Intrastriatal Transplantation of Adenovirus-Generated Induced Pluripotent Stem Cells for Treating Neuropathological and Functional Deficits in a Rodent Model of Huntington's Disease

Author:

Fink Kyle D.12345,Crane Andrew T.1,Lévêque Xavier126,Dues Dylan J.1,Huffman Lucas D.1,Moore Allison C.1,Story Darren T.1,DeJonge Rachel E.1,Antcliff Aaron1,Starski Phillip A.1,Lu Ming16,Lescaudron Laurent24789,Rossignol Julien110,Dunbar Gary L.16

Affiliation:

1. Field Neurosciences Institute Laboratory for Restorative Neurology, Brain Research and Integrative Neuroscience Center, Program in Neuroscience, Central Michigan University, Mount Pleasant, Michigan, USA

2. Faculté des Sciences et des Techniques, Université de Nantes, Nantes, France

3. INSERM U1064, ITUN, Nantes, France

4. INSERM U791, Laboratoire d'Ingenierie Osteo-Articulaire et Dentaire, Nantes, France

5. INSERM UMR 643, Nantes, France

6. Field Neurosciences Institute, Saginaw, Michigan, USA

7. Faculté de Médecine, Université de Nantes, Nantes, France

8. Centre Hospitalier-Universitaire Hotel Dieu de Nantes, Nantes, France

9. Faculté d'Odontologie, Université de Nantes, Nantes, France

10. College of Medicine, Central Michigan University, Mount Pleasant, Michigan, USA

Abstract

Abstract Induced pluripotent stem cells (iPSCs) show considerable promise for cell replacement therapies for Huntington's disease (HD). Our laboratory has demonstrated that tail-tip fibroblasts, reprogrammed into iPSCs via two adenoviruses, can survive and differentiate into neuronal lineages following transplantation into healthy adult rats. However, the ability of these cells to survive, differentiate, and restore function in a damaged brain is unknown. To this end, adult rats received a regimen of 3-nitropropionic acid (3-NP) to induce behavioral and neuropathological deficits that resemble HD. At 7, 21, and 42 days after the initiation of 3-NP or vehicle, the rats received intrastriatal bilateral transplantation of iPSCs. All rats that received 3-NP and vehicle treatment displayed significant motor impairment, whereas those that received iPSC transplantation after 3-NP treatment had preserved motor function. Histological analysis of the brains of these rats revealed significant decreases in optical densitometric measures in the striatum, lateral ventricle enlargement, as well as an increase in striosome size in all rats receiving 3-NP when compared with sham rats. The 3-NP-treated rats given transplants of iPSCs in the 7- or 21-day groups did not exhibit these deficits. Transplantation of iPSCs at the late-stage (42-day) time point did not protect against the 3-NP-induced neuropathology, despite preserving motor function. Transplanted iPSCs were found to survive and differentiate into region-specific neurons in the striatum of 3-NP rats, at all transplantation time points. Taken together, these results suggest that transplantation of adenovirus-generated iPSCs may provide a potential avenue for therapeutic treatment of HD.

Publisher

Oxford University Press (OUP)

Subject

Cell Biology,Developmental Biology,General Medicine

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