Diabetic Retinopathy and Cardiovascular Disease. Группа авторов

Diabetic Retinopathy and Cardiovascular Disease - Группа авторов


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particular risk factors are similar in most Western and Asian populations (there are limited data for African or Latin American cohorts) [33]. However, rates of cardiovascular disease vary considerably in different populations and geographical regions for numerous reasons. Disease rates also vary significantly over time within 1 location. Therefore, average absolute risk of cardiovascular events varies and this variability needs to be factored into risk scores. Rather than continually re-creating risk scores in each population and periodically over time, models can be recalibrated as long as population-specific data is available to determine contemporary mean risk factor levels and rates of cardiovascular disease.

      Statistical assessment of risk scores involves 2 key factors: discrimination and calibration. Discrimination is the ability of the tool to identify those who will develop the disease and those who will not. This is commonly measured using the area under the curve (AUC) on a receiver operating characteristic curve, which incorporates both sensitivity and specificity. A similar measure is the concordance statistic or “c-statistic” [32]. Values range from 0.5, indicating no discrimination, to 1.0, indicating perfect discrimination. Calibration describes the correlation between risk predicted by the tool and the observed event rate in the population. There are a few methods for assessing calibration, including the Hosmer-Lemeshow test, which compares mean predicted risk to observed outcome rates across deciles of the distribution of expected risks [32].

      Model Impact Studies

      Risk Scores in Diabetes Guidelines

      There is controversy about the use of risk scores in patients with diabetes given the cardiovascular risk inferred by diabetes itself. There is also concern that scores developed in general populations may not include diabetes-specific risk factors such as duration of disease and microalbuminuria. Thus, various guidelines have differences in their recommendations relating to the use of risk scores.


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