LONDON — The incidence of coronary heart disease among young women with systemic lupus erythematosus is “startlingly” worrisome, Ian Bruce, M.D., said at the Sixth European Lupus Meeting.
Studies have shown that the annual incidence of ischemic heart disease in lupus patients is 1.3%–1.5%. In comparison, the incidence among those with newly diagnosed type 2 diabetes and among those who have had a first myocardial infarction is 2%–2.2% per annum. “This latter number may be higher, but you have to remember that these are men in their mid- to late 50s, while the lupus patients in these studies are women whose average age is 35–37,” said Dr. Bruce, of the University of Manchester (England).
The prevalence of myocardial infarction or angina in lupus cohorts ranges from 7% to 10%, depending on patient age and duration of follow-up, he said.
Moreover, as survival improves, the prevalence of the disease increases, as does the proportion of lupus patients who are older and at even greater risk for cardiovascular disease, he said.
Some epidemiologic work has suggested that the peak age of onset also is increasing and now occurs between the fifth and seventh decades. Damage accrues more quickly among patients who are older at onset, he added.
Atherosclerosis also occurs much earlier in women with lupus than in healthy women. “In women younger than 45 in the general population, you virtually do not see plaque, whereas women with lupus are beginning to acquire plaque at that early age,” Dr. Bruce said.
Classic risk factors clearly are implicated in the premature atherosclerosis and coronary heart disease seen in lupus. There is a much higher prevalence of hypertension, diabetes, and renal impairment, and lupus patients typically have other risk factors such as higher levels of LDL cholesterol and triglycerides (Arthritis Rheum. 2003;48:3159–67).
And these risk factors do have an impact. “In a cohort study, we stratified patients according to their total cholesterol levels and found that among those with persistently elevated cholesterol, 24% developed a cardiac event during 12 years of follow-up, compared with 3% whose cholesterol level was normal or varied only slightly with disease flares,” Dr. Bruce said at the meeting, sponsored by the British Society for Rheumatology.
But classic risk factors do not tell the whole story. (See box.) In the general population, risk for a cardiac event increases as risk factors accumulate. “Lupus patients, however, seem to be set at an intrinsically higher baseline, and the accumulation of risk factors has an even more devastating effect,” he said.
A great need exists for properly conducted clinical trials of potential interventions for these patients. “We need to see if what we think will work actually does work and what the magnitude of risk reduction is with a particular intervention,” he said.
Statins are an example. “Everywhere they have been used so far, they have been associated with a reduction in risk of coronary disease events by about 30%. You could assume that also might be the case in lupus, but that could be a dangerous assumption, because these drugs might not be as well tolerated by lupus patients,” Dr. Bruce said.
Mediators and Markers: Look for Clues
As the severity of atherosclerosis and heart disease in systemic lupus erythematosus (SLE) becomes clearer, so do possible mediators and markers. A series of posters presented at the meeting by researchers from the Karolinska Institute, Stockholm, explored potential contributing factors:
▸ LDL cholesterol. Increased LDL-cholesterol oxidation contributes to lupus-related cardiovascular disease, reported Anna Cederholm, M.D. She presented data on 26 women with lupus plus cardiovascular disease, 26 women with lupus but no clinical manifestations of cardiovascular disease, and 26 normal controls.
Circulating levels of oxidized LDL cholesterol were increased in both lupus groups, as was platelet-activating factor acetylhydrolase (PAF-AH). Levels of oxidized LDL cholesterol and PAF-AH also were significantly higher in the lupus patients with cardiovascular disease than in those with lupus and no heart disease. Because PAF-AH binds to LDL cholesterol, it also may contribute to atherogenesis, Dr. Cederholm said.
▸ Anti-HDL-cholesterol antibodies. SLE-related dyslipidemia showed a surprising pattern in a study of women with a history of cardiovascular disease, reported J. Su, M.D. Large, rather than small, LDL- and HDL- cholesterol particles characterized the dyslipidemia profile. This was not an expected atherogenic lipid profile.
Antibodies against apolipoprotein A1 in HDL cholesterol also were elevated and were associated with the presence of tumor necrosis factor. Whether these anti-apo A1 antibodies play a pathogenic role—for example, by inhibiting the anti-inflammatory properties of HDL—is under investigation, Dr. Su said.