New blood test spots Alzheimer's via protein shape changes

Researchers at Scripps Research have developed a blood test that detects Alzheimer's disease by analyzing structural changes in blood proteins. The method identifies differences in three specific proteins, allowing accurate distinction between healthy individuals, those with mild cognitive impairment, and Alzheimer's patients. Published in Nature Aging on February 27, 2026, the findings could enable earlier diagnosis and treatment.

Alzheimer's disease affects an estimated 7.2 million Americans aged 65 and older, according to the Alzheimer's Association. Traditional diagnostic tests measure levels of amyloid beta (Aβ) and phosphorylated tau (p-tau) in blood or spinal fluid, but these may miss the earliest changes in the disease.

A team at Scripps Research has proposed a novel approach focusing on protein folding in the bloodstream. Their study, published in Nature Aging on February 27, 2026, examined plasma samples from 520 participants divided into three groups: cognitively normal adults, individuals with mild cognitive impairment (MCI), and patients with Alzheimer's.

Using mass spectrometry, the researchers assessed how exposed or buried certain protein locations were, indicating structural changes. Machine learning helped identify patterns linked to disease stages. The analysis revealed that as Alzheimer's progressed, some blood proteins became less structurally "open," providing more insight than protein concentration levels alone.

Three proteins showed the strongest links to disease status: C1QA, involved in immune signaling; clusterin, which aids protein folding and amyloid removal; and apolipoprotein B, which transports fats and supports blood vessel health.

"The correlation was amazing," said co-author Casimir Bamberger, a senior scientist at Scripps Research. "It was very surprising to find three lysine sites on three different proteins that correlate so highly with disease state."

This three-protein model classified participants with 83% overall accuracy, rising above 93% when comparing two groups, such as healthy versus MCI. It remained reliable in independent groups and repeat tests months apart, achieving 86% accuracy and tracking diagnostic changes over time. The structural score also correlated with cognitive test results and moderately with MRI brain shrinkage measures.

"Many neurodegenerative diseases are driven by changes in protein structure," noted senior author John Yates, a professor at Scripps Research.

The method could complement existing amyloid and tau tests by focusing on proteostasis disruptions, the system's role in maintaining proper protein folding. It may help identify disease stages, monitor progression, and assess treatments.

"Detecting markers of Alzheimer’s early is absolutely critical to developing effective therapeutics," Yates added. Larger studies are needed for clinical use, and the approach might apply to other conditions like Parkinson's and cancer.

Authors include Ahrum Son, Hyunsoo Kim, Jolene K. Diedrich, Heather M. Wilkins, Jeffrey M. Burns, Jill K. Morris, Robert A. Rissman, and Russell H. Swerdlow. The work was supported by National Institutes of Health grants.

संबंधित लेख

Realistic split-image illustration showing obesity-linked faster rise in Alzheimer’s blood biomarkers versus normal weight, highlighting blood tests detecting changes earlier than brain scans.
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Obesity linked to faster rise in Alzheimer’s blood biomarkers, study finds

AI द्वारा रिपोर्ट किया गया AI द्वारा उत्पन्न छवि तथ्य-जाँच किया गया

New research finds that blood biomarkers associated with Alzheimer’s disease increase significantly faster in people with obesity than in those without. Drawing on five years of data from 407 volunteers, the study suggests that blood tests can detect obesity‑related changes earlier than brain scans, underscoring obesity as a major modifiable risk factor for Alzheimer’s.

Scientists at Washington University School of Medicine in St. Louis have developed a blood test that estimates when Alzheimer's symptoms may begin, using levels of the protein p-tau217. The model predicts onset within about three to four years, potentially aiding clinical trials and early interventions. This advance relies on data from 603 older adults in ongoing studies.

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European scientists have developed a preliminary method to identify Alzheimer's using a drop of dried blood from a finger, achieving 86% accuracy in detecting amyloid pathology. The study, validated in 337 patients from several countries, is published in Nature Medicine and aims to simplify early diagnosis of this disease affecting over 50 million people worldwide.

Researchers in Sweden and Norway have identified biological markers in the blood that signal the earliest stages of Parkinson's disease, potentially allowing detection up to 20 years before motor symptoms appear. The study, published in npj Parkinson's Disease, highlights a brief window where these markers are detectable, offering hope for earlier diagnosis and treatment. Blood tests based on this discovery could enter healthcare testing within five years.

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A large study of nearly 2 million older adults has found that cerebral amyloid angiopathy, a condition where amyloid proteins build up in brain blood vessels, sharply increases the risk of dementia. Within five years of diagnosis, people with this disorder were four times more likely to develop dementia than those without it, even absent a history of stroke. The findings, drawn from Medicare records, underscore the need for early cognitive screening in affected individuals.

Researchers have demonstrated that restoring levels of a key brain energy molecule can reverse advanced Alzheimer's disease in mouse models, repairing damage and restoring cognitive function. The study, published on December 22, challenges the long-held view that the condition is irreversible. Findings from human brain tissue support the approach's potential relevance to patients.

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A large-scale international study has found that age-related memory decline stems from broad structural changes across the brain, rather than a single region or gene. Analyzing over 10,000 MRI scans from thousands of healthy adults, researchers observed that brain shrinkage's impact on memory intensifies nonlinearly in later life. The findings highlight a distributed vulnerability that accelerates memory loss once a tipping point is reached.

 

 

 

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