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Different polarization and functionality of CD4+ T helper subsets in people with post-COVID condition

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https://hdl.handle.net/20.500.12080/50960
dc.contributor.author Sánchez-Menéndez, Clara
dc.contributor.author de la Calle-Jiménez, Olivia
dc.contributor.author Mateos, Elena
dc.contributor.author Vigón, Lorena
dc.contributor.author Fuertes, Daniel
dc.contributor.author Murciano Antón, María Aranzazu
dc.contributor.author San José, Esther
dc.contributor.author García-Gutiérrez, Valentín
dc.contributor.author Cervero, Miguel
dc.contributor.author Torres, Montserrat
dc.contributor.author Coiras, Mayte
dc.date.accessioned 2025-11-18T10:31:40Z
dc.date.available 2025-11-18T10:31:40Z
dc.date.created 2024
dc.date.issued 2024
dc.identifier.uri https://hdl.handle.net/20.500.12080/50960
dc.description.abstract Introduction: After mild COVID-19 that does not require hospitalization, some individuals develop persistent symptoms that may worsen over time, producing a multisystemic condition termed Post-COVID condition (PCC). Among other disorders, PCC is characterized by persistent changes in the immune system that may not be solved several months after COVID-19 diagnosis. Methods: People with PCC were recruited to determine the distribution and functionality of CD4+ T helper (Th) subsets in comparison with individuals with mild, severe, and critical presentations of acute COVID-19 to evaluate their contribution as risk or protective factors for PCC. Results: People with PCC showed low levels of Th1 cells, similar to individuals with severe and critical COVID-19, although these cells presented a higher capacity to express IFNg in response to stimulation. Th2/Th1 correlation was negative in individuals with acute forms of COVID-19, but there was no significant Th2/Th1 correlation in people with PCC. Th2 cells from people with PCC presented high capacity to express IL-4 and IL-13, which are related to low ventilation and death associated with COVID-19. Levels of proinflammatory Th9 and Th17 subsets were significantly higher in people with PCC in comparison with acute COVID-19, being Th1/Th9 correlation negative in these individuals, which probably contributed to a more pro-inflammatory than antiviral scenario. Th17 cells from approximately 50% of individuals with PCC had no capacity to express IL-17A and IL-22, similar to individuals with critical COVID-19, which would prevent clearing extracellular pathogens. Th2/Th17 correlation waspositive in people with PCC, which in the absence of negative Th1/Th2 correlation could also contribute to the proinflammatory state. Finally, Th22 cells from most individuals with PCC had no capacity to express IL-13 or IL-22, which could increase tendency to reinfections due to impaired epithelial regeneration. Discussion: People with PCC showed skewed polarization of CD4+ Th subsets with altered functionality that was more similar to individuals with severe and critical presentations of acute COVID-19 than to people who fully recovered from mild disease. New strategies aimed at reprogramming the immune response and redirecting CD4+ Th cell polarization may be necessary to reduce the proinflammatory environment characteristic of PCC. es_ES
dc.format application/pdf es_ES
dc.language eng es_ES
dc.publisher Frontiers es_ES
dc.rights CC-BY es_ES
dc.rights.uri http://creativecommons.org/licenses/by/4.0/deed.es es_ES
dc.source Frontiers in Immunology es_ES
dc.title Different polarization and functionality of CD4+ T helper subsets in people with post-COVID condition es_ES
dc.type Artículo es_ES
dc.description.curso 2024 es_ES
dc.rights.accessrights info:eu-repo/semantics/openAccess es_ES
dc.identifier.dl 2024
dc.identifier.location N/A es_ES


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