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Highly enhanced leukemia therapy and oral bioavailability from a novel amphiphilic prodrug of cytarabine

机译:高度增强的白血病治疗和口腔生物利用度从新型两亲性药物前药中的糖醇

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摘要

Cytarabine (1-beta-D-arabinofuranosylcytosine, Ara-C), an attractive medicinal treatment for myeloblastic leukemia, is subject to low oral bioavailability due to its weak membrane permeability and lipophilicity as well as its poor metabolic stability. Based on these considerations, we proposed a chemical linkage of cytarabine with lauric acid (LA), a long-chain fatty acid with 12 carbons, leading to a new prodrug, LA-Ara. The NH2 group of Ara-C is protected by conjugation and thus cannot not be deactivated by deamination; moreover, notably high liposolubility and penetrability were obtained. When dispersed in water, this new amphiphilic molecule can adopt a nanofiber configuration. It was found that LA-Ara molecules are stable in artificial biological media, indicating that the prodrug could be administrated orally. MTT assays on HL60 and K562 cells were performed, and the significantly higher cytotoxicity compared to the pure drug suggested that the prodrug has conspicuously superior antiproliferative activity. Following oral administration, the elimination half-life and bioavailability of the LA-Ara group dramatically increased to 6.6- and 32.8-fold of those of free Ara-C, respectively. It appears that this new prodrug could be an effective oral alternative treatment to Ara-C and supply a promising therapy index for leucocythemia.
机译:氰基(1-Beta-D-阿拉伯呋喃糖苷基胞嘧啶,ARA-C),对髓细胞白血病的有吸引力的药物治疗,由于其薄膜渗透性和亲脂性以及其代谢稳定性差,因此受到低口服生物利用度。基于这些考虑,我们提出了一种用11种碳酸(La)的红糖酸(La)的化学键,导致新的前药,La-Araa。 NH 2基团ARA-C受缀合保护,因此不能通过脱氨酸去激活;此外,获得了显着的脂质溶解度和渗透性。当分散在水中时,这种新的两亲分子可以采用纳米纤维配置。发现La-ARA分子在人工生物介质中是稳定的,表明前药可以口服给药。进行HL60和K562细胞上的MTT测定,与纯药物相比的细胞毒性显着提高,表明前药具有显着优异的抗增殖活性。在口服给药后,Sa-ARA组的消除半衰期和生物利用度分别从ara-c的自由ara-c的6.6-和32.8倍。似乎这个新的前药可能是ARA-C的有效口服替代治疗,并为白细胞血症提供有前途的治疗指数。

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  • 来源
    《RSC Advances 》 |2016年第42期| 共9页
  • 作者单位

    Shandong Univ Sch Pharmaceut Sci 44 West Wenhua Rd Jinan 250012 Shandong Peoples R China;

    Shandong Univ Sch Pharmaceut Sci 44 West Wenhua Rd Jinan 250012 Shandong Peoples R China;

    Shandong Univ Sch Pharmaceut Sci 44 West Wenhua Rd Jinan 250012 Shandong Peoples R China;

    Shandong Univ Sch Pharmaceut Sci 44 West Wenhua Rd Jinan 250012 Shandong Peoples R China;

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  • 正文语种 eng
  • 中图分类 化学 ;
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