含有38的卷曲螺旋结构域是小鼠顶体生物发生和纤维鞘组装所必需的。

Yaling Wang, Xueying Huang, Guoying Sun, Jingwen Chen, Bangguo Wu, Jiahui Luo, Shuyan Tang, Peng Dai, Feng Zhang, Jinsong Li, Lingbo Wang
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引用次数: 0

摘要

在精子发生过程中,单倍体精子细胞发生显著的形态变化,形成细长的精子鞭毛和帽状顶体,这是成功受精所必需的。鞭毛的严重畸形会导致男性不育综合征,鞭毛的多种形态异常(MMAF),而顶体发育不全在某些情况下会导致胚胎发育潜能低下。然而,关于MMAF顶体发育不全发生的证据有限。在这里,我们报道了通过诱导无义突变而敲除含有卷曲线圈结构域38(Ccdc38)的碱基编辑小鼠的一代,并发现雄性不育。Ccdc38KO精子表现出顶体发育不全和典型的MMAF表型。我们发现,在Ccdc38KO精子中,顶体膜松散地固定在细胞核上,纤维鞘紊乱。进一步的分析表明,Ccdc38敲除导致睾丸中与顶体生物发生相关的蛋白质TEKT3水平降低,并导致TEKT3在精子中的异常分布。我们最终证明细胞质内精子注射可以克服与Ccdc38相关的不孕。因此,我们的研究揭示了CCDC38在顶体生物发生中先前未知的作用,并为MMAF中顶体发育不全的发生提供了额外的证据。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Coiled-coil domain-containing 38 is required for acrosome biogenesis and fibrous sheath assembly in mice.

Coiled-coil domain-containing 38 is required for acrosome biogenesis and fibrous sheath assembly in mice.

During spermiogenesis, haploid spermatids undergo dramatic morphological changes to form slender sperm flagella and cap-like acrosomes, which are required for successful fertilization. Severe deformities in flagella cause a male infertility syndrome, multiple morphological abnormalities of the flagella (MMAF), while acrosomal hypoplasia in some cases leads to sub-optimal embryonic developmental potential. However, evidence regarding the occurrence of acrosomal hypoplasia in MMAF is limited. Here, we report the generation of base-edited mice knocked out for coiled-coil domain-containing 38 (Ccdc38) via inducing a nonsense mutation and find that the males are infertile. The Ccdc38-KO sperm display acrosomal hypoplasia and typical MMAF phenotypes. We find that the acrosomal membrane is loosely anchored to the nucleus and fibrous sheaths are disorganized in Ccdc38-KO sperm. Further analyses reveal that Ccdc38 knockout causes a decreased level of TEKT3, a protein associated with acrosome biogenesis, in testes and an aberrant distribution of TEKT3 in sperm. We finally show that intracytoplasmic sperm injection overcomes Ccdc38-related infertility. Our study thus reveals a previously unknown role for CCDC38 in acrosome biogenesis and provides additional evidence for the occurrence of acrosomal hypoplasia in MMAF.

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