Functional Amyloids Are Involved in Long Term Memory

For decades, amyloids have been synonymous with neurodegeneration, their insoluble fibrils blamed for Alzheimer’s, Parkinson’s, and related disorders. This bias stemmed from early biochemical studies that highlighted toxic aggregates while overlooking the evolutionary advantage of controlled protein assembly. Recent advances in proteostasis research, however, have uncovered a spectrum of amyloid functions, ranging from structural scaffolds to signaling platforms, prompting a reassessment of their role in healthy physiology.

The breakthrough study in Drosophila centers on a J‑domain chaperone dubbed Funes, which orchestrates the conversion of the prion‑like protein Orb2 into a functional amyloid at synaptic sites. By systematically varying the expression of thirty chaperones, the team demonstrated that elevated Funes levels dramatically extend odor‑reward memory beyond the typical 24‑hour window. Crucially, mutant Funes that bind Orb2 yet fail to trigger amyloid formation abolish this memory boost, establishing a causal link between regulated amyloid assembly and long‑term information storage. These findings illuminate a precise molecular switch that toggles protein conformation to encode persistent neural changes.

Implications extend far beyond fruit flies. Mammalian homologs such as CPEB exhibit similar amyloid‑dependent translational control, suggesting a conserved mechanism across species. Understanding how chaperones fine‑tune amyloid dynamics could inspire novel interventions for age‑related cognitive decline, where dysregulated protein aggregation erodes memory. Moreover, the study challenges the binary view of amyloids as purely pathological, encouraging biotech ventures to explore therapeutic modulation of functional amyloids for memory enhancement and neuroprotection.