Gong Y, Vikkula M, Boon L, Liu J, Beighton P, Ramesar R, Peltonen L, Somer H, Hirose T, Dallapiccola B, De Paepe A, Swoboda W, Zabel B, Superti-Furga A, Steinmann B, Brunner H G, Jans A, Boles R G, Adkins W, van den Boogaard M J, Olsen B R, Warman M L
Department of Genetics, Case Western Reserve University School of Medicine, Cleveland OH 44106, USA.
Am J Hum Genet. 1996 Jul;59(1):146-51.
Osteoporosis-pseudoglioma syndrome (OPS) is an autosomal recessive disorder characterized by severe juvenile-onset osteoporosis and congenital or juvenile-onset blindness. The pathogenic mechanism is not known. Clinical, biochemical, and microscopic analyses suggest that OPS may be a disorder of matrix homeostasis rather than a disorder of matrix structure. Consequently, identification of the OPS gene and its protein product could provide insights regarding common osteoporotic conditions, such as postmenopausal and senile osteoporosis. As a first step toward determining the cause of OPS, we utilized a combination of traditional linkage analysis and homozygosity mapping to assign the OPS locus to chromosome region 11q12-13. Mapping was accomplished by analyzing 16 DNA samples (seven affected individuals) from three different consanguineous kindreds. Studies in 10 additional families narrowed the candidate region, supported locus homogeneity, and did not detect founder effects. The OPS locus maps to a 13-cM interval between D11S1298 and D11S971 and most likely lies in a 3-cM region between GSTP1 and D11S1296. At present, no strong candidate genes colocalize with OPS.
骨质疏松-假性胶质瘤综合征(OPS)是一种常染色体隐性疾病,其特征为严重的幼年型骨质疏松以及先天性或幼年型失明。其致病机制尚不清楚。临床、生化及显微镜分析表明,OPS可能是一种基质稳态紊乱而非基质结构紊乱。因此,鉴定OPS基因及其蛋白产物可能为诸如绝经后骨质疏松和老年性骨质疏松等常见骨质疏松症提供见解。作为确定OPS病因的第一步,我们采用传统连锁分析和纯合性定位相结合的方法,将OPS基因座定位于染色体区域11q12 - 13。通过分析来自三个不同近亲家族的16个DNA样本(7个患病个体)完成了定位。对另外10个家族的研究缩小了候选区域,支持基因座同质性,且未检测到奠基者效应。OPS基因座定位于D11S1298和D11S971之间13厘摩的区间内,最有可能位于GSTP1和D11S1296之间3厘摩的区域。目前,没有强候选基因与OPS共定位。
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