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Literature DB >> 29958899

Cadherin-6B proteolytic N-terminal fragments promote chick cranial neural crest cell delamination by regulating extracellular matrix degradation.

Andrew T Schiffmacher¹, Ashrifia Adomako-Ankomah¹, Vivien Xie¹, Lisa A Taneyhill².

Abstract

During epithelial-to-mesenchymal transitions (EMTs), chick cranial neural crest cells simultaneously delaminate from the basement membrane and segregate from the epithelia, in part, via multiple protease-mediated mechanisms. Proteolytic processing of Cadherin-6B (Cad6B) in premigratory cranial neural crest cells by metalloproteinases not only disassembles cadherin-based junctions but also generates shed Cad6B ectodomains or N-terminal fragments (NTFs) that may possess additional roles. Here we report that Cad6B NTFs promote delamination by enhancing local extracellular proteolytic activity around neural crest cells undergoing EMT en masse. During EMT, Cad6B NTFs of varying molecular weights are observed, indicating that Cad6B may be cleaved at different sites by A Disintegrin and Metalloproteinases (ADAMs) 10 and 19 as well as by other matrix metalloproteinases (MMPs). To investigate Cad6B NTF function, we first generated NTF constructs that express recombinant NTFs with similar relative mobilities to those NTFs shed in vivo. Overexpression of either long or short Cad6B NTFs in premigratory neural crest cells reduces laminin and fibronectin levels within the basement membrane, which then facilitates precocious neural crest cell delamination. Zymography assays performed with supernatants of neural crest cell explants overexpressing Cad6B long NTFs demonstrate increased MMP2 activity versus controls, suggesting that Cad6B NTFs promote delamination through a mechanism involving MMP2. Interestingly, this increase in MMP2 does not involve up-regulation of MMP2 or its regulators at the transcriptional level but instead may be attributed to a physical interaction between shed Cad6B NTFs and MMP2. Taken together, these results highlight a new function for Cad6B NTFs and provide insight into how cadherins regulate cellular delamination during normal developmental EMTs as well as aberrant EMTs that underlie human disease.

Entities: CellLine Chemical Disease Gene Species

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Year: 2018 PMID： 29958899 PMCID： PMC6310115 DOI： 10.1016/j.ydbio.2018.06.018

Source DB: PubMed Journal: Dev Biol ISSN： 0012-1606 Impact factor: 3.582

67 in total

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5. Cadherin-6B undergoes macropinocytosis and clathrin-mediated endocytosis during cranial neural crest cell EMT.

Authors: Rangarajan Padmanabhan; Lisa A Taneyhill
Journal: J Cell Sci Date: 2015-03-20 Impact factor: 5.285

Review 6. Should I stay or should I go? Cadherin function and regulation in the neural crest.

Authors: Lisa A Taneyhill; Andrew T Schiffmacher
Journal: Genesis Date: 2017-03-20 Impact factor: 2.487

7. Differential expression of the metalloproteinase MMP3 and the alpha5 integrin subunit in human myometrium at labour.

Authors: Margaret O'Brien; Deirdre O'Shaughnessy; Elodie Ahamide; John J Morrison; Terry J Smith
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8. Cadherin-mediated cell sorting not determined by binding or adhesion specificity.

Authors: Carien M Niessen; Barry M Gumbiner
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9. Cell delamination in the mesencephalic neural fold and its implication for the origin of ectomesenchyme.

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10. The ectodomain of cadherin-11 binds to erbB2 and stimulates Akt phosphorylation to promote cranial neural crest cell migration.

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6 in total

Cadherin-6B proteolytic N-terminal fragments promote chick cranial neural crest cell delamination by regulating extracellular matrix degradation.

1. Inhibition of matrix metalloproteinases enhances in vitro repair of the meniscus.

2. Tools for studying the role of N-cadherin mediated extracellular interaction in neuronal development and function.

3. Potent mechanism-based inhibitors for matrix metalloproteinases.

4. MT2-MMP expression during early avian morphogenesis.

5. Cadherin-6B undergoes macropinocytosis and clathrin-mediated endocytosis during cranial neural crest cell EMT.

Review 6. Should I stay or should I go? Cadherin function and regulation in the neural crest.

7. Differential expression of the metalloproteinase MMP3 and the alpha5 integrin subunit in human myometrium at labour.

8. Cadherin-mediated cell sorting not determined by binding or adhesion specificity.

9. Cell delamination in the mesencephalic neural fold and its implication for the origin of ectomesenchyme.

10. The ectodomain of cadherin-11 binds to erbB2 and stimulates Akt phosphorylation to promote cranial neural crest cell migration.

1. Cadherin-7 mediates proper neural crest cell-placodal neuron interactions during trigeminal ganglion assembly.

Review 2. The road best traveled: Neural crest migration upon the extracellular matrix.

3. The gap junction protein connexin 43 controls multiple aspects of cranial neural crest cell development.

Review 4. Epithelial-to-mesenchymal transition and different migration strategies as viewed from the neural crest.

Review 5. Cellular dynamics of EMT: lessons from live in vivo imaging of embryonic development.

6. Conservation of Epithelial-to-Mesenchymal Transition Process in Neural Crest Cells and Metastatic Cancer.