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早期干预后环孢素诱导胰岛素依赖型糖尿病缓解。环孢素治疗1年与胰岛素分泌增强的关联。加拿大 - 欧洲随机对照试验组。

Cyclosporin-induced remission of IDDM after early intervention. Association of 1 yr of cyclosporin treatment with enhanced insulin secretion. The Canadian-European Randomized Control Trial Group.

出版信息

Diabetes. 1988 Nov;37(11):1574-82.

PMID:2903105
Abstract

A randomized double-blind placebo-controlled trial was undertaken to determine whether cyclosporin enhances remission of insulin-dependent diabetes mellitus (IDDM) through the 1st yr after diagnosis. Dosage with insulin was minimized with target control of blood glucose levels less than or equal to 7.8 mM (140 mg/dl) before meals. Metabolic control was evaluated by serial determinations of glycosylated hemoglobin levels, and endogenous secretion of insulin was evaluated by determination of the levels of glucagon-stimulated insulin-connecting peptide (CP) in the plasma at 3-mo intervals. A compound definition of remission required a glucagon-stimulated CP level in plasma greater than or equal to 0.6 nM or a non-insulin-receiving state (NIR) in which target control of glycemia was maintained without administration of insulin. A clinical definition of remission required only the NIR state as defined. One hundred eighty-eight patients aged 10-35 yr entered the study within 6 wk of initiation of insulin therapy and within 14 wk of onset of symptoms and were studied for 1 yr. There were no significant differences in metabolic control between the two treatment groups during the study. The anticipated adverse effects of cyclosporin were not more frequent or severe than in other experience with the drug, but histological changes attributable to cyclosporin were present in some kidney biopsies obtained from selected patients after 1 yr. At 1 yr, by the compound definition, 33% of the cyclosporin-group and 21% of the placebo-group patients were in remission, when the corresponding rates for NIR remissions were 24 and 10%.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

进行了一项随机双盲安慰剂对照试验,以确定环孢素是否能在诊断后的第1年内增强胰岛素依赖型糖尿病(IDDM)的缓解。通过将餐前血糖水平控制在小于或等于7.8 mM(140 mg/dl)的目标值,尽量减少胰岛素用量。通过连续测定糖化血红蛋白水平评估代谢控制情况,并每隔3个月通过测定血浆中胰高血糖素刺激的胰岛素连接肽(CP)水平评估胰岛素的内源性分泌。缓解的复合定义要求血浆中胰高血糖素刺激的CP水平大于或等于0.6 nM,或处于无需接受胰岛素治疗即可维持血糖目标控制的非胰岛素接受状态(NIR)。缓解的临床定义仅要求达到上述定义的NIR状态。188名年龄在10至35岁之间的患者在开始胰岛素治疗的6周内且症状出现后的14周内进入研究,并接受了1年的研究。在研究期间,两个治疗组的代谢控制情况没有显著差异。环孢素预期的不良反应并不比该药物的其他使用经验更频繁或严重,但在1年后从部分选定患者获取的肾活检中出现了归因于环孢素的组织学变化。1年后,根据复合定义,环孢素组33%的患者和安慰剂组21%的患者处于缓解状态,而NIR缓解的相应比例分别为24%和10%。(摘要截取自250字)

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