CYTOCHROME-C-OXIDASE - STRUCTURE, FUNCTION, AND MEMBRANE TOPOLOGY OF THE POLYPEPTIDE SUBUNITS

被引：77

作者：

COOPER, CE

NICHOLLS, P

FREEDMAN, JA

机构：

[1] BROCK UNIV, DEPT BIOL SCI, ST CATHARINES L2S 3A1, ONTARIO, CANADA

[2] SYRACUSE RES CORP, SYRACUSE, NY 13210 USA

来源：

BIOCHEMISTRY AND CELL BIOLOGY | 1991年 / 69卷 / 09期

关键词：

CYTOCHROME OXIDASE; POLYPEPTIDE SUBUNITS; ANTIBODIES; MEMBRANE PROTEIN; ORIENTATION;

D O I：

10.1139/o91-089

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：

Mitochondrial cytochrome c oxidase and its bacterial homologs catalyze electron transfer and proton translocation reactions across membranes. The eukaryotic enzyme complex consists of a large number of polypeptide subunits. Three of the subunits (I, II, and III) are mitochondrially encoded while the remaining 6 (yeast) to 10 (bovine) are nuclear-encoded. Antibody and chemical-labelling experiments suggest that subunits I-111 and most (but not all) of the nuclear-encoded subunits span the inner mitochondrial membrane. Subunits I and II are the catalytic core of the enzyme. Subunit I contains haem a, haem a3 and Cu(B), while subunit II contains Cu(A) and the cytochrome c binding site. Subunit III and most of the nuclear subunits are essential for the assembly of a functional catalytic enzyme. Some nuclear subunits are present as isozymes, although little functional difference has yet been detected between enzyme complexes composed of different isozymes. Therefore, any additional role attributed to the nuclear-encoded subunits beyond that of enzyme assembly must be tentative. We suggest that enough evidence exists to support the idea that modification of the larger nuclear subunits (IV, V, and possibly VI) can affect enzyme turnover in vitro. Whether this is a physiological control mechanism remains to be seen.

引用

页码：586 / 607

页数：22

共 284 条

[91] THE MECHANISM OF ANTIBODY INHIBITION OF PROTON PUMPING BY CYTOCHROME-OXIDASE VESICLES [J].

FREEDMAN, JA ;

BRATCHER, RL ;

CHAN, SHP .

BIOCHEMICAL AND BIOPHYSICAL RESEARCH COMMUNICATIONS, 1984, 120 (01) :52-58

[92] EFFECTS OF SUBUNIT-V ANTIBODIES ON THE TOPOLOGY OF THE SUBUNIT AND THE ACTIVITY OF BEEF-HEART CYTOCHROME-C OXIDASE [J].

FREEDMAN, JA ;

LEECE, B ;

COOPER, CE ;

NICHOLLS, P ;

CHAN, SHP .

BIOCHEMISTRY AND CELL BIOLOGY, 1988, 66 (11) :1210-1217

[93] STRUCTURE OF THE CYTOCHROME-C OXIDASE DIMER ELECTRON-MICROSCOPY OF TWO-DIMENSIONAL CRYSTALS [J].

FREY, TG ;

COSTELLO, MJ ;

KARLSSON, B ;

HASELGROVE, JC ;

LEIGH, JS .

JOURNAL OF MOLECULAR BIOLOGY, 1982, 162 (01) :113-130

[94] ENERGIZED TRANSPORT OF CATIONS BY CYTOCHROME-OXIDASE [J].

FRY, M ;

GREEN, DE .

BIOCHEMICAL AND BIOPHYSICAL RESEARCH COMMUNICATIONS, 1980, 95 (04) :1529-1535

[95] 2 KM VALUES FOR CYTOCHROME-C OF ALPHA-ALPHA-3-TYPE 2-SUBUNIT CYTOCHROME-C OXIDASE FROM NITROBACTER-AGILIS [J].

FUKUMORI, Y ;

YAMANAKA, T .

FEBS LETTERS, 1984, 170 (02) :301-304

[96] STRUCTURE OF CYTOCHROME-C OXIDASE IN DEOXYCHOLATE-DERIVED 2-DIMENSIONAL CRYSTALS [J].

FULLER, SD ;

CAPALDI, RA ;

HENDERSON, R .

JOURNAL OF MOLECULAR BIOLOGY, 1979, 134 (02) :305-327

[97] COVALENT COMPLEX BETWEEN YEAST CYTOCHROME-C AND BEEF-HEART CYTOCHROME-C OXIDASE WHICH IS ACTIVE IN ELECTRON-TRANSFER [J].

FULLER, SD ;

DARLEYUSMAR, VM ;

CAPALDI, RA .

BIOCHEMISTRY, 1981, 20 (24) :7046-7053

[98] PREPARATION OF TWO-DIMENSIONAL ARRAYS FROM PURIFIED BEEF-HEART CYTOCHROME-C OXIDASE [J].

FULLER, SD ;

CAPALDI, RA ;

HENDERSON, R .

BIOCHEMISTRY, 1982, 21 (10) :2525-2529

[99] 2 MONOCLONAL-ANTIBODY LINES DIRECTED AGAINST SUBUNIT-IV OF CYTOCHROME-OXIDASE - A STUDY OF OPPOSITE EFFECTS [J].

GAI, WZ ;

SUN, SM ;

DING, YZ ;

FREEDMAN, JA ;

CHAN, SHP .

ARCHIVES OF BIOCHEMISTRY AND BIOPHYSICS, 1988, 266 (02) :628-638

[100] CYTOCHROME-OXIDASE FROM THERMOPHILIC BACTERIUM PS3 CONTAINS A 4TH PROTEIN SUBUNIT [J].

GAI, WZ ;

SUN, SM ;

SONE, N ;

CHAN, SHP .

BIOCHEMICAL AND BIOPHYSICAL RESEARCH COMMUNICATIONS, 1990, 169 (02) :414-421

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