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Independence of exogenous insulin following immunoablation and stem cell reconstitution in newly diagnosed diabetes type I.

机译:在新诊断的I型糖尿病中,免疫消融和干细胞重建后外源胰岛素的独立性。

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Type I diabetes mellitus is a metabolic disease caused by chronic immune attack against the insulin-producing cells of the pancreas. It has recently been shown that the clinical course of this disease can be interrupted by immune ablation and PBSCT. In this report, we describe our experience with this treatment modality in a series of eight cases. Patients with newly diagnosed type I diabetes were received treatment consisting of two to three plasmaphereses, hematopoietic stem cell mobilization with CY and G-CSF, collection of at least 3 x 10(6) per kg of CD34+ cells, and conditioning with CY and anti-thymocyte globulin followed by stem cell infusion. All patients became independent of exogenous insulin after the transplantation. One patient resumed low-dose insulin 7 months after transplantation. Six out of eight patients were given acarbose for better glycemic control after transplantation. All patients exhibited good glycemic control: the average HbA1c concentrations were 12.3% at diagnosis, and 5.6 and 6.2% at 3 and 6 months after transplantation, respectively. We conclude that at least temporary independence of exogenous insulin can be achieved in type I diabetes patients following immunoablation and reconstitution of the immune system with autologous PBSCs.
机译:I型糖尿病是由对胰腺的产生胰岛素的细胞的慢性免疫攻击引起的代谢疾病。最近显示,该疾病的临床病程可以通过免疫消融和PBSCT来中断。在本报告中,我们将在一系列八例病例中描述我们在这种治疗方式上的经验。刚诊断为I型糖尿病的患者接受的治疗包括两到三个血浆,CY和G-CSF造血干细胞动员,每公斤CD34 +细胞至少收集3 x 10(6),以及CY和抗-胸腺细胞球蛋白,然后输注干细胞。移植后所有患者均独立于外源胰岛素。一名患者在移植后7个月恢复了低剂量胰岛素治疗。八分之六的患者在移植后接受了阿卡波糖治疗,以更好地控制血糖。所有患者均表现出良好的血糖控制:在诊断后,平均HbA1c浓度分别为12.3%,在移植后3和6个月分别为5.6和6.2%。我们得出的结论是,在I型糖尿病患者通过自体PBSC进行免疫消融和免疫系统重建后,至少可以暂时获得外源性胰岛素的独立性。

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