The percentage of CD39+ monocytes is higher in pregnant COVID-19+ patients than in nonpregnant COVID-19+ patients

妊娠期新冠病毒感染患者体内CD39+单核细胞的百分比高于非妊娠期新冠病毒感染患者。

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作者:A Cérbulo-Vázquez ,M García-Espinosa ,J C Briones-Garduño ,L Arriaga-Pizano ,E Ferat-Osorio ,B Zavala-Barrios ,G L Cabrera-Rivera ,P Miranda-Cruz ,M T García de la Rosa ,J L Prieto-Chávez ,V Rivero-Arredondo ,R L Madera-Sandoval ,A Cruz-Cruz ,E Salazar-Rios ,M E Salazar-Rios ,D Serrano-Molina ,R C De Lira-Barraza ,A H Villanueva-Compean ,A Esquivel-Pineda ,R Ramirez-Montes de Oca ,F Caldiño-Soto ,L A Ramírez-García ,G Flores-Padilla ,O Moreno-Álvarez ,G M L Guerrero-Avendaño ,C López-Macías

Abstract

Current medical guidelines consider pregnant women with COVID-19 to be a high-risk group. Since physiological gestation downregulates the immunological response to maintain "maternal-fetal tolerance", SARS-CoV-2 infection may constitute a potentially threatening condition to both the mother and the fetus. To establish the immune profile in pregnant COVID-19+ patients, a cross-sectional study was conducted. Pregnant women with COVID-19 (P-COVID-19+; n = 15) were analyzed and compared with nonpregnant women with COVID-19 (NP-COVID-19+; n = 15) or those with physiological pregnancy (P-COVID-19-; n = 13). Serological cytokine and chemokine concentrations, leucocyte immunophenotypes, and mononuclear leucocyte responses to polyclonal stimuli were analyzed in all groups. Higher concentrations of serological TNF-α, IL-6, MIP1b and IL-4 were observed within the P-COVID-19+ group, while cytokines and chemokines secreted by peripheral leucocytes in response to LPS, IL-6 or PMA-ionomicin were similar among the groups. Immunophenotype analysis showed a lower percentage of HLA-DR+ monocytes in P-COVID-19+ than in P-COVID-19- and a higher percentage of CD39+ monocytes in P-COVID-19+ than in NP-COVID-19+. After whole blood polyclonal stimulation, similar percentages of T cells and TNF+ monocytes between groups were observed. Our results suggest that P-COVID-19+ elicits a strong inflammatory response similar to NP-COVID19+ but also displays an anti-inflammatory response that controls the ATP/adenosine balance and prevents hyperinflammatory damage in COVID-19.

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