Role of B lymphocytes in the infarcted mass in patients with acute myocardial infarction

Introduction: Almost 20% of patients with acute myocardial infarction (MI) develop heart failure, even when early reperfused [1]. Left ventricular remodeling seems related to the size of myocardial infarction and timely reperfusion, as well as to the inflammatory responses and residual ischemia [2]. Experimental studies suggested that B lymphocytes may influence the myocardial infarcted mass [3], although there are few data about the role of these cells in humans. Furthermore, a possible atheroprotective role for B1 lymphocytes has been proposed based on the production of interleukin 10 (IL-10) and natural antibodies, which may switch the proinflammatory response to more appropriate healing, promoting cell recovery and the clearance of apoptotic cellular debris [4]. On the other hand, classic B lymphocytes or B2 cells are linked to progression of atherosclerosis, possibly by their interaction with CD4+ T lymphocytes [4]. In 2011, Griffin and colleagues proposed CD19+CD20+CD43+CD70- lymphocyte cells as the human B1 phenotype, and these cells spontaneously produced IgM and IL-10 [5]. However, according to the presence or absence of the CD11b on the surface of these cells, the capacity of IgM production and activation Stem cells in blood marrow differentiate in T or B lymphocyte, according to the presence of CD3 or CD19, respectively. Lymphocyte final maturation takes place in thymus for T cells; or in spleen and lymphatic tissue for classic B cells. B1 lymphocytes are well described in experimental studies. These cells are notorious for their capacity of spontaneous production of IgM and according to the presence of the CD11b, two distinct subtypes are recognized: CD11b- B1 lymphocytes, producing IgM, and CD11b+ B1 lymphocytes, related to the expansion of CD4+ T lymphocytes.

Role of B lymphocytes in the infarcted mass in patients with acute myocardial infarction.

Despite early reperfusion, patients with ST segment elevation myocardial infarction (STEMI) may present large myocardial necrosis and significant impairment of ventricular function. The present study aimed to evaluate the role of subtypes of B lymphocytes and related cytokines in the infarcted mass and left ventricular ejection fraction obtained by cardiac magnetic resonance imaging performed after 30 days of STEMI. This prospective study included 120 subjects with STEMI submitted to pharmacoinvasive strategy. Blood samples were collected in subjects in the first (D1) and 30th (D30) days post STEMI. The amount of CD11b+ B1 lymphocytes (cells/ml) at D1 were related to the infarcted mass (rho = 0.43; P=0.033), measured by cardiac MRI at D30. These B1 cells were associated with CD4+ T lymphocytes at D1 and D30, while B2 classic lymphocytes at day 30 were related to left ventricular ejection fraction (LVEF). Higher titers of circulating IL-4 and IL-10 were observed at D30 versus D1 (P=0.013 and P<0.001, respectively). Titers of IL-6 at D1 were associated with infarcted mass (rho = 0.41, P<0.001) and inversely related to LVEF (rho = -0.38, P<0.001). After multiple linear regression analysis, high-sensitivity troponin T and IL-6 collected at day 1 were independent predictors of infarcted mass and, at day 30, only HDL-C. Regarding LVEF, high-sensitivity troponin T and high-sensitivity C-reactive protein were independent predictors at day 1, and B2 classic lymphocytes, at day 30. In subjects with STEMI, despite early reperfusion, the amount of infarcted mass and ventricular performance were related to inflammatory responses triggered by circulating B lymphocytes.