Dual targeting of TGF-ß and PD-L1 inhibits tumor growth in TGF-ß/PD-L1-driven colorectal carcinoma

被引:11
|
作者
Khalili-Tanha, Ghazaleh [1 ]
Fiuji, Hamid [1 ]
Gharib, Masoumeh [2 ]
Moghbeli, Meysam [1 ]
Khalili-Tanha, Nima [1 ]
Rahmani, Farzad [1 ,3 ]
Shakour, Neda [4 ]
Maftooh, Mina [1 ]
Hassanian, Seyed Mahdi [1 ,3 ]
Asgharzadeh, Fereshteh [5 ]
Shahidsales, Soodabeh [6 ]
Anvari, Kazem [6 ]
Mozafari, M. R. [8 ]
Ferns, Gordon A. [9 ]
Batra, Jyotsna [10 ,12 ]
Giovannetti, Elisa [13 ,14 ]
Khazaei, Majid [1 ,5 ]
Avan, Amir [1 ,7 ,10 ,11 ]
机构
[1] Mashhad Univ Med Sci, Metab Syndrome Res Ctr, Mashhad, Iran
[2] Mashhad Univ Med Sci, Fac Med, Dept Pathol, Mashhad, Iran
[3] Mashhad Univ Med Sci, Fac Med, Dept Med Biochem, Mashhad, Iran
[4] Mashhad Univ Med Sci, Sch Pharm, Dept Med Chem, Mashhad, Iran
[5] Mashhad Univ Med Sci, Fac Med, Dept Physiol, Mashhad, Iran
[6] Mashhad Univ Med Sci, Canc Res Ctr, Mashhad, Iran
[7] Univ Warith Al Anbiyaa, Coll Med, Karbala, Iraq
[8] Monash Univ LPO, Australasian Nanosci & Nanotechnol Initiat ANNI, Clayton, Vic, Australia
[9] Brighton & Sussex Med Sch, Div Med Educ, Brighton BN1 9PH, Sussex, England
[10] Queensland Univ Technol, Fac Hlth, Sch Biomed Sci, Brisbane, Qld 4059, Australia
[11] Queensland Univ Technol, Sci & Engn Fac, Sch Mech Med & Proc Engn, 2 George St, Brisbane, Qld 4000, Australia
[12] Translat Res Inst, 37 Kent St, Woolloongabba, Qld 4102, Australia
[13] VU Univ Med Ctr VUMC, Canc Ctr Amsterdam, Dept Med Oncol, Amsterdam UMC, Amsterdam, Netherlands
[14] Fdn Pisana Sci, AIRC Start Unit, Canc Pharmacol Lab, Pisa, Italy
关键词
Colorectal Cancer; Bifunctional fusion protein; PD-L1/TGF-beta; Targeted therapy; CELL-MEDIATED CYTOTOXICITY; M7824; MSB0011359C; FACTOR-BETA; EXPRESSION; RESISTANCE; ACTIVATION; AVELUMAB; ALPHA;
D O I
10.1016/j.lfs.2023.121865
中图分类号
R-3 [医学研究方法]; R3 [基础医学];
学科分类号
1001 ;
摘要
Immunosuppressive factors within the tumor microenvironment (TME), such as Transforming growth factor beta (TGF-ss), constitute a crucial hindrance to immunotherapeutic approaches in colorectal cancer (CRC). Furthermore, immune checkpoint factors (e.g., programmed death-ligand 1 [PD-L1]) inhibit T-cell proliferation and activation. To cope with the inhibitory effect of immune checkpoints, the therapeutic value of dual targeting PDL1 and TGF-ss pathways via M7824 plus 5-FU in CRC has been evaluated. Integrative-systems biology approaches and RNAseq were used to assess the differential level of genes associated with 88 metastatic-CRC patients. The level of PD-L1 and TGF-ss was evaluated in a validation cohort. The anti-proliferative, migratory, and apoptotic effects of PD-L1/TGF-ss inhibitor, M7824, were assessed by MTT, wound-healing assay, and flow cytometry. Antitumor activity was assessed in a xenograft model, followed by biochemical studies and histological staining, and gene/protein expression analyses by RT-PCR and ELISA/IHC. The result of differentially expressed genes (DEGs) analysis showed 1268 upregulated and 1074 downregulated genes in CRC patients. Among the highest scoring genes and dysregulated pathways associated with CRC, PD-L1, and TGF- ss were identified and further validated in 92 CRC patients. Targeting of PD-L1-TGF- ss inhibited cell growth and migration, associated with modulation of CyclinD1 and MMP9. Furthermore, M7824 inhibited tumor growth via targeting TGF-ss and PD-L1 pathways, resulting in modulation of inflammatory response and fibrosis via TNF-alpha/IL6/CD4-8 and COL1A1/1A2, respectively. In conclusion, our data illustrated that co-targeting PD-L1 and TGF-ss pathways increased the effect of Fluorouracil (5-FU) and reduced the tumor growth in PD-L1/TGF-ss expressing tumors, providing a new therapeutic option in the treatment of CRC.
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页数:12
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