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Sequencing of Ipilimumab Plus Nivolumab and Encorafenib Plus Binimetinib for Untreated -Mutated Metastatic Melanoma (SECOMBIT): A Randomized, Three-Arm, Open-Label Phase II Trial.Ipilimumab 联合 Nivolumab、Encorafenib 联合 Binimetinib 治疗未经治突变型转移性黑色素瘤(SECOMBIT):一项随机、三臂、开放标签的 II 期试验。
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A phase 1-2 trial of sitravatinib and nivolumab in clear cell renal cell carcinoma following progression on antiangiogenic therapy.在抗血管生成治疗进展后,西他拉替尼联合纳武利尤单抗治疗透明细胞肾细胞癌的 1-2 期临床试验。
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Pan-cancer analysis of SETD2 mutation and its association with the efficacy of immunotherapy.SETD2突变的泛癌分析及其与免疫治疗疗效的关联
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High tumor mutation burden fails to predict immune checkpoint blockade response across all cancer types.高肿瘤突变负担未能预测所有癌症类型的免疫检查点阻断反应。
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SETD2 缺失与 ATR 抑制协同作用促进肾细胞癌的 cGAS 信号转导和免疫治疗反应。

SETD2 Loss and ATR Inhibition Synergize to Promote cGAS Signaling and Immunotherapy Response in Renal Cell Carcinoma.

机构信息

Department of Genitourinary Medical Oncology, The University of Texas MD Anderson Cancer Center, Houston, Texas.

Center for Immunotherapy and Precision Immuno-Oncology, Cleveland Clinic, Cleveland, Ohio.

出版信息

Clin Cancer Res. 2023 Oct 2;29(19):4002-4015. doi: 10.1158/1078-0432.CCR-23-1003.

DOI:10.1158/1078-0432.CCR-23-1003
PMID:37527013
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC10592192/
Abstract

PURPOSE

Immune checkpoint blockade (ICB) demonstrates durable clinical benefits in a minority of patients with renal cell carcinoma (RCC). We aimed to identify the molecular features that determine the response and develop approaches to enhance it.

EXPERIMENTAL DESIGN

We investigated the effects of SET domain-containing protein 2 (SETD2) loss on the DNA damage response pathway, the cytosolic DNA-sensing pathway, the tumor immune microenvironment, and the response to ataxia telangiectasia and rad3-related (ATR) and checkpoint inhibition in RCC.

RESULTS

ATR inhibition activated the cyclic GMP-AMP synthase (cGAS)-interferon regulatory factor 3 (IRF3)-dependent cytosolic DNA-sensing pathway, resulting in the concurrent expression of inflammatory cytokines and immune checkpoints. Among the common RCC genotypes, SETD2 loss is associated with preferential ATR activation and sensitizes cells to ATR inhibition. SETD2 knockdown promoted the cytosolic DNA-sensing pathway in response to ATR inhibition. Treatment with the ATR inhibitor VE822 concurrently upregulated immune cell infiltration and immune checkpoint expression in Setd2 knockdown Renca tumors, providing a rationale for ATR inhibition plus ICB combination therapy. Setd2-deficient Renca tumors demonstrated greater vulnerability to ICB monotherapy or combination therapy with VE822 than Setd2-proficient tumors. Moreover, SETD2 mutations were associated with a higher response rate and prolonged overall survival in patients with ICB-treated RCC but not in patients with non-ICB-treated RCC.

CONCLUSIONS

SETD2 loss and ATR inhibition synergize to promote cGAS signaling and enhance immune cell infiltration, providing a mechanistic rationale for the combination of ATR and checkpoint inhibition in patients with RCC with SETD2 mutations.

摘要

目的

免疫检查点阻断(ICB)在少数肾细胞癌(RCC)患者中显示出持久的临床获益。我们旨在确定决定反应的分子特征,并开发增强反应的方法。

实验设计

我们研究了 SET 结构域包含蛋白 2(SETD2)缺失对 DNA 损伤反应途径、细胞质 DNA 感应途径、肿瘤免疫微环境以及对共济失调毛细血管扩张症和 rad3 相关(ATR)和检查点抑制的影响在 RCC 中。

结果

ATR 抑制激活了环鸟苷酸-AMP 合酶(cGAS)-干扰素调节因子 3(IRF3)依赖性细胞质 DNA 感应途径,导致炎症细胞因子和免疫检查点的同时表达。在常见的 RCC 基因型中,SETD2 缺失与 ATR 的优先激活相关,并使细胞对 ATR 抑制敏感。SETD2 敲低促进了 ATR 抑制时细胞质 DNA 感应途径的激活。用 ATR 抑制剂 VE822 同时上调 Setd2 敲低 Renca 肿瘤中的免疫细胞浸润和免疫检查点表达,为 ATR 抑制加 ICB 联合治疗提供了依据。与 Setd2 功能正常的肿瘤相比,Setd2 缺陷的 Renca 肿瘤对 ICB 单药治疗或与 VE822 的联合治疗更敏感。此外,SETD2 突变与接受 ICB 治疗的 RCC 患者的更高反应率和更长的总生存期相关,但与接受非 ICB 治疗的 RCC 患者无关。

结论

SETD2 缺失和 ATR 抑制协同促进 cGAS 信号转导并增强免疫细胞浸润,为 SETD2 突变的 RCC 患者联合应用 ATR 和检查点抑制剂提供了机制依据。