Plasma membrane Ca2+ pump isoform 4 function in cell migration and cancer metastasis

Author:

Naffa Randa1ORCID,Hegedűs Luca2ORCID,Hegedűs Tamás34ORCID,Tóth Sarolta5ORCID,Papp Béla678ORCID,Tordai Attila5ORCID,Enyedi Ágnes45ORCID

Affiliation:

1. Molecular Biology Research Laboratory, School of Medicine The University of Jordan Amman Jordan

2. Department of Thoracic Surgery, Ruhrlandklinik University Clinic Essen Essen Germany

3. Department of Biophysics and Radiation Biology Semmelweis University Budapest Hungary

4. ELKH‐SE Biophysical Virology Research Group Eötvös Loránd Research Network Budapest Hungary

5. Department of Transfusion Medicine Semmelweis University Budapest Hungary

6. Institut National de la Santé et de la Recherche Médicale, Institut de Recherche Saint‐Louis Hôpital Saint‐Louis Paris France

7. Institut de Recherche Saint‐Louis, Hôpital Saint‐Louis Université de Paris Paris France

8. CEA, DRF‐Institut Francois Jacob, Department of Hemato‐Immunology Research Hôpital Saint‐Louis Paris France

Abstract

AbstractThe Ca2+ ion is a universal second messenger involved in many vital physiological functions including cell migration and development. To fulfil these tasks the cytosolic Ca2+ concentration is tightly controlled, and this involves an intricate functional balance between a variety of channels and pumps of the Ca2+ signalling machinery. Among these proteins, plasma membrane Ca2+ ATPases (PMCAs) represent the major high‐affinity Ca2+ extrusion systems in the cell membrane that are effective in maintaining free Ca2+ concentration at exceedingly low cytosolic levels, which is essential for normal cell function. An imbalance in Ca2+ signalling can have pathogenic consequences including cancer and metastasis. Recent studies have highlighted the role of PMCAs in cancer progression and have shown that a particular variant, PMCA4b, is downregulated in certain cancer types, causing delayed attenuation of the Ca2+ signal. It has also been shown that loss of PMCA4b leads to increased migration and metastasis of melanoma and gastric cancer cells. In contrast, an increased PMCA4 expression has been reported in pancreatic ductal adenocarcinoma that coincided with increased cell migration and shorter patient survival, suggesting distinct roles of PMCA4b in various tumour types and/or different stages of tumour development. The recently discovered interaction of PMCAs with basigin, an extracellular matrix metalloproteinase inducer, may provide further insights into our understanding of the specific roles of PMCA4b in tumour progression and cancer metastasis. image

Funder

National Research, Development and Innovation Office

Publisher

Wiley

Subject

Physiology

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