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Effectiveness of a bivalent mRNA vaccine dose against symptomatic SARS-CoV-2 infection among U.S. Healthcare personnel, September 2022-May 2023.

Plumb, Ian D; Briggs Hagen, Melissa; Wiegand, Ryan; Dumyati, Ghinwa; Myers, Christopher; Harland, Karisa K; Krishnadasan, Anusha; James Gist, Jade; Abedi, Glen; Fleming-Dutra, Katherine E; Chea, Nora; Lee, Jane E; Kellogg, Melissa; Edmundson, Alexandra; Britton, Amber; Wilson, Lucy E; Lovett, Sara A; Ocampo, Valerie; Markus, Tiffanie M; Smithline, Howard A; Hou, Peter C; Lee, Lilly C; Mower, William; Rwamwejo, Fernand; Steele, Mark T; Lim, Stephen C; Schrading, Walter A; Chinnock, Brian; Beiser, David G; Faine, Brett; Haran, John P; Nandi, Utsav; Chipman, Anne K; LoVecchio, Frank; Eucker, Stephanie; Femling, Jon; Fuller, Matthew; Rothman, Richard E; Curlin, Marcel E; Talan, David A; Mohr, Nicholas M.

Vaccine ; 42(10): 2543-2552, 2024 Apr 11.

Article En | MEDLINE | ID: mdl-37973512

BACKGROUND: Bivalent mRNA vaccines were recommended since September 2022. However, coverage with a recent vaccine dose has been limited, and there are few robust estimates of bivalent VE against symptomatic SARS-CoV-2 infection (COVID-19). We estimated VE of a bivalent mRNA vaccine dose against COVID-19 among eligible U.S. healthcare personnel who had previously received monovalent mRNA vaccine doses. METHODS: We conducted a case-control study in 22 U.S. states, and enrolled healthcare personnel with COVID-19 (case-participants) or without COVID-19 (control-participants) during September 2022-May 2023. Participants were considered eligible for a bivalent mRNA dose if they had received 2-4 monovalent (ancestral-strain) mRNA vaccine doses, and were ≥67 days after the most recent vaccine dose. We estimated VE of a bivalent mRNA dose using conditional logistic regression, accounting for matching by region and four-week calendar period. We adjusted estimates for age group, sex, race and ethnicity, educational level, underlying health conditions, community COVID-19 exposure, prior SARS-CoV-2 infection, and days since the last monovalent mRNA dose. RESULTS: Among 3,647 healthcare personnel, 1,528 were included as case-participants and 2,119 as control-participants. Participants received their last monovalent mRNA dose a median of 404 days previously; 1,234 (33.8%) also received a bivalent mRNA dose a median of 93 days previously. Overall, VE of a bivalent dose was 34.1% (95% CI, 22.6%-43.9%) against COVID-19 and was similar by product, days since last monovalent dose, number of prior doses, age group, and presence of underlying health conditions. However, VE declined from 54.8% (95% CI, 40.7%-65.6%) after 7-59 days to 21.6% (95% CI 5.6%-34.9%) after ≥60 days. CONCLUSIONS: Bivalent mRNA COVID-19 vaccines initially conferred approximately 55% protection against COVID-19 among U.S. healthcare personnel. However, protection waned after two months. These findings indicate moderate initial protection against symptomatic SARS-CoV-2 infection by remaining up-to-date with COVID-19 vaccines.

COVID-19 , Humans , Infant, Newborn , COVID-19/prevention & control , COVID-19 Vaccines , Vaccines, Combined , mRNA Vaccines , Case-Control Studies , SARS-CoV-2 , RNA, Messenger , Delivery of Health Care

Effectiveness of a Messenger RNA Vaccine Booster Dose Against Coronavirus Disease 2019 Among US Healthcare Personnel, October 2021-July 2022.

Plumb, Ian D; Mohr, Nicholas M; Hagen, Melissa; Wiegand, Ryan; Dumyati, Ghinwa; Harland, Karisa K; Krishnadasan, Anusha; Gist, Jade James; Abedi, Glen; Fleming-Dutra, Katherine E; Chea, Nora; Lee, Jane; Barter, Devra; Brackney, Monica; Fridkin, Scott K; Wilson, Lucy E; Lovett, Sara A; Ocampo, Valerie; Phipps, Erin C; Marcus, Tiffanie M; Smithline, Howard A; Hou, Peter C; Lee, Lilly C; Moran, Gregory J; Krebs, Elizabeth; Steele, Mark T; Lim, Stephen C; Schrading, Walter A; Chinnock, Brian; Beiser, David G; Faine, Brett; Haran, John P; Nandi, Utsav; Chipman, Anne K; LoVecchio, Frank; Talan, David A; Pilishvili, Tamara.

Open Forum Infect Dis ; 10(10): ofad457, 2023 Oct.

Article En | MEDLINE | ID: mdl-37799130

Background: Protection against symptomatic severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) infection (coronavirus disease 2019 [COVID-19]) can limit transmission and the risk of post-COVID conditions, and is particularly important among healthcare personnel. However, lower vaccine effectiveness (VE) has been reported since predominance of the Omicron SARS-CoV-2 variant. Methods: We evaluated the VE of a monovalent messenger RNA (mRNA) booster dose against COVID-19 from October 2021 to June 2022 among US healthcare personnel. After matching case-participants with COVID-19 to control-participants by 2-week period and site, we used conditional logistic regression to estimate the VE of a booster dose compared with completing only 2 mRNA doses >150 days previously, adjusted for multiple covariates. Results: Among 3279 case-participants and 3998 control-participants who had completed 2 mRNA doses, we estimated that the VE of a booster dose against COVID-19 declined from 86% (95% confidence interval, 81%-90%) during Delta predominance to 65% (58%-70%) during Omicron predominance. During Omicron predominance, VE declined from 73% (95% confidence interval, 67%-79%) 14-60 days after the booster dose, to 32% (4%-52%) ≥120 days after a booster dose. We found that VE was similar by age group, presence of underlying health conditions, and pregnancy status on the test date, as well as among immunocompromised participants. Conclusions: A booster dose conferred substantial protection against COVID-19 among healthcare personnel. However, VE was lower during Omicron predominance, and waning effectiveness was observed 4 months after booster dose receipt during this period. Our findings support recommendations to stay up to date on recommended doses of COVID-19 vaccines for all those eligible.