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人乳胆汁盐刺激脂肪酶:功能与分子层面

Human milk bile salt-stimulated lipase: functional and molecular aspects.

作者信息

Hernell O, Bläckberg L

机构信息

Department of Pediatrics, University of Umeå, Sweden.

出版信息

J Pediatr. 1994 Nov;125(5 Pt 2):S56-61. doi: 10.1016/s0022-3476(06)80737-7.

Abstract

In breast-fed infants, digestion of milk triglycerides, the major source of energy and long-chain polyunsaturated fatty acids, is catalyzed by a concerted action of gastric lipase, colipase-dependent pancreatic lipase, and bile salt-stimulated lipase (BSSL). The major part of BSSL is present in the milk and the lesser part originates in the infant's exocrine pancreas. Gastric lipase is important in initiating digestion of milk fat globule triglycerides in the stomach. BSSL shifts the final products of triglyceride digestion from monoglyceride and free fatty acid (the products of colipase-dependent pancreatic lipase) to glycerol and free fatty acid, which may promote efficient absorption. Moreover, BSSL is likely to promote efficient use of milk cholesteryl- and fat-soluble vitaminesters and long-chain polyunsaturated fatty acids (> C18). The cDNA sequence has shown that BSSL has a unique primary structure. The N-terminal half is highly conserved between species and shows striking homology to typical esterases, for example, acetylcholine esterase. In contrast, the C-terminal half, containing 16 proline-rich repeats of 11 amino acid residues, is unique to BSSL. Using several recombinant variants of BSSL, we have found that these unique repeats and the glycosylation are completely dispensable for activity. Thus all typical properties of BSSL reside in the N-terminal half of the molecule.

摘要

在母乳喂养的婴儿中,作为能量和长链多不饱和脂肪酸主要来源的乳甘油三酯的消化,是由胃脂肪酶、辅脂酶依赖性胰脂肪酶和胆汁盐刺激脂肪酶(BSSL)协同作用催化的。BSSL的主要部分存在于乳汁中,较少部分源自婴儿的外分泌胰腺。胃脂肪酶在启动胃中乳脂肪球甘油三酯的消化方面很重要。BSSL将甘油三酯消化的最终产物从甘油单酯和游离脂肪酸(辅脂酶依赖性胰脂肪酶的产物)转变为甘油和游离脂肪酸,这可能促进有效吸收。此外,BSSL可能促进乳胆固醇酯、脂溶性维生素酯和长链多不饱和脂肪酸(>C18)的有效利用。cDNA序列显示BSSL具有独特的一级结构。N端的一半在物种间高度保守,与典型酯酶(如乙酰胆碱酯酶)具有显著同源性。相反,C端的一半包含16个富含脯氨酸的11个氨基酸残基的重复序列,这是BSSL独有的。通过使用BSSL的几种重组变体,我们发现这些独特的重复序列和糖基化对于活性完全是可有可无的。因此,BSSL的所有典型特性都存在于分子的N端一半。

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