树突状细胞疗法通过释放系统性 CD4 T 细胞应答,增强 CDK4/6 抑制和免疫检查点阻断引发的抗肿瘤免疫。
Dendritic cell therapy augments antitumor immunity triggered by CDK4/6 inhibition and immune checkpoint blockade by unleashing systemic CD4 T-cell responses.
机构信息
Department of Pathology, The Ohio State University, Columbus, Ohio, USA
Department of Internal Medicine, University of Texas Southwestern Medical Center, Dallas, Texas, USA
出版信息
J Immunother Cancer. 2023 May;11(5). doi: 10.1136/jitc-2022-006019.
BACKGROUND
Cyclin-dependent kinase 4/6 inhibitors (CDK4/6i) combined with endocrine therapy are a mainstay treatment for hormone receptor-positive breast cancer. While their principal mechanism is inhibition of cancer cell proliferation, preclinical and clinical evidence suggests that CDK4/6i can also promote antitumor T-cell responses. However, this pro-immunogenic property is yet to be successfully harnessed in the clinic, as combining CDK4/6i with immune checkpoint blockade (ICB) has not shown a definitive benefit in patients.
METHOD
We performed an in-depth analysis of the changes in the tumor immune microenvironment and systemic immune modulation associated with CDK4/6i treatment in muring breast cancer models and in patients with breast cancer using high dimensional flow cytometry and RNA sequencing. Gain and loss of function in vivo experiments employing cell transfer and depletion antibody were performed to uncover immune cell populations critical for CDK4/6i-mediated stimulation of antitumor immunity.
RESULTS
We found that loss of dendritic cells (DCs) within the tumor microenvironment resulting from CDK4/6 inhibition in bone marrow progenitors is a major factor limiting antitumor immunity after CDK4/6i and ICB. Consequently, restoration of DC compartment by adoptively transferring ex vivo differentiated DCs to mice treated with CDK4/6i and ICB therapy enabled robust tumor inhibition. Mechanistically, the addition of DCs promoted the induction of tumor-localized and systemic CD4 T-cell responses in mice receiving CDK4/6i-ICB-DC combination therapy, as characterized by enrichment of programmed cell death protein-1-negative T helper (Th)1 and Th2 cells with an activated phenotype. CD4 T-cell depletion abrogated the antitumor benefit of CDK4/6i-ICB-DC combination, with outgrowing tumors displaying an increased proportion of terminally exhausted CD8 T cells.
CONCLUSIONS
Our findings suggest that CDK4/6i-mediated DC suppression limits CD4 T-cell responses essential for the sustained activity of CD8 T cells and tumor inhibition. Furthermore, they imply that restoring DC-CD4 T-cell crosstalk via DC transfer enables effective breast cancer immunity in response to CDK4/6i and ICB treatment.
背景
细胞周期蛋白依赖性激酶 4/6 抑制剂(CDK4/6i)联合内分泌治疗是激素受体阳性乳腺癌的主要治疗方法。虽然其主要机制是抑制癌细胞增殖,但临床前和临床证据表明,CDK4/6i 还可以促进抗肿瘤 T 细胞反应。然而,这种免疫原性特性尚未在临床上成功利用,因为 CDK4/6i 与免疫检查点阻断(ICB)联合使用并未在患者中显示出明确的益处。
方法
我们使用高维流式细胞术和 RNA 测序,对 CDK4/6i 治疗在乳腺癌模型和乳腺癌患者中引起的肿瘤免疫微环境变化和全身免疫调节进行了深入分析。通过细胞转移和耗竭抗体进行体内增益和功能丧失实验,以揭示对 CDK4/6i 介导的抗肿瘤免疫刺激至关重要的免疫细胞群。
结果
我们发现,骨髓祖细胞中 CDK4/6 抑制导致肿瘤微环境中树突状细胞(DC)的丧失是 CDK4/6i 和 ICB 后限制抗肿瘤免疫的主要因素。因此,通过将体外分化的 DC 过继转移到接受 CDK4/6i 和 ICB 治疗的小鼠中,恢复 DC 区室,使肿瘤得到强有力的抑制。从机制上讲,在接受 CDK4/6i-ICB-DC 联合治疗的小鼠中,DC 的添加促进了肿瘤局部和全身 CD4 T 细胞反应的诱导,其特征是富含程序性死亡蛋白-1 阴性 Th1 和 Th2 细胞,具有激活表型。CD4 T 细胞耗竭消除了 CDK4/6i-ICB-DC 联合治疗的抗肿瘤益处,生长的肿瘤显示出终末耗尽的 CD8 T 细胞比例增加。
结论
我们的研究结果表明,CDK4/6i 介导的 DC 抑制限制了 CD4 T 细胞反应,而 CD4 T 细胞反应是 CD8 T 细胞持续活性和肿瘤抑制所必需的。此外,它们表明通过 DC 转移恢复 DC-CD4 T 细胞串扰可使乳腺癌对 CDK4/6i 和 ICB 治疗产生有效的免疫反应。
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