Franco B, Meroni G, Parenti G, Levilliers J, Bernard L, Gebbia M, Cox L, Maroteaux P, Sheffield L, Rappold G A, Andria G, Petit C, Ballabio A
Department of Molecular and Human Genetics, Baylor College of Medicine, Houston, Texas 77030, USA.
Cell. 1995 Apr 7;81(1):15-25. doi: 10.1016/0092-8674(95)90367-4.
X-linked recessive chondrodysplasia punctata (CDPX) is a congenital defect of bone and cartilage development characterized by aberrant bone mineralization, severe underdevelopment of nasal cartilage, and distal phalangeal hypoplasia. A virtually identical phenotype is observed in the warfarin embryopathy, which is due to the teratogenic effects of coumarin derivatives during pregnancy. We have cloned the genomic region within Xp22.3 where the CDPX gene has been assigned and isolated three adjacent genes showing highly significant homology to the sulfatase gene family. Point mutations in one of these genes were identified in five patients with CDPX. Expression of this gene in COS cells resulted in a heat-labile arylsulfatase activity that is inhibited by warfarin. A deficiency of a heat-labile arylsulfatase activity was demonstrated in patients with deletions spanning the CDPX region. These data indicate that CDPX is caused by an inherited deficiency of a novel sulfatase and suggest that warfarin embryopathy might involve drug-induced inhibition of the same enzyme.
X连锁隐性点状软骨发育不良(CDPX)是一种骨和软骨发育的先天性缺陷,其特征为骨矿化异常、鼻软骨严重发育不全以及远端指骨发育不全。在华法林胚胎病中观察到几乎相同的表型,这是由于孕期香豆素衍生物的致畸作用所致。我们已经克隆了位于Xp22.3的基因组区域,CDPX基因已定位于此,并且分离出了三个与硫酸酯酶基因家族具有高度显著同源性的相邻基因。在五名CDPX患者中鉴定出其中一个基因的点突变。该基因在COS细胞中的表达产生了一种对华法林敏感的芳基硫酸酯酶活性。在跨越CDPX区域存在缺失的患者中证实了对华法林敏感的芳基硫酸酯酶活性缺乏。这些数据表明CDPX是由一种新型硫酸酯酶的遗传性缺乏引起的,并提示华法林胚胎病可能涉及药物诱导的对同一酶的抑制作用。