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A novel role of vitronectin in promoting survival of mesenchymal stem cells under serum deprivation stress.

Umesh Goyal, Malancha Ta

Stem cell research & therapy 2020 May 19


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  • apoptosis (4)
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  • g0 phase (1)
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  • mesenchymal stem cells (9)
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  • VTN (14)
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    Due to their immunomodulatory and trophic support functions, mesenchymal stem cells (MSCs) are promising in the field of cell-based regenerative medicine. However, MSC survival post-transplantation is challenged by various microenvironment stress factors. Here, we investigated the role of vitronectin (VTN) in the survival strategy of MSCs under serum deprivation stress condition. Proliferation kinetics and cell adhesion of MSCs under serum deprivation were determined from population doublings and cell-matrix de-adhesion studies, respectively. mRNA and protein expression levels of VTN were confirmed by qRT-PCR and Western blotting, respectively. Immunofluorescence technique revealed distribution of VTN under serum deprivation stress. siRNA and inhibitor-based studies were performed to confirm the role and regulation of VTN. Apoptosis and cell cycle status of MSCs were assessed using flow cytometric analysis. Subjecting MSCs to serum deprivation led to significant increase in cell spread area and cell-matrix adhesion. An upregulation of VTN expression was noted with an arrest in G0/G1 phase of cell cycle and no appreciable apoptotic change. Pro-survival PI3kinase pathway inhibition led to further increase in VTN expression with no apoptotic change. siRNA-mediated inhibition of VTN resulted in reversal in G0/G1 cell cycle arrest and a marked increase in apoptosis, suggesting a role of VTN in preventing serum deprivation-induced apoptotic cell death. In addition, p65 knockdown resulted in downregulation of VTN establishing an association between NF-κβ pathway and VTN. VTN was identified as a survival factor in providing protection from serum deprivation-induced apoptosis in MSCs.

    Citation

    Umesh Goyal, Malancha Ta. A novel role of vitronectin in promoting survival of mesenchymal stem cells under serum deprivation stress. Stem cell research & therapy. 2020 May 19;11(1):181

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    PMID: 32429996

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