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  The late endosomal p14-MP1 (LAMTOR2/3) complex regulates focal adhesion dynamics during cell migration

Schiefermeier, N., Scheffler, J. M., de Araujo, M. E. G., Stasyk, T., Yordanov, T., Ebner, H. L., et al. (2014). The late endosomal p14-MP1 (LAMTOR2/3) complex regulates focal adhesion dynamics during cell migration. JOURNAL OF CELL BIOLOGY, 205(4), 525-540.

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 Creators:
Schiefermeier, Natalia, Author
Scheffler, Julia M., Author
de Araujo, M. E. G., Author
Stasyk, T., Author
Yordanov, T., Author
Ebner, H. L., Author
Offterdinger, M., Author
Munck, S., Author
Hess, M. W., Author
Wickström, S. A.1, Author           
Lange, A., Author
Wunderlich, W., Author
Faessler, R., Author
Teis, D., Author
Huber, L. A., Author
Affiliations:
1Wickström – Skin Homeostasis and Ageing, Max Planck Research Groups, Max Planck Institute for Biology of Ageing, Max Planck Society, ou_1942298              

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Free keywords: ADP-Ribosylation Factors/metabolism Adaptor Proteins, Signal Transducing/genetics/*metabolism Animals Cell Line Cell Movement/*physiology Endosomes/*metabolism Fibroblasts/cytology Focal Adhesions/*metabolism HeLa Cells Humans Mice Mice, 129 Strain Mice
 Abstract: Cell migration is mediated by the dynamic remodeling of focal adhesions (FAs). Recently, an important role of endosomal signaling in regulation of cell migration was recognized. Here, we show an essential function for late endosomes carrying the p14-MP1 (LAMTOR2/3) complex in FA dynamics. p14-MP1-positive endosomes move to the cell periphery along microtubules (MTs) in a kinesin1- and Arl8b-dependent manner. There they specifically target FAs to regulate FA turnover, which is required for cell migration. Using genetically modified fibroblasts from p14-deficient mice and Arl8b-depleted cells, we demonstrate that MT plus end-directed traffic of p14-MP1-positive endosomes triggered IQGAP1 disassociation from FAs. The release of IQGAP was required for FA dynamics. Taken together, our results suggest that late endosomes contribute to the regulation of cell migration by transporting the p14-MP1 scaffold complex to the vicinity of FAs.

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Language(s): eng - English
 Dates: 2014
 Publication Status: Issued
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 Rev. Type: -
 Identifiers: ISSN: 1540-8140 (Electronic)0021-9525 (Linking)
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Title: JOURNAL OF CELL BIOLOGY
Source Genre: Journal
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Pages: - Volume / Issue: 205 (4) Sequence Number: - Start / End Page: 525 - 540 Identifier: -