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亚洲青少年起病糖尿病的分类和管理面临的挑战-单中心研究的经验教训。

Challenges in the classification and management of Asian youth-onset diabetes mellitus- lessons learned from a single centre study.

机构信息

Department of Medicine, Penang Medical College, Penang, Malaysia.

Department of Medicine, Division of Endocrinology, Penang General Hospital, Penang, Malaysia.

出版信息

PLoS One. 2019 Jan 25;14(1):e0211210. doi: 10.1371/journal.pone.0211210. eCollection 2019.

Abstract

It remains widely perceived that early-onset Type 2 Diabetes (T2D) in children and adolescents is rare and clinically distinct from Type 1 Diabetes (T1D). We studied the challenges of classifying subtypes of early-onset diabetes using clinical features and biomarkers, and management of these patients. We reviewed retrospectively the record of patients < 25 years old who attended the diabetes clinic in Penang General Hospital, Malaysia between 1st December 2012 and 30th June 2015. We examined their clinical features, C-peptide and pancreatic autoantibodies. Comparisons were made between T1D and T2D for magnitude, demographics, metabolic status and complications. We studied 176 patients with a mean age of 20 ± 3.7 years, 43.2% had T1D, 13.6% had T2D, and 13.6% had mixed features of both. When tested, pancreatic autoantibodies were positive in 59.4% of the T1D. T2D presented two years later than T1D at 14.3 years, 20% were asymptomatic at presentation, and 50% required insulin supplementation despite fasting c-peptide of > 250 pmol/L. HbA1C of ≤ 8.0% (64 mmol/mol) was achieved in 30.3% of T1D, 58.3% of T2D on OAD and 16.7% of T2D on insulin. The T2D had greater cardiovascular risk with higher body mass index, more dyslipidaemia, higher blood pressure and earlier onset of nephropathy. The overlapping clinical features, variable autoimmunity, and beta-cell loss complicate classification of young diabetes. Pancreatic autoantibodies and C-peptide did not always predict diabetes subtypes nor respond to insulin. The poor metabolic control and high cardiovascular risk burden among the T2D highlight the need for population-based study and focused intervention.

摘要

人们普遍认为,儿童和青少年的 2 型糖尿病(T2D)发病较早且与 1 型糖尿病(T1D)在临床上有明显区别。我们研究了使用临床特征和生物标志物对早期发病的糖尿病亚型进行分类的挑战,以及这些患者的管理。我们回顾性分析了 2012 年 12 月 1 日至 2015 年 6 月 30 日期间在马来西亚槟城总医院糖尿病门诊就诊的年龄<25 岁的患者的记录。我们检查了他们的临床特征、C 肽和胰腺自身抗体。对 T1D 和 T2D 的数量、人口统计学、代谢状态和并发症进行了比较。我们研究了 176 名平均年龄为 20 ± 3.7 岁的患者,其中 43.2%患有 T1D,13.6%患有 T2D,13.6%为两者的混合特征。在检测时,59.4%的 T1D 患者胰腺自身抗体呈阳性。T2D 的发病时间比 T1D 晚两年,为 14.3 岁,20%的患者在发病时无症状,50%的患者尽管空腹 C 肽>250pmol/L,仍需要胰岛素补充。30.3%的 T1D、58.3%的 T2D 在 OAD 治疗下和 16.7%的 T2D 在胰岛素治疗下实现了≤8.0%(64mmol/mol)的 HbA1C。T2D 患者的体重指数更高、血脂异常更严重、血压更高、肾病发病更早,心血管风险更高。重叠的临床特征、可变的自身免疫和β细胞缺失使年轻糖尿病的分类变得复杂。胰腺自身抗体和 C 肽并不总是能预测糖尿病的亚型,也不能预测对胰岛素的反应。T2D 的代谢控制不佳和心血管风险负担高,突出了需要进行基于人群的研究和有针对性的干预。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1e39/6347175/dc9951162d98/pone.0211210.g001.jpg

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