De Filippo G, Carel J C, Boitard C, Bougnères P F
U342 Institut National de la Sante et de la Recherche Medicale (INSERM), Saint Vincent de Paul Hospital, René Descartes University, Paris, France.
Diabetes. 1996 Jan;45(1):101-4. doi: 10.2337/diab.45.1.101.
In juvenile IDDM patients, immunosuppression with cyclosporin A allows partial beta-cell function recovery and transient remissions of insulin dependency. The effects of this therapeutic approach, however, have not been evaluated in the long-term, since no reported trial exceeded 1 year. Here we analyze 130 diabetic children followed at our institution during the first years of their disease. Cyclosporin was given to 83 of them at an initial dose of 7.2 +/- 0.1 mg.kg-1.day-1, which was decreased stepwise then interrupted after 6-62 months, depending on the response to therapy. A total of 47 diabetic children, who served as control subjects in two trials, were pooled for comparison. Over 4 years, the cyclosporin-treated group kept plasma C-peptide approximately twice as high as the control group (P < 0.02). It took 5.8 +/- 0.6 years for C-peptide secretion stimulated by glucagon to become undetectable in the cyclosporin group versus 3.2 +/- 0.6 years in the control group (P < 0.02). Average insulin dose remained lower by 0.2-0.4 U.kg-1.day-1 and glycated hemoglobin by approximately 1% in cyclosporin-treated patients (P < 0.02), who also had less hypoglycemia than the diabetic control subjects (P < 0.05). After 4 years, differences between the groups became nonsignificant. We observed no significant secondary effects of cyclosporin. In conclusion, positive effects of low-dose cyclosporin in recently diagnosed clinical IDDM patients are prolonged beyond interruption of the drug. The magnitude and duration of the benefit, however, do not appear sufficient to justify this immunosuppressive treatment in clinical practice.
在青少年型胰岛素依赖型糖尿病(IDDM)患者中,使用环孢素A进行免疫抑制可使部分β细胞功能恢复,并使胰岛素依赖出现短暂缓解。然而,这种治疗方法的长期效果尚未得到评估,因为尚无报道的试验超过1年。在此,我们分析了在我院随访的130名患病初期的糖尿病儿童。其中83名儿童接受环孢素治疗,初始剂量为7.2±0.1mg·kg⁻¹·d⁻¹,随后根据治疗反应逐步减量,并在6至62个月后停药。在两项试验中作为对照的47名糖尿病儿童被合并用于比较。4年多来,环孢素治疗组的血浆C肽水平约为对照组的两倍(P<0.02)。在环孢素组,胰高血糖素刺激的C肽分泌在5.8±0.6年后变得无法检测,而对照组为3.2±0.6年(P<0.02)。环孢素治疗的患者平均胰岛素剂量每天每千克体重低0.2 - 0.4单位,糖化血红蛋白低约1%(P<0.02),且低血糖情况也比糖尿病对照组少(P<0.05)。4年后,两组之间的差异变得不显著。我们未观察到环孢素的明显副作用。总之,低剂量环孢素对近期诊断的临床IDDM患者的积极作用在停药后仍会持续。然而,这种益处的程度和持续时间似乎不足以证明在临床实践中采用这种免疫抑制治疗是合理的。
