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早晨一剂甘精胰岛素可预防在使用赖脯胰岛素进行餐后皮下胰岛素持续输注中断后出现的夜间酮症。

A morning dose of insulin glargine prevents nocturnal ketosis after postprandial interruption of continuous subcutaneous insulin infusion with insulin lispro.

作者信息

Johansson U B, Wredling R, Adamson U, Lins P E

机构信息

Department of Clinical Sciences, Karolinska Institute, Danderyd Hospital, Division of Internal Medicine, and Sophiahemmet University College, Box 5605, SE-114 86 Stockholm, Sweden.

出版信息

Diabetes Metab. 2007 Dec;33(6):469-71. doi: 10.1016/j.diabet.2007.06.005. Epub 2007 Nov 26.

Abstract

AIM

The aim of this crossover trial was to evaluate the potential of partial substitution of basal insulin with glargine, administered once daily in the morning, to protect against nocturnal ketosis after postprandial interruption of continuous subcutaneous insulin infusion (CSII).

METHODS

Seven patients with type 1 diabetes received 4 weeks of treatment with insulin lispro, administered by CSII, and 4 weeks of treatment with CSII and a partial basal replacement dose of insulin glargine administered in the morning. On day 28 of each treatment phase, patients were admitted to the research unit where dinner was served and their usual dinner insulin bolus dose given, after which CSII was discontinued at 7 pm. Plasma (p) beta-hydroxybutyrate and p glucose were measured every hour for 12 h thereafter.

RESULTS

Plasma beta-hydroxybutyrate at 7 pm was 0.16+/-0.05 and 0.13+/-0.07 mmol/l with and without glargine, respectively, and increased to 0.17+/-0.10 and 0.60+/-0.3 mmol/l within 6 h (P=0.02). Plasma glucose increased without glargine, from 8.6+/-2.9 to 21.1+/-3.0 mmol/l (P=0.003), but did not rise significantly following glargine (13.6+/-4.7 vs. 12.6+/-5.6 mmol/l; P=0.65).

CONCLUSIONS

Partial replacement with a morning dose of insulin glargine protects against the development of ketosis for as much as 12 h after postprandial interruption of CSII. This treatment strategy could, therefore, be useful for patients who are prone to ketosis but, for other reasons, are deemed suitable for CSII.

摘要

目的

本交叉试验旨在评估每日清晨一次注射甘精胰岛素部分替代基础胰岛素,以预防餐后中断持续皮下胰岛素输注(CSII)后夜间酮症的可能性。

方法

7例1型糖尿病患者接受4周赖脯胰岛素CSII治疗,以及4周CSII联合清晨部分基础替代剂量甘精胰岛素治疗。在每个治疗阶段的第28天,患者入住研究单位,进食晚餐并给予常规晚餐胰岛素推注剂量,之后晚上7点停止CSII。此后12小时内每小时测量血浆β-羟基丁酸和血糖。

结果

晚上7点时,使用和未使用甘精胰岛素时血浆β-羟基丁酸分别为0.16±0.05和0.13±0.07 mmol/l,6小时内分别升至0.17±0.10和0.60±0.3 mmol/l(P=0.02)。未使用甘精胰岛素时血糖从8.6±2.9 mmol/l升至21.1±3.0 mmol/l(P=0.003),而使用甘精胰岛素后血糖未显著升高(13.6±4.7 vs. 12.6±(此处原文似乎有误,推测为5.6) mmol/l;P=0.65)。

结论

清晨剂量的甘精胰岛素部分替代可预防餐后中断CSII后长达12小时的酮症发生。因此,这种治疗策略可能对易发生酮症但因其他原因适合CSII的患者有用。

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