Altered Actin Dynamics in Cell Migration of GNE Mutant Cells

Altered Actin Dynamics in Cell Migration of GNE Mutant Cells

Cell migration is an essential cellular process that requires coordination of cytoskeletal dynamics, reorganization, and signal transduction. The actin cytoskeleton is central in maintaining the cellular structure as well as regulating the mechanisms of cell motility. Glycosylation, particularly sia...

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Published in:Frontiers in cell and developmental biology Vol. 9; p. 603742
Main Authors: Devi, Shamulailatpam Shreedarshanee, Yadav, Rashmi, Arya, Ranjana
Format: Journal Article
Language:English
Published: Switzerland Frontiers Media S.A 18-03-2021
Subjects:
actin dynamics
Cell and Developmental Biology
cell migration
cofilin
GNE myopathy
RhoA
sialylation
cell migration
actin dynamics
sialylation
GNE myopathy
cofilin
RhoA
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Summary:Cell migration is an essential cellular process that requires coordination of cytoskeletal dynamics, reorganization, and signal transduction. The actin cytoskeleton is central in maintaining the cellular structure as well as regulating the mechanisms of cell motility. Glycosylation, particularly sialylation of cell surface proteins like integrins, regulates signal transduction from the extracellular matrix to the cytoskeletal network. The activation of integrin by extracellular cues leads to recruitment of different focal adhesion complex proteins (Src, FAK, paxillin, etc.) and activates the signal including Rho GTPases for the regulation of actin assembly and disassembly. During cell migration, the assembly and disassembly of actin filament provides the essential force for the cell to move. Abnormal sialylation can lead to actin signaling dysfunction leading to aberrant cell migration, one of the main characteristics of cancer and myopathies. In the present study, we have reported altered F-actin to G-actin ratios in GNE mutated cells. These cells exhibit pathologically relevant mutations of GNE (UDP N-acetylneuraminic 2-epimerase/N-acetylmannosamine kinase), a key sialic acid biosynthetic enzyme. It was found that GNE neither affects the actin polymerization nor binds directly to actin. However, mutation in GNE resulted in increased binding of α-actinin to actin filaments. Further, through confocal imaging, GNE was found to be localized in focal adhesion complex along with paxillin. We further elucidated that mutation in GNE resulted in upregulation of RhoA protein and Cofilin activity is downregulated, which could be rescued with Rhosin and chlorogenic acid, respectively. Lastly, mutant in GNE reduced cell migration as implicated from wound healing assay. Our study indicates that molecules altering Cofilin function could significantly revert the cell migration defect due to GNE mutation in sialic acid-deficient cells. We propose cytoskeletal proteins to be alternate drug targets for disorders associated with GNE such as GNE myopathy.
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This article was submitted to Cell Adhesion and Migration, a section of the journal Frontiers in Cell and Developmental Biology
Edited by: Shamik Sen, Indian Institute of Technology Bombay, India
Reviewed by: Nagaraj Balasubramanian, Indian Institute of Science Education and Research, Pune, India; Ramray Bhat, Indian Institute of Science (IISc), India
ISSN:2296-634X
2296-634X
DOI:10.3389/fcell.2021.603742