Functional antigen processing and presentation mechanism as a prerequisite factor of response to treatment with dendritic cell vaccines and anti-PD-1 in preclinical murine LLC1 and GL261 tumor models

被引:9
|
作者
Zilionyte, Karolina [1 ,2 ]
Bagdzeviciute, Ugne [1 ,3 ]
Mlynska, Agata [1 ,3 ]
Urbstaite, Elena [4 ]
Paberale, Emilija [1 ,2 ]
Dobrovolskiene, Neringa [1 ]
Krasko, Jan Aleksander [1 ,3 ]
Pasukoniene, Vita [1 ,3 ]
机构
[1] Natl Canc Inst, Lab Immunol, Vilnius, Lithuania
[2] Vilnius Univ, Life Sci Ctr, Vilnius, Lithuania
[3] Vilnius Gediminas Tech Univ, Dept Chem & Bioengn, Vilnius, Lithuania
[4] Vilnius Univ, Fac Med, Vilnius, Lithuania
关键词
Ag processing and presentation mechanism; Immunogenicity; Dendritic cell vaccine; Anti-PD-1; Experimental tumor models; Predictive biomarkers; DEFECTS;
D O I
10.1007/s00262-022-03190-9
中图分类号
R73 [肿瘤学];
学科分类号
100214 ;
摘要
Low efficacy of cancer immunotherapy encourages the search for possible resistance mechanisms and biomarkers that would predict the outcome of immunotherapy in oncology patients. Most cancer immunotherapies act on T lymphocytes, which can specifically recognize and kill tumor cells. However, for immunotherapy-activated T lymphocytes to be able to perform these functions, proper tumor Ag processing and surface presentation by MHC-I molecule is important. Knowing the significance of Ag processing and presentation mechanism (APM) in anti-tumor immune response, we sought to evaluate how the functionality of APM affects tumor immune microenvironment and response to dendritic cell vaccines (DCV) and anti-PD-1. By comparing murine Lewis lung carcinoma LLC1 and glioma GL261 models a decreased expression of APM-related genes, such as Psmb8, Psmb9, Psmb10, Tap1, Tap2, Erap1, B2m, and low expression of surface MHC-I molecule were found in LLC1 cells. Changes in APM-related gene expression affected the ability of T lymphocytes to recognize and kill LLC1 cells, resulting in the absence of cytotoxic immune response and resistance to DCV and anti-PD-1. An emerging cytotoxic immune reaction and sensitivity to DCV and anti-PD-1 were observed in GL261 tumors where APM remained functional. This study demonstrates that one of the possible mechanisms of tumor resistance to immunotherapy is a dysfunctional APM and reveals a predictive potential of APM-related gene set expression for the personalization of dendritic cell vaccine and anti-PD-1 therapies in murine pre-treated tumors.
引用
收藏
页码:2691 / 2700
页数:10
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