학술논문

Genetic evaluation of newborns with critical congenital heart defects admitted to the intensive care unit.
Document Type
Article
Source
European Journal of Pediatrics. Oct2021, Vol. 180 Issue 10, p3219-3227. 9p. 1 Color Photograph, 6 Charts.
Subject
*CONGENITAL heart disease
*NEWBORN infants
*INTENSIVE care units
*CHROMOSOME analysis
*22Q11 deletion syndrome
Language
ISSN
0340-6199
Abstract
Rapid and efficient diagnostics is crucial for newborns with congenital heart defects (CHD) in intensive care unit (ICU) but is often challenging. Given that genetic factors play a role in 20–30% cases of CHD, it is likely that genetic tests could improve both its speed and efficiency. We aimed to analyze the utility of rapid and cost-effective multiplex ligation dependent probe amplification analysis (MLPA) for chromosomal analysis in newborns with critical CHD. One hundred consecutive newborns admitted with critical CHD to the ICU were included in the study. Those with normal MLPA findings were further tested by chromosomal microarray and clinical exome sequencing. Overall, pathogenic/likely pathogenic variants were determined in ten (10%) newborns by MLPA, three (3%) by chromosomal microarray, and three (3%) by clinical exome sequencing. The most common variant detected was deletion of 22q11.2 region. Conclusion: MLPA is fast and cost-effective analysis that could be used as the first-tier test in newborns with critical CHD admitted to the ICU. What is Known: • MLPA is an established method for chromosome analysis in patients with CHD, but detection rate in newborns with critical CHD is unknown. What is New: • Study suggests that detection rate of casual variants using MLPA in newborns with critical CHD is 10%. [ABSTRACT FROM AUTHOR]