AGG interspersion pattern

  • 文章类型: Journal Article
    背景:脆性X信使核糖核蛋白1(FMR1)基因的前突变,定义为55和200CGG之间,与脆性X相关的原发性卵巢功能不全(FXPOI)有关。只有20%的女性前突变携带者出现早期排卵功能障碍,这种不完整的外显率的原因是未知的。本研究在前突变等位基因中验证了数学模型,在分配每个等位基因后,一个代表等位基因复杂性的分数。随后,等位基因评分用于调查先前发表的58例前突变病例(116个等位基因)的等位基因复杂性对闭经时年龄的影响.
    方法:使用我们组先前描述的公式确定等位基因评分。使用Pearson检验分析每个等位基因评分对闭经年龄的影响,并生成等高线图以可视化效果。
    结果:等位基因评分的相关性揭示了前突变等位基因中两种不同的复杂性行为。在闭经时,前突变等位基因的等位基因评分与年龄之间没有显着相关性。关于正常大小的等位基因,观察到同样缺乏显著的相关性,尽管有一个几乎显著的趋势。
    结论:我们的结果表明,等位基因评分组合的使用有可能解释女性不孕症,即FXPOI的发展,或卵巢功能障碍,尽管闭经与年龄缺乏相关性。这一发现对于早期识别有排卵障碍风险的女性具有重要的临床意义。加强生育力保存技术,并增加具有前突变的女性成功怀孕的可能性。额外的调查是必要的,以验证这一假设。
    BACKGROUND: Premutations in the Fragile X Messenger Ribonucleoprotein 1 (FMR1) gene, defined as between 55 and 200 CGGs, have been implicated in fragile X-associated primary ovarian insufficiency (FXPOI). Only 20% of female premutation carriers develop early ovulatory dysfunction, the reason for this incomplete penetrance is unknown. This study validated the mathematical model in premutation alleles, after assigning each allele a score representing allelic complexity. Subsequently, allelic scores were used to investigate the impact of allele complexity on age at amenorrhea for 58 premutation cases (116 alleles) previously published.
    METHODS: The allelic score was determined using a formula previously described by our group. The impact of each allelic score on age at amenorrhea was analyzed using Pearson\'s test and a contour plot generated to visualize the effect.
    RESULTS: Correlation of allelic score revealed two distinct complexity behaviors in premutation alleles. No significant correlation was observed between the allelic score of premutation alleles and age at amenorrhea. The same lack of significant correlation was observed regarding normal-sized alleles, despite a nearly significant trend.
    CONCLUSIONS: Our results suggest that the use of allelic scores combination have the potential to explain female infertility, namely the development of FXPOI, or ovarian dysfunction, despite the lack of correlation with age at amenorrhea. Such a finding is of great clinical significance for early identification of females at risk of ovulatory dysfunction, enhancement of fertility preservation techniques, and increasing the probability for a successful pregnancy in females with premutations. Additional investigation is necessary to validate this hypothesis.
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  • 文章类型: Journal Article
    FMR1基因5'UTR中的多态三核苷酸重复区包含AGG穿插,特别是在正常大小的等位基因中(CGG<45)。在此范围内,重复拉伸通常会中断一次或两次,尽管也可以观察到没有或具有三个或更多个AGG穿插的等位基因。AGG穿插与重复区的总长度一起赋予稳定性并阻碍扩展到致病范围:前突变(55200)。AGG的散布早已被认定为FMR1重复稳固性的最重要特征之一,对于确定女性前突变携带者的扩展风险估计尤为重要。我们试图计算组合的AGG穿插数量和模式,旨在定义FMR1重复道复杂性组合。一个数学模型,第一个计算这种累积效应的人,使用来自131名年轻健康女性的数据进行开发和验证。对其等位基因复杂性的作图能够鉴定两个统计学上不同的组-等效和不相似的等位基因组合。结果,指定等位基因得分的数值参数,描绘了每个等位基因的重复亚结构,测量FMR1基因的等位基因复杂性,包括AGGs负担,从而允许对女性正常大小的等位基因进行新的行为审查。
    The polymorphic trinucleotide repetitive region in the FMR1 gene 5\'UTR contains AGG interspersions, particularly in normal-sized alleles (CGG < 45). In this range repetitive stretches are typically interrupted once or twice, although alleles without or with three or more AGG interspersions can also be observed. AGG interspersions together with the total length of the repetitive region confer stability and hinder expansion to pathogenic ranges: either premutation (55 < CGG < 200) or full mutation (CGG > 200). The AGG interspersions have long been identified as one of the most important features of FMR1 repeat stability, being particularly important to determine expansion risk estimates in female premutation carriers. We sought to compute the combined AGG interspersion numbers and patterns, aiming to define FMR1 repetitive tract complexity combinations. A mathematical model, the first to compute this cumulative effect, was developed and validated using data from 131 young and healthy females. Plotting of their allelic complexity enabled the identification of two statistically distinct groups - equivalent and dissimilar allelic combinations. The outcome, a numerical parameter designated allelic score, depicts the repeat substructure of each allele, measuring the allelic complexity of the FMR1 gene including the AGGs burden, thus allowing new behavioral scrutiny of normal-sized alleles in females.
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