Structure-Based Rational Design of Constrained Peptides as TIM-3 Inhibitors

被引:4
作者
Abdel-Rahman, Somaya A. [1 ,2 ]
Ovchinnikov, Victor [3 ]
Gabr, Moustafa T. [1 ]
机构
[1] Weill Cornell Med, Mol Imaging Innovat Inst MI3, Dept Radiol, New York, NY 10065 USA
[2] Mansoura Univ, Fac Pharm, Dept Med Chem, Mansoura 35516, Egypt
[3] Harvard Univ, Dept Chem & Chem Biol, Cambridge, MA 02138 USA
来源
ACS MEDICINAL CHEMISTRY LETTERS | 2024年 / 15卷 / 06期
关键词
checkpoints; TIM-3; cancer immunotherapy; peptides; molecular dynamics simulation; CANCER; IMMUNOTHERAPY; PHAGOCYTOSIS; RESISTANCE; IG;
D O I
10.1021/acsmedchemlett.3c00567
中图分类号
R914 [药物化学];
学科分类号
100701 ;
摘要
Blocking the immunosuppressive function of T-cell immunoglobulin mucin-3 (TIM-3) is an established therapeutic strategy to maximize the efficacy of immune checkpoint inhibitors for cancer immunotherapy. Currently, effective inhibition of TIM-3 interactions relies on monoclonal antibodies (mAbs), which come with drawbacks such as immunogenicity risk, limited tumor penetration, and high manufacturing costs. Guided by the X-ray cocrystal structures of TIM-3 with mAbs, we report an in silico structure-based rational design of constrained peptides as potent TIM-3 inhibitors. The top cyclic peptide from our study (P2) binds TIM-3 with a K-D value of 166.3 +/- 12.1 nM as determined by surface plasmon resonance (SPR) screening. Remarkably, P2 efficiently inhibits key TIM-3 interactions with natural TIM-3 ligands at submicromolar concentrations in a panel of cell-free and cell-based assays. The capacity of P2 to reverse immunosuppression in T-cell/cancer cell cocultures, coupled with favorable in vitro pharmacokinetic properties, highlights the potential of P2 for further evaluation in preclinical models of immuno-oncology.
引用
收藏
页码:806 / 813
页数:8
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