Peripheral microcirculatory alterations are associated with the severity of acute respiratory distress syndrome in COVID-19 patients admitted to intermediate respiratory and intensive care units

the HEMOCOVID-19 Consortium

doi:10.1186/s13054-021-03803-2

Peripheral microcirculatory alterations are associated with the severity of acute respiratory distress syndrome in COVID-19 patients admitted to intermediate respiratory and intensive care units

the HEMOCOVID-19 Consortium

Research output: Contribution to journal › Article › peer-review

17 Scopus citations

Abstract

Background: COVID-19 is primarily a respiratory disease; however, there is also evidence that it causes endothelial damage in the microvasculature of several organs. The aim of the present study is to characterize in vivo the microvascular reactivity in peripheral skeletal muscle of severe COVID-19 patients. Methods: This is a prospective observational study carried out in Spain, Mexico and Brazil. Healthy subjects and severe COVID-19 patients admitted to the intermediate respiratory (IRCU) and intensive care units (ICU) due to hypoxemia were studied. Local tissue/blood oxygen saturation (StO₂) and local hemoglobin concentration (THC) were non-invasively measured on the forearm by near-infrared spectroscopy (NIRS). A vascular occlusion test (VOT), a three-minute induced ischemia, was performed in order to obtain dynamic StO₂ parameters: deoxygenation rate (DeO₂), reoxygenation rate (ReO₂), and hyperemic response (H_AUC). In COVID-19 patients, the severity of ARDS was evaluated by the ratio between peripheral arterial oxygen saturation (SpO₂) and the fraction of inspired oxygen (FiO₂) (SF ratio). Results: Healthy controls (32) and COVID-19 patients (73) were studied. Baseline StO₂ and THC did not differ between the two groups. Dynamic VOT-derived parameters were significantly impaired in COVID-19 patients showing lower metabolic rate (DeO₂) and diminished endothelial reactivity. At enrollment, most COVID-19 patients were receiving invasive mechanical ventilation (MV) (53%) or high-flow nasal cannula support (32%). Patients on MV were also receiving sedative agents (100%) and vasopressors (29%). Baseline StO₂ and DeO₂ negatively correlated with SF ratio, while ReO₂ showed a positive correlation with SF ratio. There were significant differences in baseline StO₂ and ReO₂ among the different ARDS groups according to SF ratio, but not among different respiratory support therapies. Conclusion: Patients with severe COVID-19 show systemic microcirculatory alterations suggestive of endothelial dysfunction, and these alterations are associated with the severity of ARDS. Further evaluation is needed to determine whether these observations have prognostic implications. These results represent interim findings of the ongoing HEMOCOVID-19 trial. Trial registration ClinicalTrials.gov NCT04689477. Retrospectively registered 30 December 2020.

Original language	English (US)
Article number	381
Journal	Critical Care
Volume	25
Issue number	1
DOIs	https://doi.org/10.1186/s13054-021-03803-2
State	Published - Dec 2021

Keywords

COVID-19
Endothelial dysfunction
Microcirculation
Near-infrared spectroscopy

ASJC Scopus subject areas

Critical Care and Intensive Care Medicine

Access to Document

10.1186/s13054-021-03803-2

Cite this

@article{7eecaa9c7bda4b56a3d90bbe7f8f187a,

title = "Peripheral microcirculatory alterations are associated with the severity of acute respiratory distress syndrome in COVID-19 patients admitted to intermediate respiratory and intensive care units",

abstract = "Background: COVID-19 is primarily a respiratory disease; however, there is also evidence that it causes endothelial damage in the microvasculature of several organs. The aim of the present study is to characterize in vivo the microvascular reactivity in peripheral skeletal muscle of severe COVID-19 patients. Methods: This is a prospective observational study carried out in Spain, Mexico and Brazil. Healthy subjects and severe COVID-19 patients admitted to the intermediate respiratory (IRCU) and intensive care units (ICU) due to hypoxemia were studied. Local tissue/blood oxygen saturation (StO2) and local hemoglobin concentration (THC) were non-invasively measured on the forearm by near-infrared spectroscopy (NIRS). A vascular occlusion test (VOT), a three-minute induced ischemia, was performed in order to obtain dynamic StO2 parameters: deoxygenation rate (DeO2), reoxygenation rate (ReO2), and hyperemic response (HAUC). In COVID-19 patients, the severity of ARDS was evaluated by the ratio between peripheral arterial oxygen saturation (SpO2) and the fraction of inspired oxygen (FiO2) (SF ratio). Results: Healthy controls (32) and COVID-19 patients (73) were studied. Baseline StO2 and THC did not differ between the two groups. Dynamic VOT-derived parameters were significantly impaired in COVID-19 patients showing lower metabolic rate (DeO2) and diminished endothelial reactivity. At enrollment, most COVID-19 patients were receiving invasive mechanical ventilation (MV) (53%) or high-flow nasal cannula support (32%). Patients on MV were also receiving sedative agents (100%) and vasopressors (29%). Baseline StO2 and DeO2 negatively correlated with SF ratio, while ReO2 showed a positive correlation with SF ratio. There were significant differences in baseline StO2 and ReO2 among the different ARDS groups according to SF ratio, but not among different respiratory support therapies. Conclusion: Patients with severe COVID-19 show systemic microcirculatory alterations suggestive of endothelial dysfunction, and these alterations are associated with the severity of ARDS. Further evaluation is needed to determine whether these observations have prognostic implications. These results represent interim findings of the ongoing HEMOCOVID-19 trial. Trial registration ClinicalTrials.gov NCT04689477. Retrospectively registered 30 December 2020.",

keywords = "COVID-19, Endothelial dysfunction, Microcirculation, Near-infrared spectroscopy",

author = "{the HEMOCOVID-19 Consortium} and Jaume Mesquida and A. Caballer and L. Cortese and C. Vila and U. Karadeniz and M. Pagliazzi and M. Zanoletti and Pacheco, {A. P{\'e}rez} and P. Castro and M. Garc{\'i}a-de-Acilu and Mesquita, {R. C.} and Busch, {D. R.} and T. Durduran and Turgut Durduran and Marco Pagliazzi and Lorenzo Cortese and Marta Zanoletti and Umut Karadeniz and Jaume Mesquida and Alba Caballer and Sara Nogales and Cristina Espinal and Guillem Gruartmoner and Ter{\'a}n, {Puri P{\'e}rez} and Clara Vil{\`a} and Luc{\'i}a Picazo and Ricard Ferrer and {De Acilu}, {Marina Garc{\'i}a} and Luis Chiscano and Abraham Mera and Pedro Castro and Adri{\'a}n T{\'e}llez and Sara Fern{\'a}ndez and Ana Matas and Fernando Fuentes and Isabel Serra and David Romero and Francesc Font and Tim Myers and Busch, {David R.} and Siddharth Dave and Sreekanth Cheruku and Christopher Choi and Peiman Lahsaei and Olson, {Dai Wai} and Pacheco, {Argelia P{\'e}rez} and {Quispe Siccha}, {Rosa Mar{\'i}a} and Eduardo Liceaga and {De Oca Hern{\'a}ndez}, {F{\'e}lix Jerandy Monte} and Besen, {Bruno Adler Maccagnan Pinheiro}",

note = "Funding Information: The study has received funding from Fundaci{\'o} CELLEX Barcelona, Fundaci{\'o} Mir-Puig, Ajuntament de Barcelona, Agencia Estatal de Investigaci{\'o}n (PHOTOMETABO, PID2019-106481RB-C31/10.13039/501100011033), the {"}Severo Ochoa{"} Programme for Centers of Excellence in R&D (CEX2019-000910-S), the Obra social “La Caixa” Foundation (LlumMedBcn), Generalitat de Catalunya (CERCA, AGAUR-2017-SGR-1380, RIS3CAT-001-P-001682 CECH), European Commission Horizon 2020 (FEDER, 688303/LUCA, 101016087/VASCOVID, 87114/LASERLAB-EUROPE V). We also acknowledge the collaboration and an instrument loan from Artinis (Netherlands). Funding Information: The members of the HEMOCOVID-19 Consortium are listed as ICFO-Institute of Photonic Sciences?ICFO: Turgut Durduran, Marco Pagliazzi, Lorenzo Cortese, Marta Zanoletti, and Umut Karadeniz. Parc Taul? Hospital Universitari (Spain): Jaume Mesquida, Alba Caballer, Sara Nogales, Cristina Espinal, Guillem Gruartmoner. Hospital del Mar-IMIM (Spain): Judith Marin Corral, Puri P?rez Ter?n, Clara Vil?, Luc?a Picazo. Hospital Vall D?Hebron (Spain): Ricard Ferrer, Marina Garc?a De Acilu, Luis Chiscano, Abraham Mera. Hospital Cl?nic de Barcelona (Spain): Pedro Castro, Adri?n T?llez, Sara Fern?ndez, Ana Matas, Fernando Fuentes. Centre de Recerca Matem?tica (Spain): Isabel Serra, David Romero, Francesc Font, Tim Myers. University of Texas Southwestern Medical Center (USA): David R. Busch, Siddharth Dave, Sreekanth Cheruku, Christopher Choi, Peiman Lahsaei, DaiWai Olson. Hospital General De M?xico (Mexico): Argelia P?rez Pacheco, Ra?l Serrano Loyola, Ver?nica Carbajal Robles, Rosa Mar?a Quispe Siccha, Enrique Santillan Aguayo, Melvin Parada Guzm?n, Eduardo Liceaga, F?lix Jerandy?Monte De Oca Hern?ndez. Hospital Das Cl?nicas University of Sao Paulo Medical School (Brazil): Bruno Adler Maccagnan Pinheiro Besen, Leandro Utino Taniguchi, Pedro Vitale Mendes. Institute of Physics, University of Campinas (Brazil): Rickson Coelho Mesquita, Rodrigo Menezes Forti, Andr?s Fabi?n Quiroga Soto. Clinical Hospital, University of Campinas (Brazil): Italo Karmann Aventurato, La?s Bacchin de Oliveira, Lilian Elisabete Bernardes Delazari?, Gabriela L?vio Em?dio, L?gia dos Santos, Roceto Ratti, Antonio Luis Eiras Falc?o. Collaborating authors: Sara Nogales, Cristina Espinal, Guillem Gruartmoner, Judith Marin-Corral, Puri Perez-Teran, Luc?a Picazo, Ricard Ferrer, Luis Chiscano, Abraham Mera, Adri?n T?llez, Sara Fern?ndez, Ana Matas, Fernando Fuentes, Ra?l Serrano-Loyola, Ver?nica Carbajal-Robles, Rosa M. Quispe-Siccha, Enrique Santillan-Aguayo, Melvin Parada-Guzm?n, Eduardo Liceaga, F?lix J. Monte-De-Oca, Bruno A. Besen, Leandro U. Taniguchi, Pedro V. Mendes, Rodrigo Menezes-Forti, Andr?s F. Quiroga, Italo Karmann, Luis Bacchin, Lilian E. Bernardes, Gabriela L?vio-Emidio, L?gia dos Santos, Roceto Ratti, Antonio L. Eiras-Falcao. Publisher Copyright: {\textcopyright} 2021, The Author(s).",

year = "2021",

month = dec,

doi = "10.1186/s13054-021-03803-2",

language = "English (US)",

volume = "25",

journal = "Critical Care",

issn = "1364-8535",

publisher = "Springer Science + Business Media",

number = "1",

}

TY - JOUR

T1 - Peripheral microcirculatory alterations are associated with the severity of acute respiratory distress syndrome in COVID-19 patients admitted to intermediate respiratory and intensive care units

AU - the HEMOCOVID-19 Consortium

AU - Mesquida, Jaume

AU - Caballer, A.

AU - Cortese, L.

AU - Vila, C.

AU - Karadeniz, U.

AU - Pagliazzi, M.

AU - Zanoletti, M.

AU - Pacheco, A. Pérez

AU - Castro, P.

AU - García-de-Acilu, M.

AU - Mesquita, R. C.

AU - Busch, D. R.

AU - Durduran, T.

AU - Durduran, Turgut

AU - Pagliazzi, Marco

AU - Cortese, Lorenzo

AU - Zanoletti, Marta

AU - Karadeniz, Umut

AU - Mesquida, Jaume

AU - Caballer, Alba

AU - Nogales, Sara

AU - Espinal, Cristina

AU - Gruartmoner, Guillem

AU - Terán, Puri Pérez

AU - Vilà, Clara

AU - Picazo, Lucía

AU - Ferrer, Ricard

AU - De Acilu, Marina García

AU - Chiscano, Luis

AU - Mera, Abraham

AU - Castro, Pedro

AU - Téllez, Adrián

AU - Fernández, Sara

AU - Matas, Ana

AU - Fuentes, Fernando

AU - Serra, Isabel

AU - Romero, David

AU - Font, Francesc

AU - Myers, Tim

AU - Busch, David R.

AU - Dave, Siddharth

AU - Cheruku, Sreekanth

AU - Choi, Christopher

AU - Lahsaei, Peiman

AU - Olson, Dai Wai

AU - Pacheco, Argelia Pérez

AU - Quispe Siccha, Rosa María

AU - Liceaga, Eduardo

AU - De Oca Hernández, Félix Jerandy Monte

AU - Besen, Bruno Adler Maccagnan Pinheiro

N1 - Funding Information: The study has received funding from Fundació CELLEX Barcelona, Fundació Mir-Puig, Ajuntament de Barcelona, Agencia Estatal de Investigación (PHOTOMETABO, PID2019-106481RB-C31/10.13039/501100011033), the "Severo Ochoa" Programme for Centers of Excellence in R&D (CEX2019-000910-S), the Obra social “La Caixa” Foundation (LlumMedBcn), Generalitat de Catalunya (CERCA, AGAUR-2017-SGR-1380, RIS3CAT-001-P-001682 CECH), European Commission Horizon 2020 (FEDER, 688303/LUCA, 101016087/VASCOVID, 87114/LASERLAB-EUROPE V). We also acknowledge the collaboration and an instrument loan from Artinis (Netherlands). Funding Information: The members of the HEMOCOVID-19 Consortium are listed as ICFO-Institute of Photonic Sciences?ICFO: Turgut Durduran, Marco Pagliazzi, Lorenzo Cortese, Marta Zanoletti, and Umut Karadeniz. Parc Taul? Hospital Universitari (Spain): Jaume Mesquida, Alba Caballer, Sara Nogales, Cristina Espinal, Guillem Gruartmoner. Hospital del Mar-IMIM (Spain): Judith Marin Corral, Puri P?rez Ter?n, Clara Vil?, Luc?a Picazo. Hospital Vall D?Hebron (Spain): Ricard Ferrer, Marina Garc?a De Acilu, Luis Chiscano, Abraham Mera. Hospital Cl?nic de Barcelona (Spain): Pedro Castro, Adri?n T?llez, Sara Fern?ndez, Ana Matas, Fernando Fuentes. Centre de Recerca Matem?tica (Spain): Isabel Serra, David Romero, Francesc Font, Tim Myers. University of Texas Southwestern Medical Center (USA): David R. Busch, Siddharth Dave, Sreekanth Cheruku, Christopher Choi, Peiman Lahsaei, DaiWai Olson. Hospital General De M?xico (Mexico): Argelia P?rez Pacheco, Ra?l Serrano Loyola, Ver?nica Carbajal Robles, Rosa Mar?a Quispe Siccha, Enrique Santillan Aguayo, Melvin Parada Guzm?n, Eduardo Liceaga, F?lix Jerandy?Monte De Oca Hern?ndez. Hospital Das Cl?nicas University of Sao Paulo Medical School (Brazil): Bruno Adler Maccagnan Pinheiro Besen, Leandro Utino Taniguchi, Pedro Vitale Mendes. Institute of Physics, University of Campinas (Brazil): Rickson Coelho Mesquita, Rodrigo Menezes Forti, Andr?s Fabi?n Quiroga Soto. Clinical Hospital, University of Campinas (Brazil): Italo Karmann Aventurato, La?s Bacchin de Oliveira, Lilian Elisabete Bernardes Delazari?, Gabriela L?vio Em?dio, L?gia dos Santos, Roceto Ratti, Antonio Luis Eiras Falc?o. Collaborating authors: Sara Nogales, Cristina Espinal, Guillem Gruartmoner, Judith Marin-Corral, Puri Perez-Teran, Luc?a Picazo, Ricard Ferrer, Luis Chiscano, Abraham Mera, Adri?n T?llez, Sara Fern?ndez, Ana Matas, Fernando Fuentes, Ra?l Serrano-Loyola, Ver?nica Carbajal-Robles, Rosa M. Quispe-Siccha, Enrique Santillan-Aguayo, Melvin Parada-Guzm?n, Eduardo Liceaga, F?lix J. Monte-De-Oca, Bruno A. Besen, Leandro U. Taniguchi, Pedro V. Mendes, Rodrigo Menezes-Forti, Andr?s F. Quiroga, Italo Karmann, Luis Bacchin, Lilian E. Bernardes, Gabriela L?vio-Emidio, L?gia dos Santos, Roceto Ratti, Antonio L. Eiras-Falcao. Publisher Copyright: © 2021, The Author(s).

PY - 2021/12

Y1 - 2021/12

N2 - Background: COVID-19 is primarily a respiratory disease; however, there is also evidence that it causes endothelial damage in the microvasculature of several organs. The aim of the present study is to characterize in vivo the microvascular reactivity in peripheral skeletal muscle of severe COVID-19 patients. Methods: This is a prospective observational study carried out in Spain, Mexico and Brazil. Healthy subjects and severe COVID-19 patients admitted to the intermediate respiratory (IRCU) and intensive care units (ICU) due to hypoxemia were studied. Local tissue/blood oxygen saturation (StO2) and local hemoglobin concentration (THC) were non-invasively measured on the forearm by near-infrared spectroscopy (NIRS). A vascular occlusion test (VOT), a three-minute induced ischemia, was performed in order to obtain dynamic StO2 parameters: deoxygenation rate (DeO2), reoxygenation rate (ReO2), and hyperemic response (HAUC). In COVID-19 patients, the severity of ARDS was evaluated by the ratio between peripheral arterial oxygen saturation (SpO2) and the fraction of inspired oxygen (FiO2) (SF ratio). Results: Healthy controls (32) and COVID-19 patients (73) were studied. Baseline StO2 and THC did not differ between the two groups. Dynamic VOT-derived parameters were significantly impaired in COVID-19 patients showing lower metabolic rate (DeO2) and diminished endothelial reactivity. At enrollment, most COVID-19 patients were receiving invasive mechanical ventilation (MV) (53%) or high-flow nasal cannula support (32%). Patients on MV were also receiving sedative agents (100%) and vasopressors (29%). Baseline StO2 and DeO2 negatively correlated with SF ratio, while ReO2 showed a positive correlation with SF ratio. There were significant differences in baseline StO2 and ReO2 among the different ARDS groups according to SF ratio, but not among different respiratory support therapies. Conclusion: Patients with severe COVID-19 show systemic microcirculatory alterations suggestive of endothelial dysfunction, and these alterations are associated with the severity of ARDS. Further evaluation is needed to determine whether these observations have prognostic implications. These results represent interim findings of the ongoing HEMOCOVID-19 trial. Trial registration ClinicalTrials.gov NCT04689477. Retrospectively registered 30 December 2020.

AB - Background: COVID-19 is primarily a respiratory disease; however, there is also evidence that it causes endothelial damage in the microvasculature of several organs. The aim of the present study is to characterize in vivo the microvascular reactivity in peripheral skeletal muscle of severe COVID-19 patients. Methods: This is a prospective observational study carried out in Spain, Mexico and Brazil. Healthy subjects and severe COVID-19 patients admitted to the intermediate respiratory (IRCU) and intensive care units (ICU) due to hypoxemia were studied. Local tissue/blood oxygen saturation (StO2) and local hemoglobin concentration (THC) were non-invasively measured on the forearm by near-infrared spectroscopy (NIRS). A vascular occlusion test (VOT), a three-minute induced ischemia, was performed in order to obtain dynamic StO2 parameters: deoxygenation rate (DeO2), reoxygenation rate (ReO2), and hyperemic response (HAUC). In COVID-19 patients, the severity of ARDS was evaluated by the ratio between peripheral arterial oxygen saturation (SpO2) and the fraction of inspired oxygen (FiO2) (SF ratio). Results: Healthy controls (32) and COVID-19 patients (73) were studied. Baseline StO2 and THC did not differ between the two groups. Dynamic VOT-derived parameters were significantly impaired in COVID-19 patients showing lower metabolic rate (DeO2) and diminished endothelial reactivity. At enrollment, most COVID-19 patients were receiving invasive mechanical ventilation (MV) (53%) or high-flow nasal cannula support (32%). Patients on MV were also receiving sedative agents (100%) and vasopressors (29%). Baseline StO2 and DeO2 negatively correlated with SF ratio, while ReO2 showed a positive correlation with SF ratio. There were significant differences in baseline StO2 and ReO2 among the different ARDS groups according to SF ratio, but not among different respiratory support therapies. Conclusion: Patients with severe COVID-19 show systemic microcirculatory alterations suggestive of endothelial dysfunction, and these alterations are associated with the severity of ARDS. Further evaluation is needed to determine whether these observations have prognostic implications. These results represent interim findings of the ongoing HEMOCOVID-19 trial. Trial registration ClinicalTrials.gov NCT04689477. Retrospectively registered 30 December 2020.

KW - COVID-19

KW - Endothelial dysfunction

KW - Microcirculation

KW - Near-infrared spectroscopy

UR - http://www.scopus.com/inward/record.url?scp=85118840727&partnerID=8YFLogxK

UR - http://www.scopus.com/inward/citedby.url?scp=85118840727&partnerID=8YFLogxK

U2 - 10.1186/s13054-021-03803-2

DO - 10.1186/s13054-021-03803-2

M3 - Article

C2 - 34749792

AN - SCOPUS:85118840727

SN - 1364-8535

VL - 25

JO - Critical Care

JF - Critical Care

IS - 1

M1 - 381

ER -

Peripheral microcirculatory alterations are associated with the severity of acute respiratory distress syndrome in COVID-19 patients admitted to intermediate respiratory and intensive care units

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