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线粒体靶向纳米颗粒用于产生氧气和一氧化碳的响应释放,以增强癌症的光气疗法。

Mitochondria targeted nanoparticles to generate oxygen and responsive-release of carbon monoxide for enhanced photogas therapy of cancer.

作者信息

Ren Hao, Yang Qingqing, Yong Jiahui, Fang Xue, Yang Zheng, Liu Zhangya, Jiang Xing, Miao Wenjun, Li Xueming

机构信息

School of Pharmaceutical Science, Nanjing Tech University, Nanjing 211816, China.

出版信息

Biomater Sci. 2021 Apr 7;9(7):2709-2720. doi: 10.1039/d0bm02028a. Epub 2021 Feb 22.

DOI:10.1039/d0bm02028a
PMID:33616151
Abstract

Carbon monoxide (CO) based gas therapy has been an emerging strategy for cancer treatment. However, the uncontrolled release of CO and limited therapeutic efficacy of monotherapy are two major obstacles for clinical application. To overcome these issues, human serum albumin (HSA) nanoparticles combined with manganese dioxide (MnO) were developed to deliver a photosensitizer (IR780) and CO donor (MnCO) for a synergistic therapy combining CO gas therapy and phototherapy. The nanoparticles (HIM-MnO) formed catalyze hydrogen peroxide to produce oxygen for hypoxia relief. With laser irradiation, it can increase the generation of reactive oxygen species for the enhancement of photodynamic therapy (PDT). Furthermore, the generated heat of photothermal therapy (PTT) induced by nanoparticles could trigger the release of CO to achieve a therapeutic window for enhanced gas therapy. Due to the co-localization of IR780 in mitochondria, HIM-MnO could accumulate in mitochondria for the synergistic therapy combining CO gas therapy and phototherapy, and could oxidize the mitochondrial membrane and induce more apoptosis. After intravenous injection into tumor bearing mice, HIM-MnO could accumulate at tumor sites and with laser irradiation, tumor growth was significantly inhibited due to the enhanced PDT, PTT, and CO gas therapy. This study provides a strategy with oxygen generating and thermal-responsive CO release to combine phototherapy and CO gas therapy for cancer treatment.

摘要

基于一氧化碳(CO)的气体疗法已成为一种新兴的癌症治疗策略。然而,CO的无控制释放和单一疗法有限的治疗效果是临床应用的两个主要障碍。为克服这些问题,研发了结合人血清白蛋白(HSA)纳米颗粒与二氧化锰(MnO)的制剂,用于递送光敏剂(IR780)和CO供体(MnCO),以实现CO气体疗法与光疗的协同治疗。形成的纳米颗粒(HIM-MnO)催化过氧化氢产生氧气以缓解缺氧。在激光照射下,它可增加活性氧的生成以增强光动力疗法(PDT)。此外,纳米颗粒诱导的光热疗法(PTT)产生的热量可触发CO的释放,从而实现增强气体疗法的治疗窗口。由于IR780在线粒体中共定位,HIM-MnO可在线粒体中积累,用于CO气体疗法与光疗的协同治疗,并可氧化线粒体膜并诱导更多细胞凋亡。将HIM-MnO静脉注射到荷瘤小鼠体内后,HIM-MnO可在肿瘤部位积聚,并且在激光照射下,由于增强的PDT、PTT和CO气体疗法,肿瘤生长受到显著抑制。本研究提供了一种具有产氧和热响应性CO释放功能的策略,将光疗与CO气体疗法相结合用于癌症治疗。

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