Measuring hemoglobin A 1c (HbA 1c ) levels in patients with diabetes is associated with improvement in models for predicting risk for cardiovascular disease (CVD), according to a report published Online First today by Archives of Internal Medicine, one of the JAMA/Archives journals.
According to background information in the article, diabetes has been recognized as a risk factor for CVD. But recent research indicates that the level of risk may vary among patients with diabetes. "Simulated cost-benefit analyses have suggested that this variability in CVD risk could provide an opportunity for tailored preventive therapy in diabetic patients," write the authors. They sought to investigate the predictive value of HbA 1c levels; this test reflects the average blood glucose level over the previous two to three months, and generally indicates how well the diabetes is being managed.
Nina P. Paynter, Ph.D., from Brigham and Women's Hospital, Boston, and colleagues, used data from participants of the Women's Health Study and the Physician's Health Study II. To generate the model, they included data from 24,674 women, of whom 685 had diabetes at baseline, and 11,280 men, of whom 563 had diabetes at baseline. Questionnaires provided participants' health history, and baseline blood samples were evaluated for cholesterol, C-reactive protein and HbA 1c levels. The researchers followed up participants for incident (new cases) CVD; women were followed up for a median (midpoint) of 10.2 years and men for a median of 11.8 years.
During follow-up, 125 cardiovascular events occurred in the 685 women with diabetes and 170 events occurred in the 563 men with diabetes (compared with 666 and 1,382 events, respectively, in participants without diabetes). In both sexes, including HbA 1c into risk modeling for CVD improved prediction of CVD compared to classification of all diabetic participants as high risk (10-year risk at least 20 percent). This association was especially pronounced in women. The risk modeling demonstrated that 71.9 percent of female diabetic participants had less than a 20 percent risk of CVD over 10 years, whereas only 24.5 percent of male diabetic participants had a predicted 10-year CVD risk of less than 20 percent. In models that included a term for HbA 1c , there was substantial improvement in CVD risk prediction for women, and more modest improvement in risk prediction for men. Using a yes/no term for diabetes instead of HbA 1c also improved prediction over classification as high risk in both men and women. In women, however, HbA 1c further improved prediction over the yes/no term.
"We found that in these large population-based cohorts of both men and women, presence of diabetes alone did not confer a 10-year risk of CVD higher than 20 percent, and measurement of HbA 1c level in diabetic subjects improved risk prediction compared with classification as cardiovascular risk equivalent," note the researchers. They propose that the difference in risk between the sexes may be partly attributed to the increase in CVD risk with age and the delayed risk in women. The authors call for further research to replicate their results, but conclude, "Our findings suggest that the improvement in CVD risk prediction, and possibly calibration, obtained with adding HbA 1c levels is highest in lower-risk populations."
(Arch Intern Med. Published July 25, 2011. doi:10.1001/archinternmed.2011.351. Available pre-embargo to the media at www.jamamedia.org.)
Editor's Note: This work was carried out with support from F. Hoffmann-La Roche Ltd; and grants from the National Heart Lung and Blood Institute, the National Cancer Institute and the Donald W. Reynolds Foundation, Las Vegas. Please see the article for additional information, including other authors, author contributions and affiliations, financial disclosures, funding and support, etc.
Commentary: Cardiovascular Risk Stratification, Hemoglobin A 1c , and the Tempo of Translation
An accompanying commentary by Mark J. Pletcher, M.D., M.P.H., from the University of California, San Francisco, notes that the Adult Treatment Panel III (ATP III) guidelines and other cardiovascular disease (CVD) prevention guidelines will be updated soon.
"One specific guideline refinement up for consideration this year is the approach to CVD risk stratification in patients with diabetes," writes Pletcher. He states that under current ATP III guidelines, diabetes is considered a "CHD [coronary heart disease] risk equivalent." Patients with diabetes may be subject to relatively aggressive goals for lowering cholesterol levels, as well as treatment thresholds.
The article by Paynter and colleagues, which includes the HbA 1c level as well as other standard risk factors, appears to improve discrimination and may lead to "more accurate classification of individuals into risk categories," writes Pletcher. The results would be stronger, he adds, if the research had included more patients with diabetes, especially those whose condition was not well controlled; if it had not included revascularizations and strokes, as these were not considered when the current ATP III CHD risk-prediction equation was developed and calibrated; and if the model had included a diabetes indicator variable as well as the HbA 1c measurement.
Pletcher points out that reclassifying some patients with diabetes to lower risk levels would disqualify them from statin therapy to reduce cholesterol levels, and considers whether this is beneficial. "It is not enough to know whether discrimination or reclassification improves with the additional measurement; harm from the new measurement/strategy (both direct and indirect) must be considered and weighed against a realistic estimate of the expected health benefits," he writes.
(Arch Intern Med. Published July 25, 2011. doi:10.1001/archinternmed.2011.352. Available pre-embargo to the media at www.jamamedia.org.)
Editor's Note: Please see the article for additional information, including other authors, author contributions and affiliations, financial disclosures, funding and support, etc.
To contact Nina P. Paynter, Ph.D., call Lori Shanks at 617-534-1604 or e-mail ljshanks@partners.org. To reach Mark J. Pletcher, M.D., M.P.H., call Kristen Bole at 415-476-2743 or e-mail kristen.bole@ucsf.edu.
Journal
Archives of Internal Medicine