a) 睪丸重構(gòu)的模式圖��。將新生睪丸中特定細(xì)胞通過(guò)流式分選去掉�,混合攜帶綠色熒光蛋白的該類(lèi)細(xì)胞后進(jìn)行皮下重構(gòu)���,可以研究這類(lèi)細(xì)胞在睪丸重構(gòu)中的作用��。
b) 系統(tǒng)分析c-Kit 陽(yáng)性細(xì)胞在睪丸重構(gòu)中的作用����,發(fā)現(xiàn)c-kit+:CD140a+:F4/80+對(duì)睪丸重構(gòu)起到?jīng)Q定性作用��。
現(xiàn)代社會(huì)�,男性不育問(wèn)題日趨嚴(yán)重。而了解睪丸的發(fā)育,研究精子發(fā)生的過(guò)程則有助于人類(lèi)最終解決這一問(wèn)題��。然而�����,目前缺乏一個(gè)成熟的體外生成精子系統(tǒng)����,這大大阻礙了科學(xué)家們對(duì)精子發(fā)生的研究。李勁松研究組的科研人員張滿等人發(fā)現(xiàn)��,新生的小鼠睪丸細(xì)胞可以在免疫缺陷的小鼠皮下自發(fā)形成類(lèi)睪丸組織���,這種組織不僅具有完整的曲精管結(jié)構(gòu)��,而且曲精管中含有大量的生殖細(xì)胞,從這種組織中分選出的單倍體配子細(xì)胞注射到卵母細(xì)胞中后能夠獲得健康小鼠�。
利用這一系統(tǒng),研究人員通過(guò)結(jié)合流式細(xì)胞分選技術(shù)進(jìn)一步分析了新生小鼠睪丸中c-Kit陽(yáng)性細(xì)胞不同組分在睪丸重構(gòu)中的作用�����。最后發(fā)現(xiàn)��,小鼠睪丸中很少一部分的c-Kit陽(yáng)性細(xì)胞(c-kit+:CD140a+:F4/80+,占新生睪丸細(xì)胞的0.35%)��,即睪丸巨噬細(xì)胞����,對(duì)睪丸皮下重構(gòu)起了決定性的作用。如果缺失這部分細(xì)胞��,睪丸重構(gòu)不能發(fā)生�����。與此同時(shí)�����,研究結(jié)果還顯示���,這些巨噬細(xì)胞在睪丸重構(gòu)過(guò)程中逐漸減少并被受體免疫缺陷小鼠的巨噬細(xì)胞的前體細(xì)胞所取代�。
李勁松研究組的科研人員張滿為本文的第一作者���。參與該研究的合作單位和人員包括中科院健康所時(shí)玉舫研究組��、中科院上海生科院生化與細(xì)胞所王紅艷研究組����、中科院上海生命科學(xué)信息中心李黨生研究員、上?�?萍即髮W(xué)生命科學(xué)與技術(shù)學(xué)院等�����,工作得到了國(guó)家科技部��、國(guó)家基金委���、中國(guó)科學(xué)院(干細(xì)胞先導(dǎo)專(zhuān)項(xiàng))以及上海市科委經(jīng)費(fèi)的支持�����。
原文摘要:
The Roles of Testicular C-kit Positive Cells in De novo Morphogenesis of Testis
Man Zhang, Hai Zhou, Chunxing Zheng, Jun Xiao, Erwei Zuo, Wujuan Liu, Da Xie, Yufang Shi, Chunlian Wu, Hongyan Wang, Dangsheng Li & Jinsong Li
C-kit positive (c-kit+) cells are usual tissue-specific stem cells. However, in postnatal testis, undifferentiated spermatogonial stem cells (SSCs) are c-kit negative (c-kit−) and activation of c-kit represents the start of SSC differentiation, leaving an intriguing question whether other c-kit+ cells exist and participate in the postnatal development of testis. To this end, a feasible system for testicular reconstitution, in which a specific type of cells can be manipulated, is needed. Here, we first establish de novo morphogenesis of testis by subcutaneous injection of testicular cells from neonatal testes into the backs of nude mice. We observe testicular tissue formation and spermatogenesis from all injected sites. importantly, functional spermatids can be isolated from these testicular tissues. Using this system, we systemically analyze the roles of c-kit+ cells in testicular reconstitution and identify a small population of cells (c-kit+:CD140a+:F4/80+), which express typical markers of macrophages, are critical for de novo morphogenesis of testis. Interestingly, we demonstrate that these cells are gradually replaced by peripheral blood cells of recipient mice during the morphogenesis of testis. Thus, we develop a system, which may mimic the complete developmental process of postnatal testis, for investigating the testicular development and spermatogenesis. |
