Valentonyte Ruta, Hampe Jochen, Huse Klaus, Rosenstiel Philip, Albrecht Mario, Stenzel Annette, Nagy Marion, Gaede Karoline I, Franke Andre, Haesler Robert, Koch Andreas, Lengauer Thomas, Seegert Dirk, Reiling Norbert, Ehlers Stefan, Schwinger Eberhard, Platzer Matthias, Krawczak Michael, Müller-Quernheim Joachim, Schürmann Manfred, Schreiber Stefan
Institute for Clinical Molecular Biology, Christian-Albrechts-University Kiel, Universitätsklinikum Schleswig-Holstein, Campus Kiel, Schittenhelmstr. 12, 24105 Kiel, Germany.
Nat Genet. 2005 Apr;37(4):357-64. doi: 10.1038/ng1519. Epub 2005 Feb 27.
Sarcoidosis is a polygenic immune disorder with predominant manifestation in the lung. Genome-wide linkage analysis previously indicated that the extended major histocompatibility locus on chromosome 6p was linked to susceptibility to sarcoidosis. Here, we carried out a systematic three-stage SNP scan of 16.4 Mb on chromosome 6p21 in as many as 947 independent cases of familial and sporadic sarcoidosis and found that a 15-kb segment of the gene butyrophilin-like 2 (BTNL2) was associated with the disease. The primary disease-associated variant (rs2076530; P(TDT) = 3 x 10(-6), P(case-control) = 1.1 x 10(-8); replication P(TDT) = 0.0018, P(case-control) = 1.8 x 10(-6)) represents a risk factor that is independent of variation in HLA-DRB1. BTNL2 is a member of the immunoglobulin superfamily and has been implicated as a costimulatory molecule involved in T-cell activation on the basis of its homology to B7-1. The G --> A transition constituting rs2076530 leads to the use of a cryptic splice site located 4 bp upstream of the affected wild-type donor site. Transcripts of the risk-associated allele have a premature stop in the spliced mRNA. The resulting protein lacks the C-terminal IgC domain and transmembrane helix, thereby disrupting the membrane localization of the protein, as shown in experiments using green fluorescent protein and V5 fusion proteins.
结节病是一种多基因免疫疾病,主要表现在肺部。全基因组连锁分析先前表明,6号染色体短臂上的扩展主要组织相容性位点与结节病易感性相关。在此,我们对多达947例家族性和散发性结节病独立病例的6号染色体短臂21区16.4 Mb进行了系统的三阶段单核苷酸多态性扫描,发现嗜乳脂蛋白样2(BTNL2)基因的一个15 kb片段与该疾病相关。主要疾病相关变异(rs2076530;家系传递不平衡检验P值 = 3×10⁻⁶,病例对照P值 = 1.1×10⁻⁸;重复验证家系传递不平衡检验P值 = 0.0018,病例对照P值 = 1.8×10⁻⁶)代表一个独立于HLA - DRB1变异的危险因素。BTNL2是免疫球蛋白超家族的成员,基于其与B7 - 1的同源性,被认为是参与T细胞活化的共刺激分子。构成rs2076530的G→A转换导致使用一个位于受影响野生型供体位点上游4 bp处的隐蔽剪接位点。风险相关等位基因的转录本在剪接后的mRNA中有一个过早的终止密码子。所产生的蛋白质缺乏C末端IgC结构域和跨膜螺旋,从而破坏了该蛋白质的膜定位,这在使用绿色荧光蛋白和V5融合蛋白的实验中得到了证实。
