自噬阻断上调肺癌中HLA-I类分子表达并增强抗PD-L1免疫治疗疗效。
Autophagy Blockage Up-Regulates HLA-Class-I Molecule Expression in Lung Cancer and Enhances Anti-PD-L1 Immunotherapy Efficacy.
作者信息
Xanthopoulou Erasmia, Lamprou Ioannis, Mitrakas Achilleas G, Michos Georgios D, Zois Christos E, Giatromanolaki Alexandra, Harris Adrian L, Koukourakis Michael I
机构信息
Department of Radiotherapy/Oncology, University Hospital of Alexandroupolis, Democritus University of Thrace, 68100 Alexandroupolis, Greece.
Department of Oncology, University of Oxford, Old Road Campus Research Building, Roosevelt Drive, Oxford OX3 7DQ, UK.
出版信息
Cancers (Basel). 2024 Sep 26;16(19):3272. doi: 10.3390/cancers16193272.
BACKGROUND/OBJECTIVES: Immune checkpoint inhibitors have an established role in non-small cell lung cancer (NSCLC) therapy. The loss of HLA-class-I expression allows cancer cell evasion from immune surveillance, disease progression, and failure of immunotherapy. The restoration of HLA-class-I expression may prove to be a game-changer in current immunotherapy strategies. Autophagic activity has been recently postulated to repress HLA-class-I expression in cancer cells.
METHODS
NSCLC cell lines (A549 and H1299) underwent late-stage (chloroquine and bafilomycin) and early-stage autophagy blockage (ULK1 inhibitors and MAP1LC3A silencing). The HLA-class-I expression was assessed with flow cytometry, a Western blot, and RT-PCR. NSCLC tissues were examined for MAP1LC3A and HLA-class-I expression using double immunohistochemistry. CD8+ T-cell cytotoxicity was examined in cancer cells pre-incubated with chloroquine and anti-PD-L1 monoclonal antibodies (Moabs); Results: A striking increase in HLA-class-I expression following incubation with chloroquine, bafilomycin, and IFNγ was noted in A549 and H1299 cancer cells, respectively. This effect was further confirmed in CD133+ cancer stem cells. HLA-class-I, β2-microglobulin, and TAP1 mRNA levels remained stable. Prolonged exposure to chloroquine further enhanced HLA-class-I expression. Similar results were noted following exposure to a ULK1 and a PIKfyve inhibitor. Permanent silencing of the MAP1LC3A gene resulted in enhanced HLA-class-I expression. In immunohistochemistry experiments, double LC3A+/HLA-class-I expression was seldom. Pre-incubation of H1299 cancer cells with chloroquine and anti-PD-L1 MoAbs increased the mean % of apoptotic/necrotic cells from 2.5% to 18.4%; Conclusions: Autophagy blockers acting either at late or early stages of the autophagic process may restore HLA-class-I-mediated antigen presentation, eventually leading to enhanced immunotherapy efficacy.
背景/目的:免疫检查点抑制剂在非小细胞肺癌(NSCLC)治疗中已确立了作用。HLA-I类分子表达缺失使癌细胞能够逃避免疫监视、疾病进展以及免疫治疗失败。HLA-I类分子表达的恢复可能会成为当前免疫治疗策略中的一个改变游戏规则的因素。最近有研究推测自噬活性可抑制癌细胞中HLA-I类分子的表达。
方法
NSCLC细胞系(A549和H1299)接受晚期(氯喹和巴弗洛霉素)和早期自噬阻断(ULK1抑制剂和MAP1LC3A基因沉默)。通过流式细胞术、蛋白质免疫印迹法和逆转录-聚合酶链反应评估HLA-I类分子的表达。使用双重免疫组织化学检查NSCLC组织中MAP1LC3A和HLA-I类分子的表达。在用氯喹和抗PD-L1单克隆抗体(MoAbs)预孵育的癌细胞中检测CD8 + T细胞的细胞毒性。结果:在A549和H1299癌细胞中,分别在用氯喹、巴弗洛霉素和IFNγ孵育后,HLA-I类分子表达显著增加。在CD133 +癌症干细胞中进一步证实了这种效应。HLA-I类分子、β2-微球蛋白和TAP1 mRNA水平保持稳定。长时间暴露于氯喹可进一步增强HLA-I类分子的表达。在暴露于ULK1和PIKfyve抑制剂后也观察到类似结果。MAP1LC3A基因的永久沉默导致HLA-I类分子表达增强。在免疫组织化学实验中,很少观察到双重LC3A + /HLA-I类分子表达。用氯喹和抗PD-L1 MoAbs预孵育H1299癌细胞可使凋亡/坏死细胞的平均百分比从2.5%增加到18.4%。结论:在自噬过程的晚期或早期起作用的自噬阻断剂可能会恢复HLA-I类分子介导的抗原呈递,最终提高免疫治疗效果。
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