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Sodium–hydrogen exchanger NHA1 and NHA2 control sperm motility and male fertility

机译:钠 - 氢气交换机NHA1和NHA2控制精子运动和雄性生育

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Our previous work identified NHA1, a testis-specific sodium–hydrogen exchanger, is specifically localized on the principal piece of mouse sperm flagellum. Our subsequent study suggested that the number of newborns and fertility rate of NHA1-vaccinated female mice are significantly stepped down. In order to define the physiological function of NHA1 in spermatozoa, we generated Nha1 Fx/Fx, Zp3 -Cre (hereafter called Nha1 cKO) mice and found that Nha1 cKO males were viable and subfertile with reduced sperm motility. Notably, cyclic AMP (cAMP) synthesis by soluble adenylyl cyclase (sAC) was attenuated in Nha1 cKO spermatozoa and cAMP analogs restored sperm motility. Similar to Nha1 cKO males, Nha2 Fx/Fx, Zp3 -Cre (hereafter called Nha2 cKO) male mice were subfertile, indicating these two Nha genes may be functionally redundant. Furthermore, we demonstrated that male mice lacking Nha1 and Nha2 genes (hereafter called Nha1/2 dKO mice) were completely infertile, with severely diminished sperm motility owing to attenuated sAC-cAMP signaling. Importantly, principal piece distribution of NHA1 in spermatozoa are phylogenetically conserved in spermatogenesis. Collectively, our data revealed that NHA1 and NHA2 function as a key sodium–hydrogen exchanger responsible for sperm motility after leaving the cauda epididymidis.
机译:我们以前的工作确定了NHA1,睾丸特异性钠 - 氢气交换器,专门定位在小鼠精子鞭柱的主要部分上。我们随后的研究表明,NHA1接种母老鼠的新生儿和生育率的数量显着下降。为了在精子中定义NHA1的生理功能,我们产生NHA1 FX / FX / FX,ZP3 -CRE(以下称为NHA1 CKO)小鼠,发现NHA1 CKO男性是可行的,具有减少的精子运动的卵体。值得注意的是,通过可溶性腺苷酸环酶(SAC)合成的循环AMP(CAMP)在NHA1 CKO精子和营地类似物恢复精子运动中衰减。类似于NHA1 CKO男性,NHA2 FX / FX ,ZP3 -CRE(以下称为NHA2 CKO)雄性小鼠是雄性小鼠的,表明这两个NHA基因可以在功能上是多余的。此外,我们证明缺乏NHA1和NHA2基因的雄性小鼠(以下称为NHA1 / 2 DKO小鼠)是完全不孕的,因为由于减弱的囊阵阵营信号传导而严重减少了精子的运动。重要的是,精子中NHA1的主要分配分布在精子发生中文源保守。集体,我们的数据显示,NHA1和NHA2用作留下鲫鱼患者后负责精子运动的关键钠 - 氢气交换剂。

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