EGL-27 is similar to a metastasis-associated factor and controls cell polarity and cell migration in C. elegans

Mutations in the C. elegans gene egl-27 cause defects in cell polarity and cell migration: the polarity of the asymmetric T cell division is disrupted and the descendants of the migratory QL neuroblast migrate incorrectly because they fail to express the Hox gene mab-5. Both of these processes are k...

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Veröffentlicht in:Development (Cambridge) 1999-03, Vol.126 (5), p.1055-1064
Hauptverfasser: Herman, M A, Ch'ng, Q, Hettenbach, S M, Ratliff, T M, Kenyon, C, Herman, R K
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Sprache:eng
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Zusammenfassung:Mutations in the C. elegans gene egl-27 cause defects in cell polarity and cell migration: the polarity of the asymmetric T cell division is disrupted and the descendants of the migratory QL neuroblast migrate incorrectly because they fail to express the Hox gene mab-5. Both of these processes are known to be controlled by Wnt pathways. Mosaic analysis indicates that egl-27 function is required in the T cell for proper cell polarity. We cloned egl-27 and discovered that a domain of the predicted EGL-27 protein has similarity to Mta1, a mammalian factor overexpressed in metastatic cells. Overlaps in the phenotypes of egl-27 and Wnt pathway mutants suggest that the EGL-27 protein interacts with Wnt signaling pathways in C. elegans.
ISSN:0950-1991
1477-9129
DOI:10.1242/dev.126.5.1055