Reduced Fetuin-A Levels Are Associated With Exercise Intolerance and Predict the Risk of Adverse Outcomes in Patients With Heart Failure: The Role of Cardiac-Hepatic-Peripheral Interaction

Exercise intolerance in heart failure arises from multifactorial pathophysiological mechanisms. Hepatokines, liver-synthesized molecules, regulate systemic metabolisms in peripheral tissues. We previously identified the hepatokine fetuin-A as being linked to liver hypoperfusion in heart failure. Her...

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Veröffentlicht in:Journal of the American Heart Association 2024-09, Vol.13 (17), p.e035139
Hauptverfasser: Tomita, Yusuke, Misaka, Tomofumi, Sugawara, Yukiko, Ichijo, Yasuhiro, Anzai, Fumiya, Sato, Yu, Kimishima, Yusuke, Yokokawa, Tetsuro, Sato, Takamasa, Oikawa, Masayoshi, Kobayashi, Atsushi, Yoshihisa, Akiomi, Takeishi, Yasuchika
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Sprache:eng
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Zusammenfassung:Exercise intolerance in heart failure arises from multifactorial pathophysiological mechanisms. Hepatokines, liver-synthesized molecules, regulate systemic metabolisms in peripheral tissues. We previously identified the hepatokine fetuin-A as being linked to liver hypoperfusion in heart failure. Here, we investigated the role of fetuin-A in connecting cardiac-hepatic-peripheral interaction. We conducted a prospective study involving 202 consecutive hospitalized patients (mean age, 56.8 years; 76.2% men) with heart failure who underwent cardiopulmonary exercise testing. We measured the serum concentration of fetuin-A by ELISA. Correlation analysis revealed a negative association between fetuin-A levels and the ratio of minimum minute ventilation to carbon dioxide production, its slope, and a tendency toward a positive correlation with peak oxygen uptake. Patients with impaired exercise tolerance exhibited lower fetuin-A levels. During a median follow-up of 1045 days, 18.3% experienced cardiac events, including 4 cardiac deaths and 33 cases of worsening heart failure. Classification and regression tree analysis identified a high-risk subgroup with lower fetuin-A (
ISSN:2047-9980
2047-9980
DOI:10.1161/JAHA.124.035139