Detailed Study of HPRT1 Gross Deletions Found in 10 Italian Lesch-Nyhan Families

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Abstract

Background: Lesch-Nyhan disease (LND) is an X-linked rare pathology involving the purine nucleotides salvage pathway. Its incidence is estimated in 1:350.000 born. The condition is due to mutations in the HPRT1 (hypoxanthine phosphoribosyl transferase 1) gene of which in our cohort 28% (10/35) are large deletions. In order to better assess the nature of the observed deletions in our LND population we analyzed 10 families carrying large deletions in the HPRT1 gene region and studied the underlying pathogenic mechanisms. Methods: We performed PCR based localization of the break points and sequenced the gap-junction fragments. Bioinformatics analysis was performed through several web tools on the 5’ and 3’ break points to determine the factors involved in the deletion mechanism. Results: We precisely mapped 10 unique large deletions involving the HPRT1 gene region that span from 300 bp to 64 kbp. No common breakpoints were found and each deletion appears to be family specific. Conclusions: The deletions in the HPRT1 gene area are consistent with the Micro homology-Mediated Break-Induced Replication (MMBIR) mechanism. There are strong links with Alu-s and no recurrent break points with all of the observed deletions being unique. The relatively large amount of deletions in the HPRT1 region is peculiar and linked with the almost absolute lack of polymorphic sites in the HPRT1 gene making it a very interesting region for further studies.
意大利10个Lesch-Nyhan家族HPRT1基因缺失的详细研究
背景:Lesch-Nyhan病(LND)是一种涉及嘌呤核苷酸挽救途径的x连锁罕见病理。其发病率估计为1:35万。这种情况是由于HPRT1(次黄嘌呤磷酸核糖基转移酶1)基因的突变,在我们的队列中28%(10/35)是大缺失。为了更好地评估LND人群中观察到的缺失的性质,我们分析了10个携带HPRT1基因区域大缺失的家庭,并研究了潜在的致病机制。方法:采用PCR方法对断裂点进行定位,并对间隙连接片段进行测序。通过几种网络工具对5 '和3 '断点进行生物信息学分析,以确定涉及删除机制的因素。结果:我们精确定位了涉及HPRT1基因区域的10个独特的大缺失,范围从300 bp到64 kbp。没有发现共同的断点,而且每个删除似乎都是特定于家族的。结论:HPRT1基因区域的缺失符合微同源介导的断裂诱导复制(MMBIR)机制。与Alu-s有很强的联系,并且所有观察到的缺失都是唯一的,没有重复的断点。HPRT1区域相对大量的缺失是特殊的,并且与HPRT1基因中几乎绝对缺乏多态性位点有关,使其成为一个非常有趣的区域,值得进一步研究。
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