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PU.1(Sfpi1),一种从胚胎发育早期就开始表达的多效性调节因子,在生发祖细胞中具有关键作用。

PU.1 (Sfpi1), a pleiotropic regulator expressed from the first embryonic stages with a crucial function in germinal progenitors.

作者信息

Olive Virginie, Wagner Nicole, Chan Susan, Kastner Philippe, Vannetti Christine, Cuzin François, Rassoulzadegan Minoo

机构信息

Inserm U636, F-06108, Nice, France.

出版信息

Development. 2007 Nov;134(21):3815-25. doi: 10.1242/dev.003467. Epub 2007 Oct 3.

Abstract

In the adult mammalian testis, spermatogenic differentiation starts from a minute population of spermatogonial stem cells (SSCs). SSCs are generated after birth from the fetal gonocytes, themselves derived from the primordial germ cells (PGCs), which are specified during the first days after implantation. Transcriptome profiling of purified preparations evidenced the preferential accumulation in SSCs of transcripts of PU.1 (Sfpi1), a regulatory gene previously identified in hematopoietic progenitors. In situ immunolabeling and RNA determination showed a complex pattern of expression in the adult testis, first in SSCs and early spermatogonia followed by de novo expression in pachytene spermatocytes. Spermatogenesis in a null mutant (PU.1(G/G)) was arrested at the prenatal stage, with reduced numbers of gonocytes owing to a defect in proliferation already noticeable at E12.5. Transcripts of several germinal markers, including vasa (Mvh, Ddx4), Oct4 (Pou5f1), Dazl and Taf4b, were detected, whereas stella (PGC7, Dppa3) was not. Germ cells of PU.1(G/G) newborn testes grafted in nude mice did not initiate the postnatal replicative stage, whereas grafts of their wild-type littermates underwent complete spermatogenesis. During embryonic development, PU.1 transcription was initiated as early as the blastocyst stage, with a generalized expression at E6.5 in the embryonic ectoderm. PU.1 therefore appears to play a determinant role in at least two distinct lineages and, given its wide range of expression, possibly in other stem cells.

摘要

在成年哺乳动物睾丸中,生精分化始于少量精原干细胞(SSCs)。SSCs在出生后由胎儿生殖母细胞产生,而胎儿生殖母细胞本身源自原始生殖细胞(PGCs),PGCs在植入后的头几天就已确定。对纯化制剂的转录组分析表明,PU.1(Sfpi1)转录本在SSCs中优先积累,PU.1是先前在造血祖细胞中鉴定出的一个调控基因。原位免疫标记和RNA测定显示,PU.1在成年睾丸中的表达模式复杂,首先在SSCs和早期精原细胞中表达,随后在粗线期精母细胞中重新表达。在一个基因敲除突变体(PU.1(G/G))中,精子发生在产前阶段就停止了,由于在E12.5时就已明显出现的增殖缺陷,生殖母细胞数量减少。检测到了几种生殖标记物的转录本,包括vasa(Mvh,Ddx4)、Oct4(Pou5f1)、Dazl和Taf4b,而stella(PGC7,Dppa3)未被检测到。移植到裸鼠体内的PU.1(G/G)新生睾丸的生殖细胞没有进入出生后的复制阶段,而其野生型同窝小鼠的移植睾丸则经历了完整的精子发生过程。在胚胎发育过程中,PU.1转录最早在囊胚期开始,在E6.5时在胚胎外胚层广泛表达。因此,PU.1似乎在至少两个不同的细胞谱系中发挥决定性作用,鉴于其广泛的表达范围,它可能也在其他干细胞中发挥作用。

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