4.5 Article

Facile preparation of copper-gallic acid nanoparticles as a high reproducible and drug loading platform for doxorubicin

出版社

ELSEVIER
DOI: 10.1016/j.jddst.2022.103686

关键词

Doxorubicin; Anticancer; Metal ions; Drug delivery system

资金

  1. Science &TechnologySupport Program of Changzhou (Application Basic Research)
  2. Natural Science Foundation of Jiangsu Province [CJ20210142, CE20225047]
  3. International Scientific Cooperation Project of Changzhou Scientific Bureau [BK20210851, BK20190566, BK20221381]
  4. QingLan Project of Jiangsu Province [CZ20200015]
  5. China Postdoctoral Science Foundation Funded Project
  6. Jiangsu Postdoctoral Science Foundation [2021M690482, 2020M671279]
  7. Project of Jiangsu Province Key Laboratory of Radiation Medicine and Protection, Soochow University [2021K014A]
  8. Scientific Research Foundation of Jiangsu Provincial Education Department, China [KJS2104]
  9. [21KJD350003]

向作者/读者索取更多资源

In this study, a convenient method was used to prepare DOX loaded DDSs with high reproducibility and drug loading. The DDSs showed uniform particle size, good biocompatibility, and decent anticancer performance.
Purpose: Doxorubicin (DOX) is the first line drug for cancer chemotherapy but its application is limited by the poor bioavailability and high side effects. Current drug delivery systems (DDSs) of DOX can overcome the above mentioned shortages, but also brings new challenges including low reproducibility and DOX loading. Therefore, the one-step preparation of related DDSs with high DOX loading capacity is highly desirable.Methods: Herein, taking advantage of the high complexing ability of both gallic acid (GA) and DOX to metal ions, copper ion was selected as a model ion to serve as a medium, not only to form nanostructured platform with GA, but also as a linker to give high DOX loading capacity to the developed DDSs.Results: We herein introduced a facile method to conveniently prepare DOX loaded DDSs (Cu-GA-DOX NPs) with high reproducibility and drug loading of DOX (23.07%), which also showed uniform particle size, good biocompatibility as well as decent anticancer performance on model colorectal cancers (CT26). Conclusion: This study provides a new strategy and pave the way for the subsequent development of DDS with high reproducibility and DOX loading.

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