Effectiveness of Monovalent mRNA COVID-19 Vaccination in Preventing COVID-19–Associated Invasive Mechanical Ventilation and Death Among Immunocompetent Adults During the Omicron Variant Period — IVY Network, 19 U.S. States, February 1, 2022–January 31, 2023

As of April 2023, the COVID-19 pandemic has resulted in 1.1 million deaths in the United States, with approximately 75% of deaths occurring among adults aged ≥65 years (1). Data on the durability of protection provided by monovalent mRNA COVID-19 vaccination against critical outcomes of COVID-19 are limited beyond the Omicron BA.1 lineage period (December 26, 2021–March 26, 2022). In this case-control analysis, the effectiveness of 2–4 monovalent mRNA COVID-19 vaccine doses was evaluated against COVID-19–associated invasive mechanical ventilation (IMV) and in-hospital death among immunocompetent adults aged ≥18 years during February 1, 2022–January 31, 2023. Vaccine effectiveness (VE) against IMV and in-hospital death was 62% among adults aged ≥18 years and 69% among those aged ≥65 years. When stratified by time since last dose, VE was 76% at 7–179 days, 54% at 180–364 days, and 56% at ≥365 days. Monovalent mRNA COVID-19 vaccination provided substantial, durable protection against IMV and in-hospital death among adults during the Omicron variant period. All adults should remain up to date with recommended COVID-19 vaccination to prevent critical COVID-19–associated outcomes.

Monovalent mRNA COVID-19 vaccination has been shown to prevent hospitalization and critical outcomes, including IMV and death, during SARS-CoV-2 Alpha, Delta, and early Omicron variant periods (2,3). However, rapid waning of COVID-19 VE against infection, outpatient illness, and hospitalization has been observed during Omicron variant predominance (4). Understanding the durability of protection provided by monovalent mRNA vaccination against critical outcomes is vital. Although a bivalent mRNA dose was recommended on September 1, 2022, for all persons who had completed a primary COVID-19 vaccination series, bivalent vaccination coverage among adults aged ≥18 years is 20%, and most adults have only received monovalent mRNA vaccines (1,5). In addition, COVID-19 VE against hospitalization might be artificially reduced by routine testing for SARS-CoV-2 at admission, which can detect SARS-CoV-2 infection in patients admitted for reasons other than COVID-19 (4,6,7). VE against critical outcomes might be less susceptible to this bias and is therefore needed to help guide COVID-19 vaccination policy regarding revaccination intervals.

Data from the Investigating Respiratory Viruses in the Acutely Ill (IVY) Network^§ were used to conduct a case-control analysis measuring the effectiveness of monovalent mRNA COVID-19 vaccination against COVID-19–associated IMV and in-hospital death. During February 1, 2022–January 31, 2023, adults aged ≥18 years admitted to 24 hospitals in 19 U.S. states who met a COVID-19–like illness case definition^¶ and received SARS-CoV-2 testing were enrolled. IVY Network methods have been described previously (2,3). Briefly, case-patients were defined as those who received a positive SARS-CoV-2 reverse transcription–polymerase chain reaction (RT-PCR) or antigen test result within 10 days of illness onset and within 3 days of hospital admission, and either received IMV or died in the hospital within 28 days of admission. Control patients were defined as those who received negative SARS-CoV-2 and influenza test results by RT-PCR within 10 days of illness onset and within 3 days of hospital admission. Patients who received positive influenza test results were excluded from the analysis because of potential correlation between COVID-19 and influenza vaccination behaviors (8).

Demographic and clinical data, including receipt of IMV and in-hospital death within 28 days of admission, were collected through electronic medical record (EMR) review and patient or proxy interview. COVID-19 vaccination history was ascertained from state or jurisdictional registries, EMRs, vaccination cards, and self-report. Patients were included in the analysis if they 1) received zero COVID-19 vaccines doses (unvaccinated) or 2) received 2, 3, or 4 monovalent mRNA COVID-19 vaccine doses (monovalent-vaccinated), with the last dose received ≥14 days before illness onset for a primary series dose or ≥7 days before illness onset for a booster dose. Patients were excluded from the analysis if they were immunocompromised,** received a non-mRNA COVID-19 vaccine dose, received only 1 monovalent mRNA COVID-19 vaccine dose, received a bivalent mRNA COVID-19 vaccine dose, or for other reasons^†† that made the patient ineligible.

VE against IMV and in-hospital death was calculated using logistic regression, in which the odds of monovalent mRNA vaccination (versus being unvaccinated) were compared between COVID-19 case-patients and control patients. Logistic regression models were adjusted for U.S. Department of Health and Human Services region, calendar time in biweekly intervals, age, sex, and self-reported race and Hispanic ethnicity. VE was calculated as (1 − adjusted odds ratio) x 100%. Results were stratified by age group, time since receipt of last monovalent mRNA vaccine dose, and number of monovalent mRNA vaccine doses received.^§§ Differences between VE point estimates with nonoverlapping 95% CIs were considered statistically significant. Analyses were conducted using SAS (version 9.4; SAS Institute). This activity was determined to be public health surveillance by each participating site and CDC and was conducted in a manner consistent with all applicable federal laws and CDC policy.^¶¶

During February 1, 2022–January 31, 2023, a total of 6,354 immunocompetent control patients and COVID-19 case-patients with IMV or in-hospital death were enrolled in the IVY Network. After exclusion of 1,933 patients,*** 4,421 (70%) were included in the analysis (362 case-patients and 4,059 control patients). Patients were most commonly excluded because of receipt of a bivalent mRNA COVID-19 vaccine dose (446 [23% of excluded patients]), receipt of a non-mRNA COVID-19 vaccine (392 [20%]), or receipt of only 1 monovalent mRNA COVID-19 vaccine dose (260 [13%]). Among included patients, the median age was 64 years (IQR = 53–75 years) (Table 1). Ninety-one percent of patients had one or more chronic condition, and 20% had a previous self-reported or documented SARS-CoV-2 infection. Among 362 case-patients with IMV or in-hospital death, 146 (40%) were unvaccinated, 216 (60%) were monovalent-vaccinated, 293 (81%) received IMV, and 156 (43%) died in the hospital within 28 days of admission. Among 4,059 control patients, 979 (24%) were unvaccinated, and 3,080 (76%) were monovalent-vaccinated.

Among monovalent-vaccinated patients, the median interval from receipt of last dose to illness onset was 248 days (IQR = 138–378 days) (Table 2). When compared with unvaccinated patients, the VE of 2–4 monovalent mRNA vaccine doses against IMV and in-hospital death was 62%. VE was 57% among patients aged 18–64 years and 69% among patients aged ≥65 years. When stratified by interval since receipt of last monovalent dose, VE against IMV and in-hospital death was 76% at 7–179 days, 54% at 180–364 days, and 56% at ≥365 days. Within each interval since receipt of last monovalent dose, VE estimates did not differ significantly by number of doses received. VE point estimates were higher 7–179 days since last dose compared with ≥180 days since last dose, although 95% CIs overlapped.

Corresponding author: Jennifer DeCuir, media@cdc.gov.

¹National Center for Immunization and Respiratory Diseases, CDC; ²Vanderbilt University Medical Center, Nashville, Tennessee; ³Baylor Scott & White Health, Temple, Texas; ⁴Texas A&M University College of Medicine, Temple, Texas; ⁵Baylor Scott & White Health, Dallas, Texas; ⁶University of Colorado School of Medicine, Aurora, Colorado; ⁷University of Iowa, Iowa City, Iowa; ⁸Wake Forest University Baptist Medical Center, Winston-Salem, North Carolina; ⁹Johns Hopkins Hospital, Baltimore, Maryland; ¹⁰Hennepin County Medical Center, Minneapolis, Minnesota; ¹¹Montefiore Healthcare Center, Albert Einstein College of Medicine, New York, New York; ¹²University of Washington School of Medicine, Seattle, Washington; ¹³Baystate Medical Center, Springfield, Massachusetts; ¹⁴Intermountain Medical Center and University of Utah, Salt Lake City, Utah; ¹⁵University of Michigan School of Public Health, Ann Arbor, Michigan; ¹⁶Oregon Health & Science University Hospital, Portland, Oregon; ¹⁷Emory University School of Medicine, Atlanta, Georgia; ¹⁸Cleveland Clinic, Cleveland, Ohio; ¹⁹Stanford University School of Medicine, Stanford, California; ²⁰Ronald Reagan UCLA Medical Center, Los Angeles, California; ²¹University of Miami, Miami, Florida; ²²Washington University, St. Louis, Missouri; ²³The Ohio State University Wexner Medical Center, Columbus, Ohio; ²⁴University of Michigan School of Medicine, Ann Arbor, Michigan; ²⁵Beth Israel Deaconess Medical Center, Boston, Massachusetts; ²⁶Henry Ford Health, Detroit, Michigan; ²⁷Yale University School of Medicine, New Haven, Connecticut.

References

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Abbreviations: HHS = U.S. Department of Health and Human Services; IMV = invasive mechanical ventilation.
* Hospitals by HHS region included Region 1: Baystate Medical Center (Springfield, Massachusetts), Beth Israel Deaconess Medical Center (Boston, Massachusetts), and Yale University (New Haven, Connecticut); Region 2: Montefiore Medical Center (New York, New York); Region 3: Johns Hopkins Hospital (Baltimore, Maryland); Region 4: Emory University Medical Center (Atlanta, Georgia), University of Miami Medical Center (Miami, Florida), Vanderbilt University Medical Center (Nashville, Tennessee), and Wake Forest University Baptist Medical Center (Winston-Salem, North Carolina); Region 5: Cleveland Clinic (Cleveland, Ohio), Hennepin County Medical Center (Minneapolis, Minnesota), Henry Ford Health (Detroit, Michigan), The Ohio State University Wexner Medical Center (Columbus, Ohio), and University of Michigan Hospital (Ann Arbor, Michigan); Region 6: Baylor Scott & White Medical Center (Temple, Texas) and Baylor University Medical Center (Dallas, Texas); Region 7: Barnes-Jewish Hospital (St. Louis, Missouri) and University of Iowa Hospitals (Iowa City, Iowa); Region 8: Intermountain Medical Center (Murray, Utah) and UCHealth University of Colorado Hospital (Aurora, Colorado); Region 9: Stanford University Medical Center (Stanford, California) and Ronald Reagan UCLA Medical Center (Los Angeles, California); and Region 10: Oregon Health & Science University Hospital (Portland, Oregon) and University of Washington (Seattle, Washington).
^† Other race, non-Hispanic includes American Indian or Alaska Native, Asian, and Native Hawaiian or other Pacific Islander categories, which were combined because of small counts.
^§ Other includes patients who self-reported their race and ethnicity as “Other” and those for whom race and ethnicity were unknown.
^¶ Chronic medical condition categories include autoimmune, cardiovascular, endocrine, gastrointestinal, hematologic, neurologic, pulmonary, and renal diseases.
** Previous SARS-CoV-2 infection was defined as any self-reported or documented previous SARS-CoV-2 infection. Previous Omicron infection was defined as any self-reported or documented previous SARS-CoV-2 infection that occurred during December 26, 2021–January 31, 2023.

Abbreviations: IMV = invasive mechanical ventilation; VE = vaccine effectiveness.
* https://www.cdc.gov/flu/vaccines-work/ivy.htm
^† Monovalent-vaccinated patients received 2–4 monovalent mRNA COVID-19 vaccine doses and zero bivalent mRNA COVID-19 vaccine doses.
^§ VE was estimated by comparing the odds of monovalent mRNA vaccination among case-patients and control patients, calculated as VE = 100 × (1 − odds ratio). Logistic regression models were adjusted for date of hospital admission (biweekly intervals), U.S. Department of Health and Human Services region (10 regions), categorical age (18–49, 50–64, and ≥65 years), sex, and race and ethnicity (Black or African American, non-Hispanic; White, non-Hispanic; Hispanic or Latino, any race; Other race, non-Hispanic; and Other, unknown) unless otherwise noted. Logistic regression models for age group–specific VE estimates were adjusted for continuous age.
^¶ Logistic regression models for VE of 4 monovalent doses were restricted to patients aged ≥50 years admitted during April 5, 2022–January 31, 2023, and were adjusted for continuous age.
** VE estimate was not reported because of insufficient sample size.