强化胰岛素治疗对新诊断2型糖尿病患者β细胞功能及血糖控制的影响：一项多中心随机平行组试验

Effect of intensive insulin therapy on beta-cell function and glycaemic control in patients with newly diagnosed type 2 diabetes: a multicentre randomised parallel-group trial.

作者信息

Weng Jianping, Li Yanbing, Xu Wen, Shi Lixin, Zhang Qiao, Zhu Dalong, Hu Yun, Zhou Zhiguang, Yan Xiang, Tian Haoming, Ran Xingwu, Luo Zuojie, Xian Jing, Yan Li, Li Fangping, Zeng Longyi, Chen Yanming, Yang Liyong, Yan Sunjie, Liu Juan, Li Ming, Fu Zuzhi, Cheng Hua

机构信息

Third Affiliated Hospital of Sun Yat-Sen University, Guangzhou, China.

出版信息

Lancet. 2008 May 24;371(9626):1753-60. doi: 10.1016/S0140-6736(08)60762-X.

DOI:10.1016/S0140-6736(08)60762-X

PMID:18502299

Abstract

BACKGROUND

Early intensive insulin therapy in patients with newly diagnosed type 2 diabetes might improve beta-cell function and result in extended glycaemic remissions. We did a multicentre, randomised trial to compare the effects of transient intensive insulin therapy (continuous subcutaneous insulin infusion [CSII] or multiple daily insulin injections [MDI]) with oral hypoglycaemic agents on beta-cell function and diabetes remission rate.

METHODS

382 patients, aged 25-70 years, were enrolled from nine centres in China between September, 2004, and October, 2006. The patients, with fasting plasma glucose of 7.0-16.7 mmol/L, were randomly assigned to therapy with insulin (CSII or MDI) or oral hypoglycaemic agents for initial rapid correction of hyperglycaemia. Treatment was stopped after normoglycaemia was maintained for 2 weeks. Patients were then followed-up on diet and exercise alone. Intravenous glucose tolerance tests were done and blood glucose, insulin, and proinsulin were measured before and after therapy withdrawal and at 1-year follow-up. Primary endpoint was time of glycaemic remission and remission rate at 1 year after short-term intensive therapy. Analysis was per protocol. This study was registered with ClinicalTrials.gov, number NCT00147836.

FINDINGS

More patients achieved target glycaemic control in the insulin groups (97.1% [133 of 137] in CSII and 95.2% [118 of 124] in MDI) in less time (4.0 days [SD 2.5] in CSII and 5.6 days [SD 3.8] in MDI) than those treated with oral hypoglycaemic agents (83.5% [101 of 121] and 9.3 days [SD 5.3]). Remission rates after 1 year were significantly higher in the insulin groups (51.1% in CSII and 44.9% in MDI) than in the oral hypoglycaemic agents group (26.7%; p=0.0012). beta-cell function represented by HOMA B and acute insulin response improved significantly after intensive interventions. The increase in acute insulin response was sustained in the insulin groups but significantly declined in the oral hypoglycaemic agents group at 1 year in all patients in the remission group.

INTERPRETATION

Early intensive insulin therapy in patients with newly diagnosed type 2 diabetes has favourable outcomes on recovery and maintenance of beta-cell function and protracted glycaemic remission compared with treatment with oral hypoglycaemic agents.

摘要

背景

新诊断的2型糖尿病患者早期强化胰岛素治疗可能改善β细胞功能，并导致血糖缓解期延长。我们进行了一项多中心随机试验，比较短期强化胰岛素治疗（持续皮下胰岛素输注[CSII]或多次皮下注射胰岛素[MDI]）与口服降糖药对β细胞功能和糖尿病缓解率的影响。

方法

2004年9月至2006年10月期间，从中国9个中心招募了382例年龄在25 - 70岁之间的患者。这些患者空腹血糖为7.0 - 16.7 mmol/L，被随机分配接受胰岛素治疗（CSII或MDI）或口服降糖药，以初始快速纠正高血糖。在血糖正常维持2周后停止治疗。然后患者仅通过饮食和运动进行随访。进行静脉葡萄糖耐量试验，并在停止治疗后及1年随访时测量血糖、胰岛素和胰岛素原。主要终点是短期强化治疗后1年的血糖缓解时间和缓解率。按方案进行分析。本研究已在ClinicalTrials.gov注册，注册号为NCT00147836。

结果

与口服降糖药治疗的患者相比，胰岛素组更多患者在更短时间内实现了血糖目标控制（CSII组为97.1%[137例中的133例]，MDI组为95.2%[124例中的118例]）（CSII组为4.0天[标准差2.5]，MDI组为5.6天[标准差3.8]），而口服降糖药组为83.5%[121例中的101例]，时间为9.3天[标准差5.3]）。1年后胰岛素组的缓解率显著高于口服降糖药组（CSII组为51.1%，MDI组为44.9%），口服降糖药组为26.7%；p = 0.0012）。强化干预后，以HOMA B和急性胰岛素反应表示的β细胞功能显著改善。缓解组所有患者中，1年时胰岛素组急性胰岛素反应的增加持续存在，而口服降糖药组则显著下降。