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磷脂、胰腺磷脂酶A2和脂肪酸对膳食脂肪消化的重要性:猪酶的体外实验

Importance of phospholipids, pancreatic phospholipase A2, and fatty acid for the digestion of dietary fat: in vitro experiments with the porcine enzymes.

作者信息

Borgström B

出版信息

Gastroenterology. 1980 May;78(5 Pt 1):954-62.

PMID:7380202
Abstract

Long chain triglycerides emulsified with phospholipid are not directly available for hydrolysis by pancreatic lipase in vitro even in the presence of bile salts and colipase. The inhibition can be overcome by pancreatic phospholipase A2. There is a limited hydrolysis of the phospholipid during this period. The inhibition is explained by the finding that lipase does not bind to triglyceride emulsified by phospholipid but remains in the aqueous phase. A limited hydrolysis of the phospholipid by phospholipase A2 results in the binding of lipase to the substrate interface and a rapid rate of hydrolysis of the triglyceride. With time the inhibition of lipase activity can also be overcome by pancreatic lipase. A lag phase is seen before the accelerated hydrolysis of triglyceride reaches a high rate. The length of the lag phase is dependent on factors such as lipase and colipase concentration, pH, Ca++, and concentration of bile salt. During the lag phase no significant hydrolysis of phospholipid occurs. The primary factor is the binding of colipase to the substrate interface. Fatty acid present in the oil phase or produced from it by a limited hydrolysis of phospholipid by phospholipase A2 or triglyceride by lipase, changes the properties of the interface so that colipase can bind and thereby lipase via its binding to colipase. The milieu of small intestinal content favors the concerted action of several factors to make dietary triglyceride available for an effective hydrolysis by pancreatic lipase.

摘要

即使在存在胆盐和辅脂酶的情况下,用磷脂乳化的长链甘油三酯在体外也不能直接被胰脂肪酶水解。这种抑制作用可被胰磷脂酶A2克服。在此期间磷脂的水解有限。这种抑制作用的解释是,脂肪酶不与磷脂乳化的甘油三酯结合,而是留在水相中。磷脂酶A2对磷脂的有限水解导致脂肪酶与底物界面结合,甘油三酯的水解速率加快。随着时间的推移,胰脂肪酶也能克服脂肪酶活性的抑制作用。在甘油三酯加速水解达到高速之前会出现一个延迟期。延迟期的长度取决于脂肪酶和辅脂酶浓度、pH值、钙离子以及胆盐浓度等因素。在延迟期内,磷脂不会发生显著水解。主要因素是辅脂酶与底物界面的结合。油相中存在的脂肪酸或由磷脂酶A2对磷脂的有限水解或脂肪酶对甘油三酯的水解产生的脂肪酸,会改变界面的性质,使辅脂酶能够结合,从而脂肪酶通过与辅脂酶的结合而结合。小肠内容物的环境有利于多种因素协同作用,使膳食甘油三酯能够被胰脂肪酶有效水解。

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