{"title":"A158:向树突状细胞输送I型干扰素可促进肿瘤根除和免疫联合治疗","authors":"J. Tavernier","doi":"10.1158/2326-6074.CRICIMTEATIAACR18-A158","DOIUrl":null,"url":null,"abstract":"An ideal generic cancer immunotherapy should mobilize the immune system to destroy tumor cells without harming healthy cells and remain active in case of recurrence. Furthermore, it should preferably not rely on tumor-specific surface markers, as these are only available in a limited set of malignancies. Despite approval for treatment of various cancers, clinical application of cytokines is still impeded by their multiple toxic side effects. Type I interferon (IFN), for instance, has a long history in the treatment of cancer, but its multifaceted activity pattern and complex side effects prevent its optimal clinical use. Here we develop AcTakines (Activity-on-Target cytokines), optimized (mutated) immunocytokines that are up to 1000-fold more potent on targeT-cells, allowing specific signaling in selected cell types only. As conventional dendritic cells (cDC) are essential for IFN antitumor efficacy, we targeted type I IFN-derived “AcTaferon (AFN)” to Clec9A+ cDC. Clec9A-AFN therapy displayed strong antitumor activity in murine melanoma (B16), breast carcinoma (4T1) and lymphoma models (A20), as well as against human RL lymphoma in immunodeficient NSG mice reconstituted with a human immune system. In sharp contrast to wild-type IFN therapy, the antitumor efficacy of Clec9A-AFN was not accompanied by any detectable toxicity, assessed by body weight and several hematologic parameters. Clec9A-AFN effects were lost in CD8-depleted or Batf3-/- mice, and depended on IFN signaling in cDCs but not in T lymphocytes. Combined with anti-PDL1 immune checkpoint blockade, Treg-depleting anti-CTLA4 + anti-OX40 therapy, immunogenic chemotherapy, or low-dose TNF, complete tumor regressions and long-lasting tumor immunity (memory) were obtained, still without any adverse effects. Our findings thus indicate that DC-targeted AFN provides a highly efficient, off-the-shelf and safe cancer immunotherapy, with possible application in a broad range of malignancies. Citation Format: Jan H. Tavernier. Delivering type I interferon to dendritic cells empowers tumor eradication and immune combination treatments [abstract]. In: Proceedings of the Fourth CRI-CIMT-EATI-AACR International Cancer Immunotherapy Conference: Translating Science into Survival; Sept 30-Oct 3, 2018; New York, NY. 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Despite approval for treatment of various cancers, clinical application of cytokines is still impeded by their multiple toxic side effects. Type I interferon (IFN), for instance, has a long history in the treatment of cancer, but its multifaceted activity pattern and complex side effects prevent its optimal clinical use. Here we develop AcTakines (Activity-on-Target cytokines), optimized (mutated) immunocytokines that are up to 1000-fold more potent on targeT-cells, allowing specific signaling in selected cell types only. As conventional dendritic cells (cDC) are essential for IFN antitumor efficacy, we targeted type I IFN-derived “AcTaferon (AFN)” to Clec9A+ cDC. Clec9A-AFN therapy displayed strong antitumor activity in murine melanoma (B16), breast carcinoma (4T1) and lymphoma models (A20), as well as against human RL lymphoma in immunodeficient NSG mice reconstituted with a human immune system. In sharp contrast to wild-type IFN therapy, the antitumor efficacy of Clec9A-AFN was not accompanied by any detectable toxicity, assessed by body weight and several hematologic parameters. Clec9A-AFN effects were lost in CD8-depleted or Batf3-/- mice, and depended on IFN signaling in cDCs but not in T lymphocytes. Combined with anti-PDL1 immune checkpoint blockade, Treg-depleting anti-CTLA4 + anti-OX40 therapy, immunogenic chemotherapy, or low-dose TNF, complete tumor regressions and long-lasting tumor immunity (memory) were obtained, still without any adverse effects. Our findings thus indicate that DC-targeted AFN provides a highly efficient, off-the-shelf and safe cancer immunotherapy, with possible application in a broad range of malignancies. Citation Format: Jan H. Tavernier. Delivering type I interferon to dendritic cells empowers tumor eradication and immune combination treatments [abstract]. In: Proceedings of the Fourth CRI-CIMT-EATI-AACR International Cancer Immunotherapy Conference: Translating Science into Survival; Sept 30-Oct 3, 2018; New York, NY. 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引用次数: 0
摘要
一种理想的通用癌症免疫疗法应该动员免疫系统在不伤害健康细胞的情况下摧毁肿瘤细胞,并在复发的情况下保持活性。此外,它最好不依赖于肿瘤特异性表面标志物,因为这些仅在有限的恶性肿瘤中可用。尽管已被批准用于治疗多种癌症,但细胞因子的临床应用仍然受到其多重毒副作用的阻碍。例如,I型干扰素(IFN)在治疗癌症方面有着悠久的历史,但其多方面的活性模式和复杂的副作用阻碍了其最佳临床应用。在这里,我们开发了AcTakines(活性靶细胞因子),优化(突变)免疫细胞因子,其对靶细胞的效力高达1000倍,仅在选定的细胞类型中允许特定的信号传导。由于传统的树突状细胞(cDC)对IFN的抗肿瘤作用至关重要,我们将I型IFN衍生的“AcTaferon (AFN)”靶向Clec9A+ cDC。Clec9A-AFN治疗在小鼠黑色素瘤(B16)、乳腺癌(4T1)和淋巴瘤模型(A20)中显示出较强的抗肿瘤活性,在用人类免疫系统重建的免疫缺陷NSG小鼠中也显示出较强的抗人RL淋巴瘤活性。与野生型IFN治疗形成鲜明对比的是,通过体重和几个血液学参数评估,Clec9A-AFN的抗肿瘤疗效没有任何可检测到的毒性。在cd8缺失或Batf3-/-小鼠中,Clec9A-AFN的作用消失,并且依赖于cDCs中的IFN信号,而不依赖于T淋巴细胞。联合抗pdl1免疫检查点阻断、treg消耗抗ctla4 +抗ox40治疗、免疫原性化疗或低剂量TNF,获得肿瘤完全消退和持久的肿瘤免疫(记忆),仍无任何不良反应。因此,我们的研究结果表明,针对dc的AFN提供了一种高效、现成和安全的癌症免疫疗法,可能应用于广泛的恶性肿瘤。引用格式:Jan H. Tavernier。将I型干扰素输送到树突状细胞使肿瘤根除和免疫联合治疗成为可能[摘要]。第四届CRI-CIMT-EATI-AACR国际癌症免疫治疗会议:将科学转化为生存;2018年9月30日至10月3日;纽约,纽约。费城(PA): AACR;癌症免疫学杂志,2019;7(2增刊):摘要nr A158。
Abstract A158: Delivering type I interferon to dendritic cells empowers tumor eradication and immune combination treatments
An ideal generic cancer immunotherapy should mobilize the immune system to destroy tumor cells without harming healthy cells and remain active in case of recurrence. Furthermore, it should preferably not rely on tumor-specific surface markers, as these are only available in a limited set of malignancies. Despite approval for treatment of various cancers, clinical application of cytokines is still impeded by their multiple toxic side effects. Type I interferon (IFN), for instance, has a long history in the treatment of cancer, but its multifaceted activity pattern and complex side effects prevent its optimal clinical use. Here we develop AcTakines (Activity-on-Target cytokines), optimized (mutated) immunocytokines that are up to 1000-fold more potent on targeT-cells, allowing specific signaling in selected cell types only. As conventional dendritic cells (cDC) are essential for IFN antitumor efficacy, we targeted type I IFN-derived “AcTaferon (AFN)” to Clec9A+ cDC. Clec9A-AFN therapy displayed strong antitumor activity in murine melanoma (B16), breast carcinoma (4T1) and lymphoma models (A20), as well as against human RL lymphoma in immunodeficient NSG mice reconstituted with a human immune system. In sharp contrast to wild-type IFN therapy, the antitumor efficacy of Clec9A-AFN was not accompanied by any detectable toxicity, assessed by body weight and several hematologic parameters. Clec9A-AFN effects were lost in CD8-depleted or Batf3-/- mice, and depended on IFN signaling in cDCs but not in T lymphocytes. Combined with anti-PDL1 immune checkpoint blockade, Treg-depleting anti-CTLA4 + anti-OX40 therapy, immunogenic chemotherapy, or low-dose TNF, complete tumor regressions and long-lasting tumor immunity (memory) were obtained, still without any adverse effects. Our findings thus indicate that DC-targeted AFN provides a highly efficient, off-the-shelf and safe cancer immunotherapy, with possible application in a broad range of malignancies. Citation Format: Jan H. Tavernier. Delivering type I interferon to dendritic cells empowers tumor eradication and immune combination treatments [abstract]. In: Proceedings of the Fourth CRI-CIMT-EATI-AACR International Cancer Immunotherapy Conference: Translating Science into Survival; Sept 30-Oct 3, 2018; New York, NY. Philadelphia (PA): AACR; Cancer Immunol Res 2019;7(2 Suppl):Abstract nr A158.
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