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基于真菌脂肪酶-抑制剂复合物结构的脂肪酶界面激活模型。

A model for interfacial activation in lipases from the structure of a fungal lipase-inhibitor complex.

作者信息

Brzozowski A M, Derewenda U, Derewenda Z S, Dodson G G, Lawson D M, Turkenburg J P, Bjorkling F, Huge-Jensen B, Patkar S A, Thim L

机构信息

Department of Chemistry, University of York, Heslington, UK.

出版信息

Nature. 1991 Jun 6;351(6326):491-4. doi: 10.1038/351491a0.

Abstract

Lipases are hydrolytic enzymes which break down triacylglycerides into free fatty acids and glycerols. They have been classified as serine hydrolases owing to their inhibition by diethyl p-nitrophenyl phosphate. Lipase activity is greatly increased at the lipid-water interface, a phenomenon known as interfacial activation. X-ray analysis has revealed the atomic structures of two triacylglycerol lipases, unrelated in sequence: the human pancreatic lipase (hPL)4, and an enzyme isolated from the fungus Rhizomucor (formerly Mucor) miehei (RmL). In both enzymes the active centres contain structurally analogous Asp-His-Ser triads (characteristic of serine proteinases), which are buried completely beneath a short helical segment, or 'lid'. Here we present the crystal structure (at 3 A resolution) of a complex of R. miehei lipase with n-hexylphosphonate ethyl ester in which the enzyme's active site is exposed by the movement of the helical lid. This movement also increases the nonpolarity of the surface surrounding the catalytic site. We propose that the structure of the enzyme in this complex is equivalent to the activated state generated by the oil-water interface.

摘要

脂肪酶是一种水解酶,可将三酰甘油分解为游离脂肪酸和甘油。由于它们会被对硝基苯基磷酸二乙酯抑制,因此被归类为丝氨酸水解酶。脂肪酶的活性在脂质-水界面处会大幅增加,这一现象被称为界面激活。X射线分析揭示了两种序列不相关的三酰甘油脂肪酶的原子结构:人胰脂肪酶(hPL)4和从米黑根毛霉(以前的毛霉属)中分离出的一种酶(RmL)。在这两种酶中,活性中心都含有结构类似的天冬氨酸-组氨酸-丝氨酸三联体(丝氨酸蛋白酶的特征),它们完全埋藏在一个短的螺旋片段或“盖子”之下。在此,我们展示了米黑根毛霉脂肪酶与正己基膦酸乙酯复合物的晶体结构(分辨率为3埃),其中酶的活性位点通过螺旋盖子的移动而暴露。这种移动还增加了催化位点周围表面的非极性。我们认为该复合物中酶的结构等同于由油水界面产生的活化状态。

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