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Controlled release of insulin and modified insulin from a novel injectable biodegradable gel.

机译:从新型可注射生物降解凝胶中控制释放胰岛素和修饰的胰岛素。

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摘要

The objective of the study was to develop a controlled release dosage form of insulin, which can provide basal concentrations of insulin in diabetic rats for 1 to 2 weeks after a single subcutaneous injection.;A biodegradable injectable drug delivery gel was prepared by dissolving a biodegradable polymer, poly(lactic-co-glycolic acid) (PLGA), in biocompatible plasticizer(s), triethyl citrate (TEC) and/or acetyl triethyl citrate (ATEC). Insulin was then loaded into the blank gel to form an insulin suspension in the polymer solution. After the insulin-loaded gel was injected subcutaneously, the plasticizer(s) dissolved in the aqueous media and were gradually taken away from the gel. The polymer precipitated after the plasticizer(s) were extracted by the aqueous medium and a solid depot of insulin was formed. The insulin was released slowly from the depot by a combination of drug diffusion and erosion of the polymer.;In the first part of this study, the effect of different water-soluble and water-insoluble zinc salts on blood glucose lowering effect of insulin in type-2 diabetic ZDF rats was investigated. Insulin formulations containing varying concentrations of different water-soluble and water-insoluble zinc salts were prepared and injected subcutaneously in type-2 ZDF rats and blood glucose concentration lowering effect was studied. Insulin in presence of water-soluble salts of zinc could suppress blood glucose concentrations in ZDF rats for up to 16 hours.;Insulin was loaded into different gel formulations (5% PLGA (i.v. 0.09, acid end group), ATEC:TEC (3:1) and 4% insulin) and tested in vivo. However, the insulin-loaded gel formulations only suppressed the blood glucose concentrations in the ZDF rats for 1 day after a single subcutaneous injection. In order to achieve longer control over the release of insulin from the gels, a water-soluble salt, zinc sulfate was incorporated in these insulin containing gels at different concentrations. A biodegradable injectable gel formulation prepared with zinc sulfate was able to maintain low blood glucose concentrations for up to 8 to 10 days following a single subcutaneous injection.;In order to achieve better glucose control after the release of insulin from the gels, insulin glargine particles were purified from commercially available LantusRTM formulation. The freeze dried insulin glargine particles were then loaded into the blank gels and tested in vivo. The formulation prepared with 5% PLGA (i.v. 0.09, acid end group), ATEC:TEC (3:1) and 4% insulin glargine was able to suppress the blood glucose concentrations of the ZDF rats significantly for 10 days after a single subcutaneous injection. The concentration of insulin glargine was maintained between 260 +/- 134.9 mIU/L and 188 +/- 55.9 mIU/L until day 10 after single subcutaneous injection. The addition of zinc sulfate to the formulations prepared with purified insulin glargine particles further slowed down the drop in blood glucose concentrations.
机译:该研究的目的是开发一种胰岛素的控释剂型,该剂型可以在单次皮下注射后的1至2周内为糖尿病大鼠提供基础浓度的胰岛素。通过溶解可生物降解的药物制备可生物降解的可注射药物递送凝胶生物相容性增塑剂中的聚合物,聚乳酸-乙醇酸共聚物(PLGA),柠檬酸三乙酯(TEC)和/或乙酰基柠檬酸三乙酯(ATEC)。然后将胰岛素加载到空白凝胶中,以在聚合物溶液中形成胰岛素悬浮液。皮下注射负载胰岛素的凝胶后,增塑剂溶解在水性介质中,并逐渐从凝胶中取出。用水性介质萃取增塑剂后沉淀出的聚合物,形成胰岛素的固体贮库。胰岛素通过药物扩散和聚合物侵蚀的结合而从贮库中缓慢释放。;在本研究的第一部分,不同水溶性和水不溶性锌盐对胰岛素降血糖作用的影响研究了2型糖尿病ZDF大鼠。制备了包含不同浓度的不同水溶性和非水溶性锌盐的胰岛素制剂,并将其皮下注射到2型ZDF大鼠中,研究了降低血糖浓度的作用。含有锌的水溶性锌盐的胰岛素可以抑制ZDF大鼠长达16小时的血糖浓度;将胰岛素装入不同的凝胶制剂(5%PLGA(iv 0.09,酸性端基),ATEC:TEC(3 :1)和4%胰岛素),并在体内进行了测试。但是,在单次皮下注射后的1天内,装载胰岛素的凝胶制剂只能抑制ZDF大鼠的血糖浓度。为了更长久地控制胰岛素从凝胶中的释放,将水溶性盐硫酸锌以不同浓度掺入这些含胰岛素的凝胶中。单次皮下注射后,用硫酸锌制备的可生物降解的注射用凝胶制剂能够在长达8至10天的时间内保持低血糖浓度。为了从凝胶中释放胰岛素后更好地控制葡萄糖,甘精胰岛素颗粒从市售的LantusRTM制剂中纯化纯化的产物。然后将冷冻干燥的甘精胰岛素颗粒装载到空白凝胶中并进行体内测试。用5%PLGA(静脉内0.09,酸性端基),ATEC:TEC(3:1)和4%甘精胰岛素制备的制剂能够在单次皮下注射后的10天内显着抑制ZDF大鼠的血糖浓度。一次皮下注射后第10天,甘精胰岛素的浓度一直保持在260 +/- 134.9 mIU / L和188 +/- 55.9 mIU / L之间。将硫酸锌添加到用纯化的甘精胰岛素颗粒制备的制剂中进一步减慢了血糖浓度的下降。

著录项

  • 作者

    Anand, Om.;

  • 作者单位

    The University of Tennessee Health Science Center.;

  • 授予单位 The University of Tennessee Health Science Center.;
  • 学科 Health Sciences Pharmacy.
  • 学位 Ph.D.
  • 年度 2008
  • 页码 131 p.
  • 总页数 131
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

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