New susceptibility locus for rheumatoid arthritis suggested by a genome-wide linkage study

François Cornélis(Hôpital Saint-Louis), Sabine Fauré(Hôpital Saint-Louis), María Martínez(Hôpital Saint-Louis), Jean-François Prud’homme(Hôpital Saint-Louis), P Fritz(Hôpital Saint-Louis), Colette Dib(Hôpital Saint-Louis), Helena Alves(Hôpital Saint-Louis), Pilar Barrera(Hôpital Saint-Louis), Niek de Vries(Hôpital Saint-Louis), Alejandro Balsa(Hôpital Saint-Louis), Dora Pascual‐Salcedo(Hôpital Saint-Louis), K Maenaut(Hôpital Saint-Louis), R. Westhovens(Hôpital Saint-Louis), Paola Migliorini(Istituto di Fisiologia Clinica), Tuyet-Hoa Tran(Istituto di Fisiologia Clinica), A Delaye(Hôpital Saint-Louis), Nathalie Prince(Hôpital Saint-Louis), Caroline Lefèvre(Hôpital Saint-Louis), G Thomas(Hôpital Saint-Louis), M Poirier(Hôpital Saint-Louis), Stéphane Soubigou(Hôpital Saint-Louis), Olivier Alibert(Hôpital Saint-Louis), Sandra Lasbleiz(Hôpital Saint-Louis), Sylvaine Fouix(Hôpital Saint-Louis), Christiane Bouchier(Hôpital Saint-Louis), Frédéric Lioté(Hôpital Saint-Louis), M.N. Loste(Hôpital Saint-Louis), Virginia Lepage(Hôpital Saint-Louis), Dominique Charron(Hôpital Saint-Louis), Gàbor Gyapay(Hôpital Saint-Louis), Antonio Lopes-Vaz(Hôpital Saint-Louis), Daniel Kuntz(Hospital Universitario La Paz), Thomas Bardin(Hôpital Saint-Louis), Jean Weissenbach(Hôpital Saint-Louis)
Proceedings of the National Academy of Sciences
September 1, 1998
10.1073/pnas.95.18.10746
Cited by 470Open Access

Abstract

Rheumatoid arthritis (RA), the most common autoimmune disease, is associated in families with other autoimmune diseases, including insulin-dependent diabetes mellitus (IDDM). Its genetic component has been suggested by familial aggregation (lambdas = 5), twin studies, and segregation analysis. HLA, which is the only susceptibility locus known, has been estimated to account for one-third of this component. The aim of this paper was to identify new RA loci. A genome scan was performed with 114 European Caucasian RA sib pairs from 97 nuclear families. Linkage was significant only for HLA (P < 2.5.10(-5)) and nominal for 19 markers in 14 other regions (P < 0.05). Four of the loci implicated in IDDM potentially overlap with these regions: the putative IDDM6, IDDM9, IDDM13, and DXS998 loci. The first two of these candidate regions, defined in the RA genome scan by the markers D18S68-D18S61-D18S469 (18q22-23) and D3S1267 (3q13), respectively, were studied in 194 additional RA sib pairs from 164 nuclear families. Support for linkage to chromosome 3 only was extended significantly (P = 0.002). The analysis of all 261 families provided a linkage evidence of P = 0. 001 and suggested an interaction between this putative RA locus and HLA. This locus could account for 16% of the genetic component of RA. Candidate genes include those coding for CD80 and CD86, molecules involved in antigen-specific T cell recognition. In conclusion, this first genome scan in RA Caucasian families revealed 14 candidate regions, one of which was supported further by the study of a second set of families.

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