特发性矮小症患者SHOX基因启动子突变的功能分析  被引量:9

A functional analysis of short stature homeobox (SHOX) gene promoter mutation in idiopathic short stature

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作  者:董治亚[1] 杜晓飞[2] 王伟[1] 覃克难[2] 肖园[1] 王德芬[1] 

机构地区:[1]上海交通大学医学院附属瑞金医院儿内科 [2]芝加哥大学儿童医院

出  处:《中华内分泌代谢杂志》2009年第2期147-149,共3页Chinese Journal of Endocrinology and Metabolism

基  金:基金项目:上海市人口和计划生育委员会局管科技发展基金项目资助(05JG05007)

摘  要:目的研究矮身材同源盒基因(SHOX)启动子-372G—A突变对其转录活性的影响及机制。方法构建含SHOX基因启动子野生型-372G和-372A纯合突变的荧光素酶报告基因载体,在鸡的软骨细胞中检测其转录活性;PCR扩增产生-372G及-372A转录活性的双链DNA探针,凝胶电泳迁移率(EMSA)检测结合在-400/-290片段的转录因子。结果报告基因结果显示$HOX基因启动子-372A转录活性高于-372G30%(P〈0.01)。EMSA结果显示-372A突变的DNA片段不能与核蛋白结合。结论SHOX基因-372A突变降低核转录因子与其启动子的结合力,增加了启动子的活性,可能与特发性矮小症患者长骨的生长障碍有关。Objective To investigate the effect of short stature homeobox (SHOX) gene promoter -372G →A mutation on the promoter activity and its mechanism. Methods The luciferase report gene vectors containing human SHOX gene promoter -372G or -372A were contructed. Their transcription activities were detected in chicken chondrocytes. Double-stranded DNA probes containing -372G or -372A were produced by PCR, and used for detecting the affinity with nuclear transcription factors by electrophoretic mobility shift assay (EMSA). Results The transcription activity in a -372A promoter construct was significantly higher than that in the wild type -372G ( P〈0.01 ). The result of EMSA showed that -372A gene mutation resulted in loss of the binding affinity to nuclear transcription factors. Conclusion The -372A mutation increases SHOX promoter activity with decreased DNA binding affinity to transcription factors, which may contribute to impaired long bone growth in patients with idiopathic short stature.

关 键 词:特发性矮小症 SHOX基因 功能 多态现象 遗传 

分 类 号:R725.8[医药卫生—儿科] R450[医药卫生—临床医学]

 

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