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Cfap97d1 对于鞭毛轴丝的维持和雄性小鼠的生育能力很重要。

Cfap97d1 is important for flagellar axoneme maintenance and male mouse fertility.

机构信息

Research Institute for Microbial Diseases, Osaka University, Suita, Osaka, Japan.

Faculty of Biochemistry and Molecular Medicine, University of Oulu, Oulu, Finland.

出版信息

PLoS Genet. 2020 Aug 12;16(8):e1008954. doi: 10.1371/journal.pgen.1008954. eCollection 2020 Aug.

Abstract

The flagellum is essential for sperm motility and fertilization in vivo. The axoneme is the main component of the flagella, extending through its entire length. An axoneme is comprised of two central microtubules surrounded by nine doublets, the nexin-dynein regulatory complex, radial spokes, and dynein arms. Failure to properly assemble components of the axoneme in a sperm flagellum, leads to fertility alterations. To understand this process in detail, we have defined the function of an uncharacterized gene, Cfap97 domain containing 1 (Cfap97d1). This gene is evolutionarily conserved in mammals and multiple other species, including Chlamydomonas. We have used two independently generated Cfap97d1 knockout mouse models to study the gene function in vivo. Cfap97d1 is exclusively expressed in testes starting from post-natal day 20 and continuing throughout adulthood. Deletion of the Cfap97d1 gene in both mouse models leads to sperm motility defects (asthenozoospermia) and male subfertility. In vitro fertilization (IVF) of cumulus-intact oocytes with Cfap97d1 deficient sperm yielded few embryos whereas IVF with zona pellucida-free oocytes resulted in embryo numbers comparable to that of the control. Knockout spermatozoa showed abnormal motility characterized by frequent stalling in the anti-hook position. Uniquely, Cfap97d1 loss caused a phenotype associated with axonemal doublet heterogeneity linked with frequent loss of the fourth doublet in the sperm stored in the epididymis. This study demonstrates that Cfap97d1 is required for sperm flagellum ultra-structure maintenance, thereby playing a critical role in sperm function and male fertility in mice.

摘要

鞭毛对于精子的运动和体内受精至关重要。轴丝是鞭毛的主要组成部分,贯穿其全长。轴丝由两个中央微管组成,周围环绕着九个双联微管、连接蛋白-动力蛋白调节复合物、放射辐条和动力蛋白臂。如果精子鞭毛中的轴丝组件不能正确组装,就会导致生育能力改变。为了详细了解这个过程,我们定义了一个未被表征的基因 Cfap97 结构域包含 1(Cfap97d1)的功能。该基因在哺乳动物和包括衣藻在内的多种其他物种中具有进化保守性。我们使用两种独立生成的 Cfap97d1 敲除小鼠模型来研究体内基因功能。Cfap97d1 从出生后第 20 天开始在睾丸中特异性表达,并持续到成年。在两种小鼠模型中删除 Cfap97d1 基因会导致精子运动缺陷(弱精症)和雄性生育力下降。用 Cfap97d1 缺陷精子进行卵丘完整的体外受精(IVF)产生的胚胎很少,而用透明带去除的卵母细胞进行 IVF 产生的胚胎数量与对照组相当。敲除精子表现出异常的运动特征,即在反钩位置频繁停滞。独特的是,Cfap97d1 的缺失导致了与轴丝双联体异质性相关的表型,这种异质性与附睾中储存的精子中第四双联体的频繁缺失有关。这项研究表明,Cfap97d1 对于精子鞭毛的超微结构维持是必需的,因此在小鼠的精子功能和雄性生育力中发挥着关键作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c7bc/7444823/4d5c009a099d/pgen.1008954.g001.jpg

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