TY - JOUR
T1 - Medical treatment of pulmonary hypertension in adults with congenital heart disease
T2 - updated and extended results from the International COMPERA-CHD Registry
AU - Kaemmerer, Ann Sophie
AU - Gorenflo, Matthias
AU - Huscher, Dörte
AU - Pittrow, David
AU - Ewert, Peter
AU - Pausch, Christine
AU - Delcroix, Marion
AU - Ghofrani, Hossein A.
AU - Hoeper, Marius M.
AU - Kozlik-Feldmann, Rainer
AU - Skride, Andris
AU - Stähler, Gerd
AU - Vizza, Carmine Dario
AU - Jureviciene, Elena
AU - Jancauskaite, Dovile
AU - Gumbiene, Lina
AU - Ewert, Ralf
AU - Dähnert, Ingo
AU - Held, Matthias
AU - Halank, Michael
AU - Skowasch, Dirk
AU - Klose, Hans
AU - Wilkens, Heinrike
AU - Milger, Katrin
AU - Jux, Christian
AU - Koestenberger, Martin
AU - Scelsi, Laura
AU - Brunnemer, Eva
AU - Hofbeck, Michael
AU - Ulrich, Silvia
AU - Noordegraaf, Anton Vonk
AU - Lange, Tobias J.
AU - Bruch, Leonhard
AU - Konstantinides, Stavros
AU - Claussen, Martin
AU - Löffler-Ragg, Judith
AU - Wirtz, Hubert
AU - Apitz, Christian
AU - Neidenbach, Rhoia
AU - Freilinger, Sebastian
AU - Nemes, Attila
AU - Opitz, Christian
AU - Grünig, Ekkehard
AU - Rosenkranz, Stephan
N1 - Publisher Copyright:
© Cardiovascular Diagnosis and Therapy. All rights reserved.
PY - 2021/12
Y1 - 2021/12
N2 - Background: Pulmonary arterial hypertension (PAH) is common in congenital heart disease (CHD). Because clinical-trial data on PAH associated with CHD (PAH-CHD) remain limited, registry data on the long-term course are essential. This analysis aimed to update information from the COMPERA-CHD registry on management strategies based on real-world data. Methods: The prospective international pulmonary hypertension registry COMPERA has since 2007 enrolled more than 10,000 patients. COMPERA-CHD is a sub-registry for patients with PAH-CHD Results: A total of 769 patients with PAH-CHD from 62 specialized centers in 12 countries were included into COMPERA-CHD from January 2007 through September 2020. At the last follow-up in 09/2020, patients [mean age 45.3±16.8 years; 512 (66%) female] had either post-tricuspid shunts (n=359; 46.7%), pre-tricuspid shunts (n=249; 32.4%), complex CHD (n=132; 17.2%), congenital left heart or aortic valve or aortic disease (n=9; 1.3%), or miscellaneous CHD (n=20; 2.6%). The mean 6-minute walking distance was 369±121 m, and 28.2%, 56.0%, and 3.8% were in WHO functional class I/II, III or IV, respectively (12.0% unknown). Compared with the previously published COMPERA-CHD data, after 21 months of followup, the number of included PAH-CHD patients increased by 91 (13.4%). Within this group the number of Eisenmenger patients rose by 39 (16.3%), the number of “Non-Eisenmenger PAH” patients by 45 (26.9%). Currently, among the 674 patients from the PAH-CHD group with at least one follow-up, 450 (66.8%) received endothelin receptor antagonists (ERA), 416 (61.7%) PDE-5 inhibitors, 85 (12.6%) prostacyclin analogues, and 36 (5.3%) the sGC stimulator riociguat. While at first inclusion in the COMPERA-CHD registry, treatment was predominantly monotherapy (69.3%), this has shifted to favoring combination therapy in the current group (53%). For the first time, the nature, frequency, and treatment of significant comorbidities requiring supportive care and medication are described. Conclusions: Analyzing “real life data” from the international COMPERA-CHD registry, we present a comprehensive overview about current management modalities and treatment concepts in PAH-CHD. There was an trend towards more aggressive treatment strategies and combination therapies. In the future, particular attention must be directed to the “Non-Eisenmenger PAH” group and to patients with complex CHD, including Fontan patients.
AB - Background: Pulmonary arterial hypertension (PAH) is common in congenital heart disease (CHD). Because clinical-trial data on PAH associated with CHD (PAH-CHD) remain limited, registry data on the long-term course are essential. This analysis aimed to update information from the COMPERA-CHD registry on management strategies based on real-world data. Methods: The prospective international pulmonary hypertension registry COMPERA has since 2007 enrolled more than 10,000 patients. COMPERA-CHD is a sub-registry for patients with PAH-CHD Results: A total of 769 patients with PAH-CHD from 62 specialized centers in 12 countries were included into COMPERA-CHD from January 2007 through September 2020. At the last follow-up in 09/2020, patients [mean age 45.3±16.8 years; 512 (66%) female] had either post-tricuspid shunts (n=359; 46.7%), pre-tricuspid shunts (n=249; 32.4%), complex CHD (n=132; 17.2%), congenital left heart or aortic valve or aortic disease (n=9; 1.3%), or miscellaneous CHD (n=20; 2.6%). The mean 6-minute walking distance was 369±121 m, and 28.2%, 56.0%, and 3.8% were in WHO functional class I/II, III or IV, respectively (12.0% unknown). Compared with the previously published COMPERA-CHD data, after 21 months of followup, the number of included PAH-CHD patients increased by 91 (13.4%). Within this group the number of Eisenmenger patients rose by 39 (16.3%), the number of “Non-Eisenmenger PAH” patients by 45 (26.9%). Currently, among the 674 patients from the PAH-CHD group with at least one follow-up, 450 (66.8%) received endothelin receptor antagonists (ERA), 416 (61.7%) PDE-5 inhibitors, 85 (12.6%) prostacyclin analogues, and 36 (5.3%) the sGC stimulator riociguat. While at first inclusion in the COMPERA-CHD registry, treatment was predominantly monotherapy (69.3%), this has shifted to favoring combination therapy in the current group (53%). For the first time, the nature, frequency, and treatment of significant comorbidities requiring supportive care and medication are described. Conclusions: Analyzing “real life data” from the international COMPERA-CHD registry, we present a comprehensive overview about current management modalities and treatment concepts in PAH-CHD. There was an trend towards more aggressive treatment strategies and combination therapies. In the future, particular attention must be directed to the “Non-Eisenmenger PAH” group and to patients with complex CHD, including Fontan patients.
KW - Congenital heart disease (CHD)
KW - Eisenmenger syndrome
KW - Pulmonary hypertension
KW - Registry
KW - Targeted treatment
UR - http://www.scopus.com/inward/record.url?scp=85123411832&partnerID=8YFLogxK
U2 - 10.21037/cdt-21-351
DO - 10.21037/cdt-21-351
M3 - Article
AN - SCOPUS:85123411832
SN - 2223-3652
VL - 11
SP - 1255
EP - 1268
JO - Cardiovascular Diagnosis and Therapy
JF - Cardiovascular Diagnosis and Therapy
IS - 6
ER -