Your search keyword '"Cohen, Sarah"' showing total 6 results

1. Evaluación multiparamétrica de la función ventricular derecha en la hipertensión arterial pulmonar asociada a cardiopatías congénitas

Author

Fournier, Emmanuelle, Selegny, Maëlle, Amsallem, Myriam, Haddad, Francois, Cohen, Sarah, Valdeolmillos, Estibaliz, Le Pavec, Jérôme, Humbert, Marc, Isorni, Marc-Antoine, Azarine, Arshid, Sitbon, Olivier, Jais, Xavier, Savale, Laurent, Montani, David, Fadel, Elie, Zoghbi, Joy, Belli, Emre, and Hascoët, Sebastien

Published

2023

2. Fusión de imágenes de tomografía computarizada cardiaca y ecocardiografía: un nuevo enfoque en las cardiopatías congénitas

Author

Fournier, Emmanuelle, Batteux, Clément, Mostefa-Kara, Meriem, Valdeolmillos, Estibaliz, Maltret, Alice, Cohen, Sarah, Van Aerschot, Isabelle, Guirgis, Lisa, Azarine, Arshid, Sigal-Cinqualbre, Anne, Provost, Bastien, Radojevic-Liegeois, Jelena, Roussin, Régine, Zoghbi, Joy, Belli, Emre, and Hascoët, Sebastien

Published

2023

3. Capítulo 47 - Ventilación mecánica

Author

Cohen, Sarah P.

Published

2022

4. Colaboradores

Author

Aaron, Justin G., Almarzooq, Zaid I., Amigues, Isabelle, Arakawa, Rachel, Augelli, Dianne M., Bazarbashi, Ahmad Najdat, Beckta, Jason M., Bhatt, Ankeet S., Bhattacharya, Manisha, Bilan, Victor P., Burnett, Eric J., Card, Mary Elizabeth, Choi, Bina, Chowdhury, Mohsin, Chukir, Tariq, Cohen, Margot E., Cohen, Sarah P., Cohen-Mekelburg, Shirley, Contractor, Jigar, Cook, Joshua R., Cool, Joséphine A., Cromer, Sara J., Dahhan, Talal, Dennis, Madison, DeVoe, Catherine, Diep, Robert, Djulbegovic, Mia, Dupuis, Megan M., Edmonston, Daniel, Egwim, Chidiebube C., Elias, Pierre, Engel, David J., Fahme, Sasha A., Faruqi, Fahad, Feder, Rachel, Fitzgerald, Kelly J., Gallagher, Benjamin D., Gallup, Cecily J., Ghosh, Gaurav, Gold, Stephanie L., Gondal, Maryam, Gottlieb, Armand, Grant, Michael J., Gupta, Vikas, Haghighat, Leila, Hermann, Emilia A., Hindle-Katel, Will, Holder, Tara, Infeld, Margaret, Jabbour, Gina P., Jacox, Jeremy B., Jiang, Debbie, Joerns, Elena K., Kelly, Christopher R., Kim, Judith, Kim, Richard K., Kinsey, Emily N., Komisar, Jonathan R., Kovalik, Eugene C., Krishnan, Govind M., Krishnarasa, Balakumar, Kunnirickal, Steffne, Labriola, Matthew K., Lakhanpal, Amit, Lamba, Perola, Lampert, Joshua, Laracy, Justin C., Laszkowska, Monika, Lee, Alfred, Lehrich, Ruediger W., Leppert, Bryan C., Lim, Hana I., Liu, Ying L., Lysy, Zoë, Makar, Melissa S., Malhotra, Divyanshu, Malick, Waqas A., Martin, Paul B., Mathew, Elizabeth, Mathews, Anne M., McCulloch, Matthew R., McGuinness, Julia E., McManigle, William C., Mehra, Karishma K., Mehta, Amit, Moledina, Dennis G., Mufson, Jeffrey, Murn, Michael, Mutter, Marina, Nair, Abhinav, Namn, Yunseok, Navuluri, Neelima, Nematollahi, Saman, Ngeno, G. Titus K., Novikov, Aleksey, O’Reilly, John I., Oruc, Vedran, Parikh, Kinjan, Perel-Winkler, Alexandra C., Pierce, Theodore T., Pischel, Lauren, Pumill, Christopher A., Rajagopalan, Kartik N., Roeder, Hannah, Rosenbaum, Evan, Rosenblatt, Russell, Roy-Burman, Paula, Rubin, Jonah, Saumoy, Monica, Schneider, Yecheskel, Selvadurai, Chindhuri, Shah, Shawn L., Shen, Nicole T., Sherman, Zachary, Shinnar, Eliezer, Sinha, Pranay, Smith, Colin M., Snell, David B., Spann, Ashley L., Spates, Toi N., Stahl, Maximilian, Stewart, Tyler F., Tallman, Martin S., Tang, Alice J., Tang, Stephanie J., Tchang, Beverly G., Tewani, Sunena, Traner, Christopher Bentley, Traynor, Carol, Tripathi, Nidhi, Truby, Lauren K., Tucker, Bryan M., Tucker, Jesse, Turner, Daniel J., Uy, Natalie F., Valeri, Anthony, Varghese, Merilyn S., Vivekanandarajah, Abhirami, Xie, Hao, Yang, Jessica, Yankey, George S.A., Jr, Yeung, Michele, Yi, Pauline B., Yun, Jae Hee, Zheng, Fangfei, Zhuo, Sharon, and Zietlow, Kahli E.

Published

2022

5. Multiparametric evaluation of right ventricular function in pulmonary arterial hypertension associated with congenital heart disease.

Author

Fournier E, Selegny M, Amsallem M, Haddad F, Cohen S, Valdeolmillos E, Le Pavec J, Humbert M, Isorni MA, Azarine A, Sitbon O, Jais X, Savale L, Montani D, Fadel E, Zoghbi J, Belli E, and Hascoët S

Subjects

Humans, Ventricular Function, Right, Stroke Volume, Pulmonary Arterial Hypertension complications, Atrial Fibrillation complications, Hypertension, Pulmonary diagnosis, Hypertension, Pulmonary etiology, Heart Defects, Congenital complications, Heart Defects, Congenital diagnosis, Ventricular Dysfunction, Right diagnostic imaging, Ventricular Dysfunction, Right etiology

Abstract

Introduction and Objectives: Outcome in patients with congenital heart diseases and pulmonary arterial hypertension (PAH) is closely related to right ventricular (RV) function. Two-dimensional echocardiographic parameters, such as strain imaging or RV end-systolic remodeling index (RVESRI) have emerged to quantify RV function., Methods: We prospectively studied 30 patients aged 48±12 years with pretricuspid shunt and PAH and investigated the accuracy of multiple echocardiographic parameters of RV function (tricuspid annular plane systolic excursion, tricuspid annular peak systolic velocity, RV systolic-to-diastolic duration ratio, right atrial area, RV fractional area change, RV global longitudinal strain and RVESRI) to RV ejection fraction measured by cardiac magnetic resonance., Results: RV ejection fraction <45% was observed in 13 patients (43.3%). RV global longitudinal strain (ρ [Spearman's correlation coefficient]=-0.75; P=.001; R 2 =0.58; P=.001), right atrium area (ρ=-0.74; P <.0001; R 2 =0.56; P <.0001), RVESRI (ρ=-0.64; P <.0001; R 2 =0.47; P <.0001), systolic-to-diastolic duration ratio (ρ=-0.62; P=.0004; R 2 =0.47; P <.0001) and RV fractional area change (ρ=0.48; P=.01; R 2 =0.37; P <.0001) were correlated with RV ejection fraction. RV global longitudinal strain, RVESRI and right atrium area predicted RV ejection fraction <45% with the greatest area under curve (0.88; 95%CI, 0.71-1.00; 0.88; 95%CI, 0.76-1.00, and 0.89; 95%CI, 0.77-1.00, respectively). RV global longitudinal strain >-16%, RVESRI ≥ 1.7 and right atrial area ≥ 22 cm 2 predicted RV ejection fraction <45% with a sensitivity and specificity of 87.5% and 85.7%; 76.9% and 88.3%; 92.3% and 82.4%, respectively., Conclusions: RVESRI, right atrial area and RV global longitudinal strain are strong markers of RV dysfunction in patients with pretricuspid shunt and PAH., (Copyright © 2022 Sociedad Española de Cardiología. Published by Elsevier España, S.L.U. All rights reserved.)

Published

2023

6. Cardiac tomography-echocardiography imaging fusion: a new approach to congenital heart disease.

Author

Fournier E, Batteux C, Mostefa-Kara M, Valdeolmillos E, Maltret A, Cohen S, Van Aerschot I, Guirgis L, Azarine A, Sigal-Cinqualbre A, Provost B, Radojevic-Liegeois J, Roussin R, Zoghbi J, Belli E, and Hascoët S

Subjects

Child, Adult, Humans, Male, Female, Echocardiography methods, Heart diagnostic imaging, Tomography, X-Ray Computed, Heart Defects, Congenital diagnostic imaging, Heart Defects, Congenital surgery, Echocardiography, Three-Dimensional methods

Abstract

Introduction and Objectives: Diagnosis, management, and surgical decision-making in children and adults with congenital heart disease are largely based on echocardiography findings. A recent development in cardiac imaging is fusion of different imaging modalities. Our objective was to evaluate the feasibility of computed tomography (CT) and 3-dimensional (3D) transthoracic echocardiography (TTE) fusion in children and adults with congenital heart disease., Methods: We prospectively included 14 patients, 13 of whom had congenital heart disease, and who underwent both CT and 3D TTE as part of their usual follow-up. We described the steps required to complete the fusion process (alignment, landmarks, and superimposition), navigation, and image evaluation., Results: Median age was 9.5 [2.7-15.7] years, 57% were male, and median body surface area was 0.9 m 2 [0.6-1.7]. Congenital heart disease was classified as simple (n=4, 29%), moderate (n=4, 29%), or complex (n=6, 42%). 3D TTE-CT fusion was successful in all patients. Median total time to complete the fusion process was 735 [628-1163] seconds, with no significant difference according to the degree of complexity of the defects. Landmarks were significantly modified in complex congenital heart disease., Conclusions: We established the feasibility and accuracy of 3D TTE-CT fusion in a population of children and adults with a variety of congenital heart diseases. The simultaneous visualization of many intracardiac structures may help to understand the anatomical features of congenital heart disease without limitations regarding age, weight, or complexity of the congenital defects., (Copyright © 2022 Sociedad Española de Cardiología. Published by Elsevier España, S.L.U. All rights reserved.)

Published

2023