Semantic Scholar Open Access 1997 1321 sitasi

Regulation of Cell Motility by Mitogen-activated Protein Kinase

R. Klemke S. Cai A. Giannini P. Gallagher P. de Lanerolle +1 lainnya

Lihat Sumber DOI

Abstrak

Cell interaction with adhesive proteins or growth factors in the extracellular matrix initiates Ras/ mitogen-activated protein (MAP) kinase signaling. Evidence is provided that MAP kinase (ERK1 and ERK2) influences the cells' motility machinery by phosphorylating and, thereby, enhancing myosin light chain kinase (MLCK) activity leading to phosphorylation of myosin light chains (MLC). Inhibition of MAP kinase activity causes decreased MLCK function, MLC phosphorylation, and cell migration on extracellular matrix proteins. In contrast, expression of mutationally active MAP kinase kinase causes activation of MAP kinase leading to phosphorylation of MLCK and MLC and enhanced cell migration. In vitro results support these findings since ERK-phosphorylated MLCK has an increased capacity to phosphorylate MLC and shows increased sensitivity to calmodulin. Thus, we define a signaling pathway directly downstream of MAP kinase, influencing cell migration on the extracellular matrix.

Topik & Kata Kunci

Medicine Biology

Penulis (6)

R. Klemke

S. Cai

A. Giannini

P. Gallagher

P. de Lanerolle

D. Cheresh

Format Sitasi

APA MLA BibTeX

Klemke, R., Cai, S., Giannini, A., Gallagher, P., Lanerolle, P.d., Cheresh, D. (1997). Regulation of Cell Motility by Mitogen-activated Protein Kinase. https://doi.org/10.1083/JCB.137.2.481

Akses Cepat

Lihat di Sumber doi.org/10.1083/JCB.137.2.481

Informasi Jurnal

Tahun Terbit: 1997
Bahasa: en
Total Sitasi: 1321×
Sumber Database: Semantic Scholar
DOI: 10.1083/JCB.137.2.481
Akses: Open Access ✓