Analysis of KRAS–Ligand Interaction Modes and Flexibilities Reveals the Binding Characteristics

Zhao, Zheng; Bohidar, Niraja; Bourne, Philip E.

doi:10.1021/acs.jcim.3c00097

Cited by 4 publications

(2 citation statements)

References 49 publications

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“…Briefly, the Fs-IFP method comprises three steps. The first step aligns the ligand-binding sites using a sequence order-independent strategy (SMAP). , The second step converts all the 3D binding site-ligand interaction information into a 1D bit-string representation by encoding molecular interaction fingerprints (IFPs). − The IFPs are generated based upon a set of predefined geometric rules (see the Supporting Information) that classify residue-based interactions into seven types: hydrophobic, aromatic (face-to-face), aromatic (edge-to-face), H-bond (protein as donor), H-bond (protein as acceptor), electrostatic (protein positively charged), and electrostatic (protein negatively charged) using the software IChem. , Thus, every residue-ligand interaction is represented by a seven-bit string (Supporting Information), for example, “0001000” where “1” indicates the interaction exists between this residue and ligand, and its fourth position in the seven-bit string shows the interaction is an H-bond (protein as donor). In contrast, “0” means the ligand has no interaction with this residue.…”

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confidence: 99%

How Ligands Interact with the Kinase Hinge

Zhao,

Bourne

2023

ACS Med. Chem. Lett.

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ATP-competitive kinase inhibitors form hydrogen bond interactions with the kinase hinge region at the adenine binding site. Thus, it is crucial to explore hinge-ligand recognition as part of a rational drug design strategy. Here, harnessing known ligand-bound kinase structures and experimental assay resources, we first created a kinase structure-assay database (KSAD) containing 2705 nM ligand-bound kinase complexes. Then, using KSAD, we systematically investigate hinge-ligand binding patterns using interaction fingerprints, thereby delineating 15 different hydrogen-bond interaction modes. We believe these results will be valuable for de novo drug design and/or scaffold hopping of kinasetargeted drugs.

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confidence: 99%

How Ligands Interact with the Kinase Hinge

Zhao,

Bourne

2023

ACS Med. Chem. Lett.

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“…The second step converts all the 3D binding siteligand interaction information into a 1D bit-string representation by encoding molecular interaction fingerprints (IFPs). [39][40][41] The IFPs are generated based upon a set of predefined geometric rules that classify residue-based interactions into seven types: hydrophobic, aromatic (face-to-face), aromatic (edge-to-face), H-bond (protein as donor), H-bond (protein as acceptor), electrostatic (protein positively charged), and electrostatic (protein negatively charged). 39 Thus, 6 every residue-ligand interaction is represented by a seven-bit string, for example, "0001000" where "1" indicates the interaction exists between this residue and ligand, and its fourth position in the seven-bit string shows the interaction is an H-bond (protein as donor).…”

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How Ligands Interact with the Kinase Hinge

Zhao¹,

Bourne

2023

Preprint

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ATP-competitive kinase inhibitors form hydrogen bond interactions with the kinase hinge region at the adenine binding site. Thus, it is crucial to explore hinge-ligand recognition as part of a rational drug design strategy. Here, harnessing known ligand-bound kinase structures and experimental assay resources, we first create a kinase structure-assay database (KSAD) containing 2915 nanomolar ligand-bound kinase complexes. Then, using the KSAD, we systematically investigate hinge-ligand binding patterns using interaction fingerprints, thereby delineating 15 different hydrogen-bond interaction modes. We believe these results will be valuable for de novo drug design and/or scaffold hopping of kinase-targeted drugs.

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In Silico Identification of Selective KRAS G12D Inhibitor via Machine Learning‐Based Molecular Docking Combined with Molecular Dynamics Simulation

Nadee,

Prompat,

Yamabhai

et al. 2024

Advcd Theory and Sims

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KRAS G12D mutation is prevalent in various cancers and is associated with poor prognosis. This study aimed to identify potential drug candidates targeting KRAS G12D using combined machine learning, virtual screening, molecular docking, and molecular dynamics (MD) simulations. The training and test sets are constructed based on a selection of inhibitors targeting the KRAS G12D mutant from the ChEMBL library. A random forest machine learning algorithm is developed to predict potential KRAS G12D binders. Molecular docking and the MM/PBSA binding energy are used to identify the lead compounds. The compound NPC489264 is identified as the top candidate, exhibiting favorable docking energy for the KRAS G12D mutant (−13.16 kcal mol−1). A hydrogen bond between the mutated Asp12 residue in the KRAS G12D mutant and NPC489264 is found to be a key interaction between these 2 molecules. MD simulations and MM/PBSA analysis revealed the strong binding affinity of NPC489264 to the G12D mutant (−5.49 kcal mol−1) compared to the wild type (10.17 kcal mol−1). These findings suggest that NPC489264 is a promising lead compound for further development of KRAS G12D‐targeted cancer therapies.

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Analysis of KRAS–Ligand Interaction Modes and Flexibilities Reveals the Binding Characteristics

Cited by 4 publications

References 49 publications

How Ligands Interact with the Kinase Hinge

How Ligands Interact with the Kinase Hinge

How Ligands Interact with the Kinase Hinge

In Silico Identification of Selective KRAS G12D Inhibitor via Machine Learning‐Based Molecular Docking Combined with Molecular Dynamics Simulation

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