What question did this study set out to answer?

To highlight a case of pregnancy-related myocardial infarction possibly linked to ritodrine treatment.

March 25, 2026Open Access

Pregnancy-related acute myocardial infarction after treatment with ritodrine hydrochloride: A case report

Resultado clave

Ritodrine tocolysis for preterm labor can induce silent acute myocardial infarction due to transient coronary vasospasm, necessitating careful cardiac monitoring during treatment.

Puntos clave

To highlight a case of pregnancy-related myocardial infarction possibly linked to ritodrine treatment.
Case report of a 34-year-old woman at 30 weeks of gestation receiving ritodrine.
ECG monitoring and evaluation of cardiac biomarkers performed after treatment discontinuation.
Emergency Cesarean delivery initiated due to fetal bradycardia; follow-up cardiac imaging conducted.
New ST-segment elevation observed on ECG without chest pain.
High-sensitivity troponin I levels were significantly elevated at 5392 pg/mL.
No obstructive coronary disease was found on follow-up imaging; infant discharged without adverse effects.

PICO estructurado

Población

A 34-year-old Japanese primigravida at 30 weeks of gestation receiving treatment for preterm labor

Intervención

Ritodrine hydrochloride (β₂-agonist tocolysis)

Resultado

Pregnancy-associated myocardial infarction (PAMI)safety

Ritodrine tocolysis in pregnancy may be associated with silent myocardial infarction, highlighting the need for careful cardiac monitoring including ECG and biomarkers.

Resultado numérico

Tasa de eventos absoluta: 0% vs 0%

Resumen

Pregnancy-associated myocardial infarction (PAMI) is a rare but potentially life-threatening condition for the mother and fetus. Pregnancy also confers a three- to fourfold increased risk of MI compared with the non-pregnant state. However, recognizing PAMI promptly in obstetric settings remains challenging. A 34-year-old Japanese primigravida at 30 weeks of gestation had been receiving ritodrine for preterm labor. On hospital day 2, approximately 4 h after discontinuation of tocolytics, repeat electrocardiography (ECG) indicated new ST-segment elevation in leads I, aVL, and V3-V6 without chest pain. High-sensitivity troponin I was 5392 pg/mL, CK-MB was 21 IU/L, and transthoracic ECG revealed mild apical hypokinesis. That night, prolonged fetal bradycardia prompted emergency Cesarean delivery. Maternal cardiac biomarkers then declined rapidly, and the ECG and wall-motion abnormalities resolved. Myocardial perfusion scintigraphy (day 5) and coronary computed tomography angiography (day 6) showed no perfusion defect or obstructive coronary disease. The infant, weighing 1546 g, was admitted to the neonatal intensive care unit. No adverse effects attributable to ritodrine were observed, and the infant was discharged on postnatal day 58. The report describes probable drug-induced PAMI temporally associated with β₂-agonist tocolysis, with plausible mechanisms including transient coronary vasospasm and supply-demand mismatch in the hemodynamic milieu of pregnancy. This case suggests that women receiving β₂-agonist tocolysis should be monitored for vital signs, electrolytes, and ECG changes. Even without chest pain, new ECG abnormalities or palpitations warrant immediate cardiac evaluation. • In the reported case silent myocardial infarction occurred during ritodrine tocolysis for threatened preterm labor. • Electrocardiography, echocardiography, and high-sensitivity troponin identified myocardial injury. • Careful cardiac monitoring should be considered when using ritodrine in pregnancy.

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