| Literature DB >> 35755006 |
Gabriele G Schiattarella1,2,3,4,5, Pilar Alcaide6, Gianluigi Condorelli7,8, Thomas G Gillette5, Stephane Heymans9,10, Elizabeth A V Jones9,10, Marinos Kallikourdis7,11, Andrew Lichtman12, Federica Marelli-Berg13, Sanjiv Shah14, Edward B Thorp15, Joseph A Hill5,16.
Abstract
Heart failure with preserved ejection fraction (HFpEF) is increasing in prevalence worldwide, already accounting for at least half of all heart failure (HF). As most patients with HFpEF are obese with metabolic syndrome, metabolic stress has been implicated in syndrome pathogenesis. Recently, compelling evidence for bidirectional crosstalk between metabolic stress and chronic inflammation has emerged, and alterations in systemic and cardiac immune responses are held to participate in HFpEF pathophysiology. Indeed, based on both preclinical and clinical evidence, comorbidity-driven systemic inflammation, coupled with metabolic stress, have been implicated together in HFpEF pathogenesis. As metabolic alterations impact immune function(s) in HFpEF, major changes in immune cell metabolism are also recognized in HFpEF and in HFpEF-predisposing conditions. Both arms of immunity - innate and adaptive - are implicated in the cardiomyocyte response in HFpEF. Indeed, we submit that crosstalk among adipose tissue, the immune system, and the heart represents a critical component of HFpEF pathobiology. Here, we review recent evidence in support of immunometabolic mechanisms as drivers of HFpEF pathogenesis, discuss pivotal biological mechanisms underlying the syndrome, and highlight questions requiring additional inquiry.Entities:
Keywords: HFpEF; immune system; metabolism
Year: 2022 PMID: 35755006 PMCID: PMC9229992 DOI: 10.1038/s44161-022-00032-w
Source DB: PubMed Journal: Nat Cardiovasc Res ISSN: 2731-0590