Dear Editor,
We were excited to read the manuscript by Asada et al. investigating bubble contrast echocardiography in children after total cavopulmonary connection.Reference Asada, Morishita, Kawai, Kajiyama and Ikeda1 Asada et al. retrospectively analysed the medical records of patients who underwent cardiac catheterisations and bubble contrast (agitated saline) transthoracic echocardiograms from 2010 to 2018. Their study impressively included 140 patients (mean age 7.6 [range 2.5–20.8] years) who previously underwent total cavopulmonary connection (mean of 5.3 [range 0.6–18.1] years after total cavopulmonary connection). They reported that only 13 patients (9.3%) had negative bubble studies bilaterally and that there was no correlation between bubble study grade and pulmonary capillary wedge saturation (a surrogate for pulmonary vein oxygen saturation). They concluded that bubble contrast echocardiography may create false positive findings for detecting pulmonary arteriovenous fistulas and further standardisation of bubble echocardiograms is required.
We advocate for more conservative interpretation of their findings. Asada et al. reported that bubble contrast grade did not correlate with pulmonary capillary wedge saturation, but this was well demonstrated more than 20 years ago.Reference Chang, Alejos and Atkinson2,Reference Feinstein, Moore, Rosenthal, Puchalski and Brook3 Feinstein et al. rationalised that bubble echocardiography is a sensitive test capable of identifying pulmonary microvascular disease before pulmonary vein desaturation. They recommended improving echo correlation by assessing the partial pressure of oxygen (PaO2) in pulmonary veins while patients inspire 100% O2. Abnormally low PaO2 (<500 mmHg) on supplemental oxygen indicates impaired gas exchange in the pulmonary capillaries despite normal saturation and has a negative predictive value of 100%.Reference Kjeldsen, Oxhoj and Andersen4 Recent guidelines for assessing pulmonary arteriovenous malformations in patients with hereditary haemorrhagic telangiectasia support the use of transthoracic bubble contrast echocardiography as the initial screening test given its high sensitivity, and a positive bubble study without other abnormalities is diagnostic of microscopic pulmonary arteriovenous malformations.Reference Faughnan, Palda and Garcia-Tsao5 Importantly, it is unknown if or how pulmonary arteriovenous malformations differ between patients with univentricular CHD and patients with hereditary haemorrhagic telangiectasia.
Regardless of bubble contrast correlation with oxygen saturation or PaO2, it is unknown if gradually improved oxygen saturations that are normally observed after total cavopulmonary connection indicate pulmonary vascular reverse remodelling with complete microscopic resolution of pulmonary arteriovenous malformations or simply functional improvement in gas exchange.Reference McElhinney, Kreutzer, Lang, Mayer, del Nido and Lock6,Reference Kutty, Frommelt, Danford and Tweddel7 A positive bubble study 5 years after total cavopulmonary connection with normal oxygen saturation may indicate functional resolution of pulmonary arteriovenous malformations without complete microvascular remodelling. In this scenario, a positive bubble study is not a false positive but rather a sensitive biomarker of subclinical pulmonary microvascular disease. In other words, once pulmonary arteriovenous malformations are established, they may never fully remodel to normal pulmonary microvasculature.
Asada et al. assert that the efficacy of bubble echocardiography for the diagnosis of pulmonary arteriovenous malformations has not been properly evaluated and standardisation of the technique is required. We agree in principal with their concerns about bubble echocardiography assessing pulmonary arteriovenous malformations in patients with univentricular CHD; however, we propose that the main limitation falls on our poor understanding of pulmonary arteriovenous malformations and pulmonary vascular remodelling in patients with palliated univentricular CHD.
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