A pentavalent peptide vaccine elicits Aβ and tau antibodies with prophylactic activity in an Alzheimer's disease mouse model

被引:0
|
作者
Song, Yiting [1 ]
Dai, Chun-Ling [2 ]
Shinohara, Mitsuru [3 ]
Tung, Yunn Chyn [2 ]
Zhou, Shiqi [1 ]
Huang, Wei-Chiao [1 ,4 ]
Seffouh, Amal [5 ]
Luo, Yuan [1 ]
Willadsen, Matthew [4 ]
Jiao, Yang [1 ]
Morishima, Maho [6 ]
Saito, Yuko [6 ]
Koh, Seong-Ho [7 ]
Ortega, Joaquin [5 ]
Gong, Cheng-Xin [2 ]
Lovell, Jonathan F. [1 ]
机构
[1] SUNY Buffalo, Dept Biomed Engn, Buffalo, NY 14260 USA
[2] New York State Inst Basic Res Dev Disabil, Dept Neurochem, Inge Grundke Iqbal Res Floor, Staten Isl, NY 10314 USA
[3] Natl Ctr Geriatr & Gerontol, Res Inst, Dept Aging Neurobiol, 7-430 Obu, Morioka, Aichi 4748511, Japan
[4] POP Biotechnol, Buffalo, NY 14228 USA
[5] McGill Univ, Dept Anat & Cell Biol, Montreal, PQ H3A 0C7, Canada
[6] Tokyo Metropolitan Geriatr Hosp & Inst Gerontol, Dept Neuropathol, Brain Bank Aging Res, 35-2 Sakaecho,Itabashi Ku, Tokyo 1730015, Japan
[7] Hanyang Univ, Dept Neurol, Guri Hosp, Guri Si 11923, Gyeonggi Do, South Korea
关键词
Active immunotherapy; Vaccine; Peptides; Tau; A beta; MORRIS WATER MAZE; AMYLOID-BETA; ABNORMAL PHOSPHORYLATION; PROTEIN-TAU; IMMUNOTHERAPY; PATHOLOGY; TANGLES; TRIALS; MICE; MICROHEMORRHAGE;
D O I
10.1016/j.bbi.2024.08.028
中图分类号
R392 [医学免疫学]; Q939.91 [免疫学];
学科分类号
100102 ;
摘要
Amyloid-(3 (A(3) and hyperphosphorylated tau protein are targets for Alzheimer's Disease (AD) immunotherapies, which are generally focused on single epitopes within A(3 or tau. However, due to the complexity of both A(3 and tau in AD pathogenesis, a multipronged approach simultaneously targeting multiple epitopes of both proteins could overcome limitations of monotherapies. Herein, we propose an active AD immunotherapy based on a nanoparticle vaccine comprising two A(3 peptides (1-14 and pyroglutamate pE3-14) and three tau peptides (centered on phosphorylated pT181, pT217 and pS396/404). These correspond to both soluble and aggregated targets and are displayed on the surface of immunogenic liposomes in an orientation that maintains reactivity with epitope-specific monoclonal antibodies. Intramuscular immunization of mice with individual epitopes resulted in minimally cross-reactive antibody induction, while simultaneous co-display of 5 antigens ("5-plex") induced antibodies against all epitopes without immune interference. Post-immune sera recognized plaques and neurofibrillary tangles from human AD brain tissue. Vaccine administration to 3xTg-AD mice using a prophylactic dosing schedule inhibited tau and amyloid pathologies and resulted in improved cognitive function. Immunization was well tolerated and did not induce antigen-specific cellular responses or persistent inflammatory responses in the peripheral or central nervous system. Antibody levels could be reversed by halting monthly vaccinations. Altogether, these results indicate that active immune therapies based on nanoparticle formulations of multiple A(3 and tau epitopes warrant further study for treating early-stage AD.
引用
收藏
页码:185 / 201
页数:17
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