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Articles

Co-delivery of F7 and crizotinib by thermosensitive liposome for breast cancer treatment

, , , , , , , , & show all
Pages 265-275 | Received 01 Sep 2021, Accepted 26 Oct 2021, Published online: 14 Dec 2021
 

Abstract

In order to enhance the targeting efficiency and reduce the side effects and drug resistance, crizotinib (Cri) and F7 were co-loaded in a thermosensitive liposome (TSL) (F7-Cri-TSL), which showed enhanced permeability and retention in breast cancer model, as well as local controlled release by external hyperthermia. Cri is an inhibitor for cell proliferation and a promoter of apoptosis, by inhibiting the phosphorylation of intracellular ALK and c-Met, but its drug resistance limits its application. F7 is a novel drug candidate with significant resistance to cyclin-dependent kinase, but its use was restricted by its high toxicity. The F7-Cri-TSL was found with excellent particle size (about 108 nm), high entrapment efficiency (>95%), significant thermosensitive property, and good stability. Furthermore, F7-Cri-TSL/H had strongest cell lethality compared with other formulations. On the MCF-7 xenograft mice model, the F7-Cri-TSL also exhibited therapeutic synergism of Cri, F7 and hyperthermia. Meanwhile, it was shown that the TSL reduced the systemic toxicity of the chemotherapy drug. Therefore, the F7-Cri-TSL may serve as a promising system for temperature triggered breast cancer treatment.

Disclosure statement

No potential conflict of interest was reported by the author(s).

Additional information

Funding

Authors are thankful to the support of Tianjin Natural Science General Project Fund [2018KJ124] and Open Fund of Tianjin Enterprise Key Laboratory on Hyaluronic Acid Application Research [no. KTRDHA-Y201906] provided by Tianjin Kangting Bioengineering Group Corp. Ltd.

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