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Primary azoospermia factor C duplication associated with spermatogenic impariment: a case–control study based on Y‐chromosome haplogrouping in a Han Chinese population

单倍群 基因复制 生物 遗传学 男性不育 无精子症因子 无精子症 Y染色体 拷贝数变化 人口 优势比 等位基因 单倍型 不育 基因 内科学 医学 基因组 怀孕 环境卫生
作者
Shengyu Xie,Yongyi Ma,Yunqiang Liu,Dachang Tao,Zhaokun Wang,Yuan Yang
出处
期刊:International Journal of Andrology [Wiley]
卷期号:12 (3): 561-569 被引量:1
标识
DOI:10.1111/andr.13510
摘要

Abstract Background Azoospermia factor C (AZFc) in the male‐specific region of Y‐chromosome (MSY) presents wide structure variation mainly due to frequent non‐allele homologous recombination, leading to significant copy number variation of the AZFc‐linked coding sequences involving in spermatogenesis. A large number of studies had been conducted to investigate the association between AZFc deletions and male infertility in certain Y chromosome genetic backgrounds, however, the influence of primary AZFc duplication on spermatogenesis remained controversial and the cause of the discrepant outcomes is unknown. Methods In the present study, a total of 1,102 unrelated Han Chinese males without any detectable AZF deletions were recruited from 2014 to 2019, including 411 controls with normozoospermia and 691 patients with idiopathic spermatogenic failure. Using multiple paralog ratio tests (PRTs), the structure duplications were classified by the copy number of the AZFc‐linked amplicons and genes. The Y‐chromosome haplogroup (Y‐hg) was categorized by genetyping of MSY‐linked polymorphism loci. The association of primary AZFc duplication with spermatogenic phenotype was investigated in males with the same Y‐hg. Results Within Y‐hg O3 * group, the frequency of the gr/gr duplication in patients is significantly higher than that of controls ( P = 1.29×10 −3 , odds ratio (OR) 7.64, 95% confidence interval (CI) 1.79–32.57). Moreover, Y‐hg O3 * males with the gr/gr duplication presented a significantly lower sperm production compared with non‐AZFc duplicated ones (sperm concentration: P = 1.46×10 −3 ; total sperm count: P = 1.82 ×10 −3 ). The b2/b3 duplication were identified clustered in Y‐hg Cα2*, and the significant difference in the distribution was not observed between patients with spermatogenic failure and controls. Conclusion The results suggest that, in the Han Chinese population, the gr/gr duplication is a predisposing genetic factor for spermatogenic impairment in males harboring Y‐hg O3 * . Meanwhile, the b2/b3 duplication may be fixed on a yet‐unidentified subbranch of Y‐hg Cα2* without significantly deleterious effect on spermatogenesis. Our findings provide evidence that the difference in the Y‐hg composition may cause the discrepancy on the association of AZFc duplication with spermatogenic failure among the studied populations.
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