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Thermodynamic Evolution of a Metamorphic Protein: A Theoretical-Computational Study of Human Lymphotactin

Academic Article
Publication Date:
2023
abstract:
Metamorphic, or fold-switching, proteins feature different folds that are physiologically relevant. The human chemokine XCL1 (or Lymphotactin) is a metamorphic protein that features two native states, an alpha - beta and an all-beta fold, which have similar stability at physiological condition. Here, extended molecular dynamics (MD) simulations, principal component analysis of atomic fluctuations and thermodynamic modeling based on both the configurational volume and free energy landscape, are used to obtain a detailed characterization of the conformational thermodynamics of human Lymphotactin and of one of its ancestors (as was previously obtained by genetic reconstruction). Comparison of our computational results with the available experimental data show that the MD-based thermodynamics can explain the experimentally observed variation of the conformational equilibrium between the two proteins. In particular, our computational data provide an interpretation of the thermodynamic evolution in this protein, revealing the relevance of the configurational entropy and of the shape of the free energy landscape within the essential space ( i.e., the space defined by the generalized internal coordinates providing the largest, typically non-Gaussian, structural fluctuations).
Iris type:
01.01 Articolo in rivista
Keywords:
Fold-switching proteins; Thermodynamic evolution; Molecular dynamics; Essential dynamics
List of contributors:
ZANETTI POLZI, Laura
Authors of the University:
ZANETTI POLZI LAURA
Handle:
https://iris.cnr.it/handle/20.500.14243/456850
Published in:
PROTEIN JOURNAL
Journal
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URL

https://link.springer.com/article/10.1007/s10930-023-10123-7
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