PRELIMINARY CRYOCRYSTALLOGRAPHIC STUDY OF THE MITOCHONDRIAL CYTOCHROME BC(1) COMPLEX - IMPROVED CRYSTALLIZATION AND FLASH-COOLING OF A LARGE MEMBRANE-PROTEIN

被引：17

作者：

LEE, JW ^{[1
]}

CHAN, M ^{[1
]}

LAW, TV ^{[1
]}

KWON, HJ ^{[1
]}

JAP, BK ^{[1
]}

机构：

[1] UNIV CALIF BERKELEY,LAWRENCE BERKELEY LAB,DIV LIFE SCI,BERKELEY,CA 94720

来源：

JOURNAL OF MOLECULAR BIOLOGY | 1995年 / 252卷 / 01期

关键词：

CRYOCRYSTALLOGRAPHY; CYTOCHROME BC(1) COMPLEX; MEMBRANE PROTEIN; FLASH-COOLING; CRYSTALLIZATION;

D O I：

10.1006/jmbi.1994.0470

中图分类号：

Q5 [生物化学]; Q7 [分子生物学];

学科分类号：

071010 ; 081704 ;

摘要：

Ubiquinol-cytochrome c reductase is a crucial integral membrane protein in the mitochondrial respiratory cycle. Eleven subunits containing three cytochrome heme groups and a 2Fe-2S Rieske center make up this 240 kDa enzyme complex. Previously, many different crystal forms of the bc(1) complex have displayed diffraction to as far as 4.5 Angstrom. However, rapid degradation of the protein in the X-ray beam at room temperature has obstructed the collection of a full data set from a single crystal. As slight heterogeneities between crystals severely hampered merging of data from different crystals, we sought a method to stabilize the protein crystal in the X-ray beam in order to collect a full data set from one crystal sample. To this end, water soluble protein crystals are frequently flash-cooled to cryogenic temperatures; however, there is no report of cryocrystallography for membrane proteins. In this communication, we report on a successful experiment in which flash-cooled bc(1) membrane protein crystals have given rise to sustained diffraction over a 60 hour data collection period at a synchrotron source. Furthermore, we present an improved purification and crystallization protocol yielding crystals readily diffracting out to 3.3 Angstrom. These results should greatly aid in the future realization of the molecular structure of the bc(1) complex as well as other membrane proteins. (C) 1995 Academic Press Limited

引用

页码：15 / 19

页数：5

共 30 条

[1] COMPLETE SEQUENCE OF BOVINE MITOCHONDRIAL-DNA - CONSERVED FEATURES OF THE MAMMALIAN MITOCHONDRIAL GENOME [J].

ANDERSON, S ;

DEBRUIJN, MHL ;

COULSON, AR ;

EPERON, IC ;

SANGER, F ;

YOUNG, IG .

JOURNAL OF MOLECULAR BIOLOGY, 1982, 156 (04) :683-717

[2]

[Anonymous], P CCP4 STUD WEEK

[3] X-RAY-DIFFRACTION BY CRYSTALS OF BEEF-HEART UBIQUINOL - CYTOCHROME-C OXIDOREDUCTASE [J].

BERRY, EA ;

HUANG, LS ;

EARNEST, TN ;

JAP, BK .

JOURNAL OF MOLECULAR BIOLOGY, 1992, 224 (04) :1161-1166

[4] A NEW CRYSTAL FORM OF BOVINE HEART UBIQUINOL - CYTOCHROME-C OXIDOREDUCTASE - DETERMINATION OF SPACE GROUP AND UNIT-CELL PARAMETERS [J].

BERRY, EA ;

SHULMEISTER, VM ;

HUANG, LS ;

KIM, SH .

ACTA CRYSTALLOGRAPHICA SECTION D-BIOLOGICAL CRYSTALLOGRAPHY, 1995, 51 :235-239

[5]

BERRY EA, 1986, METHOD ENZYMOL, V126, P305

[6]

BERRY EA, 1990, J BIOL CHEM, V266, P9064

[7] ISOLATION AND AMINO-ACID-SEQUENCE OF THE 9.5 KDA PROTEIN OF BEEF-HEART UBIQUINOL - CYTOCHROME-C REDUCTASE [J].

BORCHART, U ;

MACHLEIDT, W ;

SCHAGGER, H ;

LINK, TA ;

VONJAGOW, G .

FEBS LETTERS, 1986, 200 (01) :81-86

[8] ISOLATION AND AMINO-ACID SEQUENCE OF THE 8 KDA DCCD-BINDING PROTEIN OF BEEF-HEART UBIQUINOL-CYTOCHROME C-REDUCTASE [J].

BORCHART, U ;

MACHLEIDT, W ;

SCHAGGER, H ;

LINK, TA ;

VONJAGOW, G .

FEBS LETTERS, 1985, 191 (01) :125-130

[9] BIOCHEMICAL AND MOLECULAR ASPECTS OF HUMAN MITOCHONDRIAL RESPIRATORY-CHAIN DISORDERS [J].

COOPER, JM ;

SCHAPIRA, AHV ;

HOLT, IJ ;

TOSCANO, A ;

HARDING, AE ;

MORGANHUGHES, JA ;

CLARK, JB .

BIOCHEMICAL SOCIETY TRANSACTIONS, 1990, 18 (04) :517-519

[10] CORE-I PROTEIN OF BOVINE UBIQUINOL CYTOCHROME-C REDUCTASE - AN ADDITIONAL MEMBER OF THE MITOCHONDRIAL-PROTEIN-PROCESSING FAMILY - CLONING OF BOVINE CORE-I AND CORE-II CDNAS AND PRIMARY STRUCTURE OF THE PROTEINS [J].

GENCIC, S ;

SCHAGGER, H ;

VONJAGOW, G .

EUROPEAN JOURNAL OF BIOCHEMISTRY, 1991, 199 (01) :123-131

← 1 2 3 →