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Iron deficiency as therapeutic target in heart failure: a translational approach. | LitMetric

AI Article Synopsis

  • Heart failure (HF) is a serious condition with a prognosis similar to cancer, often complicated by anemia and iron deficiency (ID), which worsen patient outcomes.
  • Iron plays a vital role in heart cell functions, including oxygen transport and energy production, and its deficiency affects heart stability and contractility.
  • Recent studies and clinical trials suggest that intravenous (IV) iron therapy may improve the health, quality of life, and prognosis for HF patients by addressing ID and enhancing heart muscle function.

Article Abstract

Heart failure (HF) is a potentially debilitating condition, with a prognosis comparable to many forms of cancer. It is often complicated by anemia and iron deficiency (ID), which have been shown to even further harm patients' functional status and hospitalization risk. Iron is a cellular micronutrient that is essential for oxygen uptake and transportation, as well as mitochondrial energy production. Iron is crucially involved in electrochemical stability, maintenance of structure, and contractility of cardiomyocytes. There is mounting evidence that ID indeed hampers the homeostasis of these properties. Animal model and stem cell research has verified these findings on the cellular level, while clinical trials that treat ID in HF patients have shown promising results in improving real patient outcomes, as electromechanically compromised cardiomyocytes translate to HF exacerbations and arrhythmias in patients. In this article, we review our current knowledge on the role of iron in cardiac muscle cells, the contribution of ID to anemia and HF pathophysiology and the capacity of IV iron therapy to ameliorate the patients' arrhythmogenic profile, quality of life, and prognosis.

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Source
http://dx.doi.org/10.1007/s10741-019-09815-zDOI Listing

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