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. 2019 Mar:128:77-89.
doi: 10.1016/j.yjmcc.2018.12.018. Epub 2019 Jan 3.

High-throughput single-molecule RNA imaging analysis reveals heterogeneous responses of cardiomyocytes to hemodynamic overload

Masahiro Satoh  1 Seitaro Nomura  2 Mutsuo Harada  3 Toshihiro Yamaguchi  3 Toshiyuki Ko  2 Tomokazu Sumida  3 Haruhiro Toko  3 Atsuhiko T Naito  3 Norifumi Takeda  3 Takashige Tobita  4 Takanori Fujita  5 Masamichi Ito  3 Kanna Fujita  3 Masato Ishizuka  3 Taro Kariya  3 Hiroshi Akazawa  3 Yoshio Kobayashi  6 Hiroyuki Morita  3 Eiki Takimoto  3 Hiroyuki Aburatani  7 Issei Komuro  8
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Free article

High-throughput single-molecule RNA imaging analysis reveals heterogeneous responses of cardiomyocytes to hemodynamic overload

Masahiro Satoh et al. J Mol Cell Cardiol. 2019 Mar.
Free article

Abstract

Background: The heart responds to hemodynamic overload through cardiac hypertrophy and activation of the fetal gene program. However, these changes have not been thoroughly examined in individual cardiomyocytes, and the relation between cardiomyocyte size and fetal gene expression remains elusive. We established a method of high-throughput single-molecule RNA imaging analysis of in vivo cardiomyocytes and determined spatial and temporal changes during the development of heart failure.

Methods and results: We applied three novel single-cell analysis methods, namely, single-cell quantitative PCR (sc-qPCR), single-cell RNA sequencing (scRNA-seq), and single-molecule fluorescence in situ hybridization (smFISH). Isolated cardiomyocytes and cross sections from pressure overloaded murine hearts after transverse aortic constriction (TAC) were analyzed at an early hypertrophy stage (2 weeks, TAC2W) and at a late heart failure stage (8 weeks, TAC8W). Expression of myosin heavy chain β (Myh7), a representative fetal gene, was induced in some cardiomyocytes in TAC2W hearts and in more cardiomyocytes in TAC8W hearts. Expression levels of Myh7 varied considerably among cardiomyocytes. Myh7-expressing cardiomyocytes were significantly more abundant in the middle layer, compared with the inner or outer layers of TAC2W hearts, while such spatial differences were not observed in TAC8W hearts. Expression levels of Myh7 were inversely correlated with cardiomyocyte size and expression levels of mitochondria-related genes.

Conclusions: We developed a new image-analysis pipeline to allow automated and unbiased quantification of gene expression at the single-cell level and determined the spatial and temporal regulation of heterogenous Myh7 expression in cardiomyocytes after pressure overload.

Keywords: Heart failure; Immunostaining; Single-cell spatial analysis; Single-molecule fluorescence in situ hybridization.

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