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共有 62504 条符合本次的查询结果, 用时 2.2809665 秒

1361. Discrimination Between Anterior and Posterior Left Atrial Roof Area Ablation by a Cryoballoon.

作者: Tetsuma Kawaji.;Takanori Aizawa.;Misaki Naka.;Saki Yamano.;Bao Bingyuan.;Shun Hojo.;Yuji Tezuka.;Shintaro Matsuda.;Masashi Kato.;Takafumi Yokomatsu.;Shinji Miki.
来源: Circ Arrhythm Electrophysiol. 2025年18卷1期e013093页

1362. Impact of Age on Smartphone-Based Screening for Atrial Fibrillation: A Prespecified Subgroup Analysis of the eBRAVE-AF Trial.

作者: Luisa Freyer.;Peter Spielbichler.;Lukas von Stülpnagel.;Aresa Krasniqi.;Maximilian Wörndl.;Lukas Tenbrink.;Laura Elisa Villegas Sierra.;Maria F Vogl.;Lauren E Sams.;Ann-Kathrin Mayer.;Michael Schreinlechner.;Elodie Eiffener.;Annika Schneidewind.;Mathias Klemm.;Steffen Massberg.;Axel Bauer.;Konstantinos D Rizas.
来源: Circ Arrhythm Electrophysiol. 2025年18卷1期e013293页

1363. Left Ventricular Ejection Fraction and Implantable Cardioverter Defibrillator in Nonischemic Heart Failure With Reduced Ejection Fraction: Insights From DANISH.

作者: Seiko N Doi.;Jawad H Butt.;Jens Jakob Thune.;Jens C Nielsen.;Jens Haarbo.;Niels E Bruun.;Line L Olesen.;Lars Videbæk.;Finn Gustafsson.;Hans Eiskjær.;Christian Hassager.;Jesper H Svendsen.;Dan E Høfsten.;Steen Pehrson.;Lars Køber.
来源: Circulation. 2025年151卷12期887-889页

1364. Elevated Donor-Derived Cell-Free DNA Levels Are Associated With Reduced Myocardial Blood Flow but Not Angiographic Cardiac Allograft Vasculopathy: The EVIDENT Study.

作者: Cathrine M Moeller.;Daniel Oren.;Andrea Fernandez Valledor.;Gal Rubinstein.;Ersilia M DeFilippis.;Salwa Rahman.;Yonatan Mehlman.;Elena M Donald.;Dor Lotan.;Edward Lin.;Kyung T Oh.;Sun H Lee.;Jayant K Raikhelkar.;Justin A Fried.;David Majure.;Farhana Latif.;Gabriel T Sayer.;Nir Uriel.;Kevin J Clerkin.
来源: Circ Heart Fail. 2025年18卷1期e011756页
Cardiac allograft vasculopathy (CAV) leads to impaired myocardial blood flow (MBF), increasing the risk of cardiovascular death or retransplant among heart transplantation (HT) recipients. Data on elevation in donor-derived cell-free DNA (dd-cfDNA) and CAV in the absence of rejection are mixed. We sought to test the hypothesis that CAV with reduced MBF (RMBF) is associated with elevated dd-cfDNA.

1365. Inositol 1,4,5-Trisphosphate Receptor 1 Gain-of-Function Increases the Risk for Cardiac Arrhythmias in Mice and Humans.

作者: Bo Sun.;Mingke Ni.;Yanhui Li.;Zhenpeng Song.;Hui Wang.;Hai-Lei Zhu.;Jinhong Wei.;Darrell Belke.;Shitian Cai.;Wenting Guo.;Jinjing Yao.;Shanshan Tian.;John Paul Estillore.;Ruiwu Wang.;Mads Toft Søndergaard.;Malene Brohus.;Palle Duun Rohde.;Yongxin Mu.;Alexander Vallmitjana.;Raul Benitez.;Leif Hove-Madsen.;Michael Toft Overgaard.;Glenn I Fishman.;Ju Chen.;Shubhayan Sanatani.;Arthur A M Wilde.;Michael Fill.;Josefina Ramos-Franco.;Mette Nyegaard.;S R Wayne Chen.
来源: Circulation. 2025年151卷12期847-862页
Ca2+ mishandling in cardiac Purkinje cells is a well-known cause of cardiac arrhythmias. The Purkinje cell resident inositol 1,4,5-trisphosphate receptor 1 (ITPR1) is believed to play an important role in Ca2+ handling, and ITPR1 gain-of-function (GOF) has been implicated in cardiac arrhythmias. However, nearly all known disease-associated ITPR1 variants are loss-of-function and are primarily linked to neurological disorders. Whether ITPR1 GOF has pathological consequences, such as cardiac arrhythmias, is unclear. This study aimed to identify human ITPR1 GOF variants and determine the impact of ITPR1 GOF on Ca2+ handling and arrhythmia susceptibility.

1366. Cognitive Dysfunction in Heart Failure With Preserved Ejection Fraction: Uncovering the Consequences of an Overlooked Comorbidity.

作者: Jesús Álvarez-García.
来源: Circulation. 2024年150卷24期1928-1930页

1367. Letter by Huang et al Regarding Article, "Atherosclerosis Is a Smooth Muscle Cell-Driven Tumor-Like Disease".

作者: Huixin Huang.;Xuqi Yang.;Kai Yang.
来源: Circulation. 2024年150卷24期e517-e518页

1368. Precision Medicine in People at Risk for Diabetes and Atherosclerotic Cardiovascular Disease: A Fresh Perspective on Prevention.

作者: Andreas L Birkenfeld.;Paul W Franks.;Viswanathan Mohan.
来源: Circulation. 2024年150卷24期1910-1912页

1369. A Polygenic Predictor of Baseline QTc is Associated With Sotalol-Induced QT Prolongation.

作者: Megan C Lancaster.;Giovanni Davogustto.;Edi Prifti.;Claire Perret.;Christian Funck-Brentano.;Dan M Roden.;Joe-Elie Salem.
来源: Circulation. 2024年150卷24期1984-1986页

1370. Scientific and Clinical Impacts of UK Biobank in Cardiovascular Medicine.

作者: Adam J Lewandowski.;Martin K Rutter.;Rory Collins.
来源: Circulation. 2024年150卷24期1907-1909页

1371. Clinical Management and Transplant Considerations in Pediatric Pulmonary Hypertension Due to Left Heart Disease: A Scientific Statement From the American Heart Association.

作者: Rachel K Hopper.;Georg Hansmann.;Seth A Hollander.;Anne I Dipchand.;Oscar van der Have.;Colleen Iler.;Cynthia Herrington.;Erika B Rosenzweig.;Juan C Alejos.;Karin Tran-Lundmark.; .
来源: Circ Heart Fail. 2025年18卷1期e000086页
Children with left heart disease are at risk for developing pulmonary hypertension, initially secondary to pulmonary venous hypertension that can progress to include elevated pulmonary vascular resistance, known as combined pre- and postcapillary pulmonary hypertension. Elevated pulmonary vascular resistance may pose a risk to the right ventricle of a newly transplanted heart because of increased afterload and is an important consideration for heart transplant eligibility. However, the epidemiology, pathophysiology, optimal diagnostic and treatment approaches, and thresholds for pulmonary vascular resistance in pulmonary hypertension associated with left heart disease remain unclear because of lack of evidence, particularly in pediatrics. The result is heterogeneity with respect to hemodynamic assessment, use of pulmonary vasodilator therapies, and heart transplant listing. This scientific statement aims to synthesize the available data and highlight areas of general consensus as well as important knowledge gaps.

1372. Insights From a 20-Year Follow-Up of the First Heart Transplant Recipient to Complete an Ironman Triathlon.

作者: Stephen J Foulkes.;Rachel J Skow.;Andre La Gerche.;Wayne J Tymchak.;Mark J Haykowsky.
来源: Circ Heart Fail. 2025年18卷3期e012027页

1373. Aerobic Capacity of Adults With Fontan Palliation: Disease-Specific Reference Values and Relationship to Outcomes.

作者: Alexander C Egbe.;Ahmed E Ali.;William R Miranda.;Heidi M Connolly.;Barry A Borlaug.
来源: Circ Heart Fail. 2025年18卷2期e011981页
Patients with Fontan palliation have reduced aerobic capacity because of impaired cardiac, pulmonary, and skeletal muscle function. However, the assessment of aerobic capacity in this population still relies on comparisons with people without cardiovascular disease rather than comparison with the expected aerobic capacity of other Fontan patients. The purpose of this study was to determine the expected aerobic capacity of adults with Fontan palliation.

1374. Cognitive and Procedural Competencies in the Cardiac Intensive Care Unit.

作者: Willard N Applefeld.;Jacob C Jentzer.;Saraschandra Vallabhajosyula.
来源: Circ Heart Fail. 2025年18卷2期e011641页

1375. Association of T-Cell Phenotypes With Peri-Coronary Inflammation in People With and Without HIV and Without Cardiovascular Disease.

作者: Michael L Freeman.;Mian B Hossain.;Shana A B Burrowes.;Jean Jeudy.;Felisa Diaz-Mendez.;Sarah E Mitchell.;Sumanth D Prabhu.;Michael M Lederman.;Shashwatee Bagchi.
来源: Circ Cardiovasc Imaging. 2025年18卷1期e017033页
Persistent immune activation is linked to elevated cardiovascular diseases in people with HIV on antiretroviral therapy. The fat attenuation index (FAI) is a measure of peri-coronary inflammation that independently predicts cardiovascular disease risk in people without HIV. Whether FAI is associated with immune activation is unknown.

1376. Assessing the Accuracy of Cardiovascular Disease Prediction Using Female-Specific Risk Factors in Women Aged 45 to 69 Years in the UK Biobank Study.

作者: Jenny Doust.;Mohammad Reza Baneshi.;Hsin-Fang Chung.;Louise Forsyth Wilson.;Gita Devi Mishra.
来源: Circ Cardiovasc Qual Outcomes. 2024年17卷12期e010842页
Cardiovascular disease (CVD) is the leading cause of mortality in women. We aimed to assess whether adding female-specific risk factors to traditional factors could improve CVD risk prediction.

1377. Female-Specific Risk Factors in Cardiovascular Disease: Important or Superfluous?

作者: Setareh Salehi Omran.;Michelle Leppert.
来源: Circ Cardiovasc Qual Outcomes. 2024年17卷12期e011666页

1378. Sympathetic Response to 1-Leg Cycling Exercise Predicts Exercise Capacity in Patients With Heart Failure With Preserved Ejection Fraction.

作者: Mark B Badrov.;Tomoyuki Tobushi.;Catherine F Notarius.;Evan Keys.;Massimo Nardone.;David Z Cherney.;Susanna Mak.;John S Floras.
来源: Circ Heart Fail. 2025年18卷1期e011962页
In heart failure, sympathetic excess and exercise intolerance impair quality of life. In heart failure with reduced ejection fraction, exercise stimulates a reflex increase in muscle sympathetic nerve activity (MSNA) that relates inversely to peak oxygen uptake (V̇O2peak). Whether similar sympathoexcitatory responses are present in heart failure with preserved EF (HFpEF) and relate to V̇O2peak are unknown.

1379. Low Penetrance Sarcomere Variants Contribute to Additive Risk in Hypertrophic Cardiomyopathy.

作者: Joshua K Meisner.;Aaron Renberg.;Eric D Smith.;Yao-Chang Tsan.;Brynn Elder.;Abbey Bullard.;Owen L Merritt.;Sean L Zheng.;Neal K Lakdawala.;Anjali T Owens.;Thomas D Ryan.;Erin M Miller.;Joseph W Rossano.;Kimberly Y Lin.;Brian L Claggett.;Euan A Ashley.;Michelle Michels.;Rachel Lampert.;John C Stendahl.;Dominic Abrams.;Christopher Semsarian.;Victoria N Parikh.;Matthew T Wheeler.;Jodie Ingles.;Iacopo Olivotto.;Sharlene M Day.;Sara Saberi.;Mark W Russell.;Michael Previs.;Carolyn Y Ho.;James S Ware.;Adam S Helms.
来源: Circulation. 2025年151卷11期783-798页
Classically, hypertrophic cardiomyopathy (HCM) has been viewed as a single-gene (monogenic) disease caused by pathogenic variants in sarcomere genes. Pathogenic sarcomere variants are individually rare and convey high risk for developing HCM (highly penetrant). Recently, important polygenic contributions have also been characterized. Low penetrance sarcomere variants (LowSVs) at intermediate frequencies and effect sizes have not been systematically investigated. We hypothesize that LowSVs may be common in HCM with substantial influence on disease risk and severity.

1380. Sickle Trait and Alpha Thalassemia Increase NOS-Dependent Vasodilation of Human Arteries Through Disruption of Endothelial Hemoglobin-eNOS Interactions.

作者: Steven D Brooks.;A Parker Ruhl.;Xianke Zeng.;Phillip Cruz.;Sergio A Hassan.;Olena Kamenyeva.;Md Abdul Hakim.;Lauryn A Ridley.;Bianca M Nagata.;Juraj Kabat.;Sundar Ganesan.;Rachel L Smith.;Mary Jackson.;Jessica Nino de Rivera.;Alison J McLure.;Jarrett M Jackson.;Robert O Emeh.;Naomi Tesfuzigta.;Kyeisha Laurence.;Stacy Joyce.;Christina Yek.;Sophana Chea.;Derron A Alves.;Brant E Isakson.;Jessica Manning.;Jeremy L Davis.;Hans C Ackerman.
来源: Circulation. 2025年151卷1期8-30页
Severe malaria is associated with impaired nitric oxide (NO) synthase (NOS)-dependent vasodilation, and reversal of this deficit improves survival in murine models. Malaria might have selected for genetic polymorphisms that increase endothelial NO signaling and now contribute to heterogeneity in vascular function among humans. One protein potentially selected for is alpha globin, which, in mouse models, interacts with endothelial NOS (eNOS) to negatively regulate NO signaling. We sought to evaluate the impact of alpha globin gene deletions on NO signaling and unexpectedly found human arteries use not only alpha but also beta globin to regulate eNOS.
共有 62504 条符合本次的查询结果, 用时 2.2809665 秒