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通过单晶光谱学和衍射对蛋白质晶体中血红素配体中间态进行光还原和验证

Photoreduction and validation of haem-ligand intermediate states in protein crystals by single-crystal spectroscopy and diffraction.

作者信息

Kekilli Demet, Moreno-Chicano Tadeo, Chaplin Amanda K, Horrell Sam, Dworkowski Florian S N, Worrall Jonathan A R, Strange Richard W, Hough Michael A

机构信息

School of Biological Sciences, University of Essex, Wivenhoe Park, Colchester CO4 3SQ, England.

Swiss Light Source, Paul Scherrer Institut, 5232 Villigen-PSI, Switzerland.

出版信息

IUCrJ. 2017 Apr 10;4(Pt 3):263-270. doi: 10.1107/S2052252517002159. eCollection 2017 May 1.

Abstract

Powerful synergies are available from the combination of multiple methods to study proteins in the crystalline form. Spectroscopies which probe the same region of the crystal from which X-ray crystal structures are determined can give insights into redox, ligand and spin states to complement the information gained from the electron-density maps. The correct assignment of crystal structures to the correct protein redox and ligand states is essential to avoid the misinterpretation of structural data. This is a particular concern for haem proteins, which can occupy a wide range of redox states and are exquisitely sensitive to becoming reduced by solvated electrons generated from interactions of X-rays with water molecules in the crystal. Here, single-crystal spectroscopic fingerprinting has been applied to investigate the laser photoreduction of ferric haem in cytochrome '. Furthermore, X-ray-driven generation of haem intermediates in crystals of the dye-decolourizing-type peroxidase A (DtpA) from is described.

摘要

多种研究晶体形式蛋白质的方法相结合可产生强大的协同效应。能探测用于确定X射线晶体结构的晶体相同区域的光谱学,可以深入了解氧化还原、配体和自旋状态,以补充从电子密度图获得的信息。将晶体结构正确对应到正确的蛋白质氧化还原和配体状态对于避免错误解读结构数据至关重要。对于血红素蛋白来说,这是一个特别需要关注的问题,因为它们可以处于多种氧化还原状态,并且对被晶体中X射线与水分子相互作用产生的溶剂化电子还原极为敏感。在此,单晶光谱指纹图谱已被用于研究细胞色素中高铁血红素的激光光还原。此外,还描述了X射线驱动在来自的染料脱色型过氧化物酶A(DtpA)晶体中产生血红素中间体的过程。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3f27/5414400/289dfec3093a/m-04-00263-fig1.jpg

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