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体外人类精子发生的进化途径:下一个目标是什么?

The Evolutionary Route of in vitro Human Spermatogenesis: What is the Next Destination?

机构信息

Department of Stem Cell Sciences, Graduate School of Health Sciences, Hacettepe University, 06100, Ankara, Turkey.

METU MEMS Center, 06530, Ankara, Turkey.

出版信息

Stem Cell Rev Rep. 2024 Aug;20(6):1406-1419. doi: 10.1007/s12015-024-10726-2. Epub 2024 Apr 29.

Abstract

Malfunction in spermatogenesis due to genetic diseases, trauma, congenital disorders or gonadotoxic treatments results in infertility in approximately 7% of males. The behavior of spermatogonial stem cells (SSCs) within three-dimensional, multifactorial, and dynamic microenvironment implicates a niche that serves as a repository for fertility, since can serve as a source of mature and functional male germ cells. Current protocols enable reprogramming of mature somatic cells into induced pluripotent stem cells (iPSCs) and their limited differentiation to SSCs within the range of 0-5%. However, the resulting human iPSC-derived haploid spermatogenic germ cell yield in terms of number and functionality is currently insufficient for transfer to infertility clinic as a therapeutic tool. In this article, we reviewed the evolution of experimental culture platforms and introduced a novel iPSCs-based approach for in vitro spermatogenesis based on a niche perspective bearing cellular, chemical, and physical factors that provide the complex arrangement of testicular seminiferous tubules embedded within a vascularized stroma. We believe that bioengineered organoids supported by smart bio-printed tubules and microfluidic organ-on-a-chip systems offer efficient, precise, personalized platforms for autologous pluripotent stem cell sources to undergo the spermatogenetic cycle, presenting a promising tool for infertile male patients with complete testicular aplasia.

摘要

由于遗传疾病、创伤、先天性疾病或性腺毒性治疗,精子发生功能障碍导致大约 7%的男性不育。精原干细胞(SSC)在三维、多因素和动态微环境中的行为暗示了一个巢位,作为生育能力的储存库,因为它可以作为成熟和功能正常的雄性生殖细胞的来源。目前的方案能够将成熟的体细胞重编程为诱导多能干细胞(iPSC),并在 0-5%的范围内将其有限地分化为 SSCs。然而,由此产生的人类 iPSC 衍生的单倍体精子发生生殖细胞的数量和功能目前不足以作为治疗工具转移到不孕不育诊所。在本文中,我们回顾了实验培养平台的发展,并介绍了一种基于巢位的新型 iPSC 体外精子发生方法,该方法基于细胞、化学和物理因素,提供了包含在血管化基质中的睾丸曲细精管的复杂排列。我们相信,由智能生物打印管和微流控器官上芯片系统支持的生物工程类器官为自体多能干细胞来源提供了高效、精确、个性化的平台,使其能够经历精子发生周期,为完全睾丸发育不全的男性不育患者提供了一种有前途的工具。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/39e8/11319530/a2b54e1361fa/12015_2024_10726_Fig1_HTML.jpg

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