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Perivascular Mesenchymal Stem/Stromal Cells, an Immune Privileged Niche for Viruses?

Journal

Publisher

MDPI
DOI: 10.3390/ijms23148038

Keywords

immunity; mesenchymal stem cells; stromal cells; fibroblast; pericytes; virus; persistence; chronic inflammation; innate immunity; immune-regulation; neural crest; COVID-19; chikungunya

Funding

  1. Regional Council of La Reunion, French State [GURDTI 2017-1198-0002583, CPER-FEDER 20192211-0022768]
  2. Regional Council of La Reunion, Europe [GURDTI 2017-1198-0002583, CPER-FEDER 20192211-0022768]

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Mesenchymal stem cells (MSCs) play a critical role in response to infection and can remove cell debris, regulate immune activities, control pathogens, and contribute to tissue remodeling. However, chronic infection and inflammation can affect the functions and immune regulatory activities of MSCs.
Mesenchymal stem cells (MSCs) play a critical role in response to stress such as infection. They initiate the removal of cell debris, exert major immunoregulatory activities, control pathogens, and lead to a remodeling/scarring phase. Thus, host-derived 'danger' factors released from damaged/infected cells (called alarmins, e.g., HMGB1, ATP, DNA) as well as pathogen-associated molecular patterns (LPS, single strand RNA) can activate MSCs located in the parenchyma and around vessels to upregulate the expression of growth factors and chemoattractant molecules that influence immune cell recruitment and stem cell mobilization. MSC, in an ultimate contribution to tissue repair, may also directly trans- or de-differentiate into specific cellular phenotypes such as osteoblasts, chondrocytes, lipofibroblasts, myofibroblasts, Schwann cells, and they may somehow recapitulate their neural crest embryonic origin. Failure to terminate such repair processes induces pathological scarring, termed fibrosis, or vascular calcification. Interestingly, many viruses and particularly those associated to chronic infection and inflammation may hijack and polarize MSC's immune regulatory activities. Several reports argue that MSC may constitute immune privileged sanctuaries for viruses and contributing to long-lasting effects posing infectious challenges, such as viruses rebounding in immunocompromised patients or following regenerative medicine therapies using MSC. We will herein review the capacity of several viruses not only to infect but also to polarize directly or indirectly the functions of MSC (immunoregulation, differentiation potential, and tissue repair) in clinical settings.

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