4.4 Article

Tumor-Targeted Delivery of Bufalin-Loaded Modified Albumin-Polymer Hybrid for Enhanced Antitumor Therapy and Attenuated Hemolysis Toxicity and Cardiotoxicity

Journal

AAPS PHARMSCITECH
Volume 22, Issue 4, Pages -

Publisher

SPRINGER
DOI: 10.1208/s12249-021-02000-2

Keywords

bufalin; modified albumin polymer hybrid; tumor targetability; toxicity evaluation

Funding

  1. National Natural Science Foundation of China [81202930]
  2. China Postdoctoral Science Foundation [2017M610309, 2019T120403]
  3. Training Program for the Young Scholar of Jiangsu University, Henan Scientific and Technological Project [182102311187]
  4. Henan Medical Scientific and Technological Project [2018020408]

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A novel albumin polymer hybrid was designed for targeted delivery of the anticancer drug bufalin, demonstrating improved antitumor effects and reduced side effects.
A novel albumin polymer hybrid with a core-shell structure was designed to target delivery of bufalin, which is an antineoplastic monomer with serious cardiotoxicity. The sheath layer was composed of ursodeoxycholic acid (UA)-modified bovine serum albumin (UA-BSA), while the stable core consisted of poly n-butyl cyanoacrylate (PBCA) nanoparticles. The UA-BSA was synthetized, and the substitution degree was characterized. The physical properties of bufalin-loaded UA-modified protein-PBCA nanocomplexes (BF-uPPNCs), such as morphology, particle size, and encapsulation efficiency, were evaluated. FTIR and DSC revealed the bufalin to be in an amorphous state. Furthermore, the in vitro release study indicated a sustained release profile of BF-uPPNCs. The MTT and cellular uptake study demonstrated that BF-uPPNCs significantly improved the inhibitory effect of the bufalin accompanied with an enhanced cell uptake capacity on HepG2 cells. In addition, in vivo research demonstrated that BF-uPPNCs had a better antitumor effect coupled with improved therapeutic effect, and reduced hemolysis, vascular irritation, and cardiotoxicity. This work therefore presented a novel albumin polymer hybrid with favorable stability, efficient tumor-targeted delivery potential, and side effect reduction ability, which can be a potential vehicle for an anticancer drug.

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