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Common AZFc structure may possess the optimal spermatogenesis efficiency relative to the rearranged structures mediated by non-allele homologous recombination

机译:相对于由非等位基因同源重组介导的重排结构常见的AZFc结构可能具有最佳的精子发生效率

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摘要

The azoopsermia factor c (AZFc) region of human Y-chromosome is an essential genomic segment for spermatogenesis with frequent non-allele homologous recombination (NAHR). Recent case-control studies on the association of the NAHR-based AZFc structural mutations with spermatogenic failure produced inconsistent results. To more precisely evaluate their spermatogenesis effects, we investigated the correlation between the subdivided AZFc mutations and sperm production in 3,439 Han Chinese males. Our results showed that both partial AZFc deletion-only and primary duplication mutation presented a significant risk for decreased sperm production. Restoration of the reduced dosage of the AZFc content to the normal level had a milder effect, whereas an overdose of the AZFc content arising from multiple duplications of a partial AZFc-deleted structure produced a more serious consequence compared to the partial deletion-only mutation. Additionally, the AZFc-mutated structures with excessive NAHR-substrate showed a notably negative effect on spermatogenesis. These results suggest that the recurrent NAHR-based AZFc mutations may be associated with decreased spermatogenesis efficiency in present population. More significantly, our finding implies that the overdose of AZFc NAHR-substrate may produce an additional risk for the massive AZFbc deletions during the multi-stage division process of germ cells and thus impair the global spermatogenesis efficiency in the carriers.
机译:人Y染色体的无精症因子c(AZFc)区是精子发生的必需基因组片段,具有频繁的非等位基因同源重组(NAHR)。最近关于基于NAHR的AZFc结构突变与生精失败相关的病例对照研究产生了不一致的结果。为了更准确地评估其精子发生效果,我们调查了3439名汉族男性中细分的AZFc突变与精子产生之间的相关性。我们的结果表明,仅部分AZFc缺失和原发性复制突变均表现出降低精子产生的显着风险。将减少剂量的AZFc含量恢复至正常水平具有较温和的作用,而与仅部分缺失的突变相比,由部分重复的AZFc缺失的结构的多次重复产生的过量的AZFc含量产生了更严重的后果。另外,具有过量NAHR底物的AZFc突变结构显示出对精子发生的显着负面影响。这些结果表明,复发的基于NAHR的AZFc突变可能与当前人群精子发生效率降低有关。更重要的是,我们的发现暗示过量剂量的AZFc NAHR底物可能在生殖细胞的多阶段分裂过程中产生大量AZFbc缺失的额外风险,从而损害了载体中的整体精子发生效率。

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