Scaling the Andean Shilajit: A Novel Neuroprotective Agent for Alzheimer’s Disease

Author:

Andrade Víctor123ORCID,Wong-Guerra Maylin14,Cortés Nicole1,Pastor Gabriela14,González Andrea1,Calfío Camila1ORCID,Guzmán-Martínez Leonardo1,Navarrete Leonardo P.15,Ramos-Escobar Nicolas1,Morales Inelia1,Santander Rocío6,Andrades-Lagos Juan78ORCID,Bacho Mitchell910,Rojo Leonel E.4,Maccioni Ricardo Benjamín1ORCID

Affiliation:

1. Laboratory of Neuroscience and Functional Medicine, International Center for Biomedicine, Faculty of Sciences, University of Chile, Santiago 7800003, Chile

2. Division of Neurogenetics and Molecular Psychiatry, Department of Psychiatry and Psychotherapy, Medical Faculty, University of Cologne, 50923 Köln, Germany

3. Department of Neurodegenerative Diseases and Geriatric Psychiatry, University Hospital Bonn, 53127 Bonn, Germany

4. Laboratory of Toxicology and Metabolism, Faculty of Chemistry and Biology, University of Santiago of Chile, Santiago 9170022, Chile

5. Biochemistry School, Faculty of Health Sciences, Andres Bello University, Santiago 8370035, Chile

6. Laboratory of Kinetics and Photochemistry, Faculty of Chemistry and Biology, University of Santiago of Chile, Santiago 9170022, Chile

7. Facultad de Medicina y Ciencia, Universidad San Sebastián, Santiago 7510157, Chile

8. Drug Development Laboratory, Faculty of Chemical and Pharmaceutical Sciences, University of Chile, Santiago 8380492, Chile

9. Organic and Organometallic Synthesis Laboratory, Faculty of Chemistry, Andrés Bello University, Santiago 8370186, Chile

10. Laboratory of Natural Resources, Faculty of Sciences, University of Chile, Santiago 7750000, Chile

Abstract

Alzheimer’s disease (AD) is a multifactorial neurodegenerative disorder without a cure, despite the enormous number of investigations and therapeutic approaches. AD is a consequence of microglial responses to “damage signals”, such as aggregated tau oligomers, which trigger a neuro-inflammatory reaction, promoting the misfolding of cytoskeleton structure. Since AD is the most prevalent cause of dementia in the elderly (>60 years old), new treatments are essential to improve the well-being of affected subjects. The pharmaceutical industry has not developed new drugs with efficacy for controlling AD. In this context, major attention has been given to nutraceuticals and novel bioactive compounds, such as molecules from the Andean Shilajit (AnSh), obtained from the Andes of Chile. Primary cultures of rat hippocampal neurons and mouse neuroblastoma cells were evaluated to examine the functional and neuroprotective role of different AnSh fractions. Our findings show that AnSh fractions increase the number and length of neuronal processes at a differential dose. All fractions were viable in neurons. The AnSh fractions inhibit tau self-aggregation after 10 days of treatment. Finally, we identified two candidate molecules in M3 fractions assayed by UPLC/MS. Our research points to a novel AnSh-derived fraction that is helpful in AD. Intensive work toward elucidation of the molecular mechanisms is being carried out. AnSh is an alternative for AD treatment or as a coadjuvant for an effective treatment.

Funder

Innova, High Technology Project CORFO

CONICYT FONDEQUIP/UHPLC MS/MS EQM

FONDEQUIP EQM

Corfo Project on High Technology

International Center for Biomedicine

Publisher

MDPI AG

Subject

Drug Discovery,Pharmaceutical Science,Molecular Medicine

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