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​Ishemija in fibroza desnega prekata pri odraslih s prirojenimi srčnimi napakami in tlačno obremenitvijo desnega prekata
ID Pavšič, Nejc (Author), ID Prokšelj, Katja (Mentor) More about this mentor... This link opens in a new window

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Abstract
Ozadje. Bolniki s prirojeno srčno napako in kronično tlačno obremenitvijo desnega prekata (DP) so nagnjeni k pogosti odpovedi DP in pojavu srčnega popuščanja. Natančen mehanizem odpovedi DP pri teh bolnikih ni znan, a je proces najverjetneje odvisen od številnih različnih dejavnikov. Pomembno vlogo naj bi imeli tudi ishemija in fibroza DP, a so trenutni podatki o tem v tej skupini bolnikov skopi. Cilj naše raziskave je bil oceniti ishemijo in fibrozo DP pri bolnikih s prirojenimi srčnimi napakami in kronično tlačno obremenitvijo DP ter njuno povezavo s kliničnimi, laboratorijskimi, funkcionalnimi in slikovnimi označevalci delovanja DP. Hipoteze. 1. Ishemija in fibroza desnega prekata sta prisotni in povezani najdbi pri odraslih bolnikih s prirojenimi srčnimi napakami in kronično tlačno obremenitvijo desnega prekata. 2. Ishemija in fibroza desnega prekata sta povezani s sistolično in diastolično disfunkcijo desnega prekata pri odraslih bolnikih s prirojenimi srčnimi napakami in kronično tlačno obremenitvijo desnega prekata. 3. Biooznačevalci srčne fibroze, elektrokardiografskimi in ehokardiografskimi parametri so povezani z ishemijo in fibrozo desnega prekata pri odraslih bolnikih s prirojenimi srčnimi napakami in kronično tlačno obremenitvijo desnega prekata. Zasnova in metode raziskave. V presečno, kohortno raziskavo smo vključili odrasle bolnike s sistemskim desnim prekatom (bolniki s transpozicijo velikih arterij po operaciji na ravni preddvorov (TGA-AS) in bolniki s kongenitalno korigirano transpozicijo velikih arterij (CCTGA)) ter bolnike s pljučno arterijsko hipertenzijo in Eisenmengerjevim sindromom. Izključili smo bolnike z akutnim ali napredovalim srčnim popuščanjem, neobvladanimi aritmijami, genetskimi sindromi in tiste, ki niso bili zmožni obremenitvenega testiranja. Vsak vključen bolnik je opravil klinični pregled, odvzem krvi za določitev več biooznačevalcev (N-terminalni fragment pro B-tipa natriuretičnega peptida (NT-proBNP), visoko občutljivi troponin I, biooznačevalci metabolizma kolagena), kardiopulmonalno obremenitveno testiranje, ehokardiografijo za oceno sistolične in diastolične funkcije DP, obremenitveno perfuzijsko scintigrafijo miokarda (SPECT) za opredelitev ishemije DP in magnetno resonančno slikanje srca s kontrastom (MR) za opredelitev fokalne (pozno obarvanje z gadolinijem (LGE) in difuzne fibroze (ocena zunajcelične prostornine (ECV)) DP. S statistično analizo smo iskali razlike v kliničnih, laboratorijskih, funkcionalnih in slikovnih označevalcih med bolniki z in brez ishemije ali fibroze DP. Rezultati. V končno analizo je bilo vključenih 32 bolnikov (povprečna starost 40±10 let, 12 (33 %) žensk) s kronično tlačno obremenitvijo DP, med katerimi je bilo 15 bolnikov s TGA-AS, 8 CCTGA in 9 bolnikov z ES. SPECT je pokazal reverzibilno ishemijo DP pri 12 bolnikih (37 %). Med posameznimi podskupinami bolnikov ni bilo razlik v prisotnosti ishemije DP ((TGA-AS: 5 (33%), CCTGA: 2 (22%), ES: 5 (55%); p=0,41). Obseg ishemije DP je bil blag z mediano prizadetostjo 1.5 ([1-2]) segmentov DP. Izpadi kopičenja pa so bili najpogostejši v segmentih sprednje in proste stene DP. MR s kontrastom je bil mogoč pri 25 (78 %) bolnikih in pri 12 (48 %) bolnikih smo potrdili žariščno fibrozo DP z metodo LGE. Glede na prisotnost žariščne fibroze DP ni bilo razlik med podskupinami (TGA-AS: 5 (42%), CCTGA: 2 (33%), ES: 5 (71%); p=0,35). Glede na MR oceno ECV DP je prekomerna difuzna fibroza DP prisotna pri 28% bolnikov, pomembnih razlik v ECV med posameznimi podskupinami ni bilo (p=0,152). Bolniki z dokazno ishemijo DP so imeli pogosteje dokazano tudi žariščno fibrozo DP na MR, medtem ko razlik v difuzni fibrozi DP ni bilo. Žariščna fibroza DP je bila prisotna pri 5 (31 %) bolnikih brez ishemije in pri 7 (78 %) z ishemijo DP (p=0,041). Analiza podskupin je pokazala, da je povezava med ishemijo in žariščno fibrozo DP statistično značilna izključno za bolnike s sistemskim DP ((2 (15%) proti 5 (100%), p=0,002), pri bolnikih z ES pa ne (3 (100%) proti 2 (50%), p=0,43). Primerjava kliničnih značilnosti vseh vključenih bolnikov je pokazala, da so bolniki z dokazano ishemijo DP pomembno starejši kot tisti z normalno prekrvitvijo DP (42,6±11,0 proti 38,4±10,6 let; p=0,049). Analiza laboratorijskih, slikovnih in funkcijskih parametrov med podskupinami bolnikov je pokazala, da imajo bolniki z ES in dokazano ishemijo DP pomembno zmanjšano telesno zmogljivost napram tistim z normalno prekrvitvijo DP (dosežen odstotek predvidene največje porabe kisika 45,0±5,1 proti 56,7±2,9%, p=0,005). Drugih povezav med ishemijo ali fibrozo DP in ehokardiografskimi ali MR označevalci sistolične in diastolične funkcije DP nismo potrdili. Prav tako ni bilo razlik v primerjavi različnih laboratorijskih označevalcih med obema skupinama. Zaključki. Rezultati naše multidisciplinarne raziskave so pokazali, da sta ishemija in fibroza DP pogosti pri odraslih bolnikih s prirojeno srčno napako in kronično tlačno obremenitvijo DP. S tem smo potrdili rezultate redkih predhodnih raziskav na to temo. Naši rezultati kažejo tudi na povezanost ishemije DP in žariščne fibroze DP pri bolnikih s sistemskim DP. To verjetno patofiziološko povezavo bo potrebno zaradi majhnega števila vključenih bolnikov in preostalih omejitev naše raziskave potrditi v nadaljnjih večjih raziskavah. Boljše razumevanje povezave ishemije in fibroze DP bi namreč lahko vodilo v tarčno zdravljenje ishemije še pred pojavom fibroze miokarda. Kljub pogostnosti pa ishemija in fibroza DP v naši skupini bolnikov nista bili povezani z različnimi slikovnimi označevalci delovanja DP. To kaže na večplastno naravo nastanka poslabšanja delovanja in odpovedi DP, ki vključuje več različnih dejavnikov. Tudi za dokaz medsebojne povezanosti ishemije, fibroze in odpovedi DP bodo potrebne nadaljnje raziskave.

Language:Slovenian
Keywords:prirojene srčne napake, desni prekat, kronična tlačna obremenitev, ishemija, fibroza, sistemski desni prekat, transpozicija velikih žil, pljučna hipertenzija, Eisenmengerjev sindrom
Work type:Doctoral dissertation
Organization:MF - Faculty of Medicine
Year:2024
PID:20.500.12556/RUL-163669 This link opens in a new window
Publication date in RUL:10.10.2024
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Downloads:946
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Secondary language

Language:English
Title:​Right ventricular ischaemia and fibrosis in adults with congenital heart disease and right ventricular pressure overload
Abstract:
Background. Patients with congenital heart defects (CHD) and chronic pressure overload of the right ventricle (RV) are prone to long-term RV dysfunction and failure. The exact mechanism of RV dysfunction is unknown, but both pressure overload and pressure-independent factors are believed to play an important role. While myocardial ischemia and fibrosis are well known factors in acquired left-heart disease, their exact role in RV dysfunction and failure due to chronic pressure overload remains unknown. Imaging methods nowadays allow accurate non-invasive evaluation of both myocardial ischemia and fibrosis. The aim of our study was to assess myocardial ischemia and fibrosis in patients with CHD and chronic pressure overload of the RV and their possible association with clinical, laboratory, functional and imaging markers of RV function. Hypotheses. 1. Right ventricular ischaemia and fibrosis are present and related findings in adults with congenital heart disease and chronic right ventricular pressure overload. 2. Ischaemia and fibrosis are associated with right ventricular systolic and diastolic dysfunction in adults with congenital heart disease and chronic right ventricular pressure overload. 3. Serum biomarkers of cardiac fibrosis, electrocardiographic and echocardiographic parameters are associated with right ventricular ischaemia and fibrosis in adults with congenital heart disease and chronic right ventricular pressure overload. Research design and methods. This was a single centre cohort study, approved by the Slovenian Medical Ethics Committee. All patients with CHD and chronic RV pressure overload, including those with systemic RV (patients with transposition of the great arteries after atrial switch operation (TGA-AS) or patients with congenitally corrected transposition of the great arteries (CCTGA)) and patients with pulmonary arterial hypertension (PAH) and Eisenmenger syndrome, followed at the national referral centre for ACHD patients were invited to participate. Patients with acute or advanced chronic heart failure, uncontrolled arrhythmias, physical limitation precluding exercise testing or known genetic syndrome were excluded. After obtaining informed consent, each patient underwent a comprehensive multimodality study protocol that included echocardiography for assessment of RV systolic and diastolic function, single-photon emission computerized tomography (SPECT) for evaluation of RV ischemia and contrast enhanced cardiac magnetic resonance (CMR) for assessment of both focal (late gadolinium enhancement (LGE)) and diffuse (RV extracellular volume fraction (ECV)) RV fibrosis. Additionally, venous blood sampling for evaluation of different serum biomarkers (high-sensitivity troponin I, N-terminal prohormone of brain natriuretic peptide (NT-proBNP) and collagen turnover biomarkers) and cardiopulmonary exercise testing were also performed. Statistical analysis investigated the differences in clinical, laboratory, functional and imaging markers of the RV in patients with and without RV ischemia or fibrosis. Results. The final analysis included 32 adult patients with chronic RV pressure overload, including 15 patients with TGA-AS, 8 with CCTGA and 9 with ES. The mean age was 40 ± 10 years and 12 (33%) were women. Myocardial perfusion imaging with SPECT revealed reversible perfusion defects indicating RV ischemia in 12 patients (37%). No patient had chest pain, ischemic ECG changes or clinically important arrhythmias during exercise testing. In patients with RV ischemia, reversible perfusion defects were detected in a median of 1.5 (IQR [1-2]) RV segments and were most commonly observed in the anterior and free RV wall. There was no significant difference in RV ischemia between different patient subgroups (TGA-AS: 5 (33%), CCTGA: 2 (22%), ES: 5 (55%); p=0.41). Contrast enhanced CMR was possible in 25 (78%) patients and late gadolinium enhancement (LGE) indicating focal RV fibrosis was detected in 12 patients (48%). There was no significant difference in focal RV fibrosis between different patient subgroups (TGA-AS: 5 (42%), CCTGA: 2 (33%), ES: 5 (71%); p=0.35). Average values of RV ECV, representing a marker of diffuse RV fibrosis, did not differ between patient subgroups (p=0.152) and 28% of patients had abnormal RV ECV. Patients with confirmed RV ischemia more commonly had focal RV fibrosis, while there was no difference in the presence of diffuse RV fibrosis. Areas of LGE indicating focal RV fibrosis were present in 5 (31%) patients with normal RV perfusion and 7 (78%) patients with RV ischemia; p=0.041). Notably, subgroup analysis revealed that this association between RV ischemia and focal fibrosis was observed exclusively in patients with SRV (2 (15%) with normal RV perfusion vs 5 (100%) with RV ischemia, p=0.002), while patients with ES did not show the same relationship (3 (100%) vs 2 (50%), p=0.43). Comparison of clinical characteristics of all included patients revealed that patients with RV ischemia were significantly older than those with normal RV perfusion (42.6 ± 11.0 vs 38.4 ± 10.6 years; p= 0.049). There were no significant differences in other clinical parameters, such as history of arrhythmias or heart failure. Patient subgroup analysis of laboratory, imaging and functional parameters showed that patients with ES and confirmed RV ischemia had significantly lower exercise capacity compared to those without RV ischemia (percent-predicted peak oxygen consumption 45.0±5.1 vs 56.7±2.9%, p=0.005). However, there was no other association between RV ischemia or focal RV fibrosis and other echocardiographic or CMR parameters of RV systolic or diastolic function in both groups of patients. Laboratory markers were also similar. Conclusions. Our single centre, multimodality study demonstrated that RV ischemia and focal RV fibrosis are prevalent in adult patients with CHD and chronic RV pressure overload. These findings support limited previous studies on this topic. The observed association between RV ischemia and focal RV fibrosis in patients with SRV suggests a possible pathophysiological link. However, due to the small sample size and other study limitations, larger studies are necessary to gain a better understanding of this concept, which could potentially lead to targeted therapy for preventing myocardial fibrosis. Interestingly, RV ischemia or fibrosis did not show any association with various imaging markers of RV systolic or diastolic dysfunction. This finding emphasizes the intricate and multifaceted nature of RV dysfunction, necessitating further investigation to uncover the precise underlying mechanisms. A better understanding of the interconnected relationship between RV ischemia, fibrosis, and dysfunction may pave the way for targeted therapies aimed at preventing the development of myocardial dysfunction in these patients.

Keywords:congenital heart defects, right ventricle, chronic pressure overload, ischemia, fibrosis, systemic right ventricle, transposition of the great arteries, pulmonary hypertension, Eisenmenger syndrome

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