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A biopsy sample reduction approach to identify significant alterations of the testicular transcriptome in the presence of Y-chromosomal microdeletions that are independent of germ cell composition

机译:一种活检样本减少方法,可在不依赖生殖细胞组成的Y染色体微缺失的情况下,识别睾丸转录组的显着变化

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Y-chromosomal microdeletions (YCMD) are the major genetic cause of male infertility. To date, it is not known which global changes are induced by the presence of AZFc or AZFb + c deletions in the human testicular transcriptome. We investigated this question by microarray analysis in which we had to eliminate the ‘germ cell effect’, i.e., the dominating effect of germ cell transcripts due to the quantitative difference in germ cell composition in samples with/without YCMD. This problem was tackled by selecting 26 samples from an initial cohort of 34 samples by their homogeneity in respect to cellular composition as obtained from gene expression clustering. This way, the ‘germ cell effect’ was minimized, and a distinct ‘deletion effect’ became more apparent. Several hundred genes are influenced by YCMD as shown on the three different phenotypes hypospermatogenesis, meiotic arrest, and Sertoli-cell only syndrome. We validated on an independent cohort of samples five genes by quantitative real-time PCR that are expressed in germ cells or the somatic compartment and which are exclusively altered by the presence of YCMD. We conclude that the deletion of Y-chromosomal genes has a significant effect on spermatogenesis by modulating the transcriptional network of the germ cell and somatic compartment.
机译:Y染色体微缺失(YCMD)是男性不育的主要遗传原因。迄今为止,尚不清楚人类睾丸转录组中AZFc或AZFb + c缺失的存在引起了哪些总体变化。我们通过微阵列分析调查了这个问题,其中我们必须消除“生殖细胞效应”,即由于有/无YCMD的样品中生殖细胞成分的数量差异,生殖细胞转录本的主要作用。通过从34个样本的初始队列中选择26个样本来解决此问题,这些样本均相对于从基因表达聚类获得的细胞组成具有同质性。这样,“生殖细胞效应”被最小化,独特的“删除效应”变得更加明显。 YCMD影响了数百个基因,如以下三种不同的表型:生精不足,减数分裂停滞和仅支持细胞综合征。我们通过定量实时PCR在一个样本的独立队列中验证了五个基因,这些基因在生殖细胞或体细胞区室中表达,并且仅因YCMD的存在而改变。我们的结论是,通过调节生殖细胞和体细胞室的转录网络,Y染色体基因的缺失对精子发生有重要影响。

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