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Literature DB >> 35572351

Endophenotype-based in silico network medicine discovery combined with insurance record data mining identifies sildenafil as a candidate drug for Alzheimer's disease.

Jiansong Fang¹, Pengyue Zhang², Yadi Zhou¹, Chien-Wei Chiang³, Juan Tan¹, Yuan Hou¹, Shaun Stauffer⁴, Lang Li³, Andrew A Pieper⁵, Jeffrey Cummings⁶, Feixiong Cheng^1,7,8.

Abstract

We developed an endophenotype disease module-based methodology for Alzheimer's disease (AD) drug repurposing and identified sildenafil as a potential disease risk modifier. Based on retrospective case-control pharmacoepidemiologic analyses of insurance claims data for 7.23 million individuals, we found that sildenafil usage was significantly associated with a 69% reduced risk of AD (hazard ratio = 0.31, 95% confidence interval 0.25-0.39, P<1.0×10-8). Propensity score stratified analyses confirmed that sildenafil is significantly associated with a decreased risk of AD across all four drug cohorts we tested (diltiazem, glimepiride, losartan and metformin) after adjusting age, sex, race, and disease comorbidities. We also found that sildenafil increases neurite growth and decreases phospho-tau expression in AD patient-induced pluripotent stem cells-derived neuron models, supporting mechanistically its potential beneficial effect in Alzheimer's disease. The association between sildenafil use and decreased incidence of AD does not establish causality or its direction, which requires a randomized clinical trial approach.

Entities: Chemical

Year: 2021 PMID： 35572351 PMCID： PMC9097949 DOI： 10.1038/s43587-021-00138-z

Source DB: PubMed Journal: Nat Aging ISSN： 2662-8465

88 in total

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10. Resurrection of sildenafil: potential for Huntington's Disease, too?

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