Clinical and pulmonary function analysis in long-COVID revealed that long-term pulmonary dysfunction is associated with vascular inflammation pathways and metabolic syndrome

Sergio Sanhueza; Mabel A. Vidal; Mauricio A. Hernandez; Mario E. Henriquez-Beltran; Camilo Cabrera; Romina Quiroga; Bárbara E. Antilef; Kevin P. Aguilar; Daniela A. Castillo; Faryd J. Llerena; Marco Fraga Figueroa; Mauricio Nazal; Eritson Castro; Paola Lagos; Alexa Moreno; Jaime J. Lastra; Jorge Gajardo; Pamela Garcés; Benilde Riffo; Jorge Buchert; Rocío Sanhueza; Valeska Ormazába; Pablo Saldivia; Cristian Vargas; Guillermo Nourdin; Elard Koch; Felipe A. Zuñiga; Liliana Lamperti; Paula Bustos; Enrique Guzmán-Gutiérrez; Claudio A. Tapia; Luciano Ferrada; Gustavo Cerda; Ute Woehlbier; Erick Riquelme; Maria Isabel Yuseff; Braulio A. Muñoz Ramirez; Giovanna Lombardi; David De Gonzalo-Calvo; Carlos Salomon; Ricardo A. Verdugo; Luis A. Quiñones; Alicia Colombo; Maria I. Barría; Gonzalo Labarca; Estefania Nova-Lamperti

doi:10.3389/fmed.2023.1271863

Clinical and pulmonary function analysis in long-COVID revealed that long-term pulmonary dysfunction is associated with vascular inflammation pathways and metabolic syndrome

Sergio Sanhueza, Mabel A. Vidal, Mauricio A. Hernandez, Mario E. Henriquez-Beltran, Camilo Cabrera, Romina Quiroga, Bárbara E. Antilef, Kevin P. Aguilar, Daniela A. Castillo, Faryd J. Llerena, Marco Fraga Figueroa, Mauricio Nazal, Eritson Castro, Paola Lagos, Alexa Moreno, Jaime J. Lastra, Jorge Gajardo, Pamela Garcés, Benilde Riffo, Jorge BuchertRocío Sanhueza, Valeska Ormazába, Pablo Saldivia, Cristian Vargas, Guillermo Nourdin, Elard Koch, Felipe A. Zuñiga, Liliana Lamperti, Paula Bustos, Enrique Guzmán-Gutiérrez, Claudio A. Tapia, Luciano Ferrada, Gustavo Cerda, Ute Woehlbier, Erick Riquelme, Maria Isabel Yuseff, Braulio A. Muñoz Ramirez, Giovanna Lombardi, David De Gonzalo-Calvo, Carlos Salomon, Ricardo A. Verdugo, Luis A. Quiñones, Alicia Colombo, Maria I. Barría, Gonzalo Labarca, Estefania Nova-Lamperti^*

^*Autor correspondiente de este trabajo

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Resumen

Introduction: Long-term pulmonary dysfunction (L-TPD) is one of the most critical manifestations of long-COVID. This lung affection has been associated with disease severity during the acute phase and the presence of previous comorbidities, however, the clinical manifestations, the concomitant consequences and the molecular pathways supporting this clinical condition remain unknown. The aim of this study was to identify and characterize L-TPD in patients with long-COVID and elucidate the main pathways and long-term consequences attributed to this condition by analyzing clinical parameters and functional tests supported by machine learning and serum proteome profiling. Methods: Patients with L-TPD were classified according to the results of their computer-tomography (CT) scan and diffusing capacity of the lungs for carbon monoxide adjusted for hemoglobin (DLCOc) tests at 4 and 12-months post-infection. Results: Regarding the acute phase, our data showed that L-TPD was favored in elderly patients with hypertension or insulin resistance, supported by pathways associated with vascular inflammation and chemotaxis of phagocytes, according to computer proteomics. Then, at 4-months post-infection, clinical and functional tests revealed that L-TPD patients exhibited a restrictive lung condition, impaired aerobic capacity and reduced muscular strength. At this time point, high circulating levels of platelets and CXCL9, and an inhibited FCgamma-receptor-mediated-phagocytosis due to reduced FcγRIII (CD16) expression in CD14+ monocytes was observed in patients with L-TPD. Finally, 1-year post infection, patients with L-TPD worsened metabolic syndrome and augmented body mass index in comparison with other patient groups. Discussion: Overall, our data demonstrated that CT scan and DLCOc identified patients with L-TPD after COVID-19. This condition was associated with vascular inflammation and impair phagocytosis of virus-antibody immune complexes by reduced FcγRIII expression. In addition, we conclude that COVID-19 survivors required a personalized follow-up and adequate intervention to reduce long-term sequelae and the appearance of further metabolic diseases.

Idioma original	Inglés
Número de artículo	1271863
Publicación	Frontiers in Medicine
Volumen	10
DOI	https://doi.org/10.3389/fmed.2023.1271863
Estado	Publicada - 2023

Nota bibliográfica

Publisher Copyright:
Copyright © 2023 Sanhueza, Vidal, Hernandez, Henriquez-Beltran, Cabrera, Quiroga, Antilef, Aguilar, Castillo, Llerena, Fraga Figueroa, Nazal, Castro, Lagos, Moreno, Lastra, Gajardo, Garcés, Riffo, Buchert, Sanhueza, Ormazába, Saldivia, Vargas, Nourdin, Koch, Zuñiga, Lamperti, Bustos, Guzmán-Gutiérrez, Tapia, Ferrada, Cerda, Woehlbier, Riquelme, Yuseff, Muñoz Ramirez, Lombardi, De Gonzalo-Calvo, Salomon, Verdugo, Quiñones, Colombo, Barría, Labarca and Nova-Lamperti.

Áreas temáticas de ASJC Scopus

Medicina General

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10.3389/fmed.2023.1271863

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Sanhueza, S., Vidal, M. A., Hernandez, M. A., Henriquez-Beltran, M. E., Cabrera, C., Quiroga, R., Antilef, B. E., Aguilar, K. P., Castillo, D. A., Llerena, F. J., Fraga Figueroa, M., Nazal, M., Castro, E., Lagos, P., Moreno, A., Lastra, J. J., Gajardo, J., Garcés, P., Riffo, B., ... Nova-Lamperti, E. (2023). Clinical and pulmonary function analysis in long-COVID revealed that long-term pulmonary dysfunction is associated with vascular inflammation pathways and metabolic syndrome. Frontiers in Medicine, 10, Artículo 1271863. https://doi.org/10.3389/fmed.2023.1271863

@article{791c7ea876bb43eb9cc9fa8b3a88afcb,

title = "Clinical and pulmonary function analysis in long-COVID revealed that long-term pulmonary dysfunction is associated with vascular inflammation pathways and metabolic syndrome",

abstract = "Introduction: Long-term pulmonary dysfunction (L-TPD) is one of the most critical manifestations of long-COVID. This lung affection has been associated with disease severity during the acute phase and the presence of previous comorbidities, however, the clinical manifestations, the concomitant consequences and the molecular pathways supporting this clinical condition remain unknown. The aim of this study was to identify and characterize L-TPD in patients with long-COVID and elucidate the main pathways and long-term consequences attributed to this condition by analyzing clinical parameters and functional tests supported by machine learning and serum proteome profiling. Methods: Patients with L-TPD were classified according to the results of their computer-tomography (CT) scan and diffusing capacity of the lungs for carbon monoxide adjusted for hemoglobin (DLCOc) tests at 4 and 12-months post-infection. Results: Regarding the acute phase, our data showed that L-TPD was favored in elderly patients with hypertension or insulin resistance, supported by pathways associated with vascular inflammation and chemotaxis of phagocytes, according to computer proteomics. Then, at 4-months post-infection, clinical and functional tests revealed that L-TPD patients exhibited a restrictive lung condition, impaired aerobic capacity and reduced muscular strength. At this time point, high circulating levels of platelets and CXCL9, and an inhibited FCgamma-receptor-mediated-phagocytosis due to reduced FcγRIII (CD16) expression in CD14+ monocytes was observed in patients with L-TPD. Finally, 1-year post infection, patients with L-TPD worsened metabolic syndrome and augmented body mass index in comparison with other patient groups. Discussion: Overall, our data demonstrated that CT scan and DLCOc identified patients with L-TPD after COVID-19. This condition was associated with vascular inflammation and impair phagocytosis of virus-antibody immune complexes by reduced FcγRIII expression. In addition, we conclude that COVID-19 survivors required a personalized follow-up and adequate intervention to reduce long-term sequelae and the appearance of further metabolic diseases.",

keywords = "COVID-19, chemokines, metabolic syndrome, pulmonary dysfunction, sequelae, vascular inflammation",

author = "Sergio Sanhueza and Vidal, {Mabel A.} and Hernandez, {Mauricio A.} and Henriquez-Beltran, {Mario E.} and Camilo Cabrera and Romina Quiroga and Antilef, {B{\'a}rbara E.} and Aguilar, {Kevin P.} and Castillo, {Daniela A.} and Llerena, {Faryd J.} and {Fraga Figueroa}, Marco and Mauricio Nazal and Eritson Castro and Paola Lagos and Alexa Moreno and Lastra, {Jaime J.} and Jorge Gajardo and Pamela Garc{\'e}s and Benilde Riffo and Jorge Buchert and Roc{\'i}o Sanhueza and Valeska Ormaz{\'a}ba and Pablo Saldivia and Cristian Vargas and Guillermo Nourdin and Elard Koch and Zu{\~n}iga, {Felipe A.} and Liliana Lamperti and Paula Bustos and Enrique Guzm{\'a}n-Guti{\'e}rrez and Tapia, {Claudio A.} and Luciano Ferrada and Gustavo Cerda and Ute Woehlbier and Erick Riquelme and Yuseff, {Maria Isabel} and {Mu{\~n}oz Ramirez}, {Braulio A.} and Giovanna Lombardi and {De Gonzalo-Calvo}, David and Carlos Salomon and Verdugo, {Ricardo A.} and Qui{\~n}ones, {Luis A.} and Alicia Colombo and Barr{\'i}a, {Maria I.} and Gonzalo Labarca and Estefania Nova-Lamperti",

note = "Publisher Copyright: Copyright {\textcopyright} 2023 Sanhueza, Vidal, Hernandez, Henriquez-Beltran, Cabrera, Quiroga, Antilef, Aguilar, Castillo, Llerena, Fraga Figueroa, Nazal, Castro, Lagos, Moreno, Lastra, Gajardo, Garc{\'e}s, Riffo, Buchert, Sanhueza, Ormaz{\'a}ba, Saldivia, Vargas, Nourdin, Koch, Zu{\~n}iga, Lamperti, Bustos, Guzm{\'a}n-Guti{\'e}rrez, Tapia, Ferrada, Cerda, Woehlbier, Riquelme, Yuseff, Mu{\~n}oz Ramirez, Lombardi, De Gonzalo-Calvo, Salomon, Verdugo, Qui{\~n}ones, Colombo, Barr{\'i}a, Labarca and Nova-Lamperti.",

year = "2023",

doi = "10.3389/fmed.2023.1271863",

language = "English",

volume = "10",

journal = "Frontiers in Medicine",

issn = "2296-858X",

publisher = "Frontiers Media S.A.",

}

Sanhueza, S, Vidal, MA, Hernandez, MA, Henriquez-Beltran, ME, Cabrera, C, Quiroga, R, Antilef, BE, Aguilar, KP, Castillo, DA, Llerena, FJ, Fraga Figueroa, M, Nazal, M, Castro, E, Lagos, P, Moreno, A, Lastra, JJ, Gajardo, J, Garcés, P, Riffo, B, Buchert, J, Sanhueza, R, Ormazába, V, Saldivia, P, Vargas, C, Nourdin, G, Koch, E, Zuñiga, FA, Lamperti, L, Bustos, P, Guzmán-Gutiérrez, E, Tapia, CA, Ferrada, L, Cerda, G, Woehlbier, U, Riquelme, E, Yuseff, MI, Muñoz Ramirez, BA, Lombardi, G, De Gonzalo-Calvo, D, Salomon, C, Verdugo, RA, Quiñones, LA, Colombo, A, Barría, MI, Labarca, G & Nova-Lamperti, E 2023, 'Clinical and pulmonary function analysis in long-COVID revealed that long-term pulmonary dysfunction is associated with vascular inflammation pathways and metabolic syndrome', Frontiers in Medicine, vol. 10, 1271863. https://doi.org/10.3389/fmed.2023.1271863

Clinical and pulmonary function analysis in long-COVID revealed that long-term pulmonary dysfunction is associated with vascular inflammation pathways and metabolic syndrome. / Sanhueza, Sergio; Vidal, Mabel A.; Hernandez, Mauricio A. et al.
En: Frontiers in Medicine, Vol. 10, 1271863, 2023.

Producción científica: Contribución a una revista › Artículo › revisión exhaustiva

TY - JOUR

T1 - Clinical and pulmonary function analysis in long-COVID revealed that long-term pulmonary dysfunction is associated with vascular inflammation pathways and metabolic syndrome

AU - Sanhueza, Sergio

AU - Vidal, Mabel A.

AU - Hernandez, Mauricio A.

AU - Henriquez-Beltran, Mario E.

AU - Cabrera, Camilo

AU - Quiroga, Romina

AU - Antilef, Bárbara E.

AU - Aguilar, Kevin P.

AU - Castillo, Daniela A.

AU - Llerena, Faryd J.

AU - Fraga Figueroa, Marco

AU - Nazal, Mauricio

AU - Castro, Eritson

AU - Lagos, Paola

AU - Moreno, Alexa

AU - Lastra, Jaime J.

AU - Gajardo, Jorge

AU - Garcés, Pamela

AU - Riffo, Benilde

AU - Buchert, Jorge

AU - Sanhueza, Rocío

AU - Ormazába, Valeska

AU - Saldivia, Pablo

AU - Vargas, Cristian

AU - Nourdin, Guillermo

AU - Koch, Elard

AU - Zuñiga, Felipe A.

AU - Lamperti, Liliana

AU - Bustos, Paula

AU - Guzmán-Gutiérrez, Enrique

AU - Tapia, Claudio A.

AU - Ferrada, Luciano

AU - Cerda, Gustavo

AU - Woehlbier, Ute

AU - Riquelme, Erick

AU - Yuseff, Maria Isabel

AU - Muñoz Ramirez, Braulio A.

AU - Lombardi, Giovanna

AU - De Gonzalo-Calvo, David

AU - Salomon, Carlos

AU - Verdugo, Ricardo A.

AU - Quiñones, Luis A.

AU - Colombo, Alicia

AU - Barría, Maria I.

AU - Labarca, Gonzalo

AU - Nova-Lamperti, Estefania

N1 - Publisher Copyright: Copyright © 2023 Sanhueza, Vidal, Hernandez, Henriquez-Beltran, Cabrera, Quiroga, Antilef, Aguilar, Castillo, Llerena, Fraga Figueroa, Nazal, Castro, Lagos, Moreno, Lastra, Gajardo, Garcés, Riffo, Buchert, Sanhueza, Ormazába, Saldivia, Vargas, Nourdin, Koch, Zuñiga, Lamperti, Bustos, Guzmán-Gutiérrez, Tapia, Ferrada, Cerda, Woehlbier, Riquelme, Yuseff, Muñoz Ramirez, Lombardi, De Gonzalo-Calvo, Salomon, Verdugo, Quiñones, Colombo, Barría, Labarca and Nova-Lamperti.

PY - 2023

Y1 - 2023

N2 - Introduction: Long-term pulmonary dysfunction (L-TPD) is one of the most critical manifestations of long-COVID. This lung affection has been associated with disease severity during the acute phase and the presence of previous comorbidities, however, the clinical manifestations, the concomitant consequences and the molecular pathways supporting this clinical condition remain unknown. The aim of this study was to identify and characterize L-TPD in patients with long-COVID and elucidate the main pathways and long-term consequences attributed to this condition by analyzing clinical parameters and functional tests supported by machine learning and serum proteome profiling. Methods: Patients with L-TPD were classified according to the results of their computer-tomography (CT) scan and diffusing capacity of the lungs for carbon monoxide adjusted for hemoglobin (DLCOc) tests at 4 and 12-months post-infection. Results: Regarding the acute phase, our data showed that L-TPD was favored in elderly patients with hypertension or insulin resistance, supported by pathways associated with vascular inflammation and chemotaxis of phagocytes, according to computer proteomics. Then, at 4-months post-infection, clinical and functional tests revealed that L-TPD patients exhibited a restrictive lung condition, impaired aerobic capacity and reduced muscular strength. At this time point, high circulating levels of platelets and CXCL9, and an inhibited FCgamma-receptor-mediated-phagocytosis due to reduced FcγRIII (CD16) expression in CD14+ monocytes was observed in patients with L-TPD. Finally, 1-year post infection, patients with L-TPD worsened metabolic syndrome and augmented body mass index in comparison with other patient groups. Discussion: Overall, our data demonstrated that CT scan and DLCOc identified patients with L-TPD after COVID-19. This condition was associated with vascular inflammation and impair phagocytosis of virus-antibody immune complexes by reduced FcγRIII expression. In addition, we conclude that COVID-19 survivors required a personalized follow-up and adequate intervention to reduce long-term sequelae and the appearance of further metabolic diseases.

AB - Introduction: Long-term pulmonary dysfunction (L-TPD) is one of the most critical manifestations of long-COVID. This lung affection has been associated with disease severity during the acute phase and the presence of previous comorbidities, however, the clinical manifestations, the concomitant consequences and the molecular pathways supporting this clinical condition remain unknown. The aim of this study was to identify and characterize L-TPD in patients with long-COVID and elucidate the main pathways and long-term consequences attributed to this condition by analyzing clinical parameters and functional tests supported by machine learning and serum proteome profiling. Methods: Patients with L-TPD were classified according to the results of their computer-tomography (CT) scan and diffusing capacity of the lungs for carbon monoxide adjusted for hemoglobin (DLCOc) tests at 4 and 12-months post-infection. Results: Regarding the acute phase, our data showed that L-TPD was favored in elderly patients with hypertension or insulin resistance, supported by pathways associated with vascular inflammation and chemotaxis of phagocytes, according to computer proteomics. Then, at 4-months post-infection, clinical and functional tests revealed that L-TPD patients exhibited a restrictive lung condition, impaired aerobic capacity and reduced muscular strength. At this time point, high circulating levels of platelets and CXCL9, and an inhibited FCgamma-receptor-mediated-phagocytosis due to reduced FcγRIII (CD16) expression in CD14+ monocytes was observed in patients with L-TPD. Finally, 1-year post infection, patients with L-TPD worsened metabolic syndrome and augmented body mass index in comparison with other patient groups. Discussion: Overall, our data demonstrated that CT scan and DLCOc identified patients with L-TPD after COVID-19. This condition was associated with vascular inflammation and impair phagocytosis of virus-antibody immune complexes by reduced FcγRIII expression. In addition, we conclude that COVID-19 survivors required a personalized follow-up and adequate intervention to reduce long-term sequelae and the appearance of further metabolic diseases.

KW - COVID-19

KW - chemokines

KW - metabolic syndrome

KW - pulmonary dysfunction

KW - sequelae

KW - vascular inflammation

UR - http://www.scopus.com/inward/record.url?scp=85174803931&partnerID=8YFLogxK

U2 - 10.3389/fmed.2023.1271863

DO - 10.3389/fmed.2023.1271863

M3 - Article

AN - SCOPUS:85174803931

SN - 2296-858X

VL - 10

JO - Frontiers in Medicine

JF - Frontiers in Medicine

M1 - 1271863

ER -

Clinical and pulmonary function analysis in long-COVID revealed that long-term pulmonary dysfunction is associated with vascular inflammation pathways and metabolic syndrome

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