Structures prediction and replica exchange molecular dynamics simulations of α-synuclein: A case study for intrinsically disordered proteins
Citation
Coşkuner Weber, O. (2024). Structures prediction and replica exchange molecular dynamics simulations of α-synuclein: A case study for intrinsically disordered proteins. International Journal of Biological Macromolecules, 276.Abstract
In recent years, a variety of three-dimensional structure prediction tools, including AlphaFold2, AlphaFold3, ITASSER, C-I-TASSER, Phyre2, ESMFold, and RoseTTAFold, have been employed in the investigation of intrinsically disordered proteins. However, a comprehensive validation of these tools specifically for intrinsically
disordered proteins has yet to be conducted. In this study, we utilize AlphaFold2, AlphaFold3, I-TASSER, C-ITASSER, Phyre2, ESMFold, and RoseTTAFold to predict the structure of a model intrinsically disordered
α-synuclein protein. Additionally, extensive replica exchange molecular dynamics simulations of the intrinsically
disordered protein are conducted. The resulting structures from both structure prediction tools and replica exchange molecular dynamics simulations are analyzed for radius of gyration, secondary and tertiary structure
properties, as well as Cα and Hα chemical shift values. A comparison of the obtained results with experimental
data reveals that replica exchange molecular dynamics simulations provide results in excellent agreement with
experimental observations. However, none of the structure prediction tools utilized in this study can fully capture
the structural characteristics of the model intrinsically disordered protein. This study shows that a cluster of
ensembles are required for intrinsically disordered proteins. Artificial-intelligence based structure prediction
tools such as AlphaFold3 and C-I-TASSER could benefit from stochastic sampling or Monte Carlo simulations for
generating an ensemble of structures for intrinsically disordered proteins.