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Optogenetic Modulation of Neural Progenitor Cells Improves Neuroregenerative Potential
Authors:Esther Giraldo  David Palmero-Canton  Beatriz Martinez-Rojas  Maria del Mar Sanchez-Martin  Victoria Moreno-Manzano
Affiliation:1.Neuronal and Tissue Regeneration Laboratory, Centro de Investigación Príncipe Felipe, 46012 Valencia, Spain; (E.G.); (D.P.-C.); (B.M.-R.); (M.d.M.S.-M.);2.Department of Biotechnology, Universitat Politècnica de València, 46022 Valencia, Spain
Abstract:Neural progenitor cell (NPC) transplantation possesses enormous potential for the treatment of disorders and injuries of the central nervous system, including the replacement of lost cells or the repair of host neural circuity after spinal cord injury (SCI). Importantly, cell-based therapies in this context still require improvements such as increased cell survival and host circuit integration, and we propose the implementation of optogenetics as a solution. Blue-light stimulation of NPCs engineered to ectopically express the excitatory light-sensitive protein channelrhodopsin-2 (ChR2-NPCs) prompted an influx of cations and a subsequent increase in proliferation and differentiation into oligodendrocytes and neurons and the polarization of astrocytes from a pro-inflammatory phenotype to a pro-regenerative/anti-inflammatory phenotype. Moreover, neurons derived from blue-light-stimulated ChR2-NPCs exhibited both increased branching and axon length and improved axon growth in the presence of axonal inhibitory drugs such as lysophosphatidic acid or chondroitin sulfate proteoglycan. Our results highlight the enormous potential of optogenetically stimulated NPCs as a means to increase neuroregeneration and improve cell therapy outcomes for enhancing better engraftments and cell identity upon transplantation in conditions such as SCI.
Keywords:spinal cord injury   neural progenitor cells   optogenetics   channelrhodopsin-2   cell therapy   neural differentiation   axon growth   astrocyte activation
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