TY - JOUR
T1 - Real-world utilization of SARS-CoV-2 serological testing in RNA positive patients across the United States
AU - Rodriguez-Watson, Carla V.
AU - Sheils, Natalie E.
AU - Louder, Anthony M.
AU - Eldridge, Elizabeth H.
AU - Lin, Nancy D.
AU - Pollock, Benjamin D.
AU - Gatz, Jennifer L.
AU - Grannis, Shaun J.
AU - Vashisht, Rohit
AU - Ghauri, Kanwal
AU - Valo, Gina
AU - Chakravarty, Aloka G.
AU - Lasky, Tamar
AU - Jung, Mary
AU - Lovell, Stephen L.
AU - Major, Jacqueline M.
AU - Kabelac, Carly
AU - Knepper, Camille
AU - Leonard, Sandy
AU - Embi, Peter J.
AU - Jenkinson, William G.
AU - Klesh, Reyna
AU - Garner, Omai B.
AU - Patel, Ayan
AU - Dahm, Lisa
AU - Barin, Aiden
AU - Cooper, Dan M.
AU - Andriola, Tom
AU - Byington, Carrie L.
AU - Crews, Bridgit O.
AU - Butte, Atul J.
AU - Allen, Jeff
N1 - Publisher Copyright:
© 2023 Public Library of Science. All rights reserved.
PY - 2023/2
Y1 - 2023/2
N2 - Background As diagnostic tests for COVID-19 were broadly deployed under Emergency Use Authorization, there emerged a need to understand the real-world utilization and performance of serological testing across the United States. Methods Six health systems contributed electronic health records and/or claims data, jointly developed a master protocol, and used it to execute the analysis in parallel. We used descriptive statistics to examine demographic, clinical, and geographic characteristics of serology testing among patients with RNA positive for SARS-CoV-2. Results Across datasets, we observed 930,669 individuals with positive RNA for SARS-CoV-2. Of these, 35,806 (4%) were serotested within 90 days; 15% of which occurred <14 days from the RNA positive test. The proportion of people with a history of cardiovascular disease, obesity, chronic lung, or kidney disease; or presenting with shortness of breath or pneumonia appeared higher among those serotested compared to those who were not. Even in a population of people with active infection, race/ethnicity data were largely missing (>30%) in some datasets—limiting our ability to examine differences in serological testing by race. In datasets where race/ethnicity information was available, we observed a greater distribution of White individuals among those serotested; however, the time between RNA and serology tests appeared shorter in Black compared to White individuals. Test manufacturer data was available in half of the datasets contributing to the analysis. Conclusion Our results inform the underlying context of serotesting during the first year of the COVID-19 pandemic and differences observed between claims and EHR data sources–a critical first step to understanding the real-world accuracy of serological tests. Incomplete reporting of race/ethnicity data and a limited ability to link test manufacturer data, lab results, and clinical data challenge the ability to assess the real-world performance of SARS-CoV-2 tests in different contexts and the overall U.S. response to current and future disease pandemics.
AB - Background As diagnostic tests for COVID-19 were broadly deployed under Emergency Use Authorization, there emerged a need to understand the real-world utilization and performance of serological testing across the United States. Methods Six health systems contributed electronic health records and/or claims data, jointly developed a master protocol, and used it to execute the analysis in parallel. We used descriptive statistics to examine demographic, clinical, and geographic characteristics of serology testing among patients with RNA positive for SARS-CoV-2. Results Across datasets, we observed 930,669 individuals with positive RNA for SARS-CoV-2. Of these, 35,806 (4%) were serotested within 90 days; 15% of which occurred <14 days from the RNA positive test. The proportion of people with a history of cardiovascular disease, obesity, chronic lung, or kidney disease; or presenting with shortness of breath or pneumonia appeared higher among those serotested compared to those who were not. Even in a population of people with active infection, race/ethnicity data were largely missing (>30%) in some datasets—limiting our ability to examine differences in serological testing by race. In datasets where race/ethnicity information was available, we observed a greater distribution of White individuals among those serotested; however, the time between RNA and serology tests appeared shorter in Black compared to White individuals. Test manufacturer data was available in half of the datasets contributing to the analysis. Conclusion Our results inform the underlying context of serotesting during the first year of the COVID-19 pandemic and differences observed between claims and EHR data sources–a critical first step to understanding the real-world accuracy of serological tests. Incomplete reporting of race/ethnicity data and a limited ability to link test manufacturer data, lab results, and clinical data challenge the ability to assess the real-world performance of SARS-CoV-2 tests in different contexts and the overall U.S. response to current and future disease pandemics.
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U2 - 10.1371/journal.pone.0281365
DO - 10.1371/journal.pone.0281365
M3 - Article
C2 - 36763574
AN - SCOPUS:85147869342
SN - 1932-6203
VL - 18
JO - PloS one
JF - PloS one
IS - 2 February
M1 - e0281365
ER -