Aβ plaques do not protect against HSV-1 infection in a mouse model of familial Alzheimer's disease, and HSV-1 does not induce Aβ pathology in a model of late onset Alzheimer's disease

Olga V Bocharova; Aidan Fisher; Narayan P Pandit; Kara Molesworth; Olga Mychko; Alison J Scott; Natallia Makarava; Rodney Ritzel; Ilia V Baskakov

doi:10.1111/bpa.13116

Aβ plaques do not protect against HSV-1 infection in a mouse model of familial Alzheimer's disease, and HSV-1 does not induce Aβ pathology in a model of late onset Alzheimer's disease

Brain Pathol. 2023 Jan;33(1):e13116. doi: 10.1111/bpa.13116. Epub 2022 Sep 5.

Authors

Olga V Bocharova^{1

2}, Aidan Fisher^{1

2}, Narayan P Pandit^{1

2}, Kara Molesworth^{1

2}, Olga Mychko^{1

2}, Alison J Scott³, Natallia Makarava^{1

2}, Rodney Ritzel⁴, Ilia V Baskakov^{1

2}

Affiliations

¹ Center for Biomedical Engineering and Technology, University of Maryland School of Medicine, Baltimore, Maryland, USA.
² Department of Anatomy and Neurobiology, University of Maryland School of Medicine, Baltimore, Maryland, USA.
³ Department of Microbial Pathogenesis, University of Maryland School of Dentistry, Baltimore, Maryland, USA.
⁴ Department of Anesthesiology and Center for Shock, Trauma and Anesthesiology Research (STAR), University of Maryland School of Medicine, Baltimore, Maryland, USA.

Abstract

The possibility that the etiology of late onset Alzheimer's disease is linked to viral infections of the CNS has been actively debated in recent years. According to the antiviral protection hypothesis, viral pathogens trigger aggregation of Aβ peptides that are produced as a defense mechanism in response to infection to entrap and neutralize pathogens. To test the causative relationship between viral infection and Aβ aggregation, the current study examined whether Aβ plaques protect the mouse brain against Herpes Simplex Virus 1 (HSV-1) infection introduced via a physiological route and whether HSV-1 infection triggers formation of Aβ plaques in a mouse model of late-onset AD that does not develop Aβ pathology spontaneously. In aged 5XFAD mice infected via eye scarification, high density of Aβ aggregates did not improve survival time or rate when compared with wild type controls. In 5XFADs, viral replication sites were found in brain areas with a high density of extracellular Aβ deposits, however, no association between HSV-1 and Aβ aggregates could be found. To test whether HSV-1 triggers Aβ aggregation in a mouse model that lacks spontaneous Aβ pathology, 13-month-old hAβ/APOE4/Trem2*R47H mice were infected with HSV-1 via eye scarification with the McKrae HSV-1 strain, intracranial inoculation with McKrae, intracranial inoculation after priming with LPS for 6 weeks, or intracranial inoculation with high doses of McKrae or 17syn + strains that represent different degrees of neurovirulence. No signs of Aβ aggregation were found in any of the experimental groups. Instead, extensive infiltration of peripheral leukocytes was observed during the acute stage of HSV-1 infection, and phagocytic activity of myeloid cells was identified as the primary defense mechanism against HSV-1. The current results argue against a direct causative relationship between HSV-1 infection and Aβ pathology.

Keywords: 5XFAD mice; Alzheimer's disease; Aβ aggregates; amyloid precursor protein; hAβ/APOE4/Trem2*R47H mice; herpes simplex virus 1; infiltrating myeloid cells; microglia.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Alzheimer Disease* / pathology
Amyloid beta-Peptides / metabolism
Animals
Brain / pathology
Disease Models, Animal
Herpes Simplex* / complications
Herpesvirus 1, Human* / metabolism
Membrane Glycoproteins
Mice
Mice, Transgenic
Receptors, Immunologic

Substances

Amyloid beta-Peptides
Trem2 protein, mouse
Membrane Glycoproteins
Receptors, Immunologic

Abstract

Publication types

MeSH terms

Substances

Grants and funding