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Cxorf5(71-7A)的特征描述,这是一种新的人类cDNA,定位于Xp22,编码一种含有卷曲螺旋α螺旋结构域的蛋白质。

Characterization of Cxorf5 (71-7A), a novel human cDNA mapping to Xp22 and encoding a protein containing coiled-coil alpha-helical domains.

作者信息

de Conciliis L, Marchitiello A, Wapenaar M C, Borsani G, Giglio S, Mariani M, Consalez G G, Zuffardi O, Franco B, Ballabio A, Banfi S

机构信息

Department of Molecular and Human Genetics, Baylor College of Medicine, Houston, Texas 77030, USA.

出版信息

Genomics. 1998 Jul 15;51(2):243-50. doi: 10.1006/geno.1998.5348.

Abstract

The human X chromosome is known to contain several disease genes yet to be cloned. In the course of a project aimed at the construction of a transcription map of the Xp22 region, we fully characterized a novel cDNA, Cxorf5 (HGMW-approved symbol, alias 71-7A), previously mapped to this region but for which no sequence information was available. We isolated and sequenced the full-length transcript, which encodes a predicted protein of unknown function containing a large number of coiled-coild domains, typically presented in a variety of different molecules, from fibrous proteins to transcription factors. We showed that the Cxorf5 cDNA is ubiquitously expressed, undergoes alternative splicing, and escapes X inactivation. Furthermore, we precisely mapped two additional Cxorf5-related loci on the Y chromosome and on chromosome 5. By virtue of its mapping assignment to the Xp22 region, Cxorf5 represents a candidate gene for at least four human diseases, namely spondyloepiphiseal dysplasia late, oral-facial-digital syndrome type 1, craniofrontonasal syndrome, and a nonsyndromic sensorineural deafness.

摘要

已知人类X染色体包含几个尚未克隆的疾病基因。在构建Xp22区域转录图谱的项目过程中,我们对一个新的cDNA(Cxorf5,HGMW批准符号,别名71 - 7A)进行了全面表征,该cDNA先前已定位到该区域,但尚无序列信息。我们分离并测序了全长转录本,其编码一种功能未知的预测蛋白,该蛋白含有大量卷曲螺旋结构域,这些结构域通常存在于从纤维蛋白到转录因子等多种不同分子中。我们发现Cxorf5 cDNA在全身广泛表达,经历可变剪接,并且逃避X染色体失活。此外,我们在Y染色体和5号染色体上精确地定位了另外两个与Cxorf5相关的基因座。鉴于其定位到Xp22区域,Cxorf5代表了至少四种人类疾病的候选基因,即晚发性脊椎骨骺发育不良、1型口面指综合征、颅额鼻综合征和一种非综合征性感音神经性耳聋。

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