Novel mutations and a mutational hotspot in the MODY3 gene

被引：88

作者：

Glucksmann, MA

Lehto, M

Tayber, O

Scotti, S

Berkemeier, L

Pulido, JC

Wu, Y

Nir, WJ

Fang, L

Markel, P

Munnelly, KD

Goranson, J

Orho, M

Young, BM

Whitacre, JL

McMenimen, C

Wantman, M

Tuomi, T

Warram, J

Forsblom, CM

Carlsson, M

Rosenzweig, J

Kennedy, G

Duyk, GM

Krolewski, AS

Groop, LC

Thomas, JD

机构：

[1] MILLENNIUM PHARMACEUT INC,CAMBRIDGE,MA 02139

[2] LUND UNIV,MALMO UNIV HOSP,WALLENBERG LAB,DEPT ENDOCRINOL,MALMO,SWEDEN

[3] HARVARD UNIV,SCH MED,JOSLIN DIABET CTR,SECT EPIDEMIOL & GENET,BOSTON,MA 02115

[4] UNIV HELSINKI HOSP,DIV INTERNAL MED,HELSINKI,FINLAND

[5] CHIRON CORP,EMERYVILLE,CA 94608

来源：

DIABETES | 1997年 / 46卷 / 06期

关键词：

D O I：

10.2337/diabetes.46.6.1081

中图分类号：

R5 [内科学];

学科分类号：

1002 ; 100201 ;

摘要：

Maturity-onset diabetes of the young 3 (MODY3) is a type of NIDDM caused by mutations in the transcription factor hepatocyte nuclear factor-1 alpha (HNF-1 alpha) located on chromosome 12q. We have identified four novel HNF-1 alpha missense mutations in MODY3 families, In four additional and unrelated families, we observed an identical insertion mutation that had occurred in a polycytidine tract in exon 4. Among those families, one exhibited a de novo mutation at this location. We propose that instability of this sequence represents a general mutational mechanism in MODY3. We observed no HNF-1 alpha mutations among 86 unrelated late-onset diabetic patients with relative insulin deficiency. Hence mutations in this gene appear to be most strongly associated with early-onset diabetes.

引用

收藏

页码：1081 / 1086

页数：6

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