Vaccine Therapy for Heart Failure Targeting the Inflammatory Cytokine Igfbp7-Reference-Cited by-同舟云学术

Vaccine Therapy for Heart Failure Targeting the Inflammatory Cytokine Igfbp7

Published:2024-07-30 Issue:5 Volume:150 Page:374-389
ISSN:0009-7322
Container-title:Circulation
language:en
Short-container-title:Circulation

Author:

Katoh Manami¹²³^ORCID,Nomura Seitaro¹²³^ORCID,Yamada Shintaro¹^ORCID,Ito Masamichi¹,Hayashi Hiroki⁴,Katagiri Mikako¹^ORCID,Heryed Tuolisi¹,Fujiwara Takayuki¹^ORCID,Takeda Norifumi¹^ORCID,Nishida Miyuki⁵,Sugaya Maki⁵,Kato Miki⁵,Osawa Tsuyoshi⁵^ORCID,Abe Hiroyuki⁶^ORCID,Sakurai Yoshitaka⁷,Ko Toshiyuki¹²^ORCID,Fujita Kanna¹^ORCID,Zhang Bo¹,Hatsuse Satoshi¹^ORCID,Yamada Takanobu¹^ORCID,Inoue Shunsuke²^ORCID,Dai Zhehao¹^ORCID,Kubota Masayuki¹^ORCID,Sawami Kousuke¹,Ono Minoru⁸^ORCID,Morita Hiroyuki¹,Kubota Yoshiaki⁹^ORCID,Mizuno Seiya¹⁰^ORCID,Takahashi Satoru¹⁰^ORCID,Nakanishi Makoto¹¹^ORCID,Ushiku Tetsuo⁶,Nakagami Hironori¹^ORCID,Aburatani Hiroyuki³^ORCID,Komuro Issei²¹⁰^ORCID

Affiliation:

1. Departments of Cardiovascular Medicine (M.Katoh, S.N., S.Y., M.I., M.Katagiri, T.H., T.F., N.T., T.K., K.F., B.Z., S.H., T.Y., S.I., Z.D., M.Kubota, K.S., H.M., I.K.), The University of Tokyo, Japan.

2. Frontier Cardiovascular Science (M.Katoh, T.K., S.I., S.N., I.K.), The University of Tokyo, Japan.

3. Genome Science Division (M.Katoh, S.N., H. Aburatani), The University of Tokyo, Japan.

4. Department of Health Development and Medicine, Graduate School of Medicine, Osaka University, Suita, Japan (H.H., H.N.).

5. Division of Integrative Nutriomics and Oncology, Research Center for Advanced Science and Technology (M. Nishida, M.S., M.K., T.O.), The University of Tokyo, Japan.

6. Pathology (H. Abe, T.U.), The University of Tokyo, Japan.

7. Diabetes and Metabolic Diseases, Graduate School of Medicine (Y.S.), The University of Tokyo, Japan.

8. Cardiothoracic Surgery (M.O.), The University of Tokyo, Japan.

9. Department of Anatomy, Keio University School of Medicine, Tokyo, Japan (Y.K.).

10. Laboratory Animal Resource Center, Transborder Medical Research Center, Institute of Medicine, University of Tsukuba, Ibaraki, Japan (S.M., S.T.).

11. Division of Cancer Cell Biology, The Institute of Medical Science (M. Nakanishi), The University of Tokyo, Japan.

Abstract

BACKGROUND: The heart comprises many types of cells such as cardiomyocytes, endothelial cells (ECs), fibroblasts, smooth muscle cells, pericytes, and blood cells. Every cell type responds to various stressors (eg, hemodynamic overload and ischemia) and changes its properties and interrelationships among cells. To date, heart failure research has focused mainly on cardiomyocytes; however, other types of cells and their cell-to-cell interactions might also be important in the pathogenesis of heart failure. METHODS: Pressure overload was imposed on mice by transverse aortic constriction and the vascular structure of the heart was examined using a tissue transparency technique. Functional and molecular analyses including single-cell RNA sequencing were performed on the hearts of wild-type mice and EC-specific gene knockout mice. Metabolites in heart tissue were measured by capillary electrophoresis-time of flight-mass spectrometry system. The vaccine was prepared by conjugating the synthesized epitope peptides with keyhole limpet hemocyanin and administered to mice with aluminum hydroxide as an adjuvant. Tissue samples from heart failure patients were used for single-nucleus RNA sequencing to examine gene expression in ECs and perform pathway analysis in cardiomyocytes. RESULTS: Pressure overload induced the development of intricately entwined blood vessels in murine hearts, leading to the accumulation of replication stress and DNA damage in cardiac ECs. Inhibition of cell proliferation by a cyclin-dependent kinase inhibitor reduced DNA damage in ECs and ameliorated transverse aortic constriction–induced cardiac dysfunction. Single-cell RNA sequencing analysis revealed upregulation of Igfbp7 (insulin-like growth factor-binding protein 7) expression in the senescent ECs and downregulation of insulin signaling and oxidative phosphorylation in cardiomyocytes of murine and human failing hearts. Overexpression of Igfbp7 in the murine heart using AAV9 (adeno-associated virus serotype 9) exacerbated cardiac dysfunction, while EC-specific deletion of Igfbp7 and the vaccine targeting Igfbp7 ameliorated cardiac dysfunction with increased oxidative phosphorylation in cardiomyocytes under pressure overload. CONCLUSIONS: Igfbp7 produced by senescent ECs causes cardiac dysfunction and vaccine therapy targeting Igfbp7 may be useful to prevent the development of heart failure.

Publisher

Ovid Technologies (Wolters Kluwer Health)

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