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负载α-香树脂醇的纳米胶囊在白血病细胞中产生选择性细胞毒性活性。

α-amyrin-loaded nanocapsules produce selective cytotoxic activity in leukemic cells.

作者信息

Neto Serafim Florentino, Prada Ariadna Lafourcade, Achod Leonardo Domingo Rosales, Torquato Heron Fernandes Vieira, Lima Cauê Santos, Paredes-Gamero Edgar Julian, Silva de Moraes Maria Oneide, Lima Emerson Silva, Sosa Edgar Hernandez, de Souza Tatiane Pereira, Amado Jesus Rafael Rodriguez

机构信息

Laboratory of Innovation and Development in Pharmaceutical Technology (LIDETEF), Faculty of Pharmaceutical Sciences, Universidade Federal do Amazonas, Av. Rodrigo Octavio Ramos, 6200, Coroado, Manaus, AM CEP 69077-000, Brazil.

Biochemistry Department, Universidade Federal de São Paulo, Rua Três de Maio 100, São Paulo, SP, CEP 04044-020, Brazil.

出版信息

Biomed Pharmacother. 2021 Jul;139:111656. doi: 10.1016/j.biopha.2021.111656. Epub 2021 May 8.

Abstract

INTRODUCTION

Amyrins are triterpenes that have attractive pharmacological potential; however, their low water solubility and erratic stomach absorption hinders their use as a drug. The aim of this paper was to develop a novel α-amyrin-loaded nanocapsule for intestinal delivery and evaluate, preliminarily, its cytotoxic ability against leukemic cells.

MATERIAL AND METHODS

Five nanocapsule formulations were designed by the solvent displacement-evaporation method. Poly-ε-caprolactone, Eudragit® E100, and Kollicoat® Mae 100 P were used as film-former materials. Particle size, polydispersity index (PdI), zeta potential, and the pH of all formulations were measured. The cytotoxic potential of the nanocapsules was evaluated in vitro using different leukemic lineages RESULTS: Nanocapsules coated with Kollicoat® Mae 100 P presented the smallest particle size (130 nm), the lowest zeta-potential (-38 mV), and the narrowest size distribution (PdI = 0.100). The entrapment efficiency was 65.47%, while the loading capacity was 2.40%. Nanocapsules release 100% of α-amyrin in 40 min (pH 7.4), by using a possible mechanism of swelling-diffusion. The formulation showed excellent on-shelf physicochemical stability during one year. Additionally, nanocapsules produced a selective cytotoxic effect on a human leukemia lineage Kasumi-1, an acute myeloid leukemia cell line, and produced cell death by apoptosis CONCLUSION: α-amyrin-loaded nanocapsules appear to be a promising nanoformulation that could be used against leukemia.

摘要

引言

羽扇豆醇是具有诱人药理潜力的三萜类化合物;然而,其低水溶性和不稳定的胃吸收性阻碍了它们作为药物的应用。本文的目的是开发一种用于肠道给药的新型载α-羽扇豆醇纳米胶囊,并初步评估其对白血病细胞的细胞毒性能力。

材料与方法

采用溶剂置换蒸发法设计了五种纳米胶囊制剂。聚ε-己内酯、Eudragit® E100和Kollicoat® Mae 100 P用作成膜材料。测量了所有制剂的粒径、多分散指数(PdI)、zeta电位和pH值。使用不同的白血病谱系在体外评估纳米胶囊的细胞毒性潜力。结果:用Kollicoat® Mae 100 P包衣的纳米胶囊呈现出最小的粒径(130 nm)、最低的zeta电位(-38 mV)和最窄的粒径分布(PdI = 0.100)。包封率为65.47%,而载药量为2.40%。纳米胶囊在40分钟内(pH 7.4)释放100%的α-羽扇豆醇,可能通过溶胀扩散机制。该制剂在一年内表现出优异的货架期物理化学稳定性。此外,纳米胶囊对人白血病谱系Kasumi-1(一种急性髓性白血病细胞系)产生了选择性细胞毒性作用,并通过凋亡导致细胞死亡。结论:载α-羽扇豆醇纳米胶囊似乎是一种有前途的纳米制剂,可用于对抗白血病。

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