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首页> 外文期刊>Science Immunology >A tumor-specific pro-IL-12 activates preexisting cytotoxic T cells to control established tumors
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A tumor-specific pro-IL-12 activates preexisting cytotoxic T cells to control established tumors

机译:肿瘤特异性的pro-IL-12激活了先前存在的细胞毒性T细胞以控制已建立的肿瘤

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摘要

It is a challenge to effectively reactivate preexisting tumor-infiltrating lymphocytes (TILs) without causing severe toxicity. Interleukin-12 (IL-12) can potently activate lymphocytes, but its clinical use is limited by its short half-life and dose-related toxicity. In this study, we developed a tumor-conditional IL-12 (pro-IL-12), which masked IL-12 with selective extracellular receptor–binding domains of the IL-12 receptor while preferentially and persistently activating TILs after being unmaskedby matrix metalloproteinases expressed by tumors. Systemic delivery of pro-IL-12 demonstrated reduced toxicity but better control of established tumors compared with IL-12-Fc. Mechanistically, antitumor responses induced by pro-IL-12 were dependent on TILs and IFNγ. Furthermore, direct binding of IL-12 to IL-12R on CD8~+, not CD4~+, T cells was essential for maximal effectiveness. Pro-IL-12 improved the efficacy of both immune checkpoint blockade and targeted therapy when used in combination. Therefore, our study demonstrated that pro-IL-12 could rejuvenate TILs, which then combined with current treatment modalities while limiting adverse effects for treating established tumors.
机译:有效地重新激活已经存在的肿瘤浸润淋巴细胞(TIL)而不会引起严重毒性是一个挑战。白介素12(IL-12)可以有效地激活淋巴细胞,但其临床使用受到其短期寿命和剂量相关的毒性的限制。在这项研究中,我们开发了一个肿瘤 - 条件IL-12(Pro-IL-12),该IL-12用选择性的IL-12受体 - 结合域的IL-12受体的结合域掩盖了IL-12受体的结合,同时优先且持久地激活til,在透露蛋白质酶后,以基质金属蛋白酶酶掩盖。由肿瘤表达。与IL-12-FC相比,Pro-IL-12的全身递送表现出降低的毒性,但对已建立的肿瘤的控制更好。从机械上讲,Pro-IL-12诱导的抗肿瘤反应取决于TIL和IFNγ。此外,IL-12与IL-12R的直接结合在CD8〜+上,而不是CD4〜+,T细胞对于最大有效性至关重要。组合使用时,Pro-IL-12提高了免疫检查点阻滞和靶向治疗的疗效。因此,我们的研究表明,Pro-IL-12可以恢复活力,然后将其与当前的治疗方式结合在一起,同时限制治疗已建立肿瘤的不良反应。

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