TY - JOUR
T1 - Performance of prediction models for nephropathy in people with type 2 diabetes
T2 - Systematic review and external validation study
AU - Slieker, Roderick C.
AU - van der Heijden, Amber A. W. A.
AU - Siddiqui, Moneeza K.
AU - Langendoen-Gort, Marlous
AU - Nijpels, Giel
AU - Herings, Ron
AU - Feenstra, Talitha L.
AU - Moons, Karel G. M.
AU - Bell, Samira
AU - Elders, Petra J.
AU - THart, Leen M.
AU - Beulens, Joline W. J.
N1 - Funding Information: Funding: This research was supported by the Dutch Diabetes Research Foundation (grant No 2014.00.1753). The funder had no role in the study design; collection, analysis, and interpretation of data; or preparation of the manuscript. GoDARTS is funded and supported by the Wellcome Trust Type 2 Diabetes Case Control Collection (072960/Z/03/Z, 084726/Z/08/Z, 084727/Z/08/Z, Funding Information: This research was supported by the Dutch Diabetes Research Foundation (grant No 2014.00.1753). The funder had no role in the study design; collection, analysis, and interpretation of data; or preparation of the manuscript. GoDARTS is funded and supported by the Wellcome Trust Type 2 Diabetes Case Control Collection (072960/Z/03/Z, 084726/Z/08/Z, 084727/Z/08/Z, 085475/Z/ 08/Z, 085475/B/08/Z) and as part of the EU IMISUMMIT programme. Publisher Copyright: © Author(s) (or their employer(s)) 2019. Copyright: Copyright 2021 Elsevier B.V., All rights reserved.
PY - 2021/9/28
Y1 - 2021/9/28
N2 - Objectives To identify and assess the quality and accuracy of prognostic models for nephropathy and to validate these models in external cohorts of people with type 2 diabetes. Design Systematic review and external validation. Data sources PubMed and Embase. Eligibility criteria Studies describing the development of a model to predict the risk of nephropathy, applicable to people with type 2 diabetes. Methods Screening, data extraction, and risk of bias assessment were done in duplicate. Eligible models were externally validated in the Hoorn Diabetes Care System (DCS) cohort (n=11 450) for the same outcomes for which they were developed. Risks of nephropathy were calculated and compared with observed risk over 2, 5, and 10 years of follow-up. Model performance was assessed based on intercept adjusted calibration and discrimination (Harrell's C statistic). Results 41 studies included in the systematic review reported 64 models, 46 of which were developed in a population with diabetes and 18 in the general population including diabetes as a predictor. The predicted outcomes included albuminuria, diabetic kidney disease, chronic kidney disease (general population), and end stage renal disease. The reported apparent discrimination of the 46 models varied considerably across the different predicted outcomes, from 0.60 (95% confidence interval 0.56 to 0.64) to 0.99 (not available) for the models developed in a diabetes population and from 0.59 (not available) to 0.96 (0.95 to 0.97) for the models developed in the general population. Calibration was reported in 31 of the 41 studies, and the models were generally well calibrated. 21 of the 64 retrieved models were externally validated in the Hoorn DCS cohort for predicting risk of albuminuria, diabetic kidney disease, and chronic kidney disease, with considerable variation in performance across prediction horizons and models. For all three outcomes, however, at least two models had C statistics >0.8, indicating excellent discrimination. In a secondary external validation in GoDARTS (Genetics of Diabetes Audit and Research in Tayside Scotland), models developed for diabetic kidney disease outperformed those for chronic kidney disease. Models were generally well calibrated across all three prediction horizons. Conclusions This study identified multiple prediction models to predict albuminuria, diabetic kidney disease, chronic kidney disease, and end stage renal disease. In the external validation, discrimination and calibration for albuminuria, diabetic kidney disease, and chronic kidney disease varied considerably across prediction horizons and models. For each outcome, however, specific models showed good discrimination and calibration across the three prediction horizons, with clinically accessible predictors, making them applicable in a clinical setting.
AB - Objectives To identify and assess the quality and accuracy of prognostic models for nephropathy and to validate these models in external cohorts of people with type 2 diabetes. Design Systematic review and external validation. Data sources PubMed and Embase. Eligibility criteria Studies describing the development of a model to predict the risk of nephropathy, applicable to people with type 2 diabetes. Methods Screening, data extraction, and risk of bias assessment were done in duplicate. Eligible models were externally validated in the Hoorn Diabetes Care System (DCS) cohort (n=11 450) for the same outcomes for which they were developed. Risks of nephropathy were calculated and compared with observed risk over 2, 5, and 10 years of follow-up. Model performance was assessed based on intercept adjusted calibration and discrimination (Harrell's C statistic). Results 41 studies included in the systematic review reported 64 models, 46 of which were developed in a population with diabetes and 18 in the general population including diabetes as a predictor. The predicted outcomes included albuminuria, diabetic kidney disease, chronic kidney disease (general population), and end stage renal disease. The reported apparent discrimination of the 46 models varied considerably across the different predicted outcomes, from 0.60 (95% confidence interval 0.56 to 0.64) to 0.99 (not available) for the models developed in a diabetes population and from 0.59 (not available) to 0.96 (0.95 to 0.97) for the models developed in the general population. Calibration was reported in 31 of the 41 studies, and the models were generally well calibrated. 21 of the 64 retrieved models were externally validated in the Hoorn DCS cohort for predicting risk of albuminuria, diabetic kidney disease, and chronic kidney disease, with considerable variation in performance across prediction horizons and models. For all three outcomes, however, at least two models had C statistics >0.8, indicating excellent discrimination. In a secondary external validation in GoDARTS (Genetics of Diabetes Audit and Research in Tayside Scotland), models developed for diabetic kidney disease outperformed those for chronic kidney disease. Models were generally well calibrated across all three prediction horizons. Conclusions This study identified multiple prediction models to predict albuminuria, diabetic kidney disease, chronic kidney disease, and end stage renal disease. In the external validation, discrimination and calibration for albuminuria, diabetic kidney disease, and chronic kidney disease varied considerably across prediction horizons and models. For each outcome, however, specific models showed good discrimination and calibration across the three prediction horizons, with clinically accessible predictors, making them applicable in a clinical setting.
UR - http://www.scopus.com/inward/record.url?scp=85116365047&partnerID=8YFLogxK
U2 - https://doi.org/10.1136/bmj.n2134
DO - https://doi.org/10.1136/bmj.n2134
M3 - Review article
C2 - 34583929
SN - 0959-8146
VL - 374
JO - The BMJ
JF - The BMJ
M1 - n2134
ER -