Multiplex protein profiling of bronchial aspirates reveals disease-, mortality- and respiratory sequelae-associated signatures in critically ill patients with ARDS secondary to SARS-CoV-2 infection

INTRODUCTION: Bronchial aspirates (BAS) obtained during invasive mechanical ventilation (IMV) constitutes a useful tool for molecular phenotyping and decision making. AIM: To identify the proteomic determinants associated with disease pathogenesis, all-cause mortality and respiratory sequelae in BAS...

Descripción completa

Detalles Bibliográficos
Autores principales: Molinero, Marta, Gómez, Silvia, Benítez, Iván D., Vengoechea, J. J., González, Jessica, Polanco, Dinora, Gort-Paniello, Clara, Moncusí-Moix, Anna, García-Hidalgo, María C., Perez-Pons, Manel, Belmonte, Thalía, Torres, Gerard, Caballero, Jesús, Barberà, Carme, Ayestarán Rota, Jose Ignacio, Socías Crespí, Lorenzo, Ceccato, Adrián, Fernández-Barat, Laia, Ferrer, Ricard, Garcia-Gasulla, Dario, Lorente-Balanza, Jose Ángel, Menéndez, Rosario, Motos, Ana, Peñuelas, Oscar, Riera, Jordi, Torres, Antoni, Barbé, Ferran, de Gonzalo-Calvo, David
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2022
Materias:
Immunology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9373836/
https://www.ncbi.nlm.nih.gov/pubmed/35967328
http://dx.doi.org/10.3389/fimmu.2022.942443
_version_ 1784767671488741376
author Molinero, Marta
Gómez, Silvia
Benítez, Iván D.
Vengoechea, J. J.
González, Jessica
Polanco, Dinora
Gort-Paniello, Clara
Moncusí-Moix, Anna
García-Hidalgo, María C.
Perez-Pons, Manel
Belmonte, Thalía
Torres, Gerard
Caballero, Jesús
Barberà, Carme
Ayestarán Rota, Jose Ignacio
Socías Crespí, Lorenzo
Ceccato, Adrián
Fernández-Barat, Laia
Ferrer, Ricard
Garcia-Gasulla, Dario
Lorente-Balanza, Jose Ángel
Menéndez, Rosario
Motos, Ana
Peñuelas, Oscar
Riera, Jordi
Torres, Antoni
Barbé, Ferran
de Gonzalo-Calvo, David
author_facet Molinero, Marta
Gómez, Silvia
Benítez, Iván D.
Vengoechea, J. J.
González, Jessica
Polanco, Dinora
Gort-Paniello, Clara
Moncusí-Moix, Anna
García-Hidalgo, María C.
Perez-Pons, Manel
Belmonte, Thalía
Torres, Gerard
Caballero, Jesús
Barberà, Carme
Ayestarán Rota, Jose Ignacio
Socías Crespí, Lorenzo
Ceccato, Adrián
Fernández-Barat, Laia
Ferrer, Ricard
Garcia-Gasulla, Dario
Lorente-Balanza, Jose Ángel
Menéndez, Rosario
Motos, Ana
Peñuelas, Oscar
Riera, Jordi
Torres, Antoni
Barbé, Ferran
de Gonzalo-Calvo, David
author_sort Molinero, Marta
collection PubMed
description INTRODUCTION: Bronchial aspirates (BAS) obtained during invasive mechanical ventilation (IMV) constitutes a useful tool for molecular phenotyping and decision making. AIM: To identify the proteomic determinants associated with disease pathogenesis, all-cause mortality and respiratory sequelae in BAS samples from critically ill patients with SARS-CoV-2-induced ARDS METHODS: Multicenter study including 74 critically ill patients with COVID-19 and non-COVID-19 ARDS. BAS were obtained by bronchoaspiration after IMV initiation. Three hundred sixty-four proteins were quantified using proximity extension assay (PEA) technology. Random forest models were used to assess predictor importance. RESULTS: After adjusting for confounding factors, CST5, NADK, SRPK2 and TGF-α were differentially detected in COVID-19 and non-COVID-19 patients. In random forest models for COVID-19, CST5, DPP7, NADK, KYAT1 and TYMP showed the highest variable importance. In COVID-19 patients, reduced levels of ENTPD2 and PTN were observed in nonsurvivors of ICU stay, even after adjustment. AGR2, NQO2, IL-1α, OSM and TRAIL showed the strongest associations with in-ICU mortality and were used to construct a protein-based prediction model. Kaplan-Meier curves revealed a clear separation in mortality risk between subgroups of PTN, ENTPD2 and the prediction model. Cox regression models supported these findings. In survivors, the levels of FCRL1, NTF4 and THOP1 in BAS samples obtained during the ICU stay correlated with lung function (i.e., D(LCO) levels) 3 months after hospital discharge. Similarly, Flt3L and THOP1 levels were correlated with radiological features (i.e., TSS). These proteins are expressed in immune and nonimmune lung cells. Poor host response to viral infectivity and an inappropriate reparative mechanism seem to be linked with the pathogenesis of the disease and fatal outcomes, respectively. CONCLUSION: BAS proteomics identified novel factors associated with the pathology of SARS-CoV-2-induced ARDS and its adverse outcomes. BAS-based protein testing emerges as a novel tool for risk assessment in the ICU.
format Online
Article
Text
id pubmed-9373836
institution National Center for Biotechnology Information
language English
publishDate 2022
publisher Frontiers Media S.A.
record_format MEDLINE/PubMed
spelling pubmed-93738362022-08-13 Multiplex protein profiling of bronchial aspirates reveals disease-, mortality- and respiratory sequelae-associated signatures in critically ill patients with ARDS secondary to SARS-CoV-2 infection Molinero, Marta Gómez, Silvia Benítez, Iván D. Vengoechea, J. J. González, Jessica Polanco, Dinora Gort-Paniello, Clara Moncusí-Moix, Anna García-Hidalgo, María C. Perez-Pons, Manel Belmonte, Thalía Torres, Gerard Caballero, Jesús Barberà, Carme Ayestarán Rota, Jose Ignacio Socías Crespí, Lorenzo Ceccato, Adrián Fernández-Barat, Laia Ferrer, Ricard Garcia-Gasulla, Dario Lorente-Balanza, Jose Ángel Menéndez, Rosario Motos, Ana Peñuelas, Oscar Riera, Jordi Torres, Antoni Barbé, Ferran de Gonzalo-Calvo, David Front Immunol Immunology INTRODUCTION: Bronchial aspirates (BAS) obtained during invasive mechanical ventilation (IMV) constitutes a useful tool for molecular phenotyping and decision making. AIM: To identify the proteomic determinants associated with disease pathogenesis, all-cause mortality and respiratory sequelae in BAS samples from critically ill patients with SARS-CoV-2-induced ARDS METHODS: Multicenter study including 74 critically ill patients with COVID-19 and non-COVID-19 ARDS. BAS were obtained by bronchoaspiration after IMV initiation. Three hundred sixty-four proteins were quantified using proximity extension assay (PEA) technology. Random forest models were used to assess predictor importance. RESULTS: After adjusting for confounding factors, CST5, NADK, SRPK2 and TGF-α were differentially detected in COVID-19 and non-COVID-19 patients. In random forest models for COVID-19, CST5, DPP7, NADK, KYAT1 and TYMP showed the highest variable importance. In COVID-19 patients, reduced levels of ENTPD2 and PTN were observed in nonsurvivors of ICU stay, even after adjustment. AGR2, NQO2, IL-1α, OSM and TRAIL showed the strongest associations with in-ICU mortality and were used to construct a protein-based prediction model. Kaplan-Meier curves revealed a clear separation in mortality risk between subgroups of PTN, ENTPD2 and the prediction model. Cox regression models supported these findings. In survivors, the levels of FCRL1, NTF4 and THOP1 in BAS samples obtained during the ICU stay correlated with lung function (i.e., D(LCO) levels) 3 months after hospital discharge. Similarly, Flt3L and THOP1 levels were correlated with radiological features (i.e., TSS). These proteins are expressed in immune and nonimmune lung cells. Poor host response to viral infectivity and an inappropriate reparative mechanism seem to be linked with the pathogenesis of the disease and fatal outcomes, respectively. CONCLUSION: BAS proteomics identified novel factors associated with the pathology of SARS-CoV-2-induced ARDS and its adverse outcomes. BAS-based protein testing emerges as a novel tool for risk assessment in the ICU. Frontiers Media S.A. 2022-07-29 /pmc/articles/PMC9373836/ /pubmed/35967328 http://dx.doi.org/10.3389/fimmu.2022.942443 Text en Copyright © 2022 Molinero, Gómez, Benítez, Vengoechea, González, Polanco, Gort-Paniello, Moncusí-Moix, García-Hidalgo, Perez-Pons, Belmonte, Torres, Caballero, Barberà, Ayestarán Rota, Socías Crespí, Ceccato, Fernández-Barat, Ferrer, Garcia-Gasulla, Lorente-Balanza, Menéndez, Motos, Peñuelas, Riera, Torres, Barbé and de Gonzalo-Calvo https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Immunology
Molinero, Marta
Gómez, Silvia
Benítez, Iván D.
Vengoechea, J. J.
González, Jessica
Polanco, Dinora
Gort-Paniello, Clara
Moncusí-Moix, Anna
García-Hidalgo, María C.
Perez-Pons, Manel
Belmonte, Thalía
Torres, Gerard
Caballero, Jesús
Barberà, Carme
Ayestarán Rota, Jose Ignacio
Socías Crespí, Lorenzo
Ceccato, Adrián
Fernández-Barat, Laia
Ferrer, Ricard
Garcia-Gasulla, Dario
Lorente-Balanza, Jose Ángel
Menéndez, Rosario
Motos, Ana
Peñuelas, Oscar
Riera, Jordi
Torres, Antoni
Barbé, Ferran
de Gonzalo-Calvo, David
Multiplex protein profiling of bronchial aspirates reveals disease-, mortality- and respiratory sequelae-associated signatures in critically ill patients with ARDS secondary to SARS-CoV-2 infection
title Multiplex protein profiling of bronchial aspirates reveals disease-, mortality- and respiratory sequelae-associated signatures in critically ill patients with ARDS secondary to SARS-CoV-2 infection
title_full Multiplex protein profiling of bronchial aspirates reveals disease-, mortality- and respiratory sequelae-associated signatures in critically ill patients with ARDS secondary to SARS-CoV-2 infection
title_fullStr Multiplex protein profiling of bronchial aspirates reveals disease-, mortality- and respiratory sequelae-associated signatures in critically ill patients with ARDS secondary to SARS-CoV-2 infection
title_full_unstemmed Multiplex protein profiling of bronchial aspirates reveals disease-, mortality- and respiratory sequelae-associated signatures in critically ill patients with ARDS secondary to SARS-CoV-2 infection
title_short Multiplex protein profiling of bronchial aspirates reveals disease-, mortality- and respiratory sequelae-associated signatures in critically ill patients with ARDS secondary to SARS-CoV-2 infection
title_sort multiplex protein profiling of bronchial aspirates reveals disease-, mortality- and respiratory sequelae-associated signatures in critically ill patients with ards secondary to sars-cov-2 infection
topic Immunology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9373836/
https://www.ncbi.nlm.nih.gov/pubmed/35967328
http://dx.doi.org/10.3389/fimmu.2022.942443
work_keys_str_mv AT molineromarta multiplexproteinprofilingofbronchialaspiratesrevealsdiseasemortalityandrespiratorysequelaeassociatedsignaturesincriticallyillpatientswithardssecondarytosarscov2infection
AT gomezsilvia multiplexproteinprofilingofbronchialaspiratesrevealsdiseasemortalityandrespiratorysequelaeassociatedsignaturesincriticallyillpatientswithardssecondarytosarscov2infection
AT benitezivand multiplexproteinprofilingofbronchialaspiratesrevealsdiseasemortalityandrespiratorysequelaeassociatedsignaturesincriticallyillpatientswithardssecondarytosarscov2infection
AT vengoecheajj multiplexproteinprofilingofbronchialaspiratesrevealsdiseasemortalityandrespiratorysequelaeassociatedsignaturesincriticallyillpatientswithardssecondarytosarscov2infection
AT gonzalezjessica multiplexproteinprofilingofbronchialaspiratesrevealsdiseasemortalityandrespiratorysequelaeassociatedsignaturesincriticallyillpatientswithardssecondarytosarscov2infection
AT polancodinora multiplexproteinprofilingofbronchialaspiratesrevealsdiseasemortalityandrespiratorysequelaeassociatedsignaturesincriticallyillpatientswithardssecondarytosarscov2infection
AT gortpanielloclara multiplexproteinprofilingofbronchialaspiratesrevealsdiseasemortalityandrespiratorysequelaeassociatedsignaturesincriticallyillpatientswithardssecondarytosarscov2infection
AT moncusimoixanna multiplexproteinprofilingofbronchialaspiratesrevealsdiseasemortalityandrespiratorysequelaeassociatedsignaturesincriticallyillpatientswithardssecondarytosarscov2infection
AT garciahidalgomariac multiplexproteinprofilingofbronchialaspiratesrevealsdiseasemortalityandrespiratorysequelaeassociatedsignaturesincriticallyillpatientswithardssecondarytosarscov2infection
AT perezponsmanel multiplexproteinprofilingofbronchialaspiratesrevealsdiseasemortalityandrespiratorysequelaeassociatedsignaturesincriticallyillpatientswithardssecondarytosarscov2infection
AT belmontethalia multiplexproteinprofilingofbronchialaspiratesrevealsdiseasemortalityandrespiratorysequelaeassociatedsignaturesincriticallyillpatientswithardssecondarytosarscov2infection
AT torresgerard multiplexproteinprofilingofbronchialaspiratesrevealsdiseasemortalityandrespiratorysequelaeassociatedsignaturesincriticallyillpatientswithardssecondarytosarscov2infection
AT caballerojesus multiplexproteinprofilingofbronchialaspiratesrevealsdiseasemortalityandrespiratorysequelaeassociatedsignaturesincriticallyillpatientswithardssecondarytosarscov2infection
AT barberacarme multiplexproteinprofilingofbronchialaspiratesrevealsdiseasemortalityandrespiratorysequelaeassociatedsignaturesincriticallyillpatientswithardssecondarytosarscov2infection
AT ayestaranrotajoseignacio multiplexproteinprofilingofbronchialaspiratesrevealsdiseasemortalityandrespiratorysequelaeassociatedsignaturesincriticallyillpatientswithardssecondarytosarscov2infection
AT sociascrespilorenzo multiplexproteinprofilingofbronchialaspiratesrevealsdiseasemortalityandrespiratorysequelaeassociatedsignaturesincriticallyillpatientswithardssecondarytosarscov2infection
AT ceccatoadrian multiplexproteinprofilingofbronchialaspiratesrevealsdiseasemortalityandrespiratorysequelaeassociatedsignaturesincriticallyillpatientswithardssecondarytosarscov2infection
AT fernandezbaratlaia multiplexproteinprofilingofbronchialaspiratesrevealsdiseasemortalityandrespiratorysequelaeassociatedsignaturesincriticallyillpatientswithardssecondarytosarscov2infection
AT ferrerricard multiplexproteinprofilingofbronchialaspiratesrevealsdiseasemortalityandrespiratorysequelaeassociatedsignaturesincriticallyillpatientswithardssecondarytosarscov2infection
AT garciagasulladario multiplexproteinprofilingofbronchialaspiratesrevealsdiseasemortalityandrespiratorysequelaeassociatedsignaturesincriticallyillpatientswithardssecondarytosarscov2infection
AT lorentebalanzajoseangel multiplexproteinprofilingofbronchialaspiratesrevealsdiseasemortalityandrespiratorysequelaeassociatedsignaturesincriticallyillpatientswithardssecondarytosarscov2infection
AT menendezrosario multiplexproteinprofilingofbronchialaspiratesrevealsdiseasemortalityandrespiratorysequelaeassociatedsignaturesincriticallyillpatientswithardssecondarytosarscov2infection
AT motosana multiplexproteinprofilingofbronchialaspiratesrevealsdiseasemortalityandrespiratorysequelaeassociatedsignaturesincriticallyillpatientswithardssecondarytosarscov2infection
AT penuelasoscar multiplexproteinprofilingofbronchialaspiratesrevealsdiseasemortalityandrespiratorysequelaeassociatedsignaturesincriticallyillpatientswithardssecondarytosarscov2infection
AT rierajordi multiplexproteinprofilingofbronchialaspiratesrevealsdiseasemortalityandrespiratorysequelaeassociatedsignaturesincriticallyillpatientswithardssecondarytosarscov2infection
AT torresantoni multiplexproteinprofilingofbronchialaspiratesrevealsdiseasemortalityandrespiratorysequelaeassociatedsignaturesincriticallyillpatientswithardssecondarytosarscov2infection
AT barbeferran multiplexproteinprofilingofbronchialaspiratesrevealsdiseasemortalityandrespiratorysequelaeassociatedsignaturesincriticallyillpatientswithardssecondarytosarscov2infection
AT degonzalocalvodavid multiplexproteinprofilingofbronchialaspiratesrevealsdiseasemortalityandrespiratorysequelaeassociatedsignaturesincriticallyillpatientswithardssecondarytosarscov2infection

Ejemplares similares