Monozytäre Expression von CD 14 ("Endotoxin-Rezeptor") und proinflammatorische Subpopulationen antigenpräsentierender Leukozyten

Fragestellung: Um mögliche proinflammatorische Zeichen bzw. Frühindikatoren (sog. Mikroinflammation) bei Patienten mit chronischem Nierenversagen und nierentransplantierten Patienten aufzuspüren, die an späteren Organkomplikationen (chronische Transplantatdysfunktion, Herz-Kreislaufmorbidität, endotheliale Dysfunktion, Infektanfälligkeiten) beteiligt sein können, untersuchten wir die Expression funktioneller monozytärer Oberflächenantigene. Als immunologischen Marker der Aktivität einer Entzündungsreaktion verglichen wir die in der Durchflusszytometrie (fluorescence-activated cell sorter (FACS))gemessene Expression sog. mCD14-Rezeptoren und der CD14+CD16++-Rezeptoren auf peripheren Blut-Monozyten mit serologischen Parametern wie C-reaktives Protein und Leukozytenzahl. Die Frage, ob die beiden Oberflächenantigene CD14 und CD16 sowie die Koexpression beider Antigene (proinflammatorisch aktivierte Monozyten) zum „immunologischen Monitoring“ geeignet sind, sollte erstmalig klinisch an Gesunden, Patienten nach Nierentransplantation sowie Patienten mit chronischer Niereninsuffizienz im Endstadium ohne Dialysebehandlung untersucht werden. Ergänzend wurden nichtorgantransplantierte Patienten mit akuten infektiösen Komplikationen auf mögliche Modulationen proinflammatorischer Blutmonozyten (CD14+/CD16++-Zellen) hin untersucht. CD14 existiert membrangebunden (mCD14) und in löslicher Form (sCD14) und ist verantwortlich für die Interaktion von Endotoxin (LPS) mit Monozyten und Neutrophilen. LPS ist ein Glykoprotein der äußeren Membranschicht gramnegativer Bakterien. CD14 ist der wichtigste Rezeptor für gram-negative bakterielle Lipopolysaccharide (Endotoxin), jedoch auch für Peptidoglykan und Lipoteichonsäure gram-positiver Erreger. CD 16 ist der funktionell wichtige Fcγ–Rezeptor Typ III (FcγRIII, IgG-Rezeptor Typ III), der mit niedriger Affinität monomeres IgG sowie polymeres IgG oder Immunkomplexe bindet. Er vermittelt wichtige immunphysiologische Funktionen wie antikörperabhängige zellvermittelte Zytotoxizität, Beseitigung zirkulierender Immunkomplexe, Superoxidbildung und ist auch an der Signaltransduktion beteiligt. Die untersuchten CD14+CD16++-Monozyten bewirken im Zusammenwirken von TNFα, IL-1, IL-6 und IL-10 bewirkt eine stärkere Entzündungsreaktion als die konventionellen CD14++CD16negativen-Zellen; sie sind sehr potente Antigen-präsentierende Zellen, besitzen eine hohe Phagozytoseaktivität und verstärken die endotheliale Adhäsion. Untersuchungsaufbau: Wir untersuchten 69 Patienten nach Nierentransplantation (23 Frauen, 46 Männer) im Alter von durchschnittlich 52,63 +/- 11,42 Jahren (Median 53,84 Jahre). Die Patienten erhielten durchschnittlich vor 6,38 +/- 5,2 Jahren ein Nieren- Transplantat (Median 8,16 Jahre). Wir unterschieden diese Patienten hinsichtlich ihrer Immunsuppression in folgende Gruppen: 1) Mycophenolat-Mofetil-Monotherapie (MMFmono), 2) Cyclosporin-Monotherapie (CyAmono) und 3) einer Kombination aus MMF und CyA (MMF-CyAkombi). In die Gruppe mit MMF-Monotherapie wurden16 Personen eingeschlossen (3 Frauen, 13 Männer) im Alter von durchschnittlich 51,29 +/- 10,47 Jahren (Median 51,15 Jahre). In der Gruppe der CyA-monotherapierten Patienten befanden sich 11 Personen (3 Frauen, 8 Männer) im Durchschnittsalter von 58,43 +/- 8,01 Jahren (Median 59,96 Jahre). Zur Gruppe der MMF-CyA-kombinationstherapierten Patienten gehörten 18 Patienten (3 Frauen, 15 Männer) im Alter von 46,69 +/- 10,22 Jahren (Median 47,44 Jahre). Des weiteren wurden 13 Patienten mit chronischer Niereninsuffizienz (12 Männer, eine Frau) im Alter von 32 bis 74 Jahren (Median 65,0 Jahre; Mittelwert 63,5 Jahre +/- 10,3 Jahre) in die Analysen miteinbezogen. Parallel wurden 8 Patienten (6 Frauen, 2 Männer) im Verlauf einer akuten Infektion erfasst (Mittelwert 74,6 +/- 10,53 Jahre; Median 78 Jahre). Unser Kontrollkollektiv bestand aus 18 klinisch gesunden freiwilligen Probanden im Alter zwischen 24 und 54 Jahren (Median 31Jahre; Mittelwert 33,42 +/- 9,91 Jahre; 10 Frauen, 8 Männer). Ergebnisse: 1. Patienten mit chronischer Niereninsuffizienz hatten signifikant höhere CRP-Serumkonzentrationen als Gesunde (p=0,010)(Gesunde 0,33 mg/dl vs. Urämiker 0,7 mg/dl). 2. Die mCD14-Expression auf peripheren Blutmonozyten war bei Urämikern (p=0,024) und bei nierentransplantierten Patienten (p=0,026) signifikant niedriger als bei Gesunden.(Gesunde 517 MFI vs. Urämiker 426 MFI vs. NTX 433 MFI) 3. Der prozentuale Anteil CD14+CD16++-Monozyten im Blut war sowohl bei Patienten mit chronischer Niereninsuffizienz (p=0,00000487; MFI= 13,0%) als auch bei Patienten nach Nierentransplantation (p=0,00298; MFI=9,3%) signifikant höher. 4. Die Leukozytenzahl im Blut war weder bei immunsupprimierten Nierentransplantierten noch bei Patienten mit chronischer Niereninsuffizienz im Endstadium signifikant gegenüber Gesunden verändert. 5. Hinsichtlich der verschiedenen Strategien der immunsuppressiven Therapie ließen sich keine Unterschiede zwischen den Gruppen der MMF-mono, der CyA-mono und der MMF-CyA-kombi-behandelten Nt-Patienten feststellen. 6. Die Absolutzahl CD14+CD16++-Monozyten war sowohl bei urämischen Patienten (p=0,003; 430/µl) als auch bei nierentransplantierten Patienten (p=0,005; 413/µl) gegenüber Gesunden signifikant erhöht. 7. Bei Nierentransplantierten fiel die CRP-Konzentration im Serum mit steigendem Alter des Transplantates logarithmisch ab (p=0,065), die mCD14-Expression fiel linear ab (p=0,063) wohingegen der prozentuale Anteil der CD14+CD16++- Monozyten invers ansteigt (p=0,0036). 8. Im Verlauf akuter infektiöser Erkrankungen war der Anteil der CD14+CD16++- Monozyten signifikant höher als bei Gesunden (p=0,000049) und fiel bis zur stationären Entlassung so signifikant ab (p=0,012), so dass kein Unterschied mehr zwischen Gesunden und Kranken mehr nachweisbar war. Schlußfolgerungen: 1. Sowohl bei Patienten mit chronischer Niereninsuffizienz wie bei Nierentransplantierten finden sich anhand erhöhter Zahlen proinflammatorischer Blutmonozyten (CD14+CD16++-Phänotyp) eindeutig Zeichen einer sog. „Mikroinflammation“; dies ausdrücklich auch bei NTX-Patienten, obwohl diese unter einer dauerhaften immunsuppressiven Behandlung stehen. 2. Proinflammatorische Blutmonozyten sind Ziel- und Effektorzellen der Immunabwehr. Darüber hinaus sind sie pathophysiologisch an den Vorgängen einer Atheromatose beteiligt. CD14+CD16++-Blutmonozyten entsprechen dem Phänotyp von Gewebsmakrophagen. Erhöhte Anteile CD14+CD16++-Blutmonozyten gehen möglicherweise parallel mit der erhöhten Progressionsrate der Atheromatose von Organtransplantierten und Patienten mit Niereninsuffizienz. Andererseits sind sie an der Auslösung und Perpetuation der chronischen Transplantatdysfunktion (chronisches Transplantatversagen) ursächlich beteiligt, was aus Biopsiedaten hervorgeht. Die hier erfolgten Blutzellanalysen unterstützen diese These. 3. Dauerimmunsuppression bei Nierentransplantierten vermag nicht den proinflammatorischen Status diese Patienten zu unterdrücken. Damit gilt für alle NTXPatienten, dass sich mehr oder weniger schnell trotz potenter Immunsuppression irgendwann ein Transplantatversagen einstellt. Es spricht alles dafür, dass aktivierte Blutmonozyten hier die Schlüsselrolle spielen. Wir postulieren, dass dies nur dann abgeschwächt oder vermindert werden könnte, wenn sich die zellulären Marker, die auf chronische inflammatorische Aktivität hinweisen, pharmakologisch günstig beeinflussen ließen

Permanent pacemaker dependency in patients with new left bundle branch block and new first degree atrioventricular block after transcatheter aortic valve implantation

Conduction disorders with need for permanent pacemaker (PPM) implantation remain frequent complications after transcatheter aortic valve implantation (TAVI). Up to 22% of PPM after TAVI are implanted for new onset left bundle branch block (LBBB) and atrioventricular block (AVB) I. However, clinical benefit and predictors of ventricular pacing in TAVI patients receiving PPM for this indication remain unclear. We retrospectively evaluated pacemaker interrogation data of patients who received a PPM post TAVI for new LBBB and new AVB I. The primary endpoint of this study was relevant ventricular pacing (ventricular pacing rate: Vp ≥ 1%) at the first outpatient pacemaker interrogation. Secondary endpoints were predictors for relevant ventricular pacing. At the first pacemaker interrogation (median follow up at 6.23 2.8-14.8 months), median ventricular pacing frequency was 1.0{\%} 0.1-17.8. Out of 61 patients, 36 (59{\%}) had Vp rates ≥ 1{\%}. Patients with frequent ventricular pacing showed longer QRS duration (155~ms ± 17~ms vs. 144~ms ± 18~ms, p = 0.018) at the time of PPM implantation and were less likely treated with a balloon-expandable Edwards Sapiens Valve (39{\%} vs. 12{\%}, p = 0.040). Our findings suggest that the majority of patients with new LBBB and new AVB I after TAVI show relevant ventricular pacing rates at follow up. Further prospective studies are necessary to identify patients at higher risk of pacemaker dependency

Recent advances in the genetics of atrial fibrillation: from rare and common genetic variants to microRNA signaling

Besides traditional risk factors, atrial fibrillation (AF) also shares a strong genetic component. Here, we review the genetics of AF including monogenic forms of AF, heritability of AF, complex genetic risk of AF, and the role of microRNAs in AF pathophysiology. Thirtytwo mutations (17 genes) have been reported to cause familial AF. Mutations in cardiac ion channel genes or their subunits alter electrical properties and thereby lead to AF. Recently, also non-ion channel gene mutations have been identified to cause familial AF. Twin and community-based studies suggested AF to be heritable also on the population level. The AF risk in the offspring of an affected first-degree relative ranged between 2- to 5-fold, depending on the age of onset. Thereby, the risk of AF increases gradually the earlier the youngest relative of an AF patient developed the arrhythmia. African Americans bear a lesser risk of AF compared to individuals of European ancestry. Their risk rises with increasing European admixture. Genome wide association studies have revealed loci on chromosomes 4q25, 16q21 and 1q21 conferring risk of AF. Very recently, another consortial effort has identified a novel locus on chromosome 1, intronic to IL6R. IL6R encodes the a subunit of the interleukin 6 receptor. MicroRNAs were shown to regulate gene expression, and are increasingly reported to modify AF. A hallmark of AF pathophysiology is electrical and structural remodeling. MicroRNAs are involved in this process by regulating gene expression of cardiac ion channels, calcium handling proteins, transcription factors, and extracellular matrix related proteins

Massive Accumulation of Myofibroblasts in the Critical Isthmus Is Associated With Ventricular Tachycardia Inducibility in Post-Infarct Swine Heart

Objectives In this study the authors determined the extent of cellular infiltration and dispersion, and regional vascularization in electrophysiologically (EP) defined zones in post–myocardial infarction (MI) swine ventricle. Background The critical isthmus (CI) in post-MI re-entrant ventricular tachycardia (VT) is a target for catheter ablation. In vitro evidence suggests that myofibroblasts (MFB) within the scar border zone (BZ) may increase the susceptibility to slow conduction and VT, but whether this occurs in vivo remains unproven. Methods Six weeks after mid–left anterior descending coronary artery occlusion, EP catheter-based mapping was used to assess susceptibility to VT induction. EP data were correlated with detailed cellular profiling of ventricular zones using immunohistochemistry and spatial distribution analysis of cardiomyocytes, fibroblasts, MFB, and vascularization. Results In pigs with induced sustained monomorphic VT (mean cycle length: 353 ± 89 ms; n = 6) the area of scar that consisted of the BZ (i.e., between the normal and the low-voltage area identified by substrate mapping) was greater in VT-inducible hearts (iVT) than in noninducible hearts (non-VT) (p 100 times that in normal myocardium and >5 times higher than that in the BZ in non-VT hearts) and by a 1.7-fold increase in blood vessel density within the dense scar region extending towards the CI. Sites of local abnormal ventricular activity potentials exhibited cellularity and vascularization that were intermediate to the CI in iVT and BZ in non-VT hearts. Conclusions The authors reported the first cellular analysis of the VT CI following an EP-based zonal analysis of iVT and non-VT hearts in pigs post-MI. The data suggested that VT susceptibility was defined by a remarkable number of MFB in the VT CI, which appeared to bridge the few remaining dispersed clusters of cardiomyocytes. These findings define the cellular substrate for the proarrhythmic slow conduction pathway

Alteration of Endothelin 1, MCP-1 and Chromogranin A in patients with atrial fibrillation undergoing pulmonary vein isolation

Background: The relation between arrhythmias and stress is known. The aim of our current study was to elucidate whether plasma levels of previously described stress parameters are altered in highly symptomatic patients with atrial fibrillation (AF) per se and in patients undergoing ablation therapy by pulmonary vein isolation (PVI). Methods: 96 patients with AF undergoing PVI were recruited. Plasma levels of Endothelin-1 (ET-1), MCP-1 and Chromogranin-A (CGA) were measured before and three months after ablation completed with clinical follow-up with respect to AF recurrence. Additionally, we examined 40 healthy age-and sex-matched volunteers as a reference. Results: Symptomatic AF patients showed increased levels of ET-1 compared to healthy controls (2.62pg/ml vs. 1.57pg/ml;p<0.01). Baseline levels of ET-1 were higher in patients presenting with AF after PVI (2.96pg/ml vs. 2.57pg/ml;p = 0.02). The temporal comparison revealed decreased ET-1 levels in patients without (2.57pg/ml vs. 2.33pg/ml;p< 0.01) and unchanged ET-1 levels in patients with AF after PVI. Baseline MCP-1 was increased in AF patients vs. controls (268pg/ml vs. 227 pg/ml;p = 0.03). Both groups, with and without AF after PVI, showed an increase of MCP-1 compared to baseline (268pg/ml vs. 349pg/ml;p< 0.01;281pg/ml vs. 355pg/ml;p = 0.03). CGA was lower in AF patients compared to healthy controls (13.8ng/ml vs. 25.6ng/ml;p< 0.01). Over time patients without AF after PVI showed an increase of CGA (14.2ng/ml vs. 20.7ng/ml;p< 0.01). No change was observed in patients with AF after PVI. Conclusion: Our study demonstrated dysregulated levels of ET-1, MCP-1 and CGA in symptomatic AF patients. We could demonstrate an association between ET-1 to presence or absence of AF. Furthermore, we could show that a decrease of ET-1 as well as an increase of CGA after PVI, representing a trend towards control cohort levels, were both associated with restoration of sinus rhythm. These results provide new insights into the role of stress-related biomarkers in AF and AF treatment by ablation therapy

Evaluation of state-of-the-art segmentation algorithms for left ventricle infarct from late Gadolinium enhancement MR images

Studies have demonstrated the feasibility of late Gadolinium enhancement (LGE) cardiovascular magnetic resonance (CMR) imaging for guiding the management of patients with sequelae to myocardial infarction, such as ventricular tachycardia and heart failure. Clinical implementation of these developments necessitates a reproducible and reliable segmentation of the infarcted regions. It is challenging to compare new algorithms for infarct segmentation in the left ventricle (LV) with existing algorithms. Benchmarking datasets with evaluation strategies are much needed to facilitate comparison. This manuscript presents a benchmarking evaluation framework for future algorithms that segment infarct from LGE CMR of the LV. The image database consists of 30 LGE CMR images of both humans and pigs that were acquired from two separate imaging centres. A consensus ground truth was obtained for all data using maximum likelihood estimation. Six widely-used fixed-thresholding methods and five recently developed algorithms are tested on the benchmarking framework. Results demonstrate that the algorithms have better overlap with the consensus ground truth than most of the n-SD fixed-thresholding methods, with the exception of the FullWidth-at-Half-Maximum (FWHM) fixed-thresholding method. Some of the pitfalls of fixed thresholding methods are demonstrated in this work. The benchmarking evaluation framework, which is a contribution of this work, can be used to test and benchmark future algorithms that detect and quantify infarct in LGE CMR images of the LV. The datasets, ground truth and evaluation code have been made publicly available through the website: https://www.cardiacatlas.org/web/guest/challenges

EHRA expert consensus document on the management of arrhythmias in frailty syndrome, endorsed by the Heart Rhythm Society (HRS), Asia Pacific Heart Rhythm Society (APHRS), Latin America Heart Rhythm Society (LAHRS), and Cardiac Arrhythmia Society of Southern Africa (CASSA)

There is an increasing proportion of the general population surviving to old age with significant chronic disease, multimorbidity, and disability. The prevalence of pre-frail state and frailty syndrome increases exponentially with advancing age and is associated with greater morbidity, disability, hospitalization, institutionalization, mortality, and health care resource use. Frailty represents a global problem, making early identification, evaluation, and treatment to prevent the cascade of events leading from functional decline to disability and death, one of the challenges of geriatric and general medicine. Cardiac arrhythmias are common in advancing age, chronic illness, and frailty and include a broad spectrum of rhythm and conduction abnormalities. However, no systematic studies or recommendations on the management of arrhythmias are available specifically for the elderly and frail population, and the uptake of many effective antiarrhythmic therapies in these patients remains the slowest. This European Heart Rhythm Association (EHRA) consensus document focuses on the biology of frailty, common comorbidities, and methods of assessing frailty, in respect to a specific issue of arrhythmias and conduction disease, provide evidence base advice on the management of arrhythmias in patients with frailty syndrome, and identifies knowledge gaps and directions for future research

Outcomes of long-standing persistent atrial fibrillation ablation: A systematic review

BackgroundAblation of long-standing persistent atrial fibrillation (AF) is highly variable, with differing techniques and outcomes.ObjectiveThe purpose of this study was to undertake a systematic review of the literature with regard to the impact of ablation technique on the outcomes of long-standing persistent AF ablation.MethodsA systematic search of the contemporary English scientific literature (from January 1, 1990 to June 1, 2009) in the PubMed database identified 32 studies on persistent/long-standing persistent or long-standing persistent AF ablation (including four randomized controlled trials). Data on single-procedure, drug-free success, multiple procedure success, and pharmaceutically assisted success at longest follow-up were collated.ResultsFour studies performed pulmonary vein isolation alone (21%-22% success). Four studies performed pulmonary vein antrum ablation with isolation (PVAI; n = 2; 38%-40% success) or without confirmed isolation (PVA; n = 2; 37%-56% success). Ten studies performed linear ablation in addition to PVA (n = 5; 11%-74% success) or PVAI (n = 5; 38%-57% success). Three studies performed posterior wall box isolation (n = 3; 44%-50% success). Five studies performed complex fractionated atrial electrogram ablation (n = 5; 24%-63% success). Six studies performed complex fractionated atrial electrogram ablation as an adjunct to PVA (n = 2; 50%-51% success), PVAI (n = 3; 36%-61% success), or PVAI and linear (n = 1; 68% success) ablation. Five studies performed the stepwise ablation approach (38%-62% success).ConclusionThe variation in success within and between techniques suggests that the optimal ablation technique for long-standing persistent AF is unclear. Nevertheless, long-standing persistent AF can be effectively treated with a composite of extensive index catheter ablation, repeat procedures, and/or pharmaceuticals.Anthony G. Brooks, Martin K. Stiles, Julien Laborderie, Dennis H. Lau, Pawel Kuklik, Nicholas J. Shipp, Li-Fern Hsu, and Prashanthan Sandershttp://www.elsevier.com/wps/find/journaldescription.cws_home/702333/description#descriptio

EHRA expert consensus document on the management of arrhythmias in frailty syndrome, endorsed by the Heart Rhythm Society (HRS), Asia Pacific Heart Rhythm Society (APHRS), Latin America Heart Rhythm Society (LAHRS), and Cardiac Arrhythmia Society of Southern Africa (CASSA).

There is an increasing proportion of the general population surviving to old age with significant chronic disease, multi-morbidity, and disability. The prevalence of pre-frail state and frailty syndrome increases exponentially with advancing age and is associated with greater morbidity, disability, hospitalization, institutionalization, mortality, and health care resource use. Frailty represents a global problem, making early identification, evaluation, and treatment to prevent the cascade of events leading from functional decline to disability and death, one of the challenges of geriatric and general medicine. Cardiac arrhythmias are common in advancing age, chronic illness, and frailty and include a broad spectrum of rhythm and conduction abnormalities. However, no systematic studies or recommendations on the management of arrhythmias are available specifically for the elderly and frail population, and the uptake of many effective antiarrhythmic therapies in these patients remains the slowest. This European Heart Rhythm Association (EHRA) consensus document focuses on the biology of frailty, common comorbidities, and methods of assessing frailty, in respect to a specific issue of arrhythmias and conduction disease, provide evidence base advice on the management of arrhythmias in patients with frailty syndrome, and identifies knowledge gaps and directions for future research