Dipartimento di Biologia, Università di Pisa, Pisa 56100, Italy.
Proc Natl Acad Sci U S A. 2009 Dec 15;106(50):21179-84. doi: 10.1073/pnas.0909167106. Epub 2009 Nov 24.
Cell identity is acquired in different brain structures according to a stereotyped timing schedule, by accommodating the proliferation of multipotent progenitor cells and the generation of distinct types of mature nerve cells at precise times. However, the molecular mechanisms coupling the identity of a specific neuron and its birth date are poorly understood. In the neural retina, only late progenitor cells that divide slowly can become bipolar neurons, by the activation of otx2 and vsx1 genes. In Xenopus, we found that Xotx2 and Xvsx1 translation is inhibited in early progenitor cells that divide rapidly by a set of cell cycle-related microRNAs (miRNAs). Through expression and functional screenings, we selected 4 miRNAs--mir-129, mir-155, mir-214, and mir-222--that are highly expressed at early developmental stages in the embryonic retina and bind to the 3' UTR of Xotx2 and Xvsx1 mRNAs inhibiting their translation. The functional inactivation of these miRNAs in vivo releases the inhibition, supporting the generation of additional bipolar cells. We propose a model in which the proliferation rate and the age of a retinal progenitor are linked to each other and determine the progenitor fate through the activity of a set of miRNAs.
细胞身份是根据一个刻板的时间时间表在不同的大脑结构中获得的,通过适应多能祖细胞的增殖和在精确的时间产生不同类型的成熟神经细胞。然而,将特定神经元的身份与其出生日期联系起来的分子机制还知之甚少。在神经视网膜中,只有增殖缓慢的晚期祖细胞才能通过激活 otx2 和 vsx1 基因成为双极神经元。在非洲爪蟾中,我们发现一组与细胞周期相关的 microRNAs(miRNAs)抑制了快速分裂的早期祖细胞中 Xotx2 和 Xvsx1 的翻译。通过表达和功能筛选,我们选择了 4 种 miRNA--mir-129、mir-155、mir-214 和 mir-222--它们在胚胎视网膜的早期发育阶段高度表达,并与 Xotx2 和 Xvsx1 mRNA 的 3'UTR 结合,抑制其翻译。这些 miRNA 在体内的功能失活释放了抑制作用,支持产生额外的双极细胞。我们提出了一个模型,其中视网膜祖细胞的增殖率和年龄相互关联,并通过一组 miRNAs 的活性决定祖细胞的命运。