首页> 外文期刊>The Lancet >Nasal insulin to prevent type 1 diabetes in children with HLA genotypes and autoantibodies conferring increased risk of disease: a double-blind, randomised controlled trial.
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Nasal insulin to prevent type 1 diabetes in children with HLA genotypes and autoantibodies conferring increased risk of disease: a double-blind, randomised controlled trial.

机译:鼻胰岛素预防患有HLA基因型和自身抗体的儿童会增加患病风险的1型糖尿病:一项双盲,随机对照试验。

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BACKGROUND: In mouse models of diabetes, prophylactic administration of insulin reduced incidence of the disease. We investigated whether administration of nasal insulin decreased the incidence of type 1 diabetes, in children with HLA genotypes and autoantibodies increasing the risk of the disease. METHODS: At three university hospitals in Turku, Oulu, and Tampere (Finland), we analysed cord blood samples of 116 720 consecutively born infants, and 3430 of their siblings, for the HLA-DQB1 susceptibility alleles for type 1 diabetes. 17 397 infants and 1613 siblings had increased genetic risk, of whom 11 225 and 1574, respectively, consented to screening of diabetes-associated autoantibodies at every 3-12 months. In a double-blind trial, we randomly assigned 224 infants and 40 siblings positive for two or more autoantibodies, in consecutive samples, to receive short-acting human insulin (1 unit/kg; n=115 and n=22) or placebo (n=109 and n=18) once a day intranasally. We used a restricted randomisation, stratified by site, with permuted blocks of size two. Primary endpoint was diagnosis of diabetes. Analysis was by intention to treat. The study was terminated early because insulin had no beneficial effect. This study is registered with ClinicalTrials.gov, number NCT00223613. FINDINGS: Median duration of the intervention was 1.8 years (range 0-9.7). Diabetes was diagnosed in 49 index children randomised to receive insulin, and in 47 randomised to placebo (hazard ratio [HR] 1.14; 95% CI 0.73-1.77). 42 and 38 of these children, respectively, continued treatment until diagnosis, with yearly rates of diabetes onset of 16.8% (95% CI 11.7-21.9) and 15.3% (10.5-20.2). Seven siblings were diagnosed with diabetes in the insulin group, versus six in the placebo group (HR 1.93; 0.56-6.77). In all randomised children, diabetes was diagnosed in 56 in the insulin group, and 53 in the placebo group (HR 0.98; 0.67-1.43, p=0.91). INTERPRETATION: In children with HLA-conferred susceptibility to diabetes, administration of nasal insulin, started soon after detection of autoantibodies, could not be shown to prevent or delay type 1 diabetes.
机译:背景:在糖尿病小鼠模型中,胰岛素的预防性给药降低了疾病的发生率。我们调查了在患有HLA基因型和自身抗体的儿童中,鼻腔胰岛素的施用是否降低了1型糖尿病的发病率,从而增加了患该病的风险。方法:在图尔库,奥卢和坦佩雷(芬兰)的三所大学医院中,我们分析了116 720名连续出生的婴儿及其兄弟姐妹3430的脐带血样本中1型糖尿病的HLA-DQB1易感性等位基因。每3-12个月就有17 397例婴儿和1613兄弟姐妹的遗传风险增加,其中分别有11 225和1574例同意筛查与糖尿病相关的自身抗体。在一项双盲试验中,我们在连续的样本中随机分配了224个婴儿和40个兄弟姐妹,两个或多个自身抗体呈阳性,接受短效人胰岛素(1单位/ kg; n = 115和n = 22)或安慰剂( n = 109,n = 18),每天一次鼻内注射。我们使用了受限的随机化方法,按位置分层,排列大小为2。主要终点是诊断为糖尿病。分析是按意向进行的。由于胰岛素没有有益作用,该研究提前终止。该研究已在ClinicalTrials.gov上注册,编号为NCT00223613。结果:干预的中位时间为1.8年(范围0-9.7)。在随机分配接受胰岛素治疗的49名索引儿童和随机分配接受安慰剂的47名儿童中诊断出糖尿病(危险比[HR] 1.14; 95%CI 0.73-1.77)。这些儿童中分别有42和38名儿童继续接受治疗直至被诊断出患糖尿病的年发病率分别为16.8%(95%CI 11.7-21.9)和15.3%(10.5-20.2)。胰岛素组中有七个兄弟姐妹被诊断出患有糖尿病,而安慰剂组中有六个兄弟姐妹被诊断出患有糖尿病(HR 1.93; 0.56-6.77)。在所有随机分组的儿童中,胰岛素组中56例被诊断为糖尿病,安慰剂组中53例被诊断为糖尿病(HR 0.98; 0.67-1.43,p = 0.91)。解释:在患有HLA的糖尿病易感儿童中,鼻内胰岛素的注射是在发现自身抗体后不久开始的,无法证明可以预防或延迟1型糖尿病。

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