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1.
SARS-CoV-2 Seroprevalence Among Parturient Women
Dustin D. Flannery; Sigrid Gouma; Miren B. Dhudasia; Sagori Mukhopadhyay; Madeline R. Pfeifer; Emily C. Woodford; Jeffrey S. Gerber; Claudia P. Arevalo; Marcus J. Bolton; Madison E. Weirick; Eileen C. Goodwin; Elizabeth M. Anderson; Allison R. Greenplate; Justin Kim; Nicholas Han; Ajinkya Pattekar; Jeanette Dougherty; Olivia Kuthuru; Divij Mathew; Amy E. Baxter; Laura A. Vella; JoEllen Weaver; Anurag Verma; Rita Leite; Jeffrey S. Morris; Daniel J. Rader; Michal A. Elovitz; E. John Wherry; Karen M. Puopolo; Scott E. Hensley.
Preprint em Inglês | medRxiv | ID: ppmedrxiv-20149179

RESUMO

Limited data are available for pregnant women affected by SARS-CoV-2. Serological tests are critically important to determine exposure and immunity to SARS-CoV-2 within both individuals and populations. We completed SARS-CoV-2 serological testing of 1,293 parturient women at two centers in Philadelphia from April 4 to June 3, 2020. We tested 834 pre-pandemic samples collected in 2019 and 15 samples from COVID-19 recovered donors to validate our assay, which has a [~]1% false positive rate. We found 80/1,293 (6.2%) of parturient women possessed IgG and/or IgM SARS-CoV-2-specific antibodies. We found race/ethnicity differences in seroprevalence rates, with higher rates in Black/non-Hispanic and Hispanic/Latino women. Of the 72 seropositive women who also received nasopharyngeal polymerase chain reaction testing during pregnancy, 46 (64%) were positive. Continued serologic surveillance among pregnant women may inform perinatal clinical practices and can potentially be used to estimate seroprevalence within the community. One Sentence SummarySix percent of pregnant women delivering from April 4 to June 3, 2020 had serological evidence of exposure to SARS-CoV-2 with notable race/ethnicity differences in seroprevalence rates.

2.
Immunologic perturbations in severe COVID-19/SARS-CoV-2 infection
Leticia Kuri-Cervantes; M. Betina Pampena; Wenzhao Meng; Aaron M Rosenfeld; Caroline A.G. Ittner; Ariel R Weisman; Roseline Agyekum; Divij Mathew; Amy E Baxter; Laura Vella; Olivia Kuthuru; Sokratis Apostolidis; Luanne Bershaw; Jeanette Dougherty; Allison R. Greenplate; Ajinkya Pattekar; Justin Kim; Nicholas Han; Sigrid Gouma; Madison E. Weirick; Claudia P Arevalo; Marcus J Bolton; Eileen C. Goodwin; Elizabeth M Anderson; Scott E. Hensley; Tiffanie K. Jones; Nilam S. Mangalmurti; Eline T. Luning Prak; Nuala J Meyer; Justin Kim; Michael R Betts.
Preprint em Inglês | bioRxiv | ID: ppbiorxiv-101717

RESUMO

Although critical illness has been associated with SARS-CoV-2-induced hyperinflammation, the immune correlates of severe COVID-19 remain unclear. Here, we comprehensively analyzed peripheral blood immune perturbations in 42 SARS-CoV-2 infected and recovered individuals. We identified broad changes in neutrophils, NK cells, and monocytes during severe COVID-19, suggesting excessive mobilization of innate lineages. We found marked activation within T and B cells, highly oligoclonal B cell populations, profound plasmablast expansion, and SARS-CoV-2-specific antibodies in many, but not all, severe COVID-19 cases. Despite this heterogeneity, we found selective clustering of severe COVID-19 cases through unbiased analysis of the aggregated immunological phenotypes. Our findings demonstrate broad immune perturbations spanning both innate and adaptive leukocytes that distinguish dysregulated host responses in severe SARS-CoV-2 infection and warrant therapeutic investigation. One Sentence SummaryBroad immune perturbations in severe COVID-19

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