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Publication : N-cadherin can structurally substitute for E-cadherin during intestinal development but leads to polyp formation.

First Author  Libusova L Year  2010
Journal  Development Volume  137
Issue  14 Pages  2297-305
PubMed ID  20534673 Mgi Jnum  J:161852
Mgi Id  MGI:4461819 Doi  10.1242/dev.048488
Citation  Libusova L, et al. (2010) N-cadherin can structurally substitute for E-cadherin during intestinal development but leads to polyp formation. Development 137(14):2297-305
abstractText  We conditionally substituted E-cadherin (E-cad; cadherin 1) with N-cadherin (N-cad; cadherin 2) during intestine development by generating mice in which an Ncad cDNA was knocked into the Ecad locus. Mutant mice were born, demonstrating that N-cad can structurally replace E-cad and establish proper organ architecture. After birth, mutant mice gradually developed a mutant phenotype in both the small and large intestine and died at ~2-3 weeks of age, probably due to malnutrition during the transition to solid food. Molecular analysis revealed an extended domain of cells from the crypt into the villus region, with nuclear localization of beta-catenin (beta-cat; Ctnnb1) and enhanced expression of several beta-cat target genes. In addition, the BMP signaling pathway was suppressed in the intestinal epithelium of the villi, suggesting that N-cad might interfere with BMP signaling in the intestinal epithelial cell layer. Interestingly, mutant mice developed severe dysplasia and clusters of cells with neoplastic features scattered along the crypt-villus axis in the small and large intestine. Our experimental model indicates that, in the absence of E-cad, the sole expression of N-cad in an epithelial environment is sufficient to induce neoplastic transformations.
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