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维生素K在蓝藻集胞藻6803光系统I中的功能作用。

Functional role of vitamin K in photosystem I of the cyanobacterium Synechocystis 6803.

作者信息

Biggins J, Mathis P

机构信息

Département de Biologie, Centre d'Etudes Nucléaires de Saclay, Gif-sur-Yvette, France.

出版信息

Biochemistry. 1988 Mar 8;27(5):1494-500. doi: 10.1021/bi00405a015.

DOI:10.1021/bi00405a015
PMID:3130097
Abstract

The function of vitamin K1 in the primary electron-transfer processes of photosystem I (PS I) was investigated in the cyanobacterium Synechocystis 6803. A preparation of purified PS I was found to contain two vitamin K1's per reaction center. One vitamin K1 was removed by extraction with hexane, and further extraction using hexane including 0.3% methanol resulted in a preparation devoid of vitamin K1. The hexane-extracted PS I was functional in the photoreduction of NADP+, but the PS I after extraction using hexane-methanol was totally inactive. Activity was restored by using exogenous vitamin K1 plus the hexane extract. Vitamin K3 would not substitute. The room temperature recombination kinetics of the PS I extracted with hexane were not significantly modified. However, following the removal of both vitamin K1's, the 20-ms recombination between P-700+ and P-430- was replaced by a dominant relaxation (t 1/2 = 30 ns) due to recombination of the primary biradical P-700+ A0- and a slower component originating from the P-700 triplet. This kinetic behavior was consistent with an interruption of forward electron transfer to the acceptor A1. Addition of either vitamin K1 or vitamin K3 to such preparations resulted in restoration of the slow kinetic phase (greater than 2 ms), indicating significant competition by the two exogenous quinones for electron transfer from A0-. In the case of vitamin K3, this change in the kinetics induced by vitamin K1, suggesting successful reconstitution of the acceptor site A1. These data support the hypothesis that acceptor A1 is vitamin K1 and is a component of the electron-transfer pathway for NADP+ reduction.

摘要

在集胞藻6803中研究了维生素K1在光系统I(PS I)初级电子转移过程中的作用。发现纯化的PS I制剂每个反应中心含有两个维生素K1。用己烷萃取可去除一个维生素K1,进一步用含0.3%甲醇的己烷萃取则得到不含维生素K1的制剂。己烷萃取的PS I在NADP+的光还原中具有功能,但用己烷 - 甲醇萃取后的PS I完全无活性。通过使用外源维生素K1加己烷提取物可恢复活性。维生素K3不能替代。己烷萃取的PS I在室温下的重组动力学没有明显改变。然而,去除两个维生素K1后,P - 700 +和P - 430 -之间20毫秒的重组被主要的弛豫(t1/2 = 30纳秒)所取代,这是由于初级双自由基P - 700 + A0 -的重组以及源于P - 700三重态的较慢成分。这种动力学行为与向受体A1的正向电子转移中断一致。向此类制剂中添加维生素K1或维生素K3都会导致慢动力学相(大于2毫秒)恢复,表明两种外源醌对从A0 -进行的电子转移存在显著竞争。在维生素K3的情况下,维生素K1诱导的这种动力学变化表明受体位点A1成功重构。这些数据支持了受体A1是维生素K1且是NADP+还原电子转移途径的一个组成部分的假设。

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