Urinary C-Peptide Creatinine Ratio Is a Practical Outpatient Tool for Identifying Hepatocyte Nuclear Factor 1-α/Hepatocyte Nuclear Factor 4-α Maturity-Onset Diabetes of the Young From Long-Duration Type 1 Diabetes

被引:90
作者
Besser, Rachel E. J. [1 ]
Shepherd, Maggie H. [1 ]
McDonald, Timothy J. [1 ,2 ]
Shields, Beverley M. [1 ]
Knight, Bridget A. [1 ]
Ellard, Sian [1 ,3 ]
Hattersley, Andrew T. [1 ]
机构
[1] Univ Exeter, Peninsula Med Sch, Peninsula Natl Inst Hlth Res Clin Res Facil, Exeter, Devon, England
[2] Royal Devon & Exeter Natl Hlth Serv Fdn Trust, Dept Clin Biochem, Exeter, Devon, England
[3] Royal Devon & Exeter Natl Hlth Serv Fdn Trust, Dept Mol Genet, Exeter, Devon, England
来源
DIABETES CARE | 2011年 / 34卷 / 02期
基金
美国国家卫生研究院;
关键词
INSULIN SECRETORY RESPONSES; BETA-CELL FUNCTION; MUTATIONS; GENE; MODY3; FACTOR-1-ALPHA; DIAGNOSIS; GLUCOSE; CHILDREN;
D O I
10.2337/dc10-1293
中图分类号
R5 [内科学];
学科分类号
1002 ; 100201 ;
摘要
OBJECTIVE-Hepatocyte nuclear factor 1-alpha (HNF1A)/hepatocyte nuclear factor 4-alpha (HNF4A) maturity-onset diabetes of the young (MODY) is frequently misdiagnosed as type 1 diabetes, and patients are inappropriately treated with insulin. Blood C-peptide can aid in the diagnosis of MODY, but practical reasons limit its widespread use. Urinary C-peptide creatinine ratio (UCPCR), a stable measure of endogenous insulin secretion, is a noninvasive alternative. We aimed to compare stimulated UCPCR in adults with HNF1A/4A MODY, type 1 diabetes, and type 2 diabetes. RESEARCH DESIGN AND METHODS-Adults with diabetes for >= 5years, without renal impairment, were studied (HNF1A MODY [n = 54], HNF4A MODY [n = 23], glucokinase MODY [n = 20], type 1 diabetes [n = 69], and type 2 diabetes [n = 54]). The UCPCR was collected in boric acid 120 min after the largest meal of the day and mailed for analysis. Receiver operating characteristic (ROC) curves were used to identify optimal UCPCR cutoffs to differentiate HNF1A/4A MODY from type 1 and type 2 diabetes. RESULTS-UCPCR was lower in type 1 diabetes than HNF1A/4A MODY (median [interquartile range]) (<0.02 nmol/mmol [<0.02 to <0.02] vs. 1.72 nmol/mmol [0.98-2.90]; P < 0.0001). ROC curves showed excellent discrimination (area under curve [AUC] 0.98) and identified a cutoff UCPCR of >= 0.2 nmol/mmol for differentiating HNF1A/4A MODY from type 1 diabetes (97% sensitivity, 96% specificity). UCPCR was lower in HNF1A/4A MODY than in type 2 diabetes (1.72 nmol/mmol [0.98-2.90] vs. 2.47 nmol/mmol [1.4-4.13]); P = 0.007). ROC curves showed a weak distinction between HNF1A/4A MODY and type 2 diabetes (AUC 0.64). CONCLUSIONS-UCPCR is a noninvasive outpatient tool that can be used to discriminate HNF1A and HNF4A MODY from long-duration type 1 diabetes. To differentiate MODY from type 1 diabetes of >5 years' duration, UCPCR could be used to determine whether genetic testing is indicated.
引用
收藏
页码:286 / 291
页数:6
相关论文
共 25 条
[11]   Can complement factors 5 and 8 and transthyretin be used as biomarkers for MODY 1 (HNF4A-MODY) and MODY 3 (HNF1A-MODY)? [J].
Karlsson, E. ;
Shaat, N. ;
Groop, L. .
DIABETIC MEDICINE, 2008, 25 (07) :788-791
[12]   Identifying hepatic nuclear factor 1α mutations in children and young adults with a clinical diagnosis of type 1 diabetes [J].
Lambert, AP ;
Ellard, S ;
Allen, LIS ;
Gallen, IW ;
Gillespie, KM ;
Bingley, PJ ;
Hattersley, AT .
DIABETES CARE, 2003, 26 (02) :333-337
[13]   Stability and Reproducibility of a Single-Sample Urinary C-Peptide/Creatinine Ratio and Its Correlation with 24-h Urinary C-Peptide [J].
McDonald, Tim J. ;
Knight, Bridget A. ;
Shields, Beverley M. ;
Bowman, Pamela ;
Salzmann, Maurice B. ;
Hattersley, Andrew T. .
CLINICAL CHEMISTRY, 2009, 55 (11) :2035-2039
[14]   Mutations in the hepatocyte nuclear factor-1α gene in Caucasian families originally classified as having Type I diabetes [J].
Moller, AM ;
Dalgaard, LT ;
Pociot, F ;
Nerup, J ;
Hansen, T ;
Pedersen, O .
DIABETOLOGIA, 1998, 41 (12) :1528-1531
[15]   Evaluation of Serum 1,5 Anhydroglucitol Levels as a Clinical Test to Differentiate Subtypes of Diabetes [J].
Pal, Aparna ;
Farmer, Andrew J. ;
Dudley, Christina ;
Selwood, Mary P. ;
Barrow, Beryl A. ;
Klyne, Rhiannon ;
Grew, Jilly P. ;
McCarthy, Mark I. ;
Gloyn, Anna L. ;
Owen, Katharine R. .
DIABETES CARE, 2010, 33 (02) :252-257
[16]   Molecular genetics and phenotypic characteristics of MODY caused by hepatocyte nuclear factor 4α mutations in a large European collection [J].
Pearson, ER ;
Pruhova, S ;
Tack, CJ ;
Johansen, A ;
Castleden, HAJ ;
Lumb, PJ ;
Wierzbicki, AS ;
Clark, PM ;
Lebl, J ;
Pedersen, O ;
Ellard, S ;
Hansen, T ;
Hattersley, AT .
DIABETOLOGIA, 2005, 48 (05) :878-885
[17]   Genetic cause of hyperglycaemia and response to treatment in diabetes [J].
Pearson, ER ;
Starkey, BJ ;
Powell, RJ ;
Gribble, FM ;
Clark, PM ;
Hattersley, AT .
LANCET, 2003, 362 (9392) :1275-1281
[18]   Regulation of apolipoprotein M gene expression by MODY3 gene hepatocyte nuclear factor-1α -: Haploinsufficiency is associated with reduced serum apolipoprotein M levels [J].
Richter, S ;
Shih, DQ ;
Pearson, ER ;
Wolfrum, C ;
Fajans, SS ;
Hattersley, AT ;
Stoffell, M .
DIABETES, 2003, 52 (12) :2989-2995
[19]   Genetic, autoimmune, and clinical characteristics of childhood- and adult-onset type 1 diabetes [J].
Sabbah, E ;
Savola, K ;
Ebeling, T ;
Kulmala, P ;
Vähäsalo, P ;
Ilonen, J ;
Salmela, PI ;
Knip, M .
DIABETES CARE, 2000, 23 (09) :1326-1332
[20]   Phenotypical aspects of maturity-onset diabetes of the young (MODY diabetes) in comparison with Type 2 diabetes mellitus (T2DM) in children and adolescents: experience from a large multicentre database [J].
Schober, E. ;
Rami, B. ;
Grabert, M. ;
Thon, A. ;
Kapellen, Th. ;
Reinehr, Th. ;
Holl, R. W. .
DIABETIC MEDICINE, 2009, 26 (05) :466-473
123