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Structural Analysis of the Sulfotransferase (3-O-Sulfotransferase Isoform 3) Involved in the Biosynthesis of an Entry Receptor for Herpes Simplex Virus

机译:参与单纯疱疹病毒进入受体生物合成的硫转移酶(3-O-硫转移酶同工型3)的结构分析

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摘要

Heparan sulfate (HS) plays essential roles in assisting herpes simplex virus infection and other biological processes. The biosynthesis of HS includes numerous specialized sulfotransferases that generate a variety of sulfated saccharide sequences, conferring the selectivity of biological functions of HS. We report a structural study of human HS 3-O-sulfotransferase isoform 3 (3-OST-3), a key sulfotransferase that transfers a sulfuryl group to a specific glucosamine in HS generating an entry receptor for herpes simplex virus 1. We have obtained the crystal structure of 3-OST-3 at 1.95 Å in a ternary complex with 3′-phosphoadenosine 5′-phosphate and a tetrasaccharide substrate. Mutational analyses were also performed on the residues involved in the binding of the substrate. Residues Gln255 and Lys368 are essential for the sulfotransferase activity and lie within hydrogen bonding distances to the carboxyl and sulfo groups of the uronic acid unit. These residues participate in the substrate recognition of 3-OST-3. This structure provides atomic level evidence for delineating the substrate recognition and catalytic mechanism for 3-OST-3.
机译:硫酸乙酰肝素(HS)在协助单纯疱疹病毒感染和其他生物学过程中起重要作用。 HS的生物合成包括许多专门的磺基转移酶,可产生多种硫酸化的糖序列,赋予HS生物学功能的选择性。我们报告了人类HS 3-O-磺基转移酶同工型3(3-OST-3)的结构研究,这是一种关键的磺基转移酶,可将硫基转移到HS中的特定氨基葡萄糖上,从而产生单纯疱疹病毒1的进入受体。在与3'-磷酸腺苷5'-磷酸和四糖底物形成的三元复合物中,3-OST-3的晶体结构为1.95Å。还对涉及底物结合的残基进行了突变分析。残基Gln 255 和Lys 368 对于磺基转移酶活性至关重要,并且位于与糖醛酸单元的羧基和磺基氢键的距离之内。这些残基参与3-OST-3的底物识别。这种结构为描述3-OST-3的底物识别和催化机理提供了原子级证据。

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