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强化胰岛素治疗可降低创伤性脑损伤后的微透析葡萄糖值,但不改变葡萄糖利用率或改善乳酸/丙酮酸比值。

Intensive insulin therapy reduces microdialysis glucose values without altering glucose utilization or improving the lactate/pyruvate ratio after traumatic brain injury.

作者信息

Vespa Paul, Boonyaputthikul Robert, McArthur David L, Miller Chad, Etchepare Maria, Bergsneider Marvin, Glenn Thomas, Martin Neil, Hovda David

机构信息

UCLA Division of Neurosurgery, Los Angeles, CA, and Barrows Neurologic Institute, Phoenix, AZ, USA.

出版信息

Crit Care Med. 2006 Mar;34(3):850-6. doi: 10.1097/01.CCM.0000201875.12245.6F.

DOI:10.1097/01.CCM.0000201875.12245.6F
PMID:16505665
Abstract

OBJECTIVE

To determine that intensive glycemic control does not reduce microdialysis glucose concentration brain metabolism of glucose.

DESIGN

Prospective monitoring followed by retrospective data analysis of cerebral microdialysis and global brain metabolism.

SETTING

Single center, academic neurointensive care unit.

PATIENTS

Forty-seven moderate to severe traumatic brain injury patients.

INTERVENTIONS

A nonrandomized, consecutive design was used for glycemic control with loose insulin (n=33) for the initial 2 yrs or intensive insulin therapy (n=14) for the last year.

MEASUREMENTS AND MAIN RESULTS

In 14 patients treated with intensive insulin therapy, there was a reduction in microdialysis glucose by 70% of baseline concentration compared with a 15% reduction in 33 patients treated with a loose insulin protocol. Despite this reduction in microdialysis glucose, the global metabolic rate of glucose did not change. However, intensive insulin therapy was associated with increased incidence of microdialysis markers of cellular distress, namely elevated glutamate (38+/-37% vs. 10+/-17%, p<.01), elevated lactate/pyruvate ratio (38+/-37% vs. 19+/-26%, p<.03) and low glucose (26+/-17% vs. 11+/-15%, p<.05, and increased global oxygen extraction fraction. Mortality was similar in the intensive and loose insulin treatment groups (14% vs. 15%, p=.9), as was 6-month clinical outcome (p=.3).

CONCLUSIONS

Intensive insulin therapy results in a net reduction in microdialysis glucose and an increase in microdialysis glutamate and lactate/pyruvate without conveying a functional outcome advantage.

摘要

目的

确定强化血糖控制不会降低脑微透析葡萄糖浓度及葡萄糖的脑代谢。

设计

前瞻性监测,随后对脑微透析和全脑代谢进行回顾性数据分析。

地点

单中心学术性神经重症监护病房。

患者

47例中重度创伤性脑损伤患者。

干预措施

采用非随机连续设计进行血糖控制,最初2年采用宽松胰岛素治疗(n = 33),最后1年采用强化胰岛素治疗(n = 14)。

测量指标及主要结果

在接受强化胰岛素治疗的14例患者中,微透析葡萄糖较基线浓度降低了70%,而在接受宽松胰岛素方案治疗的33例患者中降低了15%。尽管微透析葡萄糖有所降低,但葡萄糖的整体代谢率并未改变。然而,强化胰岛素治疗与细胞应激的微透析标志物发生率增加有关,即谷氨酸升高(38±37% 对 10±17%,p <.01)、乳酸/丙酮酸比值升高(38±37% 对 19±26%,p <.03)和低血糖(26±17% 对 11±15%,p <.05),且整体氧摄取分数增加。强化胰岛素治疗组和宽松胰岛素治疗组的死亡率相似(14% 对 15%,p =.9),6个月时的临床结局也相似(p =.3)。

结论

强化胰岛素治疗导致微透析葡萄糖净减少,微透析谷氨酸和乳酸/丙酮酸增加,但未带来功能结局优势。

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