Pressure overload induces ISG15 to facilitate adverse ventricular remodeling and promote heart failure
Veera Ganesh Yerra, … , Kim A. Connelly, Andrew Advani
Veera Ganesh Yerra, … , Kim A. Connelly, Andrew Advani
Published May 1, 2023
Citation Information: J Clin Invest. 2023;133(9):e161453. https://doi.org/10.1172/JCI161453.
View: Text | PDF
Research Article Cardiology

Pressure overload induces ISG15 to facilitate adverse ventricular remodeling and promote heart failure

Abstract

Inflammation promotes adverse ventricular remodeling, a common antecedent of heart failure. Here, we set out to determine how inflammatory cells affect cardiomyocytes in the remodeling heart. Pathogenic cardiac macrophages induced an IFN response in cardiomyocytes, characterized by upregulation of the ubiquitin-like protein IFN-stimulated gene 15 (ISG15), which posttranslationally modifies its targets through a process termed ISGylation. Cardiac ISG15 is controlled by type I IFN signaling, and ISG15 or ISGylation is upregulated in mice with transverse aortic constriction or infused with angiotensin II; rats with uninephrectomy and DOCA-salt, or pulmonary artery banding; cardiomyocytes exposed to IFNs or CD4+ T cell–conditioned medium; and ventricular tissue of humans with nonischemic cardiomyopathy. By nanoscale liquid chromatography–tandem mass spectrometry, we identified the myofibrillar protein filamin-C as an ISGylation target. ISG15 deficiency preserved cardiac function in mice with transverse aortic constriction and led to improved recovery of mouse hearts ex vivo. Metabolomics revealed that ISG15 regulates cardiac amino acid metabolism, whereas ISG15 deficiency prevented misfolded filamin-C accumulation and induced cardiomyocyte autophagy. In sum, ISG15 upregulation is a feature of pathological ventricular remodeling, and protein ISGylation is an inflammation-induced posttranslational modification that may contribute to heart failure development by altering cardiomyocyte protein turnover.

Authors

Veera Ganesh Yerra, Sri Nagarjun Batchu, Harmandeep Kaur, MD Golam Kabir, Youan Liu, Suzanne L. Advani, Duc Tin Tran, Shadi Sadeghian, Phelopater Sedrak, Filio Billia, Uros Kuzmanov, Anthony O. Gramolini, Deema O. Qasrawi, Evgeniy V. Petrotchenko, Christoph H. Borchers, Kim A. Connelly, Andrew Advani

×

Figure 8

ISG15 associates with filamin-C in mouse and human hearts.

Options: View larger image (or click on image) Download as PowerPoint
ISG15 associates with filamin-C in mouse and human hearts. (A) Immunopre...
(A) Immunoprecipitation for filamin-C and immunoblotting for ISG15 in human cardiomyocytes following knockdown of ISG15 with siRNA and incubation with 500 IU/mL IFN-β for 48 hours (n = 3 per condition). (B and C) Dual immunofluorescence staining for ISG15 and filamin-C in the hearts of sham-operated mice and mice 1 week after TAC (B) and human control tissue and LV tissue from a human with NICM (C). Scale bars: 10 μm. Values are mean ± SD. *P < 0.05 by 1-way ANOVA followed by Dunnett’s post hoc test.