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Personalized Management and Treatment of Alzheimer's Disease

Ramon Cacabelos, Vinogran Naidoo, Olaia Martinez-Iglesias, Lola Corzo, Natalia Cacabelos, Rocio Pego, Juan C. Carril

LIFE-BASEL(2022)

Cited 6|Views29
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Abstract
Alzheimer's disease (AD) is a priority health problem with a high cost to society and a large consumption of medical and social resources. The management of AD patients is complex and multidisciplinary. Over 90% of patients suffer from concomitant diseases and require personalized therapeutic regimens to reduce adverse drug reactions (ADRs), drug-drug interactions (DDIs), and unnecessary costs. Men and women show substantial differences in their AD-related phenotypes. Genomic, epigenetic, neuroimaging, and biochemical biomarkers are useful for predictive and differential diagnosis. The most frequent concomitant diseases include hypertension (>25%), obesity (>70%), diabetes mellitus type 2 (>25%), hypercholesterolemia (40%), hypertriglyceridemia (20%), metabolic syndrome (20%), hepatobiliary disorder (15%), endocrine/metabolic disorders (>20%), cardiovascular disorder (40%), cerebrovascular disorder (60-90%), neuropsychiatric disorders (60-90%), and cancer (10%). Over 90% of AD patients require multifactorial treatments with risk of ADRs and DDIs. The implementation of pharmacogenetics in clinical practice can help optimize the limited therapeutic resources available to treat AD and personalize the use of anti-dementia drugs, in combination with other medications, for the treatment of concomitant disorders.
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Key words
Alzheimer's disease,anti-dementia drugs,biomarkers,cerebrovascular genomics,concomitant disorders,neurodegenerative genomics,pathogenic genes,phenotype-modifying treatments,pharmacogenomics
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