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An infant with transposition and cystic fibrosis

Published online by Cambridge University Press:  02 December 2008

Amanda L. Cook ,
Kari L. Crawford  and
Derek A. Williams
Amanda L. Cook*
Affiliation:
Department of Pediatrics, Division of Pediatric Cardiology, Wake Forest, University School of Medicine, Winston-Salem, North Carolina, United States of America
Kari L. Crawford
Affiliation:
Department of Pediatrics, Division of Pediatric Cardiology, Wake Forest, University School of Medicine, Winston-Salem, North Carolina, United States of America
Derek A. Williams
Affiliation:
Department of Pediatrics, Division of Pediatric Cardiology, Wake Forest, University School of Medicine, Winston-Salem, North Carolina, United States of America
*
Correspondence to: Amanda L. Cook, MD, Wake Forest University School of Medicine, Medical Center Boulevard, Winston-Salem, NC 27157, United States of America. Tel: (336) 716 3232; Fax: (336) 716 0533; E-mail: acook@wfubmc.edu
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Abstract

We report an infant with transposition, with the circumflex artery arising from the right coronary artery, who was diagnosed with cystic fibrosis following the occurrence of meconium ileus in the postoperative period.

Keywords

Congenital heart diseasegenetic syndromesmeconium ileus
Type
Brief Report
Information
Cardiology in the Young , Volume 19 , Issue 1 , February 2009 , pp. 111 - 112
Copyright
Copyright © Cambridge University Press 2008

Transposition, produced by the combination of concordant atrioventricular and discordant ventriculo-arterial connections, is the most common cyanotic congenital cardiac defect presenting in the neonatal period. In treating this entity, the arterial switch procedure has now been shown to have excellent results when performed in infants at low risk. Associated genetic disorders. and extracardiac anomalies, can significantly exacerbate the clinical management and outcome of these infants. Clinicians who care for children with this lesion must remain aware of the potential for other anomalies which can complicate the care. In this report, we describe an infant with both transposition and cystic fibrosis.

Case Report

The infant, born at full term, was a male weighing 2.8 kilograms. Pregnancy was complicated by insulin dependent diabetes mellitus, and a positive family history of cystic fibrosis in a sibling. Prenatal screening for the cystic fibrosis mutation was refused. Initially vigorous, he was noted to be cyanotic by the end of the first day of life. An arterial blood gas was obtained, and showed a pH of 7.34, with a partial pressure of oxygen of 12 torr. The infant was started on supplemental oxygen and prostaglandins, with saturations increasing to mid 80%. The infant was transferred to a tertiary medical facility. Upon arrival, the repeat arterial blood gas showed a pH of 7.36, and a partial pressure of oxygen of 61 torr.

Examination revealed a right ventricular lift, a normal first heart sound, a single second heart sound, and no murmurs. The lungs were clear, with shallow respirations, and no retractions. Pulses were equal and full in all extremities. There was no hepatomegaly.

A chest radiograph revealed a normal cardiac silhouette with a narrow mediastinum. The pulmonary vasculature was normal in appearance, and there were no infiltrates seen. Echocardiography demonstrated transposition, with concordant atrioventricular and discordant ventriculo-arterial connections. There was low velocity left-to-right shunting at the level of the patent oval foramen. Inspection of the coronary arteries revealed the circumflex artery arising from the right coronary artery. There was a large patent arterial duct, with left-to-right shunting. The infant was continued on 100% inspired oxygen via a hood. He passed some meconium stool on the first day of life, and received no enteral feeds preoperatively.

At 9 days of age, the patient underwent the arterial switch procedure. He initially tolerated the procedure well, and returned to the paediatric intensive care unit intubated. At 16 days of age, he was noted to have abdominal distension, having passed no stool over the previous 10 days. A barium enema was performed, which demonstrated a large meconium plug and a small left colon. His treatment for the meconium plug included broad spectrum antibiotics and acetylcysteine. After several days of treatment, he passed the meconium plug, and began tolerating enteral feeds. His blood tested positive for cystic fibrosis with ΔF508 homozygosity being found on a separate test prior to receiving the results of neonatal screening. On the 29th day of life, he was discharged home.

Discussion

Cystic fibrosis is a disorder of a membrane glycoprotein, which is present in some types of epithelia cells and contributes to the regulation of the flux of ions across cell surfaces. There is often severe injury to the organs involved, including the lungs, the exocrine pancreas, the liver, and the intestines. The pulmonary disease is often chronic and progressive, resulting in most of the morbidity and mortality. Other complications can also be severe, including infection, malnutrition, electrolytic disturbances, diabetes, nasal polyps, and vasculitis.

The life expectancy for those born with cystic fibrosis has improved from about 6 months when initially described in the 1930s, to more than 30 years.Reference Davis1 Advances in survival include the recognition of milder cases, supplementation of pancreatic enzymes, use of antibiotics, and centralized care in centres promoting aggressive treatment. It is the most common lethal autosomal recessive disease found in Caucasians in the United States of America, with an incidence of 1 per 3200 live births in Caucasians, and 1 in 15,000 in African-Americans.Reference Orenstein, Rosenstein and Stern2 The gene resides on chromosome 7, with the most common disease-causing allele in the United States of America being ΔF508.Reference Accurso3 This gene codes for the cystic fibrosis transmembrane conductance regulator, which is a membrane glycoprotein, and results in abnormal cAMP-regulated chloride channels.

Transposition accounts for 5 to 7% of all congenitally malformed hearts, having an incidence of 0.2 per 1000 live births, making it the most common cyanotic cardiac lesion encountered in the neonatal period.Reference Hoffman4 The lesion has known associations with certain genetic conditions including 22q11 deletions, acrocephalopolysyndactyly type II, CFC1 mutations, and PROSIT240 mutations.Reference Goldmuntz, Clark and Mitchell5Reference Muncke, Jung and Rudiger8 Furthermore, there is risk of familial recurrence in siblings of 1.8%, suggesting monogenic or oligogenic inheritance.Reference Digilio, Casey and Toscano9 There has been one previous case report from Saudi Arabia of an infant with transposition with a positive sweat chloride test, albeit with a normal analysis for deoxyribonucleic acid.Reference Baslaim and Jamjoom10

Although it is well recognized that transposition is frequently associated with extracardiac anomalies, including 22q11 syndrome, in our review of the literature we were unable to find other reported patients with both transposition cystic fibrosis in the United States of America. Clinicians must remain aware of genetic disorders, which may alter the clinical management of patients with congenitally malformed hearts.

References

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