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Anti-inflammatory drugs ineffective for prevention of Alzheimer’s disease

Researchers have known for decades that inflammation accompanies Alzheimer’s disease (AD) brain lesions. Several early studies suggested that “super-aspirins” or Nonsteroidal anti-inflammatory drugs (NSAID) could help avoid the disease. However, after clinical trials showed that NSAIDs don’t help patients who already have AD symptoms, doctors wondered whether these drugs could still be helpful to people who were at risk of developing the disease, but weren’t yet showing symptoms.

To test this hypothesis, researchers at McGill University’s Faculty of Medicine developed a new approach to AD prevention trials, and used it to test whether the common NSAID naproxen could indeed stop the disease in its tracks, before people developed AD symptoms. Sadly, the results were not encouraging, according to research published in the April 5, 2019, online issue of Neurology, the medical journal of the American Academy of Neurology.

“To give the NSAID story one more chance to end well, we enrolled trial participants at the earliest stages of disease development, before they exhibited cognitive impairment,” explains Dr. John Breitner, Professor of Psychiatry at McGill and the study’s senior author. “The resulting trial, known as INTREPAD, examined the effects of naproxen in people who had a strong family history of AD but ‘squeaky-clean’ memory and other cognitive abilities.”

Developing a new method to assess effectiveness

Many researchers have noted the special challenge of measuring disease development at a time when they could not rely on symptoms to assess effects of a treatment. To deal with this challenge the McGill team collaborated in developing a new Alzheimer Progression Score (APS) that was shown elsewhere to predict the onset of clinical disease over the coming decade or more. The APS measures the early development of disease by combining many little changes into a composite score.

Applying the APS to a trial sample of 200 people (100 assigned to naproxen and 100 to placebo), the INTREPAD results showed real changes over the two-year trial period. However, there was no evidence that the APS change was reduced in those taking naproxen. “The usual side effects were there,” notes Pierre- François Meyer, a Ph.D. candidate in Dr. Breitner’s lab and the study’s first author, “but there was not the slightest suggestion of any benefit.”

“We think this is the end of the road for the use of NSAIDs for treatment or prevention of Alzheimer’s disease, and it suggests a need for caution about using other anti-inflammatory drugs for this purpose,” adds Dr. Breitner, who is Founding Director of the Centre for Studies on Prevention of Alzheimer’s Disease at the Research Centre of the Douglas Mental Health University Institute. “The world desperately needs a way to prevent this horrible disease,” he says, “and many other avenues are being investigated.” In this process, researchers argue ever more strongly for the importance of publishing negative or “null” trial results like this one.


Phase III aducanumab trials for Alzheimer’s disease stopped early


More information:
“INTREPAD: A randomized trial of naproxen to slow progress of presymptomatic Alzheimer disease,” by Pierre-François Meyer, John Breitner, et al, was published online in the journal Neurology on April 5, 2019 DOI: 10.1212/WNL.0000000000007232

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McGill University

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Anti-inflammatory drugs ineffective for prevention of Alzheimer’s disease (2019, April 5)
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