Structure-Based Design of Small Peptide Ligands to Inhibit Early-Stage Protein Aggregation Nucleation

Mishra, Avinash; Bansal, Rohit; Sreenivasan, Shravan; Dash, Rozaleen; Joshi, Srishti; Rathore, Anurag S.; Goel, Gaurav

doi:10.1021/acs.jcim.0c00226

Cited by 13 publications

(31 citation statements)

References 67 publications

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“…57 The reduced interaction strength was chosen such that more than half of rigid-body docked N . A dimers, found to be metastable in earlier all-atomistic simulations, 30 stay in an associated state with a stable binding interface during CG simulation (see details in Table S1). CG-MD simulations were carried out using GROMACS at aggregation-prone experimental conditions of 338 K, pH 2, and 600 µM insulin.…”

Section: Methodsmentioning

confidence: 92%

“…Details of the protocol to obtain a total charge of +7 e on the dimer, in accordance with ion mobility mass spectroscopy measurements, are provided in our previous work. 30 The final structure from CG-MD simulations was refined by backmapping to the AA representation followed by a 20 ns MD run using the CHARMM36 force-field. 60 The central structure of the largest cluster from the stable portion of this AA MD trajectory was taken as the diffusional association complex.…”

Section: Methodsmentioning

confidence: 99%

“…A set of 16 most stable (lowest binding free energy) N.A insulin dimer conformations were taken from our earlier study wherein extensive rigid-body docking was used to generate a large ensemble of possible dimer conformations, followed by conformation ranking on basis of binding free energies calculated using the molecular mechanics Poisson-Boltzmann surface area (MM-PBSA) implicit solvent model. 30 We carried out an extensive set of molecular dynamics simulations starting with these 16 structures with a specific aim of allowing reorientation of binding partners under influence of long-range electrostatics and refinement of contacts determined from rigid-body docking. To allow for the determination of an electrostatically optimal binding mode, five replicate simulations were done for each rigid-body docked structure wherein monomer A in any given N.A dimer was moved perpendicular to the binding interface by a distance equal to twice the Debye length (2λ D =2.2 nm at 100 mm NaCl) to ensure a negligible effect of any specific proteinprotein interactions (PPIs) at this initial separation (see Figure S1).…”

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confidence: 99%

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A Multiscale Model for Quantitative Prediction of Insulin Aggregation Nucleation Kinetics

Mishra

Goel

2021

Preprint

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We combined kinetic, thermodynamic, and structural information from single molecule (protein folding) and two molecule (protein association) explicit-solvent simulations for determination of kinetic parameters in protein aggregation nucleation with insulin as model protein. A structural bioinformatics approach was developed to account for heterogeneity of aggregation-prone species with the transition complex theory, developed for native protein-receptor interactions, found applicable in modeling association kinetics involving this non-native species. We show that a key simplification arises from presence of only a few relevant modes for non-native association kinetics and that it is necessary to explicitly account for conformational rearrangement of a diffusional intermediate leading to the formation of aggregation pathway dimer and small oligomers. The kinetic parameters thus obtained were used in a population balance model and very accurate predictions for aggregation nucleation time varying over two orders of magnitude with changes in concentration of insulin or an aggregation-inhibitor ligand were obtained while an empirical parameter set was not found to be transferable for prediction of ligand effects. This physically determined kinetic parameter set also provided several insights into the mechanism of aggregation nucleation. Finally we discuss a route for application of our approach in high-throughput computational screening of ligands for inhibiting aggregation.

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Section: Methodsmentioning

confidence: 92%

Section: Methodsmentioning

confidence: 99%

mentioning

confidence: 99%

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A Multiscale Model for Quantitative Prediction of Insulin Aggregation Nucleation Kinetics

Mishra

Goel

2021

Preprint

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“…Following the work of Mishra et al,(17) se-365 quences of peptides were built by sewing a chain of spatially 366 close hotspot residues from two different binding segments of 367 the hotspot as given in Table1. A segment is defined as a 368 continuous sequence of residues on the NSP12 binding inter-369 face.…”

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confidence: 99%

Template-based design of peptides to inhibit SARS-CoV-2 RNA-dependent RNA polymerase complexation

Chenna

Khan

Dash

et al. 2022

Preprint

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The RNA-dependent RNA polymerase (RdRp) complex of SARS-CoV-2 lies at the core of its replication and transcription processes. The interfaces between the subunits of the RdRp complex are highly conserved, facilitating the design of inhibitors with high affinity for the interaction hotspots of the complex. Here, we report development and application of a structural bioinformatics protocol to design peptides that can inhibit RdRp complex formation by targeting the interface of its core subunit nonstructural protein (nsp) 12 with accesory factor nsp7. We adopt a top-down approach for protein design by using interaction hotspots of the nsp7-nsp12 complex obtained from a long molecular dynamics trajectory as template. A large library of peptide sequences constructed from multiple hotspot motifs of nsp12 is screened in-silico to determine peptide sequences with highest shape and interaction complementarity for the nsp7-nsp12 interface. Two design lead peptides are extensively characterised using orthogonal bioanalytical methods to determine their suitability for inhibition of RdRp complexation and and anti-viral activity. Their binding affinity to nsp7 (target), as determined from surface plasmon resonance (SPR) assay, is found to be comparable to that of the nsp7-nsp12 complex. Further, one of the designed peptides gives 46% inhibition of nsp7-nsp12 complex at 10:1 peptide:nsp7 molar concentration (from ELISA assay). Further optimization of cell penetrability and target affinity of these designed peptides is expected to provide lead candidates with high anti-viral activity against SARS-CoV-2.

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“…Small peptide ligands have been highlighted over the past few decades on account of their particular advantages, such as less cost, little immunogenic responses and more stable physicochemical properties ( 1 , 2 ). Especially, peptide ligands’ chemical structures are highly compatible with those of the target proteins ( 3 ).…”

mentioning

confidence: 99%

OUP accepted manuscript

Wang

et al. 2020

Database

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DPL ( http://www.peptide-ligand.cn/ ) is a comprehensive database of peptide ligand (DPL). DPL1.0 holds 1044 peptide ligand entries and provides references for the study of the polypeptide platform. The data were collected from PubMed-NCBI, PDB, APD3, CAMPR3, etc. The lengths of the base sequences are varied from 3 to78. DPL database has 923 linear peptides and 88 cyclic peptides. The functions of peptides collected by DPL are very wide. It includes 540 entries of antiviral peptides (including SARS-CoV-2), 55 entries of signal peptides, 48 entries of protease inhibitors, 45 entries of anti-hypertension, 37 entries of anticancer peptides, etc. There are 270 different kinds of peptide targets. All peptides in DPL have clear binding targets. Most of the peptides and receptors have 3D structures experimentally verified or predicted by CYCLOPS, I-TASSER and SWISS-MODEL. With the rapid development of the COVID-2019 epidemic, this database also collects the research progress of peptides against coronavirus. In conclusion, DPL is a unique resource, which allows users easily to explore the targets, different structures as well as properties of peptides.

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Structure-Based Design of Small Peptide Ligands to Inhibit Early-Stage Protein Aggregation Nucleation

Cited by 13 publications

References 67 publications

A Multiscale Model for Quantitative Prediction of Insulin Aggregation Nucleation Kinetics

A Multiscale Model for Quantitative Prediction of Insulin Aggregation Nucleation Kinetics

Template-based design of peptides to inhibit SARS-CoV-2 RNA-dependent RNA polymerase complexation

OUP accepted manuscript

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