首页> 外文期刊>The American Journal of Human Genetics >Identification of CANT1 mutations in Desbuquois dysplasia.
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Identification of CANT1 mutations in Desbuquois dysplasia.

机译:鉴定Desbuquois发育不良中的CANT1突变。

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Desbuquois dysplasia is a severe condition characterized by short stature, joint laxity, scoliosis, and advanced carpal ossification with a delta phalanx. Studying nine Desbuquois families, we identified seven distinct mutations in the Calcium-Activated Nucleotidase 1 gene (CANT1), which encodes a soluble UDP-preferring nucleotidase belonging to the apyrase family. Among the seven mutations, four were nonsense mutations (Del 5' UTR and exon 1, p.P245RfsX3, p.S303AfsX20, and p.W125X), and three were missense mutations (p.R300C, p.R300H, and p.P299L) responsible for the change of conserved amino acids located in the seventh nucleotidase conserved region (NRC). The arginine substitution at position 300 was identified in five out of nine families. The specific function of CANT1 is as yet unknown, but its substrates are involved in several major signaling functions, including Ca2+ release, through activation of pyrimidinergic signaling. Importantly, using RT-PCR analysis, we observed a specific expression in chondrocytes. We also found electron-dense material within distended rough endoplasmic reticulum in the fibroblasts of Desbuquois patients. Our findings demonstrate the specific involvement of a nucleotidase in the endochondral ossification process.
机译:Desbuquois不典型增生是一种严重的疾病,其特征是身材矮小,关节松弛,脊柱侧弯和腕骨骨化,三角洲趾骨增高。研究了9个Desbuquois家族,我们在钙激活的核苷酸酶1基因(CANT1)中发现了7个不同的突变,该基因编码一种属于腺苷三磷酸双磷酸酶家族的可溶性UDP优先核苷酸酶。在这七个突变中,四个是无义突变(Del 5'UTR和外显子1,p.P245RfsX3,p.S303AfsX20和p.W125X),三个是错义突变(p.R300C,p.R300H和p.P299L) )负责改变位于第七个核苷酸酶保守区(NRC)的保守氨基酸。在九个家庭中的五个家庭中,确定了第300位的精氨酸取代。 CANT1的具体功能尚不清楚,但其底物通过激活嘧啶能信号传导参与了几种主要的信号传导功能,包括Ca2 +释放。重要的是,使用RT-PCR分析,我们观察到了软骨细胞中的特定表达。我们还发现Desbuquois患者的成纤维细胞内扩张的粗面内质网内存在电子致密材料。我们的发现证明了核苷酸酶在软骨内骨化过程中的特定参与。

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