BMPR1A promotes ID2–ZEB1 interaction to suppress excessive endothelial to mesenchymal transition
Author(s)
Lee, Heon-Woo; Adachi, Takaomi; Pak, Boryeong; Park, Saejeong; Hu, Xiaoyue; Choi, Woosoung; Kowalski, Piotr S; Chang, C Hong; Clapham, Katharine R; Lee, Aram; Papangeli, Irinna; Kim, Jongmin; Han, Orjin; Park, Jihwan; Anderson, Daniel G; Simons, Michael; Jin, Suk-Won; Chun, Hyung J; ... Show more Show less
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Components of bone morphogenetic protein (BMP) signalling have been implicated in both pathogenesis of pulmonary arterial hypertension (PAH) and endothelial-mesenchymal transition (EndoMT). In particular, the importance of BMP type 2 receptor in these processes has been extensively analysed. However, the contribution of BMP type 1 receptors (BMPR1s) to the onset of PAH and EndoMT remains poorly understood. BMPR1A, one of BMPR1s, was recently implicated in the pathogenesis of PAH, and was found to be down-regulated in the lungs of PAH patients, neither the downstream mechanism nor its contribution to EndoMT has been described. Therefore, we aim to delineate the role of endothelial BMPR1A in modulating EndoMT and pathogenesis of PAH.
Date issued
2023-05-02Department
Koch Institute for Integrative Cancer Research at MITJournal
Cardiovascular Research
Publisher
Oxford University Press
Citation
Heon-Woo Lee, Takaomi Adachi, Boryeong Pak, Saejeong Park, Xiaoyue Hu, Woosoung Choi, Piotr S Kowalski, C Hong Chang, Katharine R Clapham, Aram Lee, Irinna Papangeli, Jongmin Kim, Orjin Han, Jihwan Park, Daniel G Anderson, Michael Simons, Suk-Won Jin, Hyung J Chun, BMPR1A promotes ID2–ZEB1 interaction to suppress excessive endothelial to mesenchymal transition, Cardiovascular Research, Volume 119, Issue 3, March 2023, Pages 813–825.
Version: Final published version