4.7 Article

Molecularly engineered carrier-free co-delivery nanoassembly for self-sensitized photothermal cancer therapy

JOURNAL OF NANOBIOTECHNOLOGY (2021)

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Journal

JOURNAL OF NANOBIOTECHNOLOGY
Volume 19, Issue 1, Pages -

Publisher

BMC
DOI: 10.1186/s12951-021-01037-6

Keywords

Photothermal photosensitizers; Thermoresistance; HSP90 inhibitor; Dual-drug nanoassembly; Self-sensitized photothermal therapy

Categories

Biotechnology & Applied Microbiology Nanoscience & Nanotechnology

Funding

  1. Science and Technology Major Project of Liaoning [2019JH1/10300004]
  2. National Natural Science Foundation of China [81872816]
  3. Excellent Youth Science Foundation of Liaoning Province [2020-YQ-06]
  4. China Postdoctoral Science Foundation [2020M670794]
  5. Liaoning Revitalization Talents Program [XLYC1907129, XLYC1902061, XLYC1808017]

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This study presents a novel and convenient dual-drug co-assembly strategy for self-sensitized cancer therapy. The carrier-free co-delivery nanoassembly of a HSP90 inhibitor and DiR demonstrates potential as a new treatment approach for tumors.
Background: Photothermal therapy (PTT) has been extensively investigated as a tumor-localizing therapeutic modality for neoplastic disorders. However, the hyperthermia effect of PTT is greatly restricted by the thermoresistance of tumor cells. Particularly, the compensatory expression of heat shock protein 90 (HSP90) has been found to significantly accelerate the thermal tolerance of tumor cells. Thus, a combination of HSP90 inhibitor and photothermal photosensitizer is expected to significantly enhance antitumor efficacy of PTT through hyperthermia sensitization. However, it remains challenging to precisely co-deliver two or more drugs into tumors. Methods: A carrier-free co-delivery nanoassembly of gambogic acid (GA, a HSP90 inhibitor) and DiR is ingeniously fabricated based on a facile and precise molecular co-assembly technique. The assembly mechanisms, photothermal conversion efficiency, laser-triggered drug release, cellular uptake, synergistic cytotoxicity of the nanoassembly are investigated in vitro. Furthermore, the pharmacokinetics, biodistribution and self-enhanced PTT efficacy were explored in vivo. Results: The nanoassembly presents multiple advantages throughout the whole drug delivery process, including carrier-free fabrication with good reproducibility, high drug co-loading efficiency with convenient dose adjustment, synchronous co-delivery of DiR and GA with long systemic circulation, as well as self-tracing tumor accumulation with efficient photothermal conversion. As expected, HSP90 inhibition-augmented PTT is observed in a 4T1 tumor BALB/c mice xenograft model. Conclusion: Our study provides a novel and facile dual-drug co-assembly strategy for self-sensitized cancer therapy.

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