Role of APRIL (TNFSF13) polymorphisms in the susceptibility to systemic lupus erythematosus in Japanese

doi:10.1093/rheumatology/kem019

Rheumatology Advance Access originally published online on February 16, 2007
Rheumatology 2007 46(5):776-782; doi:10.1093/rheumatology/kem019

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Role of APRIL (TNFSF13) polymorphisms in the susceptibility to systemic lupus erythematosus in Japanese

A. Kawasaki¹^,2, N. Tsuchiya², J. Ohashi¹, Y. Murakami³, T. Fukazawa⁴, M. Kusaoi⁴, S. Morimoto⁴, K. Matsuta⁵, H. Hashimoto⁶, Y. Takasaki⁴ and K. Tokunaga¹

¹Department of Human Genetics, Graduate School of Medicine, The University of Tokyo, Tokyo, ²Doctoral Program in Social and Environmental Medicine, Graduate School of Comprehensive Human Sciences, University of Tsukuba, Tsukuba, ³Tumor Suppression and Functional Genomics Project, National Cancer Center Research Institute, Tokyo, ⁴Department of Rheumatology and Internal Medicine, Juntendo University, Tokyo, ⁵Matsuta Clinic, Tokyo and ⁶Department of Rheumatology and Internal Medicine, Juntendo Koshigaya Hospital, Koshigaya, Japan

Correspondence to: N. Tsuchiya, Doctoral Program in Social and Environmental Medicine, Graduate School of Comprehensive Human Sciences, University of Tsukuba, Tsukuba, Ibaraki 305-8575, Japan. E-mail: tsuchiya-tky{at}umin.net

Abstract

Objectives. A polymorphism of APRIL, c.199G > A (Gly67Arg),has been reported to be associated with systemic lupus erythematosus(SLE) in Japanese. To identify the causative polymorphism, wescreened for polymorphisms of APRIL as well as TWEAK (TNFSF12),a closely located gene that generates a fusion protein TWE-PRILby intergenic splicing. Association of APRIL and TWEAK withrheumatoid arthritis (RA) was examined in parallel.

Methods. Polymorphisms were screened by direct sequencing. Associationwas analysed by case-control analysis using 266 SLE, 298 RAand 208 healthy individuals. Allele-specific difference in themRNA level was examined using RNA difference plot analysis.Serum APRIL level was measured by ELISA.

Results. The protective effect of APRIL c.199A/A homozygotesin SLE was replicated (odds ratio 0.50, 95% confidence interval0.30–0.83, P = 0.0073; pooled P = 0.0001, Pcorr = 0.007).In addition, association of c.287A > G (Asn96Ser, P = 0.0064,allele frequency) and c.*263C > T (3’ untranslatedregion, P = 0.025, allele frequency) was detected. c.199G-c.287A(67Gly-96Asn) haplotype was found to confer risk for SLE, whilec.199A-c.287G (67Arg-96Ser) was protective. Association of TWEAKwas observed neither for SLE nor RA. APRIL mRNA was increasedin SLE-associated c.*263T allele. In addition, serum APRIL wasundetectable in all six healthy controls homozygous for theprotective c.199A-c.287G haplotype (P = 0.015).

Conclusions. In addition to replicating the protective roleof APRIL c.199A/A, two additional SNPs in APRIL were found tobe associated with SLE. Presence of a protective haplotype anda risk haplotype was demonstrated. The mechanism of associationwas suggested to be altered expression at the protein and mRNAlevels.

KEY WORDS: Systemic lupus erythematosus, APRIL (TNFSF13), Polymorphism, Susceptibility, Genetics

Submitted 5 November 2006; revised version accepted 9 January 2007.
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