Elucidating the mechanisms of -Synuclein-lipid interactions using site-directed mutagenesis. uri icon

abstract

  • -Synuclein (-syn) is a small protein that is involved in cell vesicle trafficking in neuronal synapses. A progressive aggregation of this protein is the expected molecular cause of Parkinson's disease, a disease that affects millions of people around the world. A growing body of evidence indicates that phospholipids can strongly accelerate -syn aggregation and alter the toxicity of -syn oligomers and fibrils formed in the presence of lipid vesicles. This effect is attributed to the presence of high copies of lysines in the N-terminus of the protein. In this study, we performed site-directed mutagenesis and replaced one out of two lysines at each of the five sites located in the -syn N-terminus. Using several biophysical and cellular approaches, we investigated the extent to which six negatively charged fatty acids (FAs) could alter the aggregation properties of K10A, K23A, K32A, K43A, and K58A -syn. We found that FAs uniquely modified the aggregation properties of K43A, K58A, and WT -syn, as well as changed morphology of amyloid fibrils formed by these mutants. At the same time, FAs failed to cause substantial changes in the aggregation rates of K10A, K23A, and K32A -syn, as well as alter the morphology and toxicity of the corresponding amyloid fibrils. Based on these results, we can conclude that K10, K23, and K32 amino acid residues play a critical role in protein-lipid interactions since their replacement on non-polar alanines strongly suppressed -syn-lipid interactions.

published proceedings

  • Neurobiol Dis

author list (cited authors)

  • Ali, A., Holman, A. P., Rodriguez, A., Osborne, L., & Kurouski, D.

complete list of authors

  • Ali, Abid||Holman, Aidan P||Rodriguez, Axell||Osborne, Luke||Kurouski, Dmitry

publication date

  • June 2024