共 19 条
Identification of mutations in the hepatocyte nuclear factor (HNF)-1 alpha gene in Japanese subjects with IDDM
被引:60
作者:

Yamada, S
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机构: GUNMA UNIV,SCH MED,DEPT MOL GENET,MAEBASHI,GUMMA 371,JAPAN

Nishigori, H
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机构: GUNMA UNIV,SCH MED,DEPT MOL GENET,MAEBASHI,GUMMA 371,JAPAN

Onda, H
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机构: GUNMA UNIV,SCH MED,DEPT MOL GENET,MAEBASHI,GUMMA 371,JAPAN

Utsugi, T
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机构: GUNMA UNIV,SCH MED,DEPT MOL GENET,MAEBASHI,GUMMA 371,JAPAN

Yanagawa, T
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机构: GUNMA UNIV,SCH MED,DEPT MOL GENET,MAEBASHI,GUMMA 371,JAPAN

Maruyama, T
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机构: GUNMA UNIV,SCH MED,DEPT MOL GENET,MAEBASHI,GUMMA 371,JAPAN

Onigata, K
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机构: GUNMA UNIV,SCH MED,DEPT MOL GENET,MAEBASHI,GUMMA 371,JAPAN

Nagashima, K
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机构: GUNMA UNIV,SCH MED,DEPT MOL GENET,MAEBASHI,GUMMA 371,JAPAN

Nagai, R
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机构: GUNMA UNIV,SCH MED,DEPT MOL GENET,MAEBASHI,GUMMA 371,JAPAN

Morikawa, A
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机构: GUNMA UNIV,SCH MED,DEPT MOL GENET,MAEBASHI,GUMMA 371,JAPAN

Takeuchi, T
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机构: GUNMA UNIV,SCH MED,DEPT MOL GENET,MAEBASHI,GUMMA 371,JAPAN

Takeda, J
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机构: GUNMA UNIV,SCH MED,DEPT MOL GENET,MAEBASHI,GUMMA 371,JAPAN
机构:
[1] GUNMA UNIV,SCH MED,DEPT MOL GENET,MAEBASHI,GUMMA 371,JAPAN
[2] GUNMA UNIV,SCH MED,DEPT MOL MED,MAEBASHI,GUMMA 371,JAPAN
[3] GUNMA UNIV,SCH MED,INST MOL & CELLULAR REGULAT,MAEBASHI,GUMMA 371,JAPAN
[4] GUNMA UNIV,SCH MED,DEPT INTERNAL MED 2,MAEBASHI,GUMMA 371,JAPAN
[5] NERIMA GEN HOSP,DEPT INTERNAL MED,TOKYO,JAPAN
[6] SOCIAL INSURANCE SAITAMA CHUO HOSP,DEPT INTERNAL MED,SAITAMA,JAPAN
来源:
关键词:
D O I:
10.2337/diabetes.46.10.1643
中图分类号:
R5 [内科学];
学科分类号:
1002 ;
100201 ;
摘要:
One form of maturity-onset diabetes of the young, MODY3, is characterized by a severe insulin secretory defect, compared with MODY2, a glucokinase-deficient diabetes, It has recently been shown that mutations of the gene encoding the transcription factor hepatocyte nuclear factor (HNF)-1 alpha cause MODY3. Because of the rapid progress to overt diabetes and the high prevalence of required insulin treatment in patients with MODY3, we screened the HNF-1 alpha gene for mutations in Japanese subjects with IDDM, Ten exons and flanking introns of the HNF-1 alpha gene in these subjects were amplified by polymerase chain reaction and direct sequencing of the products, Mutations were identified in three (5.5%) of the 55 unrelated subjects with IDDM, A missense mutation of R272H (replacement of Arg by His in codon 272) in the DNA binding domain of HNF-1 alpha was found in a subject who developed IDDM 1 year after diagnosis of NIDDM at 8 years of age, A frameshift mutation of P291fsinsC (insertion of a C in a polyC tract around codon 291 for Pro), which would generate a mutant truncated protein of 340 amino acids, was found in a subject who started insulin treatment when hyperglycemia and ketonuria were noticed at 13 years of age, A missense mutation of R583G (replacement of Arg by Gly in codon 583) in the transactivation domain of HNF-1 alpha was found in a subject with sudden-onset IDDM at 20 years of age, None of these mutations were present in 100 nondiabetic subjects (200 normal chromosomes), These results indicate that the HNF-1 alpha gene defects could lead to the development of not only early-onset NIDDM but also IDDM, implicating the importance of subclassification of HNF-1 alpha-deficient IDDM from a classical type of autoimmune-based IDDM in Japanese.
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页码:1643 / 1647
页数:5
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机构: UNIV CHICAGO,HOWARD HUGHES MED INST,CHICAGO,IL 60637

Yamagata, K
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机构: UNIV CHICAGO,HOWARD HUGHES MED INST,CHICAGO,IL 60637

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[10]
Characterization of the MODY3 phenotype - Early-onset diabetes caused by an insulin secretion defect
[J].
Lehto, M
;
Tuomi, T
;
Mahtani, MM
;
Widen, E
;
Forsblom, C
;
Sarelin, L
;
Gullstrom, M
;
Isomaa, B
;
Lehtovirta, M
;
Hyrkko, A
;
Kanninen, T
;
Orho, M
;
Manley, S
;
Turner, RC
;
Brettin, T
;
Kirby, A
;
Thomas, J
;
Duyk, G
;
Lander, E
;
Taskinen, MR
;
Groop, L
.
JOURNAL OF CLINICAL INVESTIGATION,
1997, 99 (04)
:582-591

Lehto, M
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机构: LUND UNIV,MALMO GEN HOSP,WALLENBERG LAB,DEPT ENDOCRINOL,S-20502 MALMO,SWEDEN

Tuomi, T
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Mahtani, MM
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Widen, E
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Forsblom, C
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Sarelin, L
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Gullstrom, M
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Isomaa, B
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Lehtovirta, M
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Hyrkko, A
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Kanninen, T
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Orho, M
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Manley, S
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Turner, RC
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Brettin, T
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Kirby, A
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Thomas, J
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Duyk, G
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Lander, E
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Taskinen, MR
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Groop, L
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