Subacute Transplantation of Native and Genetically Engineered Neural Progenitors Seeded on Microsphere Scaffolds Promote Repair and Functional Recovery After Traumatic Brain Injury

Authors

Nolan B. Skop, Rutgers New Jersey Medical School
Sweta Singh, Rutgers University-Newark
Henri Antikainen, Rutgers University-Newark
Chaitali Saqcena, Rutgers University-Newark
Frances Calderon, Rutgers New Jersey Medical School
Deborah E. Rothbard, Rutgers New Jersey Medical School
Cheul H. Cho, Newark College of Engineering
Chirag D. Gandhi, New York Medical College
Steven W. Levison, Rutgers New Jersey Medical School
Radek Dobrowolski, Rutgers University-Newark

Document Type

Article

Publication Date

2-1-2019

Abstract

There is intense interest and effort toward regenerating the brain after severe injury. Stem cell transplantation after insult to the central nervous system has been regarded as the most promising approach for repair; however, engrafting cells alone might not be sufficient for effective regeneration. In this study, we have compared neural progenitors (NPs) from the fetal ventricular zone (VZ), the postnatal subventricular zone, and an immortalized radial glia (RG) cell line engineered to conditionally secrete the trophic factor insulin-like growth factor 1 (IGF-1). Upon differentiation in vitro, the VZ cells were able to generate a greater number of neurons than subventricular zone cells. Furthermore, differentiated VZ cells generated pyramidal neurons. In vitro, doxycycline-driven secretion of IGF-1 strongly promoted neuronal differentiation of cells with hippocampal, interneuron and cortical specificity. Accordingly, VZ and engineered RG-IGF-1-hemagglutinin (HA) cells were selected for subsequent in vivo experiments. To increase cell survival, we delivered the NPs attached to a multifunctional chitosan-based scaffold. The microspheres containing adherent NPs were injected subacutely into the lesion cavity of adult rat brains that had sustained controlled cortical impact injury. At 2 weeks posttransplantation, the exogenously introduced cells showed a reduction in stem cell or progenitor markers and acquired mature neuronal and glial markers. In beam walking tests assessing sensorimotor recovery, transplanted RG cells secreting IGF-1 contributed significantly to functional improvement while native VZ or RG cells did not promote significant recovery. Altogether, these results support the therapeutic potential of chitosan-based multifunctional microsphere scaffolds seeded with genetically modified NPs expressing IGF-1 to promote repair and functional recovery after traumatic brain injuries.

Identifier

85062278570 (Scopus)

Publication Title

Asn Neuro

External Full Text Location

https://doi.org/10.1177/1759091419830186

e-ISSN

17590914

PubMed ID

30818968

Volume

11

Grant

R15NS087501

Fund Ref

National Institute of Neurological Disorders and Stroke

Recommended Citation

Skop, Nolan B.; Singh, Sweta; Antikainen, Henri; Saqcena, Chaitali; Calderon, Frances; Rothbard, Deborah E.; Cho, Cheul H.; Gandhi, Chirag D.; Levison, Steven W.; and Dobrowolski, Radek, "Subacute Transplantation of Native and Genetically Engineered Neural Progenitors Seeded on Microsphere Scaffolds Promote Repair and Functional Recovery After Traumatic Brain Injury" (2019). Faculty Publications. 7829.
https://digitalcommons.njit.edu/fac_pubs/7829