From Blood to Lesioned Brain: An In Vitro Study on Migration Mechanisms of Human Nasal Olfactory Stem Cells.
Stéphane D GirardIsabelle VirardEmmanuelle LacassagneJean-Michel PaumierHanae LahlouFrançoise JabesYves MolinoDelphine StephanKevin BarangerMaya BelghaziArnaud DevezeMichel KhrestchatiskyEmmanuel NivetFrançois S RomanFrançois FéronPublished in: Stem cells international (2017)
Stem cell-based therapies critically rely on selective cell migration toward pathological or injured areas. We previously demonstrated that human olfactory ectomesenchymal stem cells (OE-MSCs), derived from an adult olfactory lamina propria, migrate specifically toward an injured mouse hippocampus after transplantation in the cerebrospinal fluid and promote functional recoveries. However, the mechanisms controlling their recruitment and homing remain elusive. Using an in vitro model of blood-brain barrier (BBB) and secretome analysis, we observed that OE-MSCs produce numerous proteins allowing them to cross the endothelial wall. Then, pan-genomic DNA microarrays identified signaling molecules that lesioned mouse hippocampus overexpressed. Among the most upregulated cytokines, both recombinant SPP1/osteopontin and CCL2/MCP-1 stimulate OE-MSC migration whereas only CCL2 exerts a chemotactic effect. Additionally, OE-MSCs express SPP1 receptors but not the CCL2 cognate receptor, suggesting a CCR2-independent pathway through other CCR receptors. These results confirm that OE-MSCs can be attracted by chemotactic cytokines overexpressed in inflamed areas and demonstrate that CCL2 is an important factor that could promote OE-MSC engraftment, suggesting improvement for future clinical trials.
Keyphrases
- stem cells
- blood brain barrier
- mesenchymal stem cells
- cerebral ischemia
- endothelial cells
- cell migration
- liver fibrosis
- liver injury
- umbilical cord
- clinical trial
- cell therapy
- cerebrospinal fluid
- drug induced
- induced pluripotent stem cells
- dendritic cells
- pluripotent stem cells
- regulatory t cells
- cell free
- brain injury
- white matter
- cognitive impairment
- randomized controlled trial
- multiple sclerosis
- bone marrow
- resting state
- gene expression
- immune response
- circulating tumor
- copy number
- open label
- functional connectivity
- cord blood
- phase ii
- binding protein