Single Nuclei Sequencing Reveals Novel Insights Into the Regulation of Cellular Signatures in Children With Dilated Cardiomyopathy | Zendy

Luka Nicin | Zendy; Wesley Abplanalp | Zendy; Anne Schänzer | Zendy; A. Sprengel | Zendy; David John | Zendy; Hannah Mellentin | Zendy; Lukas Tombor | Zendy; Matthias Keuper | Zendy; Evelyn Ullrich | Zendy; Karin Klingel | Zendy; R. Dettmeyer | Zendy; Jedrzej Hoffmann | Zendy; Hakan Akintuerk | Zendy; Christian Jux | Zendy; Dietmar Schranz | Zendy; Andreas M. Zeiher | Zendy; Stefan Rupp | Zendy; Stefanie Dimmeler | Zendy

Open Access

Single Nuclei Sequencing Reveals Novel Insights Into the Regulation of Cellular Signatures in Children With Dilated Cardiomyopathy

Author(s) -

Luka Nicin,

Wesley Abplanalp,

Anne Schänzer,

A. Sprengel,

David John,

Hannah Mellentin,

Lukas Tombor,

Matthias Keuper,

Evelyn Ullrich,

Karin Klingel,

R. Dettmeyer,

Jedrzej Hoffmann,

Hakan Akintuerk,

Christian Jux,

Dietmar Schranz,

Andreas M. Zeiher,

Stefan Rupp,

Stefanie Dimmeler

Publication year - 2021

Publication title -

circulation

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 7.795

H-Index - 607

eISSN - 1524-4539

pISSN - 0009-7322

DOI - 10.1161/circulationaha.120.051391

Subject(s) - dilated cardiomyopathy , medicine , heart failure , transcriptome , cardiomyopathy , cardiac fibrosis , population , lmna , bioinformatics , pathology , gene , genetics , gene expression , lamin , biology , environmental health

Background: Dilated cardiomyopathy (DCM) is a leading cause of death in children with heart failure. The outcome of pediatric heart failure treatment is inconsistent, and large cohort studies are lacking. Progress may be achieved through personalized therapy that takes age- and disease-related pathophysiology, pathology, and molecular fingerprints into account. We present single nuclei RNA sequencing from pediatric patients with DCM as the next step in identifying cellular signatures. Methods: We performed single nuclei RNA sequencing with heart tissues from 6 children with DCM with an age of 0.5, 0.75, 5, 6, 12, and 13 years. Unsupervised clustering of 18 211 nuclei led to the identification of 14 distinct clusters with 6 major cell types. Results: The number of nuclei in fibroblast clusters increased with age in patients with DCM, a finding that was confirmed by histological analysis and was consistent with an age-related increase in cardiac fibrosis quantified by cardiac magnetic resonance imaging. Fibroblasts of patients with DCM >6 years of age showed a profoundly altered gene expression pattern with enrichment of genes encoding fibrillary collagens, modulation of proteoglycans, switch in thrombospondin isoforms, and signatures of fibroblast activation. In addition, a population of cardiomyocytes with a high proregenerative profile was identified in infant patients with DCM but was absent in children >6 years of age. This cluster showed high expression of cell cycle activators such ascyclin D family members, increased glycolytic metabolism and antioxidative genes, and alterations in ß-adrenergic signaling genes.Conclusions: Novel insights into the cellular transcriptomes of hearts from pediatric patients with DCM provide remarkable age-dependent changes in the expression patterns of fibroblast and cardiomyocyte genes with less fibrotic but enriched proregenerative signatures in infants.

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