Study design

We conducted a secondary analysis using data collected from November 2, 2017, to February 28, 2020, from the New Vaccine Network (NVSN). NVSN is an ongoing multi-center, active, prospective ARI surveillance study in children (<18 years) funded by the Centers for Disease Control and Prevention (CDC). ^{Reference Campbell, Ogokeh and Lively14,Reference Rha, Curns and Lively15} This study only includes data collected at the Nashville, Tennessee site. Year-round recruitment occurred 4 days per week in the ED and 7 days per week in the inpatient setting at the Monroe Carell Jr. Children’s Hospital at Vanderbilt University Medical Center (VUMC). Institutional Review Boards at VUMC and the CDC reviewed and approved this study. ¹⁶

Study population

Children were eligible if they presented to an ED or were hospitalized within 48 hours of presentation and had at least one of the following symptoms in the 14 days prior to enrollment: fever, cough, earache, nasal congestion, runny nose, sore throat, post-tussive vomiting, wheezing, shortness of breath, rapid or shallow breathing, myalgia, apnea, apparent life-threatening event, or brief resolved unexplained event (eg, unresponsive, etc.). ^{Reference Campbell, Ogokeh and Lively14,Reference Rha, Curns and Lively15} In addition, eligible children had to live within the catchment/surveillance area (eg, Davidson, Williamson, Cheatham, Dickson, Rutherford, Montgomery, Roberson, and Sumner Counties). Children were excluded if they met any of the following criteria: chemotherapy-associated fever and neutropenia (absolute neutrophil count <500 × 10³/µL), newborns never discharged since birth, transferred to VUMC from another hospital >48 hours after initial admission, recently hospitalized (≤5 days), or previously enrolled in the study within the past 14 days. ^{Reference Campbell, Ogokeh and Lively14,Reference Rha, Curns and Lively15}

We also excluded children younger than 30 days to minimize the inclusion of serious bacterial infections due to differences in clinical management practices, and children with multiple ARI enrollments <90 days apart. We considered children with multiple ARI enrollments (≥90 days from the prior visit) as susceptible to a new viral or bacterial ARI, thus increasing the potential for additional provider-ordered viral testing and antibiotic use.

Illness history, clinical characteristics, and provider-ordered testing

After obtaining informed consent, parents/guardians of enrolled children were interviewed by trained research personnel to collect demographic (age, sex, race, and ethnicity) information, parent-reported clinical symptoms (eg, fever, myalgia, lethargy, etc.), and past medical history using a standardized form. Provider-ordered viral testing (ie, influenza antigen, respiratory syncytial virus (RSV) antigen, and molecular respiratory testing), vital signs at time of presentation, physical exam findings, other clinical lab testing (ie, rapid Streptococcus antigen testing and bacterial cultures), the first five discharge diagnoses (International Classification of Diseases, Tenth Revision [ICD-10]), and active and completed antibiotics were abstracted from each child’s medical record. Final clinical disposition was determined by the highest level of care provided to the child during the visit (ie, children enrolled in the ED and later hospitalized were considered inpatient). At VUMC, molecular respiratory testing is performed using BioFire® FilmArray Respiratory Pathogen Panel 2.0 and consists of the following targets: adenovirus, non-pandemic coronavirus strains (229E, HKU1, NL63, OC43), human metapneumovirus, influenza, parainfluenza (types 1–4), rhinovirus/enterovirus, RSV, and respiratory bacterial pathogens (ie, Bordetella pertussis, Chlamydophilia pneumoniae, Legionella pneumophilia, and Mycoplasma pneumoniae). ^{Reference Haddadin, Rankin and Lipworth17,Reference Probst, Datyner and Haddadin18} The exposure variable was defined as receipt of at least one provider-order viral test, including rapid influenza antigen, rapid RSV antigen, and/or molecular, dichotomized as tested versus not tested (referent).

Interview, medical record, and laboratory results were maintained in a secure REDCap™ (Research Electronic Data Capture, Vanderbilt University, Nashville, TN, USA) database. ^{Reference Harris, Taylor, Thielke, Payne, Gonzalez and Conde19}

Antibiotic administration and tiered discharge diagnoses

We defined our outcome variable as antibiotic prescribed during the child’s ED visit or administered during hospitalization. Antibiotics were categorized in three main groups: (1) None administered; (2) Narrow-spectrum (eg, penicillins, tetracyclines, first-generation cephalosporins, and sulfonamides); and (3) Broad-spectrum [eg, macrolides (azithromycin), amoxicillin-clavulanate, advanced-generation cephalosporins, quinolones, and clindamycin]. ^{Reference Havers, Hicks and Chung20,Reference Gerber, Hersh, Kronman, Newland, Ross and Metjian21} In the instance both narrow- and broad-spectrum antibiotics were administered/prescribed during the child’s healthcare visit/stay, broad-spectrum was assigned (eTable 1 in Supplement).

We classified ICD-10 discharge diagnoses based on the indication for an antibiotic using CDC’s tiered diagnosis system (Tier 1—antibiotics almost always indicated; Tier 2—antibiotics may be indicated; Tier 3—antibotics are not indicated or indications are unclear). ^{Reference Hersh, King, Shapiro, Hicks and Fleming-Dutra6} If a child’s visit had ICD-10 codes in multiple tiers, priority was given to Tier 1 diagnoses, followed by Tier 2 and Tier 3 diagnoses. ^{Reference Hersh, King, Shapiro, Hicks and Fleming-Dutra6} Tiered diagnoses were further compared to antibiotic treatment and provider-ordered viral testing in healthcare setting.

Statistical analysis

We summarized children’s sociodemographic and clinical characteristics by setting using frequency (percent) for categorical variables and mean (standard deviation) for continuous variables. We performed multiple imputations for 213 children with ≥1 missing covariate information, using predictive mean matching with 10 imputation samples. ^{Reference Frank and Harrell22}

For each healthcare setting, confounders were assessed through directed acyclic graphs (eFigure 1 in Supplement) generated using prior knowledge. Setting-specific models were built using unconditional polytomous logistic regression with robust sandwich estimators (to account for repeat enrollments) to estimate adjusted odds ratios (aORs) and 95% confidence intervals between provider-ordered viral testing (ie, tested versus not tested) and provider-ordered viral test result (ie, positive test versus not tested and negative test versus not tested) and three-level antibiotic administration (ie, no antibiotics prescribed/administered [referent], narrow-spectrum, or broad-spectrum). Restricted cubic splines were generated for continuous covariates (eTable 2 in Supplement). Models were adjusted for parent-reported pulmonary symptoms (cough, nasal congestion, rhinorrhea, wheezing, and shortness of breath; yes or no), provider documented wheezing (yes or no), retractions (yes or no), time of year (respiratory season [October–April] or non-respiratory season), any underlying medical condition (yes or no), insurance (none/self-pay, private, or public), temperature [none, moderate (≥100.4°F to <102.0°F), or severe (≥102.0°F)], age (years), heart rate (beats/minute), respiratory rate (breaths/minute), oxygen saturation (capillary), illness duration (days), and multiplicative interactions between age and heart rate and age and respiratory rate. We performed an exploratory analysis evaluating the impact of viral/bacterial pathogen detected and the receipt of antibiotics. Statistical tests were based on two-tailed probability with a significance level (α) set at 5%. All analyses were performed in R (version 3.6.1).