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1,262 results on '"Schnabel, Renate B."'

1. Subtle signs of atrial cardiomyopathy and left ventricular diastolic dysfunction are associated with reduced cognitive function: results from the Hamburg City Health Study

Author

Ohlrogge, Amelie H., Camen, Stephan, Nagel, Lina, Brederecke, Jan, Jensen, Märit, Stenmans, Ewgenia, Engler, Daniel, Schulte, Christian, Albrecht, Jan, Csengeri, Dora, Kirchhof, Paulus, Cheng, Bastian, Petersen, Marvin, Mayer, Carola, Börschel, Christin S., Wenzel, Jan-Per, Blankenberg, Stefan, Kühn, Simone, Thomalla, Götz, and Schnabel, Renate B.

Published
2024
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4. Gut microbiome and atrial fibrillation—results from a large population-based study

Author

Palmu, Joonatan, Börschel, Christin S, Ortega-Alonso, Alfredo, Markó, Lajos, Inouye, Michael, Jousilahti, Pekka, Salido, Rodolfo A, Sanders, Karenina, Brennan, Caitriona, Humphrey, Gregory C, Sanders, Jon G, Gutmann, Friederike, Linz, Dominik, Salomaa, Veikko, Havulinna, Aki S, Forslund, Sofia K, Knight, Rob, Lahti, Leo, Niiranen, Teemu, and Schnabel, Renate B

Subjects
Epidemiology, Biomedical and Clinical Sciences, Clinical Sciences, Health Sciences, Cardiovascular, Heart Disease, Prevention, Genetics, 2.1 Biological and endogenous factors, Aetiology, Humans, Atrial Fibrillation, Gastrointestinal Microbiome, Heart, Bacteria, Aging, Incidence, Atrial fibrillation, Gut microbiome, Metagenomics, Public Health and Health Services, Clinical sciences
Abstract

BackgroundAtrial fibrillation (AF) is an important heart rhythm disorder in aging populations. The gut microbiome composition has been previously related to cardiovascular disease risk factors. Whether the gut microbial profile is also associated with the risk of AF remains unknown.MethodsWe examined the associations of prevalent and incident AF with gut microbiota in the FINRISK 2002 study, a random population sample of 6763 individuals. We replicated our findings in an independent case-control cohort of 138 individuals in Hamburg, Germany.FindingsMultivariable-adjusted regression models revealed that prevalent AF (N = 116) was associated with nine microbial genera. Incident AF (N = 539) over a median follow-up of 15 years was associated with eight microbial genera with false discovery rate (FDR)-corrected P

Published
2023

5. Monitoring for atrial fibrillation prior to patent foramen ovale closure after cryptogenic stroke

Author

Diener, Hans-Christoph, Wachter, Rolf, Wong, Andrew, Thijs, Vincent, Schnabel, Renate B, Ntaios, George, Kasner, Scott, Rothwell, Peter M, Passman, Rod, Saver, Jeffrey L, Albers, Bert A, and Bernstein, Richard A

Subjects
Biomedical and Clinical Sciences, Cardiovascular Medicine and Haematology, Clinical Research, Neurosciences, Brain Disorders, Heart Disease, Cardiovascular, Detection, screening and diagnosis, 2.1 Biological and endogenous factors, Aetiology, 4.2 Evaluation of markers and technologies, Stroke, Humans, Atrial Fibrillation, Foramen Ovale, Patent, Natriuretic Peptide, Brain, Ischemic Stroke, Risk Factors, Cryptogenic stroke, atrial fibrillation, patent foramen ovale closure, cardiac rhythm monitoring, stroke recurrence, monitoring strategy, Clinical Sciences, Neurology & Neurosurgery, Clinical sciences, Allied health and rehabilitation science
Abstract

BackgroundPatients who had a cryptogenic stroke (CS) suspected to be causally related to a patent foramen ovale (PFO) are candidates for percutaneous PFO closure. In such patients, it is important to screen for atrial fibrillation (AF). Limited guidance is available regarding AF monitoring strategies in CS patients with PFO addressing optimal monitoring technology and duration.AimTo provide a narrative review of cardiac rhythm monitoring in CS patients considered for PFO closure, including current practices, stroke recurrences after CS, findings from monitoring studies in CS patients, and predictors for AF detection published in the literature. To propose a personalized strategy for cardiac monitoring in CS patients, accounting for aspects predicting AF detection.Summary of reviewAF detection in CS patients is predicted by age, left atrial enlargement, prolonged PR interval, frequent premature atrial contractions, interatrial conduction block, diabetes, prior brain infarctions, leukoaraiosis, elevated B-type natriuretic peptide (BNP)/N-terminal pro B-type natriuretic peptide (NT-proBNP) levels, and a family history of AF, as well as composed scores (e.g. CHA2DS2-VASc, atrial fibrillation in embolic stroke of undetermined source (AF-ESUS)). The causal role of the PFO may be accounted for by the risk of paradoxical embolism (RoPE) score and/or the PFO-Associated Stroke Causal Likelihood (PASCAL) classification.ConclusionA personalized approach to AF detection in CS patients is proposed, accounting for the likelihood of AF detection and aimed at obtaining sufficient confidence regarding the absence of AF in patients considered for PFO closure. In addition, the impact of high-risk PFO features on the monitoring strategy is discussed.

Published
2023

8. The DZHK research platform: maximisation of scientific value by enabling access to health data and biological samples collected in cardiovascular clinical studies

Author

Hoffmann, Julia, Hanß, Sabine, Kraus, Monika, Schaller, Jens, Schäfer, Christian, Stahl, Dana, Anker, Stefan D., Anton, Gabriele, Bahls, Thomas, Blankenberg, Stefan, Blumentritt, Arne, Boldt, Leif-Hendrik, Cordes, Steffen, Desch, Steffen, Doehner, Wolfram, Dörr, Marcus, Edelmann, Frank, Eitel, Ingo, Endres, Matthias, Engelhardt, Stefan, Erdmann, Jeanette, Eulenburg, Katharina, Falk, Volkmar, Felix, Stephan B., Frank, Derk, Franke, Thomas, Frey, Norbert, Friede, Tim, Geidel, Lars, Germans, Lisa, Grabmaier, Ulrich, Halle, Martin, Hausleiter, Jörg, Jakobi, Vera, Jebran, Ahmad-Fawad, Jobs, Alexander, Kääb, Stefan, Karakas, Mahir, Katus, Hugo A., Klatt, Alexandra, Knosalla, Christoph, Krebser, Joachim, Landmesser, Ulf, Lee, Mahsa, Lehnert, Kristin, Lesser, Stephanie, Leyh, Katrin, Lorbeer, Roberto, Mach-Kolb, Stephanie, Meder, Benjamin, Nagel, Eike, Nolte, Christian H., Parwani, Abdul S., Petersmann, Astrid, Puls, Miriam, Rau, Henriette, Reiser, Maximilian, Rienhoff, Otto, Scharfe, Tabea, Schattschneider, Mario, Scheel, Heiko, Schnabel, Renate B., Schuster, Andreas, Schmitt, Boris, Seidler, Tim, Seiffert, Moritz, Stähli, Barbara-Elisabeth, Stas, Adriane, J. Stocker, Thomas, von Stülpnagel, Lukas, Thiele, Holger, Wachter, Rolf, Wakili, Reza, Weis, Tanja, Weitmann, Kerstin, Wichmann, Heinz-Erich, Wild, Philipp, Zeller, Tanja, Hoffmann, Wolfgang, Zeisberg, Elisabeth Maria, Zimmermann, Wolfram-Hubertus, Krefting, Dagmar, Kühne, Titus, Peters, Annette, Hasenfuß, Gerd, Massberg, Steffen, Sommer, Thomas, Dimmeler, Stefanie, Eschenhagen, Thomas, and Nauck, Matthias

Published
2023
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11. An arrhythmogenic metabolite in atrial fibrillation

Author

Krause, Julia, Nickel, Alexander, Madsen, Alexandra, Aitken-Buck, Hamish M., Stoter, A. M. Stella, Schrapers, Jessica, Ojeda, Francisco, Geiger, Kira, Kern, Melanie, Kohlhaas, Michael, Bertero, Edoardo, Hofmockel, Patrick, Hübner, Florian, Assum, Ines, Heinig, Matthias, Müller, Christian, Hansen, Arne, Krause, Tobias, Park, Deung-Dae, Just, Steffen, Aïssi, Dylan, Börnigen, Daniela, Lindner, Diana, Friedrich, Nele, Alhussini, Khaled, Bening, Constanze, Schnabel, Renate B., Karakas, Mahir, Iacoviello, Licia, Salomaa, Veikko, Linneberg, Allan, Tunstall-Pedoe, Hugh, Kuulasmaa, Kari, Kirchhof, Paulus, Blankenberg, Stefan, Christ, Torsten, Eschenhagen, Thomas, Lamberts, Regis R., Maack, Christoph, Stenzig, Justus, and Zeller, Tanja

Published
2023
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15. Physiologists as medical scientists: An early warning from the German academic system.

Author

Streckfuss‐Bömeke, Katrin, Kränkel, Nicolle, Maack, Christoph, Schnabel, Renate B., Zelarayán, Laura C., Frey, Norbert, Jezzard, Peter, Krüger, Martina, Lachmann, Nico, Lutz, Susanne, Noack, Claudia, Schoger, Eric, Schröder, Katrin, Sommerfeld, Laura C., Steffens, Sabine, Winkels, Holger, Würtz, Christina, Zeller, Tanja, Rog‐Zielinska, Eva A., and Kohl, Peter

Subjects
CAREER development, MEDICAL scientists, ACADEMIC employment, PHYSIOLOGISTS, ADMINISTRATIVE reform
Abstract

"Medical scientists" are postgraduate investigators who are engaged in biomedical research, and either hold a biomedical PhD or are qualified in medicine but do not participate in patient care. Medical scientists constitute ~40% of staff at medical faculties and >90% at nonuniversity medical research institutions in Germany. However, medical scientists in Germany face limited long‐term career prospects and a lack of dedicated training and support programmes. They also face time limits on their career progression arising from national academic employment legislation, and imminent reforms by the German government are likely to make this worse. Nevertheless, recent developments in the educational landscape including the introduction of increasingly focused MSc, pre‐PhD, and doctoral programmes to train medically aware basic scientists, as well as improved general recognition of the roles and relevance of medical scientists in health research, are encouraging. Physiologists have taken essential steps to improve the recognition of medical scientists in Germany by introducing a "specialist physiologist" qualification; this initiative could be applied to support medical scientists in other fields and countries. In this review, we describe the particular challenges facing medical scientists in Germany and make recommendations that may apply to other academic systems. [ABSTRACT FROM AUTHOR]

Published
2024
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16. Cross-sectional study on the association of periodontitis with arterial hypertension in the Hamburg City Health Study

Author

Könnecke, Henrieke, Schnabel, Renate B., Walther, Carolin, Lamprecht, Ragna, Heydecke, Guido, Seedorf, Udo, Jagodzinski, Annika, Borof, Katrin, Zeller, Tanja, Beikler, Thomas, Smeets, Ralf, Gosau, Martin, Behrendt, Christian-Alexander, Wenzel, Ulrich, Börschel, Christin S., Karakas, Mahir, Blankenberg, Stefan, and Aarabi, Ghazal

Published
2022
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18. Mapping the interplay of atrial fibrillation, brain structure, and cognitive dysfunction

Author

Petersen, Marvin, primary, Chevalier, Céleste, additional, Naegele, Felix L., additional, Ingwersen, Thies, additional, Omidvarnia, Amir, additional, Hoffstaedter, Felix, additional, Patil, Kaustubh, additional, Eickhoff, Simon B., additional, Schnabel, Renate B., additional, Kirchhof, Paulus, additional, Schlemm, Eckhard, additional, Cheng, Bastian, additional, Thomalla, Götz, additional, and Jensen, Märit, additional

Published
2024
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19. Embolic strokes of undetermined source: a clinical consensus statement of the ESC Council on Stroke, the European Association of Cardiovascular Imaging and the European Heart Rhythm Association of the ESC

Author

Ntaios, George, primary, Baumgartner, Helmut, additional, Doehner, Wolfram, additional, Donal, Erwan, additional, Edvardsen, Thor, additional, Healey, Jeff S, additional, Iung, Bernard, additional, Kamel, Hooman, additional, Kasner, Scott E, additional, Korompoki, Eleni, additional, Navi, Babak B, additional, Pristipino, Christian, additional, Saba, Luca, additional, Schnabel, Renate B, additional, Svennberg, Emma, additional, and Lip, Gregory Y H, additional

Published
2024
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20. Blood-based cardiometabolic phenotypes in atrial fibrillation and their associated risk: EAST-AFNET 4 biomolecule study

Author

Fabritz, Larissa, primary, Chua, Winnie, additional, Cardoso, Victor R, additional, Al-Taie, Christoph, additional, Borof, Katrin, additional, Suling, Anna, additional, Krause, Linda, additional, Kany, Shino, additional, Magnussen, Christina, additional, Wegscheider, Karl, additional, Breithardt, Guenter, additional, Crijns, Harry J G M, additional, Camm, A John, additional, Gkoutos, George, additional, Ellinor, Patrick T, additional, Goette, Andreas, additional, Schotten, Ulrich, additional, Wienhues-Thelen, Ursula-Henrike, additional, Zeller, Tanja, additional, Schnabel, Renate B, additional, Zapf, Antonia, additional, and Kirchhof, Paulus, additional

Published
2024
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21. Oral anticoagulation in device-detected atrial fibrillation: effects of age, sex, cardiovascular comorbidities, and kidney function on outcomes in the NOAH-AFNET 6 trial

Author

Lip, Gregory Y H, primary, Nikorowitsch, Julius, additional, Sehner, Susanne, additional, Becher, Nina, additional, Bertaglia, Emanuele, additional, Blomstrom-Lundqvist, Carina, additional, Brandes, Axel, additional, Beuger, Vincent, additional, Calvert, Melanie, additional, Camm, A John, additional, Chlouverakis, Gregory, additional, Dan, Gheorghe-Andrei, additional, Dichtl, Wolfgang, additional, Diener, Hans Christoph, additional, Fierenz, Alexander, additional, Goette, Andreas, additional, de Groot, Joris R, additional, Hermans, Astrid, additional, Lubinski, Andrzej, additional, Marijon, Eloi, additional, Merkely, Béla, additional, Mont, Lluís, additional, Ozga, Ann-Kathrin, additional, Rajappan, Kim, additional, Sarkozy, Andrea, additional, Scherr, Daniel, additional, Schnabel, Renate B, additional, Schotten, Ulrich, additional, Simantirakis, Emmanuel, additional, Toennis, Tobias, additional, Vardas, Panos, additional, Wichterle, Dan, additional, Zapf, Antonia, additional, and Kirchhof, Paulus, additional

Published
2024
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22. Rationale and Design of the Hamburg City Health Study

Author

Jagodzinski, Annika, Johansen, Christoffer, Koch-Gromus, Uwe, Aarabi, Ghazal, Adam, Gerhard, Anders, Sven, Augustin, Matthias, der Kellen, Ramona B., Beikler, Thomas, Behrendt, Christian-Alexander, Betz, Christian S., Bokemeyer, Carsten, Borof, Katrin, Briken, Peer, Busch, Chia-Jung, Büchel, Christian, Brassen, Stefanie, Debus, Eike S., Eggers, Larissa, Fiehler, Jens, Gallinat, Jürgen, Gellißen, Simone, Gerloff, Christian, Girdauskas, Evaldas, Gosau, Martin, Graefen, Markus, Härter, Martin, Harth, Volker, Heidemann, Christoph, Heydecke, Guido, Huber, Tobias B., Hussein, Yassin, Kampf, Marvin O., von dem Knesebeck, Olaf, Konnopka, Alexander, König, Hans-Helmut, Kromer, Robert, Kubisch, Christian, Kühn, Simone, Loges, Sonja, Löwe, Bernd, Lund, Gunnar, Meyer, Christian, Nagel, Lina, Nienhaus, Albert, Pantel, Klaus, Petersen, Elina, Püschel, Klaus, Reichenspurner, Hermann, Sauter, Guido, Scherer, Martin, Scherschel, Katharina, Schiffner, Ulrich, Schnabel, Renate B., Schulz, Holger, Smeets, Ralf, Sokalskis, Vladislavs, Spitzer, Martin S., Terschüren, Claudia, Thederan, Imke, Thoma, Tom, Thomalla, Götz, Waschki, Benjamin, Wegscheider, Karl, Wenzel, Jan-Per, Wiese, Susanne, Zyriax, Birgit-Christiane, Zeller, Tanja, and Blankenberg, Stefan

Published
2020

26. Systematic monitoring for detection of atrial fibrillation in patients with acute ischaemic stroke (MonDAFIS): a randomised, open-label, multicentre study

Author

Bauerle, Michael, Besselmann, Michael, Büttner, T, Dem, Petra, Diekmann, Jens, Dietzel, Joanna, Dziewas, Rainer, Ehrlich, Sven, Evens, Annette, Gahn, Georg, Günther, Albrecht, Hamann, Gerhard F, Hartmann, Andreas, Harvey, Karen Louise, Heidenreich, Fedor, Helberg, T, Hobohm, Carsten, Hoffmann, F, Hoffmann, Olaf, Jungehulsing, Gerhard J, Kampschulte, Eva-Maria, Kraft, Peter, Krogias, Christos, Leinisch, Elke, Maschke, Matthias, Merkelbach, Stefan, Muehler, Johannes, Niehaus, Ludwig, Nören, Gesa, Oschmann, P, Palm, Frederick, Petzold, Gabor C, Pfeiler, Larissa, Pfeilschifter, Waltraud, Prince, Marie, Ringleb, Peter, Rosenkranz, Michael, Royl, Georg, Schnabel, Renate B, Schurig, Johannes, Steinbrecher, A, Stingele, Robert, Tanislav, Christian, Tyler, Louise, Urbanek, Christian, Haeusler, Karl Georg, Kirchhof, Paulus, Kunze, Claudia, Tütüncü, Serdar, Fiessler, Cornelia, Malsch, Carolin, Olma, Manuel C, Jawad-Ul-Qamar, Muhammad, Krämer, Michael, Wachter, Rolf, Michalski, Dominik, Kraft, Andrea, Rizos, Timolaos, Gröschel, Klaus, Thomalla, Götz, Nabavi, Darius G, Röther, Joachim, Laufs, Ulrich, Veltkamp, Roland, Heuschmann, Peter U, and Endres, Matthias

Published
2021
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27. Transcriptome-Wide Analysis Identifies Novel Associations With Blood Pressure

Author

Zeller, Tanja, Schurmann, Claudia, Schramm, Katharina, Müller, Christian, Kwon, Soonil, Wild, Philipp S, Teumer, Alexander, Herrington, David, Schillert, Arne, Iacoviello, Licia, Kratzer, Adelheid, Jagodzinski, Annika, Karakas, Mahir, Ding, Jingzhong, Neumann, Johannes T, Kuulasmaa, Kari, Gieger, Christian, Kacprowski, Tim, Schnabel, Renate B, Roden, Michael, Wahl, Simone, Rotter, Jerome I, Ojeda, Francisco, Carstensen-Kirberg, Maren, Tregouet, David-Alexandre, Dörr, Marcus, Meitinger, Thomas, Lackner, Karl J, Wolf, Petra, Felix, Stephan B, Landmesser, Ulf, Costanzo, Simona, Ziegler, Andreas, Liu, Yongmei, Völker, Uwe, Palmas, Walter, Prokisch, Holger, Guo, Xiuqing, Herder, Christian, Blankenberg, Stefan, and Homuth, Georg

Subjects
Hypertension, Biotechnology, Human Genome, Cardiovascular, Clinical Research, Heart Disease, Genetics, 2.1 Biological and endogenous factors, Aetiology, Good Health and Well Being, Adult, Blood Pressure, Blood Pressure Determination, CCAAT-Enhancer-Binding Proteins, Carrier Proteins, Female, Gene Expression, Gene Expression Profiling, Genome-Wide Association Study, Humans, LIM Domain Proteins, Male, Myelin and Lymphocyte-Associated Proteolipid Proteins, Nucleoside Transport Proteins, Poly(ADP-ribose) Polymerases, Polymorphism, Single Nucleotide, Risk Factors, Stroke, Transcription Factors, blood pressure, gene expression, genome-wide association study, hypertension, transcriptome, Cardiorespiratory Medicine and Haematology, Clinical Sciences, Public Health and Health Services, Cardiovascular System & Hematology
Abstract

Hypertension represents a major cardiovascular risk factor. The pathophysiology of increased blood pressure (BP) is not yet completely understood. Transcriptome profiling offers possibilities to uncover genetics effects on BP. Based on 2 populations including 2549 individuals, a meta-analyses of monocytic transcriptome-wide profiles were performed to identify transcripts associated with BP. Replication was performed in 2 independent studies of whole-blood transcriptome data including 1990 individuals. For identified candidate genes, a direct link between long-term changes in BP and gene expression over time and by treatment with BP-lowering therapy was assessed. The predictive value of protein levels encoded by candidate genes for subsequent cardiovascular disease was investigated. Eight transcripts (CRIP1, MYADM, TIPARP, TSC22D3, CEBPA, F12, LMNA, and TPPP3) were identified jointly accounting for up to 13% (95% confidence interval, 8.7-16.2) of BP variability. Changes in CRIP1, MYADM, TIPARP, LMNA, TSC22D3, CEBPA, and TPPP3 expression associated with BP changes-among these, CRIP1 gene expression was additionally correlated to measures of cardiac hypertrophy. Assessment of circulating CRIP1 (cystein-rich protein 1) levels as biomarkers showed a strong association with increased risk for incident stroke (hazard ratio, 1.06; 95% confidence interval, 1.03-1.09; P=5.0×10-5). Our comprehensive analysis of global gene expression highlights 8 novel transcripts significantly associated with BP, providing a link between gene expression and BP. Translational approaches further established evidence for the potential use of CRIP1 as emerging disease-related biomarker.

Published
2017

28. Expert opinion paper on cardiac imaging after ischemic stroke

Author

Schnabel, Renate B., Camen, Stephan, Knebel, Fabian, Hagendorff, Andreas, Bavendiek, Udo, Böhm, Michael, Doehner, Wolfram, Endres, Matthias, Gröschel, Klaus, Goette, Andreas, Huttner, Hagen B., Jensen, Christoph, Kirchhof, Paulus, Korosoglou, Grigorios, Laufs, Ulrich, Liman, Jan, Morbach, Caroline, Nabavi, Darius Günther, Neumann-Haefelin, Tobias, Pfeilschifter, Waltraud, Poli, Sven, Rizos, Timolaos, Rolf, Andreas, Röther, Joachim, Schäbitz, Wolf Rüdiger, Steiner, Thorsten, Thomalla, Götz, Wachter, Rolf, and Haeusler, Karl Georg

Published
2021
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29. The budget impact of implementing atrial fibrillation-screening in European countries

Author

Eklund, Michaela, Bernfort, Lars, Appelberg, Kajsa, Engler, Daniel, Schnabel, Renate B, Martinez, Carlos, Wallenhorst, Christopher, Boriani, Giuseppe, Buckley, Claire M, Diederichsen, Søren Zöga, Svendsen, Jesper Hastrup, Montaner, Joan, Potpara, Tatjana, Levin, Lars-Åke, Lyth, Johan, Eklund, Michaela, Bernfort, Lars, Appelberg, Kajsa, Engler, Daniel, Schnabel, Renate B, Martinez, Carlos, Wallenhorst, Christopher, Boriani, Giuseppe, Buckley, Claire M, Diederichsen, Søren Zöga, Svendsen, Jesper Hastrup, Montaner, Joan, Potpara, Tatjana, Levin, Lars-Åke, and Lyth, Johan

Abstract

A budget impact analysis estimates the short-term difference between the cost of the current treatment strategy and a new treatment strategy, in this case to implement population screening for atrial fibrillation (AF). The aim of this study is to estimate the financial impact of implementing population-based AF-screening of 75-year-olds compared with the current setting of no screening from a healthcare payer perspective in eight European countries. The net budget impact of AF-screening was estimated in country-specific settings for Denmark, Germany, Ireland, Italy, Netherlands, Serbia, Spain, and Sweden. Country-specific parameters were used to allow for variations in healthcare systems and to reflect the healthcare sector in the country of interest. Similar results can be seen in all countries AF-screening incurs savings of stroke-related costs since AF treatment reduces the number of strokes. However, the increased number of detected AF and higher drug acquisition will increase the drug costs as well as the costs of physician- and control visits. The net budget impact per invited varied from 10 in Ireland to 122 in the Netherlands. The results showed the increased costs of implementing AF-screening were mainly driven by increased drug costs and screening costs. In conclusion, across Europe, though the initial cost of screening and more frequent use of oral anti-coagulants will increase the healthcare payers' costs, introducing population screening for AF will result in savings of stroke-related costs., Funding Agencies|This work has received funding from the European Union's Horizon 2020 research and innovation programme under the grant agreement No 847770 (AFFECT-EU). Data from the LOOP Study was used and LOOP was supported by Innovation Fund Denmark [grant number 12-1352259], The Research Foundation for the Capital Region of Denmark, The Danish Heart Foundation [grant number 11-04-R83-A3363-22625], Aalborg University Talent Management Program, Arvid Nilssons Fond, Skibsreder Per Henriksen, Rog Hustrus Fond, the European Union's Horizon 2020 program [grant number 847770 to the AFFECT-EU consortium], Laege Sophus Carl Emil Friis og hustru Olga Doris Friis' Legat, and an unrestricted grant from Medtronic. R.B.S. has received funding from the European Research Council (ERC) under the European Union's Horizon 2020 research and innovation programme under the grant agreement No 648131, from the European Union's Horizon 2020 research and innovation programme under the grant agreement No 847770 (AFFECT-EU) and German Center for Cardiovascular Research (DZHK e.V.) (81Z1710103 and 81Z0710114); German Ministry of Research and Education (BMBF 01ZX1408A) and ERACoSysMed3 (031L0239). Wolfgang Seefried project funding German Heart Foundation. From the European Union's Horizon Europe research and innovation programme under the grant agreement No. 101095480 (HYPERMAKER) DAS:Data available on request.

Published
2024
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30. Anticoagulation with edoxaban in patients with long atrial high-rate episodes ≥24 h

Author

Becher, Nina, Toennis, Tobias, Bertaglia, Emanuele, Blomström-Lundqvist, Carina, Brandes, Axel, Cabanelas, Nuno, Calvert, Melanie, Camm, A. John, Chlouverakis, Gregory, Dan, Gheorghe-Andrei, Dichtl, Wolfgang, Diener, Hans Christoph, Fierenz, Alexander, Goette, Andreas, de Groot, Joris R., Hermans, Astrid N. L., Lip, Gregory Y. H., Lubinski, Andrzej, Marijon, Eloi, Merkely, Bela, Mont, Lluis, Ozga, Ann-Kathrin, Rajappan, Kim, Sarkozy, Andrea, Scherr, Daniel, Schnabel, Renate B., Schotten, Ulrich, Sehner, Susanne, Simantirakis, Emmanuel, Vardas, Panos, Velchev, Vasil, Wichterle, Dan, Zapf, Antonia, Kirchhof, Paulus, Becher, Nina, Toennis, Tobias, Bertaglia, Emanuele, Blomström-Lundqvist, Carina, Brandes, Axel, Cabanelas, Nuno, Calvert, Melanie, Camm, A. John, Chlouverakis, Gregory, Dan, Gheorghe-Andrei, Dichtl, Wolfgang, Diener, Hans Christoph, Fierenz, Alexander, Goette, Andreas, de Groot, Joris R., Hermans, Astrid N. L., Lip, Gregory Y. H., Lubinski, Andrzej, Marijon, Eloi, Merkely, Bela, Mont, Lluis, Ozga, Ann-Kathrin, Rajappan, Kim, Sarkozy, Andrea, Scherr, Daniel, Schnabel, Renate B., Schotten, Ulrich, Sehner, Susanne, Simantirakis, Emmanuel, Vardas, Panos, Velchev, Vasil, Wichterle, Dan, Zapf, Antonia, and Kirchhof, Paulus

Abstract

Background and Aims Patients with long atrial high-rate episodes (AHREs) >= 24 h and stroke risk factors are often treated with anticoagulation for stroke prevention. Anticoagulation has never been compared with no anticoagulation in these patients. Methods This secondary pre-specified analysis of the Non-vitamin K antagonist Oral anticoagulants in patients with Atrial High-rate episodes (NOAH-AFNET 6) trial examined interactions between AHRE duration at baseline and anticoagulation with edoxaban compared with placebo in patients with AHRE and stroke risk factors. The primary efficacy outcome was a composite of stroke, systemic embolism, or cardiovascular death. The safety outcome was a composite of major bleeding and death. Key secondary outcomes were components of these outcomes and electrocardiogram (ECG)-diagnosed atrial fibrillation. Results Median follow-up of 2389 patients with core lab-verified AHRE was 1.8 years. AHRE >= 24 h were present at baseline in 259/2389 patients (11%, 78 +/- 7 years old, 28% women, CHA2DS2-VASc 4). Clinical characteristics were not different from patients with shorter AHRE. The primary outcome occurred in 9/132 patients with AHRE >= 24 h (4.3%/patient-year, 2 strokes) treated with anticoagulation and in 14/127 patients treated with placebo (6.9%/patient-year, 2 strokes). Atrial high-rate episode duration did not interact with the efficacy (P-interaction = .65) or safety (P-interaction = .98) of anticoagulation. Analyses including AHRE as a continuous parameter confirmed this. Patients with AHRE >= 24 h developed more ECG-diagnosed atrial fibrillation (17.0%/patient-year) than patients with shorter AHRE (8.2%/patient-year; P < .001). Conclusions This hypothesis-generating analysis does not find an interaction between AHRE duration and anticoagulation therapy in patients with device-detected AHRE and stroke risk factors. Further research is needed to identify patients with long AHRE at high stroke risk.

Published
2024
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31. C-reactive protein modifies lipoprotein(a)-related risk for coronary heart disease:the BiomarCaRE project

Author

Arnold, Natalie, Blaum, Christopher, Goßling, Alina, Brunner, Fabian J., Bay, Benjamin, Ferrario, Marco M., Brambilla, Paolo, Cesana, Giancarlo, Leoni, Valerio, Palmieri, Luigi, Donfrancesco, Chiara, Padró, Teresa, Andersson, Jonas, Jousilahti, Pekka, Ojeda, Francisco, Zeller, Tanja, Linneberg, Allan, Söderberg, Stefan, Iacoviello, Licia, Gianfagna, Francesco, Sans, Susana, Veronesi, Giovanni, Thorand, Barbara, Peters, Annette, Tunstall-Pedoe, Hugh, Kee, Frank, Salomaa, Veikko, Schnabel, Renate B., Kuulasmaa, Kari, Blankenberg, Stefan, Koenig, Wolfgang, Waldeyer, Christoph, Arnold, Natalie, Blaum, Christopher, Goßling, Alina, Brunner, Fabian J., Bay, Benjamin, Ferrario, Marco M., Brambilla, Paolo, Cesana, Giancarlo, Leoni, Valerio, Palmieri, Luigi, Donfrancesco, Chiara, Padró, Teresa, Andersson, Jonas, Jousilahti, Pekka, Ojeda, Francisco, Zeller, Tanja, Linneberg, Allan, Söderberg, Stefan, Iacoviello, Licia, Gianfagna, Francesco, Sans, Susana, Veronesi, Giovanni, Thorand, Barbara, Peters, Annette, Tunstall-Pedoe, Hugh, Kee, Frank, Salomaa, Veikko, Schnabel, Renate B., Kuulasmaa, Kari, Blankenberg, Stefan, Koenig, Wolfgang, and Waldeyer, Christoph

Abstract

Background and Aims Recent investigations have suggested an interdependence of lipoprotein(a) [Lp(a)]-related risk for cardiovascular disease with background inflammatory burden. The aim the present analysis was to investigate whether high-sensitive C-reactive protein (hsCRP) modulates the association between Lp(a) and coronary heart disease (CHD) in the general population. Methods Data from 71 678 participants from 8 European prospective population-based cohort studies were used (65 661 without/6017 with established CHD at baseline; median follow-up 9.8/13.8 years, respectively). Fine and Gray competing risk-adjusted models were calculated according to accompanying hsCRP concentration (<2 and ≥2 mg/L). Results Among CHD-free individuals, increased Lp(a) levels were associated with incident CHD irrespective of hsCRP concentration: fully adjusted sub-distribution hazard ratios [sHRs (95% confidence interval)] for the highest vs. lowest fifth of Lp(a) distribution were 1.45 (1.23–1.72) and 1.48 (1.23–1.78) for a hsCRP group of <2 and ≥2 mg/L, respectively, with no interaction found between these two biomarkers on CHD risk (Pinteraction = 0.82). In those with established CHD, similar associations were seen only among individuals with hsCRP ≥ 2 mg/L [1.34 (1.03–1.76)], whereas among participants with a hsCRP concentration <2 mg/L, there was no clear association between Lp(a) and future CHD events [1.29 (0.98–1.71)] (highest vs. lowest fifth, fully adjusted models; Pinteraction = 0.024). Conclusions While among CHD-free individuals Lp(a) was significantly associated with incident CHD regardless of hsCRP, in participants with CHD at baseline, Lp(a) was related to recurrent CHD events only in those with residual inflammatory risk. These findings might guide adequate selection of high-risk patients for forthcoming Lp(a)-targeting compounds., Background and Aims Recent investigations have suggested an interdependence of lipoprotein(a) [Lp(a)]-related risk for cardiovascular disease with background inflammatory burden. The aim the present analysis was to investigate whether high-sensitive C-reactive protein (hsCRP) modulates the association between Lp(a) and coronary heart disease (CHD) in the general population. Methods Data from 71 678 participants from 8 European prospective population-based cohort studies were used (65 661 without/6017 with established CHD at baseline; median follow-up 9.8/13.8 years, respectively). Fine and Gray competing risk-adjusted models were calculated according to accompanying hsCRP concentration (<2 and ≥2 mg/L). Results Among CHD-free individuals, increased Lp(a) levels were associated with incident CHD irrespective of hsCRP concentration: fully adjusted sub-distribution hazard ratios [sHRs (95% confidence interval)] for the highest vs. lowest fifth of Lp(a) distribution were 1.45 (1.23-1.72) and 1.48 (1.23-1.78) for a hsCRP group of <2 and ≥2 mg/L, respectively, with no interaction found between these two biomarkers on CHD risk (Pinteraction = 0.82). In those with established CHD, similar associations were seen only among individuals with hsCRP ≥ 2 mg/L [1.34 (1.03-1.76)], whereas among participants with a hsCRP concentration <2 mg/L, there was no clear association between Lp(a) and future CHD events [1.29 (0.98-1.71)] (highest vs. lowest fifth, fully adjusted models; Pinteraction = 0.024). Conclusions While among CHD-free individuals Lp(a) was significantly associated with incident CHD regardless of hsCRP, in participants with CHD at baseline, Lp(a) was related to recurrent CHD events only in those with residual inflammatory risk. These findings might guide adequate selection of high-risk patients for forthcoming Lp(a)-targeting compounds.

Published
2024

32. Antithrombotic management and outcomes of patients with atrial fibrillation treated with NOACs early at the time of market introduction: Main results from the PREFER in AF Prolongation Registry

Author

Renda, Giulia, Pecen, Ladislav, Patti, Giuseppe, Ricci, Fabrizio, Kotecha, Dipak, Siller-Matula, Jolanta M., Schnabel, Renate B., Wachter, Rolf, Sellal, Jean-Marc, Rohla, Miklos, Lucerna, Markus, Huber, Kurt, Verheugt, Freek W. A., Zamorano, Jose Luis, Brüggenjürgen, Bernd, Darius, Harald, Duytschaever, Mattias, Le Heuzey, Jean-Yves, Schilling, Richard J., Kirchhof, Paulus, and De Caterina, Raffaele

Published
2021
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33. 2024 ESC Guidelines for the management of atrial fibrillation developed in collaboration with the European Association for Cardio-Thoracic Surgery (EACTS): Developed by the task force for the management of atrial fibrillation of the European Society of Cardiology (ESC), with the special contribution of the European Heart Rhythm Association (EHRA) of the ESC. Endorsed by the European Stroke Organisation (ESO)

Author

Gelder, Isabelle C Van, Rienstra, Michiel, Bunting, Karina V, Casado-Arroyo, Ruben, Caso, Valeria, Crijns, Harry J G M, Potter, Tom J R De, Dwight, Jeremy, Guasti, Luigina, Hanke, Thorsten, Jaarsma, Tiny, Lettino, Maddalena, Løchen, Maja-Lisa, Lumbers, R Thomas, Maesen, Bart, Mølgaard, Inge, Rosano, Giuseppe M C, Sanders, Prashanthan, Schnabel, Renate B, and Suwalski, Piotr

Subjects
CARDIAC pacing, HEART failure, VENTRICULAR ejection fraction, ATRIAL flutter, BRAIN natriuretic factor, MEDICAL personnel, LOW-molecular-weight heparin, BIOPROSTHETIC heart valves, CLINICAL decision support systems
Abstract

The document titled "2024 ESC Guidelines for the management of atrial fibrillation developed in collaboration with the European Association for Cardio-Thoracic Surgery (EACTS)" provides comprehensive guidelines for the management of atrial fibrillation (AF). It covers various aspects of AF, including definitions, diagnostic criteria, symptoms, patient pathways, comorbidity and risk factor management, stroke prevention, rate and rhythm control, evaluation, and dynamic reassessment. The guidelines also address specific clinical settings, such as acute coronary syndromes, stroke, pregnancy, and congenital heart disease. Additionally, it discusses screening and prevention strategies for AF. The document aims to provide evidence-based recommendations to improve the care and outcomes of patients with AF. [Extracted from the article]

Published
2024
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34. Genetic testing in early-onset atrial fibrillation.

Author

Kany, Shinwan, Jurgens, Sean J, Rämö, Joel T, Christophersen, Ingrid E, Rienstra, Michiel, Chung, Mina K, Olesen, Morten S, Ackerman, Michael J, McNally, Elizabeth M, Semsarian, Christopher, Schnabel, Renate B, Wilde, Arthur A M, Benjamin, Emelia J, Rehm, Heidi L, Kirchhof, Paulus, Bezzina, Connie R, Roden, Dan M, Shoemaker, M Benjamin, and Ellinor, Patrick T

Subjects
GENETIC testing, ATRIAL fibrillation, PATIENT education, MEDICAL screening, CARDIOMYOPATHIES
Abstract

Atrial fibrillation (AF) is a globally prevalent cardiac arrhythmia with significant genetic underpinnings, as highlighted by recent large-scale genetic studies. A prominent clinical and genetic overlap exists between AF, heritable ventricular cardiomyopathies, and arrhythmia syndromes, underlining the potential of AF as an early indicator of severe ventricular disease in younger individuals. Indeed, several recent studies have demonstrated meaningful yields of rare pathogenic variants among early-onset AF patients (∼4%–11%), most notably for cardiomyopathy genes in which rare variants are considered clinically actionable. Genetic testing thus presents a promising opportunity to identify monogenetic defects linked to AF and inherited cardiac conditions, such as cardiomyopathy, and may contribute to prognosis and management in early-onset AF patients. A first step towards recognizing this monogenic contribution was taken with the Class IIb recommendation for genetic testing in AF patients aged 45 years or younger by the 2023 American College of Cardiology/American Heart Association guidelines for AF. By identifying pathogenic genetic variants known to underlie inherited cardiomyopathies and arrhythmia syndromes, a personalized care pathway can be developed, encompassing more tailored screening, cascade testing, and potentially genotype-informed prognosis and preventive measures. However, this can only be ensured by frameworks that are developed and supported by all stakeholders. Ambiguity in test results such as variants of uncertain significance remain a major challenge and as many as ∼60% of people with early-onset AF might carry such variants. Patient education (including pretest counselling), training of genetic teams, selection of high-confidence genes, and careful reporting are strategies to mitigate this. Further challenges to implementation include financial barriers, insurability issues, workforce limitations, and the need for standardized definitions in a fast-moving field. Moreover, the prevailing genetic evidence largely rests on European descent populations, underscoring the need for diverse research cohorts and international collaboration. Embracing these challenges and the potential of genetic testing may improve AF care. However, further research—mechanistic, translational, and clinical—is urgently needed. [ABSTRACT FROM AUTHOR]

Published
2024
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35. Atrial fibrillation burden: a new outcome predictor and therapeutic target.

Author

Becher, Nina, Metzner, Andreas, Toennis, Tobias, Kirchhof, Paulus, and Schnabel, Renate B

Subjects
STROKE, TECHNOLOGICAL innovations, ARRHYTHMIA, HEART failure patients, ATRIAL fibrillation, HEART failure
Abstract

Atrial fibrillation (AF), the most common sustained cardiac arrhythmia, is not a dichotomous disease trait. Technological innovations enable long-term rhythm monitoring in many patients and can estimate AF burden. These technologies are already used to detect and monitor AF. This review describes the relation between AF burden and outcomes and potential effects of AF burden reduction. A lower AF burden is associated with a lower risk of stroke and heart failure in patients with AF: stroke risk without anticoagulation is lower in patients with device-detected AF and a low AF burden (stroke rate 1%/year) than in patients with persistent and permanent AF (stroke rate 3%/year). Paroxysmal AF shows intermediate stroke rates (2%/year). Atrial fibrillation burden–reducing interventions can reduce cardiovascular outcomes in patients with AF: early rhythm control reduces cardiovascular events including stroke and heart failure in patients with recently diagnosed AF and cardiovascular conditions. In patients with heart failure and AF, early rhythm control and AF ablation, interventions that reduce AF burden, reduce mortality and heart failure events. Recent technological innovations allow to estimate AF burden in clinical care, creating opportunities and challenges. While evidence remains limited, the existing data already suggest that AF burden reduction could be a therapeutic goal. In addition to anticoagulation and treatment of cardiovascular conditions, AF burden reduction emerges as a therapeutic goal. Future research will define the AF burden that constitutes a relevant risk of stroke and heart failure. Technologies quantifying AF burden need careful validation to advance the field. [ABSTRACT FROM AUTHOR]

Published
2024
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38. Practical Guide on Left Atrial Appendage Closure for the Non-implanting Physician. An International Consensus Paper

Author

Potpara, Tatjana, primary, Grygier, Marek, additional, Haeusler, Karl Georg, additional, Nielsen-Kudsk, Jens Erik, additional, Berti, Sergio, additional, Genovesi, Simonetta, additional, Marijon, Eloi, additional, Boveda, Serge, additional, Tzikas, Apostolos, additional, Boriani, Giuseppe, additional, Boersma, Lucas V A, additional, Tondo, Claudio, additional, De Potter, Tom, additional, Lip, Gregory Y H, additional, Schnabel, Renate B, additional, Bauersachs, Rupert, additional, Senzolo, Marco, additional, Basile, Carlo, additional, Bianchi, Stefano, additional, Osmancik, Pavel, additional, Schmidt, Boris, additional, Landmesser, Ulf, additional, Doehner, Wolfram, additional, Hindricks, Gerhard, additional, Kovac, Jan, additional, and Camm, A John, additional

Published
2024
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39. Disturbed atrial metabolism, shear stress, and cardiac load AF after ablation: AXAFA biomolecule study

Author

Chua, Winnie, primary, Khashaba, Alya, additional, Canagarajah, Hansel, additional, Nielsen, Jens Cosedis, additional, di Biase, Luigi, additional, Haeusler, Karl Georg, additional, Hindricks, Gerhard, additional, Mont, Lluis, additional, Piccini, Jonathan, additional, Schnabel, Renate B, additional, Schotten, Ulrich, additional, Wienhues-Thelen, Ursula-Henrike, additional, Zeller, Tanja, additional, Fabritz, Larissa, additional, and Kirchhof, Paulus, additional

Published
2024
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40. C-reactive protein modifies lipoprotein(a)-related risk for coronary heart disease: the BiomarCaRE project

Author

Arnold, Natalie, primary, Blaum, Christopher, additional, Goßling, Alina, additional, Brunner, Fabian J, additional, Bay, Benjamin, additional, Ferrario, Marco M, additional, Brambilla, Paolo, additional, Cesana, Giancarlo, additional, Leoni, Valerio, additional, Palmieri, Luigi, additional, Donfrancesco, Chiara, additional, Padró, Teresa, additional, Andersson, Jonas, additional, Jousilahti, Pekka, additional, Ojeda, Francisco, additional, Zeller, Tanja, additional, Linneberg, Allan, additional, Söderberg, Stefan, additional, Iacoviello, Licia, additional, Gianfagna, Francesco, additional, Sans, Susana, additional, Veronesi, Giovanni, additional, Thorand, Barbara, additional, Peters, Annette, additional, Tunstall-Pedoe, Hugh, additional, Kee, Frank, additional, Salomaa, Veikko, additional, Schnabel, Renate B, additional, Kuulasmaa, Kari, additional, Blankenberg, Stefan, additional, Koenig, Wolfgang, additional, and Waldeyer, Christoph, additional

Published
2024
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42. Fine-mapping, novel loci identification, and SNP association transferability in a genome-wide association study of QRS duration in African Americans

Author

Evans, Daniel S, Avery, Christy L, Nalls, Mike A, Li, Guo, Barnard, John, Smith, Erin N, Tanaka, Toshiko, Butler, Anne M, Buxbaum, Sarah G, Alonso, Alvaro, Arking, Dan E, Berenson, Gerald S, Bis, Joshua C, Buyske, Steven, Carty, Cara L, Chen, Wei, Chung, Mina K, Cummings, Steven R, Deo, Rajat, Eaton, Charles B, Fox, Ervin R, Heckbert, Susan R, Heiss, Gerardo, Hindorff, Lucia A, Hsueh, Wen-Chi, Isaacs, Aaron, Jamshidi, Yalda, Kerr, Kathleen F, Liu, Felix, Liu, Yongmei, Lohman, Kurt K, Magnani, Jared W, Maher, Joseph F, Mehra, Reena, Meng, Yan A, Musani, Solomon K, Newton-Cheh, Christopher, North, Kari E, Psaty, Bruce M, Redline, Susan, Rotter, Jerome I, Schnabel, Renate B, Schork, Nicholas J, Shohet, Ralph V, Singleton, Andrew B, Smith, Jonathan D, Soliman, Elsayed Z, Srinivasan, Sathanur R, Taylor, Herman A, Van Wagoner, David R, Wilson, James G, Young, Taylor, Zhang, Zhu-Ming, Zonderman, Alan B, Evans, Michele K, Ferrucci, Luigi, Murray, Sarah S, Tranah, Gregory J, Whitsel, Eric A, Reiner, Alex P, Consortium, CHARGE QRS, and Sotoodehnia, Nona

Subjects
Biological Sciences, Genetics, Human Genome, Heart Disease, Cardiovascular, Black or African American, Alleles, Cardiovascular Diseases, Electrocardiography, Female, Genome-Wide Association Study, Genotype, Heart Ventricles, Humans, Male, Myocardium, NAV1.5 Voltage-Gated Sodium Channel, Polymorphism, Single Nucleotide, White People, CHARGE QRS Consortium, Medical and Health Sciences, Genetics & Heredity
Abstract

The electrocardiographic QRS duration, a measure of ventricular depolarization and conduction, is associated with cardiovascular mortality. While single nucleotide polymorphisms (SNPs) associated with QRS duration have been identified at 22 loci in populations of European descent, the genetic architecture of QRS duration in non-European populations is largely unknown. We therefore performed a genome-wide association study (GWAS) meta-analysis of QRS duration in 13,031 African Americans from ten cohorts and a transethnic GWAS meta-analysis with additional results from populations of European descent. In the African American GWAS, a single genome-wide significant SNP association was identified (rs3922844, P = 4 × 10-14) in intron 16 of SCN5A, a voltage-gated cardiac sodium channel gene. The QRS-prolonging rs3922844 C allele was also associated with decreased SCN5A RNA expression in human atrial tissue (P = 1.1 × 10-4). High density genotyping revealed that the SCN5A association region in African Americans was confined to intron 16. Transethnic GWAS meta-analysis identified novel SNP associations on chromosome 18 in MYL12A (rs1662342, P = 4.9 × 10-8) and chromosome 1 near CD1E and SPTA1 (rs7547997, P = 7.9 × 10-9). The 22 QRS loci previously identified in populations of European descent were enriched for significant SNP associations with QRS duration in African Americans (P = 9.9 × 10-7), and index SNP associations in or near SCN5A, SCN10A, CDKN1A, NFIA, HAND1, TBX5 and SETBP1 replicated in African Americans. In summary, rs3922844 was associated with QRS duration and SCN5A expression, two novel QRS loci were identified using transethnic meta-analysis, and a significant proportion of QRS-SNP associations discovered in populations of European descent were transferable to African Americans when adequate power was achieved.

Published
2016

43. HMG-coenzyme A reductase inhibition, type 2 diabetes, and bodyweight: evidence from genetic analysis and randomised trials

Author

Swerdlow, Daniel I, Preiss, David, Kuchenbaecker, Karoline B, Holmes, Michael V, Engmann, Jorgen EL, Shah, Tina, Sofat, Reecha, Stender, Stefan, Johnson, Paul CD, Scott, Robert A, Leusink, Maarten, Verweij, Niek, Sharp, Stephen J, Guo, Yiran, Giambartolomei, Claudia, Chung, Christina, Peasey, Anne, Amuzu, Antoinette, Li, KaWah, Palmen, Jutta, Howard, Philip, Cooper, Jackie A, Drenos, Fotios, Li, Yun R, Lowe, Gordon, Gallacher, John, Stewart, Marlene CW, Tzoulaki, Ioanna, Buxbaum, Sarah G, van der A, Daphne L, Forouhi, Nita G, Onland-Moret, N Charlotte, van der Schouw, Yvonne T, Schnabel, Renate B, Hubacek, Jaroslav A, Kubinova, Ruzena, Baceviciene, Migle, Tamosiunas, Abdonas, Pajak, Andrzej, Topor-Madry, Romanvan, Stepaniak, Urszula, Malyutina, Sofia, Baldassarre, Damiano, Sennblad, Bengt, Tremoli, Elena, de Faire, Ulf, Veglia, Fabrizio, Ford, Ian, Jukema, J Wouter, Westendorp, Rudi GJ, de Borst, Gert Jan, de Jong, Pim A, Algra, Ale, Spiering, Wilko, der Zee, Anke H Maitland-van, Klungel, Olaf H, de Boer, Anthonius, Doevendans, Pieter A, Eaton, Charles B, Robinson, Jennifer G, Duggan, David, DIAGRAM Consortium, MAGIC Consortium, Kjekshus, John, Downs, John R, Gotto, Antonio M, Keech, Anthony C, Marchioli, Roberto, Tognoni, Gianni, Sever, Peter S, Poulter, Neil R, Waters, David D, Pedersen, Terje R, Amarenco, Pierre, Nakamura, Haruo, McMurray, John JV, Lewsey, James D, Chasman, Daniel I, Ridker, Paul M, Maggioni, Aldo P, Tavazzi, Luigi, Ray, Kausik K, Seshasai, Sreenivasa Rao Kondapally, Manson, JoAnn E, Price, Jackie F, Whincup, Peter H, Morris, Richard W, Lawlor, Debbie A, Smith, George Davey, Ben-Shlomo, Yoav, Schreiner, Pamela J, Fornage, Myriam, Siscovick, David S, Cushman, Mary, Kumari, Meena, Wareham, Nick J, Verschuren, WM Monique, Redline, Susan, Patel, Sanjay R, Whittaker, John C, and Hamsten, Anders

Subjects
Epidemiology, Biomedical and Clinical Sciences, Health Sciences, Clinical Trials and Supportive Activities, Clinical Research, Genetics, Nutrition, Diabetes, 6.1 Pharmaceuticals, Evaluation of treatments and therapeutic interventions, Metabolic and endocrine, Aged, Body Mass Index, Body Weight, Cholesterol, HDL, Cholesterol, LDL, Diabetes Mellitus, Type 2, Female, Genetic Testing, Humans, Hydroxymethylglutaryl CoA Reductases, Hydroxymethylglutaryl-CoA Reductase Inhibitors, Male, Middle Aged, Polymorphism, Single Nucleotide, Randomized Controlled Trials as Topic, Risk Factors, DIAGRAM Consortium, MAGIC Consortium, InterAct Consortium, Medical and Health Sciences, General & Internal Medicine, Biomedical and clinical sciences, Health sciences
Abstract

BackgroundStatins increase the risk of new-onset type 2 diabetes mellitus. We aimed to assess whether this increase in risk is a consequence of inhibition of 3-hydroxy-3-methylglutaryl-CoA reductase (HMGCR), the intended drug target.MethodsWe used single nucleotide polymorphisms in the HMGCR gene, rs17238484 (for the main analysis) and rs12916 (for a subsidiary analysis) as proxies for HMGCR inhibition by statins. We examined associations of these variants with plasma lipid, glucose, and insulin concentrations; bodyweight; waist circumference; and prevalent and incident type 2 diabetes. Study-specific effect estimates per copy of each LDL-lowering allele were pooled by meta-analysis. These findings were compared with a meta-analysis of new-onset type 2 diabetes and bodyweight change data from randomised trials of statin drugs. The effects of statins in each randomised trial were assessed using meta-analysis.FindingsData were available for up to 223 463 individuals from 43 genetic studies. Each additional rs17238484-G allele was associated with a mean 0·06 mmol/L (95% CI 0·05-0·07) lower LDL cholesterol and higher body weight (0·30 kg, 0·18-0·43), waist circumference (0·32 cm, 0·16-0·47), plasma insulin concentration (1·62%, 0·53-2·72), and plasma glucose concentration (0·23%, 0·02-0·44). The rs12916 SNP had similar effects on LDL cholesterol, bodyweight, and waist circumference. The rs17238484-G allele seemed to be associated with higher risk of type 2 diabetes (odds ratio [OR] per allele 1·02, 95% CI 1·00-1·05); the rs12916-T allele association was consistent (1·06, 1·03-1·09). In 129 170 individuals in randomised trials, statins lowered LDL cholesterol by 0·92 mmol/L (95% CI 0·18-1·67) at 1-year of follow-up, increased bodyweight by 0·24 kg (95% CI 0·10-0·38 in all trials; 0·33 kg, 95% CI 0·24-0·42 in placebo or standard care controlled trials and -0·15 kg, 95% CI -0·39 to 0·08 in intensive-dose vs moderate-dose trials) at a mean of 4·2 years (range 1·9-6·7) of follow-up, and increased the odds of new-onset type 2 diabetes (OR 1·12, 95% CI 1·06-1·18 in all trials; 1·11, 95% CI 1·03-1·20 in placebo or standard care controlled trials and 1·12, 95% CI 1·04-1·22 in intensive-dose vs moderate dose trials).InterpretationThe increased risk of type 2 diabetes noted with statins is at least partially explained by HMGCR inhibition.FundingThe funding sources are cited at the end of the paper.

Published
2015

44. Association of glycated hemoglobin A1c levels with cardiovascular outcomes in the general population: results from the BiomarCaRE (Biomarker for Cardiovascular Risk Assessment in Europe) consortium

Author

Sinning, Christoph, Makarova, Nataliya, Völzke, Henry, Schnabel, Renate B., Ojeda, Francisco, Dörr, Marcus, Felix, Stephan B., Koenig, Wolfgang, Peters, Annette, Rathmann, Wolfgang, Schöttker, Ben, Brenner, Hermann, Veronesi, Giovanni, Cesana, Giancarlo, Brambilla, Paolo, Palosaari, Tarja, Kuulasmaa, Kari, Njølstad, Inger, Mathiesen, Ellisiv Bøgeberg, Wilsgaard, Tom, Blankenberg, Stefan, Söderberg, Stefan, Ferrario, Marco M., and Thorand, Barbara

Published
2021
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45. Sex-Specific Epidemiology of Heart Failure Risk and Mortality in Europe: Results From the BiomarCaRE Consortium

Author

Magnussen, Christina, Niiranen, Teemu J., Ojeda, Francisco M., Gianfagna, Francesco, Blankenberg, Stefan, Vartiainen, Erkki, Sans, Susana, Pasterkamp, Gerard, Hughes, Maria, Costanzo, Simona, Donati, Maria Benedetta, Jousilahti, Pekka, Linneberg, Allan, Palosaari, Tarja, de Gaetano, Giovanni, Bobak, Martin, den Ruijter, Hester M., Jørgensen, Torben, Söderberg, Stefan, Kuulasmaa, Kari, Zeller, Tanja, Iacoviello, Licia, Salomaa, Veikko, and Schnabel, Renate B.

Published
2019
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46. Oral anticoagulation in patients with left ventricular thrombus: a systematic review and meta-analysis

Author

Haller, Paul M, Kazem, Niema, Agewall, Stefan, Borghi, Claudio, Ceconi, Claudio, Dobrev, Dobromir, Cerbai, Elisabetta, Grove, Erik Lerkevang, Kaski, Juan Carlos, Lewis, Basil S, Niessner, Alexander, Rocca, Bianca, Rosano, Giuseppe, Savarese, Gianluigi, Schnabel, Renate B, Semb, Anne Grete, Sossalla, Samuel, Wassmann, Sven, and Sulzgruber, Patrick

Published
2024
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47. A Common SCN5A Variant Is Associated with PR Interval and Atrial Fibrillation Among African Americans

Author

ILKHANOFF, LEONARD, ARKING, DAN E, LEMAITRE, ROZENN N, ALONSO, ALVARO, CHEN, LIN Y, DURDA, PETER, HESSELSON, STEPHANIE E, KERR, KATHLEEN F, MAGNANI, JARED W, MARCUS, GREGORY M, SCHNABEL, RENATE B, SMITH, J GUSTAV, SOLIMAN, ELSAYED Z, REINER, ALEXANDER P, SOTOODEHNIA, NONA, and Investigators, on behalf of the Candidate‐Gene Association Resource Consortium and the Cardiac Arrest Blood Study

Subjects
Biomedical and Clinical Sciences, Cardiovascular Medicine and Haematology, Clinical Research, Atherosclerosis, Cardiovascular, Heart Disease, Good Health and Well Being, Adult, Black or African American, Aged, Aged, 80 and over, Atrial Fibrillation, Case-Control Studies, Cohort Studies, Death, Sudden, Cardiac, Female, Genetic Variation, Humans, Male, Middle Aged, NAV1.5 Voltage-Gated Sodium Channel, Prospective Studies, Risk Factors, Single-Blind Method, atrial fibrillation, electrocardiogram, genetics, PR interval, sudden death, Candidate-Gene Association Resource (CARE) Consortium and the Cardiac Arrest Blood Study (CABS) Investigators, Cardiorespiratory Medicine and Haematology, Cardiovascular System & Hematology, Cardiovascular medicine and haematology
Abstract

ObjectiveWe examined the association of rs7626962 (S1103Y) or rs7629265, a variant in high linkage disequilibrium with S1103Y (r(2) = 0.87 - 1), with sudden cardiac death (SCD) and atrial fibrillation (AF) among African Americans.BackgroundThe SCN5A missense variant S1103Y has been associated with SCD among African Americans in small case-control studies, but larger population-based studies are needed to validate these findings. The association of this variant with AF has not been fully explored.MethodsUsing genotyping data on over 7,000 African Americans from 5 cohorts (Atherosclerosis Risk in Communities [ARIC], Cleveland Family Study [CFS], Jackson Heart Study [JHS], Multi-Ethnic Study of Atherosclerosis [MESA], Cardiovascular Health Study [CHS]), we examined the association of rs7629265 with electrocardiographic PR, QRS, and QT intervals, and with incident AF and SCD. We examined association of S1103Y (rs7626962) with SCD using a population-based case-control study of SCD Cardiac Arrest Blood Study (CABS).ResultsMeta-analyses across 5 cohorts demonstrated that rs7629265 was significantly associated with PR duration (β = -4.1 milliseconds; P = 2.2×10(-6) ), but not significantly associated with QRS or QT intervals. In meta-analyses of prospectively followed ARIC and CHS participants (n = 3,656), rs7629265 was associated with increased AF risk (n = 299 AF cases; HR = 1.74, P = 1.9 × 10(-4) ). By contrast, rs7629265 was not significantly associated with SCD risk in ARIC (n = 83 SCD cases; P = 0.30) or CHS (n = 54 SCD cases; P = 0.47). Similarly, S1103Y was not significantly associated with SCD risk in CABS (n = 225 SCD cases; P = 0.29).ConclusionThe common SCN5A variant, rs7629265, is associated with increased AF risk and shorter PR interval among African Americans. In contrast to prior reports, we found no evidence of association of rs7629265 or rs7626962 (S1103Y) with SCD risk in the general population.

Published
2014

48. Pleiotropic genes for metabolic syndrome and inflammation

Author

Kraja, Aldi T, Chasman, Daniel I, North, Kari E, Reiner, Alexander P, Yanek, Lisa R, Kilpeläinen, Tuomas O, Smith, Jennifer A, Dehghan, Abbas, Dupuis, Josée, Johnson, Andrew D, Feitosa, Mary F, Tekola-Ayele, Fasil, Chu, Audrey Y, Nolte, Ilja M, Dastani, Zari, Morris, Andrew, Pendergrass, Sarah A, Sun, Yan V, Ritchie, Marylyn D, Vaez, Ahmad, Lin, Honghuang, Ligthart, Symen, Marullo, Letizia, Rohde, Rebecca, Shao, Yaming, Ziegler, Mark A, Im, Hae Kyung, Group, Cross Consortia Pleiotropy, Heart and, the Cohorts for, Epidemiology, Aging Research in Genetic, Consortium, the Genetic Investigation of Anthropometric Traits, Consortium, the Global Lipids Genetics, the Meta-Analyses of Glucose, Consortium, Insulin-related traits, Consortium, the Global BPgen, Consortium, The ADIPOGen, Study, the Women's Genome Health, Study, the Howard University Family, Schnabel, Renate B, Jørgensen, Torben, Jørgensen, Marit E, Hansen, Torben, Pedersen, Oluf, Stolk, Ronald P, Snieder, Harold, Hofman, Albert, Uitterlinden, Andre G, Franco, Oscar H, Ikram, M Arfan, Richards, J Brent, Rotimi, Charles, Wilson, James G, Lange, Leslie, Ganesh, Santhi K, Nalls, Mike, Rasmussen-Torvik, Laura J, Pankow, James S, Coresh, Josef, Tang, Weihong, Kao, WH Linda, Boerwinkle, Eric, Morrison, Alanna C, Ridker, Paul M, Becker, Diane M, Rotter, Jerome I, Kardia, Sharon LR, Loos, Ruth JF, Larson, Martin G, Hsu, Yi-Hsiang, Province, Michael A, Tracy, Russell, Voight, Benjamin F, Vaidya, Dhananjay, O'Donnell, Christopher J, Benjamin, Emelia J, Alizadeh, Behrooz Z, Prokopenko, Inga, Meigs, James B, and Borecki, Ingrid B

Subjects
Biological Sciences, Biomedical and Clinical Sciences, Genetics, Nutrition, Diabetes, Clinical Research, Human Genome, Cardiovascular, Obesity, Prevention, 2.1 Biological and endogenous factors, Biomarkers, Computational Biology, Gene Regulatory Networks, Genetic Pleiotropy, Genetic Predisposition to Disease, Genome-Wide Association Study, Humans, Inflammation, Meta-Analysis as Topic, Metabolic Syndrome, Phenotype, Quantitative Trait, Heritable, Metabolic syndrome, Inflammatory markers, Pleiotropic associations, Meta-analysis, Regulome, Cross Consortia Pleiotropy Group, Cohorts for Heart and, Aging Research in Genetic Epidemiology, Genetic Investigation of Anthropometric Traits Consortium, Global Lipids Genetics Consortium, Meta-Analyses of Glucose, Insulin-related traits Consortium, Global BPgen Consortium, ADIPOGen Consortium, Women's Genome Health Study, Howard University Family Study, Clinical Sciences, Genetics & Heredity, Clinical sciences
Abstract

Metabolic syndrome (MetS) has become a health and financial burden worldwide. The MetS definition captures clustering of risk factors that predict higher risk for diabetes mellitus and cardiovascular disease. Our study hypothesis is that additional to genes influencing individual MetS risk factors, genetic variants exist that influence MetS and inflammatory markers forming a predisposing MetS genetic network. To test this hypothesis a staged approach was undertaken. (a) We analyzed 17 metabolic and inflammatory traits in more than 85,500 participants from 14 large epidemiological studies within the Cross Consortia Pleiotropy Group. Individuals classified with MetS (NCEP definition), versus those without, showed on average significantly different levels for most inflammatory markers studied. (b) Paired average correlations between 8 metabolic traits and 9 inflammatory markers from the same studies as above, estimated with two methods, and factor analyses on large simulated data, helped in identifying 8 combinations of traits for follow-up in meta-analyses, out of 130,305 possible combinations between metabolic traits and inflammatory markers studied. (c) We performed correlated meta-analyses for 8 metabolic traits and 6 inflammatory markers by using existing GWAS published genetic summary results, with about 2.5 million SNPs from twelve predominantly largest GWAS consortia. These analyses yielded 130 unique SNPs/genes with pleiotropic associations (a SNP/gene associating at least one metabolic trait and one inflammatory marker). Of them twenty-five variants (seven loci newly reported) are proposed as MetS candidates. They map to genes MACF1, KIAA0754, GCKR, GRB14, COBLL1, LOC646736-IRS1, SLC39A8, NELFE, SKIV2L, STK19, TFAP2B, BAZ1B, BCL7B, TBL2, MLXIPL, LPL, TRIB1, ATXN2, HECTD4, PTPN11, ZNF664, PDXDC1, FTO, MC4R and TOMM40. Based on large data evidence, we conclude that inflammation is a feature of MetS and several gene variants show pleiotropic genetic associations across phenotypes and might explain a part of MetS correlated genetic architecture. These findings warrant further functional investigation.

Published
2014

49. Large multiethnic Candidate Gene Study for C-reactive protein levels: identification of a novel association at CD36 in African Americans

Author

Ellis, Jaclyn, Lange, Ethan M, Li, Jin, Dupuis, Josee, Baumert, Jens, Walston, Jeremy D, Keating, Brendan J, Durda, Peter, Fox, Ervin R, Palmer, Cameron D, Meng, Yan A, Young, Taylor, Farlow, Deborah N, Schnabel, Renate B, Marzi, Carola S, Larkin, Emma, Martin, Lisa W, Bis, Joshua C, Auer, Paul, Ramachandran, Vasan S, Gabriel, Stacey B, Willis, Monte S, Pankow, James S, Papanicolaou, George J, Rotter, Jerome I, Ballantyne, Christie M, Gross, Myron D, Lettre, Guillaume, Wilson, James G, Peters, Ulrike, Koenig, Wolfgang, Tracy, Russell P, Redline, Susan, Reiner, Alex P, Benjamin, Emelia J, and Lange, Leslie A

Subjects
Biological Sciences, Genetics, Human Genome, Clinical Research, Cardiovascular, Heart Disease, Adult, Black or African American, Aged, Biomarkers, C-Reactive Protein, CD36 Antigens, Cardiovascular Diseases, Female, Genetic Loci, Genetic Predisposition to Disease, Genetics, Population, Genome-Wide Association Study, Humans, Meta-Analysis as Topic, Middle Aged, Polymorphism, Single Nucleotide, Risk Factors, Complementary and Alternative Medicine, Paediatrics and Reproductive Medicine, Genetics & Heredity, Reproductive medicine
Abstract

C-reactive protein (CRP) is a heritable biomarker of systemic inflammation and a predictor of cardiovascular disease (CVD). Large-scale genetic association studies for CRP have largely focused on individuals of European descent. We sought to uncover novel genetic variants for CRP in a multiethnic sample using the ITMAT Broad-CARe (IBC) array, a custom 50,000 SNP gene-centric array having dense coverage of over 2,000 candidate CVD genes. We performed analyses on 7,570 African Americans (AA) from the Candidate gene Association Resource (CARe) study and race-combined meta-analyses that included 29,939 additional individuals of European descent from CARe, the Women's Health Initiative (WHI) and KORA studies. We observed array-wide significance (p < 2.2 × 10(-6)) for four loci in AA, three of which have been reported previously in individuals of European descent (IL6R, p = 2.0 × 10(-6); CRP, p = 4.2 × 10(-71); APOE, p = 1.6 × 10(-6)). The fourth significant locus, CD36 (p = 1.6 × 10(-6)), was observed at a functional variant (rs3211938) that is extremely rare in individuals of European descent. We replicated the CD36 finding (p = 1.8 × 10(-5)) in an independent sample of 8,041 AA women from WHI; a meta-analysis combining the CARe and WHI AA results at rs3211938 reached genome-wide significance (p = 1.5 × 10(-10)). In the race-combined meta-analyses, 13 loci reached significance, including ten (CRP, TOMM40/APOE/APOC1, HNF1A, LEPR, GCKR, IL6R, IL1RN, NLRP3, HNF4A and BAZ1B/BCL7B) previously associated with CRP, and one (ARNTL) previously reported to be nominally associated with CRP. Two novel loci were also detected (RPS6KB1, p = 2.0 × 10(-6); CD36, p = 1.4 × 10(-6)). These results highlight both shared and unique genetic risk factors for CRP in AA compared to populations of European descent.

Published
2014

50. Safety and efficacy of long-term sodium channel blocker therapy for early rhythm control: the EAST-AFNET 4 trial.

Author

Rillig, Andreas, Eckardt, Lars, Borof, Katrin, Camm, A John, Crijns, Harry J G M, Goette, Andreas, Breithardt, Günter, Lemoine, Marc D, Metzner, Andreas, Rottner, Laura, Schotten, Ulrich, Vettorazzi, Eik, Wegscheider, Karl, Zapf, Antonia, Heidbuchel, Hein, Willems, Stephan, Fabritz, Larissa, Schnabel, Renate B, Magnussen, Christina, and Kirchhof, Paulus

Abstract

Aims Clinical concerns exist about the potential proarrhythmic effects of the sodium channel blockers (SCBs) flecainide and propafenone in patients with cardiovascular disease. Sodium channel blockers were used to deliver early rhythm control (ERC) therapy in EAST-AFNET 4. Methods and results We analysed the primary safety outcome (death, stroke, or serious adverse events related to rhythm control therapy) and primary efficacy outcome (cardiovascular death, stroke, and hospitalization for worsening of heart failure (HF) or acute coronary syndrome) during SCB intake for patients with ERC (n = 1395) in EAST-AFNET 4. The protocol discouraged flecainide and propafenone in patients with reduced left ventricular ejection fraction and suggested stopping therapy upon QRS prolongation >25% on therapy. Flecainide or propafenone was given to 689 patients [age 69 (8) years; CHA2DS2-VASc 3.2 (1); 177 with HF; 41 with prior myocardial infarction, coronary artery bypass graft, or percutaneous coronary intervention; 26 with left ventricular hypertrophy >15 mm; median therapy duration 1153 [237, 1828] days]. The primary efficacy outcome occurred less often in patients treated with SCB [3/100 (99/3316) patient-years] than in patients who never received SCB [SCBnever 4.9/100 (150/3083) patient-years, P < 0.001]. There were numerically fewer primary safety outcomes in patients receiving SCB [2.9/100 (96/3359) patient-years] than in SCBnever patients [4.2/100 (135/3220) patient-years, adjusted P = 0.015]. Sinus rhythm at 2 years was similar between groups [SCB 537/610 (88); SCBnever 472/579 (82)]. Conclusion Long-term therapy with flecainide or propafenone appeared to be safe in the EAST-AFNET 4 trial to deliver effective ERC therapy, including in selected patients with stable cardiovascular disease such as coronary artery disease and stable HF. Clinical Trial Registration ISRCTN04708680, NCT01288352, EudraCT2010-021258-20, www.easttrial.org [ABSTRACT FROM AUTHOR]

Published
2024
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