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癌症衍生细胞外囊泡的异源和跨物种趋向性。

Heterologous and cross-species tropism of cancer-derived extracellular vesicles.

机构信息

Department of Oncology and Hemato-Oncology, Center of Excellence on Neurodegenerative Diseases, University of Milan, Milan, Italy.

Department of Pharmacological and Biomolecular Sciences, University of Milan, Milan, Italy.

出版信息

Theranostics. 2019 Aug 9;9(19):5681-5693. doi: 10.7150/thno.34824. eCollection 2019.

DOI:10.7150/thno.34824
PMID:31534511
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6735396/
Abstract

Extracellular vesicles (EVs) are naturally occurring cargo delivery vesicles that have recently received considerable attention for their roles in intercellular communication in many physiological and pathological processes, including tumourigenesis. EVs generated by different tissues demonstrated specific homing: in particular, cancer-derived EVs showed a selective tropism for the tumor tissue from which the vesicles originated. For this property, EVs have been proposed as drug delivery tools for anti-cancer therapies, although the limited knowledge about their tropism hinders their therapeutic applications. The current study aimed to characterize the targeting properties of cancer-derived EVs and their biodistribution , by using an imaging approach. : EVs were generated from: i) murine lung (LL/2) and colon (MC-38) cancer lines, ii) human lung cancer cell line (A549) and iii) human liver biopsy samples from healthy individuals. EVs were loaded with fluorescent dyes alone or in combination with a biopharmaceutical agent, the oncolytic adenovirus (OV), characterized for charge and size and tested for their activity in cancer cell lines. Finally, optical imaging was extensively applied to study and the biodistribution of EVs originated from different sources in different mouse models of cancer, including xenograft, syngeneic graft and the MMTV-NeuT genetically modified animal. : We initially demonstrated that even loading EVs even with a large biopharmaceutical oncolytic viruses (OVs) did not significantly change their charge and dimension properties, while increasing their anti-neoplastic activity compared to the virus or EVs alone. Interestingly, this activity was observed even if the EVs derived from lung cancer were applied to colon carcinoma cell lines and , suggesting that the EV uptake occurred without any specificity for the cancer cells from which the vesicles originated. When administered i.v (intravenously) to the mouse models of cancer, the tumour-derived EVs, but not the EVs derived from a healthy tissue, demonstrated a selective accumulation of the fluorescence at the tumour site 24 h after injection; adding OVs to the formulation did not change the tumour-specific tropism of the EVs also . Most interestingly, the experiments confirmed the observation of the generalized tropism of tumour-derived EVs for any neoplastic tissue, independent of the tumour type or even the species originating the vesicles. : Taken together, our and data demonstrate for the first time a heterologous, cross-species tumour-tropism for cancer-derived EVs. This finding challenges our current view on the homing properties of EVs and opens new avenues for the selective delivery of diagnostic/therapeutic agents to solid tumours.

摘要

细胞外囊泡 (EVs) 是天然存在的货物运输囊泡,由于它们在许多生理和病理过程(包括肿瘤发生)中的细胞间通讯中的作用,最近受到了相当大的关注。不同组织产生的 EVs 表现出特定的归巢性:特别是,源自肿瘤的癌症衍生 EVs 对起源于其的囊泡的肿瘤组织表现出选择性趋向性。由于这种特性,EVs 被提议作为抗癌疗法的药物递送工具,尽管对其趋向性的了解有限限制了它们的治疗应用。本研究旨在通过成像方法表征癌症衍生 EVs 的靶向特性及其生物分布。

EVs 是从以下来源产生的:i) 鼠肺 (LL/2) 和结肠 (MC-38) 癌细胞系,ii) 人肺癌细胞系 (A549) 和 iii) 来自健康个体的人肝活检样本。EVs 单独或与生物制药剂,溶瘤腺病毒 (OV) 一起加载荧光染料,对其电荷和大小进行表征,并在癌细胞系中测试其活性。最后,广泛应用光学成像来研究不同来源的 EVs 在不同的癌症小鼠模型中的生物分布,包括异种移植、同基因移植和 MMTV-NeuT 基因修饰动物。

我们最初证明,即使将大的生物制药溶瘤病毒 (OVs) 装载到 EVs 中,也不会显著改变其电荷和尺寸特性,同时与单独的病毒或 EVs 相比,增加其抗肿瘤活性。有趣的是,即使将源自肺癌的 EVs 应用于结肠癌细胞系,也观察到了这种活性,这表明 EV 的摄取发生时没有对源自其的囊泡的癌细胞具有任何特异性。当静脉内 (i.v.) 给予癌症小鼠模型时,源自肿瘤的 EVs,但不是源自健康组织的 EVs,在注射后 24 小时在肿瘤部位显示出荧光的选择性积聚;向制剂中添加 OVs 也不会改变 EVs 的肿瘤特异性趋向性。最有趣的是,实验证实了源自肿瘤的 EVs 对任何肿瘤组织的普遍趋向性的观察,而与肿瘤类型甚至起源于囊泡的物种无关。

总之,我们的体内和体外数据首次证明了源自癌症的 EVs 的异源、跨物种肿瘤趋向性。这一发现挑战了我们目前对 EVs 归巢特性的看法,并为将诊断/治疗剂选择性递送至实体瘤开辟了新途径。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f730/6735396/b5a5af41a0ec/thnov09p5681g006.jpg
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