Idera Pharmaceuticals, Inc., Cambridge, MA 02139, USA.
Int J Oncol. 2018 Sep;53(3):1193-1203. doi: 10.3892/ijo.2018.4456. Epub 2018 Jun 27.
The objective of cancer immunotherapy is to prime the host's immune system to recognize and attack malignant tumor cells. IMO‑2125, a Toll‑like receptor 9 (TLR9) agonist, exhibited potent antitumor effects in the murine syngeneic A20 lymphoma and the CT26 colon carcinoma models. IMO‑2125 exhibited superior A20 antitumor activity when injected intratumorally (i.t.) compared with equivalent subcutaneous doses. In mice bearing dual CT26 grafts, the i.t. injection of right flank tumors elicited infiltration of cluster of differentiation (CD)3+ T lymphocytes into tumors, resulting in the regression of injected and uninjected left flank tumors. Depletion of CD8+, but not CD4+, T‑cells abrogated the IMO‑2125‑mediated antitumor response, suggesting that CD8+ lymphocytes are required for the antitumor activity. In mice harboring right flank CT26 and left flank β‑galactosidase (β‑gal)‑expressing CT26.CL25 grafts, the i.t. administration of IMO‑2125 to the CT26 graft resulted in potent and dose‑dependent antitumor activity against the two grafts. Splenic T‑cells isolated from these mice responded to AH1 antigen (present in the two tumors) and β‑gal antigen (present only in CT26.CL25) in an interferon γ enzyme‑linked immunospot assay, suggesting the clonal expansion of T‑cells directed against antigens from the two tumors. Mice with ablated CT26 tumors by previous IMO‑2125 treatment rejected re‑implanted CT26 tumor cells, but not A20 tumor cells, demonstrating that the initial IMO‑2125 treatment created a long‑lived tumor‑specific immune memory of CT26 antigens. A quantitative increase in CD3+ T lymphocytes in injected A20 tumors and an upregulation of selected checkpoint genes, including indoleamine 2,3‑dioxygenase (IDO)‑1, IDO‑2, programmed cell death protein-1 (PD-1); programmed cell death protein ligand 1 (PD-L1), carcinoembryonic antigen‑related cell adhesion molecule 1, tumor necrosis factor receptor superfamily member 4 (OX40), OX40 ligand, T‑cell immunoglobulin and mucin‑domain‑containing 3 protein, lymphocyte‑activation gene 3, cytotoxic T‑lymphocyte‑associated protein 4, were observed following IMO‑2125 treatment. IMO‑2125 also increased immune checkpoint gene expression in injected and uninjected contralateral CT26 tumors, suggesting that the co‑administration of anti‑CTLA‑4, anti‑PD‑1 or anti‑PD‑L1 therapies with IMO‑2125 may provide additional therapeutic efficacy.
癌症免疫疗法的目的是使宿主的免疫系统能够识别和攻击恶性肿瘤细胞。IMO-2125 是一种 Toll 样受体 9(TLR9)激动剂,在鼠同源性 A20 淋巴瘤和 CT26 结肠癌细胞模型中显示出强大的抗肿瘤作用。与等效的皮下剂量相比,IMO-2125 瘤内注射(i.t.)显示出对 A20 的抗肿瘤活性更强。在携带双重 CT26 移植物的小鼠中,右 flank 肿瘤的 i.t. 注射引发了分化群(CD)3+T 淋巴细胞浸润肿瘤,导致注射和未注射的左 flank 肿瘤消退。耗尽 CD8+,而不是 CD4+,T 细胞可消除 IMO-2125 介导的抗肿瘤反应,表明 CD8+淋巴细胞是抗肿瘤活性所必需的。在携带右 flank CT26 和左 flank β-半乳糖苷酶(β-gal)表达 CT26.CL25 移植物的小鼠中,IMO-2125 对 CT26 移植物的 i.t. 给药导致对两个移植物的强大且剂量依赖性的抗肿瘤活性。从这些小鼠中分离的脾 T 细胞在干扰素 γ 酶联免疫斑点测定中对 AH1 抗原(存在于两个肿瘤中)和 β-gal 抗原(仅存在于 CT26.CL25 中)有反应,表明针对两个肿瘤抗原的 T 细胞的克隆扩增。通过先前 IMO-2125 治疗而消融 CT26 肿瘤的小鼠排斥重新植入的 CT26 肿瘤细胞,但不排斥 A20 肿瘤细胞,表明初始 IMO-2125 治疗产生了针对 CT26 抗原的长期存活的肿瘤特异性免疫记忆。在注入的 A20 肿瘤中 CD3+T 淋巴细胞的定量增加以及选定的检查点基因的上调,包括吲哚胺 2,3-双加氧酶(IDO)-1、IDO-2、程序性细胞死亡蛋白-1(PD-1);程序性细胞死亡蛋白配体 1(PD-L1)、癌胚抗原相关细胞粘附分子 1、肿瘤坏死因子受体超家族成员 4(OX40)、OX40 配体、T 细胞免疫球蛋白和粘蛋白结构域包含 3 蛋白、淋巴细胞激活基因 3、细胞毒性 T 淋巴细胞相关蛋白 4,在 IMO-2125 治疗后观察到。IMO-2125 还增加了注入和未注入的对侧 CT26 肿瘤中免疫检查点基因的表达,表明与 IMO-2125 联合使用抗 CTLA-4、抗 PD-1 或抗 PD-L1 疗法可能提供额外的治疗效果。
