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Distribution of FMR1 and FMR2 Repeats in Argentinean Patients with Primary Ovarian Insufficiency

机译:阿根廷原发性卵巢功能不全患者中FMR1和FMR2重复序列的分布

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The premutation state of FMR1 (Fragile X Mental Retardation 1) has been associated with primary ovarian insufficiency (POI), and is the most common known genetic cause for 46,XX patients. Nevertheless, very few studies have analyzed its frequency in Latin American populations. Additionally, a relationship between alleles carrying a cryptic microdeletion in the 5’UTR of FMR2 and the onset of POI has only been studied in one population. Our aim was to analyze the incidence of FMR1 premutations and putative microdeletions in exon 1 of FMR2 in a cohort of Argentinean women with POI. We studied 133 patients and 84 controls. Fluorescent PCR was performed, and the FMR2 exon 1 was further sequenced in samples presenting less than 11 repeats. We found the frequency of FMR1 premutations to be 6.7% and 2.9% for familial and sporadic patients, respectively. Among controls, 1/84 women presented a premutation. In addition, although we did not find microdeletions in FMR2 , we observed a change (T >C) adjacent to the repeats in two sisters with POI. Given the repetitive nature of the sequence involved, we could not ascertain whether this represents a single nucleotide polymorphism (SNP) or a deletion. Therefore, a relationship between FMR2 and POI could not be established for our population.
机译:FMR1的突变前状态(脆性X智力低下1)与原发性卵巢功能不全(POI)有关,是46,XX位患者最常见的遗传原因。然而,很少有研究分析其在拉丁美洲人群中的发生率。此外,仅在一个人群中研究了FMR2的5'UTR中携带隐性微缺失的等位基因与POI发作之间的关系。我们的目的是分析一组阿根廷女性POI患者中FMR2突变的FMR1突变和假定的微缺失的发生率。我们研究了133位患者和84位对照。进行了荧光PCR,并且对FMR2外显子1进行了少于11次重复的样品测序。我们发现家族性和散发性患者的FMR1突变频率分别为6.7%和2.9%。在对照组中,有1/84名妇女出现了突变。此外,尽管我们未在FMR2中发现微缺失,但我们观察到两个POI姐妹中重复序列附近的变化(T> C)。鉴于所涉及序列的重复性质,我们无法确定这是一个单核苷酸多态性(SNP)还是缺失。因此,无法为我们的人群建立FMR2和POI之间的关系。

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