FARNESYL THIOTRIAZOLE, A POTENT NEUTROPHIL AGONIST AND STRUCTURALLY NOVEL ACTIVATOR OF PROTEIN-KINASE-C

被引：15

作者：

GILBERT, BA

LIM, YH

DING, JB

BADWEY, JA

RANDO, RR

机构：

[1] HARVARD UNIV,SCH MED,DEPT BIOL CHEM & MOLEC PHARMACOL,BOSTON,MA 02115

[2] BOSTON BIOMED RES INST,DEPT MUSCLE RES,BOSTON,MA 02114

来源：

BIOCHEMISTRY | 1995年 / 34卷 / 12期

关键词：

D O I：

10.1021/bi00012a007

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：

Farnesylcysteine derivatives can initiate or inhibit superoxide (O-2(-)) release in neutrophils. The mechanism by which one of these derivatives, farnesyl thiotriazole (FTT), initiates O-2(-) release in neutrophils is the subject of this paper. Treatment of guinea pig neutrophils with FTT results in the rapid release of O-2(-) by a route shown to be independent of the chemotactic peptide N-formyl-Met-Leu-Phe (fMLP) receptor. The signal transduction pathway utilized by the chemoattractant fMLP is generally accepted as the paradigm for receptor-mediated stimulation of O-2(-) production. Antagonists of fMLP had no effect on FTT-induced O-2(-) release, and pretreatment of neutrophils with fMLP had no effect on the ability of FTT to trigger further O-2(-) generation. In fact, FTT behaves like a typical protein kinase C (PKC) activator. It promotes phosphorylation of the 47-kDa subunit of the NADH oxidase complex (p47-phox) in neutrophils, and this phosphorylation is specifically blocked by 1-(5-isoquinolinylsulfonyl)-2-methylpiperazine (H-7), an antagonist of PKC. FTT is also shown to activate PKC in vitro in a specific and saturable fashion. FTT is approximately equipotent with (S)-diolein, a physiologically relevant activator of this kinase. FTT represents a new, and quite novel, structure for a PKC activator. PKC activators include diglycerides and the structurally diverse tumor promoters.

引用

页码：3916 / 3920

页数：5

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