Tuning Proton Transfer Thermodynamics in SARS-CoV-2 Main Protease: Implications for Catalysis and Inhibitor Design

Zanetti-Polzi, Laura; Smith, Micholas Dean; Chipot, Chris; Gumbart, James C.; Lynch, Diane L.; Pavlova, Ànna; Smith, Jeremy C.; Daidone, Isabella

doi:10.1021/acs.jpclett.1c00425

Cited by 20 publications

(26 citation statements)

References 51 publications

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“…MD simulations were carried out for the Chymotrypsin-like catalytic domain I + II [ 22 , 41 ] of the two isoforms using, in turn, the Amber99sb-ildn [ 42 ] and the OPLS-AA/M FFs [ 32 ] with the GROMACS code [ 43 ] (version 2018.8). In the H–C isoform, H41 was assigned to the tautomer with the protonated N δ [ 25 ]. The potential parametrization for the PF-07321332 ligand was generated using two web interfaces: PrimadORAC [ 44 ] for AMBER FF and LigParGen [ 45 ] for OPLS-AA FF.…”

Section: Methodsmentioning

confidence: 99%

“…Most recently, a thorough MD study on the dimer [ 24 ] showed that the ion-pair configuration of the dyad is not compatible with a catalytically competent binding mode for peptide substrates. Substrate docking on the 3CL pro with the dyad in neutral form is hence supposed to favor the CYS to HIS PT [ 25 ] preceding the acylation step in the catalysis.…”

Section: Introductionmentioning

confidence: 99%

“…Recently, the catalytic mechanism in 3CL pro was investigated using hybrid QM/MM multi-scale hybrid methods [ 25 , 26 ]. Both these studies agree on the fact that in the apo (unligated) form, the neutral state for the dyad is significantly more stable than the zwitterionic state.…”

Section: Introductionmentioning

confidence: 99%

“…Regarding the role of the ligand in the holo form, however, these studies strikingly predict an opposite effect on the ion-pair state, stabilising in Ref. [ 25 ] and destabilising in Ref. [ 26 ] One weak point of these QM/MM approaches for the holo forms is that the latter are prepared [ [25] , [26] , [27] ] starting from the X-ray structures where the ligand is already covalently bound to CYS and that were presumably obtained from protein stock pre-incubated with the ligand.…”

Section: Introductionmentioning

confidence: 99%

“…[ 25 ] and destabilising in Ref. [ 26 ] One weak point of these QM/MM approaches for the holo forms is that the latter are prepared [ [25] , [26] , [27] ] starting from the X-ray structures where the ligand is already covalently bound to CYS and that were presumably obtained from protein stock pre-incubated with the ligand. The X-ray structure, on the other hand, is not necessarily similar to the actual initial non covalent bonding pose as the transition state involving the substrate and the binding site must be the result of a concerted process with a C145 to H41 PT transfer induced by the ligand non covalent docking, followed by a structural modification involving both the ligand and the nearby residues (including the oxyanion hole [ 28 ]) to arrive at the covalently bonded form seen in the ligand incubated samples.…”

Section: Introductionmentioning

confidence: 99%

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Characterization of the non-covalent interaction between the PF-07321332 inhibitor and the SARS-CoV-2 main protease

Macchiagodena

Pagliai

Procacci

2022

Journal of Molecular Graphics and Modelling

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We have studied the non-covalent interaction between PF-07321332 and SARS-CoV2 main protease at the atomic level using a computational approach based on extensive molecular dynamics simulations with explicit solvent. PF-07321332, whose chemical structure has been recently disclosed, is a promising oral antiviral clinical candidate with well-established anti-SARS-CoV-2 activity in vitro. The drug, currently in phase III clinical trials in combination with ritonavir, relies on the electrophilic attack of a nitrile warhead to the catalytic cysteine of the protease. Nonbonded interaction between the inhibitor and the residues of the binding pocket, as well as with water molecules on the protein surface, have been characterized using two different force fields and the two possible protonation states of the main protease catalytic dyad HIS41-CYS145. When the catalytic dyad is in the neutral state, the non-covalent binding is likely to be stronger. Molecular dynamics simulations seems to lend support for an inhibitory mechanism in two steps: a first non-covalent addition with the dyad in neutral form and then the formation of the thiolate-imidazolium ion pair and the ligand relocation for finalising the electrophilic attack.

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Section: Methodsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 3 more Smart Citations

Characterization of the non-covalent interaction between the PF-07321332 inhibitor and the SARS-CoV-2 main protease

Macchiagodena

Pagliai

Procacci

2022

Journal of Molecular Graphics and Modelling

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Intermolecular Photoinduced Electron Transfer in Biosystems: Impact of Conformational Transitions and Multiple Channels on Kinetics

Zanetti‐Polzi,

Pantazis,

Daidone

2024

ChemPhotoChem

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Estimating the kinetics of electron transfer (ET) processes in biologically relevant systems using theoretical‐computational methods remains a formidable task. This challenge arises from the inherent complexity of these systems, which makes it impractical to apply a fully quantum‐mechanical treatment. Hybrid quantum mechanical/classical mechanical computational approaches have been devised to enable the explicit simulation of electron transfer kinetics. This concept article focuses on a specific theoretical‐computational method employed in this context, namely the Perturbed Matrix Method (PMM), which has the merit of being able to include large‐scale conformational effects in the ET kinetics and potential multiple, alternative, ET channels. We describe its underlying physical principles, examine its advantages and limitations, and offer insights into its applications. Examples of the approach are discussed in the context of estimating photo‐induced electron transfer kinetics in proteins. The non‐exponential behavior observed in the presented case studies arises mainly from an active coupling with the environment fluctuations, but partly also stems from the presence of branching ET pathways.

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Structural insights into the substrate‐binding site of main protease for the structure‐based COVID‐19 drug discovery

2022

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An attractive drug target to combat COVID‐19 is the main protease (Mpro) because of its key role in the viral life cycle by processing the polyproteins translated from the viral RNA. Studying the crystal structures of the protease is important to enhance our understanding of its mechanism of action at the atomic‐level resolution, and consequently may provide crucial structural insights for structure‐based drug discovery. In the current study, we report a comparative structural analysis of the Mpro substrate binding site for both apo and holo forms to identify key interacting residues and conserved water molecules during the ligand‐binding process. It is shown that in addition to the catalytic dyad residues (His41 and Cys145), the oxyanion hole residues (Asn142–Ser144) and residues His164–Glu166 form essential parts of the substrate‐binding pocket of the protease in the binding process. Furthermore, we address the issue of the substrate‐binding pocket flexibility and show that two adjacent loops in the Mpro structures (residues Thr45–Met49 and Arg188–Ala191) with high flexibility can regulate the binding cavity’ accessibility for different ligand sizes. Moreover, we discuss in detail the various structural and functional roles of several important conserved and mobile water molecules within and around the binding site in the proper enzymatic function of Mpro. We also present a new docking protocol in the framework of the ensemble docking strategy. The performance of the docking protocol has been evaluated in predicting ligand binding pose and affinity ranking for two popular docking programs; AutoDock4 and AutoDock Vina. Our docking results suggest that the top‐ranked poses of the most populated clusters obtained by AutoDock Vina are the most important representative docking runs that show a very good performance in estimating experimental binding poses and affinity ranking.

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Tuning Proton Transfer Thermodynamics in SARS-CoV-2 Main Protease: Implications for Catalysis and Inhibitor Design

Cited by 20 publications

References 51 publications

Characterization of the non-covalent interaction between the PF-07321332 inhibitor and the SARS-CoV-2 main protease

Characterization of the non-covalent interaction between the PF-07321332 inhibitor and the SARS-CoV-2 main protease

Intermolecular Photoinduced Electron Transfer in Biosystems: Impact of Conformational Transitions and Multiple Channels on Kinetics

Structural insights into the substrate‐binding site of main protease for the structure‐based COVID‐19 drug discovery

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