The Effect of Human HSP70 Administration on a Mouse Model of Alzheimer’s Disease Strongly Depends on Transgenicity and Age

Article type: Research Article

Authors: Evgen’ev, Michael^{a; 1; *} | Bobkova, Natalia^{c; 1} | Krasnov, George^{a; 1} | Garbuz, David^a | Funikov, Sergei^a | Kudryavtseva, Anna^a | Kulikov, Alexei^b | Samokhin, Alexander^c | Maltsev, Andrey^d | Nesterova, Inna^c

Affiliations: [a] Engelhardt Institute of Molecular Biology, RAS, Moscow, Russia | [b] Institute of Developmental Biology, RAS, Moscow, Russia | [c] Institute of Cell Biophysics, RAS, Pushchino, Moscow region, Russia | [d] Institute of Physiologically Active Compounds, RAS, Chernogolovka, Russia

Correspondence: [*] Correspondence to: Michael B. Evgen’ev, Institute of Molecular Biology, Russian Academy of Sciences, Vavilov str., 32, Moscow 119991, Russia. E-mail: [email protected].

Note: [1] These authors contributed equally to this work.

Abstract: In humans, heat shock protein 70 is a key component of the machinery that protects neuronal cells from various stress conditions and whose production significantly declines during aging. Herein, we investigated the protective effect of sub-chronic intranasal administration of human Hsp70 on the state of neurons in the temporal cortex and areas of the hippocampus of old transgenic (Tg) 5XFAD mice (11–13 months), representing a late-onset model of hereditary Alzheimer’s disease. Quantitative analysis of the various neuronal pathologies between the two groups (Tg versus nTg) revealed maximal levels of abnormalities in the brains of aged Tg mice. Importantly, intranasal application of HSP70 had profound beneficial effects on neuron morphology in the temporal cortex and hippocampal regions when applied to the aged Tg mice but not in the case of age-matched, non-transgenic, littermate animals. Furthermore, the effect of HSP70 administration on neurons in the hippocampus and temporal cortex differed characteristically between the groups. Using RNA-Seq, we identified a lot of differentially expressed genes in the hippocampus of old Tg mice compared with those of nTg mice. Most importantly, we observed HSP70-induced upregulation of multiple genes participating in antigen processing and presentation especially the members of major histocompatibility complex (class I and II) in the brains of old 5XFAD Tg animals, suggesting that Hsp70 executes its beneficial role via activation of adaptive immunity. Overall, our data enable to conclude that Hsp70 treatment may be a safe and effective therapeutic application against Alzheimer-type neuropathologies manifested at the late stages of the disease.

Keywords: 5XFAD, Aging, hippocampus, neuronal pathology, recombinant HSP70, temporal cortex, transcriptome

DOI: 10.3233/JAD-180987

Journal: Journal of Alzheimer's Disease, vol. 67, no. 4, pp. 1391-1404, 2019