REDUCED SAMPLING PROTOCOLS IN ESTIMATION OF INSULIN SENSITIVITY AND GLUCOSE EFFECTIVENESS USING THE MINIMAL MODEL IN NIDDM

被引:27
|
作者
COATES, PA
OLLERTON, RL
LUZIO, SD
ISMAIL, IS
OWENS, DR
机构
[1] UNIV WALES COLL MED,DEPT MED,DIABET RES UNIT,HEATH PK,CARDIFF CF4 4XN,S GLAM,WALES
[2] UNIV WESTERN SYDNEY,FAC SCI & TECHNOL,DEPT MATH,NEPEAN,SYDNEY,AUSTRALIA
关键词
D O I
10.2337/diabetes.42.11.1635
中图分类号
R5 [内科学];
学科分类号
1002 ; 100201 ;
摘要
Recent work in healthy subjects, the aged, and subjects with gestational diabetes or drug-induced insulin resistance using minimal model analysis of the tolbutamide-modified frequently sampled intravenous glucose tolerance test suggested that a reduced sampling regimen of 12 time points produced unbiased and generally acceptable estimates of insulin sensitivity (S(I)) and glucose effectiveness (S(G)) compared with a full sampling schedule of 30 time points. We have used data from 26 insulin-modified frequently sampled intravenous glucose tolerance tests in 21 subjects with NIDDM to derive and compare estimates of S(I) and S(G) from the full sampling schedule (S(I(30)), S(G(30)) with those estimated from the suggested 12 time points (S(I(12)), S(G(12)) and those estimated with the addition of a 25-min time point (S(I(13)), S(G(13))). Percentage relative errors were calculated relative to the corresponding 30 time-point values. A statistically significant bias of 15% (97% confidence interval from 7.4 to 25.6%, interquartile range 25%) was introduced by the estimation of S(I(12)) but not S(I(13)) (1%, 97% confidence interval from -9.4 to 9.3%, interquartile range 21%). Results for S(G(12)) (-12%, 97% confidence interval from -46.7 to 1.2%, interquartile range 49%) and S(G(13)) (-5%, 97% confidence interval from -27.8 to 6.8%, interquartile range 37%) were statistically equivocal. The precision of estimation of S(I(12)), S(G(12)), and S(G(13)) measured by the interquartile range of the percentage relative errors was poor. The precision of determination measured by the median minimal model coefficient of variation was 18, 29, and 27% for S(I(30)), S(I(12)), and S(I(13)) and 9, 11, and 11% for S(G(30)), S(G(12)), and S(G(13)), respectively. Thus, the application of minimal model analysis to the 12 time-point protocol of the insulin-modified IVGTT for the estimation of S(I) and S(G) in NIDDM may necessitate an inordinately large number of subjects. Although the 13 time-point protocol may be more acceptable for the assessment of S(I) in population studies, we recommend retention of the full sampling schedule where feasible.
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页码:1635 / 1641
页数:7
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