用 BRAF 抑制剂、TLR 7 激动剂和 PD-1 抗体三联疗法根除 BRAF 突变黑色素瘤的肿瘤。

IF 4.5 2区医学 Q1 ONCOLOGY

Cancer Science Pub Date : 2024-06-18 DOI:10.1111/cas.16251

Kenta Nakamura, Tomonori Yaguchi, Masashi Murata, Yosuke Ota, Asuka Mikoshiba, Yukiko Kiniwa, Ryuhei Okuyama, Yutaka Kawakami

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引用次数: 0

摘要

程序性死亡 1（PD-1）/程序性死亡配体 1 抑制剂常用于治疗各种癌症，包括黑色素瘤。然而，它们作为单一疗法的疗效有限，目前正在探索联合免疫疗法以改善疗效。在这项研究中，我们研究了一种联合免疫疗法，其中包括阻断主要适应性免疫抗性机制的抗 PD-1 抗体、抑制黑色素瘤细胞增殖的 BRAF 抑制剂和多种原发性免疫抗性机制（如癌细胞衍生的免疫抑制细胞因子），以及能增强先天性免疫反应、促进抗肿瘤 T 细胞诱导和功能的 Toll 样受体 7 激动剂。利用植入人类 BRAF 突变黑色素瘤的异种裸鼠模型，研究发现 BRAF 抑制剂 vemurafenib 可通过减少人类黑色素瘤产生的免疫抑制细胞因子（包括白细胞介素 6），恢复传统树突状细胞的 T 细胞刺激活性。此外，静脉注射 Toll 样受体 7 激动剂 DSR6434 可通过刺激浆细胞树突状细胞/干扰素-α/自然杀伤细胞通路，增强传统树突状细胞的 T 细胞刺激活性，从而增强 vemurafenib 对肿瘤生长的抑制作用。在植入小鼠BRAF突变黑色素瘤的合成小鼠模型中，vemurafenib和DSR6434的组合能协同增强黑色素瘤抗原gp100特异性T细胞的诱导作用，并抑制肿瘤生长。值得注意的是，只有vemurafenib、DSR6434和抗PD-1抗体的三联疗法才能以CD8 T细胞依赖的方式使SIY抗原诱导的BRAF突变黑色素瘤完全消退。这些研究结果表明，针对适应性和原发性抗药性机制的三重组合策略，同时加强促进肿瘤特异性T细胞的先天性免疫反应，可能是有效根除肿瘤的关键。

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Tumor eradication by triplet therapy with BRAF inhibitor, TLR 7 agonist, and PD-1 antibody for BRAF-mutated melanoma

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Tumor eradication by triplet therapy with BRAF inhibitor, TLR 7 agonist, and PD-1 antibody for BRAF-mutated melanoma

Programmed death 1 (PD-1)/programmed death-ligand 1 inhibitors are commonly used to treat various cancers, including melanoma. However, their efficacy as monotherapy is limited, and combination immunotherapies are being explored to improve outcomes. In this study, we investigated a combination immunotherapy involving an anti-PD-1 antibody that blocks the major adaptive immune-resistant mechanisms, a BRAF inhibitor that inhibits melanoma cell proliferation, and multiple primary immune-resistant mechanisms, such as cancer cell-derived immunosuppressive cytokines, and a Toll-like receptor 7 agonist that enhances innate immune responses that promote antitumor T-cell induction and functions. Using a xenogeneic nude mouse model implanted with human BRAF-mutated melanoma, a BRAF inhibitor vemurafenib was found to restore T-cell-stimulatory activity in conventional dendritic cells by reducing immunosuppressive cytokines, including interleukin 6, produced by human melanoma. Additionally, intravenous administration of the Toll-like receptor 7 agonist DSR6434 enhanced tumor growth inhibition by vemurafenib through stimulating the plasmacytoid dendritic cells/interferon-α/natural killer cell pathways and augmenting the T-cell-stimulatory activity of conventional dendritic cells. In a syngeneic mouse model implanted with murine BRAF-mutated melanoma, the vemurafenib and DSR6434 combination synergistically augmented the induction of melanoma antigen gp100-specific T cells and inhibited tumor growth. Notably, only triplet therapy with vemurafenib, DSR6434, and the anti-PD-1 antibody resulted in complete regression of SIY antigen-transduced BRAF-mutated melanoma in a CD8 T-cell-dependent manner. These findings indicate that a triple-combination strategy targeting adaptive and primary resistant mechanisms while enhancing innate immune responses that promote tumor-specific T cells may be crucial for effective tumor eradication.

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来源期刊

Cancer Science 医学-肿瘤学

自引率

3.50%

发文量

406

审稿时长

2 months

期刊介绍： Cancer Science (formerly Japanese Journal of Cancer Research) is a monthly publication of the Japanese Cancer Association. First published in 1907, the Journal continues to publish original articles, editorials, and letters to the editor, describing original research in the fields of basic, translational and clinical cancer research. The Journal also accepts reports and case reports. Cancer Science aims to present highly significant and timely findings that have a significant clinical impact on oncologists or that may alter the disease concept of a tumor. The Journal will not publish case reports that describe a rare tumor or condition without new findings to be added to previous reports; combination of different tumors without new suggestive findings for oncological research; remarkable effect of already known treatments without suggestive data to explain the exceptional result. Review articles may also be published.