A Non‐Metallic Nanozyme Ameliorates Pulmonary Hypertension Through Inhibiting ROS/TGF‐β1 Signaling

Author:

Liu Ruxia1ORCID,Zhou Ting23,Li Xinsheng2,Zou Quan45,Yu Jiaojiao2,Ye Jingjing6,Wang Wenhui7,Zhou Yan8,Sun Shao‐Kai2ORCID

Affiliation:

1. Department of Rehabilitation School of Medical Technology Tianjin Medical University Tianjin 300203 China

2. School of Medical Imaging Tianjin Medical University Tianjin 300203 China

3. Department of CT Shaanxi Provincial People's Hospital Xi'an Shaanxi Province 710068 China

4. School of Medical Imaging Tianjin Key Laboratory of Functional Imaging Tianjin Medical University Tianjin 300203 China

5. Department of Radiology The Second Hospital of Tianjin Medical University Tianjin 300211 China

6. Trauma Treatment Center Peking University People's Hospital Key Laboratory of Trauma Treatment and Neural Regeneration (Peking University) Ministry of Education National Center for Trauma Medicine Beijing 100044 China

7. Department of Endocrinology The Second Hospital of Tianjin Medical University Tianjin 300211 China

8. Department of Ultrasound Tianjin Third Central Hospital Tianjin 300170 China

Abstract

AbstractPulmonary hypertension (PH) is a life‐threatening cardiovascular disease with a lack of effective treatment options. Nanozymes, though promising for PH therapy, pose safety risks due to their metallic nature. Here, a non‐metallic nanozyme is reported for the treatment of monocrotaline (MCT)‐induced PH with a therapeutic mechanism involving the ROS/TGF‐β1 signaling. The synthesized melanin‐polyvinylpyrrolidone‐polyethylene glycol (MPP) nanoparticles showcase ultra‐small size, excellent water solubility, high biocompatibility, and remarkable antioxidant capacity. The MPP nanoparticles are capable of effectively eliminating ROS in isolated pulmonary artery smooth muscle cells (PASMCs) from PH rats, and significantly reduce PASMC proliferation and migration. In vivo results from a PH model demonstrate that MPP nanoparticles significantly increase pulmonary artery acceleration time, decrease wall thickening and PCNA expression in lung tissues, as evidenced by echocardiograpy, histology and immunoblot analysis. Additionally, MPP nanoparticles treatment improve running capacity, decrease Fulton index, and attenuate right ventricular fibrosis in MCT‐PH rats by using treadmill test, picrosirius red, and trichrome Masson staining. Further transcriptomic and biochemical analyses reveal that inhibiting ROS‐driven activation of TGF‐β1 in the PA is the mechanism by which MPP nanoparticles exert their therapeutic effect. This study provides a novel approach for treating PH with non‐metallic nanozymes based on a well‐understood mechanism.

Publisher

Wiley

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