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Development of Glycosylation-Modified DPPA-1 Compounds as Innovative PD-1/PD-L1 Blockers: Design, Synthesis, and Biological Evaluation
by
Dong, Xiaodan
, Guo, Jingjing
, Wu, Ziyuan
, Peng, Lizeng
, Peng, Chune
, Mao, Longfei
, Hou, Xixi
, Zhang, Zhe
, Zhao, Wenshan
, Deng, Peng
in
Antibiotics
/ Binding sites
/ cancer immunotherapy
/ Cancer therapies
/ Dendritic cells
/ Drug development
/ Drugs
/ Glycoproteins
/ Glycosylation
/ Hydrogen bonds
/ immune checkpoint
/ Lymphocytes
/ Medical research
/ PD-1/PD-L1
/ peptide
/ Peptides
/ Physiology
/ Proteins
/ Toxicity
2024
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Development of Glycosylation-Modified DPPA-1 Compounds as Innovative PD-1/PD-L1 Blockers: Design, Synthesis, and Biological Evaluation
by
Dong, Xiaodan
, Guo, Jingjing
, Wu, Ziyuan
, Peng, Lizeng
, Peng, Chune
, Mao, Longfei
, Hou, Xixi
, Zhang, Zhe
, Zhao, Wenshan
, Deng, Peng
in
Antibiotics
/ Binding sites
/ cancer immunotherapy
/ Cancer therapies
/ Dendritic cells
/ Drug development
/ Drugs
/ Glycoproteins
/ Glycosylation
/ Hydrogen bonds
/ immune checkpoint
/ Lymphocytes
/ Medical research
/ PD-1/PD-L1
/ peptide
/ Peptides
/ Physiology
/ Proteins
/ Toxicity
2024
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Development of Glycosylation-Modified DPPA-1 Compounds as Innovative PD-1/PD-L1 Blockers: Design, Synthesis, and Biological Evaluation
by
Dong, Xiaodan
, Guo, Jingjing
, Wu, Ziyuan
, Peng, Lizeng
, Peng, Chune
, Mao, Longfei
, Hou, Xixi
, Zhang, Zhe
, Zhao, Wenshan
, Deng, Peng
in
Antibiotics
/ Binding sites
/ cancer immunotherapy
/ Cancer therapies
/ Dendritic cells
/ Drug development
/ Drugs
/ Glycoproteins
/ Glycosylation
/ Hydrogen bonds
/ immune checkpoint
/ Lymphocytes
/ Medical research
/ PD-1/PD-L1
/ peptide
/ Peptides
/ Physiology
/ Proteins
/ Toxicity
2024
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Development of Glycosylation-Modified DPPA-1 Compounds as Innovative PD-1/PD-L1 Blockers: Design, Synthesis, and Biological Evaluation
Journal Article
Development of Glycosylation-Modified DPPA-1 Compounds as Innovative PD-1/PD-L1 Blockers: Design, Synthesis, and Biological Evaluation
2024
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Overview
In the context of peptide drug development, glycosylation plays a pivotal role. Accordingly, L-type peptides were synthesized predicated upon the PD-1/PD-L1 blocker DPPA-1. Subsequent glycosylation resulted in the production of two distinct glycopeptides, D-glu-LPPA-1 and D-gal-LPPA-1, by using D-glucose (D-glu) and D-galactose (D-gal), respectively, during glycosylation. Both glycopeptides significantly inhibited the interaction between PD-1 and PD-L1, and the measured half maximal inhibitory concentrations (IC50s) were 75.5 μM and 101.9 μM for D-glu-LPPA-1 and D-gal-LPPA-1, respectively. Furthermore, D-gal-LPPA-1 displayed a pronounced ability to restore T-cell functionality. In an MC38 tumor-bearing mouse model, D-gal-LPPA-1 demonstrated a significant inhibitory effect. Notably, D-gal-LPPA-1 substantially augmented the abundance and functionality of CD8+ T cells in the tumor microenvironment. Additionally, in the lymph nodes and spleens, D-gal-LPPA-1 significantly increased the proportion of CD8+ T cells secreting interferon-gamma (IFN-γ). These strong findings position D-gal-LPPA-1 as a potent enhancer of the antitumor immune response in MC38 tumor-bearing mice, underscoring its potential as a formidable PD-1/PD-L1 blocking agent.
Publisher
MDPI AG
Subject
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