5-羟色胺受体拮抗剂相关糖尿病酮症与酮症倾向2型糖尿病之间的共同致病特征:一例报告
Shared Pathogenic Features Between Serotonin Receptor Antagonist-Associated Diabetic Ketosis and Ketosis-Prone Type 2 Diabetes: A Case Report.
作者信息
Nakanishi Shumpei, Sato Haruhiko, Oikawa Yoichi, Ikebukuro Kaori, Shimada Akira
机构信息
Department of Endocrinology and Diabetes, Saitama Medical University, Saitama, JPN.
Department of Internal Medicine, Tsurugashima Medical Clinic, Saitama, JPN.
出版信息
Cureus. 2025 Apr 23;17(4):e82833. doi: 10.7759/cureus.82833. eCollection 2025 Apr.
Ketosis-prone type 2 diabetes (KPD) is characterized by male predominance, onset at a young age, obesity, and sudden onset of diabetic ketosis/ketoacidosis without precipitating factors, negative anti-islet autoantibodies, and β-cell function preservation after recovery from diabetic ketosis/ketoacidosis following temporal insulin therapy. However, its pathogenesis remains unknown. We encountered a 49-year-old obese man presenting with diabetic ketosis, i.e., ketonuria, plasma glucose 252 mg/dL, HbA1c 12.8%, without anti-islet autoantibodies, induced by dose escalation of quetiapine, a serotonin receptor antagonist. After discontinuing quetiapine and starting subcutaneous intensive insulin therapy, diabetic ketosis rapidly resolved. Following glycemic state stabilization, insulin therapy was discontinued on the 11 day of the initiation of therapy. Instead, metformin and linagliptin were initiated, and his glycemic status remained well controlled thereafter. His clinical course closely resembled that of KPD, together with our literature review, suggesting the involvement of decreased serotonin production/action in the pathogenesis of KPD.
酮症倾向2型糖尿病(KPD)的特征为男性居多、发病年龄较轻、肥胖,且在无诱发因素的情况下突然发生糖尿病性酮症/酮症酸中毒、抗胰岛自身抗体阴性,以及在接受短期胰岛素治疗后从糖尿病性酮症/酮症酸中毒恢复后β细胞功能得以保留。然而,其发病机制仍不明。我们遇到一名49岁肥胖男性,出现糖尿病性酮症,即酮尿、血糖252mg/dL、糖化血红蛋白12.8%,无抗胰岛自身抗体,由5-羟色胺受体拮抗剂喹硫平剂量增加诱发。停用喹硫平并开始皮下强化胰岛素治疗后,糖尿病性酮症迅速缓解。血糖状态稳定后,在治疗开始的第11天停用胰岛素治疗。取而代之的是,开始使用二甲双胍和利格列汀,此后其血糖状态保持良好控制。他的临床病程与KPD极为相似,结合我们的文献综述,提示5-羟色胺生成/作用减少参与了KPD的发病机制。
Zotero 插件