TOPOGRAPHY OF THE LEYDIG-CELL MITOCHONDRIAL PERIPHERAL-TYPE BENZODIAZEPINE RECEPTOR

被引：76

作者：

PAPADOPOULOS, V ^{[1
]}

BOUJRAD, N ^{[1
]}

IKONOMOVIC, MD ^{[1
]}

FERRARA, P ^{[1
]}

VIDIC, B ^{[1
]}

机构：

[1] SANOFI ELF BIORECH,LABEGE INNOPOLE,BIOCHIM PROT LAB,F-31676 LABEGE,FRANCE

来源：

MOLECULAR AND CELLULAR ENDOCRINOLOGY | 1994年 / 104卷 / 01期

关键词：

STEROIDOGENESIS; ATOMIC FORCE MICROSCOPY; CHANNEL; RECEPTORS; IMMUNOGOLD;

D O I：

10.1016/0303-7207(94)90061-2

中图分类号：

Q2 [细胞生物学];

学科分类号：

071009 ; 090102 ;

摘要：

Native MA-10 mouse Leydig tumor cell mitochondrial preparations were examined by transmission electron (TEM) and atomic force (AFM) microscopic procedures in order to investigate the topography and organization of the peripheral-type benzodiazepine receptor (PBR). Mitochondria were immunolabeled with an anti-PBR antiserum coupled to gold-labeled secondary antibodies. Results obtained indicate that the 18 000 MW PBR protein is organized in clusters of 4-6 molecules. Moreover, on many occasions, the interrelationship among the PBR molecules was found to favor the formation of a single pore. Taking into account recent observations that the 18 000 MW PBR protein is functionally associated with the pore forming 34 000 MW voltage-dependent anion channel (VDAC) these results suggest that (i) the mitochondrial PBR complex could function as a pore, thus allowing the translocation of cholesterol and other molecules to the inner mitochondrial membrane, and (ii) the native receptor is a multimeric complex of an approximate 140 000 MW composed on an average of five 18 000 PBR subunits, one 34 000 VDAC subunit, and associated lipids.

引用

页码：R5 / R9

页数：5

共 25 条

[1]

AMSTERDAM A, 1991, ENDOCRINOLOGY, V128, P503

[2] CHARACTERIZATION OF SEVERAL CLONAL LINES OF CULTURED LEYDIG TUMOR-CELLS - GONADOTROPIN RECEPTORS AND STEROIDOGENIC RESPONSES [J].

ASCOLI, M .

ENDOCRINOLOGY, 1981, 108 (01) :88-95

[3] A 3D MODEL OF THE PERIPHERAL BENZODIAZEPINE RECEPTOR AND ITS IMPLICATION IN INTRA MITOCHONDRIAL CHOLESTEROL TRANSPORT [J].

BERNASSAU, JM ;

REVERSAT, JL ;

FERRARA, P ;

CAPUT, D ;

LEFUR, G .

JOURNAL OF MOLECULAR GRAPHICS, 1993, 11 (04) :236-244

[4]

BINNIG GK, 1984, SURF SCI, V144, P321, DOI 10.1016/0039-6028(84)90104-3

[5] DIAZEPAM-BINDING INHIBITOR (DBI)-PROCESSING PRODUCTS, ACTING AT THE MITOCHONDRIAL DBI RECEPTOR, MEDIATE ADRENOCORTICOTROPIC HORMONE-INDUCED STEROIDOGENESIS IN RAT ADRENAL-GLAND [J].

CAVALLARO, S ;

KORNEYEV, A ;

GUIDOTTI, A ;

COSTA, E .

PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1992, 89 (22) :10598-10602

[6]

DEPINTO V, 1989, EUR J BIOCHEM, V183, P179

[7] DIHYDROPYRIDINE AND PERIPHERAL TYPE BENZODIAZEPINE BINDING-SITES - SUBCELLULAR-DISTRIBUTION AND MOLECULAR-SIZE DETERMINATION [J].

DOBLE, A ;

BENAVIDES, J ;

FERRIS, O ;

BERTRAND, P ;

MENAGER, J ;

VAUCHER, N ;

BURGEVIN, MC ;

UZAN, A ;

GUEREMY, C ;

LEFUR, G .

EUROPEAN JOURNAL OF PHARMACOLOGY, 1985, 119 (03) :153-167

[8]

GARNIER M, 1994, MOL PHARMACOL, V45, P201

[9] DIAZEPAM BINDING INHIBITOR IS A PARACRINE AUTOCRINE REGULATOR OF LEYDIG-CELL PROLIFERATION AND STEROIDOGENESIS - ACTION VIA PERIPHERAL-TYPE BENZODIAZEPINE RECEPTOR AND INDEPENDENT MECHANISMS [J].

GARNIER, M ;

BOUJRAD, N ;

OKE, BO ;

BROWN, AS ;

RIOND, J ;

FERRARA, P ;

SHOYAB, M ;

SUAREZQUIAN, CA ;

PAPADOPOULOS, V .

ENDOCRINOLOGY, 1993, 132 (01) :444-458

[10] SILVER FILMS CONDENSED AT 300-K AND 90-K - SCANNING TUNNELING MICROSCOPY OF THEIR SURFACE-TOPOGRAPHY [J].

GIMZEWSKI, JK ;

HUMBERT, A ;

BEDNORZ, JG ;

REIHL, B .

PHYSICAL REVIEW LETTERS, 1985, 55 (09) :951-954

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