iScience (Jan 2024)

Impact of sacubitril/valsartan on cardiac and systemic hypoxia in chronic heart failure

  • Hélène Nougué,
  • François Picard,
  • Alain Cohen-Solal,
  • Damien Logeart,
  • Jean-Marie Launay,
  • Nicolas Vodovar

Journal volume & issue
Vol. 27, no. 1
p. 108520

Abstract

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Summary: In heart failure patients with reduced ejection fraction, Sacubitril/valsartan (S/V) increased proBNP T71 glycosylation, which is regulated negatively by hypoxia via miR-30a in vitro. Using a cohort of 73 HFrEF patients who were transitioned from standard HF medication to S/V, we found that the increase in proBNP T71 glycosylation after S/V was associated with a decrease in cardiac hypoxia. We further found that plasma levels of K709-acteylated HIF1α, HIF-regulated and HIF-independent biomarkers also evolved consistently with a decrease in hypoxia. We further confirmed that biomarker changes were related to hypoxia, in a rat model subjected to isobaric hypoxia. We measured them in rats subjected to isobaric hypoxia. Overall, these data strongly suggest that optimally treated HFrEF patients exhibited subclinical hypoxia that is improved by S/V. The data also posit proBNP T71 glycosylation as a biomarker of cardiac hypoxia.

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