COVID-19 Infection, Reinfection, and Vaccine Effectiveness in a Prospective Cohort of Arizona Frontline/Essential Workers: The AZ HEROES Research Protocol.

BACKGROUND: The Arizona Healthcare, Emergency Response, and Other Essential workers Study (AZ HEROES) aims to examine the epidemiology of SARS-CoV-2 infection and COVID-19 illness among adults with high occupational exposure risk.
OBJECTIVE: Study objectives include estimating incidence of SARS-CoV-2 infection in essential workers by symptom presentation and demographic factors, determining independent effects of occupational and community exposures on incidence of SARS-CoV-2 infection, establishing molecular and immunologic characteristics of SARS-CoV-2 infection in essential workers, describing the duration and patterns of rRT-PCR-positivity, and examining post-vaccine immunologic response.
METHODS: Eligible participants include Arizona residents aged 18-85 years who work at least 20 hours per week in an occupation involving regular direct contact (within three feet) with others. Recruitment goals are stratified by demographic characteristics (50% aged 40 or older, 50% women, and 50% Hispanic or American Indian), by occupation (40% healthcare personnel, 30% first responders, and 30% other essential workers), and by prior SARS-CoV-2 infection (with up to 50% seropositive at baseline). Information on sociodemographics, health and medical history, vaccination status, exposures to individuals with suspected or confirmed SARS-CoV-2 infection, use of personal protective equipment, and perceived risks are collected at enrollment and updated through quarterly surveys. Every week, participants complete active surveillance for COVID-19-like illness (CLI) and self-collect nasal swabs. Additional self-collected nasal swab and saliva specimens are collected in the event of CLI onset. Respiratory specimens are sent to Marshfield Laboratories and tested for SARS-CoV-2 by real-time reverse transcription polymerase chain reaction (rRT-PCR) assay. CLI symptoms and impact on work and productivity are followed through illness resolution. Serum specimens are collected every 3 months and additional sera are collected following incident rRT-PCR positivity and after each COVID-19 vaccine dose. Incidence of SARS-CoV-2 infections will be calculated by person-weeks at risk and compared by occupation and demographic characteristics and by seropositivity status and infection and vaccination history.
RESULTS: The AZ HEROES study was funded by the Centers for Disease Control and Prevention. Enrollment began July 27, 2020 and as of May 1, 2021 a total of 3,165 participants have been enrolled in the study.
CONCLUSIONS: AZ HEROES is unique in aiming to recruit a diverse sample of essential workers and prospectively following strata of SARS-CoV-2 seronegative and seropositive adults. Survey results combined with active surveillance data on exposure, CLI, weekly molecular diagnostic testing, and periodic serology will be used to estimate the incidence of symptomatic and asymptomatic SARS-CoV-2 infection, assess the intensity and durability of immune responses to natural infection and COVID-19 vaccination, and contribute to the evaluation of COVID-19 vaccine effectiveness. INTERNATIONAL REGISTERED REPORT: DERR1-10.2196/28925.

Introduction

COVID-19, caused by the betacoronavirus SARS-CoV-2, has spread worldwide since late 2019, with at least 80 million confirmed cases and 1.8 million deaths reported globally in the year since discovery of the virus [1].

COVID-like illness (CLI) includes symptoms of fever or chills, cough, shortness of breath, sore throat, diarrhea, muscle aches, and loss of smell or taste [2]. Outbreak reports and mass testing initiatives suggest that a substantial proportion of individuals who test positive have no symptoms [3-6]. However, the proportion of confirmed cases with true asymptomatic infection is likely overestimated due to incomplete symptom assessment, inadequate follow-up to accurately classify presymptomatic individuals, and potential misclassification of those with previously unrecognized infection as asymptomatic [7]. Immigrant, racial and ethnic minority, and low-income communities have experienced a disproportionate burden of SARS-CoV-2 infections [8]. Severity of illness also differs by sociodemographic characteristics, with older adults and those with underlying health conditions at the highest risk of severe outcomes and death [9]. Optimizing public health responses requires further scientific study to estimate the incidence of infection, severity of illness, and variable immune response in sociodemographically diverse communities at high risk for infection [10].

Individuals in certain occupations are at increased risk of SARS-CoV-2 infection because of frequent close contact with others, including health care personnel (HCP), first responders, and other essential and frontline workers (OEWs). Recent studies highlight the elevated risk of exposure and infection among HCP [11-13], with more severe outcomes experienced by racial and ethnic minority HCP [14,15]. Less evidence exists, however, on transmission risks and severity of illness among OEWs [16,17]. First responders face a variety of exposures, including entering the homes of people with unknown disease status and performing aerosol-generating procedures, such as resuscitation [18]. Other essential and/or frontline occupational sectors with potentially high SARS-CoV-2 exposure include schools and childcare, agriculture and food production, energy, water and wastewater, retail (eg, grocery stores and warehouses), trades (eg, construction and plumbing), and nonprofits and social service organizations [19-21].

Prospective monitoring of symptomatic and asymptomatic infection is necessary to assess the combined epidemiological, immunological, and clinical impact of COVID-19 among essential workers [22]. Recent studies suggest that SARS-CoV-2 immunoglobulins M, G, and A (IgM, IgG, and IgA) are detected in various combinations in variable numbers of individuals in the first 2 weeks of infection, with IgG detected in most subjects after 14 days [23-25]. Although antibody response peaks at 16 to 42 days postinfection [23-26], and IgM and IgA levels decline, levels of IgG against the spike protein remain stable; protective immunity of at least 6 months has been measured, and much longer immunity is anticipated based on previous studies of coronaviruses—up to 17 years for SARS-CoV-1—and other acute viral infections [27-29]. Factors associated with variable immune response, including neutralizing (no infection), protective (mild to asymptomatic infection), or enhanced (severe symptoms) [30,31], are not yet fully understood for SARS-CoV-2.

The US Food and Drug Administration (FDA) has authorized the distribution of the first COVID-19 vaccines under Emergency Use Authorization (EUA), and the US Centers for Disease Control and Prevention (CDC) has recommended prioritization of vaccination for HCP, first responders, and OEW populations [32,33]. However, there is limited knowledge of vaccine intent and hesitancy among essential workers and of vaccine efficacy among those who were seropositive for SARS-CoV-2 prior to vaccination.

The Arizona Healthcare, Emergency Response, and Other Essential Workers Study (AZ HEROES) will follow a cohort of 4000 essential workers who are demographically representative of Arizona and stratified by prior exposure to SARS-CoV-2, such that about half are seronegative and half seropositive. The study affords researchers the opportunity to assess multiple knowledge gaps regarding the epidemiology and immunology of SARS-CoV-2 infections among a diverse statewide sample of essential workers with high exposure potential. AZ HEROES has also been expanded to evaluate immune parameters and incidence of SARS-CoV-2 infection following COVID-19 vaccination in previously seronegative and seropositive individuals (Table 1).

Table 1

Primary and secondary objectives for the AZ HEROESa study of SARS-CoV-2 infection and immunity in a statewide cohort of essential workers stratified by seronegative and seropositive cohorts.

Type of objective	Objectives per cohort
	Seronegative cohortb	Seropositive cohortc
Primary	Estimate incidence of SARS-CoV-2 infection in essential workers by symptom presentation and demographic factors Estimate the relative risk of infection with SARS-CoV-2 versus influenza during influenza season Determine independent effects of occupational and community exposures on incidence of SARS-CoV-2 infection	Establish molecular and immunologic characteristics of SARS-CoV-2 infection in essential workers Describe the duration and patterns of rRT-PCRd positivity Describe levels of total antibodies, neutralizing antibodies, and other immune parameters over time Examine postvaccine immunologic response in those previously infected
Secondary	Examine the role of knowledge, attitudes, and practices related to SARS-CoV-2 in exposures and incident infection Identify predictors of vaccine hesitancy and uptake by occupation Compare incidence of infection in vaccinated vs unvaccinated essential workers	Describe severity and impact of illness on essential workers Examine predictors of severe disease among those naturally infected with SARS-CoV-2 Estimate incidence of SARS-CoV-2 reinfection Assess predictors of vaccine hesitancy and uptake among those with history of natural infection

aAZ HEROES: Arizona Healthcare, Emergency Response, and Other Essential Workers Study.

bIncludes person-time contributed by individuals enrolled as seronegative who do not become naturally infected during the study and person-time contributed by individuals enrolled as seronegative before becoming infected during the study.

cIncludes person-time contributed by individuals enrolled with prior evidence—viral or serologic—of SARS-CoV-2 infection and person-time contributed by individuals enrolled as seronegative after becoming naturally infected during the course of the study.

drRT-PCR: real-time reverse transcription–polymerase chain reaction.

Methods

Study Design

AZ HEROES is a prospective cohort study with the goal of following 4000 essential workers, including 2000 seronegative and 2000 seropositive—defined as evidence of SARS-CoV-2 infection by serologic testing—individuals throughout the state of Arizona (Figure 1). The study duration is planned for July 2020 through April 2022.

Figure 1

AZ HEROES flow of activities for baseline, follow-up, and event-based surveys and serology occurring in the context of weekly rRT-PCR testing and text-based symptom surveillance. AZ HEROES: Arizona Healthcare, Emergency Response, and Other Essential Workers Study; rRT-PCR: real-time reverse transcription–polymerase chain reaction.

Setting

The state of Arizona has 7.2 million people residing in 15 counties and 22 sovereign American Indian communities. Nine of Arizona’s counties are designated as rural [34], although the majority of the population resides in the greater Phoenix and Tucson metropolitan areas. Arizona has large minority populations, with 32% Hispanic and 5% American Indian populations [35].

Participants

Eligibility Criteria

Eligible participants include Arizona residents aged 18 to 85 years who currently work at least 20 hours per week in an occupation involving regular direct contact (ie, within 3 feet) with others, assessed at the participant level. We have intentionally chosen a broad occupational category for frontline and essential workers in order to capture the full breadth of occupations that cannot socially distance when conducting their work [36], as well as an inclusive age range because 13.9% of the Arizona workforce is over the age of 65 years [37]. The occupations are categorized as HCP, first responders, or OEWs. HCP include clinical providers and support staff in inpatient, outpatient, or residential settings. First responders include firefighters, emergency medical services, law enforcement, border patrol, and correctional officers. OEWs include workers in the following sectors: education, agriculture and food processing, public and other transportation services, solid waste collection, warehouse and delivery, utilities, government and community-based services, childcare, information technology, environmental services, and hospitality. All participants must have access to a smartphone or internet-connected computer, a mailing address, and the ability to speak or write English or Spanish. Exclusion criteria include receipt of a COVID-19 vaccine prior to enrollment, although we continue to follow participants who are vaccinated during the study. The majority of the cohort of the HCP and first responders were recruited prior to vaccine availability.

Recruitment Strategy

In order to enroll 4000 participants as quickly as possible, we have employed a multipronged recruitment strategy. First, we are recruiting from ongoing Arizona-based COVID-19 testing activities, such as university-driven antibody and saliva testing initiatives and serology surveillance conducted by the state health department in selected occupations (eg, nursing homes and correctional facilities). Second, we have partnered with community-based COVID-19 cohorts to recruit participants. The selected cohorts are low-touch and send periodic surveys to participants with little to no overlap in scope. For the testing and existing cohort populations, we directly contact individuals that indicate they would be willing to be contacted for future research. Third, the study accepts self-referrals, so we have developed a marketing strategy to increase general study awareness through press releases, targeted recruitment to occupations, and social media.

All recruitment and enrollment activities are conducted remotely utilizing a virtual call-center platform and REDCap (Research Electronic Data Capture) [38] to ensure staff and participant safety. Direct recruitment is conducted via phone and email. Participants are given the option to complete a self-screening questionnaire survey that is emailed to them or to complete a screening interview over the phone. Once deemed eligible and the participant is interested in the study, an electronic consent form is emailed to participants to review and sign electronically through REDCap.

Sampling targets are based on the employment demographics of Arizona, and we seek to enroll essential workers in the following proportions: 50% from 18 to 40 years old and 50% between 41 and 85 years old, 50% women, and 50% Hispanic or American Indian. By occupation, we seek to enroll 40% HCP, 30% first responders, and 30% OEWs. These sampling breakdowns are presented in Table 2. Our goal is to enroll these proportions in both seronegative and seropositive specimens (Table 2). As specified targets are met, recruitment and enrollment priorities will shift to underenrolled groups and to replace individuals that become COVID-19 positive throughout the study (Figure 2).

Table 2

Enrollment strata for age, race, ethnicity, and occupation with minimum enrollment targets for participants in the AZ HEROESa study.

Age group and race or ethnicity (target %)		Sex (target %)	Health care personnel (n=1600), n	First responders (n=1200), n	Other frontline and essential workersb (n=1200), n
18 to 39 years (50%)
	White and Non-Hispanic (50%)	Female (50%)	200	152	152
		Male (50%)	200	152	152
	Hispanic or Native American (50%)	Female (50%)	200	152	152
		Male (50%)	200	152	152
40 to 85 years (50%)
	White and Non-Hispanic (50%)	Female (50%)	200	152	152
		Male (50%)	200	152	152
	Hispanic or Native American (50%)	Female (50%)	200	152	152
		Male (50%)	200	152	152

aAZ HEROES: Arizona Healthcare, Emergency Response, and Other Essential Workers Study.

bIncludes frontline personnel who interact with the public as well as personnel who work in close proximity to each other (eg, call centers, warehouses, agriculture, and food processing).

Figure 2

Participants who enroll as seronegative will switch to the seropositive cohort during the course of the study if they become infected as confirmed by rRT-PCR or serology prior to vaccination. rRT-PCR: real-time reverse transcription–polymerase chain reaction.

Enrollment

Upon enrollment, participants are asked to complete a baseline questionnaire that collects information about sociodemographic characteristics; health status and behaviors; occupational exposure, tailored to the occupational category; history with and attitudes toward COVID-19; and influenza vaccination history during 2020-2021 and the previous five seasons (Table 3). Participants are asked to schedule a blood draw (40 mL) within 5 days of enrollment at a laboratory facility in their area in order to complete their baseline serology; a box of self-collection respiratory supplies are shipped to them so they can begin their active surveillance.

Table 3

Information sources and timing of collection for key variables through surveys, the bidirectional text platform, and specimen collection.

Collected information		Surveys				Active surveillance texts			Specimen submission
		Screen	Baseline	Follow-up	Event baseda	Weekly	Monthly (rotating)	Off schedule	Weekly	Quarterly	Event baseda
Demographics
	Age and gender	✓b
	Race or ethnicity	✓
	Date of birth	✓
	Education and income		✓
	Household composition		✓	✓
	Occupation information	✓	✓	✓
Health and medical history
	Overall health		✓	✓		✓
	Sleep quality		✓			✓
	Tobacco history		✓
	Comorbidities and medications		✓
	Height and weight		✓
	Pregnancy		✓	✓
	Influenza infection								✓
	Vaccine knowledge and attitudes		✓	✓			✓
SARS-CoV-2 infection
	rRT-PCRc pre-enrollment	✓
	rRT-PCR postenrollment								✓		✓
	Serology pre-enrollment	✓
	Serology postenrollment									✓	✓
	Occupational exposure		✓	✓			✓
	Community exposure		✓	✓			✓
	Symptoms	✓			✓	✓		✓	✓		✓
	Illness duration and recovery			✓	✓
	Illness severity and impact			✓	✓
Vaccination
	Influenza, history		✓
	Influenza, current			✓
	SARS-CoV-2, intent			✓				✓
	SARS-CoV-2, 2020-2021				✓			✓

aEvents include acute illness, recovery, and vaccination, which prompt additional study follow-up.

bCheckmarks indicate the information was collected at the indicated time and by the indicated method.

crRT-PCR: real-time reverse transcription–polymerase chain reaction.

Active Surveillance

As part of active surveillance for incident SARS-CoV-2 infection, all participants provide weekly self-collected mid-turbinate nasal swabs appropriate to test for SARS-CoV-2 and influenza, during the influenza season. Upon enrollment, study participants are provided with information that the study duration could be up to 2 years, but initial expectations are for at least 36 weeks of weekly self-collected respiratory specimens. If an individual experiences CLI, they are asked to collect an additional respiratory specimen on the date of onset of the first CLI symptom. Weekly and illness kits are differentiated by color so participants know which to take and so study staff can track supplies. Respiratory specimens are analyzed utilizing the CDC-designated reference laboratory for real-time reverse transcription–polymerase chain reaction (rRT-PCR) assay testing. Specimens are tested and results obtained 2 to 5 days from collection. If participants receive a positive test result, trained study staff contact participants to provide CDC guidance on quarantine practices and warning signs requiring medical care as well as to answer any questions they may have.

AZ HEROES staff prepare and distribute self-collection kits to the study participants, including detailed paper and video instructions. The laboratory provides feedback on specimens that were unable to be tested because of participant error in collection or shipping of the sample (eg, leaking or missing required components). This feedback is utilized to re-educate participants.

Enrolled participants participate in active surveillance via weekly surveys, explained in detail in the Data Collection section.

Data Collection

Overview

Active surveillance for acute illness is conducted throughout the study period. Participants are prompted to begin surveillance in the week following study enrollment and completion of the baseline survey. Each week, all participants are contacted via text message on their predesignated surveillance day (described in detail below). At the end of each text message exchange, the participant is reminded to collect a weekly specimen on their assigned day for collection.

Active Surveillance Surveys

As a part of active surveillance, participants are contacted weekly via secure SMS text messages, via Twilio, asking them two standardized questions about their general health status and presence of CLI symptoms. Twilio is a text messaging service that can read and write into the study REDCap database and customize questions based on participant responses. In addition to the two standardized questions, each week they receive one of four sets of rotating questions about changes in their occupational SARS-CoV-2 exposure, community and household exposure, and attitudes and beliefs surrounding COVID-19 risk. Any individual who indicates CLI in a weekly survey, or by contacting AZ HEROES staff directly, completes additional information via a mobile-friendly webform, including the participant’s symptoms, self-reported severity, duration, self-reported medical treatment, function during and after illness, and details about the resolution of their illness.

Self-reported Data

Participants who indicate they have experienced CLI in the last 7 days are moved to an acute illness monitoring flow, where they are instructed to collect and ship an acute illness kit and complete additional questions about their illness episode. Individuals can also be placed into the acute illness monitoring flow by notifying study staff that they are ill. Participants remain in the acute illness arm until they self-report that their illness has resolved. Before returning to the weekly active surveillance flow, participants complete a recovery survey in which they confirm duration of illness and answer questions about atypical symptoms, productivity loss, and use of health services. Participants continue to take weekly respiratory specimens throughout their acute illness monitoring.

Vaccine Information

Participants are asked a series of questions to assess their knowledge, attitudes, and practices (KAPs) related to SARS-CoV-2 vaccination in the enrollment and/or follow-up survey to capture the information prior to vaccination. Similar to previous KAP studies of influenza vaccines [39,40], participants are asked how much they know about the COVID-19 vaccines, if they received the vaccine, their intention to receive one if they have not, how safe and effective they think the vaccines are, and how likely they are to get sick if they do not receive a vaccine.

Through partnerships with state and county health departments, we track the timing and distribution of COVID-19 vaccines to know when they will be available to individuals within the study.

To capture vaccination information, participants are periodically asked if they have been vaccinated. If they have not, they indicate if they plan to be vaccinated in the upcoming 8 weeks, indicating how many weeks. The form is re-sent in 8 weeks if the participant indicates that they do not know when they will be vaccinated. Once vaccinated, participants complete a brief webform including date of vaccination, vaccine manufacturer, and order in sequence (eg, first or second) for vaccines requiring multiple doses. State Immunization Information System registries will be used as a backup to capture vaccine information about individuals who do not share the information with the study via text message, and for confirmation and completeness on individuals who do receive the vaccine. Participants consent to having their vaccination verified upon enrollment.

Laboratory Methods

Respiratory Specimens

Participants are asked to self-collect a respiratory specimen each week of the study period. Sampling kits are provided to all study participants, which include collection and shipping supplies for 8 weeks of collections, along with illustrated instructions on how to properly collect and ship their respiratory specimens. Study staff track the use of specimen kits and ship replenishments to participants as needed. Each week, regardless of symptoms, participants collect an anterior mid-turbinate nasal swab on both nares, using a flocked swab or equivalent, and place it into a tube containing viral transport media (VTM). If participants experience CLI, they use an acute illness kit, which consists of materials to collect a nasal swab in VTM and a saliva specimen in a saliva collection tube. All specimens are shipped with a cold pack, using priority overnight express shipping to a CDC-designated laboratory following International Air Transport Association guidelines [41]. Upon receipt by the laboratory, specimens are aliquoted and analyzed for SARS-CoV-2 using an rRT-PCR method [42] under FDA EUA. Remaining aliquots are maintained for additional analysis, banking, or long-term storage.

Blood Specimens

All participants contribute 40 mL of whole blood at enrollment, at 11- to 13-week intervals, and following positive rRT-PCR or vaccination events. Participants can submit specimens at participating laboratories closest to the participant’s residence or work. If a participant does not develop symptoms, but SARS-CoV-2 is detected in a weekly specimen, participants are instructed to submit a blood sample approximately 4 weeks following the date of first rRT-PCR detection; if the participant experiences CLI within 2 weeks of virus detection, they are instructed to submit a blood sample 4 weeks after initial symptom onset. If the participant has a convalescent blood specimen drawn prior to another planned repeat blood collection, the scheduling of the following blood collections will be 11 to 13 weeks following the convalescent draw. Participants who receive the COVID-19 vaccine during the study period are asked to provide a blood specimen 14 to 21 days after each dose of the vaccine—with the first postvaccination blood draw collected prior to the second vaccination dose, if relevant—and then every 11 to 13 weeks as described above. Information on adverse events and symptoms related to vaccination will be collected retrospectively after participants receive both doses of the vaccine.

Whole blood is collected and processed using CDC guidelines for serum collection [43]. The serum specimens are divided into aliquots labeled with the same study ID and specimen ID on all tubes, and an aliquot ID unique to each tube. All specimens are stored at −70 °C or colder prior to SARS-CoV-2 antibody analysis or long-term storage. At the University of Arizona, the serum is tested for antibodies against the receptor binding domain of the spike protein and verified with the S2 domain of S protein antibodies, as previously described [24], using the FDA EUA test (ID 201116). This testing at study entry is used to ensure correct placement of AZ HEROES participants into seronegative or seropositive groups.

Data Collection and Security

Most research activities occur through electronic communications (ie, email, text, and internet-based surveys), telephone contacts, or via postal or express mail, minimizing direct contact between study staff and participants. All surveys are self-administered by participants on a computer or smartphone. Surveys can also be administered by telephone or mail should participants be unable or become unwilling to access them online. Participant information given to study staff via phone or email conversation is entered and stored in the REDCap database by study staff. Alternatively, data are imported into the REDCap database from Twilio for participant responses to text surveillance or by direct participant response into the REDCap database.

Data Management

REDCap

A study database is maintained in REDCap. Tracking databases with patient identifiers and contact information are securely kept according to the University of Arizona standard operating procedures with respect to cybersecurity, privacy, patient confidentiality, and compliance with applicable patient privacy regulations. Any study-related documents with personal identifiers are stored in a locked cabinet in lockable offices on campus. All study-related documents and specimens contain a unique identifier for each participant. Data entry forms provide some quality assurance using logic and range checks as well as automated skip patterns. The research team performs additional data quality checks on a weekly basis, including assessments of missing data. Laboratory results are entered directly into the REDCap study database from the study reference laboratory, including results from rRT-PCR assays and serologic assays. If a reference laboratory is not able to enter data directly, the laboratory is provided with a laboratory results reporting template that is then merged with study data using the specimen ID.

Twilio

Twilio is a cloud-based communications platform that allows for automated text messaging chains to be sent to study participants. It is used to send weekly and illness monitoring questions to participants. Participant responses are stored in Twilio until sent as a batch to the REDCap database once per day.

Statistical Considerations

Power Analysis

Our goal is to recruit 4000 participants, split evenly between seronegative and seropositive individuals. Among the seronegative cohort, we estimated that a sample of more than 852 participants is required to achieve 80% power (α=.05) to detect a true incidence of SARS-CoV-2 infection of 4%; the enrolled cohort exceeds this sample estimate at the drafting of this report. Thus, we expect to be sufficiently powered to make overall estimates and estimates by two-level strata, such as age, sex, or HCP versus others. Power estimation for COVID-19 vaccine effectiveness (VE) was performed using Monte Carlo simulation to generate survival time over 12 months based on varying vaccine coverage—with quarterly increases in two-dose vaccine coverage from 0% to 80% among HCP, 70% for first responders, and 30% for OEWs—and varying SARS-CoV-2 incidence rate, from 0.67% to 1.42% monthly attack rate, using the equations proposed by Austin and a Cox marginal model [44]. Based on 1000 simulations, with 2000 participants in the seronegative stratum, the study is estimated to have over 80% power to detect a true VE of 75%. If the data are pooled with similar studies using common methodologies to a total of 5000 subjects, the combined analysis is estimated to have 99% power to detect a true VE of 75% using the same assumptions.

Data Analysis

To estimate the incidence of SARS-CoV-2 infection and the corresponding 95% confidence intervals in essential workers, we will fit negative binomial regression models with person-time at risk as an offset. We will examine incidence of rRT-PCR–confirmed infections by occupation, symptom presentation, close contact exposure, and demographic variables. Logistic regression and negative binomial models will be used to estimate the risk of infection in different occupational groups. In the logistic regression model, we will include the log-transformed person-weeks as the offset. The model will then be adjusted by symptom presentation, demographic factors, study site, and health care utilization. The VE (1 − confirmed cases of COVID-19 illness per 1000 person-weeks among vaccinated essential workers ÷ confirmed cases of COVID-19 illness per 1000 person-weeks among unvaccinated essential workers × 100%) with 95% confidence interval will be estimated by a negative binomial regression model. The potential confounders, such as study site and previously seropositive status, will be included in the model. We will apply nonlinear mixed models to describe individual and group mean trajectories in neutralizing antibody titers over time. We will classify and identify subgroups of cases by self-reported clinical severity, health care utilization, occupational and community exposures, and duration of symptoms. These models will help elucidate the patterns of serologic immunity.

Ethical Considerations

This study was reviewed and approved by the Arizona Department of Health and the University of Arizona Institutional Review Boards (IRBs) (see Code of Federal Regulations, Title 45, Part 46.114 [45]). The CDC and the Arizona Department of Health Services (ADHS) IRBs have reviewed the project. The ADHS IRB has approved the project and the CDC IRB deferred to the University of Arizona IRB. The College of Public Health at the University of Arizona houses all IRB and required study documentation. All participants complete informed consent electronically through the REDCap study database system. Research staff verify that participants understand key study activities, are aware of risks, and agree to participate prior to countersigning to confirm consent. Participants receive the results of their weekly and illness COVID-19 tests as well as the results of their antibody testing.

Results

The AZ HEROES study was funded by the CDC. Enrollment began on July 27, 2020; as of May 1, 2021, a total of 3165 participants have been enrolled in the study. Enrollment is expected to continue through December 1, 2021, with data collection continuing through at least April 2022, contingent upon funding.

Discussion

Overview

Submission of weekly and CLI-onset swabs for SARS-CoV-2 rRT-PCR testing by AZ HEROES study participants is a high priority, as it allows researchers to estimate incidence of symptomatic and asymptomatic COVID-19. Currently, interest in receiving weekly nasal swab testing is high, with participants considering regular testing to be a substantial benefit, given high SARS-CoV-2 transmission rates in the community. When transmission rates in the community drop, or seropositivity increases due to natural infection or vaccination, this testing may be perceived by the study participants as more of a burden than a benefit. To maintain submission at acceptable rates at later time points in the study, monetary incentives have been included in the protocol. Methods for participant engagement through newsletters and reminders from study staff continue to evolve as the pandemic unfolds.

Strengths

One strength of the study is the inclusion of 4000 individuals with substantial occupational exposure to SARS-CoV-2 owing to their work as HCP, first responders, and OEWs. Additionally, the enrolled population will be generally representative of the racial and ethnic demographics of Arizona, which ensures inclusion of high-risk groups, such as Hispanic and American Indian communities, previously found to be at increased risk for COVID-19 [8]. The longitudinal cohort study design allows for ongoing consistent and comprehensive symptom assessment, exposure assessment, and examination of KAPs related to SARS-CoV-2 infection and vaccination. Further, the serial blood sampling component of the study enables us to fully examine variations in immune response to infection and vaccination.

Limitations

This study has several limitations. First, the ability to generalize trends related to infection incidence, disease severity, and immunologic response in our population of essential workers will likely be biased by the healthy worker effect. Second, the information retrieved from participants is principally self-reported or self-collected, which might introduce recall bias, particularly if participants do not complete rRT-PCR specimen collection and surveys consistently. Third, there may be a sampling bias related to the requirement that participants utilize computers and phones to complete surveys. Finally, not meeting enrollment targets and/or the length of the study period (1 year) may hamper the ability to assess reinfection rates, for example, because immunity for SARS-CoV-2 might last for more than 1 year.

Conclusions

In conclusion, the design, recruitment, enrollment, and research activities of the AZ HEROES study provide a unique opportunity to improve our understanding of the incidence of SARS-CoV-2 infection, disease course, antibody and vaccine response, and KAPs among essential workers in the state of Arizona.