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American Heart Association

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Final ID: MDP1646

Treatment of pulmonary arterial hypertension by blocking integrin a5b1, a potential disease-modifying strategy

Abstract Body (Do not enter title and authors here): Introduction: Pulmonary arterial hypertension (PAH) is marked by pathological remodeling of distal arteries, driven by hyperplasia of pulmonary arterial smooth muscle cells (PASMCs), dysfunction of pulmonary arterial endothelial cells (PAECs), and increased deposition of the extracellular matrix (ECM).
Hypothesis: Considering the crucial role of ECM in vascular restructuring, we investigated the potential of therapeutically targeting a5b1, a fibronectin-binding integrin involved in cell proliferation and angiogenesis, for PAH treatment.
Aim: To evaluate the therapeutic potential of targeting a5b1 for the treatment of PAH.
Methods: We have developed potent, orally bioavailable small molecule inhibitors (SMis) and monoclonal antibodies (mAbs) targeting a5b1 to evaluate its therapeutic potential. The effect of a5b1 inhibition was assessed in cultured PASMCs, human precision-cut lung slices (PCLS), and a rat Sugen/hypoxia PAH model.
Results: PAH patients exhibited increased expression of fibronectin and a5b1 in distal pulmonary arteries. Selective inhibition of a5b1 in cultured PASMCs modulated multiple pathways involved in cell cycle regulation at both transcriptional and post-transcriptional levels, thereby blocking cellular proliferation. PCLS treated with a5b1 inhibitors showed decreased expression of pathways involved in ECM deposition and reduced levels of smooth muscle cell markers. In the rat Sugen/hypoxia PAH model, a5b1 inhibition with either an SMi or mAb significantly improved cardiac and vascular function by reducing pulmonary arterial wall thickness, right ventricular hypertrophy, and fibrosis. Cardiac improvement is further evidenced by a reduction in circulating NT-proBNP and NT-proANP levels.
Conclusion: These findings reveal a previously underappreciated role for a5b1 in PAH pathogenesis and support the potential of a5b1 inhibition as a disease-modifying therapeutic strategy for managing PAH.
  • Montesinos, Monica  ( Morphic Therapeutic , Waltham , Massachusetts , United States )
  • Moy, Terence I.  ( Morphic Therapeutic , Waltham , Massachusetts , United States )
  • Smukste, Inese  ( Morphic Therapeutic , Waltham , Massachusetts , United States )
  • Mcteague, T. Andrew  ( Morphic Therapeutic , Waltham , Massachusetts , United States )
  • Dowling, James  ( Morphic Therapeutic , Waltham , Massachusetts , United States )
  • Lama, Sujan  ( Morphic Therapeutic , Waltham , Massachusetts , United States )
  • Pondish, Jessica  ( Morphic Therapeutic , Waltham , Massachusetts , United States )
  • Qiao, Qi  ( Morphic Therapeutic , Waltham , Massachusetts , United States )
  • Monroy, Meghan Monroy  ( Morphic Therapeutic , Waltham , Massachusetts , United States )
  • Lin, Albert  ( Morphic Therapeutic , Waltham , Massachusetts , United States )
  • Wang, Hua  ( Morphic Therapeutic , Waltham , Massachusetts , United States )
  • Lemay, Sarah-eve  ( CRIUCPQ , Quebec , Quebec , Canada )
  • Boucherat, Olivier  ( IUCPQ RESEARCH CENTRE , Quebec , Quebec , Canada )
  • Sauvaget, Melanie  ( IUCPQ RESEARCH CENTRE , Quebec , Quebec , Canada )
  • Potus, Francois  ( IUCPQ RESEARCH CENTRE , Quebec , Quebec , Canada )
  • Breuils Bonnet, Sandra  ( Laval University , Quebec , Quebec , Canada )
  • Theberge, Charlie  ( CRIUCPQ-ULaval , Quebec , Quebec , Canada )
  • Provencher, Steeve  ( Laval University , Quebec , Quebec , Canada )
  • Ray, Adrian  ( Morphic Therapeutic , Waltham , Massachusetts , United States )
  • Lippa, Blaise  ( Morphic Therapeutic , Waltham , Massachusetts , United States )
  • Bonnet, Sebastien  ( Quebec Heart and Lung institute , Quebec , Quebec , Canada )
  • Goodwin, Bryan  ( Morphic Therapeutic , Waltham , Massachusetts , United States )
  • Kapoor, Parmita  ( Morphic Therapeutic , Waltham , Massachusetts , United States )
  • Lu, Min  ( Morphic Therapeutic , Waltham , Massachusetts , United States )
  • Rapisardi, Hailey  ( Morphic Therapeutic , Waltham , Massachusetts , United States )
  • Nguyen, Minh Hai  ( Morphic Therapeutic , Waltham , Massachusetts , United States )
  • Kim, Haejin  ( Morphic Therapeutics , Waltham , Massachusetts , United States )
  • Akram, Muzaffar  ( Morphic Therapeutic , Waltham , Massachusetts , United States )
  • Jain, Dhawal  ( Morphic Therapeutic , Waltham , Massachusetts , United States )
  • Konopka, Elizabeth  ( Morphic Therapeutic , Waltham , Massachusetts , United States )
  • Author Disclosures:
    Monica Montesinos: DO NOT have relevant financial relationships | Terence I. Moy: No Answer | Inese Smukste: No Answer | T. Andrew McTeague: No Answer | James Dowling: No Answer | Sujan Lama: No Answer | Jessica Pondish: No Answer | Qi Qiao: No Answer | Meghan Monroy Monroy: No Answer | Albert Lin: No Answer | Hua Wang: No Answer | Sarah-Eve Lemay: DO NOT have relevant financial relationships | Olivier Boucherat: DO NOT have relevant financial relationships | Melanie Sauvaget: No Answer | Francois Potus: No Answer | Sandra Breuils Bonnet: DO NOT have relevant financial relationships | Charlie Theberge: DO NOT have relevant financial relationships | Steeve Provencher: DO have relevant financial relationships ; Speaker:Janseen:Past (completed) ; Ownership Interest:HVL Therapeutics Inc:Active (exists now) ; Research Funding (PI or named investigator):Sunshine Bio:Active (exists now) ; Research Funding (PI or named investigator):Morphic:Active (exists now) ; Research Funding (PI or named investigator):Esperion:Active (exists now) ; Research Funding (PI or named investigator):Allinaire:Active (exists now) | Adrian Ray: No Answer | Blaise Lippa: DO have relevant financial relationships ; Employee:Morphic Therapeutic:Active (exists now) | Sebastien Bonnet: DO NOT have relevant financial relationships | Bryan Goodwin: DO have relevant financial relationships ; Employee:Morphic Tx:Active (exists now) ; Individual Stocks/Stock Options:Morphic Tx:Active (exists now) | Parmita Kapoor: No Answer | Min Lu: DO have relevant financial relationships ; Employee:Morphic Therapeutic, a wholly owned subsidiary of Eli Lilly and Company:Active (exists now) | Hailey Rapisardi: No Answer | Minh Hai Nguyen: DO NOT have relevant financial relationships | Haejin Kim: DO NOT have relevant financial relationships | MUZAFFAR AKRAM: DO NOT have relevant financial relationships | Dhawal Jain: No Answer | Elizabeth Konopka: No Answer
Meeting Info:

Scientific Sessions 2024

2024

Chicago, Illinois

Session Info:

The Next Frontier: Novel Molecular Mechanisms of Pulmonary Hypertension

Monday, 11/18/2024 , 09:30AM - 11:00AM

Moderated Digital Poster Session

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