Human and mouse PD-L1: similar molecular structure, but different druggability profiles

Magiera‐Mularz, Katarzyna; Kocik, Justyna; Musielak, Bogdan; Plewka, Jacek; Sala, Dominik; Machula, Monika; Grudnik, P.; Hajduk, Malgorzata; Czepiel, Marcin; Siedlar, Maciej; Holak, Tad A.; Skalniak, Łukasz

doi:10.1016/j.isci.2020.101960

Cited by 49 publications

(65 citation statements)

References 50 publications

(71 reference statements)

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“…Durvalumab blocks the human PD-L1 but not the mouse PD-L1 protein, as we have shown in our recent manuscript [36]. In our hands, none of the small molecules and macrocyclic peptides tested in our laboratory were able to bind to mouse PD-L1, as we have verified either with the NMR study or the hybrid, mPD-L1/hPD-1 ICB assay [36]. Importantly, similar observations have been reported by others.…”

Section: Specificity Towards the Human And Mouse Pd-l1supporting

confidence: 89%

“…Out of the tested therapeutic antibodies, atezolizumab blocks both human and mouse PD-L1 (mPD-L1). Durvalumab blocks the human PD-L1 but not the mouse PD-L1 protein, as we have shown in our recent manuscript [36]. In our hands, none of the small molecules and macrocyclic peptides tested in our laboratory were able to bind to mouse PD-L1, as we have verified either with the NMR study or the hybrid, mPD-L1/hPD-1 ICB assay [36].…”

Section: Specificity Towards the Human And Mouse Pd-l1supporting

confidence: 75%

“…When defining the right model for the in vivo evaluation of the bioactivity of a drug candidate, it is crucial to determine interspecies specificity towards the molecular target. We have shown recently that despite the remarkable similarity in the structure and sequence, the mouse and human PD-L1 analogs differ greatly in their druggability profiles [36]. In the case of molecules blocking PD-L1 protein, it is thus crucial, but rare, in the manuscripts to verify the interaction with mouse PD-L1 before proceeding to the immunocompetent syngeneic mouse models.…”

Section: Specificity Towards the Human And Mouse Pd-l1mentioning

confidence: 99%

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PD-L1 Inhibitors: Different Classes, Activities, and Mechanisms of Action

Surmiak

Magiera‐Mularz

Musielak

et al. 2021

IJMS

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Targeting the programmed cell death protein 1/programmed cell death 1 ligand 1 (PD-1/PD-L1) interaction has become an established strategy for cancer immunotherapy. Although hundreds of small-molecule, peptide, and peptidomimetic inhibitors have been proposed in recent years, only a limited number of drug candidates show good PD-1/PD-L1 blocking activity in cell-based assays. In this article, we compare representative molecules from different classes in terms of their PD-1/PD-L1 dissociation capacity measured by HTRF and in vitro bioactivity determined by the immune checkpoint blockade (ICB) co-culture assay. We point to recent discoveries that underscore important differences in the mechanisms of action of these molecules and also indicate one principal feature that needs to be considered, which is the eventual human PD-L1 specificity.

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Section: Specificity Towards the Human And Mouse Pd-l1supporting

confidence: 89%

Section: Specificity Towards the Human And Mouse Pd-l1supporting

confidence: 75%

Section: Specificity Towards the Human And Mouse Pd-l1mentioning

confidence: 99%

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PD-L1 Inhibitors: Different Classes, Activities, and Mechanisms of Action

Surmiak

Magiera‐Mularz

Musielak

et al. 2021

IJMS

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“…The results are, therefore, consistent with our previous studies, in which we showed that the biphenyl moiety from anti-PD-L1 inhibitors binds to human PD-L1 and not to the murine analogue. 31 …”

Section: Results and Discussionmentioning

confidence: 99%

Terphenyl-Based Small-Molecule Inhibitors of Programmed Cell Death-1/Programmed Death-Ligand 1 Protein–Protein Interaction

et al. 2021

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We describe a new class of potent PD-L1/PD-1 inhibitors based on a terphenyl scaffold that is derived from the rigidified biphenyl-inspired structure. Using in silico docking, we designed and then experimentally demonstrated the effectiveness of the terphenyl-based scaffolds in inhibiting PD-1/PD-L1 complex formation using various biophysical and biochemical techniques. We also present a high-resolution structure of the complex of PD-L1 with one of our most potent inhibitors to identify key PD-L1/inhibitor interactions at the molecular level. In addition, we show the efficacy of our most potent inhibitors in activating the antitumor response using primary human immune cells from healthy donors.

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“…The humanized immune checkpoint mice are carefully designed as immuno-oncology mouse models for reliable in vivo evaluation and validation of checkpoint blockers drugs and their combination with other antitumor drugs ( 29 ). According to previous studies, although there are structural similarities between human and mouse PD-L1 proteins, there are significant differences in the druggability of these two proteins ( 30 ). In line with reported results, our study showed that small molecules, peptides, and some human anti-PD-L1 antibodies bound to human PD-L1, but not to mouse PD-L1.…”

Section: Discussionmentioning

confidence: 99%

Sanguisorbae Radix Suppresses Colorectal Tumor Growth Through PD-1/PD-L1 Blockade and Synergistic Effect With Pembrolizumab in a Humanized PD-L1-Expressing Colorectal Cancer Mouse Model

Lee

Kim

et al. 2021

Front. Immunol.

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Immune checkpoints such as programmed death-1 (PD-1) have been proven as antitumor targets by enhancing cytotoxic T cell activity. All immune checkpoint blockades are antibody therapeutics that have large size and high affinity, as well as known immune-related side effects and low responses. To overcome the limitation of antibody therapeutics, we have explored PD-1/PD-L1 (programmed death-ligand 1) blockades in traditional oriental medicine, which has a long history but has not yet studied PD-1/PD-L1 blockades. Sanguisorbae Radix extract (SRE) blocked PD-1 and PD-L1 binding in competitive ELISA. SRE effectively inhibited the PD-1/PD-L1 interaction, thereby improving T cell receptor (TCR) signaling and the NFAT-mediated luciferase activity of T cells. SRE treatment reduced tumor growth in the humanized PD-L1 MC38 cell allograft humanized PD-1 mouse model. Additionally, the combination of SRE and pembrolizumab (anti-PD-1 antibody) suppressed tumor growth and increased infiltrated cytotoxic T cells to a greater extent did either agent alone. This study showed that SRE alone has anticancer effects via PD-1/PD-L1 blockade and that the combination therapy of SRE and pembrolizumab has enhanced immuno-oncologic effects.

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Human and mouse PD-L1: similar molecular structure, but different druggability profiles

Cited by 49 publications

References 50 publications

PD-L1 Inhibitors: Different Classes, Activities, and Mechanisms of Action

PD-L1 Inhibitors: Different Classes, Activities, and Mechanisms of Action

Terphenyl-Based Small-Molecule Inhibitors of Programmed Cell Death-1/Programmed Death-Ligand 1 Protein–Protein Interaction

Sanguisorbae Radix Suppresses Colorectal Tumor Growth Through PD-1/PD-L1 Blockade and Synergistic Effect With Pembrolizumab in a Humanized PD-L1-Expressing Colorectal Cancer Mouse Model

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