6 research outputs found
The association of beta-fibrinogen – 455G/A gene polymorphism with left atrial thrombus in patient with atrial fibrillation
Uvod: Do sada su poznati brojni prediktori tromboze aurikule lijevog atrija, no u tom je području još uvijek mnogo nepoznanica, pogotovo kada je riječ o genetskim prediktorima. Cilj ovoga istraživanja bio je pronaći genski marker koji može biti prediktor tromboze i time poboljšati procjenu tromboembolijskog rizika.
Metode i ispitanici: Dizajnirana je opservacijska, unicentrična, retrospektivna studija koja je uključila ukupno 181 bolesnika s atrijskom fibrilacijom. Primarni ishod istraživanja bio je detekcija tromba u aurikuli lijevoga atrija, a svim bolesnicima rađena je genska analiza na - 455 G/A polimorfizam gena za β lanac fibrinogena.
Rezultati: Nakon provedene metode uparivanja prema vjerojatnosti sklonosti dviju skupina bolesnika, niti jedna ispitivana varijabla, uključujući polimorfizam - 455 G/A beta-fibrinogena, nije se pokazala neovisnim prediktorom tromboze aurikule lijevog atrija.
Rasprava: Rezultati istraživanja u skladu su s do sada objavljenim studijama, gdje još uvijek postoji nesklad u rezultatima te su neka istraživanja pronašla povezanost - 455 G/A polimorfizma s trombogenezom, dok pak neka druga istraživanja nisu pronašla funkcionalnu vezu.
Zaključak: Rezultati upućuju na to da tromboza aurikule lijevoga atrija nije neovisno povezana sa - 455 G/A polimorfizmom za β lanac fibrinogena te je vjerojatno posljedica interakcije između gena, te gena i okoliša. No za dokazivanje navedenoga bit će nužna daljnja istraživanja.Introduction: There are many predictors of left atrial appendage thrombosis, but still there are many unknown facts, articularly in the area of genetic predictors. Purpose of this study was to find genetic predictor of thrombosis and to enhance evaluation of thromboembolic risk.
Methods: We conducted an observational, retrospective, unicentric study involving 181 patients with AF. Primary outcome of this study was to detect thrombus in left atrial appendage and all patients were scheduled for genetic analysis for - 55G/A β fibrinogen polymorphism.
Results: After performing propensity score matching method, none of tested parameters, including - 455G/A polymorphism, were not independent predictors of left atrial appendage thrombosis.
Discussion: This results are consistent with the results from many other studies in this field, where some studies have found functional relationship between thrombosis and - 455G/A polymorphism, but still many other studies have not found the same interaction.
Conclusion: Results showed that left atrial appendage thrombosis is not independently related with - 455G/A polymorphism for β chain of fibrinogen. It’s probably consequence of interactions between genes, and genes and environment. However, to confirm such statement we need to conduct more research in the future
The association of beta-fibrinogen – 455G/A gene polymorphism with left atrial thrombus in patient with atrial fibrillation
Uvod: Do sada su poznati brojni prediktori tromboze aurikule lijevog atrija, no u tom je području još uvijek mnogo nepoznanica, pogotovo kada je riječ o genetskim prediktorima. Cilj ovoga istraživanja bio je pronaći genski marker koji može biti prediktor tromboze i time poboljšati procjenu tromboembolijskog rizika.
Metode i ispitanici: Dizajnirana je opservacijska, unicentrična, retrospektivna studija koja je uključila ukupno 181 bolesnika s atrijskom fibrilacijom. Primarni ishod istraživanja bio je detekcija tromba u aurikuli lijevoga atrija, a svim bolesnicima rađena je genska analiza na - 455 G/A polimorfizam gena za β lanac fibrinogena.
Rezultati: Nakon provedene metode uparivanja prema vjerojatnosti sklonosti dviju skupina bolesnika, niti jedna ispitivana varijabla, uključujući polimorfizam - 455 G/A beta-fibrinogena, nije se pokazala neovisnim prediktorom tromboze aurikule lijevog atrija.
Rasprava: Rezultati istraživanja u skladu su s do sada objavljenim studijama, gdje još uvijek postoji nesklad u rezultatima te su neka istraživanja pronašla povezanost - 455 G/A polimorfizma s trombogenezom, dok pak neka druga istraživanja nisu pronašla funkcionalnu vezu.
Zaključak: Rezultati upućuju na to da tromboza aurikule lijevoga atrija nije neovisno povezana sa - 455 G/A polimorfizmom za β lanac fibrinogena te je vjerojatno posljedica interakcije između gena, te gena i okoliša. No za dokazivanje navedenoga bit će nužna daljnja istraživanja.Introduction: There are many predictors of left atrial appendage thrombosis, but still there are many unknown facts, articularly in the area of genetic predictors. Purpose of this study was to find genetic predictor of thrombosis and to enhance evaluation of thromboembolic risk.
Methods: We conducted an observational, retrospective, unicentric study involving 181 patients with AF. Primary outcome of this study was to detect thrombus in left atrial appendage and all patients were scheduled for genetic analysis for - 55G/A β fibrinogen polymorphism.
Results: After performing propensity score matching method, none of tested parameters, including - 455G/A polymorphism, were not independent predictors of left atrial appendage thrombosis.
Discussion: This results are consistent with the results from many other studies in this field, where some studies have found functional relationship between thrombosis and - 455G/A polymorphism, but still many other studies have not found the same interaction.
Conclusion: Results showed that left atrial appendage thrombosis is not independently related with - 455G/A polymorphism for β chain of fibrinogen. It’s probably consequence of interactions between genes, and genes and environment. However, to confirm such statement we need to conduct more research in the future
The association of beta-fibrinogen – 455G/A gene polymorphism with left atrial thrombus in patient with atrial fibrillation
Uvod: Do sada su poznati brojni prediktori tromboze aurikule lijevog atrija, no u tom je području još uvijek mnogo nepoznanica, pogotovo kada je riječ o genetskim prediktorima. Cilj ovoga istraživanja bio je pronaći genski marker koji može biti prediktor tromboze i time poboljšati procjenu tromboembolijskog rizika.
Metode i ispitanici: Dizajnirana je opservacijska, unicentrična, retrospektivna studija koja je uključila ukupno 181 bolesnika s atrijskom fibrilacijom. Primarni ishod istraživanja bio je detekcija tromba u aurikuli lijevoga atrija, a svim bolesnicima rađena je genska analiza na - 455 G/A polimorfizam gena za β lanac fibrinogena.
Rezultati: Nakon provedene metode uparivanja prema vjerojatnosti sklonosti dviju skupina bolesnika, niti jedna ispitivana varijabla, uključujući polimorfizam - 455 G/A beta-fibrinogena, nije se pokazala neovisnim prediktorom tromboze aurikule lijevog atrija.
Rasprava: Rezultati istraživanja u skladu su s do sada objavljenim studijama, gdje još uvijek postoji nesklad u rezultatima te su neka istraživanja pronašla povezanost - 455 G/A polimorfizma s trombogenezom, dok pak neka druga istraživanja nisu pronašla funkcionalnu vezu.
Zaključak: Rezultati upućuju na to da tromboza aurikule lijevoga atrija nije neovisno povezana sa - 455 G/A polimorfizmom za β lanac fibrinogena te je vjerojatno posljedica interakcije između gena, te gena i okoliša. No za dokazivanje navedenoga bit će nužna daljnja istraživanja.Introduction: There are many predictors of left atrial appendage thrombosis, but still there are many unknown facts, articularly in the area of genetic predictors. Purpose of this study was to find genetic predictor of thrombosis and to enhance evaluation of thromboembolic risk.
Methods: We conducted an observational, retrospective, unicentric study involving 181 patients with AF. Primary outcome of this study was to detect thrombus in left atrial appendage and all patients were scheduled for genetic analysis for - 55G/A β fibrinogen polymorphism.
Results: After performing propensity score matching method, none of tested parameters, including - 455G/A polymorphism, were not independent predictors of left atrial appendage thrombosis.
Discussion: This results are consistent with the results from many other studies in this field, where some studies have found functional relationship between thrombosis and - 455G/A polymorphism, but still many other studies have not found the same interaction.
Conclusion: Results showed that left atrial appendage thrombosis is not independently related with - 455G/A polymorphism for β chain of fibrinogen. It’s probably consequence of interactions between genes, and genes and environment. However, to confirm such statement we need to conduct more research in the future
Left Ventricular Ejection Fraction Can Predict Atrial Thrombosis Even in Non-High-Risk Individuals with Atrial Fibrillation
Background—Current guidelines do not recommend routine use of transesophageal echocardiography (TOE) in anticoagulated patients with atrial fibrillation (AF). The aim of our study was to identify predictors for left atrial thrombosis (LAT) in patients with AF that would require TOE despite anticoagulation therapy, using clinical, laboratory and echocardiographic data which are usually obtained in those patients in a real-world setting. Methods—We analyzed data from electronic medical records (EMR) of consecutive AF patients referred to two university hospitals between January 2014 and December 2017 for pulmonary vein isolation (PVI) or direct current cardioversion. The primary endpoint was the presence of left atrial thrombus on TOE. Multivariable and univariable logistic regression models were computed using variables that were significantly different between the LAT and the control groups. Results—A total of 838 patients were included, of whom 132 (15.8%) had LAT. After controlling for other variables, only the left ventricle ejection fraction (LVEF) remained statistically significant with an OR of 0.956 (95% CI 0.934–0.979), p p < 0.0001. Conclusions—The LVEF is an independent predictor of LAT, and it might improve thromboembolic risk stratification in future models. LVEF significantly increased the predictive value of the CHA2DS2-Vasc model and was able to identify LAT in non-high-risk patients