Three novel mutations causing a truncated protein within the RP2 gene in Italian families with X-linked retinitis pigmentosa

Alessandro De Luca , Isabella Torrente , Massimo Mangino , Rita Danesi , Bruno Dallapiccola , Giuseppe Novelli
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引用次数: 6

Abstract

X-linked retinitis pigmentosa (XLRP) results from mutations in a number of loci, including RP2 at Xp11.3, and RP3 at Xp21.1. RP2 and RP3 genes have been identified by positional cloning. RP2 mutations are found in about 10% of XLRP patients. We performed a mutational screening of RP2 gene in patients belonging to seven unrelated families in linkage with the RP2 locus. SSCP analysis detected three conformation variants, within exon 2 and 3. Direct sequencing of exon 2, disclosed a G→A transition at nucleotide 449 (W150X), and a G→T transversion in position 547 (E183X). Sequence analysis of exon 3 variant revealed an insertion (853/854insG), leading to a frameshift. In this patient, we detected an additional sequence alteration (A→G at nucleotide 848, E283G). Each mutation was co-segregating with the disease in the affected family members available for the study. These mutations are expected to introduce a stop codon within the RP2 coding sequence probably resulting in a truncated or unstable protein.

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三种新的突变导致意大利x连锁视网膜色素变性家族中RP2基因内的蛋白截短
x连锁视网膜色素变性(XLRP)是由多个基因座突变引起的,包括Xp11.3位点的RP2和Xp21.1位点的RP3。通过定位克隆鉴定了RP2和RP3基因。在10%的XLRP患者中发现RP2突变。我们对来自7个与RP2位点相关的不相关家族的患者进行了RP2基因的突变筛选。SSCP分析检测到三个构象变异,位于外显子2和3内。直接测序外显子2,发现核苷酸449 (W150X)处有G→a转位,547 (E183X)处有G→T转位。外显子3变异的序列分析显示一个插入(853/854insG),导致移码。在该患者中,我们检测到额外的序列改变(核苷酸848,E283G处A→G)。每个突变都与研究中可用的受影响家庭成员的疾病共分离。这些突变预计会在RP2编码序列中引入一个停止密码子,可能导致截断或不稳定的蛋白质。
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