International Journal of Molecular Sciences (Mar 2021)

Cardiac Oxidative Signaling and Physiological Hypertrophy in the Na/K-ATPase α1<sup>s/s</sup>α2<sup>s/s</sup> Mouse Model of High Affinity for Cardiotonic Steroids

  • Pauline V. Marck,
  • Marco T. Pessoa,
  • Yunhui Xu,
  • Laura C. Kutz,
  • Dominic M. Collins,
  • Yanling Yan,
  • Cierra King,
  • Xiaoliang Wang,
  • Qiming Duan,
  • Liquan Cai,
  • Jeffrey X. Xie,
  • Jerry B. Lingrel,
  • Zijian Xie,
  • Jiang Tian,
  • Sandrine V. Pierre

DOI
https://doi.org/10.3390/ijms22073462
Journal volume & issue
Vol. 22, no. 7
p. 3462

Abstract

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The Na/K-ATPase is the specific receptor for cardiotonic steroids (CTS) such as ouabain and digoxin. At pharmacological concentrations used in the treatment of cardiac conditions, CTS inhibit the ion-pumping function of Na/K-ATPase. At much lower concentrations, in the range of those reported for endogenous CTS in the blood, they stimulate hypertrophic growth of cultured cardiac myocytes through initiation of a Na/K-ATPase-mediated and reactive oxygen species (ROS)-dependent signaling. To examine a possible effect of endogenous concentrations of CTS on cardiac structure and function in vivo, we compared mice expressing the naturally resistant Na/K-ATPase α1 and age-matched mice genetically engineered to express a mutated Na/K-ATPase α1 with high affinity for CTS. In this model, total cardiac Na/K-ATPase activity, α1, α2, and β1 protein content remained unchanged, and the cardiac Na/K-ATPase dose–response curve to ouabain shifted to the left as expected. In males aged 3–6 months, increased α1 sensitivity to CTS resulted in a significant increase in cardiac carbonylated protein content, suggesting that ROS production was elevated. A moderate but significant increase of about 15% of the heart-weight-to-tibia-length ratio accompanied by an increase in the myocyte cross-sectional area was detected. Echocardiographic analyses did not reveal any change in cardiac function, and there was no fibrosis or re-expression of the fetal gene program. RNA sequencing analysis indicated that pathways related to energy metabolism were upregulated, while those related to extracellular matrix organization were downregulated. Consistent with a functional role of the latter, an angiotensin-II challenge that triggered fibrosis in the α1r/rα2s/s mouse failed to do so in the α1s/sα2s/s. Taken together, these results are indicative of a link between circulating CTS, Na/K-ATPase α1, ROS, and physiological cardiac hypertrophy in mice under baseline laboratory conditions.

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