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Iatrogenic transmission of Alzheimer's disease: Evidence based on experimental inoculation of Alzheimer's brains into a primate
Author(s) -
Dhenain Marc,
Lam Suzanne,
Gary Charlotte,
Herard AnneSophie,
Koch James,
Petit Fanny,
Gipchtein Pauline,
Sawiak Stephen,
Caillierez Raphaelle,
Eddarkaoui Sabiha,
Colin Morvane,
Aujard Fabienne,
Deslys JeanPhilippe,
Duyckaerts Charles,
Brouillet Emmanuel,
Comoy Emmanuel,
Pifferi Fabien,
Picq JeanLuc
Publication year - 2020
Publication title -
alzheimer's and dementia
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 6.713
H-Index - 118
eISSN - 1552-5279
pISSN - 1552-5260
DOI - 10.1002/alz.042957
Subject(s) - entorhinal cortex , hippocampus , neuroscience , atrophy , pathology , cerebral cortex , human brain , tauopathy , neuroanatomy , cognitive decline , dementia , medicine , biology , disease , neurodegeneration
Background Epidemiologic data suggest that, in humans, iatrogenic administration of compounds (cadaver‐sourced human growth hormone, dura mater graft) or cerebral surgeries with tools contaminated with Aβ and tau induce aggregated Aβ and possibly tau lesions. Aβ and tau lesions could thus be iatrogenically transmitted to humans. Several studies in mice have shown that experimental inoculation of amyloid and/or tau‐positive brain samples into transgenic (tg) mouse models overexpressing Aβ or tau promotes either Aβ or tau aggregation in the brain of the recipient animal. Unlike rodents, primates naturally express Aβ or tau under normal conditions and they have a biochemical and physical cerebral environment that is closer to that of humans than that of mice. The aim of this work was to evaluate the impact of human brain samples inoculations in the mouse lemur primates. Method 12 adult mouse lemurs, aged from 3 to 4 years old, were included in this study. Human brain homogenates from AD patients or control (CTRL) age‐matched subject were bilaterally inoculated in the hippocampus and subjacent cortex (n = 6/group). We performed longitudinal cognitive, electroencephalography (EEG) and morphological MRI studies up to 18 months post‐inoculation followed by immunohistopathological examination of brain tissues. Result Mouse lemurs inoculated with Alzheimer brain homogenates displayed progressive cognitive impairments (clinical tests assessing cognitive and motor functions), modifications of neuronal activity (detected by electroencephalography), widespread and progressive cerebral atrophy (in vivo MRI assessing cerebral volume loss using automated voxel‐based analysis), neuronal loss in the hippocampus and entorhinal cortex (post mortem stereology). They displayed parenchymal and vascular Aβ depositions and tau lesions for some of them, in regions close to the inoculation sites. Conclusion This study is the first one to highlight neuronal and clinical dysfunction following inoculation of Alzheimer’s disease brain homogenates in a primate. Based on controlled experiments, it suggests the possible iatrogen transmission of Alzheimer pathology. Acknowledgments: We thank the “GIE NeuroCEB” Brain Bank, the France‐Alzheimer Association, the Fondation Plan Alzheimer, and the CEA Bottom‐Up program.