4.8 Article

A targeting theranostics nanomedicine as an alternative approach for hyperthermia perfusion

期刊

BIOMATERIALS
卷 183, 期 -, 页码 268-279

出版社

ELSEVIER SCI LTD
DOI: 10.1016/j.biomaterials.2018.04.016

关键词

Theranostics prodrug; Real-time monitoring; Photothermal; Deep penetration; Hyperthermia perfusion

资金

  1. Shanghai Sailing Program [16YF1400900]
  2. National Natural Science Funds of China [21602030, 81172993]
  3. Scientific Research Foundation of Fudan University for Talent Introduction [JJF301103]
  4. National Science Fund for Distinguished Young Scholars [81425023]
  5. Fudan-SIMM Joint Research Fund [FU-SIMM20174009]

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Real-time monitoring drug-release is often regarded crucial in theranostics nanomedicine design, since it provides precise establishment of spatio-temporal activation of the drug-release in vitro and in vivo. A symmetrical self-immolative drug-dye conjugation (DDC) prodrug is developed in this study with disulfide bond as the trigger. The prodrug can be escorted by targeting PEG-PLGA micelles and hereby accumulated in the tumor by both active and passive targeting effect. Glutathione (GSH) with higher concentration in the tumor microenvironment can readily cleave the disulfide bond to initiate a subsequent decomposition of DDC, where the drug and dye can be released simultaneously in a strict one-to-one mode. Upon the disintegration, the Turned-On probe can emit near-infrared (NIR) fluorescence, with the aim of providing accurate and real-time information for the prodrugs' activation and biodistribution in vivo in a non-invasive way. Furthermore, the released dye can meanwhile act as a photothermic sensitizer, which can in-situ assist a deep penetration for the released drug in the tumor tissue with enhanced therapeutic efficiency. This babysitting strategy provides new reference for designing versatile theranostic nanomedicines for preclinical evaluations and an alternative approach for hyperthermia perfusion in clinic. (C) 2018 Published by Elsevier Ltd.

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