Differential regulation of insulin signalling by monomeric and oligomeric amyloid beta-peptide

Rubén Molina-Fernández; Pol Picón-Pagès; Alejandro Barranco-Almohalla; Giulia Crepin; Víctor Herrera-Fernández; Anna García-Elías; Hugo Fanlo-Ucar; Xavier Fernàndez-Busquets; Jordi García-Ojalvo; Baldomero Oliva; Francisco J Muñoz

doi:10.1093/braincomms/fcac243

Differential regulation of insulin signalling by monomeric and oligomeric amyloid beta-peptide

Brain Commun. 2022 Sep 24;4(5):fcac243. doi: 10.1093/braincomms/fcac243. eCollection 2022.

Affiliations

¹ Laboratory of Structural Bioinformatics (GRIB), Faculty of Health and Life Sciences, Universitat Pompeu Fabra, 08003 Barcelona, Spain.
² Laboratory of Molecular Physiology, Faculty of Health and Life Sciences, Universitat Pompeu Fabra, 08003 Barcelona, Spain.
³ Barcelona Institute for Global Health (ISGlobal, Hospital Clínic-Universitat de Barcelona), 08036 Barcelona, Spain.
⁴ Nanomalaria Group, Institute for Bioengineering of Catalonia (IBEC), The Barcelona Institute of Science and Technology, 08028 Barcelona, Spain.
⁵ Nanoscience and Nanotechnology Institute (IN2UB), University of Barcelona, 08028 Barcelona, Spain.
⁶ Laboratory of Dynamical Systems Biology, Faculty of Health and Life Sciences, Universitat Pompeu Fabra, 08003 Barcelona, Spain.

Abstract

Alzheimer's disease and Type 2 diabetes are pathological processes associated to ageing. Moreover, there are evidences supporting a mechanistic link between Alzheimer's disease and insulin resistance (one of the first hallmarks of Type 2 diabetes). Regarding Alzheimer's disease, amyloid β-peptide aggregation into β-sheets is the main hallmark of Alzheimer's disease. At monomeric state, amyloid β-peptide is not toxic but its function in brain, if any, is unknown. Here we show, by in silico study, that monomeric amyloid β-peptide 1-40 shares the tertiary structure with insulin and is thereby able to bind and activate insulin receptor. We validated this prediction experimentally by treating human neuroblastoma cells with increasing concentrations of monomeric amyloid β-peptide 1-40. Our results confirm that monomeric amyloid β-peptide 1-40 activates insulin receptor autophosphorylation, triggering downstream enzyme phosphorylations and the glucose Transporter 4 translocation to the membrane. On the other hand, neuronal insulin resistance is known to be associated to Alzheimer's disease since early stages. We thus modelled the docking of oligomeric amyloid β-peptide 1-40 to insulin receptor. We found that oligomeric amyloid β-peptide 1-40 blocks insulin receptor, impairing its activation. It was confirmed in vitro by observing the lack of insulin receptor autophosphorylation, and also the impairment of insulin-induced intracellular enzyme activations and the glucose Transporter 4 translocation to the membrane. By biological system analysis, we have carried out a mathematical model recapitulating the process that turns amyloid β-peptide binding to insulin receptor from the physiological to the pathophysiological regime. Our results suggest that monomeric amyloid β-peptide 1-40 contributes to mimic insulin effects in the brain, which could be good when neurons have an extra requirement of energy beside the well-known protective effects on insulin intracellular signalling, while its accumulation and subsequent oligomerization blocks the insulin receptor producing insulin resistance and compromising neuronal metabolism and protective pathways.

Keywords: Akt; Alzheimer’s disease; amyloid β-peptide; insulin; insulin resistance.