Deep sequencing of GDF5 reveals the absence of rare variants at this important osteoarthritis susceptibility locus

Dodd, A. W.; Rodriguez-Fontenla, C.; Calaza, M.; Carr, A.; Gomez-Reino, J. J.; Tsezou, A.; Reynard, L. N.; Gonzalez, A.; Loughlin, J.

dc.creator	Dodd, A. W.	en
dc.creator	Rodriguez-Fontenla, C.	en
dc.creator	Calaza, M.	en
dc.creator	Carr, A.	en
dc.creator	Gomez-Reino, J. J.	en
dc.creator	Tsezou, A.	en
dc.creator	Reynard, L. N.	en
dc.creator	Gonzalez, A.	en
dc.creator	Loughlin, J.	en
dc.date.accessioned	2015-11-23T10:25:46Z
dc.date.available	2015-11-23T10:25:46Z
dc.date.issued	2011
dc.identifier	10.1016/j.joca.2011.01.014
dc.identifier.issn	1063-4584
dc.identifier.uri	http://hdl.handle.net/11615/27147
dc.description.abstract	Objective: The common single nucleotide polymorphism (SNP) rs143383 in the 5' untranslated region (5'UTR) of growth and differentiation factor 5 (GDF5) is strongly associated with osteoarthritis (OA) and influences GDF5 allelic expression in vitro and in the joint tissues of OA patients. This effect is modulated in cis by another common SNP, also located within the 5'UTR, whilst a common SNP in the 3'UTR influences allelic expression independent of rs143383. DNA variants can be common, rare or extremely rare/unique. To therefore enhance our understanding of the allelic architecture of this very important OA susceptibility locus we sequenced the gene for potentially functional and novel rare variants. Method: Using the Sanger method we sequenced GDF5 in 992 OA patients and 944 controls, with DNA changes identified by sequencing software. We encompassed the protein-coding region of the two GDF5 exons, both untranslated regions and approximately 100 bp of the proximal promoter of the gene. Results: We detected 13 variants. Six were extremely rare with minor allele frequencies (MAFs) of <= 0.0006. One is in a predicted transcription factor binding site in the GDF5 promoter whilst two substitute conserved amino acids. The remaining seven variants were common and are previously known variants, with MAFs ranging from 0.025 to 0.39. There was a complete absence of variants with frequencies in-between the extremely rare (n = 6) and the common (n = 7). Conclusions: This is the first report of the deep sequencing of an OA susceptibility locus. The absence of rare variants informs us that within the regions of the gene that we have sequenced GDF5 does not harbour any novel variants that are able to contribute, at a population level, to the OA association signal mediated by rs143383 nor does it harbour, at a population level, any novel variants that can influence OA susceptibility independent of rs143383. (C) 2011 Osteoarthritis Research Society International. Published by Elsevier Ltd. All rights reserved.	en
dc.source.uri	<Go to ISI>://WOS:000289823500015
dc.subject	GDF5	en
dc.subject	DNA variants	en
dc.subject	Sequencing	en
dc.subject	Genetic susceptibility	en
dc.subject	HUMAN HEIGHT	en
dc.subject	ASSOCIATION	en
dc.subject	MUTATIONS	en
dc.subject	MICE	en
dc.subject	HIP	en
dc.subject	POLYMORPHISM	en
dc.subject	5'-UTR	en
dc.subject	REGION	en
dc.subject	JOINT	en
dc.subject	KNEE	en
dc.subject	Orthopedics	en
dc.subject	Rheumatology	en
dc.title	Deep sequencing of GDF5 reveals the absence of rare variants at this important osteoarthritis susceptibility locus	en
dc.type	journalArticle	en

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