| Literature DB >> 19672314 |
Bahram Jafar-Mohammadi1, Christopher J Groves, Katharine R Owen, Timothy M Frayling, Andrew T Hattersley, Mark I McCarthy, Anna L Gloyn.
Abstract
BACKGROUND: There is considerable interest in the hypothesis that low frequency, intermediate penetrance variants contribute to the proportion of Type 2 Diabetes (T2D) susceptibility not attributable to the common variants uncovered through genome-wide association approaches. Genes previously implicated in monogenic and multifactorial forms of diabetes are obvious candidates in this respect. In this study, we focussed on exons 8-10 of the HNF1A gene since rare, penetrant mutations in these exons (which are only transcribed in selected HNF1A isoforms) are associated with a later age of diagnosis of Maturity onset diabetes of the young (MODY) than mutations in exons 1-7. The age of diagnosis in the subgroup of HNF1A-MODY individuals with exon 8-10 mutations overlaps with that of early multifactorial T2D, and we set out to test the hypothesis that these exons might also harbour low-frequency coding variants of intermediate penetrance that contribute to risk of multifactorial T2D. METHODOLOGY AND PRINCIPALEntities:
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Year: 2009 PMID: 19672314 PMCID: PMC2720540 DOI: 10.1371/journal.pone.0006615
Source DB: PubMed Journal: PLoS One ISSN: 1932-6203 Impact factor: 3.240
Characteristics of subjects with T2D.
| Sample 1 | Sample 2 | |
|
| 84 | 507 |
|
| 61.9 | 53.6 |
|
| 34.3±11.4 | 55.4±8.5 |
|
| 26/66/8 | 14/69/17 |
|
| 48 | 100 |
|
| 32.3±4.8 | 28.8±5.2 |
Treatment at the time of ascertainment. ins, insulin; OHA, oral hypoglycaemic agent.
Variants identified in exons 8–10 of HNF1A.
| Coding region | Approved cDNA level description | Description used in MODY literature | rs number | MAF current study (%) | MAF in population controls (%) |
| Intron 8 | c.1623+29C>T | IVS8+29C>T | rs1169304 | 20.1 |
|
| Intron 9 | c.1769−24T>C | IVS9−24T>C | rs735396 | 33.4 |
|
| Intron 9 | c.1768+44C>T | IVS9+44C>T | N/A | 4.1 |
|
| Exon 8 | c.1545G>A | T515T | rs61953349 | 14.6 |
|
N/A; not available.
Based on screening 350 population controls (part of the UK 1958 Birth Cohort).
Based on screening 1050 population controls (part of the UK 1958 Birth Cohort).