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二肽基肽酶IV在兔肾刷状缘膜小泡中从β-酪蛋白吗啡摄取肽氮的作用。

Role of dipeptidyl peptidase IV in uptake of peptide nitrogen from beta-casomorphin in rabbit renal BBMV.

作者信息

Miyamoto Y, Ganapathy V, Barlas A, Neubert K, Barth A, Leibach F H

出版信息

Am J Physiol. 1987 Apr;252(4 Pt 2):F670-7. doi: 10.1152/ajprenal.1987.252.4.F670.

Abstract

We examined the handling of radiolabeled beta-casomorphin, Tyr-Pro-[3H]Phe-Pro-Gly, by rabbit renal brush-border membrane vesicles (BBMV). The uptake of radiolabel into the vesicles was Na+-independent, but an inward-directed H+ gradient stimulated the uptake. The H+ gradient-dependent uptake was further accelerated by an interior-negative membrane potential, but inhibited in the presence of a protonophore. Treatment of the membrane vesicles with diisopropylfluorophosphate (DFP) greatly reduced the uptake of the radiolabel. Control as well as DFP-treated vesicles exhibited H+ gradient-dependent Gly-Sar uptake. Unlabeled beta-casomorphin inhibited Gly-Sar uptake in control vesicles, but the inhibition was significantly reduced in DFP-treated vesicles. DFP inhibited the activity of dipeptidyl peptidase IV in these vesicles and there was a direct correlation between the activity of the enzyme and the capacity of beta-casomorphin to inhibit Gly-Sar uptake. Many di- and tripeptides reduced the uptake of Gly-Sar and the uptake of radiolabel from beta-[3H]casomorphin to a similar extent. We conclude that beta-casomorphin is hydrolyzed by dipeptidyl peptidase IV and the products are transported into the vesicles by the H+ gradient-driven peptide transport system. This conclusion is supported by the results from the analysis of the incubation medium by high-performance liquid chromatography that showed rapid hydrolysis of the pentapeptide by brush-border membranes to di- and tripeptides.

摘要

我们研究了兔肾刷状缘膜囊泡(BBMV)对放射性标记的β-酪蛋白吗啡,即酪氨酰-脯氨酰-[³H]苯丙氨酰-脯氨酰-甘氨酸的处理情况。放射性标记物摄入囊泡的过程不依赖于钠离子,但内向的氢离子梯度会刺激其摄入。氢离子梯度依赖性摄入在膜内负电位的情况下会进一步加速,但在质子载体存在时会受到抑制。用二异丙基氟磷酸酯(DFP)处理膜囊泡会大大降低放射性标记物的摄入。对照囊泡以及经DFP处理的囊泡均表现出氢离子梯度依赖性甘氨酰-肌氨酸摄入。未标记的β-酪蛋白吗啡会抑制对照囊泡中甘氨酰-肌氨酸的摄入,但在经DFP处理的囊泡中这种抑制作用会显著降低。DFP抑制了这些囊泡中二肽基肽酶IV的活性,并且该酶的活性与β-酪蛋白吗啡抑制甘氨酰-肌氨酸摄入的能力之间存在直接相关性。许多二肽和三肽会在相似程度上降低甘氨酰-肌氨酸的摄入以及β-[³H]酪蛋白吗啡中放射性标记物的摄入。我们得出结论,β-酪蛋白吗啡被二肽基肽酶IV水解,其产物通过氢离子梯度驱动的肽转运系统转运到囊泡中。高效液相色谱法对孵育培养基的分析结果支持了这一结论,该结果显示刷状缘膜能迅速将五肽水解为二肽和三肽。

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