Abstract
BackgroundThe protein energy landscape underscores the inherent nature of proteins as dynamic molecules interconverting between structures with varying energies. Reconstructing a protein’s energy landscape holds the key to characterizing a protein’s equilibrium conformational dynamics and its relationship to function. Many pathogenic mutations in protein sequences alter the equilibrium dynamics that regulates molecular interactions and thus protein function. In principle, reconstructing energy landscapes of a protein’s healthy and diseased variants is a central step to understanding how mutations impact dynamics, biological mechanisms, and function.ResultsRecent computational advances are yielding detailed, sample-based representations of protein energy landscapes. In this paper, we propose and describe two novel methods that leverage computed, sample-based representations of landscapes to reconstruct them and extract from them informative local structures that reveal the underlying organization of an energy landscape. Such structures constitute landscape features that, as we demonstrate here, can be utilized to detect alterations of landscapes upon mutation.ConclusionsThe proposed methods detect altered protein energy landscape features in response to sequence mutations. By doing so, the methods allow formulating hypotheses on the impact of mutations on specific biological activities of a protein. This work demonstrates that the availability of energy landscapes of healthy and diseased variants of a protein opens up new avenues to harness the quantitative information embedded in landscapes to summarize mechanisms via which mutations alter protein dynamics to percolate to dysfunction.
Highlights
The protein energy landscape underscores the inherent nature of proteins as dynamic molecules interconverting between structures with varying energies
Basins correspond to thermodynamically-stable and semi-stable conformationalstates; barriers are local landscape structures that separate basins and control basin-to-basin diffusions that correspond to state-to-state interconversions [2, 3]
Qiao et al BMC Genomics 2018, 19(Suppl 7):671 structures control the dynamics of a protein and are key to a protein’s ability to regulate its molecular interactions and so its function in the cell [1, 4]
Summary
The protein energy landscape underscores the inherent nature of proteins as dynamic molecules interconverting between structures with varying energies. Proteins are ubiquitous biological macromolecules (biomolecules) found in most processes that maintain and replicate a living cell These biomolecules are inherently dynamic, switching/interconverting between shapes/conformations with different potential energies. These interconversions regulate interactions of a protein. Many human disorders (including cancer) are proteinopathies driven by DNA mutations that percolate to protein dysfunction by affecting the state-to-state interconversions via which a protein regulates interactions with molecular partners [5]. Such mutations change the energy landscape and, in particular, the local landscape structures that control the equilibrium dynamics [2]. This task is generally infeasible [6]
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