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A missense single-nucleotide polymorphism in a gene encoding a protein tyrosine phosphatase (PTPN22) is associated with rheumatoid arthritis
Authors:Begovich Ann B  Carlton Victoria E H  Honigberg Lee A  Schrodi Steven J  Chokkalingam Anand P  Alexander Heather C  Ardlie Kristin G  Huang Qiqing  Smith Ashley M  Spoerke Jill M  Conn Marion T  Chang Monica  Chang Sheng-Yung P  Saiki Randall K  Catanese Joseph J  Leong Diane U  Garcia Veronica E  McAllister Linda B  Jeffery Douglas A  Lee Annette T  Batliwalla Franak  Remmers Elaine  Criswell Lindsey A  Seldin Michael F  Kastner Daniel L  Amos Christopher I  Sninsky John J  Gregersen Peter K
Affiliation:Celera Diagnostics, Alameda, CA 94502, USA. Ann.Begovich@celeradiagnostics.com
Abstract:Rheumatoid arthritis (RA) is the most common systemic autoimmune disease, affecting approximately 1% of the adult population worldwide, with an estimated heritability of 60%. To identify genes involved in RA susceptibility, we investigated the association between putative functional single-nucleotide polymorphisms (SNPs) and RA among white individuals by use of a case-control study design; a second sample was tested for replication. Here we report the association of RA susceptibility with the minor allele of a missense SNP in PTPN22 (discovery-study allelic P=6.6 x 10(-4); replication-study allelic P=5.6 x 10(-8)), which encodes a hematopoietic-specific protein tyrosine phosphatase also known as "Lyp." We show that the risk allele, which is present in approximately 17% of white individuals from the general population and in approximately 28% of white individuals with RA, disrupts the P1 proline-rich motif that is important for interaction with Csk, potentially altering these proteins' normal function as negative regulators of T-cell activation. The minor allele of this SNP recently was implicated in type 1 diabetes, suggesting that the variant phosphatase may increase overall reactivity of the immune system and may heighten an individual carrier's risk for autoimmune disease.
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