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1. Immunobiology of fibrin-based engineered heart tissue.

Author

Conradi, Lenard, Schmidt, Stephanie, Neofytou, Evgenios, Deuse, Tobias, Peters, Laura, Eder, Alexandra, Hua, Xiaoqin, Hansen, Arne, Robbins, Robert C, Beygui, Ramin E, Reichenspurner, Hermann, Eschenhagen, Thomas, and Schrepfer, Sonja

Subjects
Myocardium, Th1 Cells, Animals, Rats, Fibrin, Transplantation, Isogeneic, Tissue Engineering, Graft Rejection, Graft Survival, Tissue Scaffolds, Allografts, Bioluminescence imaging, Engineered heart tissue, Immune response, Rat, Rejection, Scaffold, Heart Disease, Transplantation, Cardiovascular, Stem Cell Research, Regenerative Medicine, Bioengineering, 5.2 Cellular and gene therapies, Development of treatments and therapeutic interventions, Biochemistry and Cell Biology, Medical Biotechnology, Clinical Sciences
Abstract

UnlabelledDifferent tissue-engineering approaches have been developed to induce and promote cardiac regeneration; however, the impact of the immune system and its responses to the various scaffold components of the engineered grafts remains unclear. Fibrin-based engineered heart tissue (EHT) was generated from neonatal Lewis (Lew) rat heart cells and transplanted onto the left ventricular surface of three different rat strains: syngeneic Lew, allogeneic Brown Norway, and immunodeficient Rowett Nude rats. Interferon spot frequency assay results showed similar degrees of systemic immune activation in the syngeneic and allogeneic groups, whereas no systemic immune response was detectable in the immunodeficient group (p < .001 vs. syngeneic and allogeneic). Histological analysis revealed much higher local infiltration of CD3- and CD68-positive cells in syngeneic and allogeneic rats than in immunodeficient animals. Enzyme-linked immunospot and immunofluorescence experiments revealed matrix-directed TH1-based rejection in syngeneic recipients without collateral impairment of heart cell survival. Bioluminescence imaging was used for in vivo longitudinal monitoring of transplanted luciferase-positive EHT constructs. Survival was documented in syngeneic and immunodeficient recipients for a period of up to 110 days after transplant, whereas in the allogeneic setting, graft survival was limited to only 14 ± 1 days. EHT strategies using autologous cells are promising approaches for cardiac repair applications. Although fibrin-based scaffold components elicited an immune response in our studies, syngeneic cells carried in the EHT were relatively unaffected.SignificanceAn initial insight into immunological consequences after transplantation of engineered heart tissue was gained through this study. Most important, this study was able to demonstrate cell survival despite rejection of matrix components. Generation of syngeneic human engineered heart tissue, possibly using human induced pluripotent stem cell technology with subsequent directed rejection of matrix components, may be a potential future approach to replace diseased myocardium.

Published
2015

2. Dichloroacetate prevents restenosis in preclinical animal models of vessel injury

Author

Deuse, Tobias, Hua, Xiaoqin, Wang, Dong, Maegdefessel, Lars, Heeren, Joerg, Scheja, Ludger, Bolaños, Juan P, Rakovic, Aleksandar, Spin, Joshua M, Stubbendorff, Mandy, Ikeno, Fumiaki, Länger, Florian, Zeller, Tanja, Schulte-Uentrop, Leonie, Stoehr, Andrea, Itagaki, Ryo, Haddad, Francois, Eschenhagen, Thomas, Blankenberg, Stefan, Kiefmann, Rainer, Reichenspurner, Hermann, Velden, Joachim, Klein, Christine, Yeung, Alan, Robbins, Robert C, Tsao, Philip S, and Schrepfer, Sonja

Subjects
Biochemistry and Cell Biology, Biomedical and Clinical Sciences, Biological Sciences, Prevention, 5.1 Pharmaceuticals, Development of treatments and therapeutic interventions, Cardiovascular, Angioplasty, Balloon, Animals, Aorta, Apoptosis, Arteries, Cell Proliferation, Constriction, Pathologic, Coronary Vessels, Dichloroacetic Acid, Disease Models, Animal, Enzyme Activation, Gene Knockdown Techniques, Humans, Hyperplasia, Iliac Artery, Mammary Arteries, Membrane Potential, Mitochondrial, Mitochondria, Heart, Myocytes, Smooth Muscle, Protein Serine-Threonine Kinases, Pyruvate Dehydrogenase Acetyl-Transferring Kinase, Rabbits, Rats, Secondary Prevention, Stents, Swine, Tunica Intima, Protein-Serine-Threonine Kinases, General Science & Technology
Abstract

Despite the introduction of antiproliferative drug-eluting stents, coronary heart disease remains the leading cause of death in the United States. In-stent restenosis and bypass graft failure are characterized by excessive smooth muscle cell (SMC) proliferation and concomitant myointima formation with luminal obliteration. Here we show that during the development of myointimal hyperplasia in human arteries, SMCs show hyperpolarization of their mitochondrial membrane potential (ΔΨm) and acquire a temporary state with a high proliferative rate and resistance to apoptosis. Pyruvate dehydrogenase kinase isoform 2 (PDK2) was identified as a key regulatory protein, and its activation proved necessary for relevant myointima formation. Pharmacologic PDK2 blockade with dichloroacetate or lentiviral PDK2 knockdown prevented ΔΨm hyperpolarization, facilitated apoptosis and reduced myointima formation in injured human mammary and coronary arteries, rat aortas, rabbit iliac arteries and swine (pig) coronary arteries. In contrast to several commonly used antiproliferative drugs, dichloroacetate did not prevent vessel re-endothelialization. Targeting myointimal ΔΨm and alleviating apoptosis resistance is a novel strategy for the prevention of proliferative vascular diseases.

Published
2014

3. Inducing myointimal hyperplasia versus atherosclerosis in mice: an introduction of two valid models.

Author

Stubbendorff, Mandy, Hua, Xiaoqin, Deuse, Tobias, Ali, Ziad, Reichenspurner, Hermann, Maegdefessel, Lars, Robbins, Robert C, and Schrepfer, Sonja

Subjects
Biochemistry and Cell Biology, Biological Sciences, Heart Disease - Coronary Heart Disease, Aging, Cardiovascular, Bioengineering, Atherosclerosis, Heart Disease, Animals, Apolipoproteins E, Disease Models, Animal, Female, Hyperplasia, Male, Mice, Mice, Inbred C57BL, Plaque, Atherosclerotic, Reproducibility of Results, Tunica Intima, Medicine, Issue 87, vascular diseases, atherosclerosis, coronary stenosis, neointima, myointimal hyperplasia, mice, denudation model, ApoE -/-, balloon injury, western diet, analysis, Psychology, Cognitive Sciences, Biochemistry and cell biology
Abstract

Various in vivo laboratory rodent models for the induction of artery stenosis have been established to mimic diseases that include arterial plaque formation and stenosis, as observed for example in ischemic heart disease. Two highly reproducible mouse models - both resulting in artery stenosis but each underlying a different pathway of development - are introduced here. The models represent the two most common causes of artery stenosis; namely one mouse model for each myointimal hyperplasia, and atherosclerosis are shown. To induce myointimal hyperplasia, a balloon catheter injury of the abdominal aorta is performed. For the development of atherosclerotic plaque, the ApoE -/- mouse model in combination with western fatty diet is used. Different model-adapted options for the measurement and evaluation of the results are named and described in this manuscript. The introduction and comparison of these two models provides information for scientists to choose the appropriate artery stenosis model in accordance to the scientific question asked.

Published
2014

6. The Potassium Channel KCa3.1 as New Therapeutic Target for the Prevention of Obliterative Airway Disease

Author

Hua, Xiaoqin, Deuse, Tobias, Chen, Yi-Je, Wulff, Heike, Stubbendorff, Mandy, Köhler, Ralf, Miura, Hiroto, Länger, Florian, Reichenspurner, Hermann, Robbins, Robert C, and Schrepfer, Sonja

Subjects
Medical Physiology, Biomedical and Clinical Sciences, Prevention, Genetics, 2.1 Biological and endogenous factors, Aetiology, Animals, Bronchiolitis Obliterans, Cell Proliferation, Disease Models, Animal, Enzyme-Linked Immunospot Assay, Genetic Therapy, Intermediate-Conductance Calcium-Activated Potassium Channels, Isoantibodies, Lymphocyte Activation, Macrophages, Male, Mice, Mice, Inbred C57BL, Mice, Inbred CBA, Mice, Knockout, Potassium Channel Blockers, Pyrazoles, Respiratory Mucosa, Th1 Cells, Th2 Cells, Time Factors, Trachea, KCa3.1, Obliterative airway disease, TRAM-34, Chronic rejection, Heterotopic tracheal transplantation, Medical and Health Sciences, Surgery, Clinical sciences, Immunology
Abstract

BackgroundThe calcium-activated potassium channel KCa3.1 is critically involved in T-cell activation as well as in the proliferation of smooth muscle cells and fibroblasts. We sought to investigate whether KCa3.1 contributes to the pathogenesis of obliterative airway disease (OAD) and whether knockout or pharmacologic blockade would prevent the development of OAD.MethodsTracheas from CBA donors were heterotopically transplanted into the omentum of C57Bl/6J wild-type or KCa3.1 mice. C57Bl/6J recipients were either left untreated or received the KCa3.1 blocker TRAM-34 (120 mg/kg/day). Histopathology and immunologic assays were performed on postoperative day 5 or 28.ResultsSubepithelial T-cell and macrophage infiltration on postoperative day 5, as seen in untreated allografts, was significantly reduced in the KCa3.1 and TRAM-34 groups. Also, systemic Th1 activation was significantly and Th2 mildly reduced by KCa3.1 knockout or blockade. After 28 days, luminal obliteration of tracheal allografts was reduced from 89%±21% in untreated recipients to 53%±26% (P=0.010) and 59%±33% (P=0.032) in KCa3.1 and TRAM-34-treated animals, respectively. The airway epithelium was mostly preserved in syngeneic grafts, mostly destroyed in the KCa3.1 and TRAM-34 groups, and absent in untreated allografts. Allografts triggered an antibody response in untreated recipients, which was significantly reduced in KCa3.1 animals. KCa3.1 was detected in T cells, airway epithelial cells, and myofibroblasts. TRAM-34 dose-dependently suppressed proliferation of wild-type C57B/6J splenocytes but did not show any effect on KCa3.1 splenocytes.ConclusionsOur findings suggest that KCa3.1 channels are involved in the pathogenesis of OAD and that KCa3.1 blockade holds promise to reduce OAD development.

Published
2013

7. Content Analysis on Research Data Policies of Australian University

Author

Xing Wenming and Hua Xiaoqin

Subjects
research data policy, Bibliography. Library science. Information resources
Abstract

[Purpose/significance] In order to understand the situation of research data policies formulated by Australian universities, so as to offer reference to the establishment and implementation of research data policies in Chinese universities. [Method/process] This paper took the collected 27 research data policies as sample, analyzed these policies’ general information (including policy maker, effective date and the revision cycle), the policies’ main content (including policy preamble, policy scope, definitions, roles and responsibilities, data management plan, data ownership, data storage and retention, data sharing and reuse, data transfer, the responsible officer, etc.), and the related policies, and on base of the analysis, it summarized the characteristic of Australian universities’ research data policies. [Result/conclusion] The Australian universities’ research data policies have the following characteristics: policies are normative, content is clear, rights and responsibilities are clear, emphasis on support and service for researchers, and emphasis on correlation and collaboration with other policies.

Published
2018
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8. Heterotopic and orthotopic tracheal transplantation in mice used as models to study the development of obliterative airway disease.

Author

Hua, Xiaoqin, Deuse, Tobias, Tang-Quan, Karis R, Robbins, Robert C, Reichenspurner, Hermann, and Schrepfer, Sonja

Subjects
Trachea, Animals, Mice, Airway Obstruction, Disease Models, Animal, Transplantation, Disease Models, Animal, Biochemistry and Cell Biology, Psychology, Cognitive Sciences
Abstract

Obliterative airway disease (OAD) is the major complication after lung transplantations that limits long term survival (1-7). To study the pathophysiology, treatment and prevention of OAD, different animal models of tracheal transplantation in rodents have been developed (1-7). Here, we use two established models of trachea transplantation, the heterotopic and orthotopic model and demonstrate their advantages and limitations. For the heterotopic model, the donor trachea is wrapped into the greater omentum of the recipient, whereas the donor trachea is anastomosed by end-to-end anastomosis in the orthotopic model. In both models, the development of obliterative lesions histological similar to clinical OAD has been demonstrated (1-7). This video shows how to perform both, the heterotopic as well as the orthotopic tracheal transplantation technique in mice, and compares the time course of OAD development in both models using histology.

Published
2010

13. Visual abstract - Supplemental material for Early Outcomes of Endoscopic Papillary Muscle Relocation for Secondary Mitral Regurgitation Type IIIb in Patients With Severe Left Ventricular Dysfunction

Author

Pausch, Jonas, Bhadra, Oliver D., Sequeira Gross, Tatiana M., Hua, Xiaoqin, Conradi, Lenard, Reichenspurner, Hermann, and Girdauskas, Evaldas

Subjects
FOS: Clinical medicine, 110323 Surgery
Abstract

Supplemental material, sj-pptx-1-inv-10.1177_15569845221115419 for Early Outcomes of Endoscopic Papillary Muscle Relocation for Secondary Mitral Regurgitation Type IIIb in Patients With Severe Left Ventricular Dysfunction by Jonas Pausch, Oliver D. Bhadra, Tatiana M. Sequeira Gross, Xiaoqin Hua, Lenard Conradi, Hermann Reichenspurner and Evaldas Girdauskas in Innovations: Technology and Techniques in Cardiothoracic and Vascular Surgery

Published
2022
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15. Study design and rationale of the pAtients pResenTing with cOngenital heaRt dIseAse Register (ARTORIA‐R)

Author

Sinning, Christoph, Zengin, Elvin, Diller, Gerhard-Paul, Onorati, Francesco, Castel, María-Angeles, Petit, Thibault, Chen, Yih-Sharng, Lo Rito, Mauro, Chiarello, Carmelina, Guillemain, Romain, Coniat, Karine Nubret-Le, Magnussen, Christina, Knappe, Dorit, Becher, Peter Moritz, Schrage, Benedikt, Smits, Jacqueline M., Metzner, Andreas, Knosalla, Christoph, Schoenrath, Felix, Miera, Oliver, Cho, Mi-Young, Bernhardt, Alexander, Weimann, Jessica, Goßling, Alina, Terzi, Amedeo, Amodeo, Antonio, Alfieri, Sara, Angeli, Emanuela, Ragni, Luca, Napoleone, Carlo Pace, Gerosa, Gino, Pradegan, Nicola, Rodrigus, Inez, Dumfarth, Julia, de Pauw, Michel, François, Katrien, Van Caenegem, Olivier, Ancion, Arnaut, Van Cleemput, Johan, Miličić, Davor, Moza, Ajay, Schenker, Peter, Thul, Josef, Steinmetz, Michael, Warnecke, Gregor, Ius, Fabio, Freyt, Susanne, Avsar, Murat, Sandhaus, Tim, Haneya, Assad, Eifert, Sandra, Saeed, Diyar, Borger, Michael, Welp, Henryk, Ablonczy, László, Schmack, Bastian, Ruhparwar, Arjang, Naito, Shiho, Hua, Xiaoqin, Fluschnik, Nina, Nies, Moritz, Keil, Laura, Senftinger, Juliana, Ismaili, Djemail, Kany, Shinwan, Csengeri, Dora, Cardillo, Massimo, Oliveti, Alessandra, Faggian, Giuseppe, Dorent, Richard, Jasseron, Carine, Blanco, Alicia Pérez, Márquez, José Manuel Sobrino, López-Vilella, Raquel, García-Álvarez, Ana, López, María Luz Polo, Rocafort, Alvaro Gonzalez, Fernández, Óscar González, Prieto-Arevalo, Raquel, Zatarain-Nicolás, Eduardo, Blanchart, Katrien, Boignard, Aude, Battistella, Pascal, Guendouz, Soulef, Houyel, Lucile, Para, Marylou, Flecher, Erwan, Gay, Arnaud, Épailly, Éric, Dambrin, Camille, Lam, Kaitlyn, Ka-lai, Cally Ho, Cho, Yang Hyun, Choi, Jin-Oh, Kim, Jae-Joong, Coats, Louise, Crossland, David Steven, Mumford, Lisa, Hakmi, Samer, Sivathasan, Cumaraswamy, Fabritz, Larissa, Schubert, Stephan, Gummert, Jan, Hübler, Michael, Jacksch, Peter, Zuckermann, Andreas, Laufer, Günther, Baumgartner, Helmut, Giamberti, Alessandro, Reichenspurner, Hermann, and Kirchhof, Paulus

Subjects
Heart Defects, Congenital, Adult, Cardiac & Cardiovascular Systems, Heart Defects, Congenital / therapy, Waiting Lists, Study Designs, Medizin, Heart transplantation, Heart Defects, Congenital / complications, MANAGEMENT, Diseases of the circulatory (Cardiovascular) system, Humans, ESC GUIDELINES, Heart Failure / therapy, Adults with congenital heart disease, Arrhythmia, Heart failure, Heart transplantation, Lung transplantation, Ventricular assist device, Retrospective Studies, GENERAL-POPULATION, Heart Failure, OUTCOMES, Study Design, Science & Technology, TRANSPLANTATION, MORTALITY, Heart Failure / epidemiology, Heart Transplantation / adverse effects, ADULTS, ASSOCIATION, EUROPEAN-SOCIETY, Lung transplantation, Heart Failure / etiology, RC666-701, Cardiovascular System & Cardiology, Ventricular assist device, Heart Transplantation, Heart Defects, Congenital / epidemiology, Adults with congenital heart disease, Human medicine, Life Sciences & Biomedicine, Arrhythmia, TASK-FORCE
Abstract

ESC heart failure 8(6), 5542-5550 (2021). doi:10.1002/ehf2.13574, Published by Wiley, Chichester

Published
2021

17. THALIDOMIDE TREATMENT PREVENTS CHRONIC GRAFT REJECTION AFTER AORTIC TRANSPLANTATION IN RATS

Author

Miller, Katharine K., Wang, Dong, Hu, Xiaomeng, Hua, Xiaoqin, Deuse, Tobias, Neofytou, Evgenios, Renne, Thomas, Velden, Joachim, Reichenspurner, Hermann, Schrepfer, Sonja, and Bernstein, Daniel

Subjects
Graft Rejection, Male, Myocytes, Smooth Muscle, Drug Evaluation, Preclinical, Aorta, Thoracic, Coronary Artery Disease, Article, Rats, Inbred F344, Thalidomide, Rats, Inbred Lew, Chronic Disease, Animals, Cytokines, Lymphocytes, Tunica Media, Immunosuppressive Agents
Abstract

Cardiac allograft vasculopathy (CAV) affects approximately 30% of cardiac transplant patients at 5 years post-transplantation. To date, there are few CAV treatment or prevention options, none of which are highly effective. The aim of the study was to investigate the effect of thalidomide on the development of CAV. The effect of thalidomide treatment on chronic rejection was assessed in rat orthotopic aortic transplants in allogeneic F344 or syngeneic Lew rats (n = 6 per group). Animals were left untreated or received thalidomide for 30 days post-transplant, and evidence of graft CAV was determined by histology (trichrome and immunohistochemistry) and intragraft cytokine measurements. Animals that received thalidomide treatment post-transplant showed markedly reduced luminal obliteration, with concomitant rescue of smooth muscle cells (SMCs) in the aortic media of grafts. Thalidomide counteracted neointimal hyperplasia by preventing dedifferentiation of vascular SMCs. Measurement of intragraft cytokine levels after thalidomide treatment revealed downregulation of matrix metalloproteinase 8 and monocyte chemotactic protein 1, cytokines involved in tissue remodelling and inflammation, respectively. Importantly, no negative side effects of thalidomide were observed. Thalidomide treatment prevents CAV development in a rodent model and is therefore potentially useful in clinical applications to prevent post-transplant heart rejection.

Published
2017

20. Orthotopic tracheal transplantation using human bronchus: an original xenotransplant model of obliterative airway disorder

Author

Guihaire, Julien, primary, Itagaki, Ryo, additional, Stubbendorff, Mandy, additional, Hua, Xiaoqin, additional, Deuse, Tobias, additional, Ullrich, Sebastian, additional, Fadel, Elie, additional, Dorfmüller, Peter, additional, Robbins, Robert C., additional, Reichenspurner, Hermann, additional, Schumacher, Udo, additional, and Schrepfer, Sonja, additional

Published
2016
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21. The Selective JAK1/3-Inhibitor R507 Mitigates Obliterative Airway Disease Both With Systemic Administration and Aerosol Inhalation

Author

Deuse, Tobias, primary, Hua, Xiaoqin, additional, Stubbendorff, Mandy, additional, Spin, Joshua M., additional, Neofytou, Evgenios, additional, Taylor, Vanessa, additional, Chen, Yan, additional, Park, Gary, additional, Fink, James B., additional, Renne, Thomas, additional, Kiefmann, Martina, additional, Kiefmann, Rainer, additional, Reichenspurner, Hermann, additional, Robbins, Robert C., additional, and Schrepfer, Sonja, additional

Published
2016
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22. SCNT-derived ESCs with mismatched mitochondria trigger an immune response in allogeneic hosts.

Author

Deuse, Tobias, Wang, Dong, Stubbendorff, Mandy, Itagaki, Ryo, Grabosch, Antje, Greaves, Laura C., Alawi, Malik, Grünewald, Anne, Hu, Xiaomeng, Hua, Xiaoqin, Velden, Joachim, Reichenspurner, Hermann, Robbins, Robert C., Jaenisch, Rudolf, Weissman, Irving L., Schrepfer, Sonja, Deuse, Tobias, Wang, Dong, Stubbendorff, Mandy, Itagaki, Ryo, Grabosch, Antje, Greaves, Laura C., Alawi, Malik, Grünewald, Anne, Hu, Xiaomeng, Hua, Xiaoqin, Velden, Joachim, Reichenspurner, Hermann, Robbins, Robert C., Jaenisch, Rudolf, Weissman, Irving L., and Schrepfer, Sonja

Abstract

The generation of pluripotent stem cells by somatic cell nuclear transfer (SCNT) has recently been achieved in human cells and sparked new interest in this technology. The authors reporting this methodical breakthrough speculated that SCNT would allow the creation of patient-matched embryonic stem cells, even in patients with hereditary mitochondrial diseases. However, herein we show that mismatched mitochondria in nuclear-transfer-derived embryonic stem cells (NT-ESCs) possess alloantigenicity and are subject to immune rejection. In a murine transplantation setup, we demonstrate that allogeneic mitochondria in NT-ESCs, which are nucleus-identical to the recipient, may trigger an adaptive alloimmune response that impairs the survival of NT-ESC grafts. The immune response is adaptive, directed against mitochondrial content, and amenable for tolerance induction. Mitochondrial alloantigenicity should therefore be considered when developing therapeutic SCNT-based strategies.

Published
2015
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27. SCNT-Derived ESCs with Mismatched Mitochondria Trigger an Immune Response in Allogeneic Hosts

Author

Deuse, Tobias, primary, Wang, Dong, additional, Stubbendorff, Mandy, additional, Itagaki, Ryo, additional, Grabosch, Antje, additional, Greaves, Laura C., additional, Alawi, Malik, additional, Grünewald, Anne, additional, Hu, Xiaomeng, additional, Hua, Xiaoqin, additional, Velden, Joachim, additional, Reichenspurner, Hermann, additional, Robbins, Robert C., additional, Jaenisch, Rudolf, additional, Weissman, Irving L., additional, and Schrepfer, Sonja, additional

Published
2015
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29. Immunological Properties of Extraembryonic Human Mesenchymal Stromal Cells Derived from Gestational Tissue

Author

Stubbendorff, Mandy, primary, Deuse, Tobias, additional, Hua, Xiaoqin, additional, Phan, Thang T., additional, Bieback, Karen, additional, Atkinson, Kerry, additional, Eiermann, Thomas H., additional, Velden, Joachim, additional, Schröder, Christine, additional, Reichenspurner, Hermann, additional, Robbins, Robert C., additional, Volk, Hans-Dieter, additional, and Schrepfer, Sonja, additional

Published
2013
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31. Human Internal Mammary Artery (IMA) Transplantation and Stenting: A Human Model to Study the Development of In-Stent Restenosis

Author

Hua, Xiaoqin, primary, Deuse, Tobias, primary, Michelakis, Evangelos D., primary, Haromy, Alois, primary, Tsao, Phil S., primary, Maegdefessel, Lars, primary, Erben, Reinhold G., primary, Bergow, Claudia, primary, Behnisch, Boris B., primary, Reichenspurner, Hermann, primary, Robbins, Robert C., primary, and Schrepfer, Sonja, primary

Published
2012
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33. Human Leukocyte Antigen I Knockdown Human Embryonic Stem Cells Induce Host Ignorance and Achieve Prolonged Xenogeneic Survival

Author

Deuse, Tobias, primary, Seifert, Martina, additional, Phillips, Neil, additional, Fire, Andrew, additional, Tyan, Dolly, additional, Kay, Mark, additional, Tsao, Philip S., additional, Hua, Xiaoqin, additional, Velden, Joachim, additional, Eiermann, Thomas, additional, Volk, Hans-Dieter, additional, Reichenspurner, Hermann, additional, Robbins, Robert C., additional, and Schrepfer, Sonja, additional

Published
2011
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38. Early Outcomes of Endoscopic Papillary Muscle Relocation for Secondary Mitral Regurgitation Type IIIb in Patients With Severe Left Ventricular Dysfunction.

Author

Pausch J, Bhadra OD, Sequeira Gross TM, Hua X, Conradi L, Reichenspurner H, and Girdauskas E

Subjects
Endoscopy, Humans, Papillary Muscles surgery, Retrospective Studies, Treatment Outcome, Mitral Valve Annuloplasty methods, Mitral Valve Insufficiency, Ventricular Dysfunction, Left complications, Ventricular Dysfunction, Left surgery
Abstract

Objective: Subannular mitral valve (MV) repair techniques have been developed to address increased rates of recurrent mitral regurgitation (MR) in patients with secondary MR (SMR) type IIIb. Endoscopic papillary muscle relocation (PMR) is feasible via minithoracotomy. Nevertheless, the periprocedural outcome of patients with severe left ventricular (LV) dysfunction remains unknown. Methods: A total of 98 consecutive patients with SMR type IIIb underwent PMR at our institution. Due to concomitant coronary artery bypass grafting, 62 patients underwent sternotomy and were excluded from the current analysis, whereas 36 patients were treated by a minimally invasive technique using 3-dimensional endoscopy. Of these, 18 patients had severely depressed LV ejection fraction (LVEF) ≤35% (study group) and were compared to the remaining 18 patients with LVEF >35% (control group). Periprocedural outcome was retrospectively analyzed. Results: Although LVEF was significantly worse in the study group (30% ± 4% vs 43% ± 6%, P  < 0.001), the severity of SMR and the degree of MV leaflet tethering were similar. The prevalence of concomitant procedures and the duration of surgery, cardiopulmonary bypass, and aortic cross-clamp were comparable. Periprocedural low cardiac output syndrome was favorably low in both groups (16.7% vs 5.6%, P  = 0.29). Postoperative ventilation time (5.7 h [4.2 to 8.7 h] vs 6.0 h [4.6 to 9.8 h], P  = 0.43) and duration of intensive care unit stay (2 days [1 to 3 days] vs 2 days [1 to 3 days], P  = 0.22) were similar. There was no 30-day mortality in either group. Conclusions: Standardized endoscopic PMR resulted in favorable periprocedural outcomes in patients with severe LV dysfunction, suggesting that minimally invasive surgery can safely be extended to this patient population.

Published
2022
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39. Study design and rationale of the pAtients pResenTing with cOngenital heaRt dIseAse Register (ARTORIA-R).

Author

Sinning C, Zengin E, Diller GP, Onorati F, Castel MA, Petit T, Chen YS, Lo Rito M, Chiarello C, Guillemain R, Coniat KN, Magnussen C, Knappe D, Becher PM, Schrage B, Smits JM, Metzner A, Knosalla C, Schoenrath F, Miera O, Cho MY, Bernhardt A, Weimann J, Goßling A, Terzi A, Amodeo A, Alfieri S, Angeli E, Ragni L, Napoleone CP, Gerosa G, Pradegan N, Rodrigus I, Dumfarth J, de Pauw M, François K, Van Caenegem O, Ancion A, Van Cleemput J, Miličić D, Moza A, Schenker P, Thul J, Steinmetz M, Warnecke G, Ius F, Freyt S, Avsar M, Sandhaus T, Haneya A, Eifert S, Saeed D, Borger M, Welp H, Ablonczy L, Schmack B, Ruhparwar A, Naito S, Hua X, Fluschnik N, Nies M, Keil L, Senftinger J, Ismaili D, Kany S, Csengeri D, Cardillo M, Oliveti A, Faggian G, Dorent R, Jasseron C, Blanco AP, Márquez JMS, López-Vilella R, García-Álvarez A, López MLP, Rocafort AG, Fernández ÓG, Prieto-Arevalo R, Zatarain-Nicolás E, Blanchart K, Boignard A, Battistella P, Guendouz S, Houyel L, Para M, Flecher E, Gay A, Épailly É, Dambrin C, Lam K, Ka-Lai CH, Cho YH, Choi JO, Kim JJ, Coats L, Crossland DS, Mumford L, Hakmi S, Sivathasan C, Fabritz L, Schubert S, Gummert J, Hübler M, Jacksch P, Zuckermann A, Laufer G, Baumgartner H, Giamberti A, Reichenspurner H, and Kirchhof P

Subjects
Adult, Humans, Retrospective Studies, Waiting Lists, Heart Defects, Congenital complications, Heart Defects, Congenital epidemiology, Heart Defects, Congenital therapy, Heart Failure epidemiology, Heart Failure etiology, Heart Failure therapy, Heart Transplantation adverse effects
Abstract

Aim: Due to improved therapy in childhood, many patients with congenital heart disease reach adulthood and are termed adults with congenital heart disease (ACHD). ACHD often develop heart failure (HF) as a consequence of initial palliative surgery or complex anatomy and subsequently require advanced HF therapy. ACHD are usually excluded from trials evaluating heart failure therapies, and in this context, more data about heart failure trajectories in ACHD are needed to guide the management of ACHD suffering from HF., Methods and Results: The pAtients pResenTing with cOngenital heaRt dIseAse Register (ARTORIA-R) will collect data from ACHD evaluated or listed for heart or heart-combined organ transplantation from 16 countries in Europe and the Asia/Pacific region. We plan retrospective collection of data from 1989-2020 and will include patients prospectively. Additional organizations and hospitals in charge of transplantation of ACHD will be asked in the future to contribute data to the register. The primary outcome is the combined endpoint of delisting due to clinical worsening or death on the waiting list. The secondary outcome is delisting due to clinical improvement while on the waiting list. All-cause mortality following transplantation will also be assessed. The data will be entered into an electronic database with access to the investigators participating in the register. All variables of the register reflect key components important for listing of the patients or assessing current HF treatment., Conclusion: The ARTORIA-R will provide robust information on current management and outcomes of adults with congenital heart disease suffering from advanced heart failure., (© 2021 The Authors. ESC Heart Failure published by John Wiley & Sons Ltd on behalf of European Society of Cardiology.)

Published
2021
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