Increased expression of hypoxia-induced factor 1α mRNA and its related genes in myeloid blood cells from critically ill COVID-19 patients

BACKGROUND: COVID-19 counts 46 million people infected and killed more than 1.2 million. Hypoxaemia is one of the main clinical manifestations, especially in severe cases. HIF1α is a master transcription factor involved in the cellular response to oxygen levels. The immunopathogenesis of this severe...

Descripción completa

Detalles Bibliográficos
Autores principales: Taniguchi-Ponciano, Keiko, Vadillo, Eduardo, Mayani, Héctor, Gonzalez-Bonilla, César Raúl, Torres, Javier, Majluf, Abraham, Flores-Padilla, Guillermo, Wacher-Rodarte, Niels, Galan, Juan Carlos, Ferat-Osorio, Eduardo, Blanco-Favela, Francisco, Lopez-Macias, Constantino, Ferreira-Hermosillo, Aldo, Ramirez-Renteria, Claudia, Peña-Martínez, Eduardo, Silva-Román, Gloria, Vela-Patiño, Sandra, Mata-Lozano, Carlos, Carvente-Garcia, Roberto, Basurto-Acevedo, Lourdes, Saucedo, Renata, Piña-Sanchez, Patricia, Chavez-Gonzalez, Antonieta, Marrero-Rodríguez, Daniel, Mercado, Moisés
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Taylor & Francis 2020
Materias:
Immunology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7784832/
https://www.ncbi.nlm.nih.gov/pubmed/33345622
http://dx.doi.org/10.1080/07853890.2020.1858234
_version_ 1783632361672409088
author Taniguchi-Ponciano, Keiko
Vadillo, Eduardo
Mayani, Héctor
Gonzalez-Bonilla, César Raúl
Torres, Javier
Majluf, Abraham
Flores-Padilla, Guillermo
Wacher-Rodarte, Niels
Galan, Juan Carlos
Ferat-Osorio, Eduardo
Blanco-Favela, Francisco
Lopez-Macias, Constantino
Ferreira-Hermosillo, Aldo
Ramirez-Renteria, Claudia
Peña-Martínez, Eduardo
Silva-Román, Gloria
Vela-Patiño, Sandra
Mata-Lozano, Carlos
Carvente-Garcia, Roberto
Basurto-Acevedo, Lourdes
Saucedo, Renata
Piña-Sanchez, Patricia
Chavez-Gonzalez, Antonieta
Marrero-Rodríguez, Daniel
Mercado, Moisés
author_facet Taniguchi-Ponciano, Keiko
Vadillo, Eduardo
Mayani, Héctor
Gonzalez-Bonilla, César Raúl
Torres, Javier
Majluf, Abraham
Flores-Padilla, Guillermo
Wacher-Rodarte, Niels
Galan, Juan Carlos
Ferat-Osorio, Eduardo
Blanco-Favela, Francisco
Lopez-Macias, Constantino
Ferreira-Hermosillo, Aldo
Ramirez-Renteria, Claudia
Peña-Martínez, Eduardo
Silva-Román, Gloria
Vela-Patiño, Sandra
Mata-Lozano, Carlos
Carvente-Garcia, Roberto
Basurto-Acevedo, Lourdes
Saucedo, Renata
Piña-Sanchez, Patricia
Chavez-Gonzalez, Antonieta
Marrero-Rodríguez, Daniel
Mercado, Moisés
author_sort Taniguchi-Ponciano, Keiko
collection PubMed
description BACKGROUND: COVID-19 counts 46 million people infected and killed more than 1.2 million. Hypoxaemia is one of the main clinical manifestations, especially in severe cases. HIF1α is a master transcription factor involved in the cellular response to oxygen levels. The immunopathogenesis of this severe form of COVID-19 is poorly understood. METHODS: We performed scRNAseq from leukocytes from five critically ill COVID-19 patients and characterized the expression of hypoxia-inducible factor1α and its transcriptionally regulated genes. Also performed metanalysis from the publicly available RNAseq data from COVID-19 bronchoalveolar cells. RESULTS: Critically-ill COVID-19 patients show a shift towards an immature myeloid profile in peripheral blood cells, including band neutrophils, immature monocytes, metamyelocytes, monocyte-macrophages, monocytoid precursors, and promyelocytes-myelocytes, together with mature monocytes and segmented neutrophils. May be the result of a physiological response known as emergency myelopoiesis. These cellular subsets and bronchoalveolar cells express HIF1α and their transcriptional targets related to inflammation (CXCL8, CXCR1, CXCR2, and CXCR4); virus sensing, (TLR2 and TLR4); and metabolism (SLC2A3, PFKFB3, PGK1, GAPDH and SOD2). CONCLUSIONS: The up-regulation and participation of HIF1α in events such as inflammation, immunometabolism, and TLR make it a potential molecular marker for COVID-19 severity and, interestingly, could represent a potential target for molecular therapy. KEY MESSAGES: Critically ill COVID-19 patients show emergency myelopoiesis. HIF1α and its transcriptionally regulated genes are expressed in immature myeloid cells which could serve as molecular targets. HIF1α and its transcriptionally regulated genes is also expressed in lung cells from critically ill COVID-19 patients which may partially explain the hypoxia related events.
format Online
Article
Text
id pubmed-7784832
institution National Center for Biotechnology Information
language English
publishDate 2020
publisher Taylor & Francis
record_format MEDLINE/PubMed
spelling pubmed-77848322021-01-05 Increased expression of hypoxia-induced factor 1α mRNA and its related genes in myeloid blood cells from critically ill COVID-19 patients Taniguchi-Ponciano, Keiko Vadillo, Eduardo Mayani, Héctor Gonzalez-Bonilla, César Raúl Torres, Javier Majluf, Abraham Flores-Padilla, Guillermo Wacher-Rodarte, Niels Galan, Juan Carlos Ferat-Osorio, Eduardo Blanco-Favela, Francisco Lopez-Macias, Constantino Ferreira-Hermosillo, Aldo Ramirez-Renteria, Claudia Peña-Martínez, Eduardo Silva-Román, Gloria Vela-Patiño, Sandra Mata-Lozano, Carlos Carvente-Garcia, Roberto Basurto-Acevedo, Lourdes Saucedo, Renata Piña-Sanchez, Patricia Chavez-Gonzalez, Antonieta Marrero-Rodríguez, Daniel Mercado, Moisés Ann Med Immunology BACKGROUND: COVID-19 counts 46 million people infected and killed more than 1.2 million. Hypoxaemia is one of the main clinical manifestations, especially in severe cases. HIF1α is a master transcription factor involved in the cellular response to oxygen levels. The immunopathogenesis of this severe form of COVID-19 is poorly understood. METHODS: We performed scRNAseq from leukocytes from five critically ill COVID-19 patients and characterized the expression of hypoxia-inducible factor1α and its transcriptionally regulated genes. Also performed metanalysis from the publicly available RNAseq data from COVID-19 bronchoalveolar cells. RESULTS: Critically-ill COVID-19 patients show a shift towards an immature myeloid profile in peripheral blood cells, including band neutrophils, immature monocytes, metamyelocytes, monocyte-macrophages, monocytoid precursors, and promyelocytes-myelocytes, together with mature monocytes and segmented neutrophils. May be the result of a physiological response known as emergency myelopoiesis. These cellular subsets and bronchoalveolar cells express HIF1α and their transcriptional targets related to inflammation (CXCL8, CXCR1, CXCR2, and CXCR4); virus sensing, (TLR2 and TLR4); and metabolism (SLC2A3, PFKFB3, PGK1, GAPDH and SOD2). CONCLUSIONS: The up-regulation and participation of HIF1α in events such as inflammation, immunometabolism, and TLR make it a potential molecular marker for COVID-19 severity and, interestingly, could represent a potential target for molecular therapy. KEY MESSAGES: Critically ill COVID-19 patients show emergency myelopoiesis. HIF1α and its transcriptionally regulated genes are expressed in immature myeloid cells which could serve as molecular targets. HIF1α and its transcriptionally regulated genes is also expressed in lung cells from critically ill COVID-19 patients which may partially explain the hypoxia related events. Taylor & Francis 2020-12-21 /pmc/articles/PMC7784832/ /pubmed/33345622 http://dx.doi.org/10.1080/07853890.2020.1858234 Text en © 2020 The Author(s). Published by Informa UK Limited, trading as Taylor & Francis Group https://creativecommons.org/licenses/by/4.0/This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0/ (https://creativecommons.org/licenses/by/4.0/) ), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Immunology
Taniguchi-Ponciano, Keiko
Vadillo, Eduardo
Mayani, Héctor
Gonzalez-Bonilla, César Raúl
Torres, Javier
Majluf, Abraham
Flores-Padilla, Guillermo
Wacher-Rodarte, Niels
Galan, Juan Carlos
Ferat-Osorio, Eduardo
Blanco-Favela, Francisco
Lopez-Macias, Constantino
Ferreira-Hermosillo, Aldo
Ramirez-Renteria, Claudia
Peña-Martínez, Eduardo
Silva-Román, Gloria
Vela-Patiño, Sandra
Mata-Lozano, Carlos
Carvente-Garcia, Roberto
Basurto-Acevedo, Lourdes
Saucedo, Renata
Piña-Sanchez, Patricia
Chavez-Gonzalez, Antonieta
Marrero-Rodríguez, Daniel
Mercado, Moisés
Increased expression of hypoxia-induced factor 1α mRNA and its related genes in myeloid blood cells from critically ill COVID-19 patients
title Increased expression of hypoxia-induced factor 1α mRNA and its related genes in myeloid blood cells from critically ill COVID-19 patients
title_full Increased expression of hypoxia-induced factor 1α mRNA and its related genes in myeloid blood cells from critically ill COVID-19 patients
title_fullStr Increased expression of hypoxia-induced factor 1α mRNA and its related genes in myeloid blood cells from critically ill COVID-19 patients
title_full_unstemmed Increased expression of hypoxia-induced factor 1α mRNA and its related genes in myeloid blood cells from critically ill COVID-19 patients
title_short Increased expression of hypoxia-induced factor 1α mRNA and its related genes in myeloid blood cells from critically ill COVID-19 patients
title_sort increased expression of hypoxia-induced factor 1α mrna and its related genes in myeloid blood cells from critically ill covid-19 patients
topic Immunology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7784832/
https://www.ncbi.nlm.nih.gov/pubmed/33345622
http://dx.doi.org/10.1080/07853890.2020.1858234
work_keys_str_mv AT taniguchiponcianokeiko increasedexpressionofhypoxiainducedfactor1amrnaanditsrelatedgenesinmyeloidbloodcellsfromcriticallyillcovid19patients
AT vadilloeduardo increasedexpressionofhypoxiainducedfactor1amrnaanditsrelatedgenesinmyeloidbloodcellsfromcriticallyillcovid19patients
AT mayanihector increasedexpressionofhypoxiainducedfactor1amrnaanditsrelatedgenesinmyeloidbloodcellsfromcriticallyillcovid19patients
AT gonzalezbonillacesarraul increasedexpressionofhypoxiainducedfactor1amrnaanditsrelatedgenesinmyeloidbloodcellsfromcriticallyillcovid19patients
AT torresjavier increasedexpressionofhypoxiainducedfactor1amrnaanditsrelatedgenesinmyeloidbloodcellsfromcriticallyillcovid19patients
AT majlufabraham increasedexpressionofhypoxiainducedfactor1amrnaanditsrelatedgenesinmyeloidbloodcellsfromcriticallyillcovid19patients
AT florespadillaguillermo increasedexpressionofhypoxiainducedfactor1amrnaanditsrelatedgenesinmyeloidbloodcellsfromcriticallyillcovid19patients
AT wacherrodarteniels increasedexpressionofhypoxiainducedfactor1amrnaanditsrelatedgenesinmyeloidbloodcellsfromcriticallyillcovid19patients
AT galanjuancarlos increasedexpressionofhypoxiainducedfactor1amrnaanditsrelatedgenesinmyeloidbloodcellsfromcriticallyillcovid19patients
AT feratosorioeduardo increasedexpressionofhypoxiainducedfactor1amrnaanditsrelatedgenesinmyeloidbloodcellsfromcriticallyillcovid19patients
AT blancofavelafrancisco increasedexpressionofhypoxiainducedfactor1amrnaanditsrelatedgenesinmyeloidbloodcellsfromcriticallyillcovid19patients
AT lopezmaciasconstantino increasedexpressionofhypoxiainducedfactor1amrnaanditsrelatedgenesinmyeloidbloodcellsfromcriticallyillcovid19patients
AT ferreirahermosilloaldo increasedexpressionofhypoxiainducedfactor1amrnaanditsrelatedgenesinmyeloidbloodcellsfromcriticallyillcovid19patients
AT ramirezrenteriaclaudia increasedexpressionofhypoxiainducedfactor1amrnaanditsrelatedgenesinmyeloidbloodcellsfromcriticallyillcovid19patients
AT penamartinezeduardo increasedexpressionofhypoxiainducedfactor1amrnaanditsrelatedgenesinmyeloidbloodcellsfromcriticallyillcovid19patients
AT silvaromangloria increasedexpressionofhypoxiainducedfactor1amrnaanditsrelatedgenesinmyeloidbloodcellsfromcriticallyillcovid19patients
AT velapatinosandra increasedexpressionofhypoxiainducedfactor1amrnaanditsrelatedgenesinmyeloidbloodcellsfromcriticallyillcovid19patients
AT matalozanocarlos increasedexpressionofhypoxiainducedfactor1amrnaanditsrelatedgenesinmyeloidbloodcellsfromcriticallyillcovid19patients
AT carventegarciaroberto increasedexpressionofhypoxiainducedfactor1amrnaanditsrelatedgenesinmyeloidbloodcellsfromcriticallyillcovid19patients
AT basurtoacevedolourdes increasedexpressionofhypoxiainducedfactor1amrnaanditsrelatedgenesinmyeloidbloodcellsfromcriticallyillcovid19patients
AT saucedorenata increasedexpressionofhypoxiainducedfactor1amrnaanditsrelatedgenesinmyeloidbloodcellsfromcriticallyillcovid19patients
AT pinasanchezpatricia increasedexpressionofhypoxiainducedfactor1amrnaanditsrelatedgenesinmyeloidbloodcellsfromcriticallyillcovid19patients
AT chavezgonzalezantonieta increasedexpressionofhypoxiainducedfactor1amrnaanditsrelatedgenesinmyeloidbloodcellsfromcriticallyillcovid19patients
AT marrerorodriguezdaniel increasedexpressionofhypoxiainducedfactor1amrnaanditsrelatedgenesinmyeloidbloodcellsfromcriticallyillcovid19patients
AT mercadomoises increasedexpressionofhypoxiainducedfactor1amrnaanditsrelatedgenesinmyeloidbloodcellsfromcriticallyillcovid19patients

Ejemplares similares