肿瘤相关ADAM10和ADAM17产生可溶性PD-L1 (sPD-L1, sB7-H1)并影响下游肿瘤免疫——黑色素瘤中PD-1检查点阻断的抵抗机制

Regulating T-cells and Their Response to Cancer Pub Date : 2019-02-01 DOI:10.1158/2326-6074.CRICIMTEATIAACR18-A210

J. Orme, Khalid A Jazieh, S. Harrington, M. Ball, T. Azam, Xin Liu, Tiancheng Xie, A. Mansfield, R. Dronca, Haidong Dong

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引用次数: 0

摘要

背景:肿瘤表面PD-L1 (B7-H1)信号通过t细胞表面受体PD-1抑制抗肿瘤免疫。PD-1抑制剂如pembrolizumab阻断这一途径，防止肿瘤逃避免疫监视。这些PD-1检查点抑制剂在20-30%的黑色素瘤患者中实现了客观缓解(1-3)。由于这些患者中的大多数对这种治疗有耐药性，因此迫切需要对抗黑色素瘤中PD-1检查点抑制剂的耐药性。黑色素瘤中PD-1检查点抑制剂耐药的机制是什么?我们的研究小组报道了可溶性PD-L1 (sPD-L1, sB7-H1)在PD-1抑制剂耐药黑色素瘤和非小细胞肺癌(NSCLC)患者的血清中升高(4)。我们还表明，可溶性PD-L1是由其他肿瘤类型的切割产生的，并导致CD8+ t细胞凋亡(5)。本研究的目的是确认人类黑色素瘤中sPD-L1的来源及其与预后的关系。方法:用一系列蛋白酶抑制剂处理表达b7h1的转基因黑色素瘤细胞(Mel-B7H1) 24小时。然后将细胞制成颗粒，用ELISA分析上清液中sPD-L1 (sB7-H1)的产生。同时用ELISA检测肿瘤血清中sPD-L1的产生。对黑色素瘤患者(上述研究的血清供体)的肿瘤病理切片进行免疫组化染色，抗体为抗蛋白酶ADAM10或ADAM17。通过显微镜观察载玻片是否存在这些抗原。在安慰剂或PD-1检查点抑制剂抗体存在的情况下，用重组人B7-H1 (PD-L1)蛋白、富含spd - l1或缺乏spd - l1的肿瘤细胞系上清培养活化的人CD8+ t细胞。流式细胞术测定48h细胞存活率。结果:ADAM10抑制剂GI254023X, ADAM17抑制剂TAPI-0和广泛金属蛋白酶抑制剂TAPI-2抑制sB7H1 Mel-B7H1的产生(p引用形式:Jacob J. Orme, Khalid Jazieh, Susan Harrington, Matthew Ball, Tariq U. Azam, Xin (Cindy) Liu, Tiancheng Xie, Aaron Mansfield, Roxana S. Dronca, Haidong Dong)。肿瘤相关的ADAM10和ADAM17产生可溶性PD-L1 (sPD-L1, sB7-H1)并影响下游肿瘤免疫——黑色素瘤中PD-1检查点阻断的抵抗机制[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 A210。

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Abstract A210: Tumor-associated ADAM10 and ADAM17 produce soluble PD-L1 (sPD-L1, sB7-H1) and affect downstream tumor immunity – A resistance mechanism to PD-1 checkpoint blockade in melanoma

Background: Tumor surface PD-L1 (B7-H1) signals through T-cell surface receptor PD-1 to suppress antitumor immunity. PD-1 inhibitors like pembrolizumab block this pathway to prevent tumor escape from immunosurveillance. These PD-1 checkpoint inhibitors achieve objective response in 20-30% of patients with melanoma (1-3). As the majority of these patients are resistant to this treatment, there is a critical need to combat PD-1 checkpoint inhibitor resistance in melanoma. What is the mechanism of PD-1 checkpoint inhibitor resistance in melanoma? Our group has reported that soluble PD-L1 (sPD-L1, sB7-H1) is elevated in the serum of patients with PD-1 inhibitor-resistant melanoma and non-small cell lung cancer (NSCLC) (4). We have also shown that soluble PD-L1 is produced by cleavage from other tumor types and leads to apoptosis in CD8+ T-cells (5). The aim of this study is to confirm the source of sPD-L1 in human melanoma and its relation to outcomes. Methods: B7H1-expressing transgenic melanoma cells (Mel-B7H1) were treated with an array of protease inhibitors over 24 hours. Cells were then pelleted and supernatants were analyzed by ELISA for sPD-L1 (sB7-H1) production. Tumor serum samples were also analyzed by ELISA for sPD-L1 production.Tumor pathology slides from patients with melanoma (serum donors from the above study) were stained by immunohistochemistry with antibodies against proteases ADAM10 or ADAM17. Slides were visualized by microscopy for the presence of these antigens. Activated human CD8+ T-cells were cultured with recombinant human B7-H1 (PD-L1) protein, sPD-L1-rich, or sPD-L1-depleted supernatants from a tumor cell line in the presence of placebo or PD-1 checkpoint inhibitor antibodies. Cell survival was measured at 48 hours by flow cytometry.Results: ADAM10 inhibitor GI254023X, ADAM17 inhibitor TAPI-0, and broad metalloprotease inhibitor TAPI-2 inhibited Mel-B7H1 production of sB7H1 (p Citation Format: Jacob J. Orme, Khalid Jazieh, Susan Harrington, Matthew Ball, Tariq U. Azam, Xin (Cindy) Liu, Tiancheng Xie, Aaron Mansfield, Roxana S. Dronca, Haidong Dong. Tumor-associated ADAM10 and ADAM17 produce soluble PD-L1 (sPD-L1, sB7-H1) and affect downstream tumor immunity – A resistance mechanism to PD-1 checkpoint blockade in melanoma [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 A210.

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Regulating T-cells and Their Response to Cancer

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