MD-TASK: a software suite for analyzing molecular dynamics trajectories

Brown, David K.; Penkler, David L.; Amamuddy, Olivier Sheik; Ross, Caroline Jane; Atılgan, Ali Rana; Atılgan, Canan; Bishop, Özlem Taştan

doi:10.1093/bioinformatics/btx349

Cited by 159 publications

(215 citation statements)

References 15 publications

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“…Dynamic residue networks (DRNs) 47 Starting with ΔL i (Figure 6B), it is evident that ligand binding leads to an increase in L i , particularly at the NTDs of both protomers (~1 unit), with the largest increase observed for residues belonging to ATP-lid (residues 130-160). This observation is notably accentuated in protomer B of the SANC309 complex, with ΔL i values >3.0.…”

Section: Ligand Modulation Of Residue Interaction Networkmentioning

confidence: 99%

Modulation of Human Hsp90α Conformational Dynamics by Allosteric Ligand Interaction at the C-Terminal Domain

Penkler

Bishop

2018

Preprint

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Recent years have seen heat shock protein 90 kDa (Hsp90) attract significant interest as a viable drug target, particularly for cancer. To date, designed inhibitors that target the ATPase domain demonstrate potent anti-proliferative effects, but have failed clinical trials due to high levels of associated toxicity. To circumvent this, the focus has shifted away from the ATPase domain. One option involves modulation of the protein through allosteric activation/inhibition. Here, we propose a novel approach: we use previously obtained information via residue perturbation scanning coupled with dynamic residue network analysis to identify allosteric drug targeting sites for inhibitor docking. We probe the open conformation of human Hsp90α for druggable sites that overlap with these allosteric control elements, and identify three putative natural compound allosteric modulators: Cephalostatin 17, 20(29)-Lupene-3β-isoferulate and 3'-Bromorubrolide F. We assess the allosteric potential of these ligands by examining their effect on the conformational dynamics of the protein. We find evidence for the selective allosteric activation and inhibition of Hsp90's conformational transition toward the closed state in response to ligand binding and shed valuable insight to further the understanding of allosteric drug design and Hsp90's complex allosteric mechanism of action.

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Section: Ligand Modulation Of Residue Interaction Networkmentioning

confidence: 99%

Modulation of Human Hsp90α Conformational Dynamics by Allosteric Ligand Interaction at the C-Terminal Domain

Penkler

Bishop

2018

Preprint

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“…DCC is calculated based on the reduction and normalization of the 3N x 3N covariance matrix (C). The MD-TASK (Brown et al, 2017a) software suite was used to calculate DCC for each MD trajectory. C is constructed from the MD trajectory sampling data at 100 ps intervals, and the average deviation of each C α atom from a mean structure representative of the trajectory length is calculated.…”

Section: Dynamic Cross-correlationmentioning

confidence: 99%

“…To analyse inter-and intra-domain communication, the protein is represented as a residue interaction network (RIN), where the C β atoms of each residue (C α for glycine) are treated as nodes within the network, and edges between nodes defined within a distance cut off of 6.7 Å (Atilgan et al, 2004). In this study, the MD-TASK (Brown et al, 2017a) software suite is used to construct dynamic RINs (DRN) based on the all-atom MD trajectories. Each DRN is the combination of RINs representative of time points (frames) in the MD trajectory, using a 200 ps time interval between frames.…”

Section: Dynamic Residue Network Analysismentioning

confidence: 99%

“…Finally, MD-TASK averages the ΔL i and BC matrices. Average ΔL i and BC indicates residues that experience permanent changes in ΔL i and BC as opposed to minor fluctuations over the course of the MD trajectory (Brown et al, 2017a). For comparative purposes, BC values are normalized in the range 0.0 -1.0.…”

Section: Dynamic Residue Network Analysismentioning

confidence: 99%

“…Perturbation response scanning (PRS) is a computational technique used to predict the relative response of all residues in a protein, to an external force perturbation, such as ligand binding, at a single residue. The theory of PRS has been thoroughly described in previous studies (Atilgan & (1) Atilgan, 2009;Atilgan et al, 2010;Penkler et al, 2017); the algorithm is available in the MD-TASK software suite (Brown et al, 2017a). In brief, PRS utilizes linear response theory (LRT) to approximate the shift in coordinates (R 1 ) of a given protein conformation (R 0 ) in response to a perturbation of the Hamiltonian (Yilmaz & Atilgan, 2000;Ikeguchi et al, 2005;Atilgan & Atilgan, 2009).…”

Section: Perturbation Response Scanningmentioning

confidence: 99%

See 2 more Smart Citations

Allosteric Modulation of Conformational Dynamics in Human Hsp90α: A Computational Study

Atılgan

Öt

2017

Preprint

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Computational investigations on the dynamic binding effect of molecular tweezer CLR01 toward intrinsically disordered HIV‐1 Nef

Bhattarai

Emerson

2020

Biotech and App Biochem

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Intrinsically disordered proteins (IDPs) are highly flexible molecules that undergo disorder to order transition through their interaction with other molecules. IDPs play a vital role in several biological processes ranging from molecular recognition to several human diseases through the protein-protein interaction. The dynamic flexibility of IDPs and their implications in several human diseases enable these molecules to serve as novel therapeutic targets. However, the challenging task is to develop novel drugs against IDPs because of their lack of stable structures and the nature of high conformational flexibility. In this study, we have calculated the dynamic binding effect of the supramolecular tweezer CLR01 against the intrinsically disordered HIV-1 Nef by employing molecular docking and dynamics simulation approaches. From docking results, we predicted the strong binding affinity of the tweezer with the target residues of Nef. The docking results were further validated from the molecular dynamics simulation studies confirming the conformational stability of Nef upon tweezer binding. These findings provide useful insights into the development of potent inhibitors for targeting Nef protein functions.

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MD-TASK: a software suite for analyzing molecular dynamics trajectories

Cited by 159 publications

References 15 publications

Modulation of Human Hsp90α Conformational Dynamics by Allosteric Ligand Interaction at the C-Terminal Domain

Modulation of Human Hsp90α Conformational Dynamics by Allosteric Ligand Interaction at the C-Terminal Domain

Allosteric Modulation of Conformational Dynamics in Human Hsp90α: A Computational Study

Computational investigations on the dynamic binding effect of molecular tweezer CLR01 toward intrinsically disordered HIV‐1 Nef

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