Evaluation of the antitumor effect of dexamethasone palmitate and doxorubicin co-loaded liposomes modified with a sialic acid–octadecylamine conjugate

Jing Sun, Yanzhi Song, Mei Lu, Xiangyun Lin, Yang Liu, Songlei Zhou, Yuqing Su, Yihui Deng*

*此作品的通讯作者

科研成果: 期刊稿件文章同行评审

38 引用 (Scopus)

摘要

Dexamethasone palmitate has the potential to inhibit the activity of tumor-associated macrophages, which promote cancer proliferation, invasion, and metastasis; however, only very high and frequent doses are capable of inducing antitumor effects. With the aim to reduce the anticancer dose and decrease the nonspecific toxicity, we designed a liposomal system to co-deliver dexamethasone palmitate and doxorubicin. Furthermore, a ligand conjugate sialic acid–octadecylamine, with enhanced affinity towards the membrane receptors over-expressed in tumors, was anchored on the surface of the liposomes to increase drug distribution to the tumor tissue. Co-loaded liposomes were developed using lipid film hydration method to load dexamethasone palmitate and remote loading technology to load doxorubicin. The co-loaded liposomes modified with sialic acid–octadecylamine represented comparable physicochemical properties and blood plasma profiles with conventional co-loaded liposomes, but the biodistribution proved that sialic acid–octadecylamine modified liposomes accumulated more in tumor. The co-loaded liposomes showed higher tumor growth suppression than the single-drug loaded liposomes, while showing no additional drug toxicity in S180-bearing Kunming mice. The co-loaded liposomes modified with sialic acid–octadecylamine achieved a significantly better antitumor effect, and induced “shedding” of cancerous tissue in the mice. These finding suggested that co-loaded liposomes modified with sialic acid–octadecylamine provided a safe therapeutic strategy with outstanding anticancer activity.

源语言英语
页(从-至)177-183
页数7
期刊European Journal of Pharmaceutical Sciences
93
DOI
出版状态已出版 - 10 10月 2016
已对外发布

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