Doxorubicin/cisplatin co-loaded hyaluronic acid/chitosan-based nanoparticles for in vitro synergistic combination chemotherapy of breast cancer
•DOX/CDDP-loaded polysaccharide-based nanovehicles were successfully prepared.•CDDP crosslinking enhanced the stability of NPHER2(DOX/CDDP).•CDDP and DOX were loaded onto AHA by chelation and Schiff’s base, respectively.•Nanoparticles composed of drug core and polysaccharide shell were fabricated.•C...
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Veröffentlicht in: | Carbohydrate polymers 2019-12, Vol.225, p.115206-115206, Article 115206 |
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Sprache: | eng |
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Zusammenfassung: | •DOX/CDDP-loaded polysaccharide-based nanovehicles were successfully prepared.•CDDP crosslinking enhanced the stability of NPHER2(DOX/CDDP).•CDDP and DOX were loaded onto AHA by chelation and Schiff’s base, respectively.•Nanoparticles composed of drug core and polysaccharide shell were fabricated.•Co-delivery of DOX and CDDP achieved great synergistic anticancer effect.
Combination chemotherapy has attracted more and more attention in the field of anticancer treatment. Herein, a synergetic targeted combination chemotherapy of doxorubicin (DOX) and cisplatin in breast cancer was realized by HER2 antibody-decorated nanoparticles assembled from aldehyde hyaluronic acid (AHA) and hydroxyethyl chitosan (HECS). Cisplatin and DOX were successively conjugated onto AHA through chelation and Schiff’s base reaction, respectively, forming DOX/cisplatin-loaded AHA inner core. The core was sequentially complexed with HECS and targeting HER2 antibody-conjugated AHA. The formed near-spherical nanoplatform had an average size of ∼160 nm and a zeta potential of −28 mV and displayed pH-responsive surface charge reversal and drug release behaviors. HER2 receptor-mediated active targeting significantly enhanced the cellular uptake of nanoplatform. Importantly, DOX and cisplatin exhibited a synergistic cell-killing effect in human breast cancer MCF-7 cells. These results clearly indicate that the novel nanoplatform is promising for synergistic combination chemotherapy of breast cancer. |
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ISSN: | 0144-8617 1879-1344 |
DOI: | 10.1016/j.carbpol.2019.115206 |