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Adenovirus-mediated gene delivery into mouse spermatogonial stem cells

机译:腺病毒介导的基因传递到小鼠精原干细胞中

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Spermatogonial stem cells represent a self-renewing population of spermatogonia, and continuous division of these cells supports spermatogenesis throughout the life of adult male animals. Previous attempts to introduce adenovirus vectors into spermatogenic cells, including spermatogonial stem cells, have failed to yield evidence of infection, suggesting that male germ cells may be resistant to adenovirus infection. In this study we show the feasibility of transducing spermatogonial stem cells by adenovirus vectors. When testis cells from ROSA26 Cre reporter mice were incubated in vitro with a Cre-expressing adenovirus vector, Cre-mediated recombination occurred at an efficiency of 49-76%, and the infected spermatogonial stem cells could reinitiate spermatogenesis after transplantation into seminiferous tubules of infertile recipient testes. No evidence of germ-line integration of adenovirus vector could be found in offspring from infected stem cells that underwent Cre-mediated recombination, which suggests that the adenovirus vector infected the cells but did not stably integrate into the germ line. Nevertheless, these results suggest that adenovirus may inadvertently integrate into the patient's germ line and indicate that there is no barrier to adenovirus infection in spermatogonial stem cells.
机译:精原干细胞代表了自我更新的精原细胞群,这些细胞的连续分裂在成年雄性动物的整个生命过程中都支持精子发生。先前将腺病毒载体引入包括生精干细胞在内的生精细胞的尝试均未能获得感染的证据,这表明雄性生殖细胞可能对腺病毒感染具有抵抗力。在这项研究中,我们显示了通过腺病毒载体转导精原干细胞的可行性。当将来自ROSA26 Cre报告基因小鼠的睾丸细胞与表达Cre的腺病毒载体进行体外培养时,Cre介导的重组效率为49-76%,并且感染的精原干细胞可以移植到不育症的生精小管中重新开始生精。收件人睾丸。在经过Cre介导的重组的受感染干细胞的后代中找不到腺病毒载体的种系整合证据,这表明腺病毒载体感染了这些细胞,但没有稳定地整合入种系中。然而,这些结果表明,腺病毒可能会无意间整合到患者的种系中,并表明在精原干细胞中没有腺病毒感染的屏障。

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