Semantic Scholar Open Access 2016 47 sitasi

Liprin-α1 and ERC1 control cell edge dynamics by promoting focal adhesion turnover

V. Astro D. Tonoli S. Chiaretti Sabrina Badanai Kristyna Sala +2 lainnya

Lihat Sumber DOI

Abstrak

Liprin-α1 and ERC1 are interacting scaffold proteins regulating the motility of normal and tumor cells. They act as part of plasma membrane-associated platforms at the edge of motile cells to promote protrusion by largely unknown mechanisms. Here we identify an amino-terminal region of the liprin-α1 protein (liprin-N) that is sufficient and necessary for the interaction with other liprin-α1 molecules. Similar to liprin-α1 or ERC1 silencing, expression of the liprin-N negatively affects tumor cell motility and extracellular matrix invasion, acting as a dominant negative by interacting with endogenous liprin-α1 and causing the displacement of the endogenous ERC1 protein from the cell edge. Interfering with the localization of ERC1 at the cell edge inhibits the disassembly of focal adhesions, impairing protrusion. Liprin-α1 and ERC1 proteins colocalize with active integrin β1 clusters distinct from those colocalizing with cytoplasmic focal adhesion proteins and influence the localization of peripheral Rab7-positive endosomes. We propose that liprin-α1 and ERC1 promote protrusion by displacing cytoplasmic adhesion components to favour active integrin internalization into Rab7-positive endosomes.

Topik & Kata Kunci

Medicine Biology

Penulis (7)

V. Astro

D. Tonoli

S. Chiaretti

Sabrina Badanai

Kristyna Sala

M. Zerial

I. de Curtis

Format Sitasi

APA MLA BibTeX

Astro, V., Tonoli, D., Chiaretti, S., Badanai, S., Sala, K., Zerial, M. et al. (2016). Liprin-α1 and ERC1 control cell edge dynamics by promoting focal adhesion turnover. https://doi.org/10.1038/srep33653

Akses Cepat

Lihat di Sumber doi.org/10.1038/srep33653

Informasi Jurnal

Tahun Terbit: 2016
Bahasa: en
Total Sitasi: 47×
Sumber Database: Semantic Scholar
DOI: 10.1038/srep33653
Akses: Open Access ✓