A new study has identified a more precise and effective way to prevent cancer from spreading to the brain. The paper, published in the Proceedings of the National Academy of Sciences, details the development of novel drug candidates that target a key enzyme implicated in the spread of lung, breast, skin and other cancers to the brain. The work builds on a promising new therapeutic strategy first reported by the same group of researchers last year.

The new drug candidates are designed to intercept rogue cancer cells before they depart from primary tumors and ultimately travel to the brain.

Lead author Sheila Singh, based at both King’s College London and McMaster University, says this type of cancer—called metastatic brain cancer—is the most common type of brain tumor in adults and comes with an extremely grim outlook, with 90% of patients dying within one year of diagnosis.

Background: Individuals with Down syndrome (DS) exhibit an almost complete penetrance of Alzheimer’s disease (AD) pathology but are underrepresented in clinical trials for AD. The Tau protein is associated with microtubule function in the neuron and is crucial for normal axonal transport. In several different neurodegenerative disorders, Tau misfolding leads to hyper-phosphorylation of Tau (p-Tau), which may seed pathology to bystander cells and spread. This review is focused on current findings regarding p-Tau and its potential to seed pathology as a “prion-like” spreader. It also considers the consequences of p-Tau pathology leading to AD, particularly in individuals with Down syndrome. Methods: Scopus (SC) and PubMed (PM) were searched in English using keywords “tau AND seeding AND brain AND down syndrome”

Putting brain cells into a hibernation-like state via drugs that cool down core body temperature may help to preserve them following a stroke