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嗜盐菌包膜囊泡中光诱导的亮氨酸转运:一种化学渗透系统。

Light-induced leucine transport in Halobacterium halobium envelope vesicles: a chemiosmotic system.

作者信息

MacDonald R E, Lanyi L K

出版信息

Biochemistry. 1975 Jul;14(13):2882-9. doi: 10.1021/bi00684a014.

Abstract

Halabacterium halobium cell envelope vesicles accumulate L-[14-C]leucine during illumination, against a large concentration gradient. Leucine uptake requires Na-+ and is optimal in KCl-loaded vesicles resuspended in KCl-NaCl solution (1.5 M:1.5 M). Half-maximal transport is seen at 1 X 10-minus 6 M leucine. In the dark the accumulated leucine is rapidly and exponentially lost from the vesicles. The action spectrum and the light-intensity dependence indicate that the transport is related to the extrusion of protons, mediated by bacteriorhodopsin. Since light gives rise to both a pH gradient and an opposing transmembrane potential (interior negative), it wass responsible for providing the energy for leucine transport. The following results were obtained under illumination: (1) membrane-permeant cations and valinomycin or gramicidin greatly inhibited leucine transport without altering the pH gradient; (2) buffering both inside and outside the vesicles eliminated the pH gradient while enhancing leucine transport; (3) dicyclohexylcarbodiimide increased the pH gradient without affecting leucine transport; (4) arsenate did not inhibit leucine uptake. A diffusion potential, established by adding valinomycin to KCl-loaded vesicles, caused leucine influx in the dark. These results suggest that the leucine transport system is not coupled to ATP hydrolysis, and responds to the membrane potential rather than to the pH gradient. The Na-+ dependence of the transport and the observation that a small NaCl pulse causes transient leucine influx in the dark in KCl-loaded vesicles, resuspended in KCl, even in the presence of p-trifluoromethoxycarbonylcyanide phenylhydrazone or with buffering, suggest that the translocation of leucine is facilitated by symport with Na-+.

摘要

嗜盐栖热菌的细胞膜囊泡在光照期间会逆着较大的浓度梯度积累L-[14-C]亮氨酸。亮氨酸的摄取需要Na⁺,并且在重悬于KCl-NaCl溶液(1.5 M:1.5 M)中的KCl负载囊泡中最为理想。在1×10⁻⁶ M亮氨酸时可观察到半数最大转运。在黑暗中,积累的亮氨酸会迅速且呈指数级地从囊泡中流失。作用光谱和光强度依赖性表明,该转运与由细菌视紫红质介导的质子外排有关。由于光会产生pH梯度和相反的跨膜电位(内部为负),所以它为亮氨酸转运提供能量。在光照下获得了以下结果:(1)膜通透性阳离子以及缬氨霉素或短杆菌肽在不改变pH梯度的情况下极大地抑制了亮氨酸转运;(2)对囊泡内外进行缓冲消除了pH梯度,同时增强了亮氨酸转运;(3)二环己基碳二亚胺增加了pH梯度,而不影响亮氨酸转运;(4)砷酸盐不抑制亮氨酸摄取。通过向KCl负载的囊泡中添加缬氨霉素建立的扩散电位在黑暗中导致亮氨酸流入。这些结果表明,亮氨酸转运系统不与ATP水解偶联,并且对膜电位而非pH梯度作出反应。转运对Na⁺的依赖性以及在重悬于KCl中的KCl负载囊泡中,即使存在对三氟甲氧基羰基氰化物苯腙或进行缓冲,小的NaCl脉冲在黑暗中也会导致短暂的亮氨酸流入这一观察结果表明,亮氨酸的转运通过与Na⁺同向转运而得到促进。

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