4.8 Article

Enhanced anti-metastatic therapy with down-regulation of heparinase expression by ROS-responsive micellar nanoparticles

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NANOSCALE
卷 13, 期 36, 页码 15267-15277

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ROYAL SOC CHEMISTRY
DOI: 10.1039/d1nr02964a

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资金

  1. Regional Innovation and Development Joint Fund [U20A200047]
  2. National Science Fund for Excellent Young Scholars [82022070]
  3. National Natural Science Foundation of China [81872824]

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Metastasis is a crucial factor in cancer-related deaths, and suppressing it can improve the survival rate of cancer patients. Nanoparticles with dual functionality have been developed to inhibit tumor metastasis and enhance the efficacy of loaded drugs against tumors. These versatile carriers show promise in treating invasive solid tumors and metastases by significantly reducing metastatic nodules.
Metastasis is a major sign of malignant tumors which plays a vital role in cancer-related death. Suppressing metastasis is an important way to improve the survival rate of cancer patients. Herein, multifunctional PEG-LAM-PPS nanoparticles (nPLPs) are fabricated as both nanocarriers and anti-metastatic agents for tumor treatment. In this system, laminarin sulfate (LAM) suppresses metastasis by reducing heparinase and protecting the extracellular matrix; the ROS-sensitive polypropylene sulfide (PPS) improves the release of the loaded drug in the tumor microenvironment. This is the first time that laminarin sulfate has been used as a carrier to inhibit the expression of heparinase and treat melanoma lung metastasis. The blank nanoparticles are excellently safe and showed high anti-metastatic efficacy in melanoma lung metastatic mouse models, reducing metastatic nodules by 60%. They significantly improved the anti-tumor efficacy of the loaded drug doxorubicin, provided similar to 33% further reduction of the tumor volume and 50% further reduction of the metastatic nodule number compared with free doxorubicin. Thus, these simple and versatile micellar nanoparticles composed of biocompatible materials offer a promising vehicle for treating invasive solid tumors and metastases.

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