THE MOLECULAR-BASIS OF SKELETAL-MUSCLE DIFFERENTIATION

被引：0

作者：

DIAS, P ^{[1
]}

DILLING, M ^{[1
]}

HOUGHTON, P ^{[1
]}

机构：

[1] ST JUDE CHILDRENS RES HOSP, DEPT MOLEC PHARMACOL, 332 N LAUDERDALE, MEMPHIS, TN 38101 USA

来源：

SEMINARS IN DIAGNOSTIC PATHOLOGY | 1994年 / 11卷 / 01期

关键词：

MUSCLE; MUSCLE DIFFERENTIATION; MYOGENESIS; MYOGENIC REGULATORY FACTORS; MUSCLE TRANSCRIPTION FACTORS; MYOD; MYF-5; MYOGENIN; MRF4; HERCULIN; MYF-6; BHLH; GROWTH FACTOR; ONCOGENES; RETINAL BLASTOMA; E2A; TARGETED MUTATION;

D O I：

暂无

中图分类号：

R446 [实验室诊断]; R-33 [实验医学、医学实验];

学科分类号：

1001 ;

摘要：

In recent years, significant advances have been made in understanding the molecular mechanisms involved in the regulation of skeletal-muscle differentiation. This review focuses on the role of the MyoD family of myogenic transcription factors that includes MyoD, myf-5, myogenin, and MRF4 (herculin or myf-6) in myogenesis. Members of this family share sequence homology for the basic-helix-loop-helix (bHLH) regulatory motif. The basic domain is required for DNA binding, whereas the HLH domain is required for dimerization. The bHLH motif confers both properties of transcriptional activation of muscle specific genes and inhibition of cell growth through collaboration with the E2A gene products (E12 and E47) and the retinoblastoma gene product (pRB). The functions of the MyoD family can be suppressed through inhibition of their expression or activity by various factors. These include peptide growth factors (FGF and TGF-beta), immediate early gene products (Fos, Jun and Myc), other oncogene products (Ras, Src), the Id protein, and innervation. The use of gene-knockout animal models has shown that there is some degree of functional redundancy in that inactivation of either MyoD or myf-5 has no effect on muscle development, whereas inactivation of both genes results in an absolute lack of muscle cells. In contrast, the inactivation of myogenin alone results in mice with gross deficiency of mature muscle. Copyright (C) 1994 by W.B. Saunders Company

引用

页码：3 / 4

页数：2

共 50 条

[41] MOLECULAR MECHANISMS OF SKELETAL-MUSCLE ADAPTATIONS TO EXERCISE
KARAS, RH
WILLIAMS, RS
TRENDS IN CARDIOVASCULAR MEDICINE, 1991, 1 (08) : 341 - 346
[42] VASCULAR SMOOTH-MUSCLE - A REVIEW OF THE MOLECULAR-BASIS OF CONTRACTILITY
HATHAWAY, DR
MARCH, KL
LASH, JA
ADAM, LP
WILENSKY, RL
CIRCULATION, 1991, 83 (02) : 382 - 390
[43] A MOLECULAR-BASIS OF CANCER
WEINBERG, RA
SCIENTIFIC AMERICAN, 1983, 249 (05) : 126 - +
[44] ON THE MOLECULAR-BASIS OF MEMORY
SCHIFFMANN, Y
BIOCHEMICAL SOCIETY TRANSACTIONS, 1989, 17 (06) : 1065 - 1068
[45] MOLECULAR-BASIS FOR SPECTRIN ISOFORMS IN HUMAN CARDIAC-MUSCLE
VYBIRAL, T
WALCH, ET
WINKELMANN, J
PORTER, GA
BLOCH, RJ
EPSTEIN, HF
CLINICAL RESEARCH, 1992, 40 (02): : A439 - A439
[46] MOLECULAR-BASIS OF THE PHENOTYPIC CHARACTERISTICS OF MAMMALIAN MUSCLE-FIBERS
PETTE, D
STARON, RS
CIBA FOUNDATION SYMPOSIA, 1988, 138 : 22 - 34
[47] THE MOLECULAR-BASIS OF RETINOBLASTOMAS
WEINBERG, RA
CIBA FOUNDATION SYMPOSIA, 1989, 142 : 99 - 105
[48] MOLECULAR-BASIS OF RADIORESISTANCE
COUCKE, PA
CROMPTON, NEA
EUROPEAN JOURNAL OF CANCER, 1995, 31A (05) : 844 - 846
[49] THE MOLECULAR-BASIS OF CANINE MUSCLE PHOSPHOFRUCTOKINASE DEFICIENCY IS A POINT MUTATION
SMITH, BF
STEDMAN, H
RAIPUROHIT, Y
WOLFE, JH
PATTERSON, DF
GIGER, U
AMERICAN JOURNAL OF HUMAN GENETICS, 1991, 49 (04) : 106 - 106
[50] MOLECULAR-BASIS OF COOPERATIVITY IN VERTEBRATE MUSCLE THIN-FILAMENTS
BRANDT, PW
DIAMOND, MS
GLUCK, B
KAWAI, M
SCHACHAT, F
CARLSBERG RESEARCH COMMUNICATIONS, 1984, 49 (02) : 155 - 167

← 1 2 3 4 5 →