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MultiTEP platform-based DNA vaccines for alpha-synucleinopathies: preclinical evaluation of immunogenicity and therapeutic potency

Authors :
Janet Petrosyan
Natalie R.S. Goldberg
Mathew Blurton-Jones
Eliezer Masliah
Anahit Ghochikyan
David H. Cribbs
Konstantin Kazarian
Irina Petrushina
Karen Zagorski
Hayk Davtyan
Michael G. Agadjanyan
Source :
Neurobiology of aging. 59
Publication Year :
2016

Abstract

We have previously demonstrated that anti-beta amyloid DNA vaccine (AV-1959D) based on our proprietary MultiTEP platform technology is extremely immunogenic in mice, rabbits, and monkeys. Importantly, MultiTEP platform enables development of vaccines targeting pathological molecules involved in various neurodegenerative disorders. Taking advantage of the universality of MultiTEP platform, we developed DNA vaccines targeting 3 B-cell epitopes (amino acids [aa]85-99, aa109-126, and aa126-140) of human alpha-synuclein (hα-Syn) separately or all 3 epitopes simultaneously. All 4 DNA vaccines (1) generate high titers of anti-hα-Syn antibodies and (2) induce robust MultiTEP-specific T-helper cell responses without activation of potentially detrimental autoreactive anti-hα-Syn T-helper cells. Generated antibodies recognize misfolded hα-Syn produced by neuroblastoma cells, hα-Syn in the brain tissues of transgenic mouse strains and in the brain tissues of dementia with Lewy body cases. Based on these results, the most promising vaccine targeting 3 B-cell epitopes of hα-Syn simultaneously (PV-1950D) has been chosen for ongoing preclinical assessment in mouse models of hα-Syn with the aim to translate it to the human clinical trials.

Details

ISSN :
15581497
Volume :
59
Database :
OpenAIRE
Journal :
Neurobiology of aging
Accession number :
edsair.doi.dedup.....9d7113cfba9659e58b3c3bb8fc66bca4