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Cryoimmunotherapy with local co-administration of ex vivo generated dendritic cells and CpG-ODN immune adjuvant, elicits a specific antitumor immunity.

机译:用局部共同施用的局部生成的树突细胞和CpG-ODN免疫辅助剂的冷冻免疫疗法引发了特异性抗肿瘤免疫力。

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摘要

Cryoablation is a low-invasive surgical procedure for management of malignant tumors. Tissue destruction is obtained by repeated deep freezing and thawing and results in coagulative necrosis and in apoptosis. This procedure induces the release of tumor-associated antigens and proinflammatory factors into the microenvironment. Local administration of immature dendritic cells (DCs) potentiates the immune response induced by cryoablation. To further augment the induction of long-lasting antitumor immunity, we investigated the clinical value of combining cryoimmunotherapy consisting of cryoablation and inoculation of immature DCs with administration of the immune adjuvant, CpG oligodeoxynucleotides. Injection of the murine Lewis lung carcinoma, D122-luc-5.5 that expresses the luciferase gene, results in spontaneous metastases, which can be easily monitored in vivo. The local tumor was treated by the combined treatment. The clinical outcome was assessed by monitoring tumor growth, metastasis in distant organs, overall survival, and protection from tumor recurrence. The nature of the induced T cell responses was analyzed. Combined cryoimmunotherapy results in reduced tumor growth, low metastasis and significantly prolonged survival. Moreover, this treatment induces antitumor memory that protected mice from rechallenge. The underlying suggested mechanisms are the generation of tumor-specific type 1 T cell responses, subsequent induction of cytotoxic T lymphocytes, and generation of systemic memory. Our data highlight the combined cryoimmunotherapy as a novel antitumor vaccine with promising preclinical results. Adjustment of this technique into practice will provide the therapeutic benefits of both, ablation of the primary tumor and induction of robust antitumor and antimetastatic immunity.
机译:冷冻剂是一种低侵入性的外科手术,用于治疗恶性肿瘤。通过重复深度冷冻和解冻获得组织破坏,并导致凝结性坏死和凋亡。该方法诱导肿瘤相关抗原和促炎因子的释放到微环境中。局部施用未成熟的树突细胞(DCS)增强了通过冷冻诱导的免疫应答。为了进一步增强持久抗肿瘤免疫的诱导,我们研究了将低温疗法组合的临床价值与免疫佐剂,CPG寡核苷酸的施用,CPG寡核苷酸的低温和接种。注射鼠路易斯肺癌,D122-Luc-5.5表达荧光素酶基因,导致自发转移,可以在体内容易地监测。通过组合治疗治疗局部肿瘤。通过监测肿瘤生长,远处的器官,总体存活和免受肿瘤复发的保护来评估临床结果。分析了诱导的T细胞应答的性质。结合冷冻剂治疗导致肿瘤生长减少,转移低,延长的存活率显着。此外,该处理诱导抗肿瘤记忆从重新检查中保护小鼠。潜在的建议机制是产生肿瘤特异性1 T细胞反应,随后诱导细胞毒性T淋巴细胞,以及产生全身存储器的产生。我们的数据突出了与具有前列临床前疫苗的新型抗肿瘤疫苗的结合冷冻疫苗。将该技术的调整为实践将提供两者的治疗益处,消融原发性肿瘤和诱导稳健的抗肿瘤和抗体抗疫苗。

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