containing the topoisomerase domain and one of the lyase DNA repair domains, was characterized by structural and biochemical studies. The results show that an N-terminal 69-kDa fragment is the minimal fragment with both topoisomerase and AP lyase activities. The lyase active site of Topo-78 is at the junction of the fifth and sixth (HhH)(2) domains. From the biochemical and structural data, it appears that Lys571 is the most probable nucleophile responsible for the lyase activity. Our experiments also suggest that Topo-V most likely acts as a Class I AP endonuclease in vivo.
机译:拓扑异构酶V(Topo-V)是新型拓扑异构酶亚型的唯一成员。 Topo-V是独特的,因为它是一种双功能酶,在同一蛋白质中同时具有拓扑异构酶和DNA修复裂合酶活性。先前的研究表明,拓扑异构酶结构域跨越蛋白质的N末端,后面是12个串联的螺旋-发夹-螺旋[(HhH)(2)]域。有至少两个DNA修复裂解酶活性位点用于嘌呤/嘧啶(AP)加工,一个在Topo-V的N端区域内,另一个在C端域内,但其确切位置和特征尚不清楚。在本研究中,Topo-V(Topo-78)的N端78-kDa片段包含拓扑异构酶结构域和一种裂解酶DNA修复结构域,通过结构和生化研究进行了表征。结果表明,N端69-kDa片段是具有拓扑异构酶和AP裂解酶活性的最小片段。 Topo-78的裂解酶活性位点位于第五和第六(HhH)(2)域的交界处。从生化和结构数据看,Lys571是最可能引起裂解酶活性的亲核试剂。我们的实验还表明,Topo-V最有可能在体内充当I类AP核酸内切酶。

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