Cardiac fibroblast–derived microRNA passenger strand-enriched exosomes mediate cardiomyocyte hypertrophy
Claudia Bang, … , Jan Fiedler, Thomas Thum
Claudia Bang, … , Jan Fiedler, Thomas Thum
Published April 17, 2014
Citation Information: J Clin Invest. 2014;124(5):2136-2146. https://doi.org/10.1172/JCI70577.
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Cardiac fibroblast–derived microRNA passenger strand-enriched exosomes mediate cardiomyocyte hypertrophy

Abstract

In response to stress, the heart undergoes extensive cardiac remodeling that results in cardiac fibrosis and pathological growth of cardiomyocytes (hypertrophy), which contribute to heart failure. Alterations in microRNA (miRNA) levels are associated with dysfunctional gene expression profiles associated with many cardiovascular disease conditions; however, miRNAs have emerged recently as paracrine signaling mediators. Thus, we investigated a potential paracrine miRNA crosstalk between cardiac fibroblasts and cardiomyocytes and found that cardiac fibroblasts secrete miRNA-enriched exosomes. Surprisingly, evaluation of the miRNA content of cardiac fibroblast–derived exosomes revealed a relatively high abundance of many miRNA passenger strands (“star” miRNAs), which normally undergo intracellular degradation. Using confocal imaging and coculture assays, we identified fibroblast exosomal–derived miR-21_3p (miR-21*) as a potent paracrine-acting RNA molecule that induces cardiomyocyte hypertrophy. Proteome profiling identified sorbin and SH3 domain-containing protein 2 (SORBS2) and PDZ and LIM domain 5 (PDLIM5) as miR-21* targets, and silencing SORBS2 or PDLIM5 in cardiomyocytes induced hypertrophy. Pharmacological inhibition of miR-21* in a mouse model of Ang II–induced cardiac hypertrophy attenuated pathology. These findings demonstrate that cardiac fibroblasts secrete star miRNA–enriched exosomes and identify fibroblast-derived miR-21* as a paracrine signaling mediator of cardiomyocyte hypertrophy that has potential as a therapeutic target.

Authors

Claudia Bang, Sandor Batkai, Seema Dangwal, Shashi Kumar Gupta, Ariana Foinquinos, Angelika Holzmann, Annette Just, Janet Remke, Karina Zimmer, Andre Zeug, Evgeni Ponimaskin, Andreas Schmiedl, Xiaoke Yin, Manuel Mayr, Rashi Halder, Andre Fischer, Stefan Engelhardt, Yuanyuan Wei, Andreas Schober, Jan Fiedler, Thomas Thum

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Figure 1

Cardiac fibroblasts produce and secrete exosomes.

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Cardiac fibroblasts produce and secrete exosomes. (A and B) Electron mic...
(A and B) Electron microscopy images of rat cardiac fibroblasts. (A) Cytoplasm of rat cardiac fibroblasts with MVB. MVB membrane invaginated inward (arrows), forming intraluminal vesicles (inset: higher magnification of intraluminal vesicles; scale bar: 100 nm). (B) MVB fusing with the cell membrane. (A and B) Scale bar: 200 nm (n = 3). (C) Electron microscopy image of rat cardiac fibroblast–derived exosomes, showing a size of approximately 50 to 100 nm in diameter. Scale bar: 100 nm (n = 4). (D) Western Blot of fibroblast-derived exosomes for CD63 (60 kDa) and GAPDH (34 kDa). (E) Flow cytometry analysis of CD63 of fibroblast-derived exosomes. Fibroblast-derived exosomes were immunostained against CD63 (red curve) and compared with the appropriate isotype control (gray curve). (F and G) Total RNA from (F) rat cardiac fibroblasts and (G) fibroblast-derived exosomes was analyzed by bioanalyzer. Gels and electropherograms are shown. The left gel lane is the ladder standard and the right lane is the total RNA from (F) cardiac fibroblasts or (G) exosomes. Y axis of the electropherogram is the arbitrary fluorescence unit intensity (FU) and x axis is migration time in seconds (s). (H) Western blot analysis of NSMASE2 (84 kDa) and GAPDH (34 kDa) in neonatal rat cardiac fibroblast lysates (n = 3).