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首页> 外文期刊>Food & Function >Development of a microparticulate system containing Brazilian propolis by-product and gelatine for ascorbic acid delivery: evaluation of intestinal cell viability and radical scavenging activity
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Development of a microparticulate system containing Brazilian propolis by-product and gelatine for ascorbic acid delivery: evaluation of intestinal cell viability and radical scavenging activity

机译:含有巴西蜂胶副产物和明胶的微粒系统的开发用于抗坏血酸输送:肠细胞活力和激进清除活性的评价

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摘要

The use of propolis by-product (PBP) microparticles (MP) as delivery systems can be a promising tool to surpass drawbacks related to low stability of ascorbic acid (AA). The objective of this study was to develop and characterize MP prepared with PBP containing AA. The MP was characterized regarding morphology, particle size, polydispersity index (PDI), association efficiency (AE), drug loading (DL), infrared and Raman spectroscopy as well as antioxidant and radical scavenging activity, in vitro release, and cellular studies. MP was shown to be spherical with some agglomeration. Its particle size was 1654 +/- 0.210 nm with a PDI of 0.7. The AE and DL were, respectively, 100.30 +/- 2.66% and 13.16 +/- 0.59. Spectroscopic studies indicated a possible interaction between the PBP and AA. 2,2-Diphenyl-1-picrylhydrazyl (DPPH center dot), 2,2'-azino-bis(3-ethylbenzothiazoline-6-sulphonic acid) (ABTS) and ferric reducing antioxidant power (FRAP) assays demonstrated that the MP containing AA have an excellent antioxidant capacity as well as a considerable scavenging activity against reactive oxygen and nitrogen species. The in vitro release profile showed a slow pattern of drug release of AA from MP. Viability studies with intestinal cells revealed that MP did not present toxicity in Caco-2 and HT29-MTX. Moreover, AA could permeate Caco-2 monolayers and triple co-culture substantially at the end of 8 h, opposite to the MP. Therefore, the proposed MP formulation represents a promising platform for oral delivery of AA with a local effect on intestines.
机译:使用蜂胶副产物(PBP)微粒(MP)作为递送系统可以是有前途的工具,以超越与抗坏血酸(AA)的低稳定性相关的缺点。本研究的目的是开发和表征含有AA的PBP制备的MP。该MP的特征在于形态,粒度,多分散性指数(PDI),结合效率(AE),药物负载(DL),红外和拉曼光谱以及抗氧化剂和自由基清除活性,体外释放和细胞研究。 MP被显示为具有一些聚集的球形。其粒度为1654 +/- 0.210nm,PDI为0.7。 AE和DL分别为100.30 +/- 2.66%和13.16 +/- 0.59。光谱研究表明了PBP和AA之间的可能相互作用。 2,2-二苯基-1-富铬酰基(DPPH中心点),2,2'-唑苯基 - 双(3​​-乙基苯并噻唑啉-6-磺酸)(ABTS)和还原抗氧化能力(FRAP)测定证明了含有的MP AA具有优异的抗氧化能力,以及针对反应性氧和氮物质的相当明显的清除活性。体外释放曲线显示出来自MP的AA的药物释放速度慢。肠道细胞的活力研究表明,MP在Caco-2和HT29-MTX中没有毒性。此外,AA可以在与MP相对的情况下基本上在8小时的末端渗透Caco-2单层和三重共培养。因此,所提出的MP制剂代表了对肠道局部影响的AA口服递送的有希望的平台。

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  • 来源
    《Food & Function》 |2018年第8期|共13页
  • 作者单位

    Univ Estadual Maringa Dept Pharm Lab Res &

    Dev Drug Delivery Syst Postgrad Program Pharmaceut Sci BR-87020900 Maringa Parana Brazil;

    Univ Porto Fac Pharm Dept Chem Sci LAQV REQUIMTE Rua Jorge Viterbo Ferreira 280 P-4050313 Porto Portugal;

    Univ Estadual Maringa Dept Pharm Lab Res &

    Dev Drug Delivery Syst Postgrad Program Pharmaceut Sci BR-87020900 Maringa Parana Brazil;

    Univ Estadual Maringa Dept Pharm Lab Res &

    Dev Drug Delivery Syst Postgrad Program Pharmaceut Sci BR-87020900 Maringa Parana Brazil;

    Univ Estadual Maringa Dept Pharm Lab Res &

    Dev Drug Delivery Syst Postgrad Program Pharmaceut Sci BR-87020900 Maringa Parana Brazil;

    Univ Porto Fac Pharm Dept Med Sci Lab Pharmaceut Technol Rua Jorge Viterbo Ferreira 280 P-4050313 Porto Portugal;

    Univ Porto Fac Pharm Dept Chem Sci LAQV REQUIMTE Rua Jorge Viterbo Ferreira 280 P-4050313 Porto Portugal;

    Univ Porto Fac Pharm Dept Chem Sci LAQV REQUIMTE Rua Jorge Viterbo Ferreira 280 P-4050313 Porto Portugal;

    Univ Porto i3S Rua Alfredo Allen 208 P-4200135 Porto Portugal;

    Univ Estadual Maringa Dept Pharm Lab Res &

    Dev Drug Delivery Syst Postgrad Program Pharmaceut Sci BR-87020900 Maringa Parana Brazil;

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  • 正文语种 eng
  • 中图分类 食品工业;
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