Essential Role for Trf2 in Cardiac Development and Function

Ali Hakim Shoushtari
Aysenur Danis
Michael Wayne Stoner
Jeffrey Baust
Andrea Sebastiani
Paramesha Bugga
Janet R Manning
Bellina A S Mushala
Nisha Bhattarai
Imad Al Ghouleh
Iain Scott
Maryam Sharifi-Sanjani

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Abstract

Telomere Repeat-binding Factor 2 (Trf2) is essential for protecting our telomeres. While Trf2 global deletion is lethal, its role in organ-specific development, particularly in the heart, remains less understood. In this study, we investigated the role of Trf2 in cardiac development and function. Our studies reveal that cardiomyocyte (CM)-specific loss of Trf2 leads to profound defects in heart morphology, including impaired ventricular wall formation and compromised CM proliferation, concurrent with no CM telomere length attrition. Further, in vivo functional assessment and molecular analyses of CM-Trf2 deficient ventricles revealed severe cardiac dysfunction and, interestingly, altered nuclear envelope gene expression, respectively. Our work provides new insights into the essential role of Trf2 in heart development and function, and potential avenues for therapeutic intervention targeting telomere biology.

Version published to 10.1101/2025.09.24.677933 on bioRxiv
Sep 30, 2025

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Essential Role for Trf2 in Cardiac Development and Function

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ZEB1 Is a Key Regulator of Cardiomyocyte Structure and Function

Endothelial expression of ZBTB16 protects against cardiac aging

Loss of Regulator of telomere elongation helicase (Rtel1) impairs alveolar epithelial cell progenitor function but does not exacerbate experimental fibrosis

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ZEB1 Is a Key Regulator of Cardiomyocyte Structure and Function

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