Characterization of dFMR1, a Drosophila melanogaster homolog of the fragile X mental retardation protein

被引：215

作者：

Wan, LL

Dockendorff, TC

Jongens, TA

Dreyfuss, G ^{[1
]}

机构：

[1] Univ Penn, Sch Med, Howard Hughes Med Inst, Philadelphia, PA 19104 USA

[2] Univ Penn, Sch Med, Dept Biochem & Biophys, Philadelphia, PA 19104 USA

[3] Univ Penn, Sch Med, Dept Genet, Philadelphia, PA 19104 USA

来源：

MOLECULAR AND CELLULAR BIOLOGY | 2000年 / 20卷 / 22期

关键词：

D O I：

10.1128/MCB.20.22.8536-8547.2000

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：

Fragile X syndrome is the most common inherited form of mental retardation. It is caused by loss of FMR1 gene activity due to either lack of expression or expression of a mutant form of the protein. In mammals, FMR1 is a member of a small protein family that consists of FMR1, FXR1, and FXR2. All three members bind RNA and contain sequence motifs that are commonly found in RNA-binding proteins, including two KH domains and an RGG box. The FMR1/PXR proteins also contain a 60S ribosomal subunit interaction domain and a protein-protein interaction domain which mediates homomer and heteromer formation with each family member. Nevertheless, the specific molecular functions of FMR1/FXR proteins are unknown. Here we report the cloning and characterization of a Drosophila melanogaster homolog of the mammalian PMR1/PXR gene family. This first invertebrate homolog, termed dfmr1, has a high degree of amino acid sequence identity/similarity with the defined functional domains of the FMR1/FXR proteins. The dfmr1 product binds RNA and is similar in subcellular localization and embryonic expression pattern to the mammalian FMR1/FXR proteins. Overexpression of dfmr1 driven by the UAS-GAL4 system leads to apoptotic cell loss in all adult Drosophila tissues examined. This phenotype is dependent on the activity of the KH domains. The ability to induce a dominant phenotype by overexpressing dfmr1 opens the possibility of using genetic approaches in Drosophila to identify the pathways in which the FMR1/FXR proteins function.

引用

页码：8536 / 8547

页数：12

共 74 条

[1] NUCLEUS BASALIS MAGNOCELLULARIS AND HIPPOCAMPUS ARE THE MAJOR SITES OF FMR-1 EXPRESSION IN THE HUMAN FETAL BRAIN
ABITBOL, M
MENINI, C
DELEZOIDE, AL
RHYNER, T
VEKEMANS, M
MALLET, J
[J]. NATURE GENETICS, 1993, 4 (02) : 147 - 153
[2] ABRAMS JM, 1993, DEVELOPMENT, V117, P29
[3] Expression of FMR1, FXR1, and FXR2 genes in human prenatal tissues
Agulhon, C
Blanchet, P
Kobetz, A
Marchant, D
Faucon, N
Sarda, P
Moraine, C
Sittler, A
Biancalana, V
Malafosse, A
Abitbol, M
[J]. JOURNAL OF NEUROPATHOLOGY AND EXPERIMENTAL NEUROLOGY, 1999, 58 (08) : 867 - 880
[4] FMR1 PROTEIN - CONSERVED RNP FAMILY DOMAINS AND SELECTIVE RNA-BINDING
ASHLEY, CT
WILKINSON, KD
REINES, D
WARREN, ST
[J]. SCIENCE, 1993, 262 (5133) : 563 - 566
[5] ENHANCED FMR-1 EXPRESSION IN TESTIS
BACHNER, D
STEINBACH, P
WOHRLE, D
JUST, W
VOGEL, W
HAMEISTER, H
MANCA, A
POUSTKA, A
[J]. NATURE GENETICS, 1993, 4 (02) : 115 - 116
[6] MOLECULAR CHARACTERIZATION AND EXPRESSION OF SEVENLESS, A GENE INVOLVED NEURONAL PATTERN-FORMATION IN THE DROSOPHILA EYE
BANERJEE, U
RENFRANZ, PJ
POLLOCK, JA
BENZER, S
[J]. CELL, 1987, 49 (02) : 281 - 291
[7] PHYSICAL MAPPING ACROSS THE FRAGILE-X - HYPERMETHYLATION AND CLINICAL EXPRESSION OF THE FRAGILE-X SYNDROME
BELL, MV
HIRST, MC
NAKAHORI, Y
MACKINNON, RN
ROCHE, A
FLINT, TJ
JACOBS, PA
TOMMERUP, N
TRANEBJAERG, L
FROSTERISKENIUS, U
KERR, B
TURNER, G
LINDENBAUM, RH
WINTER, R
PEMBREY, M
THIBODEAU, S
DAVIES, KE
[J]. CELL, 1991, 64 (04) : 861 - 866
[8] REGULATION OF THE COMPLEX PATTERN OF SEVENLESS EXPRESSION IN THE DEVELOPING DROSOPHILA EYE
BOWTELL, DDL
KIMMEL, BE
SIMON, MA
RUBIN, GM
[J]. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1989, 86 (16) : 6245 - 6249
[9] BRAND AH, 1993, DEVELOPMENT, V118, P401
[10] CONSERVED STRUCTURES AND DIVERSITY OF FUNCTIONS OF RNA-BINDING PROTEINS
BURD, CG
DREYFUSS, G
[J]. SCIENCE, 1994, 265 (5172) : 615 - 621

← 1 2 3 4 5 6 7 8 →