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智能人血清白蛋白-吲哚菁绿纳米粒子通过程序化组装生成,用于双模式成像引导的癌症协同光疗。

Smart human serum albumin-indocyanine green nanoparticles generated by programmed assembly for dual-modal imaging-guided cancer synergistic phototherapy.

机构信息

Guangdong Key Laboratory of Nanomedicine, CAS Key Laboratory of Health Informatics, Shenzhen Institutes of Advanced Technology, Chinese Academy of Sciences , Shenzhen 518055, PR China.

出版信息

ACS Nano. 2014 Dec 23;8(12):12310-22. doi: 10.1021/nn5062386. Epub 2014 Dec 8.

Abstract

Phototherapy, including photodynamic therapy (PDT) and photothermal therapy (PTT), is a light-activated local treatment modality that is under intensive preclinical and clinical investigations for cancer. To enhance the treatment efficiency of phototherapy and reduce the light-associated side effects, it is highly desirable to improve drug accumulation and precision guided phototherapy for efficient conversion of the absorbed light energy to reactive oxygen species (ROS) and local hyperthermia. In the present study, a programmed assembly strategy was developed for the preparation of human serum albumin (HSA)-indocyanine green (ICG) nanoparticles (HSA-ICG NPs) by intermolecular disulfide conjugations. This study indicated that HSA-ICG NPs had a high accumulation with tumor-to-normal tissue ratio of 36.12±5.12 at 24 h and a long-term retention with more than 7 days in 4T1 tumor-bearing mice, where the tumor and its margin, normal tissue were clearly identified via ICG-based in vivo near-infrared (NIR) fluorescence and photoacoustic dual-modal imaging and spectrum-resolved technology. Meanwhile, HSA-ICG NPs efficiently induced ROS and local hyperthermia simultaneously for synergetic PDT/PTT treatments under a single NIR laser irradiation. After an intravenous injection of HSA-ICG NPs followed by imaging-guided precision phototherapy (808 nm, 0.8 W/cm2 for 5 min), the tumor was completely suppressed, no tumor recurrence and treatments-induced toxicity were observed. The results suggest that HSA-ICG NPs generated by programmed assembly as smart theranostic nanoplatforms are highly potential for imaging-guided cancer phototherapy with PDT/PTT synergistic effects.

摘要

光疗,包括光动力疗法(PDT)和光热疗法(PTT),是一种光激活的局部治疗方式,目前正在进行深入的临床前和临床研究,以用于癌症治疗。为了提高光疗的治疗效率并降低与光相关的副作用,非常需要提高药物积累和精确指导光疗,以有效地将吸收的光能转化为活性氧(ROS)和局部热疗。在本研究中,通过分子间二硫键共轭开发了一种程序化组装策略,用于制备人血清白蛋白(HSA)-吲哚菁绿(ICG)纳米颗粒(HSA-ICG NPs)。本研究表明,HSA-ICG NPs 在 24 h 时具有高肿瘤积累,肿瘤与正常组织的比值为 36.12±5.12,在 4T1 荷瘤小鼠中具有超过 7 天的长期保留,通过基于 ICG 的体内近红外(NIR)荧光和光声双模态成像以及光谱分辨技术,可以清楚地识别肿瘤及其边缘的正常组织。同时,HSA-ICG NPs 在单一 NIR 激光照射下,能有效地同时诱导 ROS 和局部热疗,用于协同 PDT/PTT 治疗。静脉注射 HSA-ICG NPs 后,进行成像引导的精确光疗(808nm,0.8W/cm2 照射 5min),肿瘤完全被抑制,未观察到肿瘤复发和治疗引起的毒性。结果表明,通过程序化组装生成的 HSA-ICG NPs 作为智能治疗纳米平台,具有用于 PDT/PTT 协同治疗的成像引导癌症光疗的巨大潜力。

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