2 型糖尿病的自身免疫:当唯一有效的疗法变成免疫抑制疗法时。

Maria Laura Leo, Pietro Locantore, Caterina Policola, Alessio Michetti, Andrea Corsello, Lorenzo Lucaccini Paoli, Dario Pitocco, Alfredo Pontecorvi
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摘要

背景:B型胰岛素抵抗综合征是一种罕见的糖尿病,由于存在抗胰岛素受体抗体[1, 2],导致血糖失代偿和抗糖尿病治疗失败,而对免疫抑制治疗有反应:一名 67 岁的患者因自身免疫性溶血性贫血和血糖失调入院。我们先给他使用皮下基础胰岛素,然后又静脉注射胰岛素,但血糖水平(300 至 500 毫克/分升)没有改善。考虑到患者对治疗无反应和自身免疫性疾病(溶血性贫血和混合性结缔组织病),我们怀疑血糖失代偿的自身免疫发病机制;我们排除了 1 型糖尿病(特异性抗体阴性),并考虑了抗胰岛素抗体(已检测,阴性)和抗胰岛素受体抗体(由于该地区没有专门检测该抗体的中心,因此没有检测)。因此,我们决定开始使用利妥昔单抗。输注 2 周后,患者的血糖补偿得到改善,胰岛素需求量减少。此外,在首次输注 2 个月后,患者停用了胰岛素,恢复了二甲双胍的口服治疗。迄今为止,患者已完成了 3 个周期的利妥昔单抗治疗,血糖得到了控制(HbA1c 6.7%):结论:患者对利妥昔单抗的良好反应支持了自身免疫发病机制的假设。抗胰岛素受体抗体(B 型胰岛素抵抗综合征)主要影响中年人,尤其是女性,同时还伴有其他自身免疫性疾病。因此,有必要考虑诊断这种罕见疾病,以便进行及时有效的治疗。
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Autoimmunity in Type 2 Diabetes: When the Only Effective Therapy Becomes Immunosuppressive.

Background: Type B insulin resistance syndrome is a rare form of diabetes due to the presence of anti-insulin receptor antibodies [1, 2], which causes glycemic decompensation and antidiabetic therapy failure and instead responds to immunosuppressive therapy.

Case report: A 67-year-old patient was admitted to the hospital due to autoimmune hemolytic anemia and glycemic decompensation. We first prescribed subcutaneous basal-bolus insulin and then intravenous insulin without improvement in blood sugar levels (between 300 and 500 mg/dL). Considering the non-response to therapy and the autoimmune diathesis of the patient (hemolytic anemia and mixed connective tissue disease), we suspected an autoimmune etiopathogenesis of glycemic decompensation; we excluded type 1 diabetes mellitus (specific antibodies were negative), and we considered the anti-insulin-antibodies-(-assayed and negative) and anti-insulin receptor antibodies (not assayed due to the lack of a center specialized in this assay in the area). Therefore, we decided to start Rituximab. After 2 weeks from the infusion, the patient improved glycemic compensation, reducing insulin requirement. Further, 2 months after the first infusion, the patient stopped insulin, returning to oral therapy with Metformin. To date, the patient has completed 3 cycles of Rituximab with the benefit of glycemic control (HbA1c 6.7%).

Conclusion: The brilliant response to Rituximab supports the hypothesis of an autoimmune pathogenesis. The anti-insulin receptor antibodies (in the type B insulin resistance syndrome) affect mostly middle-aged adults, especially women, in the context of other autoimmune diseases. Hence, it is necessary to consider the diagnosis of this rare disease in order to perform timely and effective treatment.

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