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人回肠刷状缘膜囊泡对丙酸酯的转运

Transport of propionate by human ileal brush-border membrane vesicles.

作者信息

Harig J M, Soergel K H, Barry J A, Ramaswamy K

机构信息

Gastroenterology Division, Medical College of Wisconsin, Milwaukee 53226.

出版信息

Am J Physiol. 1991 May;260(5 Pt 1):G776-82. doi: 10.1152/ajpgi.1991.260.5.G776.

Abstract

Human ileal brush-border membrane vesicles were employed to study the mechanisms of short-chain fatty acid (propionate) absorption especially to determine the effects of intravesicular HCO3- and the component of nonionic diffusion. Preloading the vesicles with HCO3- resulted in up to 20-fold "overshoots" of transport, and this effect was not seen with other intravesicular anions. This transport process was very fast (peak uptake 6 s) and was not due to intravesicular buffering by HCO3-. Radiolabeled propionate transport demonstrated transstimulation when the vesicles were preloaded with unlabeled propionate. An inward H+ gradient led to stimulation of propionate transport much smaller than in the presence of trans-HCO3-, whereas an inward Na+ gradient had no effect. Propionate transport was attenuated by the anion exchange inhibitors SITS and DIDS. Under HCO3- gradient conditions, propionate transport exhibited saturation kinetics with an apparent Km of 21 +/- 3 mM and a Vmax of 50 +/- 3 nmol.mg protein-1.3 s-1. Propionate transport was inhibited up to 40% by 2-5 carbon short-chain fatty acids (10 mM) but not by other organic anions. Short-chain fatty acid transport in the human ileum is Na+ independent and occurs mostly via a specific anion exchange mechanism with HCO3-. Our results also demonstrate a small component of nonionic diffusion of the protonated fatty acid (or anion exchange for OH-).

摘要

用人回肠刷状缘膜囊泡研究短链脂肪酸(丙酸)的吸收机制,特别是确定囊泡内HCO3-和非离子扩散成分的影响。用HCO3-预加载囊泡会导致转运出现高达20倍的“过冲”,而其他囊泡内阴离子则未观察到这种效应。这种转运过程非常快(峰值摄取时间为6秒),且不是由于HCO3-对囊泡内的缓冲作用。当用未标记的丙酸预加载囊泡时,放射性标记的丙酸转运显示出转刺激作用。内向H+梯度对丙酸转运的刺激作用远小于存在跨膜HCO3-时,而内向Na+梯度则无影响。阴离子交换抑制剂SITS和DIDS可减弱丙酸转运。在HCO3-梯度条件下,丙酸转运呈现饱和动力学,表观Km为21±3 mM,Vmax为50±3 nmol·mg蛋白-1·3 s-1。2-5个碳原子的短链脂肪酸(10 mM)可使丙酸转运抑制高达40%,但其他有机阴离子则无此作用。人回肠中的短链脂肪酸转运不依赖Na+,主要通过与HCO3-的特异性阴离子交换机制进行。我们的结果还表明,质子化脂肪酸存在一小部分非离子扩散(或与OH-进行阴离子交换)。

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