University of Pittsburgh Scientists Develop Clinical Laboratory Test That Detects Alzheimer’s in Early Stages
Research could lead to new biomarkers that detect Alzheimer’s much earlier than existing tests and help scientists understand why some people with the disease do not develop dementia
Key biomarkers for detecting the progression of Alzheimer’s disease have typically been based on amyloid-beta (Aβ) plaques. But these plaques show up after the disease has well-progressed and aren’t suited to early detection of the disease.
Now, researchers at the University of Pittsburgh School of Medicine (Pitt) have developed a cerebrospinal fluid (CFS) test that detects changes in tau protein prior to the formation of neurofibrillary tangles (NFTs) that proceed Aβ plaques.
With further research, Pitt’s test could lead to new clinical laboratory biomarkers that help detect the disease earlier and with more accuracy.
“The clumping of tau protein into well-ordered structures, referred to by pathologists as neurofibrillary tangles, is a more defining event for Alzheimer’s disease as it is more strongly associated with the cognitive changes,” as compared to amyloid-beta pathology, according to a Pitt news release.
The researchers showed that their CSF biomarker test worked independent of discovery of brain amyloid deposits and “correlates with severity of cognitive decline” to enable “early-stage disease diagnosis and intervention,” reported Genetic Engineering and Biotechnology News.
The scientists published their findings in Nature Medicine titled, “Phospho-Tau Serine-262 and Serine-356 as Biomarkers of Pre-Tangle Soluble Tau Assemblies in Alzheimer’s Disease.”
“Our test identifies very early stages of tau tangle formation—up to a decade before any tau clumps can show up on a brain scan,” said Thomas Karikari, PhD (above), senior author and assistant professor of psychiatry at Pitt, in a news release. (Photo copyright: University of Pittsburgh.)
Combining Biomarkers May Lead to Better Alzheimer’s Knowledge
The new biomarkers may also work with existing markers that detect amyloid-beta pathology. This could give researchers and healthcare providers a better understanding of the early stages of Alzheimer’s in specific patients.
“Amyloid-beta is a kindling, and tau is a matchstick,” said Thomas Karikari, PhD, senior author and assistant professor of psychiatry at Pitt. Karikari previously researched amyloid-beta.
“A large percentage of people who have brain amyloid-beta deposits will never develop dementia. But once the tau tangles light up on a brain scan, it may be too late to put out the fire, and their cognitive health can quickly deteriorate. Early detection of tangle-prone tau could identify the individuals who are likely to develop Alzheimer’s-associated cognitive decline and could be helped with new generation therapies,” he added.
“P-tau-217 and p-tau-181 are fantastic biomarkers. However, in the early days after we developed these markers, we wondered why they were much more reflective of amyloid pathology than tau pathology,” Karikari told MedPage Today.
“That’s what inspired this work. We believe that methods combining, say, p-tau-217 and p-tau-262 or 356, would provide more complete information on combined early-stage amyloid and tau pathologies in Alzheimer’s disease,” he noted.
Developing the Alzheimer’s Biomarker Test
Karikari and colleagues turned to biochemistry and molecular biology to develop their new test.
Specifically, they emphasized “building blocks of NFTs including oligomers and protomers” which they called “soluble tau assemblies,” Medical News Today explained.
According to the Pitt news release, using autopsied brain tissue, the researchers found:
- A core region of the tau protein where NFTs form.
- 111 amino acids in the region.
- New “phosphorylation sites of p-tau-262 and p-tau-356 can inform the status of early-stage tau aggregation that, with an appropriate intervention, could potentially be reversed.”
In other words, p-tau-262 and p-tau-356 “could predict future NFT production, making them potential biomarkers for early disease,” Medical News Today noted.
“Together, our findings inform about the status of early-stage tau aggregation, reveal aggregation-relevant phosphorylation epitopes in tau, and offer a diagnostic biomarker and targeted therapeutic opportunities for Alzheimer’s disease,” the authors wrote in Nature Medicine.
More Research Planned Before Clinical Lab Use
About seven million Americans are affected by Alzheimer’s, according to the Alzheimer’s Association, which expects that number to grow to 13 million by 2050. A cure for the disease does not exist.
More research is needed before the Pitt researchers’ new CSF assay can be used by clinical laboratories. Karikari said the next step is developing blood assays for the biomarkers, MedPage Today reported.
—Donna Marie Pocius
