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Association between a variation in LRCH1 and knee osteoarthritis: A genome-wide single-nucleotide polymorphism association study using DNA pooling

✍ Scribed by Tim D. Spector; Richard H. Reneland; Steven Mah; Ana M. Valdes; Deborah J. Hart; Stefan Kammerer; Maria Langdown; Carolyn R. Hoyal; Josephine Atienza; Michael Doherty; Proton Rahman; Matthew R. Nelson; Andreas Braun

Publisher: John Wiley and Sons
Year: 2006
Tongue: English
Weight: 163 KB
Volume: 54
Category: Article
ISSN: 0004-3591
DOI: 10.1002/art.21624

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✦ Synopsis

Abstract

Objective

To perform a large‐scale association analysis of single‐nucleotide polymorphisms (SNPs) in patients with radiographically defined osteoarthritis (OA) of the knee.

Methods

We examined >25,000 SNPs located within ∼14,000 genes for associations with radiographically defined knee OA, using polymerase chain reaction and MassExtend amplification techniques. Allele frequencies were estimated initially in DNA pools from 335 female patients with knee OA and 335 asymptomatic and radiographically negative female control subjects. All were of northern European ancestry. Significant allele frequency differences were validated by genotyping of individual DNA samples. Confirmed significant findings were verified in 2 additional case–control samples from the UK (443 cases and 303 controls) and Newfoundland (346 cases and 264 controls). Chondrosarcoma cell lines were used to test for potential differences in gene expression.

Results

The marker most strongly associated with the risk of knee OA was rs912428, a C/T polymorphism in intron 1 of LRCH1, a gene on chromosome 13q14 that encodes a novel protein of as‐yet‐unknown function. The frequency of the T allele compared with controls was consistently increased by 40% across all 3 case–control groups. Additional subanalyses in case–control samples with hip OA and hand OA suggested similar trends, but did not reach statistical significance. Association fine‐mapping using 10 additional SNPs in LRCH1 confirmed intron 1 as the region of highest association but failed to reveal variations with significance stronger than the marker SNP, as did the haplotype analysis. LRCH1 was not up‐regulated or overexpressed in chondrosarcoma cell lines exposed to inflammatory stimuli, suggesting a possible structural role.

Conclusion

A genetic variant in LRCH1 was consistently associated with knee OA in 3 samples from 2 populations. Our results also suggest that the same association with OA may exist at other sites. Additional genetic and experimental work is needed to elucidate the precise mechanism by which the LRCH1 gene influences OA risk.

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