The Ras/Raf-1/MEK1/ERK Signaling Pathway Coupled to Integrin Expression Mediates Cholinergic Regulation of Keratinocyte Directional Migration

6533b7ddfe1ef96bd1274a84

RESEARCH PRODUCT

The Ras/Raf-1/MEK1/ERK Signaling Pathway Coupled to Integrin Expression Mediates Cholinergic Regulation of Keratinocyte Directional Migration

Alexander I. Chernyavsky Evert Karlsson Ignaz Wessler Sergei A. Grando Juan Arredondo

subject

Keratinocytes MAPK/ERK pathway Integrins alpha7 Nicotinic Acetylcholine Receptor MAP Kinase Signaling System Integrin MAP Kinase Kinase 1 Receptors Nicotinic Biology Transfection Biochemistry Muscarinic acetylcholine receptor medicine Humans RNA Small Interfering Keratinocyte migration Extracellular Signal-Regulated MAP Kinases Molecular Biology Cells Cultured Chemotaxis Receptor Muscarinic M1 Chemotaxis Cell Biology Acetylcholine Up-Regulation Cell biology Electrophysiology ras Proteins biology.protein raf Kinases Lamellipodium Signal transduction Acetylcholine Signal Transduction medicine.drug

description

The physiologic mechanisms that determine directionality of lateral migration are a subject of intense research. Galvanotropism in a direct current (DC) electric field represents a natural model of cell re-orientation toward the direction of future migration. Keratinocyte migration is regulated through both the nicotinic and muscarinic classes of acetylcholine (ACh) receptors. We sought to identify the signaling pathway mediating the cholinergic regulation of chemotaxis and galvanotropism. The pharmacologic and molecular modifiers of the Ras/Raf-1/MEK1/ERK signaling pathway altered both chemotaxis toward choline and galvanotropism toward the cathode in a similar way, indicating that the same signaling steps were involved. The galvanotropism was abrogated due to inhibition of ACh production by hemicholinium-3 and restored by exogenously added carbachol. The concentration gradients of ACh and choline toward the cathode in a DC field were established by high-performance liquid chromatographic measurements. This suggested that keratinocyte galvanotaxis is, in effect, chemotaxis toward the concentration gradient of ACh, which it creates in a DC field due to its highly positive charge. A time-course immunofluorescence study of the membrane redistribution of ACh receptors in keratinocytes exposed to a DC field revealed rapid relocation to and clustering at the leading edge of alpha7 nicotinic and M(1) muscarinic receptors. Their inactivation with selective antagonists or small interfering RNAs inhibited galvanotropism, which could be prevented by transfecting the cells with constitutively active MEK1. The end-point effect of the cooperative signaling downstream from alpha7 and M(1) through the MEK1/ERK was an up-regulated expression of alpha(2) and alpha(3) integrins, as judged from the results of real-time PCR and quantitative immunoblotting. Thus, alpha7 works together with M(1) to orient a keratinocyte toward direction of its future migration. Both alpha7 and M(1) apparently engage the Ras/Raf/MEK/ERK pathway to up-regulate expression of the "sedentary" integrins required for stabilization of the lamellipodium at the keratinocyte leading edge.

year	journal	country	edition	language
2005-09-10	Journal of Biological Chemistry

https://doi.org/10.1074/jbc.m504407200