Chagas Cardiomyopathy as the Etiology of Suspected Coronary Microvascular Disease. A Comparison Study with Suspected Coronary Microvascular Disease of Other Etiologies

Campos, Felipe Araujo; Magalhães, Mariana L.; Moreira, Henrique Turin; Pavão, Rafael B.; Lima Filho, Moyses O.; Lago, Igor M.; Badran, André V.; Chierice, João R. A.; Schmidt, André; Marin Neto, José Antonio

doi:10.36660/abc.20200381

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Original Article • Arq. Bras. Cardiol. 115 (6) • Dec 2020 • https://doi.org/10.36660/abc.20200381 copy

Chagas Cardiomyopathy as the Etiology of Suspected Coronary Microvascular Disease. A Comparison Study with Suspected Coronary Microvascular Disease of Other Etiologies

Authorship SCIMAGO INSTITUTIONS RANKINGS

Abstract

Background

Chagas disease (CD) as neglected secondary form of suspected coronary microvascular dysfunction (CMD).

Objectives

Comparison of patients with CMD related to CD (CMD-CE) versus patients with CMD caused by other etiologies (CMD-OE).

Methods

Of 1292 stable patients referred for invasive coronary angiography to elucidate the hemodynamic pattern and the cause of angina as a cardinal symptom in their medical history, 247 presented normal epicardial coronary arteries and 101 were included after strict exclusion criteria. Of those, 15 had suspected CMD-CE, and their clinical, hemodynamic, angiographic and scintigraphic characteristics were compared to those of the other 86 patients with suspected CDM-OE. Level of significance for all comparisons was p < 0.05.

Results

Patients with suspected CMD-CE showed most anthropometric, clinical, angiographic hemodynamic and myocardial perfusion abnormalities that were statistically similar to those detected in the remaining 86 patients with suspected CMD-OE. LV diastolic dysfunction, expressed by elevated LV end-diastolic pressure was equally found in both groups. However, as compared to the group of CMD-OE the group with CMD-CE exhibited lower left ventricular ejection fraction (54.8 ± 15.9 vs 61.1 ± 11.9, p= 0.049) and a more severely impaired index of regional wall motion abnormalities (1.77 ± 0.35 vs 1.18 ± 0.26, p= 0.02) respectively for the CMD-OE and CMD-CE groups.

Conclusion

Chronic Chagas cardiomyopathy was a secondary cause of suspected coronary microvascular disease in 15% of 101 stable patients whose cardinal symptom was anginal pain warranting coronary angiography. Although sharing several clinical, hemodynamic, and myocardial perfusion characteristics with patients whose suspected CMD was due to other etiologies, impairment of LV segmental and global systolic function was significantly more severe in the patients with suspected CMD related to Chagas cardiomyopathy. (Arq Bras Cardiol. 2020; 115(6):1094-1101)

Chagas Cardiomyopathy; Coronary Microvascular, Dysfunction; Dysfunction Ventricular, Left; Diastolic Dysfunction, Wall Motion Abnormality Index; Left Ventricular Ejection Fraction

	CMD-CE n = 15	CMD-OE n = 86	p-value
Age (years)	61.3 ± 6.7	68.9 ± 11.0	0.01
Female Gender (%)	60.0	67.4	0.65
Body weight (kg)	77.0 ± 13.1	80.7 ± 15.3	0.18
BMI (kg/m²)	31.0 ± 7.3	31.9 ± 5.6	0.72
Atypical angina (%)	60.0	66.3	0.86
Dyspnea (%)	53.0	64.0	0.62
Palpitation (%)	47.1	35.2	0.56
Hypertension (%)	93.3	81.3	0.46
Diabetes mellitus (%)	40	33.7	0.77
Dyslipidemia (%)	33	53.5	0.58
Smoking (%)	13.3	24.4	0.51
Use of medications
ACEI/ARB	100	71	0.037
Beta-blockers	53	54	0.79
Statins	47	53	0.90
Antidiabetics	40	42	0.88
Diuretics	47	40	0.82
Nitrates	20	12	0.63
Calcium antagonists	20	26	0.89
Antiplatelets	53	85	0.013
Normal EKG (%)	33.3	46.7	0.51

	CMD-CE n = 15	CMD-OE n = 86	p
LV hypertrophy (%)	20	53.3	0,128
LV dilation (%)	26.0	4.7	0.04
LVEDP (mmHg)	20.13 ± 5.43	19.0 ± 5.1	0.44
LVEF	54.8 ± 15.9	61.1 ± 11.9	0.049
LV segmental abnormalities (%)	86.6%	53.3%	0.02
LVWMSI	1.77 ± 0.35	1.18 ± 0.26	0.01
Ischemic perfusion defects (%)	45.5	62.3	0.31
SDS	0 (0 - 8)	3 (0 - 19)	0.23

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[1] Mailing Address: André Schmidt • Universidade de São Paulo Faculdade de Medicina de Ribeirão Preto - Centro de Cardiologia - HCFMRP-USP - Av. Bandeirantes, 3900. Postal Code 14048-900, Ribeirão Preto, SP – Brazil E-mail: aschmidt@fmrp.usp.br