Oram Richard A, McDonald Timothy J, Shields Beverley M, Hudson Michelle M, Shepherd Maggie H, Hammersley Suzanne, Pearson Ewan R, Hattersley Andrew T
National Institute for Health Research, Exeter Clinical Research Facility, University of Exeter Medical School, Exeter, U.K.
National Institute for Health Research, Exeter Clinical Research Facility, University of Exeter Medical School, Exeter, U.K. Department of Blood Sciences, Royal Devon and Exeter NHS Foundation Trust, Exeter, U.K.
Diabetes Care. 2015 Feb;38(2):323-8. doi: 10.2337/dc14-0871. Epub 2014 Dec 17.
Small studies using ultrasensitive C-peptide assays suggest endogenous insulin secretion is frequently detectable in patients with long-standing type 1 diabetes (T1D), but these studies do not use representative samples. We aimed to use the stimulated urine C-peptide-to-creatinine ratio (UCPCR) to assess C-peptide levels in a large cross-sectional, population-based study of patients with T1D.
We recruited 924 patients from primary and secondary care in two U.K. centers who had a clinical diagnosis of T1D, were under 30 years of age when they received a diagnosis, and had a diabetes duration of >5 years. The median age at diagnosis was 11 years (interquartile range 6-17 years), and the duration of diabetes was 19 years (11-27 years). All provided a home postmeal UCPCR, which was measured using a Roche electrochemiluminescence assay.
Eighty percent of patients (740 of 924 patients) had detectable endogenous C-peptide levels (UCPCR >0.001 nmol/mmol). Most patients (52%, 483 of 924 patients) had historically very low undetectable levels (UCPCR 0.0013-0.03 nmol/mmol); 8% of patients (70 of 924 patients) had a UCPCR ≥0.2 nmol/mmol, equivalent to serum levels associated with reduced complications and hypoglycemia. Absolute UCPCR levels fell with duration of disease. Age at diagnosis and duration of disease were independent predictors of C-peptide level in multivariate modeling.
This population-based study shows that the majority of long-duration T1D patients have detectable urine C-peptide levels. While the majority of patients are insulin microsecretors, some maintain clinically relevant endogenous insulin secretion for many years after the diagnosis of diabetes. Understanding this may lead to a better understanding of pathogenesis in T1D and open new possibilities for treatment.
使用超灵敏C肽检测法的小型研究表明,在长期1型糖尿病(T1D)患者中,内源性胰岛素分泌常常可被检测到,但这些研究未使用具有代表性的样本。我们旨在通过刺激后的尿C肽与肌酐比值(UCPCR),在一项针对T1D患者的大型横断面、基于人群的研究中评估C肽水平。
我们从英国两个中心的初级和二级医疗机构招募了924例临床诊断为T1D的患者,这些患者在确诊时年龄小于30岁,糖尿病病程超过5年。确诊时的中位年龄为11岁(四分位间距6 - 17岁),糖尿病病程为19年(11 - 27年)。所有人都提供了一份在家餐后的UCPCR样本,该样本使用罗氏电化学发光分析法进行检测。
80%的患者(924例患者中的740例)内源性C肽水平可被检测到(UCPCR>0.001 nmol/mmol)。大多数患者(52%,924例患者中的483例)既往的水平极低,无法检测到(UCPCR为0.0013 - 0.03 nmol/mmol);8%的患者(924例患者中的70例)UCPCR≥0.2 nmol/mmol,这相当于与并发症减少和低血糖相关的血清水平。UCPCR的绝对水平随疾病病程而下降。在多变量模型中,确诊时的年龄和疾病病程是C肽水平的独立预测因素。
这项基于人群的研究表明,大多数病程较长的T1D患者尿C肽水平可被检测到。虽然大多数患者是胰岛素微量分泌者,但一些患者在糖尿病诊断后的许多年里仍维持着与临床相关的内源性胰岛素分泌。了解这一点可能有助于更好地理解T1D的发病机制,并为治疗开辟新的可能性。
