Heller S R, Amiel S A, Evans M L, Kong M-F, Macdonald I A, Peacey S R
University of Sheffield, Sheffield, UK.
Diabetes Obes Metab. 2002 Mar;4(2):106-12. doi: 10.1046/j.1463-1326.2002.00186.x.
Insulin lispro used in an intensive basal/bolus regimen produces equivalent glycaemic control to human-soluble insulin but reduces rates of hypoglycaemia. We tested the hypothesis that the use of rapid-acting analogues might prevent the development of defective hypoglycaemic counterregulation during intensive insulin therapy.
Ten patients with type 1 diabetes (four female, mean age 33 +/- 3 years, diabetes duration 12 +/- 2 years) participated in an open, randomized cross-over study, with 2 months run-in and 4-month treatment periods using either lispro or human-soluble insulin before meals and human NPH insulin (NPH) at night. The total of reported hypoglycaemic episodes (lispro vs. soluble, 123 vs. 128) and HbA(1c) (6.1 +/- 0.2 vs. 6.6 +/- 0.2%) were similar during both treatments. At the end of each period, we measured symptomatic, counterregulatory and cognitive responses, and glycaemic thresholds during hypoglycaemia, induced with a hyperinsulinaemic clamp (blood glucose of 5, 4.5, 3.5 and 2.5 mmol/l).
We found similar overall responses of adrenaline, cortisol, growth hormone and total symptom score. Glycaemic thresholds for rises in adrenaline (3.1 +/- 0.2 vs. 3.1 +/- 0.2 mmol/l, p = 0.76), cortisol (2.2 +/- 0.1 vs. 2.2 +/- 0.1 mmol/l, p = 0.16), growth hormone (3.3 +/- 0.15 vs. 2.9 +/- 0.2 mmol/l, p = 0.13), symptoms (3.2 +/- 0.2 vs. 3.3 +/- 0.1 mmol/l, p = 0.051) and impaired cognitive function (3.0 +/- 0.2 vs. 3.0 +/-0.2 mmol/l, p = 0.20) were also similar.
Four months of intensive treatment, with insulin lispro used pre-prandially and isophane at night, produced relatively preserved but equivalent physiological responses to hypoglycaemia as those on soluble insulin. Longer periods of treatment or alternative regimens may be necessary to demonstrate beneficial effects on hypoglycaemic physiological responses.
在强化基础/餐时胰岛素治疗方案中使用赖脯胰岛素,其血糖控制效果与普通胰岛素相当,但可降低低血糖发生率。我们检验了一个假设,即在强化胰岛素治疗期间使用速效胰岛素类似物可能预防低血糖反调节功能缺陷的发生。
10例1型糖尿病患者(4例女性,平均年龄33±3岁,糖尿病病程12±2年)参与了一项开放、随机交叉研究,有2个月的导入期和4个月的治疗期,分别使用赖脯胰岛素或普通胰岛素于餐前注射,晚上使用人NPH胰岛素(NPH)。两种治疗期间报告的低血糖发作总数(赖脯胰岛素组对普通胰岛素组,分别为123次对128次)和糖化血红蛋白(HbA1c)水平(分别为6.1±0.2%对6.6±0.2%)相似。在每个治疗期结束时,我们测量了低血糖时的症状性、反调节性和认知反应以及血糖阈值,通过高胰岛素-正葡萄糖钳夹技术诱导低血糖(血糖分别为5、4.5、3.5和2.5 mmol/L)。
我们发现肾上腺素、皮质醇、生长激素的总体反应以及总症状评分相似。肾上腺素升高的血糖阈值(分别为3.1±0.2 mmol/L对3.1±0.2 mmol/L,p = 0.76)、皮质醇(分别为2.2±0.1 mmol/L对2.2±0.1 mmol/L,p = 0.16)、生长激素(分别为3.3±0.15 mmol/L对2.9±0.2 mmol/L,p = 0.13)、症状(分别为3.2±0.2 mmol/L对3.3±0.1 mmol/L,p = 0.051)和认知功能受损(分别为3.0±0.2 mmol/L对3.0±0.2 mmol/L,p = 0.20)也相似。
4个月的强化治疗,即餐前使用赖脯胰岛素、晚上使用低精蛋白胰岛素,与使用普通胰岛素相比,对低血糖产生的生理反应相对保留但相当。可能需要更长的治疗时间或替代治疗方案来证明对低血糖生理反应的有益影响。
