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Selective titin cleavage disrupts cardiac mechanical homeostasis to drive heart failure and fibrosisOpen Access

Freundt, Johanna K.; Hartmann, Paulina; Loescher, Christine M.; Unger, Andreas; Koser, Franziska; Klotz, Annika J.; Wildschütz, Lena; Wachsmuth, Lydia; Hille, Susanne; Door, Michaela M.; Helfen, Anne; Holtmeier, Richard; Faber, Cornelius; Kirk, Jonathan A.; Hoerr, Verena; Müller, Oliver J.; Linke, Wolfgang A.

Forschungsartikel (Zeitschrift) | Peer reviewed

Zusammenfassung

Titin, the largest human protein, forms the elastic sarcomeric backbone, providing passive stiffness and length-dependent activation in cardiomyocytes. Whereas titin mutations cause inherited cardiomyopathies, ischemic and chemotherapy-induced injury also provoke proteolytic cleavage of titin’s elastic segment. However, the effects of acute titin stiffness loss remain unknown. Here we develop a knock-in mouse enabling in vivo cleavage of cardiac titin springs and use multimodal analysis (cardiac magnetic resonance imaging, echocardiography, microscopy, omics) to show that titin cleavage does not dilate the heart but reduces chamber size and impairs ventricular filling. Mechanical assays of isolated cardiomyocytes reveal diminished restoring forces causing a loss of elastic recoil. In vivo cleavage disrupts junctions, including integrin linkages and connexin 43 gap junctions, widens intermyocyte space without hypertrophy or hyperplasia and drives fibroblast activation, extracellular matrix remodeling and fibrosis. Compensatory mechanisms fail, leading to decompensated heart failure. These findings establish that proteolytic titin cleavage perturbs cardiac mechanical homeostasis, driving disease and matrix stiffening.

Details zur Publikation

FachzeitschriftNature Cardiovascular Research (Nat Cardiovasc Res)
StatusVeröffentlicht
Veröffentlichungsjahr2026 (16.06.2026)
Stichwörtertitin; cardiac mechanical homeostasis; cardiomyocytes restoring forces

Autor*innen der Universität Münster

Faber, Cornelius Joachim
Klinik für Radiologie
Freundt, Johanna
Institut für Physiologie II
Hörr, Verena
Klinik für Radiologie
Koser, Franziska
Institut für Physiologie II
Unger, Andreas
Institut für Genetik von Herzerkrankungen (IfGH)
Wachsmuth, Lydia
Klinik für Radiologie