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Title: A genome-wide linkage scan for homocysteine levels suggests three regions of interest.
Author(s): Vermeulen, S. (298981033)
Vleuten, G.M. van der
Graaf, J. de (104035064)
Hermus, A.R.M.M. (07172429X)
Blom, H.J. (073808628)
Stalenhoef, A.F.H. (068700415)
Heijer, M. den (157196674)
Publication year: 2006
Document type: Article / Letter to editor
Journal: Journal of Thrombosis and Haemostasis
ISSN: 1538-7933
Volume: vol. 4
Issue: iss. 6
Start page: p. 1303
End page: p. 1307
Abstract: BACKGROUND: An elevated plasma total homocysteine (tHcy) level is a risk factor for many clinical conditions, including vascular disease and venous thrombosis. The tHcy levels are partly determined by genetic factors. Extensive candidate gene studies have identified several genetic variants, including the MTHFR 677C>T, that influence tHcy levels, but so far only part of the genetic variation in tHcy can be explained. OBJECTIVE: In order to identify chromosomal regions that influence tHcy levels, a genome-wide linkage analysis was conducted. PATIENTS/METHODS: Our study population consisted of 13 pedigrees and 469 subjects with data on fasting plasma tHcy levels. A set of 377 markers covering the genome was genotyped in 275 subjects. The variance component linkage method (SOLAR version 2.1.3) was used for the two-point and multipoint linkage analyses. RESULTS: The heritability of the age- and sex-adjusted homocysteine levels was 44%. The multipoint linkage analysis identified one region with suggestive linkage on chromosome 16q (LOD score 1.76; nominal P = 0.0024). Weaker evidence of linkage was found for regions on chromosome 12q (LOD score 1.57; nominal P = 0.0036) and chromosome 13q (LOD score 1.52; nominal P = 0.0041). CONCLUSIONS: In our families the plasma tHcy level was highly heritable. The multipoint linkage analysis identified three regions that showed weak to suggestive linkage to tHcy levels.
Subject: EBP 1: Determinants in Health and Disease
UMCN 2.2: Vascular medicine and diabetes
UMCN 5.2: Endocrinology and reproduction
Organization: Endocrinology
General Internal Medicine
Paediatrics
Epidemiology, Biostatistics & HTA
Appears in Collections:Academic bibliography

Please use this identifier to cite or link to this item: http://hdl.handle.net/2066/51184

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