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Optimization of perfusate pH to improve microdialysis recovery of lipophilic compounds.

机译:优化灌注液的pH值以改善亲脂性化合物的微透析回收率。

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摘要

Microdialysis (MD) allows sampling of compounds in-vivo from tissues' interstitial fluid. However, molecules insoluble at physiological pH have usually extremely low recovery. The addition of albumin to the perfusate or the use of isotonic lipoemulsion improves recovery of these molecules although it requires a cleaning step before HPLC analysis. This study investigates the possibility of improving the MD recovery of compounds insoluble at physiological pH but soluble at a different pH. The probe is perfused with an isotonic solution adjusted to pH values at which the compound has maximum solubility. Ketoconazole (KTC), clotrimazole (CLT) and tretinoin (TTN) were selected as model drugs because they are almost insoluble at pH 7.4 but soluble at pH 4 for KTC and CTL; and at pH 9 for TTN.;Linear microdialysis probes were used to collect KTC, CLT or TTN from a standard solution of the compounds. Probes were perfused with 0.01M pH 7.4 isotonic buffer solution (1) without or (2) with 5% Bovine Serum Albumin (BSA); or (3) with 20% isotonic lipoemulsion; or (4) with 0.01M pH 4 isotonic buffer solution for KTC and CLT or 0.01M pH 9 isotonic buffer solution for TTN. The method was then tested in vivo, in rabbit skin, to assess the skin tolerance to the non-physiological perfusates and to monitor KTC and TTN delivery from commercial cream products.;In-vitro, the optimized-pH perfusate increased MD recovery significantly (P<0.001): 6.9 (KTC), 8.3 (CLT), and 2.0 (TTN) times compared to the physiological pH and 1.4 and 1.2 compared to the BSA and lipoemulsion respectively. No evidence of irritation or edema was observed in-vivo. However, KTC and TTN were not detected in vivo with any of the modified perfusate tested.;In conclusion, these findings show that the optimized-pH perfusate effectively increases the in-vitro microdialysis recovery of KTC, CLT and TTN and that it is well tolerated in vivo. However, the compounds tested (KTC and TTN) could not be detected in-vivo..
机译:微透析(MD)允许从组织的组织液中体内采样化合物。然而,在生理pH下不溶的分子通常具有极低的回收率。向灌注液中添加白蛋白或使用等渗脂肪乳剂可改善这些分子的回收率,尽管这需要在HPLC分析之前进行清洁。这项研究探讨了改善在生理pH下不溶但在不同pH下可溶的化合物的MD回收率的可能性。用等渗溶液灌注探针,该等渗溶液的pH值调节至化合物具有最大溶解度。选择酮康唑(KTC),克霉唑(CLT)和维甲酸(TTN)作为模型药物,因为它们对于KTC和CTL在pH 7.4时几乎不溶,但在pH 4时可溶。 ;在TTN的pH值为9时。使用线性微透析探针从化合物的标准溶液中收集KTC,CLT或TTN。用0.01M pH 7.4等渗缓冲溶液(1)不含或(2)含5%牛血清白蛋白(BSA)灌注探针;或(3)含20%等渗脂肪乳剂;或或(4)对于KTC和CLT用0.01M pH 4等渗缓冲溶液,对于TTN用0.01M pH 9等渗缓冲溶液。然后对该方法进行了体内兔皮肤测试,以评估其对非生理性灌洗液的耐受性,并监测商品乳膏产品中的KTC和TTN释放量;在体外,优化的pH灌洗液可显着提高MD回收率( P <0.001):分别为生理pH值的6.9(KTC),8.3(CLT)和2.0(TTN)倍,与BSA和脂乳剂分别为1.4和1.2。体内未见刺激或水肿的迹象。但是,在测试的任何改性灌流液中均未在体内检测到KTC和TTN。总而言之,这些发现表明,优化的pH灌流液可有效提高KTC,CLT和TTN的体外微透析回收率,而且效果很好。体内耐受。但是,无法在体内检测到测试的化合物(KTC和TTN)。

著录项

  • 作者

    Tre, Emmanuelle Sandra.;

  • 作者单位

    Long Island University, The Brooklyn Center.;

  • 授予单位 Long Island University, The Brooklyn Center.;
  • 学科 Health Sciences Toxicology.;Health Sciences Pharmacology.;Health Sciences Pharmacy.
  • 学位 Ph.D.
  • 年度 2013
  • 页码 119 p.
  • 总页数 119
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

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