In vivo proximity proteomics uncovers palmdelphin (PALMD) as a Z-line-associated mitigator of isoproterenol-induced cardiac injury

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  • Author: Congting Guo, Blake D. Jardin, Junsen Lin, Rachelle L. Ambroise, Ze Wang, Luzi Yang, Neil Mazumdar, Fujian Lu, Qing Ma, Yangpo Cao, Canzhao Liu, Xujie Liu, Feng Lan, Mingming Zhao, Han Xiao, Erdan Dong, William T. Pu and Yuxuan Guo
  • Journal: BioRxiv
  • Doi: https://www.doi.org/10.1101/2023.12.06.570334
  • Publication Date: 2023 Dec 7

Products/Services used in the paper

Quotation shows PackGene:Alternatively, AAV9 was packaged at PackGene Biotech

Research Field:Cardic

AAV Serotype:AAV9

Targeted organ:heart

Animal or cell line strain:pups

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Abstract

Z-lines are core ultrastructural organizers of cardiomyocytes that modulate many facets of cardiac pathogenesis. Yet a comprehensive proteomic atlas of Z-line-associated components remain incomplete. Here, we established an adeno-associated virus (AAV)-delivered, cardiomyocyte-specific, proximity-labeling approach to characterize the Z-line proteome in vivo. We found palmdelphin (PALMD) as a novel Z-line-associated protein in both adult murine cardiomyocytes and human pluripotent stem cell-derived cardiomyocytes. Germline and cardiomyocyte-specific palmd knockout mice were grossly normal at baseline but exhibited compromised cardiac hypertrophy and aggravated cardiac injury upon long-term isoproterenol treatment. By contrast, cardiomyocyte-specific PALMD overexpression was sufficient to mitigate isoproterenol-induced cardiac injury. PALMD ablation perturbed transverse tubules (T-tubules) and their association with sarcoplasmic reticulum, which formed the Z-line-associated junctional membrane complex (JMC) essential for calcium handling and cardiac function. These phenotypes were associated with disrupted localization of T-tubule markers caveolin-3 (CAV3) and junctophilin-2 (JPH2) and the reduction of nexilin (NEXN) protein, a crucial Z-line-associated protein that is essential for both Z-line and JMC structures and functions. PALMD was found to interact with NEXN and enhance its protein stability while the Nexn mRNA level was not affected. Together, this study discovered PALMD as a potential target for myocardial protection and highlighted in vivo proximity proteomics as a powerful approach to nominate novel players regulating cardiac pathogenesis.

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