Adjunct Targeted Biologic Inhibition Agents to Treat Aggressive Multivessel Intraluminal Pediatric Pulmonary Vein Stenosis - 22/06/18
, Mark W. Kieran, MD, PhD 2, 3, Christopher W. Baird, MD 4, Steven D. Colan, MD 1, Kimberlee Gauvreau, ScD 1, Christina M. Ireland, MS, RN, FNP 1, Audrey C. Marshall, MD 5, Laureen M. Sena, MD 6, Sara O. Vargas, MD 7, Kathy J. Jenkins, MD, MPH 1Abstract |
Objective |
To evaluate the use of imatinib mesylate with or without bevacizumab targeting neoproliferative myofibroblast-like cells with tyrosine kinase receptor expression, as adjuncts to modern interventional therapies for the treatment of multivessel intraluminal pulmonary vein stenosis (PVS). We describe the 48- and 72-week outcomes among patients receiving imatinib mesylate with or without bevacizumab for multivessel intraluminal PVS.
Study design |
This single-arm, prospective, open-label US Food and Drug Administration approved trial enrolled patients with ≥2 affected pulmonary veins after surgical or catheter-based relief of obstruction between March 2009 and December 2014. Drug therapy was discontinued at 48 weeks, or after 24 weeks of stabilization, whichever occurred later.
Results |
Among 48 enrolled patients, 5 had isolated PVS, 26 congenital heart disease, 5 lung disease, and 12 both. After the 72-week follow-up, 16 patients had stabilized, 27 had recurred locally without stabilization, and 5 had progressed. Stabilization was associated with the absence of lung disease (P = .03), a higher percentage of eligible drug doses received (P = .03), and was not associated with age, diagnosis, disease laterality, or number of veins involved. Survival to 72 weeks was 77% (37 of 48). Adverse events were common (n = 1489 total), but only 16 were definitely related to drug treatment, none of which were serious.
Conclusion |
Survival to 72 weeks was 77% in a referral population with multivessel intraluminal PVS undergoing multimodal treatment, including antiproliferative tyrosine kinase blockade. Toxicity specific to tyrosine kinase blockade was minimal.
Le texte complet de cet article est disponible en PDF.Keywords : congenital heart disease, drug therapy, treatment, outcome
Abbreviations : AE, BCH, CHD, CT, DSMB, IRB, PAH, PDGFR, PVS, RTKs
Plan
| Disclosures: Novartis provided free drugs for some patients in this study. M.K. serves on a Novartis Scientific Advisory Board for the pre-clinical and therapeutic development of novel therapeutic agents for pediatric brain tumors. The other authors declare no conflicts of interest. |
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| Funded by the Ansley's Heart Endowment Fund (Boston, MA), Christina Capozzi Memorial Foundation (Boston, MA), and T.J. Reynolds Endowment Fund (Boston, MA). |
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| Portions of this study were presented as an oral abstract at the American Academy of Pediatrics Section on Cardiology and Cardiac Surgery (SOCCS), October 22-25, 2016, San Francisco, California. |
Vol 198
P. 29 - juillet 2018 Retour au numéro
Article précédent
- Epidemiologic Impact of the New Guidelines for the Diagnosis of Acute Rheumatic Fever
- Francesco Licciardi, Giacomo Scaioli, Roberta Mulatero, Agostina Marolda, Marta Delle Piane, Silvana Martino, Davide Montin, Pier Angelo Tovo
- Pulmonary Vein Stenosis in Infants: A Systematic Review, Meta-Analysis, and Meta-Regression
- Carl H. Backes, Erin Nealon, Aimee K. Armstrong, Clifford L. Cua, Courtney Mitchell, Usha Krishnan, Rachel D. Vanderlaan, Mi Kyoung Song, Nicola Viola, Charles V. Smith, Patrick I. McConnell, Brian K. Rivera, Jeffrey Bridge
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