Simultaneous Pharmacologic Inhibition of Yes‐Associated Protein 1 and Glutaminase 1 via Inhaled Poly(Lactic‐co‐Glycolic) Acid–Encapsulated Microparticles Improves Pulmonary Hypertension

Abhinav P. Acharya; Ying Tang; Thomas Bertero; Yi‐Yin Tai; Lloyd D. Harvey; Chen‐Shan C. Woodcock; Wei Sun; Ricardo Pineda; Nilay Mitash; Melanie Königshoff; Steven R. Little; Stephen Y. Chan

doi:10.1161/JAHA.120.019091

Journal of the American Heart Association: Cardiovascular and Cerebrovascular Disease (Jun 2021)

Simultaneous Pharmacologic Inhibition of Yes‐Associated Protein 1 and Glutaminase 1 via Inhaled Poly(Lactic‐co‐Glycolic) Acid–Encapsulated Microparticles Improves Pulmonary Hypertension

Abhinav P. Acharya,
Ying Tang,
Thomas Bertero,
Yi‐Yin Tai,
Lloyd D. Harvey,
Chen‐Shan C. Woodcock,
Wei Sun,
Ricardo Pineda,
Nilay Mitash,
Melanie Königshoff,
Steven R. Little,
Stephen Y. Chan

Affiliations

Abhinav P. Acharya: Department of Chemical and Petroleum Engineering University of Pittsburgh PA
Ying Tang: Center for Pulmonary Vascular Biology and Medicine Pittsburgh Heart, Lung, and Blood Vascular Medicine Institute Division of Cardiology Department of Medicine University of Pittsburgh School of Medicine PA
Thomas Bertero: Université Côte d'AzurCentre national de la recherche scientifique (CNRS) Bienvenue à l'Institut de Pharmacologie Moléculaire et Cellulaire (IPMC) Valbonne France
Yi‐Yin Tai: Center for Pulmonary Vascular Biology and Medicine Pittsburgh Heart, Lung, and Blood Vascular Medicine Institute Division of Cardiology Department of Medicine University of Pittsburgh School of Medicine PA
Lloyd D. Harvey: Center for Pulmonary Vascular Biology and Medicine Pittsburgh Heart, Lung, and Blood Vascular Medicine Institute Division of Cardiology Department of Medicine University of Pittsburgh School of Medicine PA
Chen‐Shan C. Woodcock: Center for Pulmonary Vascular Biology and Medicine Pittsburgh Heart, Lung, and Blood Vascular Medicine Institute Division of Cardiology Department of Medicine University of Pittsburgh School of Medicine PA
Wei Sun: Center for Pulmonary Vascular Biology and Medicine Pittsburgh Heart, Lung, and Blood Vascular Medicine Institute Division of Cardiology Department of Medicine University of Pittsburgh School of Medicine PA
Ricardo Pineda: Division of Pulmonary, Allergy, and Critical Care Medicine Department of Medicine University of Pittsburgh School of Medicine PA
Nilay Mitash: Division of Pulmonary, Allergy, and Critical Care Medicine Department of Medicine University of Pittsburgh School of Medicine PA
Melanie Königshoff: Division of Pulmonary, Allergy, and Critical Care Medicine Department of Medicine University of Pittsburgh School of Medicine PA
Steven R. Little: Department of Chemical and Petroleum Engineering University of Pittsburgh PA
Stephen Y. Chan: Center for Pulmonary Vascular Biology and Medicine Pittsburgh Heart, Lung, and Blood Vascular Medicine Institute Division of Cardiology Department of Medicine University of Pittsburgh School of Medicine PA

DOI: https://doi.org/10.1161/JAHA.120.019091
Journal volume & issue: Vol. 10, no. 12

Abstract

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Background Pulmonary hypertension (PH) is a deadly disease characterized by vascular stiffness and altered cellular metabolism. Current treatments focus on vasodilation and not other root causes of pathogenesis. Previously, it was demonstrated that glutamine metabolism, as catalyzed by GLS1 (glutaminase 1) activity, is mechanoactivated by matrix stiffening and the transcriptional coactivators YAP1 (yes‐associated protein 1) and transcriptional coactivator with PDZ‐binding motif (TAZ), resulting in pulmonary vascular proliferation and PH. Pharmacologic inhibition of YAP1 (by verteporfin) or glutaminase (by CB‐839) improved PH in vivo. However, systemic delivery of these agents, particularly YAP1 inhibitors, may have adverse chronic effects. Furthermore, simultaneous use of pharmacologic blockers may offer additive or synergistic benefits. Therefore, a strategy that delivers these drugs in combination to local lung tissue, thus avoiding systemic toxicity and driving more robust improvement, was investigated. Methods and Results We used poly(lactic‐co‐glycolic) acid polymer‐based microparticles for delivery of verteporfin and CB‐839 simultaneously to the lungs of rats suffering from monocrotaline‐induced PH. Microparticles released these drugs in a sustained fashion and delivered their payload in the lungs for 7 days. When given orotracheally to the rats weekly for 3 weeks, microparticles carrying this drug combination improved hemodynamic (right ventricular systolic pressure and right ventricle/left ventricle+septum mass ratio), histologic (vascular remodeling), and molecular markers (vascular proliferation and stiffening) of PH. Importantly, only the combination of drug delivery, but neither verteporfin nor CB‐839 alone, displayed significant improvement across all indexes of PH. Conclusions Simultaneous, lung‐specific, and controlled release of drugs targeting YAP1 and GLS1 improved PH in rats, addressing unmet needs for the treatment of this deadly disease.

Published in Journal of the American Heart Association: Cardiovascular and Cerebrovascular Disease

ISSN: 2047-9980 (Online)
Publisher: Wiley
Country of publisher: United States
LCC subjects: Medicine: Internal medicine: Specialties of internal medicine: Diseases of the circulatory (Cardiovascular) system
Website: https://www.ahajournals.org/journal/jaha

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