| Literature DB >> 26012633 |
Runchi Gao1, Siwei Zhao2, Xupin Jiang3, Yaohui Sun4, Sanjun Zhao5, Jing Gao5, Jane Borleis6, Stacey Willard6, Ming Tang6, Huaqing Cai6, Yoichiro Kamimura6, Yuesheng Huang3, Jianxin Jiang3, Zunxi Huang7, Alex Mogilner8, Tingrui Pan2, Peter N Devreotes6, Min Zhao9.
Abstract
Directional cell migration in an electric field, a phenomenon called galvanotaxis or electrotaxis, occurs in many types of cells, and may play an important role in wound healing and development. Small extracellular electric fields can guide the migration of amoeboid cells, and we established a large-scale screening approach to search for mutants with electrotaxis phenotypes from a collection of 563 Dictyostelium discoideum strains with morphological defects. We identified 28 strains that were defective in electrotaxis and 10 strains with a slightly higher directional response. Using plasmid rescue followed by gene disruption, we identified some of the mutated genes, including some previously implicated in chemotaxis. Among these, we studied PiaA, which encodes a critical component of TORC2, a kinase protein complex that transduces changes in motility by activating the kinase PKB (also known as Akt). Furthermore, we found that electrotaxis was decreased in mutants lacking gefA, rasC, rip3, lst8, or pkbR1, genes that encode other components of the TORC2-PKB pathway. Thus, we have developed a high-throughput screening technique that will be a useful tool to elucidate the molecular mechanisms of electrotaxis.Entities:
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Year: 2015 PMID: 26012633 PMCID: PMC4470479 DOI: 10.1126/scisignal.aab0562
Source DB: PubMed Journal: Sci Signal ISSN: 1945-0877 Impact factor: 8.192