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地特胰岛素和300 U/mL甘精胰岛素在健康犬体内的药效学和药代动力学

Pharmacodynamics and pharmacokinetics of insulin detemir and insulin glargine 300 U/mL in healthy dogs.

作者信息

Fink H, Herbert C, Gilor C

机构信息

Department of Veterinary Clinical Sciences, College of Veterinary Medicine, The Ohio State University, 601 Vernon L Tharp St, Columbus, OH 43210, USA.

Department of Veterinary Clinical Sciences, College of Veterinary Medicine, The Ohio State University, 601 Vernon L Tharp St, Columbus, OH 43210, USA.

出版信息

Domest Anim Endocrinol. 2018 Jul;64:17-30. doi: 10.1016/j.domaniend.2018.03.007. Epub 2018 Apr 10.

Abstract

Insulin glargine 300 U/mL and insulin detemir are synthetic long-acting insulin analogs associated with minimal day-to-day variability or episodes of hypoglycemia in people. Here, 8 healthy purpose-bred dogs each received 2.4 nmol/kg subcutaneous injections of insulin detemir (0.1 U/kg) and insulin glargine 300 U/mL (0.4 U/kg) on 2 different days, >1 wk apart, in random order. Blood glucose (BG) was measured every 5 min, and glucose was administered intravenously at a variable rate with the goal of maintaining BG within 10% of baseline BG ("isoglycemic clamp"). Endogenous and exogenous insulin were measured for up to 24 h after insulin injection. The effect of exogenous insulin was defined by glucose infusion rate or a decline in endogenous insulin. Isoglycemic clamps were generated in all 8 dogs after detemir but only in 4 dogs after glargine. Median time to onset of action was delayed with glargine compared to detemir (4.0 h [3.3-5.8 h] vs 0.6 h [0.6-1.2 h], P = 0.002). There was no difference in time to peak (median [range] = 6.3 h [5.0-21.3 h] vs 4.3 h [2.9-7.4 h], P = 0.15) or duration of action (16.3 h [6.1-20.1 h] vs 10.8 h [8.8-14.8 h], P = 0.21) between glargine and detemir, respectively. Glargine demonstrated a peakless time-action profile in 4/8 dogs. The total metabolic effect and peak action of detemir was significantly greater than glargine. Significant concentrations of glargine were detected in all but 1 dog following administration. Glargine might be better suited than detemir as a once-daily insulin formulation in some dogs based on its long duration of action and peakless time-action profile. Day-to-day variability in insulin action should be further assessed for both formulations.

摘要

甘精胰岛素300 U/mL和地特胰岛素是合成的长效胰岛素类似物,在人体中日常变异性或低血糖发作极少。在此,8只健康的定向培育犬在2个不同日期、间隔超过1周,随机接受皮下注射2.4 nmol/kg地特胰岛素(0.1 U/kg)和甘精胰岛素300 U/mL(0.4 U/kg)。每5分钟测量一次血糖(BG),并以可变速率静脉输注葡萄糖,目标是将BG维持在基线BG的10%以内(“等血糖钳夹”)。在胰岛素注射后长达24小时测量内源性和外源性胰岛素。外源性胰岛素的作用通过葡萄糖输注速率或内源性胰岛素的下降来定义。所有8只犬在地特胰岛素注射后均产生了等血糖钳夹,但甘精胰岛素注射后仅4只犬产生了等血糖钳夹。与地特胰岛素相比,甘精胰岛素的中位起效时间延迟(4.0小时[3.3 - 5.8小时]对0.6小时[0.6 - 1.2小时],P = 0.002)。甘精胰岛素和地特胰岛素在达峰时间(中位值[范围]=6.3小时[5.0 - 21.3小时]对4.3小时[2.9 - 7.4小时],P = 0.15)或作用持续时间(16.3小时[6.1 - 20.1小时]对10.8小时[8.8 - 14.8小时],P = 0.21)方面无差异。甘精胰岛素在8只犬中有4只表现出无峰的时间 - 作用曲线。地特胰岛素的总代谢效应和峰值作用明显大于甘精胰岛素。给药后除1只犬外,其余所有犬均检测到显著浓度的甘精胰岛素。基于其长效作用和无峰的时间 - 作用曲线,在某些犬中,甘精胰岛素可能比地特胰岛素更适合作为每日一次的胰岛素制剂。两种制剂的胰岛素作用日常变异性应进一步评估。

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