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果蝇胚胎中胚层细胞命运逐步确定的组合信号编码

Combinatorial signaling codes for the progressive determination of cell fates in the Drosophila embryonic mesoderm.

作者信息

Carmena A, Gisselbrecht S, Harrison J, Jiménez F, Michelson A M

机构信息

Centro de Biologia Molecular 'Severo Ochoa', Universidad Autónoma, 28049 Madrid, Spain.

出版信息

Genes Dev. 1998 Dec 15;12(24):3910-22. doi: 10.1101/gad.12.24.3910.

Abstract

Mesodermal progenitors arise in the Drosophila embryo from discrete clusters of lethal of scute (l'sc)-expressing cells. Using both genetic loss-of-function and targeted ectopic expression approaches, we demonstrate here that individual progenitors are specified by the sequential deployment of unique combinations of intercellular signals. Initially, the intersection between the Wingless (Wg) and Decapentaplegic (Dpp) expression domains demarcate an ectodermal prepattern that is imprinted on the adjacent mesoderm in the form of a L'sc precluster. All mesodermal cells within this precluster are competent to respond to a subsequent instructive signal mediated by two receptor tyrosine kinases (RTKs), the Drosophila epidermal growth factor receptor (DER) and the Heartless (Htl) fibroblast growth factor receptor. By monitoring the expression of the diphosphorylated form of mitogen-associated protein kinase (MAPK), we found that these RTKs are activated in small clusters of cells within the original competence domain. Each cluster represents an equivalence group because all members initially resemble progenitors in their expression of both L'sc and mesodermal identity genes. Thus, localized RTK activity induces the formation of mesodermal equivalence groups. The RTKs remain active in the single progenitor that emerges from each cluster under the subsequent inhibitory influence of the neurogenic genes. Moreover, DER and Htl are differentially involved in the specification of particular progenitors. We conclude that distinct cellular identity codes are generated by the combinatorial activities of Wg, Dpp, EGF, and FGF signals in the progressive determination of embryonic mesodermal cells.

摘要

中胚层祖细胞在果蝇胚胎中源自表达“scute致死”(l'sc)的离散细胞簇。我们通过基因功能缺失和靶向异位表达方法证明,单个祖细胞是由细胞间信号独特组合的顺序部署所指定的。最初,无翅(Wg)和五体不全(Dpp)表达域的交集划定了一个外胚层前模式,该模式以L'sc前簇的形式印记在相邻的中胚层上。这个前簇内的所有中胚层细胞都有能力响应由两种受体酪氨酸激酶(RTK)介导的后续诱导信号,即果蝇表皮生长因子受体(DER)和无心脏(Htl)成纤维细胞生长因子受体。通过监测有丝分裂原相关蛋白激酶(MAPK)双磷酸化形式的表达,我们发现这些RTK在原始能力域内的小细胞簇中被激活。每个簇代表一个等效组,因为所有成员最初在L'sc和中胚层身份基因的表达上都类似于祖细胞。因此,局部RTK活性诱导中胚层等效组的形成。在神经源性基因的后续抑制影响下,RTK在从每个簇中出现的单个祖细胞中保持活跃。此外,DER和Htl在特定祖细胞的指定中发挥不同作用。我们得出结论,在胚胎中胚层细胞的逐步确定过程中,Wg、Dpp、EGF和FGF信号的组合活动产生了不同的细胞身份编码。

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