CpG therapeutic efficacy in a murine model of metastatic Lymphangioleiomyomatosis (LAM) is mediated by plasmacytoid dendritic cell and T cell immune responses

M. Amosu, Jacob McCright, Kaitlyn Moore, K. Maisel
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Abstract

LAM is a slow growing, metastasizing neoplasm affecting women of reproductive age, marked by abnormal growth of smooth muscle-like cells leading to cystic lung destruction. LAM has hallmarks of cancer, like expression of immune checkpoint receptors. Effective cancer therapies promote robust T cell responses through activated dendritic cells (DCs). Anti-cancer strategies, like toll like receptor (TLR) activation and immune checkpoint inhibition could work as LAM therapy. In this study, we examine the effect of CpG, a TLR9 agonist, on the DC and T cell responses in murine LAM. We used a mouse model of metastatic LAM to determine survival after biweekly intranasal CpG therapy (10μg/ 5μg) with/ without systemic α-PD-1, rapamycin, or α-CD317 therapy. We used ELISA to measure the cytokine profile and flow cytometry to quantify cell populations between CpG-treated and untreated LAM lungs. We found that CpG treatment enhances median survival from 32 to 60 days in murine LAM (p <0.0001). Efficacy of CpG treatment in LAM is facilitated by plasmacytoid DCs. pDC depletion in CpG-treated mice decreases survival from 60 to 52 days (p=0.028). CpG-treated LAM lungs also produce more IFN-α (p=0.031). CpG-treated LAM lungs have increased IFN-γ (p= 0.012) and IL-12 (p= 0.005), cytokines secreted by cytotoxic T cells. CpG-treatment is synergistic with α-PD-1 checkpoint inhibition (p=0.004) and can be administered with rapamycin without adverse effects on median survival. In LAM, CpG therapy is mediated by pDC dependent immune responses and cytotoxic T cells. This suggests that adjuvant immunotherapy, like CpG, may offer new treatment options for LAM compatible with the current standard of care, rapamycin. The LAM Foundation Research Grant Award
CpG在小鼠转移性淋巴管平滑肌瘤病(LAM)模型中的治疗效果是由浆细胞样树突状细胞和T细胞免疫反应介导的
LAM是一种生长缓慢的转移性肿瘤,影响育龄妇女,其特征是平滑肌样细胞异常生长,导致囊性肺破坏。LAM有癌症的特征,比如免疫检查点受体的表达。有效的癌症治疗通过激活树突状细胞(dc)促进强大的T细胞反应。抗癌策略,如toll样受体(TLR)激活和免疫检查点抑制可以作为LAM治疗。在这项研究中,我们研究了CpG(一种TLR9激动剂)对小鼠LAM中DC和T细胞反应的影响。我们使用转移性LAM小鼠模型来测定两周鼻内CpG治疗(10μg/ 5μg)联合/不全身α-PD-1、雷帕霉素或α-CD317治疗后的生存率。我们用ELISA法测定细胞因子谱,用流式细胞术量化cpg处理和未处理的LAM肺之间的细胞群。我们发现CpG治疗提高了小鼠LAM的中位生存期(从32天到60天)(p <0.0001)。浆细胞样dc促进了CpG治疗LAM的疗效。cpg处理小鼠的pDC耗竭降低了60至52天的存活率(p=0.028)。cpg处理的LAM肺产生更多的IFN-α (p=0.031)。cpg处理的LAM肺中细胞毒性T细胞分泌的IFN-γ (p= 0.012)和IL-12 (p= 0.005)细胞因子增加。cpg治疗与α-PD-1检查点抑制具有协同作用(p=0.004),可与雷帕霉素联合使用,对中位生存期无不良影响。在LAM中,CpG治疗是由pDC依赖性免疫反应和细胞毒性T细胞介导的。这表明,辅助免疫治疗,如CpG,可能为LAM提供新的治疗选择,与当前的护理标准雷帕霉素兼容。林郑月娥基金研究资助奖
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