Foregut separation and tracheo-oesophageal malformations: The role of tracheal outgrowth, dorso-ventral patterning and programmed cell death

Ioannides, Adonis S.; Massa, Valentina; Ferraro, Elisabetta; Cecconi, Francesco; Spitz, Lewis; Henderson, Deborah J.; Copp, Andrew J.

doi:10.1016/j.ydbio.2009.11.005

Cited by 55 publications

(82 citation statements)

References 51 publications

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“…Dynamic ventral-dorsal shift in Shh signaling is required for the onset of tracheo-esophageal separation and foregut morphogenesis. Spatio-temporal disruption or shift of Shh expression is frequently associated with diminished apoptosis of the lateral epithelial ridges and the failure of tracheo-esophageal separation [Ioannides et al, 2010]. In absence of Shh, mice display a spectrum of foregut malformations, including lung hypoplasia and various defects in the trachea and esophagus.…”

Section: Tracheoesophageal Fistulamentioning

confidence: 99%

Sonic Hedgehog Signaling and VACTERL Association

Ngan¹,

Kim

Hui

2012

Mol Syndromol

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Hedgehog (Hh) signaling is vital for the patterning and organogenesis of almost every system. The specificity of these developmental processes is achieved through a tight spatio-temporal regulation of Hh signaling. Mice with defective Hh signal exhibit a wide spectrum of anomalies, including Vertebral defects, Anal atresia, Cardiovascular anomalies, Tracheoesophageal fistula, Renal dysplasia, and Limb defects, that resemble strikingly the phenotypes observed in VACTERL association in humans. In this review, we summarize our current understanding of mammalian Hh signaling and highlight the relevance of various mouse models for studying the etiology and pathogenesis of VACTERL association. In addition, recent advances in genetic study for unraveling the complexity of genetic inheritance of VACTERL and the implication of the Sonic hedgehog pathway in disease pathogenesis are also discussed.

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Section: Tracheoesophageal Fistulamentioning

confidence: 99%

Sonic Hedgehog Signaling and VACTERL Association

Ngan¹,

Kim

Hui

2012

Mol Syndromol

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“…The trachea and lung both arise from an Nkx2-1 þ region of the foregut and presumably from a common progenitor population (reviewed in Cardoso and Lu, 2006). However, the trachea does not undergo branching morphogenesis, rather it separates from the future esophagus by means of a process of septation (Ioannides et al, 2010). Indeed after the initial specification of the Nkx2-1 þ anterior foregut domain, the lung and trachea have somewhat different patterns of gene expression.…”

Section: An Overview Of Lung Developmentmentioning

confidence: 99%

The building blocks of mammalian lung development

Rawlins

2010

Developmental Dynamics

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Progress has recently been made in identifying progenitor cell populations in the embryonic lung. Some progenitor cell types have been definitively identified by lineage-tracing studies. However, others are not as well characterized and their existence is inferred on the basis of lung morphology, or mutant phenotypes. Here, I focus on lung development after the specification of the initial lung primordium. The evidence for various lung embryonic progenitor cell types is discussed and future experiments are suggested. The regulation of progenitor proliferation in the embryonic lung, and its coordinate control with morphogenesis, is also discussed. In addition, the relationship between embryonic and adult lung progenitors is considered. Developmental Dynamics 240:463-476,

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“…In mice, Sox2 is required for normal morphogenesis and homeostasis of diverse tissues, including neural stem cells; retinal stem cells taste buds; hair sensory follicles in the ear; and epithelia of trachea, lung, and esophagus (15)(16)(17)(18). In humans, Sox2 mutations are associated with eye and tracheal/esophageal malformations (18)(19)(20). Recent studies demonstrated that Sox2 is amplified in human lung and esophageal squamous cell carcinomas (21)(22)(23).…”

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confidence: 99%