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包含活性位点酪氨酸的人拓扑异构酶I C末端结构域片段是一种熔球态:对有活性的生产性复合物形成的启示。

Human topoisomerase I C-terminal domain fragment containing the active site tyrosine is a molten globule: implication for the formation of competent productive complex.

作者信息

Punchihewa Chandanamali, Dai Jixun, Carver Megan, Yang Danzhou

机构信息

College of Pharmacy, The University of Arizona, 1703 E. Mabel Street, Tucson, AZ 85721, USA.

出版信息

J Struct Biol. 2007 Jul;159(1):111-21. doi: 10.1016/j.jsb.2007.03.001. Epub 2007 Mar 12.

Abstract

Human topoisomerase I (topo I) is an essential cellular enzyme that relaxes DNA supercoiling. The 6.3 kDa C-terminal domain of topo I contains the active site tyrosine (Tyr723) but lacks enzymatic activity by itself. Activity can be fully reconstituted when the C-terminal domain is associated with the 56 kDa core domain. Even though several crystal structures of topo I/DNA complexes are available, crystal structures of the free topo I protein or its individual domain fragments have been difficult to obtain. In this report we analyze the human topo I C-terminal domain structure using a variety of biophysical methods. Our results indicate that this fragment protein (topo6.3) appears to be in a molten globule state. It appears to have a native-like tertiary fold that contains a large population of alpha-helix secondary structure and extensive surface hydrophobic regions. Topo6.3 is known to be readily activated with the association of the topo I core domain, and the molten globule state of topo6.3 is likely to be an energy-favorable conformation for the free topo I C-terminal domain protein. The structural fluctuation and plasticity may represent an efficient mechanism in the topo I functional pathway, where the flexibility aids in the complementary association with the core domain and in the formation of a fully productive topo I complex.

摘要

人拓扑异构酶I(拓扑异构酶I)是一种必需的细胞酶,可松弛DNA超螺旋。拓扑异构酶I的6.3 kDa C末端结构域包含活性位点酪氨酸(Tyr723),但自身缺乏酶活性。当C末端结构域与56 kDa核心结构域结合时,活性可以完全重建。尽管有几种拓扑异构酶I/DNA复合物的晶体结构,但游离拓扑异构酶I蛋白或其单个结构域片段的晶体结构很难获得。在本报告中,我们使用多种生物物理方法分析了人拓扑异构酶I C末端结构域的结构。我们的结果表明,该片段蛋白(拓扑6.3)似乎处于熔球状态。它似乎具有类似天然的三级折叠,包含大量的α-螺旋二级结构和广泛的表面疏水区域。已知拓扑6.3很容易被拓扑异构酶I核心结构域激活,并且拓扑6.3的熔球状态可能是游离拓扑异构酶I C末端结构域蛋白的能量有利构象。结构波动和可塑性可能代表了拓扑异构酶I功能途径中的一种有效机制,其中灵活性有助于与核心结构域的互补结合以及形成完全有活性的拓扑异构酶I复合物。

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