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利多卡因在老年人中的蛋白结合及处置情况。

Protein binding and disposition of lignocaine in the elderly.

作者信息

Cusack B, O'Malley K, Lavan J, Noel J, Kelly J G

出版信息

Eur J Clin Pharmacol. 1985;29(3):323-9. doi: 10.1007/BF00544089.

Abstract

Single dose studies were performed in six young and six elderly nonsmokers using lignocaine as a model drug with high intrinsic clearance. Subjects received lignocaine 250 mg orally and 50 mg intravenously in random order and drug concentrations in blood and plasma were measured for up to 8 h after dose. Protein binding was estimated at 37 degrees C by equilibrium dialysis. Indocyanine green kinetics were also calculated in each individual following 0.15 mg/kg intravenously. Bioavailability of lignocaine was greater in the elderly but there was no apparent difference in the rate of absorption. Intrinsic clearance of lignocaine was lower in the aged. Elimination half-life was longer in the elderly but there was no significant difference in apparent volume of distribution or systemic clearance of lignocaine. Plasma clearance of indocyanine green showed no correlation with systemic lignocaine clearance and was lower in the aged subjects. Blood/plasma lignocaine ratio was less than unity in both groups. Binding of lignocaine to plasma proteins showed concentration-dependence and was higher in the geriatric group. Maximum binding capacity of lignocaine was greater in the elderly but the binding affinity did not significantly change with age. Greater oral bioavailability of drugs like lignocaine may produce higher plasma concentrations in the elderly. Unlike indocyanine green, the systemic clearance of lignocaine was unaltered by age in this group of non-smokers. The protein-binding of lignocaine, like many other basic drugs, is increased in elderly subjects.

摘要

在6名年轻和6名老年非吸烟者中进行了单剂量研究,使用利多卡因作为具有高内在清除率的模型药物。受试者随机接受250mg口服利多卡因和50mg静脉注射利多卡因,并在给药后长达8小时测量血液和血浆中的药物浓度。通过平衡透析在37℃下估计蛋白质结合率。在静脉注射0.15mg/kg后,还计算了每个个体的吲哚菁绿动力学。利多卡因在老年人中的生物利用度更高,但吸收速率没有明显差异。利多卡因的内在清除率在老年人中较低。老年人的消除半衰期更长,但利多卡因的表观分布容积或全身清除率没有显著差异。吲哚菁绿的血浆清除率与全身利多卡因清除率无相关性,且在老年受试者中较低。两组的血/浆利多卡因比值均小于1。利多卡因与血浆蛋白的结合呈浓度依赖性,在老年组中更高。利多卡因的最大结合能力在老年人中更大,但结合亲和力不会随年龄显著变化。像利多卡因这样的药物在老年人中更高的口服生物利用度可能会产生更高的血浆浓度。与吲哚菁绿不同,在这组非吸烟者中,利多卡因的全身清除率不受年龄影响。与许多其他碱性药物一样,老年人中利多卡因的蛋白质结合增加。

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