In April 2016 Manchester eScholar was replaced by the University of Manchester’s new Research Information Management System, Pure. In the autumn the University’s research outputs will be available to search and browse via a new Research Portal. Until then the University’s full publication record can be accessed via a temporary portal and the old eScholar content is available to search and browse via this archive.

Related resources

Full-text held externally

PMID: 17133579
UKPMCID: 17133579
DOI: 10.1002/art.22270

Search for item elsewhere

University researcher(s)

William Newman's research staff profile

Academic department(s)

Rheumatoid arthritis association with the FCRL3 -169C polymorphism is restricted to PTPN22 1858T-homozygous individuals in a Canadian population.

Newman, William G; Zhang, Qing; Liu, Xiangdong; Walker, Erin; Ternan, Heather; Owen, Julie; Johnson, Ben; Greer, Wenda; Mosher, Dianne P; Maksymowych, Walter P; Bykerk, Vivian P; Keystone, Edward C; Amos, Christopher I; Siminovitch, Katherine A

Arthritis and rheumatism. 2006;54(12):3820-7.

Access to files

Full-text and supplementary files are not available from Manchester eScholar. Full-text is available externally using the following links:

Full-text held externally

PMID: 17133579
UKPMCID: 17133579
DOI: 10.1002/art.22270

Abstract

OBJECTIVE: Variants in genes encoding the Fc receptor-like 3 (FcRL-3) and the class II major histocompatibility complex (MHC) transactivator proteins have been associated with an increased risk of rheumatoid arthritis (RA) in Japanese and Nordic populations, respectively. The aim of this study was to investigate these associations in a Canadian Caucasian cohort of RA cases and healthy controls. METHODS: A total of 1,187 RA patients and 462 healthy controls were genotyped for FCRL3 and MHC2TA gene variants associated with RA. Epistasis between the FCRL3 -169C and the PTPN22 1858T variants was also examined. RESULTS: An association was detected between RA and both the FCRL3 -169C allele (OR 1.19, P = 0.023) and the homozygous genotype (OR 1.41, P = 0.027), but association of the MHC2TA promoter region variant (-168G) with RA was not replicated. Stratification of the RA cohort by PTPN22 genotypes revealed the FCRL3 risk variant and RA association was stronger in the patient subgroup lacking PTPN22 1858T variants (P = 0.004) and was not detectable in the subgroup with PTPN22 1858T variants (P = 0.52). The PTPN22 association with RA was greater in the absence than in the presence of the FCRL3 -169C allele (P = 0.0008 versus P = 0.001). The PTPN22 1858T variant also increased the risk of autoimmune thyroid disease (AITD) in the RA patients, whereas the FCRL3 risk variant was protective against AITD. CONCLUSION: Our findings support an association of RA with an FCRL3 functional polymorphism and reveal that this association is stronger in the absence of PTPN22 risk genotypes. These findings support a genetic heterogeneity across RA populations, suggesting that both the FCRL3 and PTPN22 genes play roles in RA susceptibility, but in different individuals.

Bibliographic metadata

Type of resource:

text

Content type:

Journal article

Publication type:

Review article

Author(s):

Published date:

2006-12

Article title:

Rheumatoid arthritis association with the FCRL3 -169C polymorphism is restricted to PTPN22 1858T-homozygous individuals in a Canadian population.

Journal title:

Arthritis and rheumatism

Abbreviated journal title:

Arthritis Rheum

ISSN:

0004-3591

Place of publication:

United States

Volume:

Issue:

Pagination:

3820-7

Digital Object Identifier:

10.1002/art.22270

Pubmed Identifier:

17133579

Access state:

Active

Institutional metadata

University researcher(s):

Newman, William

Academic department(s):

Record metadata

Manchester eScholar ID:

uk-ac-man-scw:194539

Created by:

Newman, William

Created:

9th May, 2013, 19:28:34

Last modified by:

Newman, William

Last modified:

9th May, 2013, 19:28:34