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Heart failure with preserved ejection fraction: insights into diagnosis and pathophysiology

Journal

CARDIOVASCULAR RESEARCH
Volume 117, Issue 4, Pages 999-1014

Publisher

OXFORD UNIV PRESS
DOI: 10.1093/cvr/cvaa228

Keywords

Diastole; Heart failure; Echocardiography; Haemodynamics; Diagnosis

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HFpEF is a prevalent form of heart failure with various cardiac and non-cardiac manifestations, diagnosis of which relies on multiple measurements. Despite increasing understanding of its pathophysiology, specific treatment for HFpEF patients remains elusive.
Heart failure with preserved ejection fraction (HFpEF) accounts for at least half the cases of heart failure, currently diagnosed. There are several cardiac and non-cardiac manifestations of the syndrome. Structure and function abnormalities can include all four cardiac chambers. The left ventricle has abnormal systolic and diastolic functions which can be examined by invasive and non-invasive measurements. In addition, the left atrium enlarges with abnormal left atrial function, pulmonary hypertension occurs, and the right ventricle can develop hypertrophy, enlargement, and systolic dysfunction. There are a paucity of data on calcium handling in HFpEF patients. Growing literature supports the presence of abnormalities in titin and its phosphorylation, and increased interstitial fibrosis contributing to increased chamber stiffness. A systemic inflammatory state causing reduced myocardial cyclic guanosine monophosphate along with defects in the unfolded protein response have been recently reported. Diagnosis relies on signs and symptoms of heart failure, preserved ejection fraction, and detection of diastolic function abnormalities based on echocardiographic findings and abnormally elevated natriuretic peptide levels or invasive measurements of wedge pressure at rest or with exercise. There are currently two diagnostic algorithms: H2FPEF, and HFA-PEFF with limited data comparing their performance head to head in the same patient population. Despite the growing understanding of the syndrome's pathophysiology, there have been little success in developing specific treatment for patients with HFpEF.

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