Acetylcholinesterase inhibitors (ChEI) are the global standard of care for the symptomatic treatment of Alz-heimer's disease (AD) and show significant positive effects in neurodegenerative diseases with cognitive and behavioral symptoms. Although experimental and large-scale clinical evidence indicates the potential long-term efficacy of ChEI, primary outcomes are generally heterogeneous across outpatient clinics and regional healthcare systems. Sub-optimal dosing or slow tapering, heterogeneous guidelines about the timing for therapy initiation (prodromal versus dementia stages), healthcare providers' ambivalence to treatment, lack of disease awareness, delayed medical consultation, prescription of ChEI in non-AD cognitive disorders, contribute to the negative outcomes. We present an evidence-based overview of determinants, spanning genetic, molecular, and large-scale networks, involved in the response to ChEI in patients with AD and other neurodegenerative diseases. A comprehensive understanding of cerebral and retinal cholinergic system dysfunctions along with ChEI response predictors in AD is crucial since disease-modifying therapies will frequently be prescribed in combination with ChEI. Therapeutic algorithms tailored to genetic, biological, clinical (endo)phenotypes, and disease stages will help leverage inter-drug synergy and attain optimal combined response outcomes, in line with the precision medicine model.

Lista, S., Vergallo, A., Teipel, S.j., Lemercier, P., Giorgi, F.s., Gabelle, A., et al. (2023). Determinants of approved acetylcholinesterase inhibitor response outcomes in Alzheimer's disease: relevance for precision medicine in neurodegenerative diseases. AGEING RESEARCH REVIEWS, 84, 101819 [10.1016/j.arr.2022.101819].

Determinants of approved acetylcholinesterase inhibitor response outcomes in Alzheimer's disease: relevance for precision medicine in neurodegenerative diseases

Garaci, Francesco;Mercuri, Nicola B;Nistico' R
2023-02-01

Abstract

Acetylcholinesterase inhibitors (ChEI) are the global standard of care for the symptomatic treatment of Alz-heimer's disease (AD) and show significant positive effects in neurodegenerative diseases with cognitive and behavioral symptoms. Although experimental and large-scale clinical evidence indicates the potential long-term efficacy of ChEI, primary outcomes are generally heterogeneous across outpatient clinics and regional healthcare systems. Sub-optimal dosing or slow tapering, heterogeneous guidelines about the timing for therapy initiation (prodromal versus dementia stages), healthcare providers' ambivalence to treatment, lack of disease awareness, delayed medical consultation, prescription of ChEI in non-AD cognitive disorders, contribute to the negative outcomes. We present an evidence-based overview of determinants, spanning genetic, molecular, and large-scale networks, involved in the response to ChEI in patients with AD and other neurodegenerative diseases. A comprehensive understanding of cerebral and retinal cholinergic system dysfunctions along with ChEI response predictors in AD is crucial since disease-modifying therapies will frequently be prescribed in combination with ChEI. Therapeutic algorithms tailored to genetic, biological, clinical (endo)phenotypes, and disease stages will help leverage inter-drug synergy and attain optimal combined response outcomes, in line with the precision medicine model.
feb-2023
Pubblicato
Rilevanza internazionale
Recensione
Esperti anonimi
Settore BIO/14 - FARMACOLOGIA
English
Acetylcholinesterase inhibitors
Alzheimer’s disease
Amyloid-β
Basal forebrain
Cholinergic system
Disease-modifying
Lista, S., Vergallo, A., Teipel, S.j., Lemercier, P., Giorgi, F.s., Gabelle, A., et al. (2023). Determinants of approved acetylcholinesterase inhibitor response outcomes in Alzheimer's disease: relevance for precision medicine in neurodegenerative diseases. AGEING RESEARCH REVIEWS, 84, 101819 [10.1016/j.arr.2022.101819].
Lista, S; Vergallo, A; Teipel, Sj; Lemercier, P; Giorgi, Fs; Gabelle, A; Garaci, F; Mercuri, Nb; Babiloni, C; Gaire, Bp; Koronyo, Y; Koronyo-Hamaoui, M; Hampel, H; Nistico', R
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/2108/325383
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