Your search keyword '"Grazioli, Serge"' showing total 44 results

1. The plasma proteome differentiates the multisystem inflammatory syndrome in children (MIS-C) from children with SARS-CoV-2 negative sepsis

Author

Patel, Maitray A., Fraser, Douglas D., Daley, Mark, Cepinskas, Gediminas, Veraldi, Noemi, and Grazioli, Serge

Published

2024

2. Cardiac assessment and inflammatory markers in children with paediatric inflammatory multisystem syndrome temporally associated with SARS-CoV2 (PIMS-TS) treated with methylprednisolone versus intravenous immunoglobulins: 6-month follow-up outcomes of the randomised controlled Swissped RECOVERY trial

Author

Andre, Maya C., Sanchez, Carlos, Bressieux-Degueldre, Sabrina, Perez, Marie-Helene, Wütz, Daniela, Blanchard-Rohner, Geraldine, Grazioli, Serge, Schöbi, Nina, Trück, Johannes, Welzel, Tatjana, Atkinson, Andrew, Schlapbach, Luregn J., Bielicki, Julia, Koehler, Henrik, Gysi, Spyridoula, Janz, Indra, Bieri, Andreas, Donner, Birgit, Hammer, Jürg, Heininger, Ulrich, von Kalckreuth, Clemens, Kohns, Malte, Mettauer, Nicole, Meyer, Alexandra, Reppucci, Diana, Schlaeppi, Chloé, Trachsel, Daniel, Vaezipour, Nina, Woerner, Andreas, Zutter, Andreas, Vanoni, Federica, Kottanattu, Lisa, Mazzara, Calogero, Conti, Alessia Severi, Aebi, Christoph, Agyeman, Philipp, Duppenthaler, Andrea, Glöckler, Martin, Pallivathukal, Sabine, Riedel, Thomas, Zimmermann, Petra, Cudré-Cung, Hong-Phuc, Pavlovic, Mladen, Bordessoule, Alice, Martin, Anne-Laure, Polito, Angelo, Wagner, Noemie, Rohr, Marie, L'Huillier, Arnaud, Amiet, Vivianne, Ferry, Thomas, Longchamp, David, Natterer, Julia, Oppenheim, Rebecca, Hofer, Michael, Buettcher, Michael, Wechselberger, Katharina, Donas, Alex, Germann, Sara, Erni, Michaela Lütolf, Kaiser, Daniela, Scholl, Katharina Schwendener, Kuen, Hans Peter, Hrup, Katja, Stritt, Janine, Bailey, Douggl G.N., Wachinger, Tanja, Beck, Ingrid, Birkenmaier, André, Rogdo, Bjarte, Lorenz, Philip, Iglowstein, Ivo, Zöhrer, Konstanze, Flade, Martin, Prader, Seraina, Schmid, Jana Pachlopnik, Seiler, Michelle, Sauteur, Patrick Meyer, Brotschi, Barbara, Weber, Kathrin, Whittaker, Elizabeth, and Faust, Saul N.

Published

2024

3. Endothelial glycocalyx degradation in multisystem inflammatory syndrome in children related to COVID-19

Author

Veraldi, Noemi, Vivès, Romain R., Blanchard-Rohner, Géraldine, L’Huillier, Arnaud G., Wagner, Noemie, Rohr, Marie, Beghetti, Maurice, De Agostini, Ariane, and Grazioli, Serge

Published

2022

4. Machine learning using the extreme gradient boosting (XGBoost) algorithm predicts 5-day delta of SOFA score at ICU admission in COVID-19 patients

Author

Alfaro-Farias, Mario, Vizmanos-Lamotte, Gerardo, Tschoellitsch, Thomas, Meier, Jens, Aguirre-Bermeo, Hernán, Apolo, Janina, Martínez, Alberto, Jurkolow, Geoffrey, Delahaye, Gauthier, Novy, Emmanuel, Losser, Marie-Reine, Wengenmayer, Tobias, Rilinger, Jonathan, Staudacher, Dawid L., David, Sascha, Welte, Tobias, Stahl, Klaus, Pavlos”, “Agios, Aslanidis, Theodoros, Korsos, Anita, Babik, Barna, Nikandish, Reza, Rezoagli, Emanuele, Giacomini, Matteo, Nova, Alice, Fogagnolo, Alberto, Spadaro, Savino, Ceriani, Roberto, Murrone, Martina, Wu, Maddalena A., Cogliati, Chiara, Colombo, Riccardo, Catena, Emanuele, Turrini, Fabrizio, Simonini, Maria Sole, Fabbri, Silvia, Potalivo, Antonella, Facondini, Francesca, Gangitano, Gianfilippo, Perin, Tiziana, Grazia Bocci, Maria, Antonelli, Massimo, Gommers, Diederik, Rodríguez-García, Raquel, Gámez-Zapata, Jorge, Taboada-Fraga, Xiana, Castro, Pedro, Tellez, Adrian, Lander-Azcona, Arantxa, Escós-Orta, Jesús, Martín-Delgado, Maria C., Algaba-Calderon, Angela, Franch-Llasat, Diego, Roche-Campo, Ferran, Lozano-Gómez, Herminia, Zalba-Etayo, Begoña, Michot, Marc P., Klarer, Alexander, Ensner, Rolf, Schott, Peter, Urech, Severin, Zellweger, Nuria, Merki, Lukas, Lambert, Adriana, Laube, Marcus, Jeitziner, Marie M., Jenni-Moser, Beatrice, Wiegand, Jan, Yuen, Bernd, Lienhardt-Nobbe, Barbara, Westphalen, Andrea, Salomon, Petra, Drvaric, Iris, Hillgaertner, Frank, Sieber, Marianne, Dullenkopf, Alexander, Petersen, Lina, Chau, Ivan, Ksouri, Hatem, Sridharan, Govind Oliver, Cereghetti, Sara, Boroli, Filippo, Pugin, Jerome, Grazioli, Serge, Rimensberger, Peter C., Bürkle, Christian, Marrel, Julien, Brenni, Mirko, Fleisch, Isabelle, Lavanchy, Jerome, Perez, Marie-Helene, Ramelet, Anne-Sylvie, Weber, Anja Baltussen, Gerecke, Peter, Christ, Andreas, Ceruti, Samuele, Glotta, Andrea, Marquardt, Katharina, Shaikh, Karim, Hübner, Tobias, Neff, Thomas, Redecker, Hermann, Moret-Bochatay, Mallory, Bentrup, FriederikeMeyer zu, Studhalter, Michael, Stephan, Michael, Brem, Jan, Gehring, Nadine, Selz, Daniela, Naon, Didier, Kleger, Gian-Reto, Pietsch, Urs, Filipovic, Miodrag, Ristic, Anette, Sepulcri, Michael, Heise, Antje, Franchitti Laurent, Marilene, Laurent, Jean-Christophe, Wendel Garcia, Pedro D., Schuepbach, Reto, Heuberger, Dorothea, Bühler, Philipp, Brugger, Silvio, Fodor, Patricia, Locher, Pascal, Camen, Giovanni, Gaspert, Tomislav, Jovic, Marija, Haberthuer, Christoph, Lussman, Roger F., Colak, Elif, Montomoli, Jonathan, Romeo, Luca, Moccia, Sara, Bernardini, Michele, Migliorelli, Lucia, Berardini, Daniele, Donati, Abele, Carsetti, Andrea, Bocci, Maria Grazia, Wendel Garcia, Pedro David, Fumeaux, Thierry, Guerci, Philippe, Schüpbach, Reto Andreas, Ince, Can, Frontoni, Emanuele, and Hilty, Matthias Peter

Published

2021

5. COVID-19 Vaccine Acceptance Among Parents of Children With Multisystem Inflammatory Syndrome in Children

Author

Blanchard-Rohner, Geraldine; https://orcid.org/0000-0002-9974-2172, Sanchez, Carlos, Andre, Maya C, Bressieux-Degueldre, Sabrina, Grazioli, Serge, Perez, Marie-Helene, Wütz, Daniela; https://orcid.org/0000-0002-5186-2634, Schöbi, Nina, Welzel, Tatjana, Atkinson, Andrew, Schlapbach, Luregn J; https://orcid.org/0000-0003-2281-2598, Bielicki, Julia A, Trück, Johannes; https://orcid.org/0000-0002-0418-7381, Swissped RECOVERY Trial Group, et al, Prader, Seraina; https://orcid.org/0000-0002-2950-5411, Pachlopnik Schmid, Jana; https://orcid.org/0000-0002-6653-9047, Seiler, Michelle; https://orcid.org/0000-0002-1263-5818, Meyer Sauteur, Patrick, Brotschi, Barbara; https://orcid.org/0000-0002-4472-5199, Weber, Kathrin, Blanchard-Rohner, Geraldine; https://orcid.org/0000-0002-9974-2172, Sanchez, Carlos, Andre, Maya C, Bressieux-Degueldre, Sabrina, Grazioli, Serge, Perez, Marie-Helene, Wütz, Daniela; https://orcid.org/0000-0002-5186-2634, Schöbi, Nina, Welzel, Tatjana, Atkinson, Andrew, Schlapbach, Luregn J; https://orcid.org/0000-0003-2281-2598, Bielicki, Julia A, Trück, Johannes; https://orcid.org/0000-0002-0418-7381, Swissped RECOVERY Trial Group, et al, Prader, Seraina; https://orcid.org/0000-0002-2950-5411, Pachlopnik Schmid, Jana; https://orcid.org/0000-0002-6653-9047, Seiler, Michelle; https://orcid.org/0000-0002-1263-5818, Meyer Sauteur, Patrick, Brotschi, Barbara; https://orcid.org/0000-0002-4472-5199, and Weber, Kathrin

Abstract

Data on COVID-19 vaccine acceptability among parents of children with multisystem inflammatory syndrome (MIS-C) are limited. In this cohort of children with MIS-C, enrolled in the Swissped RECOVERY trial (NCT04826588), comparing intravenous immunoglobulins or methylprednisolone, who, in accordance with Swiss guidelines, were recommended for SARS-CoV-2 vaccination, 65% (73/112) of parents reported being vaccinated against SARS-CoV-2 before the MIS-C, while 70% were vaccinated after the MIS-C episode of their child. None of the children were vaccinated before the occurrence of the MIS-C, and only 9% (5/56) received the COVID-19 vaccine after the MIS-C. The predominant barriers to COVID-19 vaccination were concerns over potential side effects and insufficient support from their doctors. This emphasizes the crucial role of health care providers in promoting COVID-19 vaccination among children.

Published

2024

6. Cardiac assessment and inflammatory markers in children with paediatric inflammatory multisystem syndrome temporally associated with SARS-CoV2 (PIMS-TS) treated with methylprednisolone versus intravenous immunoglobulins: 6-month follow-up outcomes of the randomised controlled Swissped RECOVERY trial

Author

Maya C, Andre; https://orcid.org/0000-0003-1555-2011, Sanchez, Carlos; https://orcid.org/0000-0002-1572-7590, Bressieux-Degueldre, Sabrina, Perez, Marie-Hélène, Wütz, Daniela; https://orcid.org/0000-0002-5186-2634, Blanchard-Rohner, Geraldine; https://orcid.org/0000-0002-9974-2172, Grazioli, Serge; https://orcid.org/0000-0002-5526-851X, Schöbi, Nina, Trück, Johannes; https://orcid.org/0000-0002-0418-7381, Welzel, Tatjana, Atkinson, Andrew; https://orcid.org/0000-0001-5834-8315, Schlapbach, Luregn J, Bielicki, Julia, Swissped RECOVERY Trial Group, Maya C, Andre; https://orcid.org/0000-0003-1555-2011, Sanchez, Carlos; https://orcid.org/0000-0002-1572-7590, Bressieux-Degueldre, Sabrina, Perez, Marie-Hélène, Wütz, Daniela; https://orcid.org/0000-0002-5186-2634, Blanchard-Rohner, Geraldine; https://orcid.org/0000-0002-9974-2172, Grazioli, Serge; https://orcid.org/0000-0002-5526-851X, Schöbi, Nina, Trück, Johannes; https://orcid.org/0000-0002-0418-7381, Welzel, Tatjana, Atkinson, Andrew; https://orcid.org/0000-0001-5834-8315, Schlapbach, Luregn J, Bielicki, Julia, and Swissped RECOVERY Trial Group

Abstract

Background: Previous findings from the Swissped RECOVERY trial showed that patients with Pediatric Inflammatory Multisystem Syndrome-Temporally Associated with SARS-CoV-2 (PIMS-TS) who were randomly assigned to intravenous immunoglobulins or methylprednisolone have a comparable length of hospital stay. Here, we report the 6-month follow-up outcomes of cardiac pathologies and normalisation of clinical or laboratory signs of inflammation from this study population. Methods: This pre-planned follow-up of patients with PIMS-TS included the Swissped RECOVERY Trial reports on the 6-month outcomes of the cohort after randomisation, with a focus on cardiac, haematological, and biochemical findings. The trial was an investigator-initiated randomised multicentre open-label two-arm trial in children and adolescents hospitalised with PIMS-TS at ten hospitals in Switzerland. Cardiological assessments and laboratory analyses were prospectively collected in the intention-to-treat analysis on pre-defined intervals after hospital discharge. Differences between randomised arms were investigated using Chi-square test for categorical and Wilcoxon test for continuous variables. The trial is registered with the Swiss National Clinical Trials Portal (SNCTP000004720) and ClinicalTrials.gov (NCT04826588). Findings: Between May 21, 2021 and April 15, 2022, 75 patients with a median age of 9.1 years (IQR 6.2-12.2) were included in the intention-to-treat population (37 in the methylprednisolone group and 38 in the intravenous immunoglobulin group). During follow-up, the incidence of abnormal left ventricular systolic function, coronary artery aneurysms (CAA), and other signs of inflammation were comparable in both groups. However, we detected cardiac abnormalities with low incidence and a mild degree grade of pathology. CAAs were observed in 2/38 children (5.3%) in the IVIG group and 1/37 children (2.7%) in the methylprednisolone group at 6-month follow-up (difference proportion 0.75; 95% conf

Published

2024

7. Prognostic factors associated with mortality risk and disease progression in 639 critically ill patients with COVID-19 in Europe: Initial report of the international RISC-19-ICU prospective observational cohort

Author

Alfaro Farias, Mario, Margarit, Antoni, Vizmanos-Lamotte, Gerardo, Tschoellitsch, Thomas, Meier, Jens, Cardona, Francesco S., Skola, Josef, Horakova, Lenka, Aguirre-Bermeo, Hernan, Apolo, Janina, Novy, Emmanuel, Losser, Marie-Reine, Jurkolow, Geoffrey, Delahaye, Gauthier, David, Sascha, Welte, Tobias, Wengenmayer, Tobias, Staudacher, Dawid L., Aslanidis, Theodoros, Babik, Barna, Korsos, Anita, Gal, Janos, Csaba, Hermann, Donati, Abele, Carsetti, Andrea, Turrini, Fabrizio, Simonini, Maria Sole, Ceriani, Roberto, Murrone, Martina, Rezoagli, Emanuele, Vitale, Giovanni, Fogagnolo, Alberto, Spadaro, Savino, Wu, Maddalena Alessandra, Cogliati, Chiara, Colombo, Riccardo, Catena, Emanuele, Facondini, Francesca, Potalivo, Antonella, Gangitano, Gianfilippo, Perin, Tiziana, Bocci, Maria Grazia, Antonelli, Massimo, Gommers, Diederik, Ince, Can, Mayor-Vázquez, Eric, Cruz, Maria, Delgado, Martin, Garcia, Raquel Rodriguez, Gamez Zapata, Jorge, Zalba-Etayo, Begoña, Lozano-Gomez, Herminia, Castro, Pedro, Tellez, Adrian, Jacas, Adriana, Muñoz, Guido, Andrea, Rut, Ortiz, Jose, Quintana, Eduard, Rovira, Irene, Reverter, Enric, Fernandez, Javier, Ferrer, Miquel, Badia, Joan R., Lander Azcona, Arantxa, Orta, Jesus Escos, Bühler, Philipp, Brugger, Silvio, Hofmaenner, Daniel, Unseld, Simone, Ruschitzka, Frank, Moret-Bochatay, Mallory, Yuen, Bernd, Hillermann, Thomas, Ksouri, Hatem, Sridharan, Govind Oliver, Ristic, Anette, Sepulcri, Michael, Filipovic, Miodrag, Pietsch, Urs, Salomon, Petra, Drvaric, Iris, Schott, Peter, Urech, Severin, Lambert, Adriana, Merki, Lukas, Laube, Marcus, Hillgaertner, Frank, Sieber, Marianne, Dullenkopf, Alexander, Petersen, Lina, Grazioli, Serge, Rimensberger, Peter C., Fleisch, Isabelle, Lavanchy, Jerome, Marquardt, Katharina, Shaikh, Karim, Redecker, Hermann, Stephan, Michael, Brem, Jan, Rogdo, Bjarte, Birkenmaier, Andre, Meyer zu Bentrup, Friederike, Fodor, Patricia, Locher, Pascal, Camen, Giovanni, Siegemund, Martin, Zellweger, Nuria, Jeitziner, Marie-Madlen, Jenni-Moser, Beatrice, Bürkle, Christian, Kleger, Gian-Reto, Franchitti Laurent, Marilene, Laurent, Jean-Christophe, Gaspert, Tomislav, Jovic, Marija, Studhalter, Michael, Haberthuer, Christoph, Lussman, Roger F., Selz, Daniela, Naon, Didier, Mauri, Romano, Ceruti, Samuele, Marrel, Julien, Brenni, Mirko, Ensner, Rolf, Gehring, Nadine, Heise, Antje, Huebner, Tobias, Neff, Thomas A., Cereghetti, Sara, Boroli, Filippo, Pugin, Jerome, Marczin, Nandor, Wong, Joyce, Wendel Garcia, Pedro David, Fumeaux, Thierry, Guerci, Philippe, Heuberger, Dorothea Monika, Montomoli, Jonathan, Roche-Campo, Ferran, Schuepbach, Reto Andreas, and Hilty, Matthias Peter

Published

2020

8. Antibody response in children with multisystem inflammatory syndrome related to COVID-19 (MIS-C) compared to children with uncomplicated COVID-19

Author

Thiriard, Anaïs, primary, Meyer, Benjamin, additional, Eberhardt, Christiane S., additional, Loevy, Natasha, additional, Grazioli, Serge, additional, Adouan, Wafae, additional, Fontannaz, Paola, additional, Marechal, Fabienne, additional, L’Huillier, Arnaud G., additional, Siegrist, Claire-Anne, additional, Georges, Daphnée, additional, Putignano, Antonella, additional, Marchant, Arnaud, additional, Didierlaurent, Arnaud M., additional, and Blanchard-Rohner, Geraldine, additional

Published

2023

9. Antibody response in children with multisystem inflammatory syndrome related to COVID-19 (MIS-C) compared to children with uncomplicated COVID-19.

Author

Thiriard, Anaïs, Meyer, Benjamin, Eberhardt, Christiane Sigrid, Loevy, Natasha, Grazioli, Serge, Adouan, Wafae, Fontannaz, Paola, Marechal, Fabienne, L'Huillier, Arnaud G, Siegrist, Claire-Anne, Georges, Daphnée, Putignano, Antonella, Marchant, Arnaud, Didierlaurent, Arnaud M, Blanchard-Rohner, Geraldine, Thiriard, Anaïs, Meyer, Benjamin, Eberhardt, Christiane Sigrid, Loevy, Natasha, Grazioli, Serge, Adouan, Wafae, Fontannaz, Paola, Marechal, Fabienne, L'Huillier, Arnaud G, Siegrist, Claire-Anne, Georges, Daphnée, Putignano, Antonella, Marchant, Arnaud, Didierlaurent, Arnaud M, and Blanchard-Rohner, Geraldine

Abstract

To comprehensively analyze the quality of the antibody response between children with Multisystem inflammatory syndrome (MIS-C) and age-matched controls at one month after SARS-CoV-2 exposure, and infected in the same time-period., SCOPUS: ar.j, info:eu-repo/semantics/published

Published

2023

10. An ultra-fast mechanically active cell culture substrate

Author

Poulin, Alexandre, Imboden, Matthias, Sorba, Francesca, Grazioli, Serge, Martin-Olmos, Cristina, Rosset, Samuel, and Shea, Herbert

Published

2018

11. Multicenter Randomized Trial of Methylprednisolone vs. Intravenous Immunoglobulins to Treat the Pediatric Inflammatory Multisystem Syndrome—Temporally Associated With SARS-CoV-2 (PIMS-TS): Protocol of the Swissped RECOVERY Trial

Author

Welzel, Tatjana, Schöbi, Nina, André, Maya C., Bailey, Douggl G. N., Blanchard-Rohner, Geraldine, Buettcher, Michael, Grazioli, Serge, Koehler, Henrik, Perez, Marie-Helene, Trück, Johannes, Vanoni, Federica, Zimmermann, Petra, Atkinson, Andrew, Sanchez, Carlos, Whittaker, Elizabeth, Faust, Saul N., Bielicki, Julia A., and Schlapbach, Luregn J.

Subjects

hemic and lymphatic diseases, Pediatrics, Perinatology and Child Health, 610 Medicine & health

Abstract

IntroductionIn 2020, a new disease entitled Pediatric Inflammatory Multisystem Syndrome temporally associated with COVID-19 (PIMS-TS), or Multisystem Inflammatory Syndrome in Children (MIS-C), emerged, with thousands of children affected globally. There is no available evidence based on randomized controlled trials (RCT) to date on the two most commonly used immunomodulatory treatments, intravenous immunoglobulins (IVIG) and corticosteroids. Therefore, the Swissped RECOVERY trial was conducted to assess whether intravenous (IV) methylprednisolone shortens hospital length of stay compared with IVIG.Methods and AnalysisSwissped RECOVERY is an ongoing investigator-initiated, open-label, multicenter two-arm RCT in children and adolescents SignificanceCurrently, robust trial evidence for the treatment of PIMS-TS is lacking, with a controversy surrounding the use of corticosteroids vs. IVIG. This trial will provide evidence for the effectiveness and safety of these two treatments.Ethics and DisseminationThe study protocol, which was designed based on the U.K. RECOVERY trial, the patient information and consent forms, and other study-specific study documents were approved by the local ethics committees (Project ID: 2021-00362).Registration DetailsThe study is registered on the Swiss National Clinical Trials Portal (SNCTP000004720) and Clinicaltrials.gov (NCT 04826588).

Published

2022

12. The SARS-CoV-2 Pandemic Impacts the Management of Swiss Pediatric Intensive Care Units

Author

Soomann, Maarja, Wendel-Garcia, Pedro D, Kaufmann, Mark, Grazioli, Serge, Perez, Marie-Helene, Hilty, Matthias P, André, Maya C, Brotschi, Barbara, Soomann, Maarja, Wendel-Garcia, Pedro D, Kaufmann, Mark, Grazioli, Serge, Perez, Marie-Helene, Hilty, Matthias P, André, Maya C, and Brotschi, Barbara

Abstract

The impact of the severe acute respiratory syndrome coronavirus-2 (SARS-CoV-2) pandemic on pediatric intensive care units (PICUs) is difficult to quantify. We conducted an observational study in all eight Swiss PICUs between 02/24/2020 and 06/15/2020 to characterize the logistical and medical aspects of the pandemic and their impact on the management of the Swiss PICUs. The nine patients admitted to Swiss PICUs during the study period suffering from pediatric inflammatory multisystem syndrome temporally associated with SARS-CoV-2 (PIMS-TS) and constituting 14% (9/63) of all SARS-CoV-2 positive hospitalized patients in Swiss children's hospitals caused a higher workload [total Nine Equivalents of nursing Manpower use Score (NEMS) points, p = 0.0008] and were classified to higher workload categories (p < 0.0001) than regular PICU patients (n = 4,881) admitted in 2019. The comparison of the characteristics of the eight Swiss PICUs shows that they were confronted by different organizational issues arising from temporary regulations put in place by the federal council. These general regulations had different consequences for the eight individual PICUs due to the differences between the PICUs. In addition, the temporal relationship of these different regulations influenced the available PICU resources, dependent on the characteristics of the individual PICUs. As pandemic continues, reflecting and learning from experience is essential to reduce workload, optimize bed occupancy and manage resources in each individual PICU. In a small country as Switzerland, with a relatively decentralized health care local differences between PICUs are considerable and should be taken into account when making policy decisions.

Published

2022

13. Commentary: “PCRRT Expert Committee ICONIC Position Paper on Prescribing Kidney Replacement Therapy in Critically Sick Children With Acute Liver Failure”

Author

Deep, Akash, primary, Alexander, Emma C., additional, Ricci, Zaccaria, additional, Grazioli, Serge, additional, Ronco, Claudio, additional, Goldstein, Stuart, additional, and Akcan-Arikan, Ayse, additional

Published

2022

14. The SARS-CoV-2 Pandemic Impacts the Management of Swiss Pediatric Intensive Care Units

Author

Soomann, Maarja, primary, Wendel-Garcia, Pedro D., additional, Kaufmann, Mark, additional, Grazioli, Serge, additional, Perez, Marie-Helene, additional, Hilty, Matthias P., additional, André, Maya C., additional, and Brotschi, Barbara, additional

Published

2022

15. Immunological assessment of pediatric multisystem inflammatory syndrome related to COVID-19

Author

Grazioli, Serge, Tavaglione, Fedora, Torriani, Giulia, Wagner, Noemie, Rohr, Marie, L’Huillier, Arnaud G, Leclercq, Charlotte, Perrin, Anne, Bordessoule, Alice, Beghetti, Maurice, Pachlopnik Schmid, Jana, Vavassori, Stefano, Perreau, Matthieu, Eberhardt, Christiane, Didierlaurent, Arnaud, Kaiser, Laurent, Eckerle, Isabella, Roux-Lombard, Pascale, Blanchard-Rohner, Geraldine, University of Zurich, and Blanchard-Rohner, Geraldine

Subjects

ddc:616, ddc:618, SARS-CoV-2, COVID-19, 610 Medicine & health, 2700 General Medicine, General Medicine, Antibodies, Neutralizing, Pediatrics, Perinatology, Systemic Inflammatory Response Syndrome, immunological and virological workup, and Child Health, AcademicSubjects/MED00290, Infectious Diseases, 10036 Medical Clinic, Humans, Original Article, AcademicSubjects/MED00670, Child, multisystem inflammatory syndrome in children

Abstract

Recently, cases of multisystem inflammatory syndrome in children (MIS-C) associated with coronavirus disease 2019 (COVID-19) have been reported worldwide. Negative polymerase chain reaction (RT-PCR) testing associated with positive serology in most of the cases suggests a postinfectious syndrome. Because the pathophysiology of this syndrome is still poorly understood, extensive virological and immunological investigations are needed.We report a series of 4 pediatric patients admitted to Geneva University Hospitals with persistent fever and laboratory evidence of inflammation meeting the published definition of MIS-C related to COVID-19, to whom an extensive virological and immunological workup was performed.RT-PCRs on multiple anatomical compartments were negative, whereas anti-severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) immunoglobulin A (IgA) and immunoglobulin G (IgG) were strongly positive by enzyme-linked immunosorbent assay and immunofluorescence. Both pseudoneutralization and full virus neutralization assays showed the presence of neutralizing antibodies in all children, confirming a recent infection with SARS-CoV-2. The analyses of cytokine profiles revealed an elevation in all cytokines, as reported in adults with severe COVID-19. Although differing in clinical presentation, some features of MIS-C show phenotypic overlap with hemophagocytic lymphohistiocytosis (HLH). In contrast to patients with primary HLH, our patients showed normal perforin expression and natural killer (NK) cell degranulation. The levels of soluble interleukin (IL)-2 receptor (sIL-2R) correlated with the severity of disease, reflecting recent T-cell activation.Our findings suggest that MIS-C related to COVID-19 is caused by a postinfectious inflammatory syndrome associated with an elevation in all cytokines, and markers of recent T-cell activation (sIL-2R) occurring despite a strong and specific humoral response to SARS-CoV-2. Further functional and genetic analyses are essential to better understand the mechanisms of host-pathogen interactions.

Published

2021

16. Machine learning using the extreme gradient boosting (XGBoost) algorithm predicts 5-day delta of SOFA score at ICU admission in COVID-19 patients

Author

Montomoli, Jonathan, primary, Romeo, Luca, additional, Moccia, Sara, additional, Bernardini, Michele, additional, Migliorelli, Lucia, additional, Berardini, Daniele, additional, Donati, Abele, additional, Carsetti, Andrea, additional, Bocci, Maria Grazia, additional, Wendel Garcia, Pedro David, additional, Fumeaux, Thierry, additional, Guerci, Philippe, additional, Schüpbach, Reto Andreas, additional, Ince, Can, additional, Frontoni, Emanuele, additional, Hilty, Matthias Peter, additional, Alfaro-Farias, Mario, additional, Vizmanos-Lamotte, Gerardo, additional, Tschoellitsch, Thomas, additional, Meier, Jens, additional, Aguirre-Bermeo, Hernán, additional, Apolo, Janina, additional, Martínez, Alberto, additional, Jurkolow, Geoffrey, additional, Delahaye, Gauthier, additional, Novy, Emmanuel, additional, Losser, Marie-Reine, additional, Wengenmayer, Tobias, additional, Rilinger, Jonathan, additional, Staudacher, Dawid L., additional, David, Sascha, additional, Welte, Tobias, additional, Stahl, Klaus, additional, Pavlos”, “Agios, additional, Aslanidis, Theodoros, additional, Korsos, Anita, additional, Babik, Barna, additional, Nikandish, Reza, additional, Rezoagli, Emanuele, additional, Giacomini, Matteo, additional, Nova, Alice, additional, Fogagnolo, Alberto, additional, Spadaro, Savino, additional, Ceriani, Roberto, additional, Murrone, Martina, additional, Wu, Maddalena A., additional, Cogliati, Chiara, additional, Colombo, Riccardo, additional, Catena, Emanuele, additional, Turrini, Fabrizio, additional, Simonini, Maria Sole, additional, Fabbri, Silvia, additional, Potalivo, Antonella, additional, Facondini, Francesca, additional, Gangitano, Gianfilippo, additional, Perin, Tiziana, additional, Grazia Bocci, Maria, additional, Antonelli, Massimo, additional, Gommers, Diederik, additional, Rodríguez-García, Raquel, additional, Gámez-Zapata, Jorge, additional, Taboada-Fraga, Xiana, additional, Castro, Pedro, additional, Tellez, Adrian, additional, Lander-Azcona, Arantxa, additional, Escós-Orta, Jesús, additional, Martín-Delgado, Maria C., additional, Algaba-Calderon, Angela, additional, Franch-Llasat, Diego, additional, Roche-Campo, Ferran, additional, Lozano-Gómez, Herminia, additional, Zalba-Etayo, Begoña, additional, Michot, Marc P., additional, Klarer, Alexander, additional, Ensner, Rolf, additional, Schott, Peter, additional, Urech, Severin, additional, Zellweger, Nuria, additional, Merki, Lukas, additional, Lambert, Adriana, additional, Laube, Marcus, additional, Jeitziner, Marie M., additional, Jenni-Moser, Beatrice, additional, Wiegand, Jan, additional, Yuen, Bernd, additional, Lienhardt-Nobbe, Barbara, additional, Westphalen, Andrea, additional, Salomon, Petra, additional, Drvaric, Iris, additional, Hillgaertner, Frank, additional, Sieber, Marianne, additional, Dullenkopf, Alexander, additional, Petersen, Lina, additional, Chau, Ivan, additional, Ksouri, Hatem, additional, Sridharan, Govind Oliver, additional, Cereghetti, Sara, additional, Boroli, Filippo, additional, Pugin, Jerome, additional, Grazioli, Serge, additional, Rimensberger, Peter C., additional, Bürkle, Christian, additional, Marrel, Julien, additional, Brenni, Mirko, additional, Fleisch, Isabelle, additional, Lavanchy, Jerome, additional, Perez, Marie-Helene, additional, Ramelet, Anne-Sylvie, additional, Weber, Anja Baltussen, additional, Gerecke, Peter, additional, Christ, Andreas, additional, Ceruti, Samuele, additional, Glotta, Andrea, additional, Marquardt, Katharina, additional, Shaikh, Karim, additional, Hübner, Tobias, additional, Neff, Thomas, additional, Redecker, Hermann, additional, Moret-Bochatay, Mallory, additional, Bentrup, FriederikeMeyer zu, additional, Studhalter, Michael, additional, Stephan, Michael, additional, Brem, Jan, additional, Gehring, Nadine, additional, Selz, Daniela, additional, Naon, Didier, additional, Kleger, Gian-Reto, additional, Pietsch, Urs, additional, Filipovic, Miodrag, additional, Ristic, Anette, additional, Sepulcri, Michael, additional, Heise, Antje, additional, Franchitti Laurent, Marilene, additional, Laurent, Jean-Christophe, additional, Wendel Garcia, Pedro D., additional, Schuepbach, Reto, additional, Heuberger, Dorothea, additional, Bühler, Philipp, additional, Brugger, Silvio, additional, Fodor, Patricia, additional, Locher, Pascal, additional, Camen, Giovanni, additional, Gaspert, Tomislav, additional, Jovic, Marija, additional, Haberthuer, Christoph, additional, Lussman, Roger F., additional, and Colak, Elif, additional

Published

2021

17. X-Linked Lymphoproliferative Disease Mimicking Multisystem Inflammatory Syndrome in Children—A Case Report

Author

Prader, Seraina, primary, Ritz, Nicole, additional, Baleydier, Frédéric, additional, Andre, Maya C., additional, Stähli, Noémie, additional, Schmid, Kevin, additional, Schmid, Hanna, additional, Woerner, Andreas, additional, Diesch, Tamara, additional, Meyer Sauteur, Patrick M., additional, Trück, Johannes, additional, Gebistorf, Fabienne, additional, Opitz, Lennart, additional, Killian, Michael P., additional, Marchetti, Tommaso, additional, Vavassori, Stefano, additional, Blanchard-Rohner, Géraldine, additional, Mc Lin, Valerie, additional, Grazioli, Serge, additional, and Pachlopnik Schmid, Jana, additional

Published

2021

18. Additional file 1 of Implications of early respiratory support strategies on disease progression in critical COVID-19: a matched subanalysis of the prospective RISC-19-ICU cohort

Author

Garcia, Pedro D. Wendel, Aguirre-Bermeo, Hernán, Buehler, Philipp K., Alfaro-Farias, Mario, Yuen, Bernd, David, Sascha, Tschoellitsch, Thomas, Wengenmayer, Tobias, Korsos, Anita, Fogagnolo, Alberto, Gian-Reto Kleger, Wu, Maddalena A., Colombo, Riccardo, Turrini, Fabrizio, Potalivo, Antonella, Rezoagli, Emanuele, Rodríguez-García, Raquel, Castro, Pedro, Lander-Azcona, Arantxa, Martín-Delgado, Maria C., Lozano-Gómez, Herminia, Ensner, Rolf, Michot, Marc P., Gehring, Nadine, Schott, Peter, Siegemund, Martin, Merki, Lukas, Wiegand, Jan, Jeitziner, Marie M., Laube, Marcus, Salomon, Petra, Hillgaertner, Frank, Dullenkopf, Alexander, Ksouri, Hatem, Cereghetti, Sara, Grazioli, Serge, Bürkle, Christian, Marrel, Julien, Fleisch, Isabelle, Marie-Helene Perez, Weber, Anja Baltussen, Ceruti, Samuele, Marquardt, Katharina, Hübner, Tobias, Redecker, Hermann, Studhalter, Michael, Stephan, Michael, Selz, Daniela, Pietsch, Urs, Ristic, Anette, Heise, Antje, Bentrup, Friederike Meyer Zu, Laurent, Marilene Franchitti, Fodor, Patricia, Gaspert, Tomislav, Haberthuer, Christoph, Colak, Elif, Heuberger, Dorothea M., Fumeaux, Thierry, Montomoli, Jonathan, Guerci, Philippe, Schuepbach, Reto A., Hilty, Matthias P., and Roche-Campo, Ferran

Abstract

Additional file 1. e-Appendix 1: Specifications on the RISC-19-ICU registry structure and data collection. e-Appendix 2: Missing data handling. e-Table 1: Overall “unmatched” baseline characteristics on Day 0. e-Figure 1: “Love Plot” presenting Standardized Mean Differences between the unmatched and matchedcohort. e-Table 2: Demographics, characteristics at ICU admission, progression of respiratory support and outcome; stratified by survivor status. e-Table 3: Progression of respiratory support stratified by respiratory support strategy at ICU admission. e-Figure 2: Temporal relationship between the period of admission to the intensive care unit and the use of respiratory support strategies or mortality rate. e-Figure 3: Kaplan Meier curves for intensive care unit mortality stratified by the period of admission to the intensive care unit. e-Table 4: Demographics, characteristics at ICU admission, progression of respiratory support and outcome for patients never requiring intubation and invasive mechanical ventilation. e-Figure 4: C-Reactive Protein stratified by respiratory support strategy on Day 0 over the first week of ICU stay. e-Table 5: Mixed Effect Model of C-Reactive Protein stratified by respiratory support strategy on Day 0 over the first week of ICU stay. e-Figure 5: Multivariable adjusted COX regression model for the incidence of intubation. e-Figure 6: Multivariable adjusted COX regression model for overall ICU mortality. e-Figure 7: Multivariable adjusted COX regression model for ICU mortality (intubated patients only). e-Figure 8: Multivariable adjusted COX regression model for ICU discharge (intubated patients only). e-Table 6: Prognostic Model for the identification of patients with lower ICU mortality risk after a failed HFNC or NIV trial. e-Figure 9: Nomogram, Receiver Operating Curves and stratified Kaplan Meier curve for a prognostic model identifying patients with lower ICU mortality risk after a failed HFNC or NIV trial. e-Table 7: Area Under the Receiver Operating Curves (AUROCs) for the Prognostic Score versus classic severity scores.

Published

2021

19. X-Linked Lymphoproliferative Disease Mimicking Multisystem Inflammatory Syndrome in Children—A Case Report

Author

Prader, Seraina, Ritz, Nicole, Baleydier, Frédéric, Andre, Maya C, Stähli, Noémie, Schmid, Kevin, Schmid, Hanna, Woerner, Andreas, Diesch, Tamara, Meyer Sauteur, Patrick M, Trück, Johannes; https://orcid.org/0000-0002-0418-7381, Gebistorf, Fabienne, Opitz, Lennart, Killian, Michael P, Marchetti, Tommaso, Vavassori, Stefano, Blanchard-Rohner, Géraldine, Mc Lin, Valerie, Grazioli, Serge, Pachlopnik Schmid, Jana; https://orcid.org/0000-0002-6653-9047, Prader, Seraina, Ritz, Nicole, Baleydier, Frédéric, Andre, Maya C, Stähli, Noémie, Schmid, Kevin, Schmid, Hanna, Woerner, Andreas, Diesch, Tamara, Meyer Sauteur, Patrick M, Trück, Johannes; https://orcid.org/0000-0002-0418-7381, Gebistorf, Fabienne, Opitz, Lennart, Killian, Michael P, Marchetti, Tommaso, Vavassori, Stefano, Blanchard-Rohner, Géraldine, Mc Lin, Valerie, Grazioli, Serge, and Pachlopnik Schmid, Jana; https://orcid.org/0000-0002-6653-9047

Abstract

Most children with a SARS-CoV-2 infection are asymptomatic or exhibit mild symptoms. However, a small number of children develop features of substantial inflammation temporarily related to the COVID-19 also called multisystem inflammatory syndrome in children (MIS-C) or pediatric inflammatory multisystem syndrome temporally associated with SARS-CoV-2 (PIMS-TS), clinically similar to Kawasaki disease, toxic shock syndrome and hemophagocytic lymphohistiocytosis (HLH). It is well-known that genetic pre-disposition plays an important role in virally-triggered diseases such as Epstein-Barr virus (EBV)-associated HLH, while this has not yet been established for patients with MIS-C. Here we describe a male patient fulfilling the diagnostic criteria of MIS-C, who was initially treated according to current consensus guidelines. Presence of hypofibrinogenemia, normal lymphocyte counts and C-reactive protein, but substantial hyperferritinemia distinguish this patient from others with MIS-C. The clinical course following initial presentation with acute respiratory distress syndrome was marked by fatal liver failure in the context of EBV-associated HLH despite treatment with steroids, intravenous immunoglobulins, interleukin (IL)-1 receptor blockade and eventually HLH-directed treatment. X-linked lymphoproliferative disease type 1 (XLP1), a subtype of primary HLH was diagnosed in this patient post-mortem. This case report highlights the importance of including HLH in the differential diagnosis in MIS-C with severe disease course to allow specific, risk-adapted treatment and genetic counseling.

Published

2021

20. Best Practice Recommendations for the Diagnosis and Management of Children With Pediatric Inflammatory Multisystem Syndrome Temporally Associated With SARS-CoV-2 (PIMS-TS; Multisystem Inflammatory Syndrome in Children, MIS-C) in Switzerland

Author

Schlapbach, Luregn J; https://orcid.org/0000-0003-2281-2598, Andre, Maya C, Grazioli, Serge; https://orcid.org/0000-0002-5526-851X, Schöbi, Nina, Ritz, Nicole; https://orcid.org/0000-0002-1498-1685, Aebi, Christoph; https://orcid.org/0000-0003-3554-7949, Agyeman, Philipp K A; https://orcid.org/0000-0002-8339-5444, Albisetti, Manuela, Bailey, Douggl G N, Berger, Christoph; https://orcid.org/0000-0002-1730-8824, Blanchard-Rohner, Geraldine; https://orcid.org/0000-0002-9974-2172, Bressieux-Degueldre, Sabrina, Hofer, Michael, L'Huillier, Arnaud G, Marston, Mark, Meyer Sauteur, Patrick M; https://orcid.org/0000-0002-4312-9803, Pachlopnik Schmid, Jana; https://orcid.org/0000-0002-6653-9047, Perez, Marie-Helene, Rogdo, Bjarte, Trück, Johannes; https://orcid.org/0000-0002-0418-7381, Woerner, Andreas, Wütz, Daniela; https://orcid.org/0000-0002-5186-2634, Zimmermann, Petra, Levin, Michael, Whittaker, Elizabeth, Rimensberger, Peter C, Schlapbach, Luregn J; https://orcid.org/0000-0003-2281-2598, Andre, Maya C, Grazioli, Serge; https://orcid.org/0000-0002-5526-851X, Schöbi, Nina, Ritz, Nicole; https://orcid.org/0000-0002-1498-1685, Aebi, Christoph; https://orcid.org/0000-0003-3554-7949, Agyeman, Philipp K A; https://orcid.org/0000-0002-8339-5444, Albisetti, Manuela, Bailey, Douggl G N, Berger, Christoph; https://orcid.org/0000-0002-1730-8824, Blanchard-Rohner, Geraldine; https://orcid.org/0000-0002-9974-2172, Bressieux-Degueldre, Sabrina, Hofer, Michael, L'Huillier, Arnaud G, Marston, Mark, Meyer Sauteur, Patrick M; https://orcid.org/0000-0002-4312-9803, Pachlopnik Schmid, Jana; https://orcid.org/0000-0002-6653-9047, Perez, Marie-Helene, Rogdo, Bjarte, Trück, Johannes; https://orcid.org/0000-0002-0418-7381, Woerner, Andreas, Wütz, Daniela; https://orcid.org/0000-0002-5186-2634, Zimmermann, Petra, Levin, Michael, Whittaker, Elizabeth, and Rimensberger, Peter C

Abstract

Background: Following the spread of the coronavirus disease 2019 (COVID-19) pandemic a new disease entity emerged, defined as Pediatric Inflammatory Multisystem Syndrome temporally associated with COVID-19 (PIMS-TS), or Multisystem Inflammatory Syndrome in Children (MIS-C). In the absence of trials, evidence for treatment remains scarce.Purpose: To develop best practice recommendations for the diagnosis and treatment of children with PIMS-TS in Switzerland. It is acknowledged that the field is changing rapidly, and regular revisions in the coming months are pre-planned as evidence is increasing.Methods: Consensus guidelines for best practice were established by a multidisciplinary group of Swiss pediatric clinicians with expertise in intensive care, immunology/rheumatology, infectious diseases, hematology, and cardiology. Subsequent to literature review, four working groups established draft recommendations which were subsequently adapted in a modified Delphi process. Recommendations had to reach >80% agreement for acceptance.Results: The group achieved agreement on 26 recommendations, which specify diagnostic approaches and interventions across anti-inflammatory, anti-infectious, and support therapies, and follow-up for children with suspected PIMS-TS. A management algorithm was derived to guide treatment depending on the phenotype of presentation, categorized into PIMS-TS with (a) shock, (b) Kawasaki-disease like, and (c) undifferentiated inflammatory presentation.Conclusion: Available literature on PIMS-TS is limited to retrospective or prospective observational studies. Informed by these cohort studies and indirect evidence from other inflammatory conditions in children and adults, as well as guidelines from international health authorities, the Swiss PIMS-TS recommendations represent best practice guidelines based on currently available knowledge to standardize treatment of children with suspected PIMS-TS. Given the absence of high-grade evidence, regular up

Published

2021

21. Case Report: Case Series of Children With Multisystem Inflammatory Syndrome Following SARS-CoV-2 Infection in Switzerland

Author

Fouriki, Athina, Fougère, Yves, De Camaret, Caroline, Blanchard Rohner, Géraldine, Grazioli, Serge, Wagner, Noémie, Relly, Christa, Pachlopnik Schmid, Jana; https://orcid.org/0000-0002-6653-9047, Trück, Johannes; https://orcid.org/0000-0002-0418-7381, Kottanatu, Lisa, Perez, Estefania, Perez, Marie-Helene, Schaffner, Damien, Asner, Sandra Andrea, Hofer, Michael, Fouriki, Athina, Fougère, Yves, De Camaret, Caroline, Blanchard Rohner, Géraldine, Grazioli, Serge, Wagner, Noémie, Relly, Christa, Pachlopnik Schmid, Jana; https://orcid.org/0000-0002-6653-9047, Trück, Johannes; https://orcid.org/0000-0002-0418-7381, Kottanatu, Lisa, Perez, Estefania, Perez, Marie-Helene, Schaffner, Damien, Asner, Sandra Andrea, and Hofer, Michael

Abstract

Since the beginning of the severe SARS-CoV-2 pandemic, an increasing number of countries reported cases of a systemic hyperinflammatory condition defined as multi-system inflammatory syndrome in children (MIS-C). The clinical features of MIS-C can be an overlap of Kawasaki Disease (KD), Toxic Shock Syndrome (TSS), Macrophage Activation Syndrome (MAS), or have often an acute abdominal presentation. Intravenous immunoglobulin (IVIG) is recommended as first line therapy in KD. Recent evidence suggests intravenous immunoglobulins (IVIG) resistance in some cases of SARS-CoV-2 related MIS-C, thereby questioning the benefit of immunomodulators such as IL-1 or IL-6 blocking agents. We report on a cohort of 6 Swiss children with SARS-CoV2 related MIS-C presenting with clinical features compatible with Incomplete KD and Toxic Shock Syndrome associated to a cytokine storm. Serum cytokine profile investigations showed increased IL1RA levels (8 to 22-fold) in 5 of the 6 patients (one patient had not been tested), whereas, IL-6 serum levels were increased only in the 3 patients of the 6 who were tested. With exception of one patient who had only benefited by Anakinra, all patients received at least one dose of IVIG. One patient has only received Anakinra with favorable evolution, and three patients had also a steroid treatment. In addition to all this anti-inflammatory medication two patients have also received one dose of anti-IL6. In conclusion, our case series reports on clinical and laboratory findings of most of Swiss cases with MIS-C and suggests the use of Anakinra as an alternative to steroids in these children, most of whom presented with high IL-1RA levels.

Published

2021

22. Comment on 'Beware of Too Aggressive Approach in Children With Acute Abdomen During COVID-19 Outbreak!'

Author

Calinescu, Ana M., Vidal, Isabelle, Grazioli, Serge, Lacroix, Laurence, and Wildhaber, Barbara E.

Subjects

Abdomen, Acute, Adult, Male, Infectious Disease Transmission, Patient-to-Professional, Clinical Laboratory Techniques, SARS-CoV-2, Clinical Decision-Making, Pneumonia, Viral, COVID-19, Middle Aged, Diagnosis, Differential, Betacoronavirus, COVID-19 Testing, Clinical Protocols, Humans, Female, Coronavirus Infections, Letter to the Editor, Pandemics, Personal Protective Equipment, Aged

Published

2020

23. Case Report: Case Series of Children With Multisystem Inflammatory Syndrome Following SARS-CoV-2 Infection in Switzerland

Author

Fouriki, Athina, primary, Fougère, Yves, additional, De Camaret, Caroline, additional, Blanchard Rohner, Géraldine, additional, Grazioli, Serge, additional, Wagner, Noémie, additional, Relly, Christa, additional, Pachlopnik Schmid, Jana, additional, Trück, Johannes, additional, Kottanatu, Lisa, additional, Perez, Estefania, additional, Perez, Marie-Helene, additional, Schaffner, Damien, additional, Asner, Sandra Andrea, additional, and Hofer, Michael, additional

Published

2021

24. Immunological Assessment of Pediatric Multisystem Inflammatory Syndrome Related to Coronavirus Disease 2019

Author

Grazioli, Serge, primary, Tavaglione, Fedora, additional, Torriani, Giulia, additional, Wagner, Noemie, additional, Rohr, Marie, additional, L’Huillier, Arnaud G, additional, Leclercq, Charlotte, additional, Perrin, Anne, additional, Bordessoule, Alice, additional, Beghetti, Maurice, additional, Schmid, Jana Pachlopnik, additional, Vavassori, Stefano, additional, Perreau, Matthieu, additional, Eberhardt, Christiane, additional, Didierlaurent, Arnaud, additional, Kaiser, Laurent, additional, Eckerle, Isabella, additional, Roux-Lombard, Pascale, additional, and Blanchard-Rohner, Geraldine, additional

Published

2020

25. Alveolar CCN1 is associated with mechanical stretch and acute respiratory distress syndrome severity

Author

Morrell, Eric D., primary, Grazioli, Serge, additional, Hung, Chi, additional, Kajikawa, Osamu, additional, Kosamo, Susanna, additional, Stapleton, Renee D., additional, Gharib, Sina A., additional, Amado-Rodríguez, Laura, additional, Albaiceta, Guillermo, additional, Wurfel, Mark M., additional, and Matute-Bello, Gustavo, additional

Published

2020

26. Prognostic factors associated with mortality risk and disease progression in 639 critically ill patients with COVID-19 in Europe: Initial report of the international RISC-19-ICU prospective observational cohort

Author

Wendel Garcia, Pedro David, primary, Fumeaux, Thierry, additional, Guerci, Philippe, additional, Heuberger, Dorothea Monika, additional, Montomoli, Jonathan, additional, Roche-Campo, Ferran, additional, Schuepbach, Reto Andreas, additional, Hilty, Matthias Peter, additional, Alfaro Farias, Mario, additional, Margarit, Antoni, additional, Vizmanos-Lamotte, Gerardo, additional, Tschoellitsch, Thomas, additional, Meier, Jens, additional, Cardona, Francesco S., additional, Skola, Josef, additional, Horakova, Lenka, additional, Aguirre-Bermeo, Hernan, additional, Apolo, Janina, additional, Novy, Emmanuel, additional, Losser, Marie-Reine, additional, Jurkolow, Geoffrey, additional, Delahaye, Gauthier, additional, David, Sascha, additional, Welte, Tobias, additional, Wengenmayer, Tobias, additional, Staudacher, Dawid L., additional, Aslanidis, Theodoros, additional, Babik, Barna, additional, Korsos, Anita, additional, Gal, Janos, additional, Csaba, Hermann, additional, Donati, Abele, additional, Carsetti, Andrea, additional, Turrini, Fabrizio, additional, Simonini, Maria Sole, additional, Ceriani, Roberto, additional, Murrone, Martina, additional, Rezoagli, Emanuele, additional, Vitale, Giovanni, additional, Fogagnolo, Alberto, additional, Spadaro, Savino, additional, Wu, Maddalena Alessandra, additional, Cogliati, Chiara, additional, Colombo, Riccardo, additional, Catena, Emanuele, additional, Facondini, Francesca, additional, Potalivo, Antonella, additional, Gangitano, Gianfilippo, additional, Perin, Tiziana, additional, Bocci, Maria Grazia, additional, Antonelli, Massimo, additional, Gommers, Diederik, additional, Ince, Can, additional, Mayor-Vázquez, Eric, additional, Cruz, Maria, additional, Delgado, Martin, additional, Garcia, Raquel Rodriguez, additional, Gamez Zapata, Jorge, additional, Zalba-Etayo, Begoña, additional, Lozano-Gomez, Herminia, additional, Castro, Pedro, additional, Tellez, Adrian, additional, Jacas, Adriana, additional, Muñoz, Guido, additional, Andrea, Rut, additional, Ortiz, Jose, additional, Quintana, Eduard, additional, Rovira, Irene, additional, Reverter, Enric, additional, Fernandez, Javier, additional, Ferrer, Miquel, additional, Badia, Joan R., additional, Lander Azcona, Arantxa, additional, Orta, Jesus Escos, additional, Bühler, Philipp, additional, Brugger, Silvio, additional, Hofmaenner, Daniel, additional, Unseld, Simone, additional, Ruschitzka, Frank, additional, Moret-Bochatay, Mallory, additional, Yuen, Bernd, additional, Hillermann, Thomas, additional, Ksouri, Hatem, additional, Sridharan, Govind Oliver, additional, Ristic, Anette, additional, Sepulcri, Michael, additional, Filipovic, Miodrag, additional, Pietsch, Urs, additional, Salomon, Petra, additional, Drvaric, Iris, additional, Schott, Peter, additional, Urech, Severin, additional, Lambert, Adriana, additional, Merki, Lukas, additional, Laube, Marcus, additional, Hillgaertner, Frank, additional, Sieber, Marianne, additional, Dullenkopf, Alexander, additional, Petersen, Lina, additional, Grazioli, Serge, additional, Rimensberger, Peter C., additional, Fleisch, Isabelle, additional, Lavanchy, Jerome, additional, Marquardt, Katharina, additional, Shaikh, Karim, additional, Redecker, Hermann, additional, Stephan, Michael, additional, Brem, Jan, additional, Rogdo, Bjarte, additional, Birkenmaier, Andre, additional, Meyer zu Bentrup, Friederike, additional, Fodor, Patricia, additional, Locher, Pascal, additional, Camen, Giovanni, additional, Siegemund, Martin, additional, Zellweger, Nuria, additional, Jeitziner, Marie-Madlen, additional, Jenni-Moser, Beatrice, additional, Bürkle, Christian, additional, Kleger, Gian-Reto, additional, Franchitti Laurent, Marilene, additional, Laurent, Jean-Christophe, additional, Gaspert, Tomislav, additional, Jovic, Marija, additional, Studhalter, Michael, additional, Haberthuer, Christoph, additional, Lussman, Roger F., additional, Selz, Daniela, additional, Naon, Didier, additional, Mauri, Romano, additional, Ceruti, Samuele, additional, Marrel, Julien, additional, Brenni, Mirko, additional, Ensner, Rolf, additional, Gehring, Nadine, additional, Heise, Antje, additional, Huebner, Tobias, additional, Neff, Thomas A., additional, Cereghetti, Sara, additional, Boroli, Filippo, additional, Pugin, Jerome, additional, Marczin, Nandor, additional, and Wong, Joyce, additional

Published

2020

27. Immunological Assessment of Pediatric Multisystem Inflammatory Syndrome Related to Coronavirus Disease 2019.

Author

Grazioli, Serge, Tavaglione, Fedora, Torriani, Giulia, Wagner, Noemie, Rohr, Marie, L'Huillier, Arnaud G, Leclercq, Charlotte, Perrin, Anne, Bordessoule, Alice, Beghetti, Maurice, Schmid, Jana Pachlopnik, Vavassori, Stefano, Perreau, Matthieu, Eberhardt, Christiane, Didierlaurent, Arnaud, Kaiser, Laurent, Eckerle, Isabella, Roux-Lombard, Pascale, and Blanchard-Rohner, Geraldine

Subjects

*REVERSE transcriptase polymerase chain reaction, *CYTOKINES, *INTERLEUKINS, *COVID-19, *IMMUNOGLOBULINS, *MULTIPLE organ failure, *IMMUNE system, *KILLER cells, *GENE expression, *ENZYME-linked immunosorbent assay, *FLUORESCENT antibody technique, *POLYMERASE chain reaction, *VIROLOGY, *CHILDREN

Abstract

Background Recently, cases of multisystem inflammatory syndrome in children (MIS-C) associated with coronavirus disease 2019 (COVID-19) have been reported worldwide. Negative polymerase chain reaction (RT-PCR) testing associated with positive serology in most of the cases suggests a postinfectious syndrome. Because the pathophysiology of this syndrome is still poorly understood, extensive virological and immunological investigations are needed. Methods We report a series of 4 pediatric patients admitted to Geneva University Hospitals with persistent fever and laboratory evidence of inflammation meeting the published definition of MIS-C related to COVID-19, to whom an extensive virological and immunological workup was performed. Results RT-PCRs on multiple anatomical compartments were negative, whereas anti-severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) immunoglobulin A (IgA) and immunoglobulin G (IgG) were strongly positive by enzyme-linked immunosorbent assay and immunofluorescence. Both pseudoneutralization and full virus neutralization assays showed the presence of neutralizing antibodies in all children, confirming a recent infection with SARS-CoV-2. The analyses of cytokine profiles revealed an elevation in all cytokines, as reported in adults with severe COVID-19. Although differing in clinical presentation, some features of MIS-C show phenotypic overlap with hemophagocytic lymphohistiocytosis (HLH). In contrast to patients with primary HLH, our patients showed normal perforin expression and natural killer (NK) cell degranulation. The levels of soluble interleukin (IL)-2 receptor (sIL-2R) correlated with the severity of disease, reflecting recent T-cell activation. Conclusion Our findings suggest that MIS-C related to COVID-19 is caused by a postinfectious inflammatory syndrome associated with an elevation in all cytokines, and markers of recent T-cell activation (sIL-2R) occurring despite a strong and specific humoral response to SARS-CoV-2. Further functional and genetic analyses are essential to better understand the mechanisms of host–pathogen interactions. [ABSTRACT FROM AUTHOR]

Published

2021

28. Mitochondrial alarmins are tissue mediators of ventilator-induced lung injury and ARDS

Author

Grazioli, Serge, primary, Dunn-Siegrist, Irène, additional, Pauchard, Laure-Anne, additional, Blot, Mathieu, additional, Charles, Pierre-Emmanuel, additional, and Pugin, Jérôme, additional

Published

2019

29. Antenatal and postnatal ultrasound in the evaluation of the risk of vesicoureteral reflux

Author

Grazioli, Serge, Parvex, Paloma, Merlini, Laura, Combescure, Christophe, Girardin, Eric, Grazioli, Serge, Parvex, Paloma, Merlini, Laura, Combescure, Christophe, and Girardin, Eric

Abstract

Antenatal hydronephrosis (ANH) is a frequent anomaly detected on fetal ultrasound scans. There is no consensus recommendation for the postnatal follow-up and/or the necessity to perform a voiding cystourethrography (VCUG) to diagnose vesicoureteral reflux (VUR). We conducted a cohort/non-randomized trial of 121 patients with ANH, defined as an anterior posterior diameter (APD) ≥5mm after the 20th week of gestation, to evaluate the ability of the antenatal and postnatal ultrasonography results to predict VUR. All infants had two successive ultrasounds at 5days and 1month, respectively, after birth. A VCUG was performed at 6weeks in children with a persistent APD ≥5mm and/or an ureteral dilatation observed on at least one of two postnatal ultrasounds. In total, 88 patients had VCUG and nine had VUR, with five having high-grade reflux (>grade II). The risk of VUR increased significantly with the degree of APD detected on the postnatal ultrasound scan (p = 0.03). The odds ratios were 5.0 [95% confidence interval (CI) 0.5-51.2] for APD = 7-9mm and 9.1 (95% CI 1.0-80.9) for APD ≥10mm. The results of this study show that among our patient cohort antenatal ultrasound was not predictive of reflux. There was, however, a relation between the importance of the postnatal renal pelvis diameter and the risk of VUR. A cut-off of 7mm showed a fair ability of ultrasonography to predict VUR and a cut-off of 10mm enabled all severe refluxes in the 88 patients who had a VCUG to be diagnosed

Published

2018

30. Mitochondrial Damage-Associated Molecular Patterns: From Inflammatory Signaling to Human Diseases

Author

Grazioli, Serge, primary and Pugin, Jérôme, additional

Published

2018

31. Rôle de l'ultrason anténatal et postnatal dans l'évaluation du risque de reflux vésico-urétéral

Author

Grazioli, Serge and Girardin, Eric

Subjects

Reflux vésico-urétéral, ddc:618, Ultrason, Hydronéphrose

Abstract

L'hydronéphrose anténatale se définit par une dilatation du système pyélocaliciel rénal et représente une des anomalies les plus fréquentes découverte à l'ultrason anténatal. Bien que les formes mineures soient la plupart du temps physiologiques et transitoires, la présence d'une dilatation du système pyélocaliciel peut néanmoins être associée à une uropathie obstructive ou à un reflux vésico-urétéral. L'importance de la dilatation se quantifie par la mesure en cm du diamètre antéro-postérieure (AP) de celle-ci. A l'heure actuelle, il n'existe aucun consensus dans la littérature concernant le diamètre AP à partir duquel il est indiqué d'effectuer un suivi postnatal et un dépistage systématique à la recherche d'un reflux vésico-urétéral lors de la découverte d'une hydronéphrose anténatale de forme mineure (diamètre antéro-postérieur du bassinet < 10mm). Cette situation engendre pour le nourrisson un nombre important d'examens invasifs et irradiants inutiles associés à un stress parental considérable. Le but de cette étude est d'évaluer de manière prospective l'habileté de l'échographie anténatale et postnatale à sélectionner les enfants à risque de présenter un reflux vésico-urétéral en fonction du diamètre AP à l'ultrason. Notre recherche a permis de démontrer que le risque de présenter un reflux vésico-urétéral était mieux corrélé avec le résultat des ultrasons postnataux que ceux des US anténataux et que ce risque augmente de manière significative en fonction du degré de dilatation pyélocalicielle présent sur l'ultrason postnatal. Ces données confirment l'utilité de l'ultrason postnatal comme examen de dépistage du reflux vésico-urétéral pour les enfants ayant présenté une hydronéphrose anténatale de forme mineure.

Published

2011

32. Reply to Dr. Weiskirchen

Author

Grazioli, Serge, primary and Matute-Bello, Gustavo, additional

Published

2015

33. CYR61 (CCN1) overexpression induces lung injury in mice

Author

Grazioli, Serge, primary, Gil, Sucheol, additional, An, Dowon, additional, Kajikawa, Osamu, additional, Farnand, Alex W., additional, Hanson, Josiah F., additional, Birkland, Timothy, additional, Chen, Peter, additional, Duffield, Jeremy, additional, Schnapp, Lynn M., additional, Altemeier, William A., additional, and Matute-Bello, Gustavo, additional

Published

2015

34. Continuous Kidney Replacement Therapy Practices in Pediatric Intensive Care Units Across Europe.

Author

Daverio, Marco, Cortina, Gerard, Jones, Andrew, Ricci, Zaccaria, Demirkol, Demet, Raymakers-Janssen, Paulien, Lion, Francois, Camilo, Cristina, Stojanovic, Vesna, Grazioli, Serge, Zaoral, Tomas, Masjosthusmann, Katja, Vankessel, Inge, and Deep, Akash

Published

2022

35. New Generation Neonatal High Frequency Ventilators: Effect of Oscillatory Frequency and Working Principles on Performance.

Author

Grazioli, Serge, Karam, Oliver, and Rimensberger, Peter C.

Subjects

COMMERCIAL product evaluation, COMPARATIVE studies, NEONATAL intensive care, STATISTICS, MECHANICAL ventilators, DATA analysis, IN vitro studies

Abstract

BACKGROUND: Several new generation neonatal ventilators that incorporate conventional as well as high frequency ventilation (HFOV) have appeared on the market. Most of them offer the possibility to use HFOV in a volume-targeted mode, despite absence of any preclinical data. With a bench test, we evaluated the performances of 4 new neonatal HFOV devices and compared them to the SensorMedics HFOV device. METHODS: Expiratory tidal volumes (VT) were measured for various ventilator settings and lung characteristics (ie, modifications of compliance and resistance of the system), to mimic several clinical conditions of pre-term and term infants. RESULTS: Increasing the frequency proportionally decreased the VT for all the ventilators, although the magnitude of the decrease was highly variable between ventilators. At 15 Hz and a pressure amplitude of 60 cm H2O, the delivered VT ranged from 3.5 to 5.9 mL between devices while simulating pre-term infant conditions and from 2.6 to 6.3 mL while simulating term infant conditions. Activating the volume-targeted mode in the 3 machines that offer this mode allowed the VT to remain constant over the range of frequencies and with changes of lung mechanical properties, for pre-term infant settings only while targeting a VT of 1 mL. CONCLUSIONS: These new generation neonatal ventilators were able to deliver adequate VT under pre-term infant, but not term infant respiratory system conditions. The clinical relevance of these findings will need to be determined by further studies. [ABSTRACT FROM AUTHOR]

Published

2015

36. Antenatal and postnatal ultrasound in the evaluation of the risk of vesicoureteral reflux

Author

Grazioli, Serge, Parvex, Paloma, Merlini, Laura, Combescure, Christophe, Girardin, Eric, Grazioli, Serge, Parvex, Paloma, Merlini, Laura, Combescure, Christophe, and Girardin, Eric

Abstract

Antenatal hydronephrosis (ANH) is a frequent anomaly detected on fetal ultrasound scans. There is no consensus recommendation for the postnatal follow-up and/or the necessity to perform a voiding cystourethrography (VCUG) to diagnose vesicoureteral reflux (VUR). We conducted a cohort/non-randomized trial of 121 patients with ANH, defined as an anterior posterior diameter (APD) ≥5mm after the 20th week of gestation, to evaluate the ability of the antenatal and postnatal ultrasonography results to predict VUR. All infants had two successive ultrasounds at 5days and 1month, respectively, after birth. A VCUG was performed at 6weeks in children with a persistent APD ≥5mm and/or an ureteral dilatation observed on at least one of two postnatal ultrasounds. In total, 88 patients had VCUG and nine had VUR, with five having high-grade reflux (>grade II). The risk of VUR increased significantly with the degree of APD detected on the postnatal ultrasound scan (p = 0.03). The odds ratios were 5.0 [95% confidence interval (CI) 0.5-51.2] for APD = 7-9mm and 9.1 (95% CI 1.0-80.9) for APD ≥10mm. The results of this study show that among our patient cohort antenatal ultrasound was not predictive of reflux. There was, however, a relation between the importance of the postnatal renal pelvis diameter and the risk of VUR. A cut-off of 7mm showed a fair ability of ultrasonography to predict VUR and a cut-off of 10mm enabled all severe refluxes in the 88 patients who had a VCUG to be diagnosed

37. Effects of ABO Matching of Platelet Transfusions in Critically Ill Children

Author

Jhuma Sankar, Anil Sapru, Laura Watkins, Jon Lillie, Anna Camporesi, Ofer Schiller, Andrew Meyer, Oliver Karam, ELENA CAVAZZONI, Fabrizio Chiusolo, Antonio Perez Ferrer, James Killinger, Kenneth Remy, Jesus Lopez-Herce, Mara L Leimanis Laurens, Edward Vincent S. Faustino, Kevin Kuo, Hari Krishnan Kanthimathinathan, Srinivas Murthy, Mark Peters, Arun Saini, Shubhi Kaushik, Andy Wen, Angela Aramburo, Critical care, Anesthesiology, Peri-operative and Emergency medicine (CAPE), Grazioli, Serge, and Pediatric Surgery

Subjects

Male, medicine.medical_treatment, Critical Care and Intensive Care Medicine, Platelet Count/statistics & numerical data, Primary outcome, Interquartile range, hemic and lymphatic diseases, and the P3T Investigators, Platelet, Prospective Studies, Prospective cohort study, Child, Pediatric, ddc:618, Hematology, Platelet Transfusion/adverse effects/methods, Intensive Care Units, Blood Grouping and Crossmatching/methods, Blood, Child, Preschool, Female, medicine.medical_specialty, congenital, hereditary, and neonatal diseases and abnormalities, Adolescent, pediatrics, Pediatric Critical Care Blood Research Network (BloodNet), Critical Illness, Platelet Transfusion, Nursing, Intensive Care Units, Pediatric, Paediatrics and Reproductive Medicine, Clinical Research, ABO blood group system, Internal medicine, parasitic diseases, medicine, Humans, Pediatric/statistics & numerical data, Preschool, ABO compatibility, Mechanical ventilation, business.industry, Critically ill, Platelet Count, Infant, Newborn, Infant, Transfusion Reaction, Newborn, Pediatric Acute Lung Injury and Sepsis Investigators (PALISI) Network, biological factors, Platelet transfusion, Blood Grouping and Crossmatching, P3T Investigators, Pediatrics, Perinatology and Child Health, Transfusion Reaction/epidemiology, sense organs, business

Abstract

OBJECTIVES: To determine if transfusing ABO compatible platelets has a greater effect on incremental change in platelet count as compared to ABO incompatible platelets in critically ill children.DESIGN: Secondary analysis of a prospective, observational study. Transfusions were classified as either ABO compatible, major incompatibility, or minor incompatibility. The primary outcome was the incremental change in platelet count. Transfusion reactions were analyzed as a secondary outcome.SETTING: Eighty-two PICUs in 16 countries.PATIENTS: Children (3 d to 16 yr old) were enrolled if they received a platelet transfusion during one of the predefined screening weeks.INTERVENTIONS: None.MEASUREMENTS AND MAIN RESULTS: Five-hundred three children were enrolled and had complete ABO information for both donor and recipient, as well as laboratory data. Three-hundred forty-two (68%) received ABO-identical platelets, 133 (26%) received platelets with major incompatibility, and 28 (6%) received platelets with minor incompatibility. Age, weight, proportion with mechanical ventilation or underlying oncologic diagnosis did not differ between the groups. After adjustment for transfusion dose, there was no difference in the incremental change in platelet count between the groups; the median (interquartile range) change for ABO-identical transfusions was 28 × 10 cells/L (8-68 × 10 cells/L), for transfusions with major incompatibility 26 × 10 cells/L (7-74 × 10 cells/L), and for transfusions with minor incompatibility 54 × 10 cells/L (14-81 × 10 cells/L) (p = 0.37). No differences in count increment between the groups were noted for bleeding (p = 0.92) and nonbleeding patients (p = 0.29). There were also no differences observed between the groups for any transfusion reaction (p = 0.07).CONCLUSIONS: No differences were seen in the incremental change in platelet count nor in transfusion reactions when comparing major ABO incompatible platelet transfusions with ABO compatible transfusions in a large study of critically ill children. Studies in larger, prospectively enrolled cohorts should be performed to validate whether ABO matching for platelet transfusions in critically ill children is necessary.

Published

2019

38. Prognostic factors associated with mortality risk and disease progression in 639 critically ill patients with COVID-19 in Europe: Initial report of the international RISC-19-ICU prospective observational cohort

Author

Pedro David Wendel Garcia, Thierry Fumeaux, Philippe Guerci, Dorothea Monika Heuberger, Jonathan Montomoli, Ferran Roche-Campo, Reto Andreas Schuepbach, Matthias Peter Hilty, Mario Alfaro Farias, Antoni Margarit, Gerardo Vizmanos-Lamotte, Thomas Tschoellitsch, Jens Meier, Francesco S. Cardona, Josef Skola, Lenka Horakova, Hernan Aguirre-Bermeo, Janina Apolo, Emmanuel Novy, Marie-Reine Losser, Geoffrey Jurkolow, Gauthier Delahaye, Sascha David, Tobias Welte, Tobias Wengenmayer, Dawid L. Staudacher, Theodoros Aslanidis, Barna Babik, Anita Korsos, Janos Gal, Hermann Csaba, Abele Donati, Andrea Carsetti, Fabrizio Turrini, Maria Sole Simonini, Roberto Ceriani, Martina Murrone, Emanuele Rezoagli, Giovanni Vitale, Alberto Fogagnolo, Savino Spadaro, Maddalena Alessandra Wu, Chiara Cogliati, Riccardo Colombo, Emanuele Catena, Francesca Facondini, Antonella Potalivo, Gianfilippo Gangitano, Tiziana Perin, Maria Grazia Bocci, Massimo Antonelli, Diederik Gommers, Can Ince, Eric Mayor-Vázquez, Maria Cruz, Martin Delgado, Raquel Rodriguez Garcia, Jorge Gamez Zapata, Begoña Zalba-Etayo, Herminia Lozano-Gomez, Pedro Castro, Adrian Tellez, Adriana Jacas, Guido Muñoz, Rut Andrea, Jose Ortiz, Eduard Quintana, Irene Rovira, Enric Reverter, Javier Fernandez, Miquel Ferrer, Joan R. Badia, Arantxa Lander Azcona, Jesus Escos Orta, Philipp Bühler, Silvio Brugger, Daniel Hofmaenner, Simone Unseld, Frank Ruschitzka, Mallory Moret-Bochatay, Bernd Yuen, Thomas Hillermann, Hatem Ksouri, Govind Oliver Sridharan, Anette Ristic, Michael Sepulcri, Miodrag Filipovic, Urs Pietsch, Petra Salomon, Iris Drvaric, Peter Schott, Severin Urech, Adriana Lambert, Lukas Merki, Marcus Laube, Frank Hillgaertner, Marianne Sieber, Alexander Dullenkopf, Lina Petersen, Serge Grazioli, Peter C. Rimensberger, Isabelle Fleisch, Jerome Lavanchy, Katharina Marquardt, Karim Shaikh, Hermann Redecker, Michael Stephan, Jan Brem, Bjarte Rogdo, Andre Birkenmaier, Friederike Meyer zu Bentrup, Patricia Fodor, Pascal Locher, Giovanni Camen, Martin Siegemund, Nuria Zellweger, Marie-Madlen Jeitziner, Beatrice Jenni-Moser, Christian Bürkle, Gian-Reto Kleger, Marilene Franchitti Laurent, Jean-Christophe Laurent, Tomislav Gaspert, Marija Jovic, Michael Studhalter, Christoph Haberthuer, Roger F. Lussman, Daniela Selz, Didier Naon, Romano Mauri, Samuele Ceruti, Julien Marrel, Mirko Brenni, Rolf Ensner, Nadine Gehring, Antje Heise, Tobias Huebner, Thomas A. Neff, Sara Cereghetti, Filippo Boroli, Jerome Pugin, Nandor Marczin, Joyce Wong, University of Zurich, Wendel Garcia, Pedro David, RISC-19 ICU investigators, Graduate School, Translational Physiology, ACS - Atherosclerosis & ischemic syndromes, ACS - Microcirculation, Intensive Care, Grazioli, Serge, and Rimensberger, Peter

Subjects

medicine.medical_specialty, ARDS, medicine.medical_treatment, 610 Medicine & health, Disease, 2700 General Medicine, 01 natural sciences, Article, NO, law.invention, 03 medical and health sciences, 0302 clinical medicine, law, Internal medicine, Medicine, 030212 general & internal medicine, 0101 mathematics, Disease burden, Mechanical ventilation, lcsh:R5-920, Public health, ddc:618, Acute respiratory distress syndrome, Pandemic, business.industry, Incidence (epidemiology), 010102 general mathematics, COVID-19, General Medicine, medicine.disease, Intensive care unit, Coronavirus, Cohort, Absolute neutrophil count, 10209 Clinic for Cardiology, 10023 Institute of Intensive Care Medicine, lcsh:Medicine (General), business

Abstract

Background Coronavirus disease 2019 (COVID-19) is associated with a high disease burden with 10% of confirmed cases progressing towards critical illness. Nevertheless, the disease course and predictors of mortality in critically ill patients are poorly understood. Methods Following the critical developments in ICUs in regions experiencing early inception of the pandemic, the European-based, international RIsk Stratification in COVID-19 patients in the Intensive Care Unit (RISC-19-ICU) registry was created to provide near real-time assessment of patients developing critical illness due to COVID-19. Findings As of April 22, 2020, 639 critically ill patients with confirmed SARS-CoV-2 infection were included in the RISC-19-ICU registry. Of these, 398 had deceased or been discharged from the ICU. ICU-mortality was 24%, median length of stay 12 (IQR, 5-21) days. ARDS was diagnosed in 74%, with a minimum P/F-ratio of 110 (IQR, 80-148). Prone positioning, ECCO2R, or ECMO were applied in 57%. Off-label therapies were prescribed in 265 (67%) patients, and 89% of all bloodstream infections were observed in this subgroup (n = 66; RR=3·2, 95% CI [1·7-6·0]). While PCT and IL-6 levels remained similar in ICU survivors and non-survivors throughout the ICU stay (p = 0·35, 0·34), CRP, creatinine, troponin, d-dimer, lactate, neutrophil count, P/F-ratio diverged within the first seven days (p

Published

2020

39. Cardiac assessment and inflammatory markers in children with paediatric inflammatory multisystem syndrome temporally associated with SARS-CoV2 (PIMS-TS) treated with methylprednisolone versus intravenous immunoglobulins: 6-month follow-up outcomes of the randomised controlled Swissped RECOVERY trial.

Author

Andre MC, Sanchez C, Bressieux-Degueldre S, Perez MH, Wütz D, Blanchard-Rohner G, Grazioli S, Schöbi N, Trück J, Welzel T, Atkinson A, Schlapbach LJ, and Bielicki J

Abstract

Background: Previous findings from the Swissped RECOVERY trial showed that patients with Pediatric Inflammatory Multisystem Syndrome-Temporally Associated with SARS-CoV-2 (PIMS-TS) who were randomly assigned to intravenous immunoglobulins or methylprednisolone have a comparable length of hospital stay. Here, we report the 6-month follow-up outcomes of cardiac pathologies and normalisation of clinical or laboratory signs of inflammation from this study population., Methods: This pre-planned follow-up of patients with PIMS-TS included the Swissped RECOVERY Trial reports on the 6-month outcomes of the cohort after randomisation, with a focus on cardiac, haematological, and biochemical findings. The trial was an investigator-initiated randomised multicentre open-label two-arm trial in children and adolescents hospitalised with PIMS-TS at ten hospitals in Switzerland. Cardiological assessments and laboratory analyses were prospectively collected in the intention-to-treat analysis on pre-defined intervals after hospital discharge. Differences between randomised arms were investigated using Chi-square test for categorical and Wilcoxon test for continuous variables. The trial is registered with the Swiss National Clinical Trials Portal (SNCTP000004720) and ClinicalTrials.gov (NCT04826588)., Findings: Between May 21, 2021 and April 15, 2022, 75 patients with a median age of 9.1 years (IQR 6.2-12.2) were included in the intention-to-treat population (37 in the methylprednisolone group and 38 in the intravenous immunoglobulin group). During follow-up, the incidence of abnormal left ventricular systolic function, coronary artery aneurysms (CAA), and other signs of inflammation were comparable in both groups. However, we detected cardiac abnormalities with low incidence and a mild degree grade of pathology. CAAs were observed in 2/38 children (5.3%) in the IVIG group and 1/37 children (2.7%) in the methylprednisolone group at 6-month follow-up (difference proportion 0.75; 95% confidence interval (CI) -0.05 to 1.0; p = 0.39)., Interpretation: Methylprednisolone alone may be an acceptable first-line treatment as left ventricular systolic dysfunction and clinical/laboratory evidence for inflammation quickly resolved in all children. However, our findings need further confirmation through larger studies as our sample size is likely to be of insufficient power to address rare clinically relevant adverse outcomes., Funding: NOMIS, Vontobel, and Gaydoul Foundation., Competing Interests: LJS was supported by grants from the NOMIS Foundation, the Vontobel Foundation, and the Gaydoul Foundation for this study. Swiss PedNet (https://www.swisspednet.ch/) provided infrastructure support for study coordination and monitoring. JB received grant support paid to the institution from the European and Developing Countries Clinical Trials Partnership (PediCaP, RIA2017MC-2023), Horizon 2020 (NeoIPC, grant 965328), the Swiss National Science Foundation (KIDS-STEP, grant 173532), National Institute for Health Research (CAP-IT, project 13/88/11), Innosuisse (SPEARHEAD flagship grant), the Swiss Personalised Health Network (Secretariat for Education Research and Innovation) (SwissPedHealth, award NDS-2021-911), in the past 36 months; consulting fees paid to the institution from Shionogi, Sandoz, Basilea, and GSK; payments to the institution for presentations, lectures, speakers bureaus, manuscript writing or educational events in the past 36 months from Pfizer, Sandoz, and Bayer; participated at independent data monitoring committee boards of Avenir trial (member, expenses), Lakana trial (member, unfunded), CURLY trial (Chair, unfunded) in the past 36 months; is the vice president of the SwissPedNet (unpaid) and leadership of Severe Bacterial Infection and Antimicrobial Resistance working group of the Penta Foundation (unpaid). TW gave presentations for Novartis (payment to the institution) in the past 36 months. All other authors declare no competing interests., (© 2023 The Author(s).)

Published

2023

40. Best Practice Recommendations for the Diagnosis and Management of Children With Pediatric Inflammatory Multisystem Syndrome Temporally Associated With SARS-CoV-2 (PIMS-TS; Multisystem Inflammatory Syndrome in Children, MIS-C) in Switzerland.

Author

Schlapbach LJ, Andre MC, Grazioli S, Schöbi N, Ritz N, Aebi C, Agyeman P, Albisetti M, Bailey DGN, Berger C, Blanchard-Rohner G, Bressieux-Degueldre S, Hofer M, L'Huillier AG, Marston M, Meyer Sauteur PM, Pachlopnik Schmid J, Perez MH, Rogdo B, Trück J, Woerner A, Wütz D, Zimmermann P, Levin M, Whittaker E, and Rimensberger PC

Abstract

Background: Following the spread of the coronavirus disease 2019 (COVID-19) pandemic a new disease entity emerged, defined as Pediatric Inflammatory Multisystem Syndrome temporally associated with COVID-19 (PIMS-TS), or Multisystem Inflammatory Syndrome in Children (MIS-C). In the absence of trials, evidence for treatment remains scarce. Purpose: To develop best practice recommendations for the diagnosis and treatment of children with PIMS-TS in Switzerland. It is acknowledged that the field is changing rapidly, and regular revisions in the coming months are pre-planned as evidence is increasing. Methods: Consensus guidelines for best practice were established by a multidisciplinary group of Swiss pediatric clinicians with expertise in intensive care, immunology/rheumatology, infectious diseases, hematology, and cardiology. Subsequent to literature review, four working groups established draft recommendations which were subsequently adapted in a modified Delphi process. Recommendations had to reach >80% agreement for acceptance. Results: The group achieved agreement on 26 recommendations, which specify diagnostic approaches and interventions across anti-inflammatory, anti-infectious, and support therapies, and follow-up for children with suspected PIMS-TS. A management algorithm was derived to guide treatment depending on the phenotype of presentation, categorized into PIMS-TS with (a) shock, (b) Kawasaki-disease like, and (c) undifferentiated inflammatory presentation. Conclusion: Available literature on PIMS-TS is limited to retrospective or prospective observational studies. Informed by these cohort studies and indirect evidence from other inflammatory conditions in children and adults, as well as guidelines from international health authorities, the Swiss PIMS-TS recommendations represent best practice guidelines based on currently available knowledge to standardize treatment of children with suspected PIMS-TS. Given the absence of high-grade evidence, regular updates of the recommendations will be warranted, and participation of patients in trials should be encouraged., Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2021 Schlapbach, Andre, Grazioli, Schöbi, Ritz, Aebi, Agyeman, Albisetti, Bailey, Berger, Blanchard-Rohner, Bressieux-Degueldre, Hofer, L'Huillier, Marston, Meyer Sauteur, Pachlopnik Schmid, Perez, Rogdo, Trück, Woerner, Wütz, Zimmermann, Levin, Whittaker, Rimensberger and the PIMS-TS working group of the Interest Group for Pediatric Neonatal Intensive Care (IGPNI) of the Swiss Society of Intensive Care and the Pediatric Infectious Diseases Group Switzerland (PIGS).)

Published

2021

41. Implications of early respiratory support strategies on disease progression in critical COVID-19: a matched subanalysis of the prospective RISC-19-ICU cohort.

Author

Wendel Garcia PD, Aguirre-Bermeo H, Buehler PK, Alfaro-Farias M, Yuen B, David S, Tschoellitsch T, Wengenmayer T, Korsos A, Fogagnolo A, Kleger GR, Wu MA, Colombo R, Turrini F, Potalivo A, Rezoagli E, Rodríguez-García R, Castro P, Lander-Azcona A, Martín-Delgado MC, Lozano-Gómez H, Ensner R, Michot MP, Gehring N, Schott P, Siegemund M, Merki L, Wiegand J, Jeitziner MM, Laube M, Salomon P, Hillgaertner F, Dullenkopf A, Ksouri H, Cereghetti S, Grazioli S, Bürkle C, Marrel J, Fleisch I, Perez MH, Baltussen Weber A, Ceruti S, Marquardt K, Hübner T, Redecker H, Studhalter M, Stephan M, Selz D, Pietsch U, Ristic A, Heise A, Meyer Zu Bentrup F, Franchitti Laurent M, Fodor P, Gaspert T, Haberthuer C, Colak E, Heuberger DM, Fumeaux T, Montomoli J, Guerci P, Schuepbach RA, Hilty MP, and Roche-Campo F

Subjects

Aged, COVID-19 mortality, Critical Illness mortality, Disease Progression, Female, Hospital Mortality, Humans, Intensive Care Units, Male, Middle Aged, Prospective Studies, Registries, Retrospective Studies, Time Factors, Treatment Outcome, COVID-19 therapy, Critical Illness therapy, Respiratory Therapy methods, Respiratory Therapy statistics & numerical data

Abstract

Background: Uncertainty about the optimal respiratory support strategies in critically ill COVID-19 patients is widespread. While the risks and benefits of noninvasive techniques versus early invasive mechanical ventilation (IMV) are intensely debated, actual evidence is lacking. We sought to assess the risks and benefits of different respiratory support strategies, employed in intensive care units during the first months of the COVID-19 pandemic on intubation and intensive care unit (ICU) mortality rates., Methods: Subanalysis of a prospective, multinational registry of critically ill COVID-19 patients. Patients were subclassified into standard oxygen therapy ≥10 L/min (SOT), high-flow oxygen therapy (HFNC), noninvasive positive-pressure ventilation (NIV), and early IMV, according to the respiratory support strategy employed at the day of admission to ICU. Propensity score matching was performed to ensure comparability between groups., Results: Initially, 1421 patients were assessed for possible study inclusion. Of these, 351 patients (85 SOT, 87 HFNC, 87 NIV, and 92 IMV) remained eligible for full analysis after propensity score matching. 55% of patients initially receiving noninvasive respiratory support required IMV. The intubation rate was lower in patients initially ventilated with HFNC and NIV compared to those who received SOT (SOT: 64%, HFNC: 52%, NIV: 49%, p = 0.025). Compared to the other respiratory support strategies, NIV was associated with a higher overall ICU mortality (SOT: 18%, HFNC: 20%, NIV: 37%, IMV: 25%, p = 0.016)., Conclusion: In this cohort of critically ill patients with COVID-19, a trial of HFNC appeared to be the most balanced initial respiratory support strategy, given the reduced intubation rate and comparable ICU mortality rate. Nonetheless, considering the uncertainty and stress associated with the COVID-19 pandemic, SOT and early IMV represented safe initial respiratory support strategies. The presented findings, in agreement with classic ARDS literature, suggest that NIV should be avoided whenever possible due to the elevated ICU mortality risk.

Published

2021

42. Alveolar CCN1 is associated with mechanical stretch and acute respiratory distress syndrome severity.

Author

Morrell ED, Grazioli S, Hung C, Kajikawa O, Kosamo S, Stapleton RD, Gharib SA, Amado-Rodríguez L, Albaiceta G, Wurfel MM, and Matute-Bello G

Subjects

Acute Lung Injury metabolism, Animals, Bronchoalveolar Lavage Fluid cytology, Inflammation metabolism, Lung metabolism, Mice, Cysteine-Rich Protein 61 metabolism, Respiration, Artificial methods, Respiratory Distress Syndrome metabolism, Ventilator-Induced Lung Injury metabolism

Abstract

The cellular communication network factor 1 (CCN1) is a matricellular protein that can modulate multiple tissue responses, including inflammation and repair. We have previously shown that adenoviral overexpression of Ccn1 is sufficient to cause acute lung injury in mice. We hypothesized that CCN1 is present in the airspaces of lungs during the acute phase of lung injury, and higher concentrations are associated with acute respiratory distress syndrome (ARDS) severity. We tested this hypothesis by measuring 1 ) CCN1 in bronchoalveolar lavage fluid (BALF) and lung homogenates from mice subjected to ventilation-induced lung injury (VILI), 2 ) Ccn1 gene expression and protein levels in MLE-12 cells (alveolar epithelial cell line) subjected to mechanical stretch, and 3 ) CCN1 in BALF from mechanically ventilated humans with and without ARDS. BALF CCN1 concentrations and whole lung CCN1 protein levels were significantly increased in mice with VILI ( n = 6) versus noninjured controls ( n = 6). Ccn1 gene expression and CCN1 protein levels were increased in MLE-12 cells cultured under stretch conditions. Subjects with ARDS ( n = 77) had higher BALF CCN1 levels compared with mechanically ventilated subjects without ARDS ( n = 45) ( P < 0.05). In subjects with ARDS, BALF CCN1 concentrations were associated with higher total protein, sRAGE, and worse [Formula: see text]/[Formula: see text] ratios (all P < 0.05). CCN1 is present in the lungs of mice and humans during the acute inflammatory phase of lung injury, and concentrations are higher in patients with increased markers of severity. Alveolar epithelial cells may be an important source of CCN1 under mechanical stretch conditions.

Published

2020

43. Reply to Dr. Weiskirchen.

Author

Grazioli S and Matute-Bello G

Subjects

Animals, Humans, Male, Acute Lung Injury metabolism, Cysteine-Rich Protein 61 metabolism, Gene Expression

Published

2015

44. CYR61 (CCN1) overexpression induces lung injury in mice.

Author

Grazioli S, Gil S, An D, Kajikawa O, Farnand AW, Hanson JF, Birkland T, Chen P, Duffield J, Schnapp LM, Altemeier WA, and Matute-Bello G

Subjects

Animals, Cysteine-Rich Protein 61 genetics, Humans, Lung metabolism, Male, Mice, Inbred C57BL, Respiratory Distress Syndrome metabolism, Acute Lung Injury metabolism, Cysteine-Rich Protein 61 metabolism, Gene Expression

Abstract

Cysteine-rich protein-61 (CYR61), also known as connective tissue growth factor, CYR61, and nephroblastoma overexpressed gene 1 (CCN1), is a heparin-binding protein member of the CCN family of matricellular proteins. Gene expression profiles showed that Cyr61 is upregulated in human acute lung injury (ALI), but its functional role is unclear. We hypothesized that CYR61 contributes to ALI in mice. First, we demonstrated that CYR61 expression increases after bleomycin-induced lung injury. We then used adenovirus-mediated gene transfer to determine whether CYR61 overexpression in the lungs was sufficient to cause ALI. Mice instilled with CYR61 adenovirus showed greater weight loss, increased bronchoalveolar lavage total neutrophil counts, increased protein concentrations, and increased mortality compared with mice instilled with empty-vector adenovirus. Immunohistochemical studies in lungs from humans with idiopathic pulmonary fibrosis revealed CYR61 expression on the luminal membrane of alveolar epithelial cells in areas of injury. We conclude that CYR61 is upregulated in ALI and that CYR61 overexpression exacerbates ALI in mice., (Copyright © 2015 the American Physiological Society.)

Published

2015