4.8 Article

High-Security Nanocluster for Switching Photodynamic Combining Photothermal and Acid-Induced Drug Compliance Therapy Guided by Multimodal Active-Targeting Imaging

Journal

ADVANCED FUNCTIONAL MATERIALS
Volume 28, Issue 36, Pages -

Publisher

WILEY-V C H VERLAG GMBH
DOI: 10.1002/adfm.201803118

Keywords

active-targeting; controlled photodynamic therapy; drug compliance; multimodal imaging; photothermal therapy

Funding

  1. National Key Research and Development Program of China [2017YFA0700402]
  2. National Natural Science Foundation of China [81471697, 81771878]
  3. Applied Basic Research Program of Wuhan City [2016060101010044]
  4. Fundamental Research Funds for the Central Universities (Hust) [2016YXMS253, 2017KFXKJC002, 2018KFYXKJC048]

Ask authors/readers for more resources

High-security nanoplatform with enhanced therapy compliance is extremely promising for tumor. Herein, using a simple and high-efficient self-assembly method, a novel active-targeting nanocluster probe, namely, Ag2S/chlorin e6 (Ce6)/DOX@DSPE-mPEG(2000)-folate (ACD-FA) is synthesized. Experiments indicate that ACD-FA is capable of specifically labeling tumor and guiding targeting ablation of the tumor via precise positioning from fluorescence and photoacoustic imaging. Importantly, the probe is endowed with a photodynamic on-off effect, that is, Ag2S could effectively quench the fluorescence of chlorin e6 (89.5%) and inhibit release of O-1(2) (92.7%), which is conducive to avoid unwanted phototoxicity during transhipment in the body, and only after nanocluster endocytosed by tumor cells could release Ce6 to produce O-1(2). Moreover, ACD-FA also achieves excellent acid-responsive drug release, and exhibits eminent chemo-photothermal and photodynamic effects upon laser irradiation. Compared with single or two treatment combining modalities, ACD-FA could provide the best cancer therapeutic effect with a relatively low dose, because it made the most of combined effect from chemo-photothermal and controlled photodynamic therapy, and significantly improves the drug compliance. Besides, the active-targeting nanocluster notably reduces nonspecific toxicity of both doxorubicin and chlorin e6. Together, this study demonstrates the potency of a newly designed nanocluster for nonradioactive concomitant therapy with precise tumor-targeting capability.

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