Bioactivity of AAV2-neurturin gene therapy (CERE-120): Differences between Parkinson's disease and nonhuman primate brains

Authors

Raymond T. Bartus, Ceregene, Inc.
Christopher D. Herzog, Ceregene, Inc.
Yaping Chu, Rush University Medical Center
Alistair Wilson, Ceregene, Inc.
Lamar Brown, Ceregene, Inc.
Joao Siffert, Ceregene, Inc.
Eugene M. Johnson, Washington University School of Medicine in St. Louis
C. Warren Olanow, Icahn School of Medicine at Mount Sinai
Elliott J. Mufson, Rush University Medical Center
Jeffrey H. Kordower, Rush University Medical Center

Document Type

Article

Abstract

Background: AAV2-neurturin (CERE-120) is designed to deliver the neurotrophic-factor, neurturin, to the striatum to restore and protect degenerating nigrostriatal neurons in Parkinson's disease (PD). A common hypothesis is that following expression in the striatum, neurotrophic-factors like neurturin (NRTN) will be transported from degenerating terminals to their cell bodies in the substantia nigra pars compacta (SNc). Methods: We tested this concept using immunohistochemistry, comparing the bioactivity of AAV2-neurturin in brains of PD patients versus those of nonhuman primates similarly treated. Results: NRTN-immunostaining in the targeted striatum was seen in all PD cases (mean putaminal coverage: ∼15% by volume); comparable expression was observed in young, aged, and parkinsonian monkeys. In the SNc cell bodies, however, only rare evidence of neurturin was seen in PD, while ample evidence of intense nigral-NRTN was observed in all monkeys. NRTN-expression was associated with occasional, sparse TH-induction in the striatum of PD, but nothing apparent in the SNc. In primates, NRTN produced robust TH-induction throughout the nigrostriatal neurons. Discussion: These data provide the first evidence that gene therapy can increase expression of a neurotrophic-factor deep in the PD brain and that clear but modest enhancement of degenerating neurons can be induced. They also provide important insight regarding deficiencies in the status of nigrostriatal neurons in advanced PD, suggesting that serious axon-transport deficits reduced the bioactivity of AAV2-NRTN by limiting the protein exposed to the cell body. Thus, future efforts using neurotrophic-factors to treat neurodegenerative diseases will need to target both the terminal fields and the cell bodies of degenerating neurons to assure maximal benefit is achieved. © 2010 Movement Disorder Society.

Keywords

Axonal transport, Neural repair, Neurodegeneration, Neurotrophic factors, Translational research

Publication Date

1-1-2011

Publication Title

Movement Disorders

ISSN

08853185

E-ISSN

15318257

Volume

26

Issue

1

First Page

27

Last Page

36

PubMed ID

21322017

Digital Object Identifier (DOI)

10.1002/mds.23442

Recommended Citation

Bartus, Raymond T.; Herzog, Christopher D.; Chu, Yaping; Wilson, Alistair; Brown, Lamar; Siffert, Joao; Johnson, Eugene M.; Olanow, C. Warren; Mufson, Elliott J.; and Kordower, Jeffrey H., "Bioactivity of AAV2-neurturin gene therapy (CERE-120): Differences between Parkinson's disease and nonhuman primate brains" (2011). Translational Neuroscience. 1731.
https://scholar.barrowneuro.org/neurobiology/1731