DIVERSITY OF THE PROTEIN-KINASE-C GENE FAMILY - IMPLICATIONS FOR CARDIOVASCULAR-DISEASE

被引:18
作者
HANINGTON, EO [1 ]
WARE, JA [1 ]
机构
[1] HARVARD UNIV,BETH ISRAEL HOSP,SCH MED,DEPT MED,HARVARD THORNDIKE LABS,BOSTON,MA 02115
来源
TRENDS IN CARDIOVASCULAR MEDICINE | 1995年 / 5卷 / 05期
关键词
D O I
10.1016/1050-1738(95)00058-H
中图分类号
R5 [内科学];
学科分类号
1002 ; 100201 ;
摘要
All eukaryotic cells are capable of responding to a changing intracellular environment and to extracellular stimuli. These functional responses ave highly regulated by diverse means; one of the most common mechanisms of regulation requires the covalent phosphorylation of intracellular proteins, which, when phosphorylated, mediate many functional events. The general class of enzymes that catalyzes the phosphorylation of effectors (substrates), the protein kinases, may be divided into two broad categories, depending on whether they phosphorylate serine and threonine residues or tyrosine residues. Evidence has accumulated that implicates abnormal activation of protein kinase C (PKC), which is one family of serine-threonine protein kinases, in cells and tissues from patients or models of cardiovascular disease. In this review, lye present the molecular and biochemical basis for the diversity of the PKC family, and briefly summarize the evidence that PKC is implicated in cardiovascular pathology and the potential therapeutic implications and approaches.
引用
收藏
页码:193 / 199
页数:7
相关论文
共 50 条
[41]   A DYNAMIC FAMILY APPROACH FOR THE PREVENTION OF CARDIOVASCULAR-DISEASE [J].
NICKLAS, TA ;
JOHNSON, CC ;
ARBEIT, ML ;
FRANKLIN, FA ;
BERENSON, GS .
JOURNAL OF THE AMERICAN DIETETIC ASSOCIATION, 1988, 88 (11) :1438-1440
[42]   THE FAMILY PHYSICIANS ROLE IN CARDIOVASCULAR-DISEASE PREVENTION [J].
MCBRIDE, PE ;
RYAN, GG .
AMERICAN FAMILY PHYSICIAN, 1992, 45 (03) :1042-1044
[43]   DIET AND CARDIOVASCULAR-DISEASE - IMPLICATIONS FOR BRITISH AGRICULTURE [J].
WHEELOCK, JV ;
FALLOWS, SJ .
RESEARCH AND DEVELOPMENT IN AGRICULTURE, 1985, 2 (03) :147-159
[44]   ALCOHOL, HYPERTENSION AND CARDIOVASCULAR-DISEASE - IMPLICATIONS FOR MANAGEMENT [J].
BEILIN, LJ ;
PUDDEY, IB .
CLINICAL AND EXPERIMENTAL HYPERTENSION, 1993, 15 (06) :1157-1170
[45]   PARTIAL CHARACTERIZATION OF PROTEIN-KINASE-C AND INHIBITOR ACTIVITY OF PROTEIN-KINASE-C IN RABBIT PERITONEAL NEUTROPHILS [J].
HUANG, CK ;
OSHANA, SC .
JOURNAL OF LEUKOCYTE BIOLOGY, 1986, 39 (06) :671-678
[46]   PROTEIN-KINASE-C IN HUMAN PHEOCHROMOCYTOMA [J].
KODA, Y ;
UEZONO, Y ;
KOBAYASHI, H ;
IZUMI, F ;
INATOMI, H ;
YAMADA, Y ;
OKAMURA, T .
NEUROSCIENCE LETTERS, 1991, 127 (01) :31-33
[47]   THE ACTIVATION OF CYCLE PROTEIN-KINASE-C [J].
WOLF, M ;
SAHYOUN, N .
BIOMEDICINE & PHARMACOTHERAPY, 1986, 40 (09) :362-362
[48]   PHOSPHORYLATION OF RHODOPSIN BY PROTEIN-KINASE-C [J].
NEWTON, AC ;
WILLIAMS, DS .
FASEB JOURNAL, 1992, 6 (01) :A9-A9
[49]   PHOSPHORYLATION OF ACTIN BY PROTEIN-KINASE-C [J].
OHTA, Y ;
AKIYAMA, T ;
NISHIDA, E ;
SAKAI, H .
CELL STRUCTURE AND FUNCTION, 1986, 11 (04) :441-441
[50]   NUCLEAR SUBSTRATES OF PROTEIN-KINASE-C [J].
BECKMANN, R ;
BUCHNER, K ;
JUNGBLUT, PR ;
ECKERSKORN, C ;
WEISE, C ;
HILBERT, R ;
HUCHO, F .
EUROPEAN JOURNAL OF BIOCHEMISTRY, 1992, 210 (01) :45-51
12345