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不育患者的精子在与精子发生相关过程中表现出DNA甲基化差异:基于芯片的分析

Spermatozoa from infertile patients exhibit differences of DNA methylation associated with spermatogenesis-related processes: an array-based analysis.

作者信息

Camprubí Cristina, Salas-Huetos Albert, Aiese-Cigliano Riccardo, Godo Anna, Pons Maria-Carme, Castellano Giancarlo, Grossmann Mark, Sanseverino Walter, Martin-Subero José I, Garrido Nicolás, Blanco Joan

机构信息

Genetics of Male Fertility Group, Unitat de Biologia Cel⋅lular (Facultat de Biociències), Universitat Autònoma de Barcelona, Bellaterra (Cerdanyola del Vallès) 08193, Spain.

Sequentia Biotech, Edifici CRAG, Campus UAB, Bellaterra (Cerdanyola del Vallès) 08193, Spain.

出版信息

Reprod Biomed Online. 2016 Dec;33(6):709-719. doi: 10.1016/j.rbmo.2016.09.001. Epub 2016 Sep 15.

Abstract

The influence of aberrant sperm DNA methylation on the reproductive capacity of couples has been postulated as a cause of infertility. This study compared the DNA methylation of spermatozoa of 19 fertile donors and 42 infertile patients using the Illumina 450K array. Clustering analysis of methylation data arranged fertile and infertile patients into two groups. Bivariate clustering analysis identified a differential distribution of samples according to the characteristics of seminogram and age, suggesting a possible link between these parameters and specific methylation profiles. The study identified 696 differentially methylated cytosine-guanine dinucleotides (CpG) associated with 501 genes between fertile donors and infertile patients. Ontological enrichment analysis revealed 13 processes related to spermatogenesis. Data filtering identified a set of 17 differentially methylated genes, some of which had functions relating to spermatogenesis. A significant association was identified between RPS6KA2 hypermethylation and advanced age (P = 0.016); APCS hypermethylation and oligozoospermia (P = 0.041); JAM3/NCAPD3 hypermethylation and numerical chromosome sperm anomalies (P = 0.048); and ANK2 hypermethylation and lower pregnancy rate (P = 0.040). This description of a set of differentially methylated genes provides a framework for further investigation into the influence of such variation in male fertility in larger patient cohorts.

摘要

异常精子DNA甲基化对夫妇生殖能力的影响已被假定为不孕的一个原因。本研究使用Illumina 450K芯片比较了19名有生育能力的供者和42名不育患者精子的DNA甲基化情况。甲基化数据的聚类分析将有生育能力者和不育患者分为两组。双变量聚类分析根据精液分析特征和年龄确定了样本的差异分布,表明这些参数与特定甲基化谱之间可能存在联系。该研究在有生育能力的供者和不育患者之间鉴定出696个与501个基因相关的差异甲基化胞嘧啶-鸟嘌呤二核苷酸(CpG)。本体富集分析揭示了13个与精子发生相关的过程。数据筛选确定了一组17个差异甲基化基因,其中一些基因具有与精子发生相关的功能。研究发现RPS6KA2高甲基化与高龄显著相关(P = 0.016);APCS高甲基化与少精子症显著相关(P = 0.041);JAM3/NCAPD3高甲基化与精子染色体数目异常显著相关(P = 0.048);ANK2高甲基化与较低的妊娠率显著相关(P = 0.040)。这组差异甲基化基因的描述为进一步研究此类变异在更大患者队列中对男性生育力的影响提供了框架。

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