Turning a Tumor Microenvironment Pitfall into Opportunity: Discovery of Benzamidoxime as PD-L1 Ligand with pH-Dependent Potency

Bianconi, Elisa; Riccio, Alessandra; Ruta, Luana; Bigiotti, Carlo; Carotti, Andrea; Moretti, Sonia; Cerra, Bruno; Gioiello, Antimo; Ferlin, Simone; Puxeddu, Efisio; Macchiarulo, Antonio

doi:10.3390/ijms24065535

Cited by 3 publications

(1 citation statement)

References 45 publications

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“…The most active compound, VIS310 ( Figure 9 ), showed a high-micromolar dissociation constant (Kd = 163.75 ± 33.61 μM), and better binding efficiency index (BEI = 21.0) than BMS-202 (Kd = 8.13 ± 1.38 μM; BEI = 12.1). Since VIS310 was the only substituted benzamidoxime of the analyzed database, the analogue-based approach to screen the REAL database of Enamine, containing about 43.8 million drug-like compounds, was used to define the structure-activity relationships of benzamidoxime compounds [ 91 ].…”

Section: Computational Studies Contributing To the Identification Of ...mentioning

confidence: 99%

A Comprehensive Computational Insight into the PD-L1 Binding to PD-1 and Small Molecules

Fantacuzzi,

Paciotti,

Agamennone

2024

Pharmaceuticals

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Immunotherapy has marked a revolution in cancer therapy. The most extensively studied target in this field is represented by the protein–protein interaction between PD-1 and its ligand, PD-L1. The promising results obtained with the clinical use of monoclonal antibodies (mAbs) directed against both PD-1 and PD-L1 have prompted the search for small-molecule binders capable of disrupting the protein–protein contact and overcoming the limitations presented by mAbs. The disclosure of the first X-ray complexes of PD-L1 with BMS ligands showed the protein in dimeric form, with the ligand in a symmetrical hydrophobic tunnel. These findings paved the way for the discovery of new ligands. To this end, and to understand the binding mechanism of small molecules to PD-L1 along with the dimerization process, many structure-based computational studies have been applied. In the present review, we examined the most relevant articles presenting computational analyses aimed at elucidating the binding mechanism of PD-L1 with PD-1 and small molecule ligands. Additionally, virtual screening studies that identified validated PD-L1 ligands were included. The relevance of the reported studies highlights the increasingly prominent role that these techniques can play in chemical biology and drug discovery.

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Section: Computational Studies Contributing To the Identification Of ...mentioning

confidence: 99%

A Comprehensive Computational Insight into the PD-L1 Binding to PD-1 and Small Molecules

Fantacuzzi,

Paciotti,

Agamennone

2024

Pharmaceuticals

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Recent developments in molecular modeling tools and applications related to pharmaceutical and biomedical research

Peluso,

Chankvetadze

2024

Journal of Pharmaceutical and Biomedical Analysis

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Interaction of telmisartan and related sartans with the programmed cell death-ligand 1 (PD-L1) protein dimer: a molecular docking analysis

Vergoten,

Bailly

2023

Futur J Pharm Sci

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BackgroundTelmisartan (TLT) is a prototypic angiotensin receptor blocker largely used to treat hypertension worldwide. In addition to its cardioprotective effects, TLT presents pleiotropic activities and notably displays noticeable anti-inflammatory and antitumor effects. The repression of the programmed cell death-1 (PD-1)/programmed death-ligand 1 (PD-L1) immune checkpoint may be implicated antitumor action of TLT, as it is the case with many other compounds equipped with a biphenyl moiety. We have used molecular modeling to compare the interaction of TLT and derivatives with the PD-L1 dimer protein.ResultsTwo molecules, TLT-dimer and TLT-acylglucuronide, were found to form more stable complexes with PD-L1 than TLT itself. In parallel, the docking analysis performed with a series of 12 sartans led to the identification of Olmesartan as a potential PD-L1 binder. The stacked biphenyl unit of Olmesartan positions the molecule along the groove delimited by the two protein monomers. The flanking tetrazole and imidazole moieties, on each side of the biphenyl unit of Olmesartan, contribute favorably to the protein interaction via specific hydrogen bonding interactions.ConclusionsThe computational analysis suggests a possible binding of Olmesartan to PD-L1 dimer and thus offers novel perspectives for the design of small molecules capable of interrupting the PD-1/PD-L1 immune checkpoint. Experimental studies are warranted to validate the hypothesis.Graphical abstract

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Turning a Tumor Microenvironment Pitfall into Opportunity: Discovery of Benzamidoxime as PD-L1 Ligand with pH-Dependent Potency

Cited by 3 publications

References 45 publications

A Comprehensive Computational Insight into the PD-L1 Binding to PD-1 and Small Molecules

A Comprehensive Computational Insight into the PD-L1 Binding to PD-1 and Small Molecules

Recent developments in molecular modeling tools and applications related to pharmaceutical and biomedical research

Interaction of telmisartan and related sartans with the programmed cell death-ligand 1 (PD-L1) protein dimer: a molecular docking analysis

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