学术探索
学术期刊
新闻热点
数据分析
智能评审

A genome-wide search for human non-insulin dependent (type 2) diabetes genes reveals a major susceptibility locus on chromosome 2

被引:485
作者
Hanis, CL
Boerwinkle, E
Chakraborty, R
Ellsworth, DL
Concannon, P
Stirling, B
Morrison, VA
Wapelhorst, B
Spielman, RS
GogolinEwens, KJ
Shephard, JM
Williams, SR
Risch, N
Hinds, D
Iwasaki, N
Ogata, M
Omori, Y
Petzold, C
Rietzsch, H
Schroder, HE
Schulze, J
Cox, NJ
Menzel, S
Boriraj, VV
Chen, X
Lim, LR
Lindner, T
Mereu, LE
Wang, YQ
Xiang, K
Yamagata, K
Yang, Y
Bell, GI
机构
[1] VIRGINIA MASON RES CTR,SEATTLE,WA 98101
[2] UNIV WASHINGTON,DEPT IMMUNOL,SEATTLE,WA 98195
[3] UNIV PENN,SCH MED,DEPT GENET,PHILADELPHIA,PA 19104
[4] STANFORD UNIV,DEPT GENET,STANFORD,CA 94305
[5] TOKYO WOMENS MED COLL,CTR DIABET,TOKYO 162,JAPAN
[6] TECH UNIV DRESDEN,UNIV CLIN CARL GUSTAV CARUS,DEPT INTERNAL MED 3,O-8027 DRESDEN,GERMANY
[7] UNIV CHICAGO,HOWARD HUGHES MED INST,CHICAGO,IL 60637
[8] UNIV CHICAGO,DEPT BIOCHEM & MOLEC BIOL,CHICAGO,IL 60637
[9] UNIV CHICAGO,DEPT MED,CHICAGO,IL 60637
来源
NATURE GENETICS | 1996年 / 13卷 / 02期
关键词
D O I
10.1038/ng0696-161
中图分类号
Q3 [遗传学];
学科分类号
071007 ; 090102 ;
摘要
Non-insulin-dependent (type 2) diabetes mellitus (NIDDM) is a common disorder of middle-aged individuals characterized by high blood glucose levels which, if untreated, can cause serious medical complications and lead to early death. Genetic factor splay an important role in determining susceptibility to this disorder. However, the number of genes involved, their chromosomal location and the magnitude of their effect on NIDDM susceptibility are unknown. We have screened the human genome for susceptibility genes for NIDDM using non- and quasi-parametric linkage analysis methods in a group of Mexican American affected sib pairs. One marker, D2S125, showed significant evidence of linkage to NIDDM and appears to be a major factor affecting the development of diabetes mellitus in Mexican Americans. We propose that this locus be designated NIDDM1.
引用
收藏
页码:161 / 166
页数:14
相关论文
共 44 条
[1]   MATERNALLY TRANSMITTED DIABETES AND DEAFNESS ASSOCIATED WITH A 10.4 KB MITOCHONDRIAL-DNA DELETION [J].
BALLINGER, SW ;
SHOFFNER, JM ;
HEDAYA, EV ;
TROUNCE, I ;
POLAK, MA ;
KOONTZ, DA ;
WALLACE, DC .
NATURE GENETICS, 1992, 1 (01) :11-15
[2]  
BISHOP DT, 1990, AM J HUM GENET, V46, P254
[3]   ALTERED INSULIN SECRETORY RESPONSES TO GLUCOSE IN SUBJECTS WITH A MUTATION IN THE MODY1 GENE ON CHROMOSOME-20 [J].
BYRNE, MM ;
STURIS, J ;
FAJANS, SS ;
ORTIZ, FJ ;
STOLTZ, A ;
STOFFEL, M ;
SMITH, MJ ;
BELL, GI ;
HALTER, JB ;
POLONSKY, KS .
DIABETES, 1995, 44 (06) :699-704
[4]   GENETIC-VARIATION IN THE BETA(3)-ADRENERGIC RECEPTOR AND AN INCREASED CAPACITY TO GAIN WEIGHT IN PATIENTS WITH MORBID-OBESITY [J].
CLEMENT, K ;
VAISSE, C ;
MANNING, BS ;
BASDEVANT, A ;
GUYGRAND, B ;
RUIZ, J ;
SILVER, KD ;
SHULDINER, AR ;
FROGUEL, P ;
STROSBERG, AD .
NEW ENGLAND JOURNAL OF MEDICINE, 1995, 333 (06) :352-354
[5]  
CURTIS D, 1995, AM J HUM GENET, V57, P703
[6]   A GENOME-WIDE SEARCH FOR HUMAN TYPE-1 DIABETES SUSCEPTIBILITY GENES [J].
DAVIES, JL ;
KAWAGUCHI, Y ;
BENNETT, ST ;
COPEMAN, JB ;
CORDELL, HJ ;
PRITCHARD, LE ;
REED, PW ;
GOUGH, SCL ;
JENKINS, SC ;
PALMER, SM ;
BALFOUR, KM ;
ROWE, BR ;
FARRALL, M ;
BARNETT, AH ;
BAIN, SC ;
TODD, JA .
NATURE, 1994, 371 (6493) :130-136
[7]   PATHOGENESIS OF NIDDM - A BALANCED OVERVIEW [J].
DEFRONZO, RA ;
BONADONNA, RC ;
FERRANNINI, E .
DIABETES CARE, 1992, 15 (03) :318-368
[8]   A comprehensive genetic map of the human genome based on 5,264 microsatellites [J].
Dib, C ;
Faure, S ;
Fizames, C ;
Samson, D ;
Drouot, N ;
Vignal, A ;
Millasseau, P ;
Marc, S ;
Hazan, J ;
Seboun, E ;
Lathrop, M ;
Gyapay, G ;
Morissette, J ;
Weissenbach, J .
NATURE, 1996, 380 (6570) :152-154
[9]   MATURITY-ONSET DIABETES OF THE YOUNG (MODY) [J].
FAJANS, SS .
DIABETES-METABOLISM REVIEWS, 1989, 5 (07) :579-606
[10]   THE GDB(TM) HUMAN GENOME DATA-BASE ANNO 1994 [J].
FASMAN, KH ;
CUTICCHIA, AJ ;
KINGSBURY, DT .
NUCLEIC ACIDS RESEARCH, 1994, 22 (17) :3462-3469
12345