| Literature DB >> 31826865 |
Rebecca McLennan1, Mary C McKinney1, Jessica M Teddy1, Jason A Morrison1, Jennifer C Kasemeier-Kulesa1, Dennis A Ridenour1, Craig A Manthe1, Rasa Giniunaite2, Martin Robinson2,3, Ruth E Baker2, Philip K Maini2, Paul M Kulesa4,5.
Abstract
Neural crest migration requires cells to move through an environment filled with dense extracellular matrix and mesoderm to reach targets throughout the vertebrate embryo. Here, we use high-resolution microscopy, computational modeling, and in vitro and in vivo cell invasion assays to investigate the function of Aquaporin 1 (AQP-1) signaling. We find that migrating lead cranial neural crest cells express AQP-1 mRNA and protein, implicating a biological role for water channel protein function during invasion. Differential AQP-1 levels affect neural crest cell speed and direction, as well as the length and stability of cell filopodia. Furthermore, AQP-1 enhances matrix metalloprotease activity and colocalizes with phosphorylated focal adhesion kinases. Colocalization of AQP-1 with EphB guidance receptors in the same migrating neural crest cells has novel implications for the concept of guided bulldozing by lead cells during migration.Entities:
Keywords: Cell invasion; Filopodia; Neural crest; Water channel
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Year: 2020 PMID: 31826865 DOI: 10.1242/dev.185231
Source DB: PubMed Journal: Development ISSN: 0950-1991 Impact factor: 6.868