自身免疫性1型糖尿病10年后的残余β细胞功能:患病率、可能的决定因素及其对代谢的影响。
Residual β-cell function after 10 years of autoimmune type 1 diabetes: prevalence, possible determinants, and implications for metabolism.
作者信息
Cheng Jin, Yin Min, Tang Xiaohan, Yan Xiang, Xie Yuting, He Binbin, Li Xia, Zhou Zhiguang
机构信息
National Clinical Research Center for Metabolic Disease, Key Laboratory of Diabetes Immunology, Ministry of Education, Department of Metabolism and Endocrinology, The Second Xiangya Hospital of Central South University, Changsha, China.
出版信息
Ann Transl Med. 2021 Apr;9(8):650. doi: 10.21037/atm-20-7471.
BACKGROUND
Type 1 diabetes (T1D) has long been considered a progressive autoimmune disease resulting in the failure of pancreatic β-cell function and absolute endogenous insulin deficiency. However, several studies have demonstrated patients with T1D have detectable C-peptide levels long after diagnosis, which has remarkable clinical significance. Since this issue has not been systematically explored in non-Caucasian populations, we aimed to identify the prevalence of residual β-cell function and its related clinical features in Chinese long-term T1D patients.
METHODS
We enrolled 109 patients with T1D for ≥10 years and administered a mixed-meal tolerance test (MMTT). Fasting and postprandial C-peptide (FCP/PCP) levels were measured to evaluate the insulin secretion function of β-cells. Patients whose FCP and PCP levels were both below the lower detection limit (16.7 pmol/L) were grouped as 'β-cell function depleted', while others were thought to have 'residual β-cell function'. Demographic data, metabolic status, and diabetic complications were compared between patients with or without residual β-cell function.
RESULTS
38.5% of subjects retained residual β-cell function, and among those, 33.3% responded to MMTT by a two-fold or greater rise of their FCP levels. Clinical features associated with residual β-cell function were older age of diagnosis [27.5 (interquartile range:11.5-37.0) 17.0 (interquartile range: 8.0-30.0) years, P=0.037], lower HbA1c (64.6±20.3 72.4±18.5 mmol/mol, P=0.026), and reduced rate of hypoglycemia (23.8% 52.2%, P=0.003). Age of diagnosis was positively correlated with detectable FCP level (r=0.393, P=0.020). Individuals diagnosed after 30 years of age tended to retain residual β-cell function (OR =3.016, P=0.044). We found no association between residual β-cell function and chronic diabetic complications.
CONCLUSIONS
Residual β-cell function can be found in nearly 40% of long-term patients with T1D in China and is associated with older age at diagnosis and better glucose control. The relationship between residual β-cell function and chronic diabetic complications remains to be explored.
背景
1型糖尿病(T1D)长期以来一直被认为是一种进行性自身免疫性疾病,会导致胰腺β细胞功能衰竭和绝对内源性胰岛素缺乏。然而,多项研究表明,T1D患者在确诊后很长时间内C肽水平仍可检测到,这具有重要的临床意义。由于该问题在非白种人群中尚未得到系统研究,我们旨在确定中国长期T1D患者中残余β细胞功能的患病率及其相关临床特征。
方法
我们纳入了109例病程≥10年的T1D患者,并进行了混合餐耐量试验(MMTT)。测量空腹和餐后C肽(FCP/PCP)水平以评估β细胞的胰岛素分泌功能。FCP和PCP水平均低于检测下限(16.7 pmol/L)的患者被归为“β细胞功能耗竭”组,而其他患者则被认为具有“残余β细胞功能”。比较有无残余β细胞功能患者的人口统计学数据、代谢状态和糖尿病并发症。
结果
38.5%的受试者保留了残余β细胞功能,其中33.3%的受试者对MMTT的反应是FCP水平升高两倍或更多。与残余β细胞功能相关的临床特征包括诊断时年龄较大[27.5(四分位间距:11.5 - 37.0)岁对17.0(四分位间距:8.0 - 30.0)岁,P = 0.037]、HbA1c较低(64.6±20.3对72.4±18.5 mmol/mol,P = 0.026)以及低血糖发生率较低(23.8%对52.2%,P = 0.003)。诊断时年龄与可检测到的FCP水平呈正相关(r = 0.393,P = 0.020)。30岁以后确诊的个体倾向于保留残余β细胞功能(OR = 3.016,P = 0.044)。我们发现残余β细胞功能与慢性糖尿病并发症之间无关联。
结论
在中国,近40%的长期T1D患者存在残余β细胞功能,且与诊断时年龄较大和更好的血糖控制相关。残余β细胞功能与慢性糖尿病并发症之间的关系仍有待探索。
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