Frazer Institute, Faculty of Medicine, The University of Queensland, Brisbane, Queensland, Australia.
Queensland Emory Drug Discovery Initiative, UniQuest, The University of Queensland, Brisbane, Queensland, Australia.
J Immunother Cancer. 2023 Sep;11(9). doi: 10.1136/jitc-2023-006783.
Immunosuppressive drugs such as tacrolimus have revolutionized our ability to transplant organs between individuals. Tacrolimus acts systemically to suppress the activity of T-cells within and around transplanted organs. However, tacrolimus also suppresses T-cell function in the skin, contributing to a high incidence of skin cancer and associated mortality and morbidity in solid organ transplant recipients. Here, we aimed to identify a compound capable of re-establishing antitumor T-cell control in the skin despite the presence of tacrolimus.
In this study, we performed time-resolved fluorescence resonance energy transfer to identify molecules capable of antagonizing the interaction between tacrolimus and FKBP12. The capacity of these molecules to rescue mouse and human T-cell function in the presence of tacrolimus was determined in vitro, and the antitumor effect of the lead compound, Q-2361, was assessed in "regressor" models of skin cancer in immunosuppressed mice. Systemic CD8 T-cell depletion and analyses of intratumoral T-cell activation markers and effector molecule production were performed to determine the mechanism of tumor rejection. Pharmacokinetic studies of topically applied Q-2361 were performed to assess skin and systemic drug exposure.
Q-2361 potently blocked the interaction between tacrolimus and FKBP12 and reversed the inhibition of the nuclear factor of activated T cells activation by tacrolimus following T-cell receptor engagement in human Jurkat cells. Q-2361 rescued T-cell function in the presence of tacrolimus, rapamycin, and everolimus. Intratumoral injection of Q-2361-induced tumor regression in mice systemically immune suppressed with tacrolimus. Mechanistically, Q-2361 treatment permitted T-cell activation, proliferation, and effector function within tumors. When CD8 T cells were depleted, Q-2361 could not induce tumor regression. A simple solution-based Q-2361 topical formulation achieved high and sustained residence in the skin with negligible drug in the blood.
Our findings demonstrate that the local application of Q-2361 permits T-cells to become activated driving tumor rejection in the presence of tacrolimus. The data presented here suggests that topically applied Q-2361 has great potential for the reactivation of T-cells in the skin but not systemically, and therefore represents a promising strategy to prevent or treat skin malignancies in immunosuppressed organ transplant recipients.
免疫抑制剂如他克莫司彻底改变了我们在个体间进行器官移植的能力。他克莫司在体内系统地抑制移植器官内和周围的 T 细胞活性。然而,他克莫司也抑制皮肤中的 T 细胞功能,导致实体器官移植受者皮肤癌发病率高,死亡率和发病率高。在这里,我们旨在确定一种能够在存在他克莫司的情况下重新建立抗肿瘤 T 细胞控制的化合物。
在这项研究中,我们进行了时间分辨荧光共振能量转移,以鉴定能够拮抗他克莫司与 FKBP12 相互作用的分子。在体外确定了这些分子在存在他克莫司的情况下恢复小鼠和人 T 细胞功能的能力,并在免疫抑制小鼠的“消退”皮肤癌模型中评估了先导化合物 Q-2361 的抗肿瘤作用。进行了全身 CD8 T 细胞耗竭以及分析肿瘤内 T 细胞激活标志物和效应分子产生的研究,以确定肿瘤排斥的机制。进行了局部应用 Q-2361 的药代动力学研究,以评估皮肤和全身的药物暴露。
Q-2361 可有效阻断他克莫司与 FKBP12 的相互作用,并在人 Jurkat 细胞中 T 细胞受体结合后逆转他克莫司对 T 细胞激活核因子的抑制作用。Q-2361 在存在他克莫司,雷帕霉素和依维莫司的情况下恢复了 T 细胞的功能。在全身性免疫抑制用他克莫司的小鼠中,肿瘤内注射 Q-2361 可诱导肿瘤消退。从机制上讲,Q-2361 治疗可允许 T 细胞在肿瘤内激活,增殖和发挥效应功能。当耗尽 CD8 T 细胞时,Q-2361 不能诱导肿瘤消退。一种简单的基于溶液的 Q-2361 局部制剂可在皮肤中实现高且持续的保留,而血液中的药物含量可忽略不计。
我们的研究结果表明,局部应用 Q-2361 可使 T 细胞在存在他克莫司的情况下激活,从而驱动肿瘤排斥。这里提供的数据表明,局部应用 Q-2361 具有在皮肤中重新激活 T 细胞但不全身激活的巨大潜力,因此代表了预防或治疗免疫抑制器官移植受者皮肤恶性肿瘤的有希望的策略。
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