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Carbon nanocage-based nanozyme as an endogenous H2O2-activated oxygenerator for real-time bimodal imaging and enhanced phototherapy of esophageal cancer

机译:碳nanocage-based nanozyme作为内生为实时双向H2O2-activated制氧机成像和增强的光疗食管癌症

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摘要

Intelligent phototherapy by theranostic nanosystems that can be activated by a tumor microenvironment has high sensitivity and specificity. However, hypoxia and low drug accumulation in tumors greatly limit its clinical application. Herein, we have designed a cage-like carbon-manganese nanozyme, which effectively relieves tumor hypoxia and delivers numerous photosensitizers (PSs) to the tumor site, for real-time imaging and enhanced phototherapy of esophageal cancer. Specifically, bovine serum albumin (BSA) was used as a template and reducing agent for preparing a BSA-MnO2 nanozyme; then a BSA-MnO2/IR820@OCNC (BMIOC) nanosystem was successfully synthesized by crosslinking BSA-MnO2 on the surface of IR820-loaded carboxylated carbon nanocages (OCNCs). Abundant PSs were successfully delivered to tumor sites via hollow OCNCs, and the final loading rate of IR820 reached 42.8%. The intratumor BMIOC nanosystem can be initiated by a tumor microenvironment to switch on its magnetic resonance (MR) imaging signal, and photothermal therapy (PTT) and photodynamic therapy (PDT) functions. Notably, the BSA-MnO2 nanozyme, with intrinsic catalase (CAT)-like activity, catalyzed endogenous H2O2 for oxygen generation to overcome tumor hypoxia and enhance PDT, thereby leading to more efficient therapeutic effects in combination with OCNC-elevated PTT. In addition, the H2O2-activated and acid-enhanced properties enable our nanosystem to be specific to tumors, protecting normal tissues from damage. By integrating a high drug loading capacity, a hypoxia regulation function, an enlarged phototherapy effect, and bimodal imaging into a nanozyme-mediated nanoreactor, this work realizes a "one for all" system and represents promising clinical translation for efficient esophageal cancer theranostics.
机译:智能光疗,theranostic纳米系统可以被激活的肿瘤微环境敏感性和高特异性。在肿瘤大大限制其临床积累应用程序。carbon-manganese nanozyme,有效减轻肿瘤缺氧和众多敏化(PSs)到肿瘤部位,实时成像和增强的光疗食道癌。白蛋白(BSA)被用作模板,减少代理准备BSA-MnO2 nanozyme;BSA-MnO2 / IR820@OCNC (BMIOC)综合成功地合成了交联BSA-MnO2IR820-loaded表面的羧酸盐碳nanocages (OCNCs)。成功地交付给肿瘤站点通过空心IR820 OCNCs,最后加载速率达到了42.8%。可以由一个肿瘤微环境开关的磁共振(MR)成像信号,光照疗法(PTT)和光动力疗法(PDT)功能。的BSA-MnO2 nanozyme,内在的过氧化氢酶(猫)同活动,催化内源性过氧化氢氧代克服肿瘤缺氧和提高PDT,从而导致更多的有效的治疗效果结合OCNC-elevated PTT。H2O2-activated和acid-enhanced属性使我们的综合具体肿瘤,保护正常组织不受损害。整合高药物装载能力,缺氧调控功能,扩大光疗效果,和双峰成像nanozyme-mediated nanoreactor,这项工作实现“我为人人”系统,是有前途的临床翻译有效的食管癌症开展。

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