Interventional Cardiology. Группа авторов. Читать онлайн. Newlib. NEWLIB.NET

Автор: Группа авторов
Издательство: John Wiley & Sons Limited
Серия:
Жанр произведения: Медицина
Год издания: 0
isbn: 9781119697381
Скачать книгу
events in patients with atherosclerotic disease. Beyond CRP’s ability to predict risk among both primary and secondary prevention patients, interest in it has increased with the recognition that statin‐induced reduction of CRP is associated with less progression in adverse cardiovascular events that is independent of the lipid‐associated changes [187] and that the efficacy of statin therapy may be related to the underlying level of vascular inflammation as detected by hs‐CRP. Among patients with stable angina and established CAD, plasma levels of hs‐CRP have consistently been shown associated with recurrent risk of cardiovascular events [188, 189]. Similarly, during acute coronary ischemia, levels of hs‐CRP are predictive of high vascular risk even if troponin levels are non‐detectable, suggesting that inflammation is associated with plaque vulnerability even in the absence of detectable myocardial necrosis [190, 191]. Despite these data, the most relevant use of hs‐CRP remains in the setting of primary prevention. To date, over two dozen large‐scale prospective studies have shown baseline levels of hs‐CRP to independently predict future myocardial infarction, stroke, cardiovascular death, and incident peripheral arterial disease [192,193]. Moreover, eight major prospective studies have had adequate power to evaluate hs‐CRP after adjustment for all Framingham covariates, and all have confirmed the independence of hs‐CRP [194]. The association of plaque morphology prone to rupture with hs‐CRP has been also shown in the preliminary study [195]. Subsequently, a number of drug approaches to the inflammatory cardiovascular residual risk have been guided by knowledge of the inflammatory basis of cardiovascular disease. Recently, the CANTOS trial with the anti‐IL‐1‐beta monoclonal antibody canakinumab, demonstrated the reduction of hs‐CRP by 35% and reduced the composite of nonfatal‐MI, nonfatal stroke or cardiovascular death (hazard ratio (HR) =0.85, 95%CI: 0.74–0.98) [196]. Additionally, canakinumab reduced MACE rates to a similar extent in patients with or without diabetes197 and was associated with a significant reduction in deaths from lung cancer [198].

      Colchicine, another anti‐inflammatory drug widely used for gout and pericarditis, has been examined to have a beneficial effect on cardiovascular disease, which showed the reduction of ischemic cardiovascular events in patients with MI [199], whereas a further trial investigating the efficacy of another anti‐inflammatory drug of methotrexate, most commonly used for arthritis, on patients with coronary artery disease was stopped given that it did not result in the lowering of IL‐1beta, IL‐6 or hs‐CRP compared to placebo and was associated with raised liver enzymes, reduction in leukocytes and hematocrit and a higher incidence of non‐basal cell skin cancer compared to placebo [200]. Thus, given unclear the anti‐inflammatory protective mechanism further investigation is required to better understand the association between inflammation and atherosclerotic disease.

Schematic illustration of a stable atherosclerotic plaque characterized by the presence of a low inflammatory infiltrate. Schematic illustration of unstable atherosclerotic plaque characterized by the presence of a thin fibrous cap rich in inflammatory macrophagic foam cells and T lymphocytes.