BACKGROUND:Namaqualand hip dysplasia (NHD) is a mild form of spondyloepiphyseal dysplasia in which progressive arthropathy of the hip joint is a major manifestation. The disorder was documented in a multigenerational South African (SA) family with antecedents from Namaqualand, a region in the north-west of the country. Linkage analysis revealed a locus that includes the collagen type II gene, COL2A1.OBJECTIVES:To identify the pathogenic COL2A1 variant causing NHD in an SA family.METHODS:One affected male with a clear diagnosis of NHD was selected for whole-exome sequencing (WES) on the Ion Torrent Proton platform. A probe-based assay and direct cycle sequencing were used to confirm that the prioritised variant segregated with the phenotype in the NHD family and was not present in unrelated controls from the same population.RESULTS:WES identified one heterozygous variant, c.2014GT; p.(Gly672Cys), in the coding sequence of the COL2A1 gene. The variant segregated with NHD in 23 affected family members and was previously reported in a Caucasian male with Perthes disease-like presentation.CONCLUSIONS:It is now possible to provide a molecular diagnosis of NHD before hip problems present. The large, clinically well-characterised NHD family is a valuable resource that could provide more insight into the mechanisms responsible for the variable expression observed in individuals with this variant.
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机译:背景:Namaqualand Hip Dysplasia(NHD)是一种温和形式的脊柱肌病发育不良,其中髋关节的渐进式关节病是一种重大表现。该疾病被记录在多岛南非(SA)家庭中,其中包括Namaqualand的一家,该国在该国西北部的一个地区。连杆分析显示,包括胶原II基因,COL2A1的基因座。鉴定致病菌的致病性COL2A1变体,导致SA家庭中的NHD。方法:选择一个受影响的男性,为全外壳测序选择明确的NHD诊断(WES )在离子洪流质子平台上。基于探针的测定和直接循环测序用于确认用NHD家族中的表型分离的优先型变体并不存在于来自同一群体的无关控制中。结果:WES鉴定了一种杂合变体,C.2014G> T. ; p。(gly672cys),在COL2A1基因的编码序列中。在23家受影响的家庭成员中,用NHD分离的变体,并以腐败疾病的呈现,在高加索男性中报道。结论:在存在的髋关节问题之前,现在可以提供NHD的分子诊断。大型临床良好的特征的NHD家族是一个有价值的资源,可以对负责该变体在个体中观察到的可变表达的机制提供更多洞察力。
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