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首页> 外文期刊>Theranostics >Integrin αsubv/subβsub3/sub-targeted radionuclide therapy combined with immune checkpoint blockade immunotherapy synergistically enhances anti-tumor efficacy
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Integrin αsubv/subβsub3/sub-targeted radionuclide therapy combined with immune checkpoint blockade immunotherapy synergistically enhances anti-tumor efficacy

机译:整合素α<亚> v β 3 - 特种放射性核素治疗与免疫检查点延迟免疫疗法协同增强抗肿瘤疗效

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Rationale: Radiotherapy combined with immunotherapy has revealed promising outcomes in both preclinical studies and ongoing clinical trials. Targeted radionuclide therapy (TRT) is a branch of radiotherapy concerned with the use of radioisotopes, radiolabeled molecules or nanoparticles that deliver particulate radiation to cancer cells. TRT is a promising approach in cases of metastatic disease where conventional treatments are no longer effective. The increasing use of TRT raises the question of how to best integrate TRT with immunotherapy. In this study, we proposed a novel therapeutic regimen that combined programmed death ligand 1 (PD-L1)-based immunotherapy with peptide-based TRT (sup177/supLu as the radionuclide) in the murine colon cancer model. Methods: To explore the most appropriate timing of immunotherapy after radionuclide therapy, the anti-PD-L1 antibody (αPD-L1 mAb) was delivered in a concurrent or sequential manner when sup177/supLu TRT was given. Results: The results demonstrated that TRT led to an acute increase in PD-L1 expression on T cells, and TRT in combination with αPD-L1 mAb stimulated the infiltration of CD8sup+/sup T cells, which improved local tumor control, overall survival and protection against tumor rechallenge. Moreover, our data revealed that the time window for this combination therapy may be critical to outcome. Conclusions: This therapeutic combination may be a promising approach to treating metastatic tumors in which TRT can be used. Clinical translation of the result would suggest that concurrent rather than sequential blockade of the PD-1/PD-L1 axis combined with TRT improves overall survival and long-term tumor control.
机译:理由:与免疫疗法相结合的放疗揭示了临床前研究和持续的临床试验中的有希望的结果。有针对性的放射性核素治疗(TRT)是有关使用放射性同位素,放射性标记分子或纳米颗粒的放射疗法的分支,其将颗粒状辐射递送给癌细胞。 TRT是一种有希望的方法,在转移性疾病的情况下,常规治疗不再有效。随着TRT的越来越多地提出了如何最好地整合TRT与免疫疗法的问题。在这项研究中,我们提出了一种新的治疗方案,所述治疗方案将编程的死亡配体1(PD-L1)与鼠结肠癌模型中的肽基TRT( 177 Lu作为放射性核素)组合的免疫疗法。方法:探讨放射性核素治疗后最合适的免疫疗法定时,当给出时,以同时或顺序方式递送抗PD-L1抗体(αPD-L1 mAb)。结果:结果表明,TRT导致T细胞上PD-L1表达的急性增加,TRT与αpd-l1 mab组合刺激CD8 + / sup> t细胞的渗透,这改善了局部肿瘤对照,整体存活和保护免受肿瘤重新检查。此外,我们的数据显示,这种组合治疗的时间窗口对结果至关重要。结论:这种治疗组合可能是治疗可以使用TRT的转移性肿瘤的有希望的方法。结果临床翻译表明,同时而不是连续的PD-1 / Pd-L1轴联合TRT的顺序阻滞,提高了整体存活率和长期肿瘤控制。

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