Discovery of low-molecular weight anti-PD-L1 peptides for cancer immunotherapy

Líu, Hao; Zhao, Zhen; zhang, Li; Li, Yuanke; Jain, Akshay; Barve, Ashutosh; Jin, Wei; Li, Yanli; Fetse, John; Cheng, Kun

doi:10.1186/s40425-019-0705-y

Cited by 80 publications

(65 citation statements)

References 52 publications

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“…In other studies, two peptide-based PD-1/PD-L1 inhibitors were tested in syngeneic mouse models ( Liu et al., 2019 ; Sasikumar et al., 2019 ). In these studies, however, in vivo experiments were preceded by either the in vitro examination of m PD-1/ m PD-L1 blockade ( Liu et al., 2019 ) or the proliferation rescue and IFN-γ release assay on mouse splenocytes inhibited with the m PD-L1 protein ( Sasikumar et al., 2019 ). Still, the direct binding of the tested agents to the m PD-L1 protein was not confirmed.…”

Section: Discussionmentioning

confidence: 99%

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

et al. 2021

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In the development of PD-L1-blocking therapeutics, it is essential to transfer initial in vitro findings into proper in vivo animal models. Classical immunocompetent mice are attractive due to high accessibility and low experimental costs. However, it is unknown whether inter-species differences in PD-L1 sequence and structure would allow for human-mouse cross applications. Here, we disclose the first structure of the mouse (m) PD-L1 and analyze its similarity to the human (h) PD-L1. We show that mPD-L1 interacts with hPD-1 and provides a negative signal toward activated Jurkat T cells. We also show major differences in druggability between the hPD-L1 and mPD-L1 using therapeutic antibodies, a macrocyclic peptide, and small molecules. Our study indicates that while the amino acid sequence is well conserved between the hPD-L1 and mPD-L1 and overall structures are almost identical, crucial differences determine the interaction with anti-PD-L1 agents, that cannot be easily predicted in silico.

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Section: Discussionmentioning

confidence: 99%

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

et al. 2021

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“…Since this approach is ambitious, it is also essential that alternative approaches are explored to block the interaction between HLA-G and its receptors. It is important to realize that antibody-based immune checkpoint inhibitors have disadvantages, including high costs, instability, immunogenicity and poor tumor penetration [ 99 , 100 , 101 ]. Due to these disadvantages, development of immune checkpoint inhibitors has been shifted to low-molecular-weight molecules, such as small molecules and peptides.…”

Section: Hla-g As Target For Immune Checkpoint Inhibition In Cancementioning

confidence: 99%

“…Currently, development of small-molecule inhibitors is mainly focused on targeting PD-1 and its ligand PD-L1, where multiple compounds are in development and one small-molecule is already licensed [ 101 ]. However, designing small-molecule drugs is challenging due to the large surface area where the binding between the receptor and ligand takes place, the need for well-defined binding pockets, and the highly hydrophobic interaction between many receptors and their ligands (including between PD-1/PD-L1, and HLA-G/ILT2/4) [ 99 , 100 , 102 ]. Another approach is to target the mRNA of the HLA-G receptor with RNA interference (RNAi).…”

Section: Hla-g As Target For Immune Checkpoint Inhibition In Cancementioning

confidence: 99%

The Molecular and Functional Characteristics of HLA-G and the Interaction with Its Receptors: Where to Intervene for Cancer Immunotherapy?

Attia

Dessens

Water

et al. 2020

IJMS

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Human leukocyte antigen G (HLA-G) mediates maternal-fetal immune tolerance. It is also considered an immune checkpoint in cancer since it may mediate immune evasion and thus promote tumor growth. HLA-G is, therefore, a potential target for immunotherapy. However, existing monoclonal antibodies directed against HLA-G lack sufficient specificity and are not suitable for immune checkpoint inhibition in a clinical setting. For this reason, it is essential that alternative approaches are explored to block the interaction between HLA-G and its receptors. In this review, we discuss the structure and peptide presentation of HLA-G, and its interaction with the receptors Ig-like transcript (ILT) 2, ILT4, and Killer cell immunoglobulin-like receptor 2DL4 (KIR2DL4). Based on our findings, we propose three alternative strategies to block the interaction between HLA-G and its receptors in cancer immunotherapy: (1) prevention of HLA-G dimerization, (2) targeting the peptide-binding groove of HLA-G, and (3) targeting the HLA-G receptors. These strategies should be an important focus of future studies that aim to develop immune checkpoint inhibitors to block the interaction between HLA-G and its receptors for the treatment of cancer.

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“…面的数量. Cheng课题组 [41] 则利用一种新的生物淘选方法筛选出了肽CLP002, 不仅可以阻断PD-1/PD-L1通路, 还可以阻断CD80/PD-L1的相互作用, 进一步增强免疫反应. Liu课题组 .…”

Section: 在一定程度上诱导Pd-l1内在化下调Pd-l1在细胞表unclassified

Progress of new strategies on screening of targeting peptides and applications in tumor immunotherapy

Li¹,

Ma²,

Wang³

2020

Sci. Sin.-Chim

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Malignant tumor has threatened human's health. Along with the deep understanding of the mechanism of tumor immune cycle, tumor immune diagnosis and therapy have become the research hot spot. Among all the theranostic reagents, peptides have good affinity, high specificity, good biocompatibility, ease of modification and so on. Peptide-based reagents have broad application prospects and great potential in tumor immune diagnosis and therapy. This review summarizes from the aspects of some new methods and new strategies on targeting peptide probes screening and construction. Furthermore, we focus on some research progress on targeting-peptide-based tumor immunol imaging and peptide-based immune checkpoint therapy.

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Discovery of low-molecular weight anti-PD-L1 peptides for cancer immunotherapy

Cited by 80 publications

References 52 publications

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

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

The Molecular and Functional Characteristics of HLA-G and the Interaction with Its Receptors: Where to Intervene for Cancer Immunotherapy?

Progress of new strategies on screening of targeting peptides and applications in tumor immunotherapy

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