Your search keyword '"Filippatos, Gerasimos' showing total 1,211 results

1. Sodium–glucose co‐transporter 2 inhibitors as an early, first‐line therapy in patients with heart failure and reduced ejection fraction

Author

Tomasoni, Daniela, Fonarow, Gregg C, Adamo, Marianna, Anker, Stefan D, Butler, Javed, Coats, Andrew JS, Filippatos, Gerasimos, Greene, Stephen J, McDonagh, Theresa A, Ponikowski, Piotr, Rosano, Giuseppe, Seferovic, Petar, Vaduganathan, Muthiah, Voors, Adriaan A, and Metra, Marco

Subjects

Biomedical and Clinical Sciences, Clinical Sciences, Patient Safety, Diabetes, Cardiovascular, Heart Disease, Clinical Research, 5.1 Pharmaceuticals, 6.1 Pharmaceuticals, Evaluation of treatments and therapeutic interventions, Development of treatments and therapeutic interventions, Metabolic and endocrine, Good Health and Well Being, Diabetes Mellitus, Type 2, Glucose, Heart Failure, Humans, Quality of Life, Sodium, Sodium-Glucose Transporter 2 Inhibitors, Stroke Volume, Symporters, Heart failure with reduced ejection fraction, Sodium-glucose co-transporter 2 inhibitors, Dapagliflozin, Empagliflozin, Sotagliflozin, Medical therapy, Cardiorespiratory Medicine and Haematology, Cardiovascular System & Hematology, Cardiovascular medicine and haematology

Abstract

Sodium-glucose co-transporter 2 (SGLT2) inhibitors have recently been recommended as a foundational therapy for patients with heart failure (HF) and reduced ejection fraction (HFrEF) because of their favourable effects on mortality, clinical events and quality of life. While clinical practice guidelines have recommended dapagliflozin or empagliflozin in all patients with HFrEF, or sotagliflozin in those with HFrEF and concomitant diabetes, the timing and practical integration of these drugs in clinical practice is less well defined. We propose that these drugs are candidates for early, upfront administration to patients with newly diagnosed HFrEF and for patients hospitalized with HF. Growing evidence has established early benefits, with clinically meaningful reductions in clinical events that reach statistical significance within days to weeks, following dapagliflozin, empagliflozin or, in diabetic patients, sotagliflozin initiation. Secondly, although major clinical trials have tested these drugs in patients already receiving background HF therapy, secondary analyses showed that their efficacy is independent of that. Third, SGLT2 inhibitors are generally safe and well tolerated, with clinical trial data reporting minimal effects on blood pressure, glycaemia-related adverse events, and no excess in acute kidney injury. Rather, they exert renal protective effects and reduce risk of hyperkalaemia, properties that favour initiation, tolerance and persistence of renin-angiotensin system inhibitors and mineralocorticoid receptor antagonists. This review supports the early initiation of dapagliflozin and empagliflozin (or sotagliflozin limited to patients with diabetes) to rapidly improve clinical outcome and quality of life of HFrEF patients.

Published

2022

2. Decongestion discriminates risk for one-year mortality in patients with improving renal function in acute heart failure.

Author

Wettersten, Nicholas, Horiuchi, Yu, van Veldhuisen, Dirk, Ix, Joachim, Mueller, Christian, Filippatos, Gerasimos, Nowak, Richard, Hogan, Christopher, Kontos, Michael, Cannon, Chad, Müeller, Gerhard, Birkhahn, Robert, Taub, Pam, Vilke, Gary, Duff, Stephen, McDonald, Kenneth, Mahon, Niall, Nuñez, Julio, Briguori, Carlo, Passino, Claudio, Maisel, Alan, and Murray, Patrick

Subjects

Acute heart failure, B-type natriuretic peptide, Congestion, Kidney function, Prognosis, Acute Disease, Aged, Biomarkers, Heart Failure, Humans, Kidney, Male, Natriuretic Peptide, Brain, Prognosis

Abstract

AIMS: Improving renal function (IRF) is paradoxically associated with worse outcomes in acute heart failure (AHF), but outcomes may differ based on response to decongestion. We explored if the relationship of IRF with mortality in hospitalized AHF patients differs based on successful decongestion. METHODS AND RESULTS: We evaluated 760 AHF patients from AKINESIS for the relationship between IRF, change in B-type natriuretic peptide (BNP), and 1-year mortality. IRF was defined as a ≥20% increase in estimated glomerular filtration rate (eGFR) relative to admission. Adequate decongestion was defined as a ≥40% decrease in last measured BNP relative to admission. IRF occurred in 22% of patients who had a mean age of 69 years, 58% were men, 72% were white, and median admission eGFR was 49 mL/min/1.73 m2 . IRF patients had more severe heart failure reflected by lower admission eGFR, higher blood urea nitrogen, lower systolic blood pressure, lower sodium, and higher use of inotropes. IRF patients had higher 1-year mortality (25%) than non-IRF patients (15%) (P

Published

2021

3. Percutaneous repair of moderate‐to‐severe or severe functional mitral regurgitation in patients with symptomatic heart failure: Baseline characteristics of patients in the RESHAPE‐HF2 trial and comparison to COAPT and MITRA‐FR trials

Author

Anker, Stefan D., primary, Friede, Tim, additional, von Bardeleben, Ralph Stephan, additional, Butler, Javed, additional, Khan, Muhammad Shahzeb, additional, Diek, Monika, additional, Heinrich, Jutta, additional, Geyer, Martin, additional, Placzek, Marius, additional, Ferrari, Roberto, additional, Abraham, William T., additional, Alfieri, Ottavio, additional, Auricchio, Angelo, additional, Bayes‐Genis, Antoni, additional, Cleland, John G.F., additional, Filippatos, Gerasimos, additional, Gustafsson, Finn, additional, Haverkamp, Wilhelm, additional, Kelm, Malte, additional, Kuck, Karl‐Heinz, additional, Landmesser, Ulf, additional, Maggioni, Aldo P., additional, Metra, Marco, additional, Ninios, Vlasis, additional, Petrie, Mark C., additional, Rassaf, Tienush, additional, Ruschitzka, Frank, additional, Schäfer, Ulrich, additional, Schulze, P. Christian, additional, Spargias, Konstantinos, additional, Vahanian, Alec, additional, Zamorano, Jose Luis, additional, Zeiher, Andreas, additional, Karakas, Mahir, additional, Koehler, Friedrich, additional, Lainscak, Mitja, additional, Öner, Alper, additional, Mezilis, Nikolaos, additional, Theofilogiannakos, Efstratios K, additional, Ninios, Ilias, additional, Chrissoheris, Michael, additional, Kourkoveli, Panagiota, additional, Papadopoulos, Konstantinos, additional, Smolka, Grzegorz, additional, Wojakowski, Wojciech, additional, Reczuch, Krzysztof, additional, Pinto, Fausto J., additional, Zmudka, Krzysztof, additional, Kalarus, Zbigniew, additional, Adamo, Marianna, additional, Santiago‐Vacas, Evelyn, additional, Ruf, Tobias Friedrich, additional, Gross, Michael, additional, Tongers, Joern, additional, Hasenfuß, Gerd, additional, Schillinger, Wolfgang, additional, and Ponikowski, Piotr, additional

Published

2024

4. Medication dosing for heart failure with reduced ejection fraction — opportunities and challenges

Author

Marti, Catherine N, Fonarow, Gregg C, Anker, Stefan D, Yancy, Clyde, Vaduganathan, Muthiah, Greene, Stephen J, Ahmed, Ali, Januzzi, James L, Gheorghiade, Mihai, Filippatos, Gerasimos, and Butler, Javed

Subjects

Pharmacology and Pharmaceutical Sciences, Biomedical and Clinical Sciences, Clinical Trials and Supportive Activities, Clinical Research, Cardiovascular, Cardiovascular Agents, Dose-Response Relationship, Drug, Heart Failure, Humans, Patient Selection, Practice Guidelines as Topic, Stroke Volume, Heart failure, Reduced ejection fraction, Medications, Doses, Outcomes, Cardiorespiratory Medicine and Haematology, Cardiovascular System & Hematology, Cardiovascular medicine and haematology

Abstract

Multiple drug classes have shown incremental benefits in heart failure with reduced ejection fraction. Most of these trials were designed to achieve specific doses of the investigational agent. Clinical practice guidelines recommend using the same target dosing of therapies, as tolerated. However, with the increasing number of available therapies, clinicians face the challenge of simultaneously using several drugs, achieving target doses, and managing side effects that are often overlapping. Blood pressure, renal function, hyperkalaemia, and other factors may impede achieving target doses of all medications, leaving clinicians with dilemmas as to how to sequence and dose these various classes of drugs. The guideline-directed eligibility for certain drugs and devices requires stability on maximally tolerated doses of background therapies. However, significant variability exists in dosing achieved in clinical practice. We discuss the existing background data regarding the doses of heart failure medications in clinical trials and in practice, and provide recommendations on how to navigate this complex therapeutic decision-making.

Published

2019

5. Burst steroid therapy for acute heart failure: The CORTAHF randomized, open‐label, pilot trial.

Author

Cotter, Gad, Davison, Beth A., Freund, Yonathan, Voors, Adriaan A., Edwards, Christopher, Novosadova, Maria, Takagi, Koji, Hayrapetyan, Hamlet, Mshetsyan, Andranik, Mayranush, Drambyan, Cohen‐Solal, Alain, ter Maaten, Jozine M., Biegus, Jan, Ponikowski, Piotr, Filippatos, Gerasimos, Chioncel, Ovidiu, Sadoune, Malha, Pagnesi, Matteo, Simon, Tabassome, and Metra, Marco

Subjects

HEART failure patients, STEROID drugs, PEPTIDES, HEART failure, VISUAL analog scale, RESPIRATORY diseases

Abstract

Aims: Burst steroid therapy, effective in acute respiratory diseases, may benefit patients with acute heart failure (AHF) in whom inflammatory activation is associated with adverse outcomes. Methods and results: CORTAHF assessed whether burst steroid therapy reduces inflammation and results in better quality of life and clinical outcomes in AHF. Patients with AHF, N‐terminal pro‐B‐type natriuretic peptide >1500 pg/ml, and high‐sensitivity C‐reactive protein (hsCRP) >20 mg/L were randomized 1:1 to oral, once daily 40 mg prednisone for 7 days or usual care, without blinding. Patients were followed for 90 days. A total of 101 patients were randomized. At day 7 the primary endpoint, hsCRP decreased in both arms – adjusted geometric mean ratios (GMRs) were 0.30 and 0.40 in the prednisone and usual care arms (ratio of GMRs 0.75, 95% confidence interval [CI] 0.56–1.00, p = 0.0498). The 90‐day risk of worsening heart failure (HF), HF readmission or death as reported by the unblinded investigators was significantly lower in the prednisone group (10.4%) than in usual care (30.8%) (hazard ratio 0.31, 95% CI 0.11–0.86, p = 0.016). The EQ‐5D visual analogue scale score as reported by the unblinded patients increased more in the prednisone group on day 7 (least squares mean difference 2.57, 95% CI 0.12–5.01 points, p = 0.040). All effects were statistically significant in the pre‐specified subgroup with centrally‐measured interleukin‐6 >13 pg/ml. Adverse events, particularly hyperglycaemia, occurred more in the prednisone group with no difference in infection rate. Conclusion: In this small open‐label study of patients with AHF, burst steroid therapy was associated with reduced inflammation as measured by hsCRP levels at day 7 (primary endpoint). Secondary endpoints showed improved quality of life at day 7 and reduced 90‐day risk of death or worsening HF. Large prospective studies are needed to evaluate these findings. [ABSTRACT FROM AUTHOR]

Published

2024

6. The right heart in patients with cancer. A scientific statement of the Heart Failure Association (HFA) of the ESC and the ESC Council of Cardio‐Oncology.

Author

Keramida, Kalliopi, Farmakis, Dimitrios, Rakisheva, Amina, Tocchetti, Carlo Gabriele, Ameri, Pietro, Asteggiano, Riccardo, Barac, Ana, Bax, Jeroen, Bayes‐Genis, Antoni, Bergler Klein, Jutta, Bucciarelli‐Ducci, Chiara, Celutkiene, Jelena, Coats, Andrew J.S., Cohen Solal, Alain, Dent, Susan, Filippatos, Gerasimos, Ghosh, Arjun, Hermann, Joerg, Koop, Yvonne, and Lenihan, Daniel

Subjects

GLOBAL longitudinal strain, CARDIAC amyloidosis, HEART failure, SINGLE-photon emission computed tomography, LOW-molecular-weight heparin, RIGHT ventricular dysfunction, SPECKLE tracking echocardiography

Published

2024

7. Similar clinical benefits from below‐target and target dose enalapril in patients with heart failure in the SOLVD Treatment trial

Author

Lam, Phillip H, Dooley, Daniel J, Fonarow, Gregg C, Butler, Javed, Bhatt, Deepak L, Filippatos, Gerasimos S, Deedwania, Prakash, Forman, Daniel E, White, Michel, Fletcher, Ross D, Arundel, Cherinne, Blackman, Marc R, Adamopoulos, Chris, Kanonidis, Ioannis E, Aban, Inmaculada B, Patel, Kanan, Aronow, Wilbert S, Allman, Richard M, Anker, Stefan D, Pitt, Bertram, and Ahmed, Ali

Subjects

Pharmacology and Pharmaceutical Sciences, Biomedical and Clinical Sciences, Clinical Sciences, Cardiovascular, Clinical Research, Clinical Trials and Supportive Activities, Heart Disease, Evaluation of treatments and therapeutic interventions, 6.1 Pharmaceuticals, Good Health and Well Being, Angiotensin-Converting Enzyme Inhibitors, Canada, Cause of Death, Dose-Response Relationship, Drug, Double-Blind Method, Enalapril, Europe, Follow-Up Studies, Heart Failure, Humans, Stroke Volume, Survival Rate, Treatment Outcome, United States, ACE inhibitors, Target dose, Placebo, Heart failure, Cardiorespiratory Medicine and Haematology, Cardiovascular System & Hematology, Cardiovascular medicine and haematology

Abstract

AimsTo examine associations of below-target and target dose of enalapril, an angiotensin-converting enzyme (ACE) inhibitor, with outcomes in patients with heart failure and reduced ejection fraction (HFrEF) in the Studies of Left Ventricular Dysfunction (SOLVD) Treatment trial.Methods and resultsTwo thousand five hundred and sixty-nine patients with HFrEF (ejection fraction ≤35%) were randomized to below-target (5-10 mg/day) dose placebo (n = 1284) or enalapril (n = 1285). One month post-randomization, blind up-titration to target (20 mg/day) dose was attempted for both study drugs in 2458 patients. Among the 1444 patients who achieved dose up-titration (placebo, n = 748; enalapril, n = 696; mean dose for both groups, 20.0 mg/day), target dose enalapril (vs. target dose placebo) was associated with a 9% absolute lower risk of the combined endpoint of heart failure hospitalization or all-cause mortality [adjusted hazard ratio (HR) 0.70; 95% confidence interval (CI) 0.60-0.81; P < 0.001] during 4 years of follow-up. Among the 1014 patients who could not achieve target dose (placebo, n = 486; enalapril, n = 528; mean dose for both groups, 8.8 mg/day), below-target dose enalapril (vs. below-target dose placebo) was associated with a 12% absolute lower risk of the combined endpoint of heart failure hospitalization or all-cause mortality (adjusted HR 0.68; 95% CI 0.57-0.81; P < 0.001). Among the 1224 patients receiving enalapril, target (vs. below-target) dose had no association with the combined endpoint of heart failure hospitalization or all-cause mortality (adjusted HR 1.04; 95% CI 0.87-1.23; P = 0.695).ConclusionIn patients with HFrEF, the clinical benefits of ACE inhibitors appear to be similar at both below-target and target doses.

Published

2018

8. Differences in presentation, diagnosis and management of heart failure in women. A scientific statement of the Heart Failure Association of the ESC

Author

Rosano, Giuseppe M.C., primary, Stolfo, Davide, additional, Anderson, Lisa, additional, Abdelhamid, Magdy, additional, Adamo, Marianna, additional, Bauersachs, Johann, additional, Bayes‐Genis, Antoni, additional, Böhm, Michael, additional, Chioncel, Ovidiu, additional, Filippatos, Gerasimos, additional, Hill, Loreena, additional, Lainscak, Mitja, additional, Lambrinou, Ekaterini, additional, Maas, Angela H.E.M., additional, Massouh, Angela R., additional, Moura, Brenda, additional, Petrie, Mark C., additional, Rakisheva, Amina, additional, Ray, Robin, additional, Savarese, Gianluigi, additional, Skouri, Hadi, additional, Van Linthout, Sophie, additional, Vitale, Cristiana, additional, Volterrani, Maurizio, additional, Metra, Marco, additional, and Coats, Andrew J.S., additional

Published

2024

9. Baseline characteristics of patients with heart failure with mildly reduced or preserved ejection fraction: The FINEARTS‐HF trial

Author

Solomon, Scott D., primary, Ostrominski, John W., additional, Vaduganathan, Muthiah, additional, Claggett, Brian, additional, Jhund, Pardeep S., additional, Desai, Akshay S., additional, Lam, Carolyn S.P., additional, Pitt, Bertram, additional, Senni, Michele, additional, Shah, Sanjiv J., additional, Voors, Adriaan A., additional, Zannad, Faiez, additional, Abidin, Imran Zainal, additional, Alcocer‐Gamba, Marco Antonio, additional, Atherton, John J., additional, Bauersachs, Johann, additional, Ma, Chang‐Sheng, additional, Chiang, Chern‐En, additional, Chioncel, Ovidiu, additional, Chopra, Vijay, additional, Comin‐Colet, Josep, additional, Filippatos, Gerasimos, additional, Fonseca, Cândida, additional, Gajos, Grzegorz, additional, Goland, Sorel, additional, Goncalvesová, Eva, additional, Kang, Seok‐Min, additional, Katova, Tzvetana, additional, Kosiborod, Mikhail N., additional, Latkovskis, Gustavs, additional, Lee, Alex Pui‐Wai, additional, Linssen, Gerard C.M., additional, Llamas‐Esperón, Guillermo, additional, Mareev, Vyacheslav, additional, Martinez, Felipe A., additional, Melenovský, Vojtěch, additional, Merkely, Béla, additional, Nodari, Savina, additional, Petrie, Mark C., additional, Saldarriaga, Clara Inés, additional, Saraiva, Jose Francisco Kerr, additional, Sato, Naoki, additional, Schou, Morten, additional, Sharma, Kavita, additional, Troughton, Richard, additional, Udell, Jacob A., additional, Ukkonen, Heikki, additional, Vardeny, Orly, additional, Verma, Subodh, additional, von Lewinski, Dirk, additional, Voronkov, Leonid G., additional, Yilmaz, Mehmet Birhan, additional, Zieroth, Shelley, additional, Lay‐Flurrie, James, additional, van Gameren, Ilse, additional, Amarante, Flaviana, additional, Viswanathan, Prabhakar, additional, and McMurray, John J.V., additional

Published

2024

10. Dietary sodium and fluid intake in heart failure. A clinical consensus statement of the Heart Failure Association of the ESC

Author

Mullens, Wilfried, primary, Damman, Kevin, additional, Dhont, Sebastiaan, additional, Banerjee, Debasish, additional, Bayes‐Genis, Antoni, additional, Cannata, Antonio, additional, Chioncel, Ovidiu, additional, Cikes, Maja, additional, Ezekowitz, Justin, additional, Flammer, Andreas J., additional, Martens, Pieter, additional, Mebazaa, Alexandre, additional, Mentz, Robert J., additional, Miró, Òscar, additional, Moura, Brenda, additional, Nunez, Julio, additional, Ter Maaten, Jozine M., additional, Testani, Jeffrey, additional, van Kimmenade, Roland, additional, Verbrugge, Frederik H., additional, Metra, Marco, additional, Rosano, Giuseppe M.C., additional, and Filippatos, Gerasimos, additional

Published

2024

11. Body mass index and cardiorenal outcomes in the EMPEROR‐Preserved trial: Principal findings and meta‐analysis with the DELIVER trial

Author

Sattar, Naveed, primary, Butler, Javed, additional, Lee, Matthew M.Y., additional, Harrington, Josephine, additional, Sharma, Abhinav, additional, Zannad, Faiez, additional, Filippatos, Gerasimos, additional, Verma, Subodh, additional, Januzzi, James L., additional, Ferreira, João Pedro, additional, Pocock, Stuart J., additional, Pfarr, Egon, additional, Ofstad, Anne P., additional, Brueckmann, Martina, additional, Packer, Milton, additional, and Anker, Stefan D., additional

Published

2024

12. Blood pressure and intensive treatment up‐titration after acute heart failure hospitalization: Insights from the STRONG‐HF trial

Author

Pagnesi, Matteo, primary, Vilamajó, Oscar Alberto Gomez, additional, Meiriño, Alejandro, additional, Dumont, Carlos Alberto, additional, Mebazaa, Alexandre, additional, Davison, Beth, additional, Adamo, Marianna, additional, Arrigo, Mattia, additional, Barros, Marianela, additional, Biegus, Jan, additional, Celutkiene, Jelena, additional, Čerlinskaitė‐Bajorė, Kamilė, additional, Chioncel, Ovidiu, additional, Cohen‐Solal, Alain, additional, Damasceno, Albertino, additional, Diaz, Rafael, additional, Edwards, Christopher, additional, Filippatos, Gerasimos, additional, Gayat, Etienne, additional, Kimmoun, Antoine, additional, Lam, Carolyn S.P., additional, Novosadova, Maria, additional, Pang, Peter S., additional, Ponikowski, Piotr, additional, Saidu, Hadiza, additional, Sliwa, Karen, additional, Takagi, Koji, additional, ter Maaten, Jozine M., additional, Tomasoni, Daniela, additional, Voors, Adriaan A., additional, Cotter, Gad, additional, and Metra, Marco, additional

Published

2024

13. Empagliflozin and risk of lower respiratory tract infection in heart failure with mildly reduced and preserved ejection fraction: An EMPEROR‐Preserved analysis

Author

Ferreira, João Pedro, primary, Zannad, Faiez, additional, Packer, Milton, additional, Filippatos, Gerasimos, additional, Pocock, Stuart J., additional, Vasques‐Nóvoa, Francisco, additional, Böhm, Michael, additional, Butler, Javed, additional, and Anker, Stefan, additional

Published

2024

14. Organ dysfunction, injury and failure in acute heart failure: from pathophysiology to diagnosis and management. A review on behalf of the Acute Heart Failure Committee of the Heart Failure Association (HFA) of the European Society of Cardiology (ESC).

Author

Harjola, Veli-Pekka, Mullens, Wilfried, Banaszewski, Marek, Bauersachs, Johann, Brunner-La Rocca, Hans-Peter, Chioncel, Ovidiu, Collins, Sean, Doehner, Wolfram, Filippatos, Gerasimos, Flammer, Andreas, Fuhrmann, Valentin, Lainscak, Mitja, Lassus, Johan, Legrand, Matthieu, Masip, Josep, Mueller, Christian, Papp, Zoltán, Parissis, John, Platz, Elke, Rudiger, Alain, Ruschitzka, Frank, Schäfer, Andreas, Seferovic, Petar, Skouri, Hadi, Yilmaz, Mehmet, and Mebazaa, Alexandre

Subjects

Heart failure, Multiple organ failure, Venous congestion, Acute Disease, Cardiology, Diagnostic Imaging, Disease Management, Europe, Heart Failure, Humans, Multiple Organ Failure, Societies, Medical

Abstract

Organ injury and impairment are commonly observed in patients with acute heart failure (AHF), and congestion is an essential pathophysiological mechanism of impaired organ function. Congestion is the predominant clinical profile in most patients with AHF; a smaller proportion presents with peripheral hypoperfusion or cardiogenic shock. Hypoperfusion further deteriorates organ function. The injury and dysfunction of target organs (i.e. heart, lungs, kidneys, liver, intestine, brain) in the setting of AHF are associated with increased risk for mortality. Improvement in organ function after decongestive therapies has been associated with a lower risk for post-discharge mortality. Thus, the prevention and correction of organ dysfunction represent a therapeutic target of interest in AHF and should be evaluated in clinical trials. Treatment strategies that specifically prevent, reduce or reverse organ dysfunction remain to be identified and evaluated to determine if such interventions impact mortality, morbidity and patient-centred outcomes. This paper reflects current understanding among experts of the presentation and management of organ impairment in AHF and suggests priorities for future research to advance the field.

Published

2017

15. Serelaxin in addition to standard therapy in acute heart failure: rationale and design of the RELAX‐AHF‐2 study

Author

Teerlink, John R, Voors, Adriaan A, Ponikowski, Piotr, Pang, Peter S, Greenberg, Barry H, Filippatos, Gerasimos, Felker, G Michael, Davison, Beth A, Cotter, Gad, Gimpelewicz, Claudio, Boer‐Martins, Leandro, Wernsing, Margaret, Hua, Tsushung A, Severin, Thomas, and Metra, Marco

Subjects

Biomedical and Clinical Sciences, Clinical Sciences, Patient Safety, Cardiovascular, Clinical Trials and Supportive Activities, Clinical Research, Aging, Heart Disease, Evaluation of treatments and therapeutic interventions, 6.1 Pharmaceuticals, Good Health and Well Being, Acute Disease, Aged, Cause of Death, Dose-Response Relationship, Drug, Double-Blind Method, Europe, Female, Follow-Up Studies, Heart Failure, Humans, Incidence, Infusions, Intravenous, Male, Recombinant Proteins, Relaxin, Renal Insufficiency, Survival Rate, Time Factors, Treatment Outcome, United States, Acute heart failure, Serelaxin, Worsening heart failure, Mortality, Phase 3 trial, Cardiorespiratory Medicine and Haematology, Cardiovascular System & Hematology, Cardiovascular medicine and haematology

Abstract

Patients admitted for acute heart failure (AHF) experience high rates of in-hospital and post-discharge morbidity and mortality despite current therapies. Serelaxin is recombinant human relaxin-2, a hormone with vasodilatory and end-organ protective effects believed to play a central role in the cardiovascular and renal adaptations of human pregnancy. In the phase 3 RELAX-AHF trial, serelaxin met its primary endpoint of improving dyspnoea through day 5 in patients admitted for AHF. Compared to placebo, serelaxin also reduced worsening heart failure (WHF) by 47% through day 5 and both all-cause and cardiovascular mortality by 37% through day 180. RELAX-AHF-2 ( ClinicalTrials.gov NCT01870778) is designed to confirm serelaxin's effect on these clinical outcomes. RELAX-AHF-2 is a multicentre, randomized, double-blind, placebo-controlled, event-driven, phase 3 trial enrolling ∼6800 patients hospitalized for AHF with dyspnoea, congestion on chest radiograph, increased natriuretic peptide levels, mild-to-moderate renal insufficiency, and systolic blood pressure ≥125 mmHg. Patients are randomized within 16 h of presentation to 48 h intravenous infusions of serelaxin (30 µg/kg/day) or placebo, both in addition to standard of care treatments. The primary objectives are to demonstrate that serelaxin is superior to placebo in reducing: (i) 180 day cardiovascular death, and (ii) occurrence of WHF through day 5. Key secondary endpoints include 180 day all-cause mortality, composite of 180 day combined cardiovascular mortality or heart failure/renal failure rehospitalization, and in-hospital length of stay during index AHF. The results from RELAX-AHF-2 will provide data on the potential beneficial effect of serelaxin on cardiovascular mortality and WHF in selected patients with AHF.

Published

2017

16. Biologically active adrenomedullin as a marker for residual congestion and early rehospitalization in patients hospitalized for acute heart failure: Data from STRONG‐HF.

Author

Voordes, Geert, Davison, Beth, Biegus, Jan, Edwards, Christopher, Damman, Kevin, ter Maaten, Jozine, Mebazaa, Alexandre, Takagi, Koji, Adamo, Marianna, Ambrosy, Andrew P., Arrigo, Mattia, Barros, Marianela, Celutkiene, Jelena, Čerlinskaitė‐Bajorė, Kamilė, Chioncel, Ovidiu, Cohen‐Solal, Alain, Damasceno, Albertino, Deniau, Benjamin, Diaz, Rafael, and Filippatos, Gerasimos

Subjects

ADRENOMEDULLIN, HEART failure, PATIENT readmissions, BRAIN natriuretic factor

Abstract

Aims: Biologically active adrenomedullin (bio‐ADM) is a promising marker of residual congestion. The STRONG‐HF trial showed that high‐intensity care (HIC) of guideline‐directed medical therapy (GDMT) improved congestion and clinical outcomes in heart failure (HF) patients. The association between bio‐ADM, decongestion, outcomes and the effect size of HIC of GDMT remains to be elucidated. Methods and results: We measured plasma bio‐ADM concentrations in 1005 patients within 2 days prior to anticipated discharge (baseline) and 90 days later. Bio‐ADM correlated with most signs of congestion, with the exception of rales. Changes in bio‐ADM were strongly correlated with change in congestion status from baseline to day 90 (gamma −0.24; p = 0.0001). Patients in the highest tertile of baseline bio‐ADM concentrations were at greater risk than patients in the lowest tertile for the primary outcome of 180‐day all‐cause mortality or HF rehospitalization (hazard ratio [HR] 2.14, 95% confidence interval [CI] 1.42–3.22) and 180‐day HF rehospitalization (HR 2.33, 95% CI 1.38–3.94). Areas under the receiver‐operating characteristic curves were 0.5977 (95% CI 0.5561–0.6393), 0.5800 (95% CI 0.5356–0.6243), and 0.6159 (95% CI 0.5711–0.6607) for bio‐ADM, N‐terminal pro‐B‐type natriuretic peptide (NT‐proBNP) and their combination, respectively, suggesting that both bio‐ADM and NT‐proBNP provided similarly modest discrimination for this outcome. A trend towards better discrimination by combined bio‐ADM and NT‐proBNP than NT‐proBNP alone was found (p = 0.059). HIC improved the primary outcome, irrespective of baseline bio‐ADM concentration (interaction p = 0.37). In contrast to NT‐proBNP, the 90‐day change in bio‐ADM did not differ significantly between HIC and usual care. Conclusions: Bio‐ADM is a marker of congestion and predicts congestion at 3 months after a HF hospitalization. Higher bio‐ADM was modestly associated with a higher risk of death and early hospital readmission and may have added value when combined with NT‐proBNP. [ABSTRACT FROM AUTHOR]

Published

2024

17. Early changes in estimated glomerular filtration rate post‐initiation of empagliflozin in EMPEROR‐Preserved

Author

Rastogi, Tripti, primary, Ferreira, João Pedro, additional, Butler, Javed, additional, Kraus, Bettina Johanna, additional, Mattheus, Michaela, additional, Brueckmann, Martina, additional, Filippatos, Gerasimos, additional, Wanner, Christoph, additional, Pocock, Stuart J., additional, Packer, Milton, additional, Anker, Stefan D., additional, and Zannad, Faiez, additional

Published

2024

18. The effect of sodium–glucose cotransporter 2 inhibitors on left cardiac remodelling in heart failure with reduced ejection fraction: Systematic review and meta‐analysis

Author

Usman, Muhammad Shariq, primary, Januzzi, James L., additional, Anker, Stefan D., additional, Salman, Ali, additional, Parikh, Puja B., additional, Adamo, Marianno, additional, Filippatos, Gerasimos, additional, Khan, Muhammad Shahzeb, additional, Lala, Anuradha, additional, Verma, Subodh, additional, Metra, Marco, additional, and Butler, Javed, additional

Published

2024

19. Epidemiology, pathophysiology, diagnosis and management of chronic right‐sided heart failure and tricuspid regurgitation. A clinical consensus statement of the Heart Failure Association (HFA) and the European Association of Percutaneous Cardiovascular Interventions (EAPCI) of the ESC

Author

Adamo, Marianna, primary, Chioncel, Ovidiu, additional, Pagnesi, Matteo, additional, Bayes‐Genis, Antoni, additional, Abdelhamid, Magdy, additional, Anker, Stefan D., additional, Antohi, Elena‐Laura, additional, Badano, Luigi, additional, Ben Gal, Tuvia, additional, Böhm, Michael, additional, Delgado, Victoria, additional, Dreyfus, Julien, additional, Faletra, Francesco F., additional, Farmakis, Dimitrios, additional, Filippatos, Gerasimos, additional, Grapsa, Julia, additional, Gustafsson, Finn, additional, Hausleiter, Jörg, additional, Jaarsma, Tiny, additional, Karam, Nicole, additional, Lund, Lars, additional, Lurz, Philipp, additional, Maisano, Francesco, additional, Moura, Brenda, additional, Mullens, Wilfred, additional, Praz, Fabien, additional, Sannino, Anna, additional, Savarese, Gianluigi, additional, Tocchetti, Carlo Gabriele, additional, van Empel, Vanessa P.M., additional, von Bardeleben, Ralph Stephan, additional, Yilmaz, Mehmet Birhan, additional, Zamorano, José Luis, additional, Ponikowski, Piotr, additional, Barbato, Emanuele, additional, Rosano, Giuseppe M.C., additional, and Metra, Marco, additional

Published

2024

20. European Society of Cardiology Core Curriculum for Cardio‐Oncology

Author

López‐Fernández, Teresa, primary, Farmakis, Dimitrios, additional, Ameri, Pietro, additional, Asteggiano, Riccardo, additional, de Azambuja, Evandro, additional, Aznar, Marianne, additional, Barac, Ana, additional, Bayes‐Genis, Antoni, additional, Bax, Jeroen J., additional, Bergler‐Klein, Jutta, additional, Boriani, Giuseppe, additional, Celutkiene, Jelena, additional, Coats, Andrew, additional, Cohen‐Solal, Alain, additional, Córdoba, Raúl, additional, Cosyns, Bernard, additional, Filippatos, Gerasimos, additional, Fox, Kevin, additional, Gulati, Geeta, additional, Inciardi, Riccardo M., additional, Lee, Geraldine, additional, Mamas, Mamas A., additional, Novo, Giuseppina, additional, Plummer, Chris, additional, Psyrri, Amanda, additional, Rakisheva, Amina, additional, Suter, Thomas, additional, Tini, Giacomo, additional, Tocchetti, Carlo Gabriele, additional, Toutouzas, Konstantinos, additional, Wilhelm, Matthias, additional, Metra, Marco, additional, Lyon, Alexander R., additional, and Rosano, Giuseppe M. C., additional

Published

2023

21. European Society of Cardiology Core Curriculum for cardio‐oncology.

Author

López‐Fernández, Teresa, Farmakis, Dimitrios, Ameri, Pietro, Asteggiano, Riccardo, de Azambuja, Evandro, Aznar, Marianne, Barac, Ana, Bayes‐Genis, Antoni, Bax, Jeroen J., Bergler‐Klein, Jutta, Boriani, Giuseppe, Celutkiene, Jelena, Coats, Andrew, Cohen‐Solal, Alain, Córdoba, Raúl, Cosyns, Bernard, Filippatos, Gerasimos, Fox, Kevin, Gulati, Geeta, and Inciardi, Riccardo M.

Subjects

CARDIO-oncology, REQUIRED courses (Education), CARDIOTOXICITY, CARDIOLOGY, DISEASE management

Abstract

Cardio‐oncology is a rapidly growing field of cardiovascular (CV) medicine that has resulted from the continuously increasing clinical demand for specialized CV evaluation, prevention and management of patients suffering or surviving from malignant diseases. Dealing with CV disease in patients with cancer requires special knowledge beyond that included in the general core curriculum for cardiology. Therefore, the European Society of Cardiology (ESC) has developed a special core curriculum for cardio‐oncology, a consensus document that defines the level of experience and knowledge required for cardiologists in this particular field. It is structured into 8 chapters, including (i) principles of cancer biology and therapy; (ii) forms and definitions of cancer therapy‐related cardiovascular toxicity (CTR‐CVT); (iii) risk stratification, prevention and monitoring protocols for CTR‐CVT; (iv) diagnosis and management of CV disease in patients with cancer; (v) long‐term survivorship programmes and cardio‐oncology rehabilitation; (vi) multidisciplinary team management of special populations; (vii) organization of cardio‐oncology services; (viii) research in cardio‐oncology. The core curriculum aims at promoting standardization and harmonization of training and evaluation in cardio‐oncology, while it further provides the ground for an ESC certification programme designed to recognize the competencies of certified specialists. [ABSTRACT FROM AUTHOR]

Published

2024

22. Efficacy and safety of CDR132L in patients with reduced left ventricular ejection fraction after myocardial infarction: Rationale and design of the HF‐REVERT trial.

Author

Bauersachs, Johann, Solomon, Scott D., Anker, Stefan D., Antorrena‐Miranda, Isabel, Batkai, Sandor, Viereck, Janika, Rump, Steffen, Filippatos, Gerasimos, Granzer, Ulrich, Ponikowski, Piotr, de Boer, Rudolf A., Vardeny, Orly, Hauke, Wilfried, and Thum, Thomas

Subjects

VENTRICULAR ejection fraction, MYOCARDIAL infarction, BRAIN natriuretic factor, ALDOSTERONE antagonists, PATIENT safety, HEART failure, LEFT ventricular dysfunction

Abstract

Aim: Inhibition of microRNA (miR)‐132 effectively prevents and reverses adverse cardiac remodelling, making it an attractive heart failure (HF) target. CDR132L, a synthetic antisense oligonucleotide selectively blocking pathologically elevated miR‐132, demonstrated beneficial effects on left ventricular (LV) structure and function in relevant preclinical models, and was safe and well tolerated in a Phase 1b study in stable chronic HF patients. Patients with acute myocardial infarction (MI) and subsequent LV dysfunction and remodelling have limited therapeutic options, and may profit from early CDR132L treatment. Methods: The HF‐REVERT (Phase 2, multicenter, randomized, parallel, 3‐arm, placebo‐controlled Study to Assess Efficacy and Safety of CDR132L in Patients with Reduced Left Ventricular Ejection Fraction after Myocardial Infarction) evaluates the efficacy and safety of CDR132L in HF patients post‐acute MI (n = 280), comparing the effect of 5 and 10 mg/kg CDR132L, administered as three single intravenous doses 28 days apart, in addition to standard of care. Key inclusion criteria are the diagnosis of acute MI, the development of systolic dysfunction (LV ejection fraction ≤45%) and elevated N‐terminal pro‐B‐type natriuretic peptide. The study consists of a 6‐month double‐blinded treatment period with the primary endpoint LV end‐systolic volume index and relevant secondary endpoints, followed by a 6‐month open‐label observation period. Conclusion: The HF‐REVERT trial may underpin the concept of miR‐132 inhibition to prevent or reverse cardiac remodelling in post‐MI HF. The results will inform the design of subsequent outcome trials to test CDR132L in HF. [ABSTRACT FROM AUTHOR]

Published

2024

23. Sacubitril/valsartan compared to ramipril in high‐risk post‐myocardial infarction patients stratified according to use of mineralocorticoid receptor antagonists: insight from the PARADISE MI trial

Author

Schou, Morten, primary, Claggett, Brian, additional, Miao, Zi Michael, additional, Fernandez, Alberto, additional, Filippatos, Gerasimos, additional, Granger, Christopher, additional, Jering, Karola, additional, Maggioni, Aldo P., additional, McCausland, Finnian, additional, Villota, Julio Nuñez, additional, Rouleau, Jean‐Lucien, additional, Mody, Freny Vaghaiwalla, additional, van der Meer, Peter, additional, Vinereanu, Dragos, additional, McGrath, Martina, additional, Zhou, Yinong, additional, Mann, Douglas L., additional, Solomon, Scott D., additional, Steg, Philippe Gabriel, additional, Braunwald, Eugene, additional, McMurray, John J.V., additional, Pfeffer, Marc A., additional, and Køber, Lars, additional

Published

2023

24. GDF‐15 and the Effect of Empagliflozin in Heart Failure: Findings from the EMPEROR Program

Author

Ferreira, João Pedro, primary, Packer, Milton, additional, Butler, Javed, additional, Filippatos, Gerasimos, additional, Pocock, Stuart J., additional, Januzzi, James L., additional, Sattar, Naveed, additional, Maldonado, Sandra González, additional, Panova‐Noeva, Marina, additional, Sumin, Mikhail, additional, Masson, Serge, additional, Anker, Stefan D., additional, and Zannad, Faiez, additional

Published

2023

25. Incidence, risk assessment and prevention of sudden cardiac death in cardiomyopathies

Author

Polovina, Marija, primary, Tschöpe, Carsten, additional, Rosano, Giuseppe, additional, Metra, Marco, additional, Crea, Filippo, additional, Mullens, Wilfried, additional, Bauersachs, Johann, additional, Sliwa, Karen, additional, de Boer, Rudolf A., additional, Farmakis, Dimitrios, additional, Thum, Thomas, additional, Corrado, Domenico, additional, Bayes‐Genis, Antoni, additional, Bozkurt, Biykem, additional, Filippatos, Gerasimos, additional, Keren, Andre, additional, Skouri, Hadi, additional, Moura, Brenda, additional, Volterrani, Maurizio, additional, Abdelhamid, Magdy, additional, Ašanin, Milika, additional, Krljanac, Gordana, additional, Tomić, Milenko, additional, Savarese, Gianluigi, additional, Adamo, Marianna, additional, Lopatin, Yuri, additional, Chioncel, Ovidiu, additional, Coats, Andrew J.S., additional, and Seferović, Petar M., additional

Published

2023

26. State‐of‐the‐art document on optimal contemporary management of cardiomyopathies

Author

Seferović, Petar M., primary, Polovina, Marija, additional, Rosano, Giuseppe, additional, Bozkurt, Biykem, additional, Metra, Marco, additional, Heymans, Stephane, additional, Mullens, Wilfried, additional, Bauersachs, Johann, additional, Sliwa, Karen, additional, de Boer, Rudolf A., additional, Farmakis, Dimitrios, additional, Thum, Thomas, additional, Olivotto, Iacopo, additional, Rapezzi, Claudio, additional, Linhart, Aleš, additional, Corrado, Domenico, additional, Tschöpe, Carsten, additional, Milinković, Ivan, additional, Bayes Genis, Antoni, additional, Filippatos, Gerasimos, additional, Keren, Andre, additional, Ašanin, Milika, additional, Krljanac, Gordana, additional, Maksimović, Ružica, additional, Skouri, Hadi, additional, Ben Gal, Tuvia, additional, Moura, Brenda, additional, Volterrani, Maurizio, additional, Abdelhamid, Magdy, additional, Lopatin, Yuri, additional, Chioncel, Ovidiu, additional, and Coats, Andrew J.S., additional

Published

2023

27. Noncardiac comorbidities and intensive up‐titration of oral treatment in patients recently hospitalized for heart failure: insights from the STRONG‐HF trial

Author

Chioncel, Ovidiu, primary, Davison, Beth, additional, Adamo, Marianna, additional, Antohi, Laura E, additional, Arrigo, Mattia, additional, Barros, Marianela, additional, Biegus, Jan, additional, Čerlinskaitė‐Bajorė, Kamilė, additional, Celutkiene, Jelena, additional, Cohen‐Solal, Alain, additional, Damasceno, Albertino, additional, Diaz, Rafael, additional, Edwards, Christopher, additional, Filippatos, Gerasimos, additional, Kimmoun, Antoine, additional, Lam, Carolyn S.P., additional, Metra, Marco, additional, Novosadova, Maria, additional, Pagnesi, Matteo, additional, Pang, Peter S., additional, Ponikowski, Piotr, additional, Radu, Razvan I, additional, Saidu, Hadiza, additional, Sliwa, Karen, additional, Voors, Adriaan A., additional, Takagi, Koji, additional, Ter Maaten, Jozine M., additional, Tomasoni, Daniela, additional, Cotter, Gad, additional, and Mebazaa, Alexandre, additional

Published

2023

28. Associations between baseline heart rate and blood pressure and time to events in heart failure with reduced ejection fraction patients: Data from the QUALIFY international registry

Author

Abdin, Amr, primary, Anker, Stefan D., additional, Cowie, Martin R., additional, Filippatos, Gerasimos S., additional, Ponikowski, Piotr, additional, Tavazzi, Luigi, additional, Schöpe, Jakob, additional, Wagenpfeil, Stefan, additional, Komajda, Michel, additional, and Böhm, Michael, additional

Published

2023

29. Decongestion strategies in patients presenting with acutely decompensated heart failure: A worldwide survey among physicians

Author

Vazir, Ali, primary, Kapelios, Chris J., additional, Agaoglu, Elif, additional, Metra, Marco, additional, Lopatin, Yury, additional, Seferovic, Petar, additional, Mullens, Wilfred, additional, Filippatos, Gerasimos, additional, Rosano, Giuseppe, additional, Coats, Andrew J.S., additional, and Chioncel, Ovidiu, additional

Published

2023

30. Impact of mitral regurgitation in patients with acute heart failure

Author

Matteo Pagnesi, Marianna Adamo, Jozine M. ter Maaten, Iris E. Beldhuis, Gad Cotter, Beth A. Davison, G. Michael Felker, Gerasimos Filippatos, Barry H. Greenberg, Peter S. Pang, Piotr Ponikowski, Iziah E. Sama, Thomas Severin, Claudio Gimpelewicz, Adriaan A. Voors, John R. Teerlink, Marco Metra, and Cardiovascular Centre (CVC)

Subjects

Hospitalization, Acute heart failure, Outcomes, Mortality, Cardiology and Cardiovascular Medicine, Valvular heart disease, Mitral regurgitation

Abstract

Aims: The impact of mitral regurgitation (MR) in patients hospitalized for acute heart failure (AHF) is not well established. We assessed the role of MR in patients enrolled in the Relaxin in Acute Heart Failure 2 (RELAX-AHF-2) trial. Methods and results: Patients enrolled in RELAX-AHF-2 with available data regarding MR status were included in this analysis. Baseline characteristics, in-hospital data, and clinical outcomes through 180-day follow-up were evaluated. The impact of moderate/severe MR was assessed. Among 6420 AHF patients with known MR status, 1810 patients (28.2%) had moderate/severe MR. Compared to patients with no/mild MR, those with moderate/severe MR were more likely to have history of heart failure (HF), prior HF hospitalization, more comorbidities, symptoms/signs of HF, lower left ventricular ejection fraction and higher N-terminal pro-B-type natriuretic peptide levels. Moderate/severe MR was associated with longer length of hospital stay, higher rates of residual dyspnoea, increased jugular venous pressure through the index hospitalization and a higher unadjusted risk of the composite of cardiovascular (CV) death or rehospitalization for HF/renal failure (RF) through 180 days (crude hazard ratio [HR] 1.15, 95% confidence interval [CI] 1.03–1.27, p = 0.01). The association between moderate/severe MR and poorer outcomes was not maintained in a multivariable model including several covariates of interest (adjusted HR 1.03, 95% CI 0.91–1.17, p = 0.65). Similar findings were observed for HF/RF rehospitalization alone. Conclusions: In patients with AHF, moderate/severe MR was associated with a worse clinical profile but did not have an independent prognostic impact on clinical outcomes.

Published

2023

31. Dyspnoea and worsening heart failure in patients with acute heart failure: results from the Pre-RELAX-AHF study.

Author

Metra, Marco, Teerlink, John R, Felker, G Michael, Greenberg, Barry H, Filippatos, Gerasimos, Ponikowski, Piotr, Teichman, Sam L, Unemori, Elaine, Voors, Adriaan A, Weatherley, Beth Davison, and Cotter, Gad

Subjects

Humans, Dyspnea, Disease Progression, Pain Measurement, Prognosis, Hospitalization, Health Status Indicators, Multivariate Analysis, Area Under Curve, Linear Models, Logistic Models, Aged, Female, Male, Heart Failure, Statistics as Topic, Kaplan-Meier Estimate, Acute heart failure, Dyspnoea, Relaxin, Cardiorespiratory Medicine and Haematology, Cardiovascular System & Hematology

Abstract

AimsAlthough dyspnoea is the most common cause of admission for acute heart failure (AHF), more needs to be known about its clinical course and prognostic significance.Methods and resultsThe Pre-RELAX-AHF study randomized 232 subjects with AHF to placebo or four doses of relaxin and evaluated early (6-24 h Likert scale) and persistent [change in visual analogue scale area under the curve (VAS AUC) through Day 5] dyspnoea relief. Worsening heart failure (WHF) was defined as worsening AHF signs and symptoms requiring additional therapy. Patients were followed until Day 180. Early dyspnoea relief was observed in only 25% of all patients, and VAS AUC at 5 days was 45% over baseline values in all patients (32% placebo; 50% all relaxin-treated patients). Worsening heart failure to Day 5 was observed in 16% of all patients (21% placebo; 14% relaxin). Lack of persistent dyspnoea relief and WHF were associated with a longer length of initial hospital stay and worse 60-day outcomes.ConclusionDyspnoea relief in patients admitted with AHF is often incomplete, and many may show WHF after the initial stabilization. Both lack of persistent dyspnoea relief and in-hospital WHF predict a longer length of stay and worse outcome.

Published

2010

32. Patient phenotype profiling in heart failure with preserved ejection fraction to guide therapeutic decision making. A scientific statement of the Heart Failure Association, the European Heart Rhythm Association of the European Society of Cardiology, and the European Society of Hypertension

Author

Anker, Stefan D., primary, Usman, Muhammad Shariq, additional, Anker, Markus S., additional, Butler, Javed, additional, Böhm, Michael, additional, Abraham, William T., additional, Adamo, Marianna, additional, Chopra, Vijay K., additional, Cicoira, Mariantonietta, additional, Cosentino, Francesco, additional, Filippatos, Gerasimos, additional, Jankowska, Ewa A., additional, Lund, Lars H., additional, Moura, Brenda, additional, Mullens, Wilfried, additional, Pieske, Burkert, additional, Ponikowski, Piotr, additional, Gonzalez‐Juanatey, Jose R., additional, Rakisheva, Amina, additional, Savarese, Gianluigi, additional, Seferovic, Petar, additional, Teerlink, John R., additional, Tschöpe, Carsten, additional, Volterrani, Maurizio, additional, von Haehling, Stephan, additional, Zhang, Jian, additional, Zhang, Yuhui, additional, Bauersachs, Johann, additional, Landmesser, Ulf, additional, Zieroth, Shelley, additional, Tsioufis, Konstantinos, additional, Bayes‐Genis, Antoni, additional, Chioncel, Ovidiu, additional, Andreotti, Felicita, additional, Agabiti‐Rosei, Enrico, additional, Merino, Jose L., additional, Metra, Marco, additional, Coats, Andrew J.S., additional, and Rosano, Giuseppe M.C., additional

Published

2023

33. Prevalence, clinical characteristics and outcomes of heart failure patients with or without isolated or combined mitral and tricuspid regurgitation: An analysis from the ESC‐HFA Heart Failure Long‐Term Registry

Author

Adamo, Marianna, primary, Chioncel, Ovidiu, additional, Benson, Lina, additional, Shahim, Bahira, additional, Crespo‐Leiro, Maria G., additional, Anker, Stefan D., additional, Coats, Andrew J.S., additional, Filippatos, Gerasimos, additional, Lainscak, Mitja, additional, McDonagh, Theresa, additional, Mebazaa, Alexander, additional, Piepoli, Massimo F., additional, Rosano, Giuseppe M.C., additional, Ruschitzka, Frank, additional, Savarese, Gianluigi, additional, Seferovic, Petar, additional, Shahim, Angiza, additional, Popescu, Bogdan A., additional, Iung, Bernard, additional, Volterrani, Maurizio, additional, Maggioni, Aldo P., additional, Metra, Marco, additional, and Lund, Lars H., additional

Published

2023

34. Acute heart failure and valvular heart disease: A scientific statement of the Heart Failure Association, the Association for Acute CardioVascular Care and the European Association of Percutaneous Cardiovascular Interventions of the European Society of Cardiology

Author

Chioncel, Ovidiu, primary, Adamo, Marianna, additional, Nikolaou, Maria, additional, Parissis, John, additional, Mebazaa, Alexandre, additional, Yilmaz, Mehmet Birhan, additional, Hassager, Christian, additional, Moura, Brenda, additional, Bauersachs, Johann, additional, Harjola, Veli‐Pekka, additional, Antohi, Elena‐Laura, additional, Ben‐Gal, Tuvia, additional, Collins, Sean P., additional, Iliescu, Vlad Anton, additional, Abdelhamid, Magdy, additional, Čelutkienė, Jelena, additional, Adamopoulos, Stamatis, additional, Lund, Lars H., additional, Cicoira, Mariantonietta, additional, Masip, Josep, additional, Skouri, Hadi, additional, Gustafsson, Finn, additional, Rakisheva, Amina, additional, Ahrens, Ingo, additional, Mortara, Andrea, additional, Janowska, Ewa A., additional, Almaghraby, Abdallah, additional, Damman, Kevin, additional, Miro, Oscar, additional, Huber, Kurt, additional, Ristic, Arsen, additional, Hill, Loreena, additional, Mullens, Wilfried, additional, Chieffo, Alaide, additional, Bartunek, Jozef, additional, Paolisso, Pasquale, additional, Bayes‐Genis, Antoni, additional, Anker, Stefan D., additional, Price, Susanna, additional, Filippatos, Gerasimos, additional, Ruschitzka, Frank, additional, Seferovic, Petar, additional, Vidal‐Perez, Rafael, additional, Vahanian, Alec, additional, Metra, Marco, additional, McDonagh, Theresa A., additional, Barbato, Emanuele, additional, Coats, Andrew J.S., additional, and Rosano, Giuseppe M.C., additional

Published

2023

35. Impact of ischaemic aetiology on the efficacy of intravenous ferric carboxymaltose in patients with iron deficiency and acute heart failure

Author

Marco, Metra, Ewa A, Jankowska, Matteo, Pagnesi, Stefan D, Anker, Javed, Butler, Fabio, Dorigotti, Vincent, Fabien, Gerasimos, Filippatos, Bridget-Anne, Kirwan, Iain C, Macdougall, Giuseppe, Rosano, Frank, Ruschitzka, Daniela, Tomasoni, Peter, van der Meer, Piotr, Ponikowski, Cardiovascular Centre (CVC), and Restoring Organ Function by Means of Regenerative Medicine (REGENERATE)

Subjects

Male, Heart Failure, RISK, Anemia, Iron-Deficiency, Iron deficiency, MORTALITY, Acute heart failure, Iron Deficiencies, Ferric carboxymaltose, Ferric Compounds, AFFIRM-AHF, Quality of Life, Ischaemic heart failure, Humans, Cardiology and Cardiovascular Medicine, Maltose

Abstract

Aims In AFFIRM-AHF, intravenous ferric carboxymaltose (FCM) reduced heart failure (HF) hospitalisations and improved quality of life versus placebo in iron-deficient patients stabilised after an acute HF episode. This analysis explored the effects of FCM versus placebo in patients with ischaemic and non-ischaemic HF aetiology. Methods and results We included 1082 patients from AFFIRM-AHF: 590 with ischaemic HF (defined as investigator-reported ischaemic HF aetiology and/or prior acute myocardial infarction and/or prior coronary revascularisation) and 492 with non-ischaemic HF. The prevalences of male sex, comorbidities, and history of HF were higher in the ischaemic versus non-ischaemic HF subgroup. Annualised event rates for the primary composite outcome of total HF hospitalisations and cardiovascular death with FCM versus placebo were 65.3 versus 100.6 per 100 patient-years in the ischaemic HF subgroup (rate ratio [RR] 0.65, 95% confidence interval [CI] 0.47-0.89, p = 0.007) and 58.3 versus 52.5 in the non-ischaemic HF subgroup (RR 1.11, 95% CI 0.75-1.66, p = 0.60) (p(interaction) = 0.039). An interaction between HF aetiology and treatment effect was also observed for the secondary outcome of total HF hospitalisations (p(interaction) = 0.038). A nominal increase in quality of life, assessed using the 12-item Kansas City Cardiomyopathy Questionnaire, was observed with FCM versus placebo, within each subgroup. Conclusions Heart failure hospitalisations and cardiovascular deaths occurred at a higher rate in patients with ishaemic versus those with non-ischaemic HF and were reduced by FCM versus placebo only in ischaemic patients. Further studies are needed to assess the role of aetiology in FCM efficacy.

Published

2022

36. Heart failure outcomes according to heart rate and effects of empagliflozin in patients of the EMPEROR‐Preserved trial

Author

Michael, Böhm, Javed, Butler, Felix, Mahfoud, Gerasimos, Filippatos, João Pedro, Ferreira, Stuart J, Pocock, Jonathan, Slawik, Martina, Brueckmann, Bruno, Linetzky, Elke, Schüler, Christoph, Wanner, Faiez, Zannad, Milton, Packer, and Stefan D, Anker

Subjects

Heart Failure, Heart Rate, Atrial Fibrillation, Humans, Stroke Volume, Cardiology and Cardiovascular Medicine, Ventricular Function, Left

Abstract

Empagliflozin reduces cardiovascular death (CVD) or heart failure hospitalization (HHF) in patients with heart failure and preserved ejection fraction (HFpEF). Treatment effects and safety in relation to resting heart rate (RHR) have not been studied.The interplay of RHR and empagliflozin effects in EMPEROR-Preserved was evaluated. We grouped patients (n = 5988) according to their baseline RHR (70 bpm [n = 2650], 70-75 bpm [n = 967],75 bpm [n = 1736]) and explored the influence of RHR on CVD or HHF (primary outcome) and its components in sinus rhythm or atrial fibrillation/flutter (AF) and adverse events. We studied the efficacy of empagliflozin across the RHR spectrum. Compared to placebo, empagliflozin did not change heart rate over time. The primary outcome (p for trend = 0.0004) and its components CVD (p trend = 0.0002), first HHF (p for trend = 0.0099) and all-cause death (p 0.0001) increased with RHR only in sinus rhythm but not AF. The risk increase with RHR was similar in patients with heart failure and mildly reduced ejection fraction (left ventricular ejection fraction [LVEF] 40-49%) and HFpEF (LVEF ≥50%). Baseline RHR had no influence on the effect of empagliflozin on the primary outcomes (p for trend = 0.20), first HHF (p for trend = 0.49). There were no clinically relevant differences in adverse events between empagliflozin and placebo across the RHR groups.Resting heart rate associates with outcomes only in sinus rhythm but not in AF. Empagliflozin reduced outcomes over the entire RHR spectrum without increase of adverse events.

Published

2022

37. Sacubitril/valsartan versus ramipril for patients with acute myocardial infarction: win‐ratio analysis of the PARADISE‐MI trial

Author

Otavio Berwanger, Marc Pfeffer, Brian Claggett, Karola S. Jering, Aldo P. Maggioni, Philippe Gabriel Steg, Roxana Mehran, Eldrin F. Lewis, Yinong Zhou, Peter van der Meer, Carmine De Pasquale, Béla Merkely, Gerasimos Filippatos, John J.V. McMurray, Christopher B. Granger, Scott D. Solomon, Eugene Braunwald, Cardiovascular Centre (CVC), and Restoring Organ Function by Means of Regenerative Medicine (REGENERATE)

Subjects

Heart Failure, Aminobutyrates, Biphenyl Compounds, Myocardial Infarction, Tetrazoles, Stroke Volume, Acute myocardial infarction, Ventricular Function, Left, Sacubitril, valsartan, Angiotensin Receptor Antagonists, Drug Combinations, NEPRILYSIN INHIBITION, Ramipril, Win ratio, Angiotensin receptor-neprilysin inhibition, Humans, Neprilysin, Cardiology and Cardiovascular Medicine, COMPOSITE END-POINTS, CLINICAL-TRIALS

Abstract

Background: \ud The win ratio can incorporate different types of outcomes and enhance statistical power, making it a useful method for analyzing composite outcomes in cardiovascular trials. The application of this approach to the PARADISE-MI trial provides an additional perspective into understanding the effects of sacubitril/valsartan in patients with acute myocardial infarction.\ud \ud Methods: \ud We conducted a post-hoc analysis of the PARADISE-MI trial, which randomly assigned patients with acute myocardial infarction complicated by a reduced left ventricular ejection fraction, pulmonary congestion, or both to receive either sacubitril/valsartan (97 mg of sacubitril and 103 mg of valsartan twice daily) or ramipril (5 mg twice daily) in addition to guideline-recommended therapy. The principal composite outcome was analyzed in the hierarchical order of death due to cardiovascular causes, first hospitalization for heart failure, and first outpatient episode of symptomatic heart failure. We included events confirmed by the clinical event classification (CEC) committee as well as events identified by investigators that did not meet study definitions. Results were analyzed by the unmatched win ratio method. A win ratio that exceeds 1.00 reflects a better outcome.\ud \ud Results: \ud A total of 5661 patients underwent randomization; 2830 were assigned to receive sacubitril-valsartan and 2831 to receive ramipril. The hierarchical analysis of the principal composite outcome demonstrated a larger number of wins [1,265,767 (15.7%)] than losses [1,079,502 (13.4%)] in the sacubitril/valsartan group (win ratio of 1.17, 95% confidence interval [CI],1.03 to 1.33; P=0.015). Sensitivity analyses using alternative definitions of the composite outcome showed results similar to those of the principal analysis, except for analysis restricted to events that met CEC definitions (win ratio of 1.11, 95% CI, 0.96 to 1.30; P=0.16).\ud \ud Conclusion: \ud In this post-hoc analysis of the PARADISE-MI trial using the win ratio and including investigator-identified events not having CEC confirmation, sacubitril/valsartan was superior to ramipril among high-risk survivors of acute myocardial infarction.

Published

2022

38. Effects of empagliflozin on collagen biomarkers in patients with heart failure: Findings from the EMPEROR trials.

Author

Ferreira, João Pedro, Butler, Javed, Anker, Stefan D., Januzzi, James L., Panova‐Noeva, Marina, Reese‐Petersen, Alexander L., Sattar, Naveed, Schueler, Elke, Pocock, Stuart J., Filippatos, Gerasimos, Packer, Milton, Sumin, Mikhail, and Zannad, Faiez

Subjects

HEART failure, SODIUM-glucose cotransporter 2 inhibitors, HEART failure patients, COLLAGEN, EMPAGLIFLOZIN, NATRIURETIC peptides

Abstract

Aims: Extracellular matrix remodelling is one of the key pathways involved in heart failure (HF) progression. Sodium–glucose cotransporter 2 inhibitors (SGLT2i) may have a role in attenuating myocardial fibrosis. The impact of SGLT2i on blood markers of collagen turnover in humans is not fully elucidated. This study aimed to investigate the effect of empagliflozin on serum markers of collagen turnover in patients enrolled in the EMPEROR‐Preserved and EMPEROR‐Reduced trials. Methods and results: Overall, 1084 patients (545 in empagliflozin and 539 in placebo) were included in the analysis. Procollagen type I carboxy‐terminal propeptide (PICP), a fragment of N‐terminal type III collagen (PRO‐C3), procollagen type I amino‐terminal peptide (PINP), a fragment of C‐terminal type VIa3 collagen (PRO‐C6), a fragment of type I collagen (C1M), and a fragment of type III collagen (C3M) were measured in serum at baseline, 12 and 52 weeks. A mixed model repeated measurements model was used to evaluate the effect of empagliflozin versus placebo on the analysed biomarkers. Higher baseline PICP, PRO‐C6 and PINP levels were associated with older age, a more severe HF presentation, higher levels of natriuretic peptides and high‐sensitivity troponin T, and the presence of comorbid conditions such as chronic kidney disease and atrial fibrillation. Higher PICP levels were associated with the occurrence of the study primary endpoint (a composite of HF hospitalization or cardiovascular death), and PRO‐C6 and PINP were associated with the occurrence of sustained worsening of kidney function. On the other hand, PRO‐C3, C1M, and C3M were not associated with worse HF severity or study outcomes. Compared to placebo, empagliflozin reduced PICP at week 12 by 5% and at week 52 by 8% (week 12: geometric mean ratio = 0.95, 95% confidence interval [CI] 0.91–0.99, p = 0.012; week 52: geometric mean ratio = 0.92, 95% CI 0.88–0.97, p = 0.003). Additionally, empagliflozin reduced PRO‐C3 at week 52 by 7% (week 12: geometric mean ratio = 0.98, 95% CI 0.95–1.02, p = 0.42; week 52: geometric mean ratio = 0.93, 95% CI 0.89–0.98, p = 0.003), without impact on other collagen markers. Conclusion: Our observations are consistent with experimental observations that empagliflozin down‐regulates profibrotic signalling. The importance of such an effect for the clinical benefits of SGLT2i in HF remains to be elucidated. [ABSTRACT FROM AUTHOR]

Published

2024

39. Sacubitril/valsartan compared to ramipril in high‐risk post‐myocardial infarction patients stratified according to use of mineralocorticoid receptor antagonists: Insight from the PARADISE MI trial.

Author

Schou, Morten, Claggett, Brian, Miao, Zi Michael, Fernandez, Alberto, Filippatos, Gerasimos, Granger, Christopher, Jering, Karola, Maggioni, Aldo P., McCausland, Finnian, Villota, Julio Nuñez, Rouleau, Jean‐Lucien, Mody, Freny Vaghaiwalla, van der Meer, Peter, Vinereanu, Dragos, McGrath, Martina, Zhou, Yinong, Mann, Douglas L., Solomon, Scott D., Steg, Philippe Gabriel, and Braunwald, Eugene

Subjects

MINERALOCORTICOID receptors, VALSARTAN, ENTRESTO, RAMIPRIL, INFARCTION

Abstract

Aim: It is unknown whether safety and clinical endpoints by use of sacubitril/valsartan (an angiotensin receptor–neprilysin inhibitor [ARNI]) are affected by mineralocorticoid receptor antagonists (MRA) in high‐risk myocardial infarction (MI) patients. The aim of this study was to examine whether MRA modifies safety and clinical endpoints by use of sacubitril/valsartan in patients with a MI and left ventricular systolic dysfunction (LVSD) and/or pulmonary congestion. Methods and results: Patients (n = 5661) included in the PARADISE MI trial (Prospective ARNI vs. ACE Inhibitor Trial to Determine Superiority in Reducing Heart Failure Events After MI) were stratified according to MRA. Primary outcomes in this substudy were worsening heart failure or cardiovascular death. Safety was defined as symptomatic hypotension, hyperkalaemia >5.5 mmol/L, or permanent drug discontinuation. A total of 2338 patients (41%) were treated with MRA. Safety of ARNI compared to ramipril was not altered significantly by ± MRA, and both groups had similar increase in symptomatic hypotension with ARNI. In patients taking MRA, the risk of hyperkalaemia or permanent drug discontinuation was not significantly altered by ARNI (p > 0.05 for all comparisons). The effect of ARNI compared with ramipril was similar in those who were and were not taking MRA (hazard ratio [HR]MRA 0.96, 95% confidence interval [CI] 0.77–1.19 and HRMRA– 0.87, 95% CI 0.71–1.05, for the primary endpoint; p = 0.51 for interaction [Clinical Endpoint Committee adjudicated]); similar findings were observed if investigator‐reported endpoints were evaluated (p = 0.61 for interaction). Conclusions: Use of a MRA did not modify safety or clinical endpoints related to initiation of ARNI compared to ramipril in the post‐MI setting in patients with LVSD and/or congestion. [ABSTRACT FROM AUTHOR]

Published

2024

40. Growth differentiation factor‐15 and the effect of empagliflozin in heart failure: Findings from the EMPEROR program.

Author

Ferreira, João Pedro, Packer, Milton, Butler, Javed, Filippatos, Gerasimos, Pocock, Stuart J., Januzzi, James L., Sattar, Naveed, Maldonado, Sandra González, Panova‐Noeva, Marina, Sumin, Mikhail, Masson, Serge, Anker, Stefan D., and Zannad, Faiez

Subjects

HEART failure, BRAIN natriuretic factor, EMPAGLIFLOZIN, SOMATOMEDIN, INSULIN-like growth factor-binding proteins, HEART failure patients

Abstract

Aims: Growth differentiation factor‐15 (GDF‐15) is upregulated in part in response to cardiomyocyte stretch and stress, and it exerts a protective role that is mediated by its action to suppress signalling through insulin‐like growth factor (IGF) and enhance signalling through adenosine monophosphate‐activated protein kinase (AMPK). Sodium–glucose cotransporter 2 (SGLT2) inhibitors improve outcomes in heart failure, which has been experimentally linked to AMPK. This study aimed at evaluating the associations of GDF‐15 with baseline characteristics, the prognostic significance of GDF‐15, and the effect of empagliflozin on GDF‐15 in patients with heart failure with a reduced and preserved ejection fraction. Methods and results: Growth differentiation factor‐15 was determined in serum samples from the EMPEROR‐Reduced and EMPEROR‐Preserved trials. Cox regression and mixed models for repeated measures were used to study the association with outcomes and the effect of empagliflozin on GDF‐15, respectively. We studied 1124 patients (560 placebo and 564 empagliflozin) with median GDF‐15 levels at baseline of 2442 (interquartile range 1603–3780) pg/ml. Patients with higher GDF‐15 levels were typically older men with more severe symptoms, higher N‐terminal pro‐B‐type natriuretic peptide levels, worse kidney function and who were prescribed metformin. Baseline levels of GDF‐15 were well correlated with levels of IGF‐binding protein 7 (rho = 0.64). Higher levels of GDF‐15 were independently associated with an increased risk of cardiovascular death, heart failure hospitalizations, and worse kidney outcomes. When considered as a continuous variable, for each doubling in GDF‐15, the adjusted hazard ratio for cardiovascular death or heart failure hospitalization was 1.40 (95% confidence interval 1.15–1.71; p < 0.001). The relative effect of empagliflozin on cardiovascular death and hospitalization for heart failure was most pronounced in patients with higher baseline levels of GDF‐15 (interaction p‐trend = 0.031). At week 52, when compared with placebo, empagliflozin increased GDF‐15 by an additional 8% (p = 0.020), an effect that was primarily seen in patients not receiving metformin, a known AMPK activator. Conclusions: Growth differentiation factor‐15 is a marker of worse heart failure severity, is an independent predictor of major heart failure outcomes and may be associated with more pronounced benefits of empagliflozin. GDF‐15 is increased among metformin users, and empagliflozin was associated with an increase in GDF‐15 levels, primarily in patients not receiving metformin. [ABSTRACT FROM AUTHOR]

Published

2024

41. Rationale and design of the ESC Heart Failure III Registry – Implementation and discovery.

Author

Lund, Lars H., Crespo‐Leiro, Maria Generosa, Laroche, Cecile, Garcia‐Pinilla, Jose M., Bennis, Ahmed, Vataman, Eleonora B., Polovina, Marija, Radovanovic, Slavica, Apostolovic, Svetlana R., Ašanin, Milika, Gackowski, Andrzej, Kaplon‐Cieslicka, Agnieszka, Cabac‐Pogorevici, Irina, Anker, Stefan D., Chioncel, Ovidiu, Coats, Andrew J.S., Filippatos, Gerasimos, Lainscak, Mitja, Mcdonagh, Theresa, and Mebazaa, Alexandre

Subjects

HEART failure, VENTRICULAR ejection fraction, GOVERNMENT policy

Abstract

Aims: Heart failure outcomes remain poor despite advances in therapy. The European Society of Cardiology Heart Failure III Registry (ESC HF III Registry) aims to characterize HF clinical features and outcomes and to assess implementation of guideline‐recommended therapy in Europe and other ESC affiliated countries. Methods: Between 1 November 2018 and 31 December 2020, 10 162 patients with chronic or acute/worsening HF with reduced, mildly reduced, or preserved ejection fraction were enrolled from 220 centres in 41 European or ESC affiliated countries. The ESC HF III Registry collected data on baseline characteristics (hospital or clinic presentation), hospital course, diagnostic and therapeutic decisions in hospital and at the clinic visit; and on outcomes at 12‐month follow‐up. These data include demographics, medical history, physical examination, biomarkers and imaging, quality of life, treatments, and interventions – including drug doses and reasons for non‐use, and cause‐specific outcomes. Conclusion: The ESC HF III Registry will provide comprehensive and unique insight into contemporary HF characteristics, treatment implementation, and outcomes, and may impact implementation strategies, clinical discovery, trial design, and public policy. [ABSTRACT FROM AUTHOR]

Published

2023

42. Early changes in renal function during rapid up‐titration of guideline‐directed medical therapy following an admission for acute heart failure.

Author

ter Maaten, Jozine M., Mebazaa, Alexandre, Davison, Beth, Edwards, Christopher, Adamo, Marianna, Arrigo, Mattia, Barros, Marianela, Biegus, Jan, Čelutkienė, Jelena, Čerlinskaitė‐Bajorė, Kamilė, Chioncel, Ovidiu, Cohen‐Solal, Alain, Damasceno, Albertino, Diaz, Rafael, Filippatos, Gerasimos, Gayat, Etienne, Kimmoun, Antoine, Lam, Carolyn S.P., Leopold, Valentine, and Novosadova, Maria

Subjects

HEART failure, BRAIN natriuretic factor, KIDNEY physiology

Abstract

Aim: In this subgroup analysis of STRONG‐HF, we explored the association between changes in renal function and efficacy of rapid up‐titration of guideline‐directed medical therapy (GDMT) according to a high‐intensity care (HIC) strategy. Methods and results: In patients randomized to the HIC arm (n = 542), renal function was assessed at baseline and during follow‐up visits. We studied the association with clinical characteristics and outcomes of a decrease in estimated glomerular filtration rate (eGFR) at week 1, defined as ≥15% decrease from baseline. Patients in the usual care group (n = 536) were seen at day 90. The treatment effect of HIC versus usual care was independent of baseline eGFR (p‐interaction = 0.4809). A decrease in eGFR within 1 week occurred in 77 (15.5%) patients and was associated with more rales on examination (p = 0.004), and a higher New York Heart Association class at the corresponding visit. Following the decrease in eGFR at 1 week, lower average optimal doses of GDMT were prescribed during follow‐up (p = 0.0210) and smaller reductions in N‐terminal pro‐B‐type natriuretic peptide occurred (geometrical mean 0.81 in no eGFR decrease vs 1.12 in GFR decrease, p = 0.0003). The rate of heart failure (HF) readmission or death at 180 days was 12.3% in no eGFR decrease versus 18.5% in eGFR decrease (p = 0.2274) and HF readmissions were 7.8% versus 16.6% (p = 0.0496). Conclusions: In the STRONG‐HF study, HIC reduced 180‐day HF readmission or death regardless of baseline eGFR. An early decrease in eGFR during rapid up‐titration of GDMT was associated with more evidence of congestion, yet lower doses of GDMT during follow‐up. [ABSTRACT FROM AUTHOR]

Published

2023

43. Safety and efficacy of istaroxime in patients with acute heart failure‐related pre‐cardiogenic shock – a multicentre, randomized, double‐blind, placebo‐controlled, parallel group study ( <scp>SEISMiC</scp> )

Author

Marco Metra, Ovidiu Chioncel, Gad Cotter, Beth Davison, Gerasimos Filippatos, Alexandre Mebazaa, Maria Novosadova, Piotr Ponikowski, Phillip Simmons, Joseph Soffer, and Steven Simonson

Subjects

Heart Failure, Cardiotonic Agents, Shock, Cardiogenic, Acute heart failure, Blood pressure, Cardiogenic shock, Istaroxime, SERCA2a, Therapeutics, Double-Blind Method, Etiocholanolone, Humans, Cardiology and Cardiovascular Medicine

Abstract

We examined the effects of istaroxime in patients hospitalized for acute heart failure (AHF) related Society for Cardiovascular Angiography and Interventions (SCAI) stage B pre-cardiogenic shock (CS).Sixty patients with AHF without acute myocardial infarction with pre-CS, defined as systolic blood pressure (SBP)90 mmHg without hypoperfusion, venous lactate ≥2 mmol/L and/or mechanical or inotropic support, were randomized to istaroxime 1.0-1.5 μg/kg/min or placebo for 24 h. The primary endpoint, the adjusted area under the curve (AUC) change in SBP from time of treatment to 6 h, was 53.1 (standard error [SE] 6.88) mmHg × hour versus 30.9 (SE 6.76) mmHg × hour with istaroxime versus placebo (p = 0.017). Adjusted SBP AUC at 24 h was 291.2 (SE 27.5) versus 208.7 (SE 27.0) mmHg × hour (p = 0.025). At 24 h, some echocardiographic measurements improved with istaroxime versus placebo including cardiac index (+0.21 L/min/mIn a phase 2a study of patients with AHF related pre-CS, istaroxime improved blood pressure and some echocardiography measures related to heart failure and was well tolerated.

Published

2022

44. Exercise testing in heart failure with preserved ejection fraction

Author

Marco Guazzi, Matthias Wilhelm, Martin Halle, Emeline Van Craenenbroeck, Hareld Kemps, Rudolph A. de Boer, Andrew J.S. Coats, Lars Lund, Donna Mancini, Barry Borlaug, Gerasimos Filippatos, Burkert Pieske, and Cardiovascular Centre (CVC)

Subjects

Heart Failure, Exercise Tolerance, Cardiology, Settore MED/11 - Malattie dell'Apparato Cardiovascolare, Stroke Volume, Exercise, Functional limitation, Gas exchange analysis, HFpEF, Dyspnea, Exercise Test, Humans, Human medicine, Cardiology and Cardiovascular Medicine

Abstract

Patients with heart failure with preserved ejection fraction (HFpEF) universally complain of exercise intolerance and dyspnoea as key clinical correlates. Cardiac as well as extracardiac components play a role for the limited exercise capacity, including an impaired cardiac and peripheral vascular reserve, a limitation in mechanical ventilation and/or gas exchange with reduced pulmonary vascular reserve, skeletal muscle dysfunction and iron deficiency/anaemia. Although most of these components can be differentiated and quantified through gas exchange analysis by cardiopulmonary exercise testing (CPET), the information provided by objective measures of exercise performance has not been systematically considered in the recent algorithms/scores for HFpEF diagnosis, by neither European nor US groups. The current clinical consensus statement by the Heart Failure Association (HFA) and European Association of Preventive Cardiology (EAPC) of the European Society of Cardiology (ESC) aims at outlining the role of exercise testing and its pathophysiological, clinical and prognostic insights, addressing the implications of a thorough functional evaluation from the diagnostic algorithm to the pathophysiology and treatment perspectives of HFpEF. Along with these goals, we provide a specific analysis of the evidence that CPET is the standard for assessing, quantifying, and differentiating the origin of dyspnoea and exercise impairment and even more so when combined with echocardiography and/or invasive haemodynamic evaluation. This will lead to improved quality of diagnosis when applying the proposed scores and may also help to implement the progressive characterization of the specific HFpEF phenotypes, a critical step toward the delivery of phenotype-specific treatments.

Published

2022

45. Biomarkers for the prediction of heart failure and cardiovascular events in patients with type 2 diabetes

Author

Peter Seferović, Dimitrios Farmakis, Antoni Bayes‐Genis, Tuvia Ben Gal, Michael Böhm, Ovidiu Chioncel, Roberto Ferrari, Gerasimos Filippatos, Loreena Hill, Ewa Jankowska, Mitja Lainscak, Yuri Lopatin, Lars H. Lund, Alexandre Mebazaa, Marco Metra, Brenda Moura, Giuseppe Rosano, Thomas Thum, Adriaan Voors, Andrew J.S. Coats, Publica, and Cardiovascular Centre (CVC)

Subjects

Cardiovascular prevention, Diabetes mellitus, Diabetes Mellitus, Type 2, Cardiology, Biomarkers, Cardiovascular risk, Heart failure, Humans, Heart Failure, Cardiology and Cardiovascular Medicine, Type 2

Abstract

Knowledge on risk predictors of incident heart failure (HF) in patients with type 2 diabetes (T2D) is crucial given the frequent coexistence of the two conditions and the fact that T2D doubles the risk of incident HF. In addition, HF is increasingly being recognized as an important endpoint in trials in T2D. On the other hand, the diagnostic and prognostic performance of established cardiovascular biomarkers may be modified by the presence of T2D. The present position paper, derived by an expert panel workshop organized by the Heart Failure Association of the European Society of Cardiology, summarizes the current knowledge and gaps in evidence regarding the use of a series of different biomarkers, reflecting various pathogenic pathways, for the prediction of incident HF and cardiovascular events in patients with T2D and in those with established HF and T2D.

Published

2022

46. Safety, tolerability and efficacy of up‐titration of guideline‐directed medical therapies for acute heart failure in elderly patients: a sub‐analysis of the STRONG‐HF randomized clinical trial

Author

Arrigo, Mattia, primary, Biegus, Jan, additional, Asakage, Ayu, additional, Mebazaa, Alexandre, additional, Davison, Beth, additional, Edwards, Christopher, additional, Adamo, Marianna, additional, Barros, Marianela, additional, Celutkiene, Jelena, additional, Čerlinskaitė‐Bajorė, Kamilė, additional, Chioncel, Ovidiu, additional, Damasceno, Albertino, additional, Diaz, Rafael, additional, Filippatos, Gerasimos, additional, Gayat, Etienne, additional, Kimmoun, Antoine, additional, Lam, Carolyn S.P., additional, Metra, Marco, additional, Novosadova, Maria, additional, Pagnesi, Matteo, additional, Pang, Peter S., additional, Ponikowski, Piotr, additional, Saidu, Hadiza, additional, Sliwa, Karen, additional, Takagi, Koji, additional, Ter Maaten, Jozine M., additional, Tomasoni, Daniela, additional, Voors, Adriaan A., additional, Cotter, Gad, additional, and Cohen‐Solal, Alain, additional

Published

2023

47. Prevalence, Characteristics and Prognostic Impact of Aortic Valve Disease in Patients with Heart Failure and Reduced, Mildly Reduced, and Preserved Ejection Fraction: An Analysis of the ESC Heart Failure Long‐Term Registry

Author

Shahim, Bahira, primary, Shahim, Angiza, additional, Adamo, Marianna, additional, Chioncel, Ovidiu, additional, Benson, Lina, additional, Shahim, Bahira, additional, Crespo‐Leiro, Maria G., additional, Anker, Stefan D., additional, Coats, Andrew J.S., additional, Filippatos, Gerasimos, additional, Lainscak, Mitja, additional, McDonagh, Theresa, additional, Mebazaa, Alexandre, additional, Piepoli, Massimo F., additional, Rosano, Giuseppe M.C., additional, Ruschitzka, Frank, additional, Savarese, Gianluigi, additional, Seferovic, Petar, additional, Volterrani, Maurizio, additional, Leiro, Marisa Crespo, additional, Cubero, Javier Segovia, additional, Amir, Offer, additional, Palic, Benjamin, additional, Maggioni, Aldo P., additional, Metra, Marco, additional, and Lund, Lars H., additional

Published

2023

48. Pre‐discharge and early post‐discharge management of patients hospitalized for acute heart failure: a scientific statement by the Heart Failure Association ( HFA ) of the ESC

Author

Metra, Marco, primary, Adamo, Marianna, additional, Tomasoni, Daniela, additional, Mebazaa, Alexandre, additional, Bayes‐Genis, Antoni, additional, Abdelhamid, Magdy, additional, Adamopoulos, Stamatis, additional, Anker, Stefan D., additional, Bauersachs, Johann, additional, Belenkov, Yuri, additional, Böhm, Michael, additional, Gal, Tuvia Ben, additional, Butler, Javed, additional, Cohen‐Solal, Alain, additional, Filippatos, Gerasimos, additional, Gustafsson, Finn, additional, Hill, Loreena, additional, Jaarsma, Tiny, additional, Jankowska, Ewa A., additional, Lainscak, Mitja, additional, Lopatin, Yuri, additional, Lund, Lars, additional, McDonagh, Theresa, additional, Milicic, Davor, additional, Moura, Brenda, additional, Mullens, Wilfried, additional, Piepoli, Massimo, additional, Polovina, Marija, additional, Ponikowski, Piotr, additional, Rakisheva, Amina, additional, Ristic, Arsen, additional, Savarese, Gianluigi, additional, Seferovic, Petar, additional, Sharma, Rajan, additional, Thum, Thomas, additional, Tocchetti, Carlo G., additional, Van Linthout, Sophie, additional, Vitale, Cristiana, additional, Von Haehling, Stephan, additional, Volterrani, Maurizio, additional, Coats, Andrew JS, additional, Chioncel, Ovidiu, additional, and Rosano, Giuseppe, additional

Published

2023

49. Sex‐specific analysis of the rapid up‐titration of guideline‐directed medical therapies after a hospitalisation for acute heart failure: insights from theSTRONG‐HFtrial

Author

Čerlinskaitė‐Bajorė, Kamilė, primary, Lam, Carolyn S.P., additional, Sliwa, Karen, additional, Adamo, Marianna, additional, Ter Maaten, Jozine M., additional, Léopold, Valentine, additional, Mebazaa, Alexandre, additional, Davison, Beth, additional, Edwards, Christopher, additional, Arrigo, Mattia, additional, Barros, Marianela, additional, Biegus, Jan, additional, Chioncel, Ovidiu, additional, Cohen‐Solal, Alain, additional, Damasceno, Albertino, additional, Diaz, Rafael, additional, Filippatos, Gerasimos, additional, Gayat, Etienne, additional, Kimmoun, Antoine, additional, Metra, Marco, additional, Novosadova, Maria, additional, Pagnesi, Matteo, additional, Pang, Peter S., additional, Ponikowski, Piotr, additional, Saidu, Hadiza, additional, Takagi, Koji, additional, Tomasoni, Daniela, additional, Voors, Adriaan A., additional, Cotter, Gad, additional, and Čelutkienė, Jelena, additional

Published

2023

50. Sodium and potassium changes during decongestion with acetazolamide – a pre‐specified analysis from the ADVOR trial

Author

Dhont, Sebastiaan, primary, Martens, Pieter, additional, Meekers, Evelyne, additional, Dauw, Jeroen, additional, Verbrugge, Frederik H., additional, Nijst, Petra, additional, ter Maaten, Jozine M., additional, Damman, Kevin, additional, Mebazaa, Alexandre, additional, Filippatos, Gerasimos, additional, Ruschitzka, Frank, additional, Tang, W.H. Wilson, additional, Dupont, Matthias, additional, and Mullens, Wilfried, additional

Published

2023