Preventing Site-Specific Calpain Proteolysis of Junctophilin-2 Protects Against Stress-Induced Excitation-Contraction Uncoupling and Heart Failure Development

Jinxi Wang; Biyi Chen; Qian Shi; Grace Ciampa; Weiyang Zhao; Guangqin Zhang; Robert M Weiss; Tianqing Peng; Duane D Hall; Long-Sheng Song

doi:10.1161/CIRCULATIONAHA.124.069329

Preventing Site-Specific Calpain Proteolysis of Junctophilin-2 Protects Against Stress-Induced Excitation-Contraction Uncoupling and Heart Failure Development

Circulation. 2024 Sep 18. doi: 10.1161/CIRCULATIONAHA.124.069329. Online ahead of print.

Authors

Jinxi Wang^#¹, Biyi Chen^#¹, Qian Shi¹, Grace Ciampa², Weiyang Zhao¹, Guangqin Zhang¹, Robert M Weiss^{1

3}, Tianqing Peng⁴, Duane D Hall¹, Long-Sheng Song^{1

2

5

3}

Affiliations

¹ Division of Cardiovascular Medicine, Department of Internal Medicine, Abboud Cardiovascular Research Center, Carver College of Medicine, University of Iowa, Iowa City. (J.W., B.C., Q.S., W.Z., G.Z. R.M.W., D.D.H., L.-S.S.).
² Department of Biochemistry and Molecular Biology, Carver College of Medicine, University of Iowa, Iowa City. (G.C., L.-S.S.).
³ Department of Veterans Affairs Medical Center, Iowa City, IA (R.M.W., L.-S.S.).
⁴ Department of Pathology and Laboratory Medicine, University of Western Ontario, London, Canada (T.P.).
⁵ Fraternal Order of Eagles Diabetes Research Center, Carver College of Medicine, University of Iowa, Iowa City. (L.-S.S.).

^# Contributed equally.

PMID: 39291390
DOI: 10.1161/CIRCULATIONAHA.124.069329

Abstract

Background: Excitation-contraction (E-C) coupling processes become disrupted in heart failure (HF), resulting in abnormal Ca²⁺ homeostasis, maladaptive structural and transcriptional remodeling, and cardiac dysfunction. Junctophilin-2 (JP2) is an essential component of the E-C coupling apparatus but becomes site-specifically cleaved by calpain, leading to disruption of E-C coupling, plasmalemmal transverse tubule degeneration, abnormal Ca²⁺ homeostasis, and HF. However, it is not clear whether preventing site-specific calpain cleavage of JP2 is sufficient to protect the heart against stress-induced pathological cardiac remodeling in vivo.

Methods: Calpain-resistant JP2 knock-in mice (JP2^CR) were generated by deleting the primary JP2 calpain cleavage site. Stress-dependent JP2 cleavage was assessed through in vitro cleavage assays and in isolated cardiomyocytes treated with 1 μmol/L isoproterenol by immunofluorescence. Cardiac outcomes were assessed in wild-type and JP2^CR mice 5 weeks after transverse aortic constriction compared with sham surgery using echocardiography, histology, and RNA-sequencing methods. E-C coupling efficiency was measured by in situ confocal microscopy. E-C coupling proteins were evaluated by calpain assays and Western blotting. The effectiveness of adeno-associated virus gene therapy with JP2^CR, JP2, or green fluorescent protein to slow HF progression was evaluated in mice with established cardiac dysfunction.

Results: JP2 proteolysis by calpain and in response to transverse aortic constriction and isoproterenol was blocked in JP2^CR cardiomyocytes. JP2^CR hearts are more resistant to pressure-overload stress, having significantly improved Ca²⁺ homeostasis and transverse tubule organization with significantly attenuated cardiac dysfunction, hypertrophy, lung edema, fibrosis, and gene expression changes relative to wild-type mice. JP2^CR preserves the integrity of calpain-sensitive E-C coupling-related proteins, including ryanodine receptor 2, Ca_V1.2, and sarcoplasmic reticulum calcium ATPase 2a, by attenuating transverse aortic constriction-induced increases in calpain activity. Furthermore, JP2^CR gene therapy after the onset of cardiac dysfunction was found to be effective at slowing the progression of HF and superior to wild-type JP2.

Conclusions: The data presented here demonstrate that preserving JP2-dependent E-C coupling by prohibiting the site-specific calpain cleavage of JP2 offers multifaceted beneficial effects, conferring cardiac protection against stress-induced proteolysis, hypertrophy, and HF. Our data also indicate that specifically targeting the primary calpain cleavage site of JP2 by gene therapy approaches holds great therapeutic potential as a novel precision medicine for treating HF.

Keywords: calpain; excitation contraction coupling; heart failure; junctophilin; proteolysis.