BackgroundRupture of atherosclerotic plaques is probably the most important mechanism underlying the sudden onset of acute coronary syndromes. Macrophages may release lytic enzymes that degrade the fibrous cap and therefore produce rupture of the atherosclerotic plaque. This study was designed to quantify macrophage content in coronary plaque tissue from patients with stable and unstable coronary syndromes.Methods and ResultsHematoxylin and eosin and immuno-staining with anti-human macrophage monoclonal antibody (PG-M1) were performed. Computerized planimetry was used to analyze26 atherectomy specimens comprising 524 pieces of tissue from 8 patients with chronic stable angina, 8 patients with unstable angina, and 10 patients with non-Q-wave myo-cardial infarction. Total plaque area was 417±87 mm2× 10−2in patients with stable angina, 601±157 mm2×10−2in patients with unstable angina, and 499±87 mm2× 10−2in patients with non-Q-wave myocardial infarction (P=NS). The macrophage-rich area was larger in plaques from patients with unstable angina (61±18 mm2x 102) and non-Q-wave myocardial infarction (87±32mm2× 10−2) than in plaques from patients with stable angina (14±5 mm2×10−2) (P=.024). The percentage of the total plaque area occupied by macrophages was also larger in patients with unstable angina (13.3 ±5.6%) and non-Q-wave myocardial infarction (14.6±4.6%) than in patients with stable angina (3.14±1%) (P=.018). Macrophagerich sclerotic tissue was largest in patients with non-Q-wave myocardial infarction (67±30 mm2× 1010−2) and unstable angina (55±19 mm2× 10−2) than in patients with stable angina (11.5±4.1 mm2× 10−2) (P=.046). Macrophage-rich atheromatous gruel was also larg-est in patients with non-Q-wave myocardial infarction (15±4 mm2×10−2) than in patients with unstable angina (3.3±1.7 mm2×10−2) or stable angina (2.4±1.2 mm2× 10−2) (P=.026).ConclusionsMacrophage-rich areas are more frequently found in patients with unstable angina and non-Q-wave myocardial infarction. This suggests that macrophages are a marker of unstable atherosclerotic plaques and may play a significant role in the pathophysiology of acute coronary syndromes.