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胆汁盐对马PLRP2的激活作用并不需要辅脂酶。

Activation of horse PLRP2 by bile salts does not require colipase.

作者信息

Jayne Sandrine, Kerfelec Brigitte, Foglizzo Edith, Granon Simone, Hermoso Juan, Chapus Catherine, Crenon Isabelle

机构信息

Nutrition humaine et lipides, INSERM-U476, 18 Avenue Mozart, 13009 Marseille, France.

出版信息

Biochemistry. 2002 Jul 2;41(26):8422-8. doi: 10.1021/bi025867j.

Abstract

Although structurally similar to pancreatic lipase (PL), the key enzyme of intestinal fat digestion, pancreatic lipase-related protein type 2 (PLRP2) differs from PL in certain functional properties. Notably, PLRP2 has a broader substrate specificity than PL, and unlike that of PL, its activity is not restored by colipase in the presence of bile salts. In the studies presented here, the activation mechanism of horse PLRP2 was studied through active site-directed inhibition experiments, and the results demonstrate fundamental differences with that of PL. The opening of the horse PLRP2 flap occurs as soon as bile salt monomers are present, is accelerated in the presence of micelles, and does not require the presence of colipase. Moreover, in contrast to PL, horse PLRP2 is able to directly interact with a bile salt micelle to form an active binary complex, without the micelle being presented by colipase, as evidenced by molecular sieving experiments. These findings, together with the sensitivity of the horse PLRP2 flap to partial proteolysis, are indicative of a higher flexibility of the flap of horse PLRP2 relative to PL. From these results, it can be concluded that PLRP2 can adopt an active conformation in the intestine, which could be important for the further understanding of the physiological role of PLRP2. Finally, this work emphasizes the essential role of colipase in lipase catalysis at the lipid-water interface in the presence of bile.

摘要

尽管胰腺脂肪酶相关蛋白2(PLRP2)在结构上与肠道脂肪消化的关键酶胰腺脂肪酶(PL)相似,但在某些功能特性上与PL有所不同。值得注意的是,PLRP2比PL具有更广泛的底物特异性,并且与PL不同,在胆盐存在的情况下,其活性不会被辅脂酶恢复。在本文所呈现的研究中,通过活性位点定向抑制实验研究了马PLRP2的激活机制,结果表明其与PL存在根本差异。一旦存在胆盐单体,马PLRP2的瓣片就会打开,在存在胶束的情况下会加速打开,并且不需要辅脂酶的存在。此外,与PL不同,马PLRP2能够直接与胆盐胶束相互作用形成活性二元复合物,而无需辅脂酶呈现胶束,分子筛实验证明了这一点。这些发现,连同马PLRP2瓣片对部分蛋白水解的敏感性,表明马PLRP2的瓣片相对于PL具有更高的灵活性。从这些结果可以得出结论,PLRP2在肠道中可以采取活性构象,这对于进一步理解PLRP2的生理作用可能很重要。最后,这项工作强调了辅脂酶在胆盐存在下脂质-水界面处脂肪酶催化中的重要作用。

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