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比较健康猫体内德谷胰岛素和甘精胰岛素 300U/mL 的药效学和药代动力学。

Comparison of pharmacodynamics and pharmacokinetics of insulin degludec and insulin glargine 300 U/mL in healthy cats.

机构信息

Department of Veterinary Medicine and Epidemiology, University of California, Davis, 1 Shields Avenue, Davis, CA 95616, USA.

Department of Veterinary Surgical and Radiological Sciences, University of California, Davis, 1 Shields Avenue, Davis, CA 95616, USA.

出版信息

Domest Anim Endocrinol. 2019 Oct;69:19-29. doi: 10.1016/j.domaniend.2019.04.001. Epub 2019 Apr 16.

Abstract

Insulin glargine 300 U/mL (IGla-U300) and insulin degludec (IDeg) are synthetic insulin analogs designed as basal insulin formulations. In people, IGla-U300 is more predictable and longer acting compared with glargine 100 U/mL. The duration of action of IDeg in people is > 42 h, allowing flexibility in daily administration. We hypothesized that IDeg would have longer duration of action compared with IGla-U300 in healthy purpose-bred cats. Seven cats received 0.4 U/kg (subcutaneous) of IDeg and IGla-U300 on two different days, >1 wk apart. Exogenous insulin was measured and pharmacodynamic parameters were derived from glucose infusion rates during isoglycemic clamps and suppression of endogenous insulin. The Shapiro-Wilk test was used to assess normality, and normally distributed parameters were compared using paired t-tests. There was no difference between IDeg and IGla-U300 in onset, peak action, or total metabolic effect. On average, time to peak action (T) of IGla-U300 was 145 ± 114 min (95% confidence interval [CI] = 25-264) longer than T of IDeg (P = 0.03) and duration of action (T) of IGla-U300 was 250 ± 173 min (95% CI = 68-432) longer than T of IDeg (P = 0.02). The "flatness" of the time-action profile (as represented by the quotient of peak action/T) was significantly greater for IGla-U300 compared with IDeg (P = 0.04). Overall, insulin concentration measurements concurred with findings from isoglycemic clamps. Based on these data, IDeg is not suitable for once-daily administration in cats. The efficacy of once-daily IGla-U300 in diabetic cats should be further investigated.

摘要

甘精胰岛素 300U/mL(IGla-U300)和德谷胰岛素(IDeg)是两种合成的胰岛素类似物,被设计用作基础胰岛素制剂。在人体中,IGla-U300 比甘精胰岛素 100U/mL 更具预测性且作用时间更长。在人体中,IDeg 的作用时间超过 42 小时,这使其在日常给药方面具有更大的灵活性。我们假设 IDeg 在健康的专门饲养的猫中的作用时间会比 IGla-U300 更长。7 只猫在相隔超过 1 周的 2 天内分别接受了 0.4U/kg(皮下注射)的 IDeg 和 IGla-U300。通过测定外源性胰岛素并从等血糖钳夹期间的葡萄糖输注率和内源性胰岛素抑制中推导药效动力学参数。采用 Shapiro-Wilk 检验评估正态性,对正态分布参数采用配对 t 检验进行比较。IDeg 和 IGla-U300 在起始、峰值作用或总代谢作用方面没有差异。IGla-U300 的作用达峰时间(T)平均比 IDeg 长 145±114 分钟(95%置信区间[CI] = 25-264;P = 0.03),IGla-U300 的作用持续时间(T)比 IDeg 长 250±173 分钟(95%CI = 68-432;P = 0.02)。IGla-U300 的时间-作用曲线的“平坦度”(以峰作用/T 的商来表示)明显大于 IDeg(P = 0.04)。总的来说,胰岛素浓度测量结果与等血糖钳夹的结果一致。根据这些数据,IDeg 不适合在猫中每日给药 1 次。还需要进一步研究糖尿病猫中每日给药 1 次的 IGla-U300 的疗效。

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