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Spermatogonial stem cell autotransplantation and germline genomic editing: a future cure for spermatogenic failure and prevention of transmission of genomic diseases

机译:精原干细胞自体移植和种系基因组编辑:生精失败和预防基因组疾病传播的未来疗法

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摘要

BACKGROUNDSubfertility affects approximately 15% of all couples, and a severe male factor is identified in 17% of these couples. While the etiology of a severe male factor remains largely unknown, prior gonadotoxic treatment and genomic aberrations have been associated with this type of subfertility. Couples with a severe male factor can resort to ICSI, with either ejaculated spermatozoa (in case of oligozoospermia) or surgically retrieved testicular spermatozoa (in case of azoospermia) to generate their own biological children. Currently there is no direct treatment for azoospermia or oligozoospermia. Spermatogonial stem cell (SSC) autotransplantation (SSCT) is a promising novel clinical application currently under development to restore fertility in sterile childhood cancer survivors. Meanwhile, recent advances in genomic editing, especially the clustered regulatory interspaced short palindromic repeats-associated protein 9 (CRISPR-Cas9) system, are likely to enable genomic rectification of human SSCs in the near future.
机译:背景生育力影响所有夫妇中约15%,在这些夫妇中有17%发现了严重的男性因素。虽然严重的男性因素的病因学仍然未知,但先前的性腺毒性治疗和基因组畸变与这种类型的不育有关。患有严重男性因素的夫妇可以诉诸ICSI,通过射精的精子(如果是少精子症)或通过手术取回睾丸的精子(如果是无精子症)来生自己的亲生孩子。目前尚无直接治疗无精症或少精症的方法。精原干细胞(SSC)自体移植(SSCT)是一种有前途的新颖临床应用,目前正在开发中,以恢复无菌儿童期癌症幸存者的生育能力。同时,基因组编辑的最新进展,尤其是簇状调控间隔的短回文重复相关蛋白9(CRISPR-Cas9)系统,很可能在不久的将来使人类SSC的基因组校正成为可能。

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