A new mutation at exon 2 of hprt1 locus causing lesch-nyhan syndrome.

IF 0.1 Q4 MULTIDISCIPLINARY SCIENCES

Revista Innovaciencia Pub Date : 2015-12-15 DOI:10.15649/2346075x.362

A. Zapata, Adriana Castillo Pico, L. Gusmão, A. Amorim, F. Sanabria

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引用次数: 0

Abstract

Introduction: Lesch-Nyhan sindrome (LNS) is an X-linked recessive inborn error of metabolism, due to deficiency of the enzyme Hypoxanthine-guanine-phosphoribosyl transferase (HGPRT; EC.2.4.2.8) resulting in hyperuricemia, neurological and behavioural disturbances. In the present work, we report the results of the study of a Colombian family, where LNS was previously clinically and biochemically diagnosed. Material and Methods: The full HPRT gene, including 9 exons and 8 introns, was amplified on eight separate DNA fragments. Both strands, forward and reverse, of the amplified DNA fragments were analyzed and the obtained sequences were compared with those deposited at National Center for Biotechnology Information. Results and conclusions: Sequence analysis allowed the detection of new LNS causing mutation, an adenine deletion in exon 2 of HPRT1 gene resulting in a frameshift which determines a premature stop codon. This study, besides adding a new mutation to the already large spectrum of disease causing variation at HPRT, allows therefore providing genetic counseling for the family as well as prenatal diagnosis.

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hprt1基因座外显子2的新突变导致lesch-nyhan综合征。

简介:Lesch-Nyhan综合征(LNS)是一种x连锁的隐性先天代谢错误，由于缺乏次黄嘌呤-鸟嘌呤-磷酸核糖基转移酶(HGPRT;EC.2.4.2.8)导致高尿酸血症、神经和行为障碍。在目前的工作中，我们报告了对一个哥伦比亚家庭的研究结果，在这个家庭中，LNS以前被临床和生化诊断。材料和方法:在8个DNA片段上扩增完整的HPRT基因，包括9个外显子和8个内含子。对扩增的DNA片段的正反两个链进行分析，并与存放在国家生物技术信息中心的序列进行比较。结果和结论:序列分析可以检测到新的LNS引起突变，HPRT1基因外显子2的腺嘌呤缺失导致移码，该移码决定过早停止密码子。这项研究，除了在已经很大的HPRT致病变异谱上增加一个新的突变外，还允许为家庭提供遗传咨询以及产前诊断。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Revista Innovaciencia MULTIDISCIPLINARY SCIENCES-

CiteScore

0.20

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0.00%

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