4.8 Article

Salinomycin nanocrystals for colorectal cancer treatment through inhibition of Wnt/β-catenin signaling

Journal

NANOSCALE
Volume 12, Issue 38, Pages 19931-19938

Publisher

ROYAL SOC CHEMISTRY
DOI: 10.1039/d0nr04552g

Keywords

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Funding

  1. National Key R&D Program of China [2018YFA0704000]
  2. National Nature Science Foundation of China [31970739, 31870754, 31501143]
  3. Shenzhen Science and Technology Program [KQTD20190929172538530, KQTD20140630100658078]
  4. Key Laboratory Project of Shenzhen [ZDSY20130329101130496]
  5. Shenzhen Basic Research Program [JCYJ20180507182413022, JCYJ20170412111100742, JCYJ20190808173601655, JCYJ20170302143447936, JCYJ20150525092941030]
  6. Guangdong Province Natural Science Foundation of Major Basic Research and Cultivation Project [2018B030308003]
  7. Fok Ying-Tong Education Foundation for Young Teachers in the Higher Education Institutions of China [161032]
  8. SZU Medical Young Scientists Program [71201-000001]

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Salinomycin (SAL) is one of the first discovered inhibitors of human cancer stem cells (CSCs), which actsviablocking the Wnt/beta-catenin pathway. However, SAL has not been clinically used to treat human diseases due to its poor aqueous solubility and considerable toxicity. In this study, we developed salinomycin nanocrystals (SAL NCs) to treat colorectal cancer through the inhibitory enhancement of Wnt/beta-catenin signaling. The as-prepared SAL NCs exhibited excellent size distribution, stability, and improved water solubility.In vitrocellular uptake andin vivofluorescence imaging studies showed that SAL NCs increased cellular uptake efficiency compared with free SAL. As a result, SAL NCs exhibited significant higher cytotoxicity, 1.5-3 times better Wnt inhibitory effect, and 10 times better cancer stem cell inhibitory effect than free SAL. Furthermore, compared with free SAL, SAL NCs exhibited 2 times better anti-colon tumor effect in APC(min/+)transgenic mice through oral administration. Our results indicated that SAL NCs with enhanced cellular internalization and tumor tissue accumulation may be a promising agent for colorectal cancer management.

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