Publication:
d-Pinitol promotes tau dephosphorylation through a cyclin-dependent kinase 5 regulation mechanism: A new potential approach for tauopathies?

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Date

2022-04-21

Authors

Medina-Vera, Dina
Navarro, Juan Antonio
Rivera, Patricia
Rosell-Valle, Cristina
Gutierrez-Adan, Alfonso
Sanjuan, Carlos
Lopez-Gambero, Antonio Jesus
Tovar, Ruben
Suarez, Juan
Pavon, Francisco Javier

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Wiley
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Abstract

Recent evidence links brain insulin resistance with neurodegenerative diseases, where hyperphosphorylated tau protein contributes to neuronal cell death. In the present study, we aimed to evaluate if d-pinitol inositol, which acts as an insulin sensitizer, affects the phosphorylation status of tau protein. We studied the pharmacological effect of d-pinitol on insulin signalling and tau phosphorylation in the hippocampus of Wistar and Zucker rats. To this end, we evaluated by western blotting the Akt pathway and its downstream proteins as being one of the main insulin-mediator pathways. Also, we explored the functional status of additional kinases phosphorylating tau, including PKA, ERK1/2, AMPK and CDK5. We utilized the 3xTg mouse model as a control for tauopathy, since it carries tau mutations that promote phosphorylation and aggregation. Surprisingly, we discovered that oral d-pinitol treatment lowered tau phosphorylation significantly, but not through the expected kinase GSK-3 regulation. An extensive search for additional kinases phosphorylating tau revealed that this effect was mediated through a mechanism dependent on the reduction of the activity of the CDK5, affecting both its p35 and p25 subunits. This effect disappeared in leptin-deficient Zucker rats, uncovering that the association of leptin deficiency, obesity, dyslipidaemia and hyperinsulinaemia abrogates d-pinitol actions on tau phosphorylation. The 3xTg mice confirmed d-pinitol effectiveness in a genetic AD-tauopathy. The present findings suggest that d-pinitol, by regulating CDK5 activity through a decrease of CDK5R1, is a potential drug for developing treatments for neurological disorders such as tauopathies.

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MeSH Terms

Animals
Cyclin-Dependent Kinase 5
Glycogen Synthase Kinase 3
Inositol
Insulins
Leptin
Mice
Phosphorylation
Rats
Rats, Wistar
Rats, Zucker
Tauopathies
tau Proteins

DeCS Terms

Fosforilación
Glucógeno sintasa quinasa 3
Inositol
Insulinas
Tauopatías

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Keywords

Akt, CDK5, d-pinitol, insulin, tau phosphorylation, tauopathy

Citation

Medina-Vera D, Navarro JA, Rivera P, Rosell-Valle C, Gutiérrez-Adán A, Sanjuan C, et al. d-Pinitol promotes tau dephosphorylation through a cyclin-dependent kinase 5 regulation mechanism: A new potential approach for tauopathies? Br J Pharmacol. 2022 Oct;179(19):4655-4672