The Plasma Membrane Ca<sup>2+</sup> Pump PMCA4b Regulates Melanoma Cell Migration Through Remodeling of the Actin Cytoskeleton

We demonstrated that the plasma membrane Ca<sup>2+</sup> ATPase PMCA4b inhibits migration and metastatic activity of BRAF mutant melanoma cells. Actin dynamics are essential for cells to move, invade and metastasize, therefore, we hypothesized that PMCA4b affected cell migration through...

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Main Authors: Randa Naffa, Rita Padányi, Attila Ignácz, Zoltán Hegyi, Bálint Jezsó, Sarolta Tóth, Karolina Varga, László Homolya, Luca Hegedűs, Katalin Schlett, Agnes Enyedi
Format: Article
Language:English
Published: MDPI AG 2021-03-01
Series:Cancers
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Online Access:https://www.mdpi.com/2072-6694/13/6/1354
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Summary:We demonstrated that the plasma membrane Ca<sup>2+</sup> ATPase PMCA4b inhibits migration and metastatic activity of BRAF mutant melanoma cells. Actin dynamics are essential for cells to move, invade and metastasize, therefore, we hypothesized that PMCA4b affected cell migration through remodeling of the actin cytoskeleton. We found that expression of PMCA4b in A375 BRAF mutant melanoma cells induced a profound change in cell shape, cell culture morphology, and displayed a polarized migratory character. Along with these changes the cells became more rounded with increased cell–cell connections, lamellipodia and stress fiber formation. Silencing PMCA4b in MCF-7 breast cancer cells had a similar effect, resulting in a dramatic loss of stress fibers. In addition, the PMCA4b expressing A375 cells maintained front-to-rear Ca<sup>2+</sup> concentration gradient with the actin severing protein cofilin localizing to the lamellipodia, and preserved the integrity of the actin cytoskeleton from a destructive Ca<sup>2+</sup> overload. We showed that both PMCA4b activity and trafficking were essential for the observed morphology and motility changes. In conclusion, our data suggest that PMCA4b plays a critical role in adopting front-to-rear polarity in a normally spindle-shaped cell type through F-actin rearrangement resulting in a less aggressive melanoma cell phenotype.
ISSN:2072-6694