Nanobody Research Center/School of Preclinical Medicine, Guangxi Medical University, Nanning, Guangxi, 530021, China.
Theranostics. 2019 May 31;9(14):4066-4083. doi: 10.7150/thno.33383. eCollection 2019.
: Adequate recruitment of highly active tumor antigen-specific cytotoxic T lymphocytes (CTLs) remains a major challenge in cancer immunotherapy. : To construct liposome (LP)-based nanocapsules with surface endoglin aptamer (ENG-Apt) encapsulating mouse interferon-inducible protein-10 (mIP-10), with the ability to target mouse tumor vascular endothelial cells (mTECs) and enhance CTLs targeting and recruitment to the tumor vasculature. : ENG-Apt/mIP-10-LP nanocapsules were prepared by grafting DSPE-PEG-ENG-Apt on the surface of liposomes containing mIP-10 plasmids, characterized and assessed for the cell binding specificity . The tumor-targeting ability of ENG-Apt/mIP-10-LP nanocapsules was evaluated . The anti-tumor efficacy of ENG-Apt/mIP-10-LP nanocapsules treatment, as well as the combination treatment of ENG-Apt/mIP-10-LP nanocapsules and adoptive TRP2CD8 T cells, were both tested in melanoma-bearing mice, by evaluation of the tumor volume and the mouse survival time. To discuss the anti-tumoral mechanism of ENG-Apt/mIP-10-LP nanocapsules-based therapies, IFN-γ secretion, proportion of TRP2CD8 T cells among TILs, MDSCs in the tumor microenvironment and Tregs in the spleen, were determined after the treatments. Proliferation and apoptosis of tumor cells, and tumor angiogenesis were also assessed. : The prepared ENG-Apt/mIP-10-LP nanocapsules possess an adequate nanometric size, good stability, high specificity to mTECs and tumor sites, along with the ability to induce mIP-10 expression and . Treatment of ENG-Apt/mIP-10-LP nanocapsules demonstrated CTLs enrichment into the tumor site, which inhibited tumor cell proliferation and angiogenesis, as well as promoted tumor-cell apoptosis, leading to a decrease in tumor progression and prolonged survival time in melanoma tumor-bearing mice. In addition, the proportion of MDSCs and Tregs was found to decrease. The combination of ENG-Apt/mIP-10-LP nanocapsules with adoptive TRP2CD8 T cells, showed stronger abilities in inhibiting tumor growth and increasing animal survival time, thereby displayed an enhanced anti-melanoma tumor efficacy, due to the recruitment of both endogenous CD8 T cells and exogenous TRP2CD8 T cells . : ENG-Apt/mIP-10-LP nanocapsules could enhance the recruitment of both endogenous and exogenous CTLs specifically targeting melanoma tumor vasculatures and exert anti-tumoral effect, therefore provides a potentially novel strategy for tumor immunotherapy.
: 充分募集高度活跃的肿瘤抗原特异性细胞毒性 T 淋巴细胞(CTLs)仍然是癌症免疫治疗的主要挑战。: 构建基于脂质体(LP)的纳米胶囊,表面内胚层糖蛋白配体(ENG-Apt)包封小鼠干扰素诱导蛋白-10(mIP-10),能够靶向小鼠肿瘤血管内皮细胞(mTECs)并增强 CTLs 靶向和募集到肿瘤血管。: 通过在含有 mIP-10 质粒的脂质体表面接枝 DSPE-PEG-ENG-Apt,制备 ENG-Apt/mIP-10-LP 纳米胶囊,对其进行表征和评估细胞结合特异性。评估 ENG-Apt/mIP-10-LP 纳米胶囊的肿瘤靶向能力。通过评估肿瘤体积和小鼠生存时间,在黑色素瘤荷瘤小鼠中测试 ENG-Apt/mIP-10-LP 纳米胶囊治疗以及 ENG-Apt/mIP-10-LP 纳米胶囊和过继性 TRP2CD8 T 细胞联合治疗的抗肿瘤疗效。为了讨论 ENG-Apt/mIP-10-LP 纳米胶囊为基础的治疗的抗肿瘤机制,在治疗后测定肿瘤微环境中 IFN-γ 分泌、TILs 中 TRP2CD8 T 细胞的比例、MDSCs 和脾脏中的 Tregs。还评估了肿瘤细胞的增殖和凋亡以及肿瘤血管生成。: 制备的 ENG-Apt/mIP-10-LP 纳米胶囊具有适当的纳米尺寸、良好的稳定性、对 mTECs 和肿瘤部位的高特异性,以及诱导 mIP-10 表达的能力。ENG-Apt/mIP-10-LP 纳米胶囊的治疗显示 CTLs 富集到肿瘤部位,抑制肿瘤细胞增殖和血管生成,并促进肿瘤细胞凋亡,从而降低肿瘤进展并延长黑色素瘤荷瘤小鼠的生存时间。此外,发现 MDSCs 和 Tregs 的比例下降。ENG-Apt/mIP-10-LP 纳米胶囊与过继性 TRP2CD8 T 细胞联合使用,在抑制肿瘤生长和增加动物生存时间方面表现出更强的能力,从而显示出增强的抗黑色素瘤肿瘤疗效,因为招募了内源性 CD8 T 细胞和外源性 TRP2CD8 T 细胞。: ENG-Apt/mIP-10-LP 纳米胶囊可以增强特异性靶向黑色素瘤肿瘤血管的内源性和外源性 CTLs 的募集,发挥抗肿瘤作用,因此为肿瘤免疫治疗提供了一种潜在的新策略。
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