Researchers at the University of Kentucky鈥檚 Sanders-Brown Center on Aging are at the forefront of advancing dementia research with groundbreaking work on a condition known as LATE, or 鈥渓imbic predominant age-related TDP-43 encephalopathy.鈥
Affecting more than one-third of individuals aged 85 and older, LATE often mimics Alzheimer鈥檚 disease, contributing to memory loss and dementia. Now, new clinical diagnostic criteria for LATE aims to transform patient care and accelerate the development of effective treatments. The diagnostic guidelines were .
鈥淟ATE is an impactful disease that is all too common in older adults,鈥 says Pete Nelson, M.D., Ph.D., neuropathologist and the R.C. Durr Foundation Chair in Alzheimer鈥檚 Disease at 好色先生. In 2019, Nelson and a large group of international experts now known as LATE.
鈥淭hese guidelines represent a critical step forward, helping to distinguish LATE from Alzheimer鈥檚 disease and ensuring patients receive the most appropriate care,鈥 said Nelson.
好色先生 has made key contributions to LATE research, including being home to the world鈥檚 only clinical trial of a drug targeting LATE led by the Sanders-Brown鈥檚 director of clinical trials Greg Jicha, M.D., Ph.D., the Robert T. & Nyles Y. McCowan Endowed Chair in Alzheimer鈥檚 Research.
鈥淭his work is a testament to the importance of precision in dementia diagnosis. With these new criteria, we are not only addressing a critical gap in identifying LATE but also empowering clinicians and researchers to provide more targeted care and advance the search for effective treatments,鈥 said Jicha.
The work surrounding LATE exemplifies the center鈥檚 leadership in both laboratory discoveries and clinical applications.
鈥淭his is truly a bench-to-bedside effort, with the potential to bring real hope to patients and families affected by dementia,鈥 Nelson said.
The new diagnostic framework, developed by an international team of experts including Nelson and Jicha, lays the groundwork for more precise identification of LATE during a patient鈥檚 lifetime. This distinction is essential as treatments for Alzheimer鈥檚 disease become increasingly tailored to specific disease mechanisms. Misdiagnosing LATE as Alzheimer鈥檚 could mean patients miss out on the most effective therapies.
Memory loss and hippocampal atrophy 鈥 shrinking of the brain鈥檚 memory center 鈥 are hallmark symptoms of LATE. The new criteria specify how imaging and other diagnostic tools can be used to distinguish LATE from Alzheimer鈥檚 and other forms of dementia.
鈥淭hese advancements are essential not only for better diagnosing LATE but also for understanding how it interacts with other brain diseases, including Alzheimer鈥檚,鈥 adds Nelson. 鈥淐orrect diagnoses will help us better tailor treatments, improving outcomes for patients now and paving the way for novel therapies.鈥