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病毒启发的金纳米棒-介孔硅核壳纳米粒子与 tTF-EG3287 整合用于协同肿瘤光热治疗和血管血栓的选择性治疗。

Virus-Inspired Gold Nanorod-Mesoporous Silica Core-Shell Nanoparticles Integrated with tTF-EG3287 for Synergetic Tumor Photothermal Therapy and Selective Therapy for Vascular Thrombosis.

机构信息

Cancer Research Center, School of Medicine, Xiamen University, Xiamen 361005, Republic of China.

The 174th Clinic College of People's Liberation Army, Anhui Medical University, Hefei 230031, Republic of China.

出版信息

ACS Appl Mater Interfaces. 2021 Sep 22;13(37):44013-44027. doi: 10.1021/acsami.1c11947. Epub 2021 Sep 8.

DOI:10.1021/acsami.1c11947
PMID:34494427
Abstract

Synergetic therapy includes the combination of two or more conventional therapeutic approaches and can be used for tumor treatment by combining the advantages and avoiding the drawbacks of each type of treatment. In the present study, truncated tissue factor (tTF)-EG3287 fusion protein-encapsulated gold nanorod (GNR)-virus-inspired mesoporous silica core-shell nanoparticles (vinyl hybrid silica nanoparticles; VSNP) (GNR@VSNP-tTF-EG3287) were synthesized to achieve synergetic therapy by utilizing selective vascular thrombosis therapy (SVTT) and photothermal therapy (PTT). By integrating the targeted coagulation activity of tTF-EG3287 and the high tumor ablation effect of GNR@VSNP, local hyperthermia could induce a high percentage of apoptosis of vascular endothelial cells by using near-infrared light. This provided additional phospholipid sites for tTF-EG3287 and enhanced its procoagulant activity . In addition, the nanoparticles, which had unique topological viral structures, exhibited superior cellular uptake properties leading to significant antitumor efficacy. The antitumor results further demonstrated an interaction between SVTT and PTT, whereas the synergetic therapy (SVTT and PTT) achieved an enhanced effect, which was superior to the respective treatment efficacy of each modality or the additive effect of their individual efficacies. In summary, the synthesized GNR@VSNP-tTF-EG3287 exerted synergetic effects and enhanced the antitumor efficiency by avoiding multiple injections and suboptimal administration. These effects simultaneously affected both tumor blood supply and cancer cell proliferation. The data suggested that the integration of SVTT induced by tTF-EG3287 and PTT could provide potential strategies for synergetic tumor therapy.

摘要

协同治疗包括两种或多种传统治疗方法的结合,可通过结合每种治疗方法的优势和避免其缺点来用于肿瘤治疗。在本研究中,合成了截断组织因子(tTF)-EG3287 融合蛋白包封的金纳米棒(GNR)-病毒启发的介孔硅核壳纳米粒子(乙烯基杂化硅纳米粒子;VSNP)(GNR@VSNP-tTF-EG3287),以通过利用选择性血管血栓形成治疗(SVTT)和光热治疗(PTT)实现协同治疗。通过整合 tTF-EG3287 的靶向凝血活性和 GNR@VSNP 的高肿瘤消融效果,近红外光可以诱导血管内皮细胞发生高比例的细胞凋亡,从而为 tTF-EG3287 提供更多的磷脂结合位点,并增强其促凝活性。此外,具有独特拓扑病毒结构的纳米粒子具有优异的细胞摄取特性,从而导致显著的抗肿瘤疗效。抗肿瘤结果进一步证明了 SVTT 和 PTT 之间的相互作用,而协同治疗(SVTT 和 PTT)则实现了增强效果,优于每种治疗方式的各自疗效或其单独疗效的加和效果。总之,合成的 GNR@VSNP-tTF-EG3287 通过避免多次注射和不理想的给药方式发挥协同作用并提高抗肿瘤效率。这些效果同时影响肿瘤的血液供应和癌细胞增殖。数据表明,tTF-EG3287 诱导的 SVTT 与 PTT 的整合可为协同肿瘤治疗提供潜在策略。

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