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Centre, University of Leicester, Leicester, United Kingdom \n AstraZeneca, Cambridge, United Kingdom \n Export Date: 22 June 2020 \n CODEN: DOMEF \n Correspondence Address: Ling, S.; Leicester Real World Evidence Unit, Leicester Diabetes Centre, University of LeicesterUnited Kingdom; email: sl617@leicester.ac.uk \n Chemicals/CAS: hemoglobin A1c, 62572-11-6; metformin, 1115-70-4, 657-24-9\nLeicester Real World Evidence Unit, Leicester Diabetes Centre, University of Leicester, Leicester, United Kingdom \n AstraZeneca, Cambridge, United Kingdom \n Cited By :1 \n Export Date: 9 July 2021 \n CODEN: DOMEF \n Correspondence Address: Ling, S.; Leicester Real World Evidence Unit, United Kingdom; email: sl617@leicester.ac.uk \n Chemicals/CAS: hemoglobin A1c, 62572-11-6; metformin, 1115-70-4, 657-24-9", "unhandledTickets" : 0, "deleted" : false, "lastRefresh" : "2023-05-03T19:12:27.977+0000", "lastModified" : "2022-01-04T11:13:37.929+0000", "created" : "2020-06-15T06:58:10.558+0000", "creator" : 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Materials and Methods DISCOVER is a 3-year, prospective observational study across six continents investigating second-line glucose-lowering therapies. In this analysis from 35 countries, we included patients on metformin initiating second-line glucose-lowering medication(s) because of physician-defined lack of efficacy. The outcome was durability of glycaemic control, defined as three consecutive levels of HbA1c at 6-, 12- and 24-month follow-up at target (HbA1c equal to or lower than the level when the physician initiated the second-line therapy in patients with baseline HbA1c <= 7% [53 mmol/mol]; and equal to or lower than 7% in those with baseline HbA1c >7%). We developed and internally validated two prognostic models: a base model, which included age, sex, ethnicity, country income group, baseline HbA1c and second-line therapy, and an advanced model, established through statistical variable selections from a model including base variables and 13 additional predictors selected from a literature review. We used logistic regression to develop and 500 bootstrapping samples to internally validate the models; discrimination and calibration were used to assess model performance. Results Overall, 896 out of 2995 participants (29.9%) had sustained glycaemic control. The base model performed well: Nagelkerke R-2 was 0.13, C-index 0.70 (95% CI: 0.68, 0.71) and bias-corrected C-index 0.69 after internal validation. Diabetes duration, insurance type, estimated glomerular filtration rate and glucose self-monitoring were additionally selected in the advanced model, which had only a slightly better performance compared with the base model: Nagelkerke R-2 0.20, C-index 0.71 (95% CI: 0.69, 0.73) and bias-corrected C-index 0.70. Calibration plots showed good calibrations of both validated models. Conclusion These prognostic models, which include simple demographic and routinely collected clinical information, enabled the estimation of the probability of 2-year sustained glycaemic control in patients after metformin failure. 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