a single nucleotide variant in hnf-1β is associated with ma¬turity-onset diabetes of the young in a large chinese family

نویسندگان

peng zhou

ran wei

zhenkui guo

haining zhu

چکیده

background: maturity-onset diabetes of the young (mody) is a heterogeneous entity of monogenic disorders characterized by autosomal dominant inheritance. eleven genes were related, including hnf4α, gck, hnf1α, ipf1, and hnf-1β, and various mutations are being reported. methods: to help the overall understanding of mody-related pathologic mutations, we studied a large mody family found in 2012, in shandong, china, which contained 9 patients over 3 generations.dna was extracted from the periphery blood samples of (i) 9 affected members, (ii) 17 unaffected members, and (iii) 1000 healthy controls. three pooled samples were obtained by mixing equal quantity ofdna of each individual within the each group. totally 400 microsatellite markers across the whole genome were genotyped by capillary electrophoresis. the known mody-related gene near the identified marker was sequenced to look for putative risk variants. results: allelic frequency of marker d17s798 on chromosome 17q11.2 were significantly different ( p <0.001) between the affected vs. unaffected members and the affected vs. healthy controls, but not between the unaffected members vs. healthy controls. mody5-related gene, hepatocyte nuclear factor-1β (hnf-1β) on 17q12 near d17s798 became the candidate gene. a single nucleotide variant (snv) of c77t in the non-coding area of exon 1 of hnf-1β was found to be related to mody5. conclusion: this novel snv of hnf-1β contributes to the diabetes development in the family through regulating gene expression most likely. the findings help presymptomatic diagnosis, and imply that mutations in the non-coding areas, as well as in the exons, play roles in the etiology of mody.

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A Single Nucleotide Variant in HNF-1β is Associated with Maturity-Onset Diabetes of the Young in a Large Chinese Family

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عنوان ژورنال:
iranian journal of public health

جلد ۴۵، شماره ۲، صفحات ۱۷۰-۱۷۸

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