Long-term TNF-alpha therapy for preserving beta cell function in new onset type 1 diabetes: a case report.

Clinical Diabetes and Endocrinology Pub Date : 2024-09-10 DOI:10.1186/s40842-024-00185-6

Adya Rao, Lauren M Quinn, Parth Narendran

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Abstract

Background: Type 1 diabetes mellitus (T1D) is an autoimmune disease caused by destruction of pancreatic islet beta-cells. There is significant residual beta-cell function, measured through circulating C-peptide, present at the time of T1D diagnosis but this subsequently decreases with time. Higher residual beta-cell function at diagnosis associates with better glycaemic control and less glucose variability, and later in the disease course with less hypoglycaemia, lower glucose variability and fewer microvascular complications. There is therefore value in preserving residual beta cell function in new onset T1D Immunotherapeutic agents can protect residual beta-cell function in type 1 diabetes. However, clinical trials of such agents, whilst demonstrating C-peptide preservation in short term studies, have yet to be taken forward into routine clinical care due to concerns around safety and long-term efficacy. Here we report the case of a gentleman with newly diagnosed T1D whose glycaemic control and insulin requirement improved whilst on a five year infusion programme of infliximab, a monoclonal antibody against TNF-alpha, for colitis.

Case presentation: A 52-year-old White Caucasian man was diagnosed with T1D in August 2018. Glucose was 25.6 mmol/L, HbA1c was 98mmol/mol and GAD antibodies were strongly positive. HbA1c marginally improved to 91mmol/mol following initiation of insulin detemir 5 units at night and 1:10 g of insulin aspart (November 2018). In June 2019, he developed rectal bleeding and abdominal pain. Following colonoscopy, he was diagnosed with "indeterminate colitis" and commenced on 6-weekly infusions of 400-450 mg infliximab. Thus far, he has received 32 doses and achieved colitis remission. Following infliximab initiation there was increased frequency of mild-moderate hypoglycaemia and he was gradually weaned off and discontinued detemir in June 2020. Since then, HbA1c improved from 57mmol/mol in August 2019 to 52mmol/mol in April 2022, remaining stable at 51mmol/mol. His most recent HbA1c is 54mmol/mol in February 2024. His c-peptide was 550pmol/L in October 2022 and 442pmol/L in February 2024, suggesting well-preserved beta-cell function almost 6 years post-diagnosis.

Conclusions: Our patient's improvement in glycaemic control can be explained by immunomodulation and C peptide preservation from infliximab. With the growing focus on type 1 diabetes disease modulation and working towards an 'insulin free T1D', our findings strengthen the evidence base for the repurposing of and long-term treatment with anti-TNF-α agents to preserve beta-cell function in new onset T1D.

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对新发 1 型糖尿病患者进行 TNF-α 长期治疗以保护β细胞功能：一份病例报告。

背景：1 型糖尿病（T1D）是一种由胰岛β细胞破坏引起的自身免疫性疾病。在诊断为 T1D 时，通过循环 C 肽可以测量到大量残留的 beta 细胞功能，但随着时间的推移，这种功能会逐渐减弱。确诊时残留β细胞功能越高，血糖控制越好，血糖变异性越小；病程后期，低血糖发生率越低，血糖变异性越小，微血管并发症越少。因此，在新发 T1D 患者中保护残余的β细胞功能是有价值的免疫治疗药物可以保护 1 型糖尿病患者残余的β细胞功能。然而，此类药物的临床试验虽然在短期研究中显示了 C 肽的保护作用，但由于安全性和长期疗效方面的顾虑，尚未将其推广到常规临床治疗中。在此，我们报告了一例新确诊的 T1D 患者的病例，该患者在输注英夫利昔单抗（一种抗 TNF-α 的单克隆抗体）治疗结肠炎的五年计划期间，血糖控制和胰岛素需求均有所改善：一名 52 岁的白种高加索男子于 2018 年 8 月被诊断为 T1D。血糖为 25.6 mmol/L，HbA1c 为 98mmol/mol，GAD 抗体强阳性。在夜间开始使用 5 单位地特米胰岛素和 1:10 克阿斯巴特胰岛素（2018 年 11 月）后，HbA1c 略微改善至 91mmol/mol。2019 年 6 月，他出现直肠出血和腹痛。结肠镜检查后，他被诊断为 "不确定结肠炎"，并开始接受每周 6 次输注 400-450 毫克英夫利昔单抗的治疗。到目前为止，他已接受了 32 次治疗，结肠炎得到了缓解。开始使用英夫利昔单抗后，轻度-中度低血糖的发生频率增加，他的血糖逐渐下降，并于 2020 年 6 月停用了地特米。此后，HbA1c 从 2019 年 8 月的 57mmol/mol 下降到 2022 年 4 月的 52mmol/mol，并稳定在 51mmol/mol。他最近的 HbA1c 是 2024 年 2 月的 54mmol/mol。他的c肽在2022年10月为550pmol/L，在2024年2月为442pmol/L，这表明他在确诊后近6年的β细胞功能保存完好：结论：英夫利昔单抗的免疫调节作用和C肽保护作用可以解释患者血糖控制的改善。随着人们越来越关注1型糖尿病的疾病调节和 "无胰岛素T1D"，我们的研究结果加强了抗TNF-α药物的再利用和长期治疗的证据基础，以保护新发T1D患者的β细胞功能。

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来源期刊

Clinical Diabetes and Endocrinology

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审稿时长

8 weeks

期刊介绍： Clinical Diabetes and Endocrinology is an open access journal publishing within the field of diabetes and endocrine disease. The journal aims to provide a widely available resource for people working within the field of diabetes and endocrinology, in order to improve the care of people affected by these conditions. The audience includes, but is not limited to, physicians, researchers, nurses, nutritionists, pharmacists, podiatrists, psychologists, epidemiologists, exercise physiologists and health care researchers. Research articles include patient-based research (clinical trials, clinical studies, and others), translational research (translation of basic science to clinical practice, translation of clinical practice to policy and others), as well as epidemiology and health care research. Clinical articles include case reports, case seminars, consensus statements, clinical practice guidelines and evidence-based medicine. Only articles considered to contribute new knowledge to the field will be considered for publication.