AI Article Synopsis
- In the last 15 years, many attempts to create drugs for Alzheimer's disease haven’t worked well, especially those targeting proteins called β-amyloid and tau.
- A new drug called Aducanumab was approved, but many experts and hospitals are skeptical about how effective it really is.
- Researchers suggest that instead of focusing on β-amyloid and tau, it's better to look for different targets and improve how drug studies are done to get more reliable results.
Article Abstract
Introduction: In the last 15 years, huge efforts against Alzheimer's disease (AD) with drugs targeting β-amyloid (Aβ) and tau have produced poor clinical results. Aducanumab, a recently FDA-approved anti-Aβ monoclonal antibody has been greeted with distrust by most experts, hospitals and insurance companies for its level of efficacy and poor tolerability.
Area Covered: We reviewed literature on Alzheimer trials using PubMed, meeting abstracts and ClnicalTrials.gov and discuss what we can learn from past failures of investigational drugs for Alzheimer's disease, especially anti-Aβ and anti-tau drugs.
Expert Opinion: It is our opinion that previous failures of anti-AD drugs suggest that soluble Aβ and tau are not appropriate drug targets. In addition, pivotal clinical trials of future clinical candidates should avoid major protocol amendments and futility analyses. Study protocols should adopt better measures to protect study blinding and minimize the potential introduction of major biases in the evaluation of clinical results. Finally, alternative biological targets should be pursued as well as more multimodal approaches to addressing neurodegeneration in AD.
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| http://dx.doi.org/10.1080/13543784.2021.2017881 | DOI Listing |
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