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高效液相色谱法在小鼠体内A14-125I标记胰岛素处置研究中的应用

Application of HPLC in disposition study of A14-125I-labeled insulin in mice.

作者信息

Sato H, Tsuji A, Hirai K, Kang Y S

机构信息

Department of Pharmaceutics, Faculty of Pharmaceutical Sciences, Kanazawa University, Japan.

出版信息

Diabetes. 1990 May;39(5):563-9. doi: 10.2337/diab.39.5.563.

DOI:10.2337/diab.39.5.563
PMID:2185107
Abstract

To describe quantitatively the in vivo distribution and elimination of insulin, high-performance liquid chromatography (HPLC) separation was applied to the pharmacokinetic study of human insulin labeled with 125I at tyrosine A14 (A14-125I-insulin) as a tracer. Intact A14-125I-insulin levels were determined by HPLC and trichloroacetic acid (TCA) precipitation in plasma and various tissues after its intravenous bolus injection into mice. TCA precipitation consistently overestimated the intactness of A14-125I-insulin compared with HPLC, possibly due to the presence of both a TCA-precipitable intermediate degradation product of labeled insulin found in HPLC elution profiles and reported high-molecular-weight forms of labeled insulin in plasma. Thus, TCA precipitation gave a considerably lower total plasma clearance (Cltot) value than HPLC. The half-life of A14-125I-insulin was prolonged by a simultaneous injection of 8 U/kg unlabeled insulin, and labeled insulin behaved similarly to [14C]inulin (an extracellular fluid marker). The concentration time profiles of HPLC-separated labeled insulin in plasma were analyzed by a noncompartmental moment method, and both Cltot and steady-state apparent volume distribution (VDss) of A14-125I-insulin were considerably decreased by unlabeled insulin coadministration. In particular, VDss of labeled insulin decreased by 79%, similar to that of inulin (181 ml/kg), suggesting that the nonspecific binding of labeled insulin to tissues was so small that VDss of labeled insulin was reduced to the extracellular fluid volume (approximately 20% of the body weight) when its receptor binding was blocked effectively by unlabeled insulin.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

为了定量描述胰岛素在体内的分布和消除情况,采用高效液相色谱(HPLC)分离技术,对以酪氨酸A14位标记125I的人胰岛素(A14-125I-胰岛素)作为示踪剂进行药代动力学研究。在向小鼠静脉推注A14-125I-胰岛素后,通过HPLC和三氯乙酸(TCA)沉淀法测定血浆和各种组织中完整的A14-125I-胰岛素水平。与HPLC相比,TCA沉淀法始终高估了A14-125I-胰岛素的完整性,这可能是由于在HPLC洗脱图谱中发现了标记胰岛素的TCA可沉淀中间降解产物,以及血浆中存在已报道的标记胰岛素高分子量形式。因此,TCA沉淀法得到的总血浆清除率(Cltot)值比HPLC法低得多。同时注射8 U/kg未标记胰岛素可延长A14-125I-胰岛素的半衰期,且标记胰岛素的行为与[14C]菊粉(一种细胞外液标记物)相似。采用非房室矩法分析血浆中HPLC分离的标记胰岛素的浓度-时间曲线,未标记胰岛素的共同给药使A14-125I-胰岛素的Cltot和稳态表观分布容积(VDss)均显著降低。特别是,标记胰岛素的VDss降低了79%,与菊粉(181 ml/kg)相似,这表明标记胰岛素与组织的非特异性结合非常小,以至于当未标记胰岛素有效阻断其受体结合时,标记胰岛素的VDss降至细胞外液体积(约占体重的20%)。(摘要截短于250字)

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Application of HPLC in disposition study of A14-125I-labeled insulin in mice.高效液相色谱法在小鼠体内A14-125I标记胰岛素处置研究中的应用
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