Abstract
Background Takotsubo cardiomyopathy (TC) aetiology has not been completely understood yet. One proposed pathogenic mechanism was coronary microvascular dysfunction (MVD). This study compared coronary flow and myocardial perfusion in patients with TC, microvascular angina (MVA), and a control group (CG). Methods Out of 42 consecutive patients presented to our centre with TC from 2013 to 2017; we retrospectively selected 27 patients. We compared them with a sex- and age-matched group of 27 MVA cases and 27 patients with normal coronary arteries (CG). The flow was evaluated in the three coronary arteries as TIMI flow and TIMI frame count (TFC). Myocardial perfusion was studied with Blush-Score and Quantitative Blush Evaluator (QuBE). Results TFC, in TC, revealed flow impairment in the three arteries compared to the CG (left anterior descending artery (LAD): 22 ± 8, 15 ± 4; p = 0.001) (right coronary artery: 12 ± 4, 10 ± 3; p = 0,025) (left circumflex: 14 ± 4, CG 11 ± 3; p = 0,006). QuBE showed myocardial perfusion impairment in the LAD territory in TC comparing with both the CG (8,9 (7,2–11,5) versus 11,4 (10–15,7); p = 0,008) and the MVA group (8,9 (7,2–11,5) versus 13,5 (10–16); p = 0,006). Conclusions Our study confirmed that coronary flow is impaired in TC, reflecting a MVD. Myocardial perfusion defect was detected only in the LAD area.
Highlights
Takotsubo cardiomyopathy (TC) was described for the first time in the 1990 in Japan
Diagnosis of TC was achieved according to the presence of all 4 Mayo Clinic criteria [7]: (1) Transient hypokinesis, akinesis, or dyskinesis of the left ventricular mid segments with or without apical involvement: the regional wall motion abnormalities extend beyond a single epicardial vascular distribution
microvascular angina (MVA) diagnosis was defined according to these features: typical chest pain according to the ESC guidelines [8], evidence of myocardial ischemia detected by perfusion test, and normal coronary angiography
Summary
Takotsubo cardiomyopathy (TC) aetiology has not been completely understood yet. One proposed pathogenic mechanism was coronary microvascular dysfunction (MVD). This study compared coronary flow and myocardial perfusion in patients with TC, microvascular angina (MVA), and a control group (CG). We compared them with a sex- and age-matched group of 27 MVA cases and 27 patients with normal coronary arteries (CG). Myocardial perfusion was studied with Blush-Score and Quantitative Blush Evaluator (QuBE). TFC, in TC, revealed flow impairment in the three arteries compared to the CG (left anterior descending artery (LAD): 22 ± 8, 15 ± 4; p = 0.001) (right coronary artery: 12 ± 4, 10 ± 3; p = 0,025) (left circumflex: 14 ± 4, CG 11 ± 3; p = 0,006). QuBE showed myocardial perfusion impairment in the LAD territory in TC comparing with both the CG (8,9 (7,2–11,5) versus 11,4 (10–15,7); p = 0,008) and the MVA group (8,9 (7,2–11,5) versus 13,5 (10–16); p = 0,006). Myocardial perfusion defect was detected only in the LAD area
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