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绘制小鼠早期发育过程中Wnt11的动态表达以及表达Wnt11的细胞的谱系贡献。

Mapping the dynamic expression of Wnt11 and the lineage contribution of Wnt11-expressing cells during early mouse development.

作者信息

Sinha Tanvi, Lin Lizhu, Li Ding, Davis Jennifer, Evans Sylvia, Wynshaw-Boris Anthony, Wang Jianbo

机构信息

Department of Cell, Developmental and Integrative Biology, University of Alabama at Birmingham, United States.

Skaggs School of Pharmacy and Pharmaceutical Sciences & Department of Medicine, University of California, San Diego, United States.

出版信息

Dev Biol. 2015 Feb 15;398(2):177-92. doi: 10.1016/j.ydbio.2014.11.005. Epub 2014 Nov 20.

Abstract

Planar cell polarity (PCP) signaling is an evolutionarily conserved mechanism that coordinates polarized cell behavior to regulate tissue morphogenesis during vertebrate gastrulation, neurulation and organogenesis. In Xenopus and zebrafish, PCP signaling is activated by non-canonical Wnts such as Wnt11, and detailed understanding of Wnt11 expression has provided important clues on when, where and how PCP may be activated to regulate tissue morphogenesis. To explore the role of Wnt11 in mammalian development, we established a Wnt11 expression and lineage map with high spatial and temporal resolution by creating and analyzing a tamoxifen-inducible Wnt11-CreER BAC (bacterial artificial chromosome) transgenic mouse line. Our short- and long-term lineage tracing experiments indicated that Wnt11-CreER could faithfully recapitulate endogenous Wnt11 expression, and revealed for the first time that cells transiently expressing Wnt11 at early gastrulation were fated to become specifically the progenitors of the entire endoderm. During mid-gastrulation, Wnt11-CreER expressing cells also contribute extensively to the endothelium in both embryonic and extraembryonic compartments, and the endocardium in all chambers of the developing heart. In contrast, Wnt11-CreER expression in the myocardium starts from late-gastrulation, and occurs in three transient, sequential waves: first in the precursors of the left ventricular (LV) myocardium from E7.0 to 8.0; subsequently in the right ventricular (RV) myocardium from E8.0 to 9.0; and finally in the superior wall of the outflow tract (OFT) myocardium from E8.5 to 10.5. These results provide formal genetic proof that the majority of the endocardium and myocardium diverge by mid-gastrulation in the mouse, and suggest a tight spatial and temporal control of Wnt11 expression in the myocardial lineage to coordinate with myocardial differentiation in the first and second heart field progenitors to form the LV, RV and OFT. The insights gained from this study will also guide future investigations to decipher the role of non-canonical Wnt/PCP signaling in endoderm development, vasculogenesis and heart formation.

摘要

平面细胞极性(PCP)信号传导是一种进化上保守的机制,可协调极化细胞行为,以在脊椎动物原肠胚形成、神经管形成和器官发生过程中调节组织形态发生。在非洲爪蟾和斑马鱼中,PCP信号传导由非经典Wnt蛋白(如Wnt11)激活,对Wnt11表达的详细了解为PCP何时、何地以及如何被激活以调节组织形态发生提供了重要线索。为了探究Wnt11在哺乳动物发育中的作用,我们通过创建和分析他莫昔芬诱导型Wnt11-CreER细菌人工染色体(BAC)转基因小鼠品系,建立了具有高时空分辨率的Wnt11表达和谱系图谱。我们的短期和长期谱系追踪实验表明,Wnt11-CreER能够忠实地重现内源性Wnt11的表达,并首次揭示在原肠胚形成早期短暂表达Wnt11的细胞注定会成为整个内胚层的特定祖细胞。在原肠胚形成中期,表达Wnt11-CreER的细胞也广泛地贡献于胚胎和胚外区域的内皮,以及发育中心脏所有腔室的内膜。相比之下,心肌中Wnt11-CreER的表达始于原肠胚形成后期,并以三个短暂的、连续的波出现:首先在E7.0至8.0期间出现在左心室(LV)心肌的前体细胞中;随后在E8.0至9.0期间出现在右心室(RV)心肌中;最后在E8.5至10.5期间出现在流出道(OFT)心肌的上壁中。这些结果提供了正式的遗传学证据,表明在小鼠中,大多数内膜和心肌在原肠胚形成中期开始分化,并提示在心肌谱系中对Wnt11表达进行严格的时空控制,以与第一和第二心脏场祖细胞中的心肌分化相协调,从而形成左心室、右心室和流出道。这项研究获得的见解也将指导未来的研究,以阐明非经典Wnt/PCP信号传导在内胚层发育、血管生成和心脏形成中的作用。

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