Characterization of Post-Thrombotic Syndrome in Children with Cardiac Disease - 09/12/18
Abstract |
Objective |
To assess the validity of existing clinical scales assessing the presence of physical and functional abnormalities for diagnosing post-thrombotic syndrome (PTS) in children, including specific evaluation of use in children with congenital heart disease (CHD).
Study design |
One hundred children aged >2 years (average age, 6 years), including 33 with CHD and previously proven extremity deep vein thrombosis (DVT), 37 with CHD and no previous DVT, and 30 healthy siblings, were blindly assessed for PTS using the modified Villalta Scale (MVS). All patients aged <6 years underwent neurodevelopmental testing and an age-appropriate quality of life assessment.
Results |
The MVS identified mild PTS in 20 children and moderate PTS in 1 child (including 14 of 33 [42%] in the CHD/DVT group, 5 of 37 [14%] in the CHD/no DVT group, and 2 of 30 controls [7%]). The diagnosis of PTS was confirmed clinically in 14 patients, all of whom had previous thrombosis and 1 of whom was MVS-negative. MVS had an accuracy of 91% and performed reasonably well as a screening tool but poorly as a diagnostic tool. MVS reliability was acceptable. Children with PTS had similar quality of life as those without PTS but had higher rates of neurodevelopmental delays in gross motor skills (70% vs 24%; P = .02) and problem-solving indicators (60% vs 15%; P = .008).
Conclusions |
Using the MVS scale for PTS screening in children with CHD is feasible and reliable, and the scale has good correlation with a clinical diagnosis of PTS despite a high prevalence of false-positive findings. Further research is needed to determine the clinical relevance of PTS in this population.
Le texte complet de cet article est disponible en PDF.Keywords : congenital heart disease, neurodevelopment, instrument validation, pediatrics
Abbreviations : ASQ, CHD, DVT, MVS, PedsQL, PTS
Plan
Supported by the Labatt Family Heart Centre Innovation Funds and the Canadian Institutes of Health Research. The authors declare no conflicts of interest. |
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Portions of this study were presented at the American Heart Association Scientific Sessions, Orlando, Florida, November 12-14, 2011, and at the XXIII Congress of the International Society on Thrombosis and Haemostasis, Kyoto, Japan, July 23-28, 2011. |
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