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首页> 美国卫生研究院文献>PLoS Genetics >Human Spermatogenic Failure Purges Deleterious Mutation Load from the Autosomes and Both Sex Chromosomes including the Gene DMRT1
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Human Spermatogenic Failure Purges Deleterious Mutation Load from the Autosomes and Both Sex Chromosomes including the Gene DMRT1

机译:人类生精失败会清除常染色体和两性染色体(包括基因DMRT1)带来的有害突变负荷

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Gonadal failure, along with early pregnancy loss and perinatal death, may be an important filter that limits the propagation of harmful mutations in the human population. We hypothesized that men with spermatogenic impairment, a disease with unknown genetic architecture and a common cause of male infertility, are enriched for rare deleterious mutations compared to men with normal spermatogenesis. After assaying genomewide SNPs and CNVs in 323 Caucasian men with idiopathic spermatogenic impairment and more than 1,100 controls, we estimate that each rare autosomal deletion detected in our study multiplicatively changes a man's risk of disease by 10% (OR 1.10 [1.04–1.16], p<2×10−3), rare X-linked CNVs by 29%, (OR 1.29 [1.11–1.50], p<1×10−3), and rare Y-linked duplications by 88% (OR 1.88 [1.13–3.13], p<0.03). By contrasting the properties of our case-specific CNVs with those of CNV callsets from cases of autism, schizophrenia, bipolar disorder, and intellectual disability, we propose that the CNV burden in spermatogenic impairment is distinct from the burden of large, dominant mutations described for neurodevelopmental disorders. We identified two patients with deletions of DMRT1, a gene on chromosome 9p24.3 orthologous to the putative sex determination locus of the avian ZW chromosome system. In an independent sample of Han Chinese men, we identified 3 more DMRT1 deletions in 979 cases of idiopathic azoospermia and none in 1,734 controls, and found none in an additional 4,519 controls from public databases. The combined results indicate that DMRT1 loss-of-function mutations are a risk factor and potential genetic cause of human spermatogenic failure (frequency of 0.38% in 1306 cases and 0% in 7,754 controls, p = 6.2×10−5). Our study identifies other recurrent CNVs as potential causes of idiopathic azoospermia and generates hypotheses for directing future studies on the genetic basis of male infertility and IVF outcomes.
机译:性腺衰竭以及早孕失败和围产期死亡可能是限制有害突变在人群中传播的重要过滤器。我们假设与具有正常精子发生能力的男性相比,具有生精功能受损,遗传结构未知,男性不育的常见原因的男性,富含罕见的有害突变。在对323名特发性生精功能障碍和1100多名对照的白人男性进行全基因组SNP和CNV检测后,我们估计在我们的研究中检测到的每一个罕见的常染色体缺失都会使一个人患病的风险增加10%(OR 1.10 [1.04–1.16], p <2×10 -3 ),稀有的X链CNV降低了29%(或1.29 [1.11-1.50],p <1×10 -3 ),和罕见的Y连锁重复产生88%(或1.88 [1.13-3.13],p <0.03)。通过将我们特定病例的CNV与自闭症,精神分裂症,双相情感障碍和智力残疾病例的CNV呼唤的特征进行对比,我们建议生精障碍中的CNV负担不同于所述的大,显性突变的负担神经发育障碍。我们鉴定了两名患者DMRT1缺失,DMRT1是染色体9p24.3上与禽类ZW染色体系统的假定性别决定基因座同源的基因。在一个独立的汉族男性样本中,我们在979例特发性无精子症中又发现了3个DMRT1缺失,在1,734个对照中没有发现,在公共数据库的4,519个对照中也没有发现。综合结果表明,DMRT1功能丧失突变是人类生精失败的危险因素和潜在遗传原因(1306例患者的发生频率为0.38%,7,754名对照中为0%,p = 6.2×10 )。我们的研究确定了其他复发性CNVs为特发性无精子症的潜在病因,并提出了假说以指导男性不育症和IVF结果的遗传基础上的未来研究。

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