The direct effect of lipopolysaccharide on an isolated heart is different from the effect on cardiac myocytes in vitro

• Published in: Archives of medical science Vol. 19; no. 1; pp. 216 - 228
• Main Authors: Kuo, Feng Yu, Lee, Shu Ping, Cheng, Juei-Tang, Wu, Ming Chang
• Format: Journal Article
• Language: English
• Published: Poland Termedia Publishing House 01.01.2023
• Subjects: cardiac contractility; Experimental Research; jak/stat pathway; langendorff apparatus; lipopolysaccharide; toll-like receptor 4; Langendorff apparatus; cardiac contractility; lipopolysaccharide; JAK/STAT pathway; Toll-like receptor 4
• ISSN: 1734-1922; 1896-9151
• DOI: 10.5114/aoms.2019.86976

Lipopolysaccharide (LPS) is widely used to induce experimental animals. However, its effects on cardiac contraction is controversial. Although LPS probably induces its influence both directly and indirectly, we focused on the direct effects of LPS in this report. Isolated ventricular myocytes mounted on a Langendorff apparatus were perfused with LPS. The changes in cultured H9c2 cells incubated with LPS over a 3-h exposure were compared with the changes after a 24-h incubation. Apoptosis was identified using flow cytometry and Western blotting. The mRNA levels were also determined. LPS directly stimulated cardiac contractility at low doses, although it produced inhibition at higher doses. The TLR4-coupled JAK2/STAT3 pathway was identified in H9c2 cells after LPS treatment, with an increase in intracellular calcium levels. LPS dose-dependently activated hypertrophic signals in H9c2 cells and induced apoptosis at the high dose. However, apoptosis was observed in H9c2 cells after a 24-h exposure to LPS, even at low doses. This observation appears to be associated with the level of paracrine cytokines. Changes in H9c2 cells by LPS were diminished by NPS2390, an inhibitor of the calcium-sensing receptor (CaSR). LPS also promoted CaSR mRNA expression in H9c2 cells, which may be unrelated to the changes in cytokine expression influenced by an inflammasome inhibitor. In contrast to the isolated hearts, LPS activated hypertrophic signals prior to apoptotic signals in cardiac cells. Thus, LPS injury appears to be associated with CaSR, which was not markedly influenced by an inflammasome inhibitor.