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Wnt2/2b and beta-catenin signaling are necessary and sufficient to specify lung progenitors in the foregut.


ABSTRACT: Patterning of the primitive foregut promotes appropriate organ specification along its anterior-posterior axis. However, the molecular pathways specifying foregut endoderm progenitors are poorly understood. We show here that Wnt2/2b signaling is required to specify lung endoderm progenitors within the anterior foregut. Embryos lacking Wnt2/2b expression exhibit complete lung agenesis and do not express Nkx2.1, the earliest marker of the lung endoderm. In contrast, other foregut endoderm-derived organs, including the thyroid, liver, and pancreas, are correctly specified. The phenotype observed is recapitulated by an endoderm-restricted deletion of beta-catenin, demonstrating that Wnt2/2b signaling through the canonical Wnt pathway is required to specify lung endoderm progenitors within the foregut. Moreover, activation of canonical Wnt/beta-catenin signaling results in the reprogramming of esophagus and stomach endoderm to a lung endoderm progenitor fate. Together, these data reveal that canonical Wnt2/2b signaling is required for the specification of lung endoderm progenitors in the developing foregut.

SUBMITTER: Goss AM 

PROVIDER: S-EPMC2763331 | biostudies-literature | 2009 Aug

REPOSITORIES: biostudies-literature

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Wnt2/2b and beta-catenin signaling are necessary and sufficient to specify lung progenitors in the foregut.

Goss Ashley M AM   Tian Ying Y   Tsukiyama Tadasuke T   Cohen Ethan David ED   Zhou Diane D   Lu Min Min MM   Yamaguchi Terry P TP   Morrisey Edward E EE  

Developmental cell 20090801 2


Patterning of the primitive foregut promotes appropriate organ specification along its anterior-posterior axis. However, the molecular pathways specifying foregut endoderm progenitors are poorly understood. We show here that Wnt2/2b signaling is required to specify lung endoderm progenitors within the anterior foregut. Embryos lacking Wnt2/2b expression exhibit complete lung agenesis and do not express Nkx2.1, the earliest marker of the lung endoderm. In contrast, other foregut endoderm-derived  ...[more]

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