103种化疗药物对犬T细胞功能和毒性的评估

doi:10.16431/j.cnki.1671-7236.2025.09.040

Abstract

Abstract: 【Objective】 The purpose of this study was to evaluate the effects of chemotherapeutic drugs on the secretion of interferon-γ (IFN-γ),antitumor function,proliferation and cytotoxicity of T cells derived from peripheral blood of dogs,so as to screen chemotherapeutic drugs with little toxicity and impact on T cell function,in order to use alone or in combination with other immunotherapeutic drugs for the clinical treatment of canine tumor disease. 【Method】 Peripheral blood was collected from healthy dogs,and canine peripheral blood mononuclear cells (PBMCs) were isolated by density gradient centrifugation.T cells were cultured and expanded in vitro,and their proportion before and after expansion was verified by flow cytometry.103 chemotherapy drugs were applied to canine T cells at a concentration of 20 μmol/L for 48 h,and the release of IFN-γ was measured by ELISA.Based on the previous experimental data in the laboratory,drugs with anti-tumor activity and a small impact on the secretion of IFN-γ in T cells were selected.After pretreating T cells at a concentration of 20 μmol/L for 12 h,the effect of the drugs on the anti-tumor function of T cells was detected by crystal violet staining,and the toxic effects of the selected chemotherapy drugs on T cells were evaluated in detail through cytotoxicity test and LDH test. 【Result】 Canine peripheral blood T cells were successfully expanded in vitro,reaching 99.70% purity.ELISA results demonstrated that of the 103 drugs tested,14 drugs (13.59%) (including docetaxel) significantly promoted the IFN-γ secretion of T cell (P＜0.05),34 drugs (33.01%) (including brusatol) significantly inhibited the release of IFN-γ (P＜0.05),while 55 drugs (53.40%) (C8-ceramide,etc.) had no statistically significant effect(P＞0.05).Combined with previous experimental data,10 candidate chemotherapy drugs including vinblastine sulfate,C8-ceramide,2'-O-(2-methoxyethyl)-cytidine and docetaxel were identified that preserved IFN-γ production in T cells while maintaining anti-tumor efficacy against canine mammary tumors.Further functional assays confirmed that drugs such as 6-mercaptopurine,docetaxel trihydrate and 2'-O-(2-methoxyethyl)-cytidine did not significantly impair T-cell-mediated antitumor activity.Among them,2'-O-(2-methoxyethyl)-cytidine showed relatively low toxicity to canine T cells,preserving ＞85% proliferation viability while causing no significant cell death. 【Conclusion】 Compounds such as vincristine sulfate,C8-ceramide,2'-O-(2-methoxyethyl)-cytidine and docetaxel had little toxicity on canine T cells.Among them,2'-O-(2-methoxyethyl)-cytidine had low toxicity on T cells and no significant inhibitory effect on their function,and it was expected to become the preferred drug for chemotherapy or combination therapy of canine tumors.

Key words: tumor immunity; canine T lymphocytes; chemotherapy; combination therapy

CLC Number:

QIN Mengke, LI Huixin, LI Sihao, ZHANG Qichao, WANG Rongjun, MENG Qingda, XIE Shanshan. Evaluation of 103 Chemotherapy Drugs on Canine T Cell Function and Toxicity[J]. China Animal Husbandry & Veterinary Medicine, 2025, 52(9): 4453-4463.

References

[1] FLEMING J M,CREEVY K E,PROMISLOW D E.Mortality in north american dogs from 1984 to 2004:An investigation into age-,size-,and breed-related causes of death[J].Journal of Veterinary Internal Medicine,2011,25(2):187-198.
[2] SIEDLECKI C T,KASS P H,JAKUBIAK M J,et al.Evaluation of an actinomycin-D-containing combination chemotherapy protocol with extended maintenance therapy for canine lymphoma[J].Canadian Veterinary Journal,2006,47(1):52-59.
[3] SABA C F,THAMM D H,VAIL D M.Combination chemotherapy with L-asparaginase,lomustine,and prednisone for relapsed or refractory canine lymphoma[J].Journal of Veterinary Internal Medicine,2007,21(1):127-132.
[4] 孟宪兵,刘微,刘秀利,等.化疗在犬肿瘤治疗中的应用[J].黑龙江畜牧兽医,2003,4:54. MENG X B,LIU W,LIU X L,et al.Application of chemotherapy in canine tumor treatment[J].Heilongjiang Animal Science and Veterinary Medicine,2003,4:54.(in Chinese)
[5] CHAN O T,YANG L X.The immunological effects of taxanes[J].Cancer Immunology,Immunotherapy,2000,49(4-5):181-185.
[6] SCHMIDT E V,CHISAMORE M J,CHANEY M F,et al.Assessment of clinical activity of PD-1 checkpoint inhibitor combination therapies reported in clinical trials[J].JAMA Network Open,2020,3(2):e1920833.
[7] ZUO S,WANG Z,JIANG X,et al.Regulating tumor innervation by nanodrugs potentiates cancer immunochemotherapy and relieve chemotherapy-induced neuropathic pain[J].Biomaterials,2024,309:122603.
[8] HIAM-GALVEZ K J,ALLEN B M,SPITZER M H.Systemic immunity in cancer[J].Nature Reviews Cancer,2021,21(6):345-359.
[9] TEDDY L,SYLVESTER S R,O’CONNOR K S,et al.Cyclical 10-day dosing of melphalan for canine multiple myeloma[J].Veterinary and Comparative Oncology,2023,21(3):533-540.
[10] COOPER M,TSAI X,BENNETT P.Combination CCNU and vinblastine chemotherapy for canine mast cell tumours:57 cases[J]. Veterinary and Comparative Oncology,2009,7(3):196-206.
[11] DUCKETT M E,CURRAN K M,BRACHA S,et al.Retrospective evaluation of melphalan,vincristine,and cytarabine chemotherapy for the treatment of relapsed canine lymphoma[J].Journal of the American Animal Hospital Association,2024,60(1):7-14.
[12] MOIRANO S,TUREK M,SANCHEZ D,et al.Intensity-modulated radiotherapy and chemotherapy for canine right atrial tumors:A retrospective study of seven dogs[J]. Veterinary Radiology & Ultrasound,2023,64(6):1099-1102.
[13] SEWELL H F,HALBERT C F,ROBINS R A,et al.Chemotherapy-induced differential changes in lymphocyte subsets and natural-killer-cell function in patients with advanced breast cancer[J]. International Journal of Cancer,1993,55(5):735-738.
[14] GUSTAFSON C E,JADHAV R,CAO W,et al.Immune cell repertoires in breast cancer patients after adjuvant chemotherapy[J].Journal of Clinical Investigation Insight,2020,5(4):e134569.
[15] KRIS M G,HELLMANN M D,CHAFT J E.Chemotherapy for lung cancers:Here to stay[J].American Society of Clinical Oncology Educational Book,2014,34(1)：e375-e380.
[16] ZHU T,CHEN Z,JIANG G,et al.Sequential targeting hybrid nanovesicles composed of chimeric antigen receptor T-cell-derived exosomes and liposomes for enhanced cancer immunochemotherapy[J].American Chemical Society Nano,2023,17(17):16770-16786.
[17] ZHOU Z,ZHAO Y,CHEN S,et al.Cisplatin promotes the efficacy of immune checkpoint inhibitor therapy by inducing ferroptosis and activating neutrophils[J].Frontiers in Pharmacology,2022,13:870178.
[18] WALTER C U,BILLER B J,LANA S E,et al.Effects of chemotherapy on immune responses in dogs with cancer[J]. Journal of Veterinary Internal Medicine,2006,20(2):342-347.
[19] ZHANG J,LIANG R,WANG K,et al.Novel CaMKII-δ inhibitor hesperadin exerts dual functions to ameliorate cardiac ischemia/reperfusion injury and inhibit tumor growth[J].Circulation,2022,145(15):1154-1168.
[20] NAIR A,MORSY M A,JACOB S.Dose translation between laboratory animals and human in preclinical and clinical phases of drug development[J].Drug Development Research,2018,79(8):373-382.
[21] CHEN Z,KOENEMAN K S,COREY D R.Consequences of telomerase inhibition and combination treatments for the proliferation of cancer cells[J].Cancer Research,2003,63(18):5917-5925.
[22] OBEID L M,LINARDIC C M,KAROLAK L A,et al.Programmed cell death induced by ceramide[J].Science,1993,259(5102):1769-1771.
[23] PRITZL C J,SEO Y J,XIA C,et al.A ceramide analogue stimulates dendritic cells to promote T cell responses upon virus infections[J].Journal of Immunology,2015,194(9):4339-4349.
[24] CHEN A,XU M,CHEN J,et al.Plasma-based metabolomics profiling of high-risk Human papillomavirus and their emerging roles in the progression of cervical cancer[J].BioMed Research International,2022,2022(1):6207701.
[25] LÓPEZ-MARURE R,GUTIÉRREZ G,MENDOZA C,et al.Ceramide promotes the death of human cervical tumor cells in the absence of biochemical and morphological markers of apoptosis[J]. Biochemical and Biophysical Research Communications,2002,293(3):1028-1036.
[26] TSUME Y,HILFINGER J M,AMIDON G L.Enhanced cancer cell growth inhibition by dipeptide prodrugs of floxuridine:Increased transporter affinity and metabolic stability[J].Molecular Pharmaceutics,2008,5(5):717-727.
[27] ZOUEIN J,HADDAD F G,EID R,et al.The combination of immune checkpoint inhibitors and chemotherapy in advanced non-small-cell lung cancer:The rational choice[J].Immunotherapy,2022,14(2):155-167.
[28] PREVEDEL N E,MEE M W,WOOD G A,et al.Effect of proteasome inhibitors on canine lymphoma cell response to CHOP chemotherapy in vitro[J].Veterinary and Comparative Oncology,2024,22(1):96-105.

Evaluation of 103 Chemotherapy Drugs on Canine T Cell Function and Toxicity

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