Illustration of a Brazilian researcher in a lab examining a rat, with screens showing brain scans and molecular structures, representing a new compound that reverses Alzheimer's-like deficits in rats.
Illustration of a Brazilian researcher in a lab examining a rat, with screens showing brain scans and molecular structures, representing a new compound that reverses Alzheimer's-like deficits in rats.
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Brazilian copper-targeting compound reverses Alzheimer’s-like deficits in rats

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Проверено фактами

Researchers at Brazil’s Federal University of ABC report a simple copper-chelating molecule that reduced beta-amyloid–linked pathology and improved memory in rats. The compound showed no detectable toxicity in preclinical tests and, based on computer modeling, is predicted to cross the blood–brain barrier. The team is seeking industry partners for clinical development.

A research team led by Giselle Cerchiaro at the Federal University of ABC (UFABC), Brazil, has developed a new copper-targeting compound that improved cognition and reduced disease markers in a rat model of Alzheimer’s disease. The work, supported by the São Paulo Research Foundation (FAPESP), is detailed in ACS Chemical Neuroscience (published August 15, 2025; DOI: 10.1021/acschemneuro.5c00291).

According to the paper and accompanying FAPESP release, the compounds act as copper chelators, binding excess copper associated with beta‑amyloid plaques and promoting their degradation. “About a decade ago, international studies began to point to the influence of copper ions as an aggregator of beta-amyloid plaques. It was discovered that genetic mutations and changes in enzymes that act in the transport of copper in cells could lead to the accumulation of the element in the brain, favoring the aggregation of these plaques. Thus, the regulation of copper homeostasis has become one of the focuses for the treatment of Alzheimer’s,” Cerchiaro said.

From an initial set of ten candidate molecules, three advanced to animal testing. In rats with an induced Alzheimer’s-like condition, one compound (identified in the study as L10) stood out: treated animals showed better performance on spatial memory tasks, along with reduced neuroinflammation and oxidative stress and a restoration of copper balance in the hippocampus. The study also reports a reversal in beta‑amyloid plaque patterns.

Safety assessments found no detectable toxicity in hippocampal cell cultures or in the treated rats at the tested doses; vital signs were monitored during experiments. In silico analyses predicted that the compound can cross the blood–brain barrier, supporting its potential as a drug candidate.

The project formed part of the doctoral thesis of Mariana L. M. Camargo, the master’s thesis of Giovana B. Bertazzo, and the undergraduate research of Augusto B. Farias. A team led by Kleber Thiago de Oliveira at the Federal University of São Carlos (UFSCar) synthesized one of the compounds. The findings have led to a patent application, and the researchers are pursuing partnerships to begin human trials. “It’s an extremely simple, safe, and effective molecule. The compound we’ve developed is much less expensive than available drugs. Therefore, even if it only works for part of the population, since Alzheimer’s disease has multiple causes, it’d represent a huge advance over current options,” Cerchiaro said.

Alzheimer’s affects an estimated 50 million people worldwide, and current treatments remain limited. If future studies confirm safety and efficacy in humans, a low‑cost, copper‑targeting approach could expand therapeutic options.

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Initial reactions on X to the Brazilian copper-chelating compound for Alzheimer's are positive and limited, focusing on its potential to reverse symptoms in rats without toxicity. Users, including scientists and caregivers, shared the news highlighting memory restoration and calls for human trials. No significant negative or skeptical opinions were found in recent posts.

Связанные статьи

Oregon State scientists tracking copper-driven amyloid-beta clumping in real time using fluorescence anisotropy, with chelators reversing aggregation, in a high-tech lab.
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Oregon State researchers track copper-driven amyloid clumping in real time, testing a copper-selective chelator

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Oregon State University scientists report they have monitored, second by second, how copper ions promote aggregation of amyloid-beta—an Alzheimer’s-associated protein—and how different metal-binding molecules can disrupt or reverse that clumping, using a fluorescence anisotropy approach described in a study published in ACS Omega.

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A team of researchers led by Professor Yan-Jiang Wang has published a review arguing that Alzheimer's disease requires integrated treatments targeting multiple factors, not single causes. New drugs like lecanemab and donanemab offer modest benefits by slowing decline, but fall short of reversal. The paper, in Science China Life Sciences, emphasizes genetics, aging, and systemic health alongside amyloid-beta and tau proteins.

New research from the University of Southern California suggests that subtle declines in brain blood flow and oxygen delivery may be early indicators of Alzheimer's disease. The study, published in Alzheimer's and Dementia, used noninvasive scans to connect vascular health with amyloid plaques and hippocampal shrinkage. These findings highlight the role of brain circulation in the disease process beyond traditional markers like amyloid and tau.

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A study involving 73 people with mild cognitive impairment or early dementia found that tailored treatment plans targeting nutritional deficiencies, infections and other factors led to significant cognitive improvements after nine months. Participants in the intervention group saw their overall cognitive scores rise by 13.7 points, while the control group declined by 4.5 points. The approach combines medical interventions with lifestyle changes like diet, exercise and cognitive training.

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