4.6 Article

A transformable gold nanocluster aggregate-based synergistic strategy for potentiated radiation/gene cancer therapy

Journal

JOURNAL OF MATERIALS CHEMISTRY B
Volume 9, Issue 9, Pages 2314-2322

Publisher

ROYAL SOC CHEMISTRY
DOI: 10.1039/d0tb02986f

Keywords

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Funding

  1. National Natural Science Foundation of China [31500802, 21628201]
  2. Natural Science Foundation of Jiangsu Province [BK20190097]
  3. Program of Qilu Young Scholars of Shandong University
  4. Taishan Scholars Program for Young Expert of Shandong Province [tsqn201909021]
  5. Youth cross-scientific innovation group of Shandong University

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The study introduces a synergistic strategy for potentiated cancer radiation/gene therapy using transformable gold nanocluster aggregates. By leveraging the size transformation of the nanocluster and survivin gene interference, the radio-sensitivity of tumor cells can be significantly improved, leading to enhanced tumor radiation therapy efficacy.
Nano-radiosensitizers provide a powerful tool for cancer radiation therapy. However, their limited tumor retention/penetration and the inherent or adaptive radiation resistance of tumor cells hamper the clinical success of radiation therapy. Herein, we report a synergistic strategy for potentiated cancer radiation/gene therapy based on transformable gold nanocluster aggregates loaded with antisense oligonucleotide-targeting survivin mRNA (named AuNC-ASON). AuNC-ASON exhibited acidic pH-triggered structure splitting from a gold nanocluster aggregate (around 80 nm) to gold nanocluster (<2 nm), leading to the tumor microenvironment-responsive size transformation of the nano-radiosensitizer and activated release of the loaded antisense oligonucleotides to perform gene silencing. The in vitro experiments demonstrated that AuNC-ASON could amplify and improve the radio-sensitivity of tumor cells (the sensitization enhancement ratio was about 1.81) as a result of the synergistic effect of the transformable gold nanocluster radiosensitizer and survivin gene interference. Remarkably, the size transformation capability realized the high tumor retention/penetration and renal metabolism of AuNC-ASON in vivo and boosted the radio-susceptibility of cancer cells with the assistance of survivin gene interference, synergistically achieving potentiated tumor radiation/gene therapy. The proposed concept of transformable nano-radiosensitizer aggregate-based synergistic therapy can be utilized as a general strategy to guide the design of activatable multifunctional nanosystems for cancer theranostics.

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