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Structure and function of a squalene cyclase

机译:角鲨烯环化酶的结构和功能

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摘要

The crystal structure of squalene-hopene cyclase from Alicyclobacillus acidocaldarius was determined at 2.9 angstrom resolution. The mechanism and sequence of this cyclase are closely related to those of 2,3-oxidosqualene cyclases that catalyze the cyclization step in cholesterol biosynthesis. The structure reveals a membrane protein with membrane-binding characteristics similar to those of prostaglandin-H2 synthase, the only other reported protein of this type. The active site of the enzyme is located in a large central cavity that is of suitable size to bind squalene in its required conformation and that is lined by aromatic residues. The structure supports a mechanism in which the acid starting the reaction by protonating a carbon-carbon double bond is an aspartate that is coupled to a histidine. Numerous surface alpha helices are connected by characteristic QW-motifs (Q is glutamine and W is tryptophan) that tighten the protein structure, possibly for absorbing the reaction energy without structural damage.
机译:来自酸热脂环酸杆菌的角鲨烯-戊环化酶的晶体结构被确定为2.9埃的分辨率。该环化酶的机理和序列与催化胆固醇生物合成中环化步骤的2,3-氧化鲨烯环化酶密切相关。该结构揭示了一种膜蛋白,该膜蛋白具有与前列腺素-H2合酶相似的膜结合特性,而前列腺素-H2合酶是这种类型的唯一报道蛋白。酶的活性位点位于大的中央空腔中,该空腔的大小适合于以其所需构象结合角鲨烯,并以芳香族残基为内衬。该结构支持这样一种机制,其中通过使碳-碳双键质子化而开始反应的酸是与组氨酸偶联的天冬氨酸。许多表面α螺旋通过特有的QW基序(Q是谷氨酰胺,W是色氨酸)连接在一起,这些基序可以收紧蛋白质结构,可能用于吸收反应能量而不会破坏结构。

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