Investigating the allosteric response of the <scp>PICK1 PDZ</scp> domain to different ligands with all‐atom simulations

Stevens, Amy O.; Kazan, I. Can; Özkan, Banu; He, Yi

doi:10.1002/pro.4474

Cited by 16 publications

(9 citation statements)

References 94 publications

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“…We found that the covid-19 S protein shows the expected high correlation between the occurrence of mutations and site flexibility (Figure 3) when we compare %DFI (DFI ranked by percentile) to the average number of variants per position found within a given %DFI bin. Previous studies have indicated that rigid residues are critical for functional dynamics, thus more likely to impact function if mutated and, generally, can lead to a loss of function and thus more conserved (Kim, H. et al 2015; Butler et al 2018; Modi, Risso, et al 2021; Modi, Campitelli, et al 2021; Kazan et al 2022; Ose, Butler, et al 2022; Stevens et al 2022; Campitelli et al 2020a; Kumar, A., Glembo, T.J., Ozkan, S.B. 2015b).…”

Section: Resultsmentioning

confidence: 99%

“…Previous studies have indicated that rigid residues are critical for functional dynamics, thus more likely to impact function if mutated and, generally, can lead to a loss of function and thus more conserved (Kim, H. et al 2015;Butler et al 2018;Modi, Risso, et al 2021;Modi, Campitelli, et al 2021;Kazan et al 2022;Ose, Butler, et al 2022;Stevens et al 2022;Campitelli et al 2020a;Kumar, A., Glembo, T.J., Ozkan, S.B. 2015b).…”

Section: Asymmetry In Communications Among the Network Of Interaction...mentioning

confidence: 99%

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Some mechanistic underpinnings of molecular adaptations of SARS-COV-2 spike protein by integrating candidate adaptive polymorphisms with protein dynamics

Ose,

Campitelli,

Modi

et al. 2023

Preprint

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We integrate evolutionary predictions based on the neutral theory of molecular evolution with protein dynamics to generate mechanistic insight into the molecular adaptations of the SARS-COV-2 Spike (S) protein. With this approach, we first identified Candidate Adaptive Polymorphisms (CAPs) of the SARS-CoV-2 Spike protein and assessed the impact of these CAPs through dynamics analysis. Not only have we found that CAPs frequently overlap with well-known functional sites, but also, using several different dynamics-based metrics, we reveal the critical allosteric interplay between SARS-CoV-2 CAPs and the S protein binding sites with the human ACE2 (hACE2) protein. CAPs interact far differently with the hACE2 binding site residues in the open conformation of S protein compared to the closed form. In particular, the CAP sites control the dynamics binding residues in the open state, suggesting an allosteric control of hACE2 binding. We also explored the characteristic mutations of different SARS-CoV-2 strains to find dynamic hallmarks and potential effects of future mutations. Our analyses reveal that Delta strain-specific variants have non-additive (i.e., epistatic) interactions with CAP sites, whereas the less pathogenic Omicron strains have mostly compensatory variants. Finally, our dynamics-based analysis suggests that the novel mutations observed in the Omicron strain epistatically interact with the CAP sites to help escape antibody binding.

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Section: Resultsmentioning

confidence: 99%

Section: Asymmetry In Communications Among the Network Of Interaction...mentioning

confidence: 99%

Some mechanistic underpinnings of molecular adaptations of SARS-COV-2 spike protein by integrating candidate adaptive polymorphisms with protein dynamics

Ose,

Campitelli,

Modi

et al. 2023

Preprint

Self Cite

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“…Our DFI metric calculates the relative flexibility/rigidity of individual residues in an protein (Campitelli et al, 2020; Kumar et al, 2015; Larrimore et al, 2017; Modi, Risso, et al, 2021; Stevens et al, 2022). The DFI algorithm, which is developed using linear response theory and perturbation response scanning, calculates the average response of a residue as a result of a perturbation on every other residue in a protein (Gerek & Ozkan, 2011).…”

Section: Methodsmentioning

confidence: 99%

Allosteric regulatory control in dihydrofolate reductase is revealed by dynamic asymmetry

2023

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We investigated the relationship between mutations and dynamics in Escherichia coli dihydrofolate reductase (DHFR) using computational methods. Our study focused on the M20 and FG loops, which are known to be functionally important and affected by mutations distal to the loops. We used molecular dynamics simulations and developed position‐specific metrics, including the dynamic flexibility index (DFI) and dynamic coupling index (DCI), to analyze the dynamics of wild‐type DHFR and compared our results with existing deep mutational scanning data. Our analysis showed a statistically significant association between DFI and mutational tolerance of the DHFR positions, indicating that DFI can predict functionally beneficial or detrimental substitutions. We also applied an asymmetric version of our DCI metric (DCIasym) to DHFR and found that certain distal residues control the dynamics of the M20 and FG loops, whereas others are controlled by them. Residues that are suggested to control the M20 and FG loops by our DCIasym metric are evolutionarily nonconserved; mutations at these sites can enhance enzyme activity. On the other hand, residues controlled by the loops are mostly deleterious to function when mutated and are also evolutionary conserved. Our results suggest that dynamics‐based metrics can identify residues that explain the relationship between mutation and protein function or can be targeted to rationally engineer enzymes with enhanced activity.

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“…Dynamic flexibility index (Butler et al, 2018; Gerek & Ozkan, 2011; Kazan et al, 2022; Kumar et al, 2015; Larrimore et al, 2017; Modi, Risso, et al, 2021; Ose et al, 2022; Stevens et al, 2022) uses the PRS technique that combines Elastic Network Model (ENM) and Linear Response Theory (LRT) (Nevin Gerek et al, 2013). In PRS, Brownian‐like unit forces

F

are applied sequentially to each residue as perturbations (Atilgan et al, 2010; Kumar et al, 2015).…”

Section: Methodsmentioning

confidence: 99%

“…We prepared the time series %DFI by averaging 3 adjacent time windows, respectively (0.5 μs-1 μs, 1 μs-1.5 μs, and 1.5 μs-2 μs). As our earlier works (Butler et al, 2015;Kazan et al, 2022;Larrimore et al, 2017;Modi, Campitelli, et al, 2021) highlight that the DFI profiles capture the related function (Butler et al, 2018;Campitelli et al, 2021;Kolbabakartchner et al, 2021;Modi, Risso, et al, 2021;Ose et al, 2022;Stevens et al, 2022;Zou et al, 2015), we cluster these time series of the DFI values of each variant using PCA (see Section 3.4) to compare their dynamics profiles. The first two principal components are responsible for most of the variance in the mutant DFI profiles.…”

Section: Binding To Group I Peptidementioning

confidence: 99%

Engineering gain‐of‐function mutants of a WW domain by dynamics and structural analysis

et al. 2023

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Proteins gain optimal fitness such as foldability and function through evolutionary selection. However, classical studies have found that evolutionarily designed protein sequences alone cannot guarantee foldability, or at least not without considering local contacts associated with the initial folding steps. We previously showed that foldability and function can be restored by removing frustration in the folding energy landscape of a model WW domain protein, CC16, which was designed based on Statistical Coupling Analysis (SCA). Substitutions ensuring the formation of five local contacts identified as “on‐path” were selected using the closest homolog native folded sequence, N21. Surprisingly, the resulting sequence, CC16‐N21, bound to Group I peptides, while N21 did not. Here, we identified single‐point mutations that enable N21 to bind a Group I peptide ligand through structure and dynamic‐based computational design. Comparison of the docked position of the CC16‐N21/ligand complex with the N21 structure showed that residues at positions 9 and 19 are important for peptide binding, whereas the dynamic profiles identified position 10 as allosterically coupled to the binding site and exhibiting different dynamics between N21 and CC16‐N21. We found that swapping these positions in N21 with matched residues from CC16‐N21 recovers nature‐like binding affinity to N21. This study validates the use of dynamic profiles as guiding principles for affecting the binding affinity of small proteins.This article is protected by copyright. All rights reserved.

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Investigating the allosteric response of the PICK1 PDZ domain to different ligands with all‐atom simulations

Cited by 16 publications

References 94 publications

Some mechanistic underpinnings of molecular adaptations of SARS-COV-2 spike protein by integrating candidate adaptive polymorphisms with protein dynamics

Some mechanistic underpinnings of molecular adaptations of SARS-COV-2 spike protein by integrating candidate adaptive polymorphisms with protein dynamics

Allosteric regulatory control in dihydrofolate reductase is revealed by dynamic asymmetry

Engineering gain‐of‐function mutants of a WW domain by dynamics and structural analysis

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