Ras, Rap, and Rac small GTP-binding proteins are targets for Clostridium sordellii lethal toxin glucosylation

被引：175

作者：

Popoff, MR

ChavesOlarte, E

Lemichez, E

vonEichelStreiber, C

Thelestam, M

Chardin, P

Cussac, D

Antonny, B

Chavrier, P

Flatau, G

Giry, M

deGunzburg, J

Boquet, P

机构：

[1] INST PASTEUR, UNITE TOXINES MICROBIENNES, F-75724 PARIS 15, FRANCE

[2] KAROLINSKA INST, MICROBIOL & TUMORBIOL CTR, S-17177 STOCKHOLM, SWEDEN

[3] CNRS, INST PHARMACOL MOLEC & CELLULAIRE, F-06560 VALBONNE, FRANCE

[4] FAC MED NICE, INSERM, U452, F-06107 NICE 2, FRANCE

[5] CTR IMMUNOL MARSEILLES LUMINY, F-13286 MARSEILLE, FRANCE

[6] UNIV MAINZ, INST MED MIKROBIOL & HYG VERFUGUNGSGEBAUDE FORSCH, D-55101 MAINZ, GERMANY

[7] INSERM, U248, F-75010 PARIS, FRANCE

来源：

JOURNAL OF BIOLOGICAL CHEMISTRY | 1996年 / 271卷 / 17期

关键词：

D O I：

10.1074/jbc.271.17.10217

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：

Lethal toxin (LT) from Clostridium sordellii is one of the high molecular mass clostridial cytotoxins. On cultured cells, it causes a rounding of cell bodies and a disruption of actin stress fibers. We demonstrate that LT is a glucosyltransferase that uses UDP-Glc as a cofactor to covalently modify 21-kDa proteins both in vitro and in vivo. LT glucosylates Ras, Rap, and Rac. In Ras, threonine at position 35 was identified as the target amino acid glucosylated by LT. Other related members of the Ras GTPase superfamily, including RhoA, Cdc42, and Rab6, were not modified by LT. Incubation of serum-starved Swiss 3T3 cells with LT prevents the epidermal growth factor-induced phosphorylation of mitogen-activated protein kinases ERK1 and ERK2, indicating that the toxin blocks Ras function in vivo. We also demonstrate that LT acts inside the cell and that the glucosylation reaction is required to observe its dramatic effect on cell morphology. LT is thus a powerful tool to inhibit Ras function in vivo.

引用

页码：10217 / 10224

页数：8

共 29 条

[1] GTP HYDROLYSIS MECHANISMS IN RAS P21 AND IN THE RAS-GAP COMPLEX STUDIED BY FLUORESCENCE MEASUREMENTS ON TRYPTOPHAN MUTANTS
ANTONNY, B
CHARDIN, P
ROUX, M
CHABRE, M
[J]. BIOCHEMISTRY, 1991, 30 (34) : 8287 - 8295
[2] TOXINS RESPONSIBLE FOR LESIONS OF CLOSTRIDIUM SORDELLII GAS GANGRENE
ARSECULERATNE, SN
PANABOKKE, RG
WIJESUNDERA, S
[J]. JOURNAL OF MEDICAL MICROBIOLOGY, 1969, 2 (01) : 37 - +
[3] RAS GENES
BARBACID, M
[J]. ANNUAL REVIEW OF BIOCHEMISTRY, 1987, 56 : 779 - 827
[4] A COMPARATIVE BIOCHEMICAL, PHARMACOLOGICAL AND IMMUNOLOGICAL STUDY OF CLOSTRIDIUM-NOVYI ALPHA-TOXIN, CLOSTRIDIUM-DIFFICILE TOXIN-B AND C-SORDELLII LETHAL TOXIN
BETTE, P
OKSCHE, A
MAULER, F
VONEICHELSTREIBER, C
POPOFF, MR
HABERMANN, E
[J]. TOXICON, 1991, 29 (07) : 877 - 887
[5] FIMBRIN IS A CYTOSKELETAL PROTEIN THAT CROSSLINKS F-ACTIN INVITRO
BRETSCHER, A
[J]. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA-BIOLOGICAL SCIENCES, 1981, 78 (11): : 6849 - 6853
[6] UDP-glucose deficiency in a mutant cell line protects against glucosyltransferase toxins from Clostridium difficile and Clostridium sordellii
ChavesOlarte, E
Florin, I
Boquet, P
Popoff, M
vonEichelStreiber, C
Thelestam, M
[J]. JOURNAL OF BIOLOGICAL CHEMISTRY, 1996, 271 (12) : 6925 - 6932
[7] EXTRACELLULAR SIGNAL-REGULATED KINASES - ERKS IN PROGRESS
COBB, MH
BOULTON, TG
ROBBINS, DJ
[J]. CELL REGULATION, 1991, 2 (12): : 965 - 978
[8] INVOLVEMENT OF P21RAS IN ACTIVATION OF EXTRACELLULAR SIGNAL-REGULATED KINASE-2
DEVRIESSMITS, AMM
BURGERING, BMT
LEEVERS, SJ
MARSHALL, CJ
BOS, JL
[J]. NATURE, 1992, 357 (6379) : 602 - 604
[9] ISOLATION OF A FIBROBLAST MUTANT RESISTANT TO CLOSTRIDIUM-DIFFICILE TOXIN-A AND TOXIN-B
FLORIN, I
[J]. MICROBIAL PATHOGENESIS, 1991, 11 (05) : 337 - 346
[10] TRANSIENT EXPRESSION OF RHOA, RHOB, AND RHOC GTPASES IN HELA-CELLS POTENTIATES RESISTANCE TO CLOSTRIDIUM-DIFFICILE TOXIN-A AND TOXIN-B BUT NOT TO CLOSTRIDIUM-SORDELLII LETHAL TOXIN
GIRY, M
POPOFF, MR
VONEICHELSTREIBER, C
BOQUET, P
[J]. INFECTION AND IMMUNITY, 1995, 63 (10) : 4063 - 4071

← 1 2 3 →