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舌脂肪酶对脂肪的消化:胃和小肠上段的脂肪分解机制。

Fat digestion by lingual lipase: mechanism of lipolysis in the stomach and upper small intestine.

作者信息

Liao T H, Hamosh P, Hamosh M

出版信息

Pediatr Res. 1984 May;18(5):402-9. doi: 10.1203/00006450-198405000-00002.

Abstract

Ten to 30% of dietary fat is hydrolyzed in the stomach by lingual lipase, an enzyme secreted from lingual serous glands. We investigated the substrate specificity of this enzyme as well as the potential of lingual lipase to act in the upper small intestine i.e., in the presence of bile salts and lecithin. The data presented show that partially purified preparations of rat lingual lipase and the lipase in gastric aspirates of newborn infants have identical substrate specificity: medium-chain triglycerides were hydrolyzed at rates 5-8-fold higher than long-chain triglycerides; the rat and human enzymes do not hydrolyze the ester bond of lecithin or cholesteryl-ester. In contrast to pancreatic lipase, the hydrolysis of triglycerides by lingual lipase is not inhibited by lecithin. But, similar to pancreatic lipase the activity of lingual lipase is inhibited by bile salts, the extent of inhibition varying with its nature and concentration. This inactivation is not prevented by colipase but is partially averted by lipids and protein, suggesting that lingual lipase can remain active in the duodenum. The pH optimum of the enzyme (2.2-6.5 in the rat and 3.5-6.0 in human gastric aspirates) is compatible with continued activity in the upper small intestine, especially during the neonatal period, when the luminal pH is under 6.5. The marked variation in lipase activity levels in gastric aspirates of newborn infants is probably due to individual variations in enzyme amounts. The characteristics of the lipase are however identical in infants with low, intermediate or high activity levels.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

膳食脂肪的10%至30%在胃中被舌脂肪酶水解,舌脂肪酶是一种由舌浆液腺分泌的酶。我们研究了这种酶的底物特异性以及舌脂肪酶在上段小肠(即存在胆盐和卵磷脂的情况下)发挥作用的潜力。所呈现的数据表明,大鼠舌脂肪酶的部分纯化制剂和新生儿胃吸出物中的脂肪酶具有相同的底物特异性:中链甘油三酯的水解速率比长链甘油三酯高5至8倍;大鼠和人类的这种酶不会水解卵磷脂或胆固醇酯的酯键。与胰脂肪酶不同,舌脂肪酶对甘油三酯的水解不受卵磷脂抑制。但是,与胰脂肪酶类似,舌脂肪酶的活性受胆盐抑制,抑制程度随胆盐的性质和浓度而变化。这种失活不受辅脂酶阻止,但脂质和蛋白质可部分避免这种失活,这表明舌脂肪酶在十二指肠中可保持活性。该酶的最适pH值(大鼠为2.2至6.5,新生儿胃吸出物中人为3.5至6.0)与在上段小肠中持续保持活性相符,尤其是在新生儿期,此时肠腔pH值低于6.5。新生儿胃吸出物中脂肪酶活性水平的显著差异可能是由于酶量的个体差异。然而,低、中或高活性水平婴儿的脂肪酶特征是相同的。(摘要截断于250字)

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