Promote Organization and Integration of Regenerated Neurons from Transplanted Human Neural Stem Cells
促进移植的人类神经干细胞再生神经元的组织和整合
基本信息
- 批准号:9392271
- 负责人:
- 金额:$ 20.44万
- 依托单位:
- 依托单位国家:美国
- 项目类别:
- 财政年份:2017
- 资助国家:美国
- 起止时间:2017-07-01 至 2019-06-30
- 项目状态:已结题
- 来源:
- 关键词:AdhesivesAdoptedAlpha CellAngiogenic FactorAnimalsBindingBiocompatible MaterialsBrainBrain DiseasesBrain InjuriesCell Differentiation processCell SurvivalCell TherapyCell TransplantsCellsCuesDevelopmentDiseaseEncapsulatedEngraftmentEnvironmentEvaluationExhibitsFiberFunctional disorderFutureHumanHyaluronic AcidHydrogelsImpairmentIn VitroInfiltrationInflammationInjuryLamininLeadLesionMediatingModelingModulusNatural regenerationNeurologicNeurological outcomeNeuronal DifferentiationNeuronsOutcomePatientsPatternPeptidesPhasePolymersPorosityRecovery of FunctionReelin Signaling PathwaySiteSpinal cord injuryStem cell transplantStem cellsStrokeStructureStructure-Activity RelationshipSurfaceTestingTherapeuticTimeTissue EngineeringTissuesToxicologyTransplantationTraumatic Brain InjuryTraumatic injuryVascular Endothelial Growth FactorsWorkaxon growthbasebiomaterial compatibilitybrain repairbrain tissuecell motilitycentral nervous system injuryclinical translationdrug discoverydrug testingfunctional improvementhuman fetus tissuehuman pluripotent stem cellimplantationimprovedin vivoinduced pluripotent stem cellinnovationmechanical propertiesmigrationnanofiberneovascularnerve stem cellneural circuitneuronal growthpolycaprolactoneregenerativerelating to nervous systemrepairedresponsescaffoldscreeningstem cell differentiationsuccessthree dimensional cell culturethree-dimensional modelingtissue regenerationtissue repair
项目摘要
PROJECT SUMMARY
The overall objective of this project is to develop a nanofiber-hydrogel composite that is capable of organizing
differentiated cells from the transplanted human pluripotent stem cell (hiPSC)-derived neural/progenitor stem
cells (NSCs) at the lesion site following brain injury, and enhancing the integration of the regenerated neurons
with host tissue. A growing body of evidences has suggested exogenous stem cell transplantation is one
promising strategy to promote injured brain tissue regeneration. However, the ongoing inflammation at the
lesion site and the lack of supportive tissue structure and vasculature within the traumatic lesion cavity present
a hostile environment that result in low cell survival and poor control over differentiation and engraftment of the
transplanted stem cells. We have recently shown that an optimized hyaluronic acid (HA) hydrogel conjugated
with laminin-derived peptide as a cell-delivery matrix with the ability to bind and enrich the endogenous
angiogenic factors, such as vascular endothelial growth factor, generated a robust neovascular network within
the hydrogel at the traumatic lesion cavity. Human fetal tissue-derived NSCs delivered in this HA hydrogel
have shown enhanced survival following implantation at the lesion site, and the majority of survived NSCs has
differentiated into neuronal progenitors and populated the entire lesion cavity. However, these neuronal
progenitors exhibited disorganized structure at the lesion site with limited integration with host cortex tissue.
Since an ordered and layered structure is important to the function of the brain cortex, control over cell
organization and integration following NSC transplantation and differentiation at the lesion site is critical to the
success of stem cell-based therapy for brain injury. Here we hypothesize that the differentiated cells from
transplanted hiPSC-derived NSCs can be guided to form aligned and organized structure by a 3D nanofiber-
hydrogel composite in brain lesion site, which in turn facilitates the integration of the regenerated neurons with
host tissue. To test this hypothesis, we will first develop a nanofiber-hydrogel composite with aligned
nanofibers and demonstrate its ability to organize NSCs during differentiation and maturation. The nanofiber-
hydrogel composite will be tailored with adhesive cues, optimized pore size and modulus to support human
iPSC-derived NSCs in directing their migration and promoting their differentiation and maturation (Aim 1). We
will then transplant the optimized composite scaffold to demonstrate the advantages of our approach in
promoting structural repair of the brain tissue and ensuing functional improvement in neurological outcomes
(Aim 2). This composite with defined compositions is highly desirable for clinical translation.
项目总结
项目成果
期刊论文数量(0)
专著数量(0)
科研奖励数量(0)
会议论文数量(0)
专利数量(0)
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Hai-Quan Mao其他文献
Hai-Quan Mao的其他文献
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