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测定羟氨及其 N-甲基衍生物对光系统 II 放氧复合物的抑制作用。

Characterization of inhibitory effects of NH2OH and its N-methyl derivatives on the O 2-evolving complex of Photosystem II.

机构信息

Department of Biology, University of Michigan, 48109-1048, Ann Arbor, MI, USA.

出版信息

Photosynth Res. 1993 Jan;38(3):449-53. doi: 10.1007/BF00046773.

Abstract

Inorganic cofactors (Mn, Ca(2+) and Cl(-)) are essential for oxidation of H2O to O2 by Photosystem II. The Mn reductants NH2OH and its N-methyl derivatives have been employed as probes to further examine the interactions between these species and Mn at the active site of H2O oxidation. Results of these studies show that the size of a hydroxylamine derivative regulates its ability to inactivate O2 evolution activity, and that this size-dependent inhibition behavior arises from the protein structure of Photosystem II. A set of anions (Cl(-), F(-) and SO4 (2-)) is able to slow NH2OH and CH3NHOH inactivation of intact Photosystem II membranes by exerting a stabilizing influence on the extrinsic 23 and 17 kDa polypeptides. In contrast to this non-specific anion effect, only Cl(-) is capable of attenuating CH3NHOH and (CH3)2NOH inhibition in salt-washed preparations lacking the 23 and 17 kDa polypeptides. However, Cl(-) fails to protect against NH2OH inhibition in salt-washed membranes. These results indicate that the attack by NH2OH and its N-methyl derivatives on Mn occurs at different sites in the O2-evolving complex. The small reductant NH2OH acts at a Cl(-)-insensitive site whereas the inhibitions by CH3NHOH and (CH3)2NOH involve a site that is Cl(-) sensitive. These findings are consistent with earlier studies showing that the size of primary amines controls the Cl(-) sensitivity of their binding to Mn in the O2-evolving complex.

摘要

无机辅助因子(Mn、Ca(2+) 和 Cl(-))对于光系统 II 将 H2O 氧化为 O2 是必需的。NH2OH 及其 N-甲基衍生物已被用作探针,以进一步研究这些物种与 Mn 在 H2O 氧化活性位点的相互作用。这些研究的结果表明,羟胺衍生物的大小调节其使 O2 释放活性失活的能力,并且这种尺寸依赖性抑制行为源自光系统 II 的蛋白质结构。一组阴离子(Cl(-)、F(-) 和 SO4 (2-))能够通过对外在的 23 和 17 kDa 多肽施加稳定影响来减缓 NH2OH 和 CH3NHOH 对完整光系统 II 膜的失活作用。与这种非特异性阴离子效应相反,只有 Cl(-)能够在缺乏 23 和 17 kDa 多肽的盐洗制剂中减弱 CH3NHOH 和 (CH3)2NOH 的抑制作用。然而,Cl(-) 不能防止盐洗膜中 NH2OH 的抑制作用。这些结果表明,NH2OH 和其 N-甲基衍生物对 Mn 的攻击发生在 O2 释放复合物的不同部位。小还原剂 NH2OH 作用于 Cl(-)不敏感部位,而 CH3NHOH 和 (CH3)2NOH 的抑制作用涉及 Cl(-)敏感部位。这些发现与早期研究一致,表明伯胺的大小控制其在 O2 释放复合物中与 Mn 结合的 Cl(-)敏感性。

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