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Relevance of TMPRSS2, CD163/CD206, and CD33 in clinical severity stratification of COVID-19.
Martínez-Diz, Silvia; Marín-Benesiu, Fernando; López-Torres, Ginesa; Santiago, Olivia; Díaz-Cuéllar, José F; Martín-Esteban, Sara; Cortés-Valverde, Ana I; Arenas-Rodríguez, Verónica; Cuenca-López, Sergio; Porras-Quesada, Patricia; Ruiz-Ruiz, Carmen; Abadía-Molina, Ana C; Entrala-Bernal, Carmen; Martínez-González, Luis J; Álvarez-Cubero, Maria Jesus.
  • Martínez-Diz S; Preventive Medicine and Public Health Service, Hospital Universitario Clínico San Cecilio, Granada, Spain.
  • Marín-Benesiu F; GENYO, Center for Genomics and Oncological Research, Granada, Spain.
  • López-Torres G; Department of Biochemistry, Molecular Biology III and Immunology, Faculty of Medicine, University of Granada, Granada, Spain.
  • Santiago O; Casería de Montijo Health Center, Granada Health District, Granada, Spain.
  • Díaz-Cuéllar JF; GENYO, Center for Genomics and Oncological Research, Granada, Spain.
  • Martín-Esteban S; GENYO, Center for Genomics and Oncological Research, Granada, Spain.
  • Cortés-Valverde AI; Loja Health Center, Metropolitan District of Granada, Loja, Spain.
  • Arenas-Rodríguez V; Casería de Montijo Health Center, Granada Health District, Granada, Spain.
  • Cuenca-López S; GENYO, Center for Genomics and Oncological Research, Granada, Spain.
  • Porras-Quesada P; GENYO, Center for Genomics and Oncological Research, Granada, Spain.
  • Ruiz-Ruiz C; GENYO, Center for Genomics and Oncological Research, Granada, Spain.
  • Abadía-Molina AC; Department of Biochemistry, Molecular Biology III and Immunology, Faculty of Medicine, University of Granada, Granada, Spain.
  • Entrala-Bernal C; Immunology Unit, Institute of Regenerative Biomedicine (IBIMER), Center for Biomedical Research Center (CIBM), University of Granada, Granada, Spain.
  • Martínez-González LJ; Department of Biochemistry, Molecular Biology III and Immunology, Faculty of Medicine, University of Granada, Granada, Spain.
  • Álvarez-Cubero MJ; Immunology Unit, Institute of Regenerative Biomedicine (IBIMER), Center for Biomedical Research Center (CIBM), University of Granada, Granada, Spain.
Front Immunol ; 13: 1094644, 2022.
Article in English | MEDLINE | ID: covidwho-2309812
ABSTRACT

Background:

Approximately 13.8% and 6.1% of coronavirus disease 2019 (COVID-19) patients require hospitalization and sometimes intensive care unit (ICU) admission, respectively. There is no biomarker to predict which of these patients will develop an aggressive stage that we could improve their quality of life and healthcare management. Our main goal is to include new markers for the classification of COVID-19 patients.

Methods:

Two tubes of peripheral blood were collected from a total of 66 (n = 34 mild and n = 32 severe) samples (mean age 52 years). Cytometry analysis was performed using a 15-parameter panel included in the Maxpar® Human Monocyte/Macrophage Phenotyping Panel Kit. Cytometry by time-of-flight mass spectrometry (CyTOF) panel was performed in combination with genetic analysis using TaqMan® probes for ACE2 (rs2285666), MX1 (rs469390), and TMPRSS2 (rs2070788) variants. GemStone™ and OMIQ software were used for cytometry analysis.

Results:

The frequency of CD163+/CD206- population of transitional monocytes (T-Mo) was decreased in the mild group compared to that of the severe one, while T-Mo CD163-/CD206- were increased in the mild group compared to that of the severe one. In addition, we also found differences in CD11b expression in CD14dim monocytes in the severe group, with decreased levels in the female group (p = 0.0412). When comparing mild and severe disease, we also found that CD45- [p = 0.014; odds ratio (OR) = 0.286, 95% CI 0.104-0.787] and CD14dim/CD33+ (p = 0.014; OR = 0.286, 95% CI 0.104-0.787) monocytes were the best options as biomarkers to discriminate between these patient groups. CD33 was also indicated as a good biomarker for patient stratification by the analysis of GemStone™ software. Among genetic markers, we found that G carriers of TMPRSS2 (rs2070788) have an increased risk (p = 0.02; OR = 3.37, 95% CI 1.18-9.60) of severe COVID-19 compared to those with A/A genotype. This strength is further increased when combined with CD45-, T-Mo CD163+/CD206-, and C14dim/CD33+.

Conclusions:

Here, we report the interesting role of TMPRSS2, CD45-, CD163/CD206, and CD33 in COVID-19 aggressiveness. This strength is reinforced for aggressiveness biomarkers when TMPRSS2 and CD45-, TMPRSS2 and CD163/CD206, and TMPRSS2 and CD14dim/CD33+ are combined.
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Full text: Available Collection: International databases Database: MEDLINE Main subject: Quality of Life / COVID-19 Type of study: Experimental Studies / Prognostic study / Randomized controlled trials Topics: Variants Limits: Female / Humans / Middle aged Language: English Journal: Front Immunol Year: 2022 Document Type: Article Affiliation country: Fimmu.2022.1094644

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Full text: Available Collection: International databases Database: MEDLINE Main subject: Quality of Life / COVID-19 Type of study: Experimental Studies / Prognostic study / Randomized controlled trials Topics: Variants Limits: Female / Humans / Middle aged Language: English Journal: Front Immunol Year: 2022 Document Type: Article Affiliation country: Fimmu.2022.1094644