Setting

This quasi experimental time series study took place at UPMC Presbyterian, a 695-bed adult tertiary academic acute care hospital which provides Level 1 trauma, critical care, and organ transplant services, comprising 34 inpatient units; all inpatient units were included. The proportion of beds in a cohorted room (two beds per room) in the hospital is approximately 26% of inpatient beds.

All patients admitted to the hospital not known to have MRSA carriage are ordered to have admission and weekly active surveillance nares screening performed by culture for MRSA; median (interquartile range) facility-wide monthly adherence rates for admission and weekly swabs during the study periods were 80.6% (77.6, 84.2) and 55.9% (49.4, 60.6), respectively (Supplemental Figure 1), and the admission prevalence during the study period was 2.0%. The median (interquartile range) intensive care unit (ICU)-specific monthly adherence rates for admission and weekly swabs during the study periods were 91.5% (87.6, 94.9) and 30.6% (20.2, 45.6), respectively (Supplemental Figure 1), and the admission prevalence during the study period was 2.3%. A patient’s MRSA carriage indicator in the electronic health record could be removed if the following criteria were met: (1) no less than 30 days had passed since the last positive culture (surveillance or clinical culture), (2) at least 7 days had passed since receipt of antimicrobial with activity against MRSA, and (3) three consecutive negative nares cultures were collected at least 24 hours apart. Prior to the intervention, patients with current or prior MRSA carriage (colonized or infected) were admitted to a single occupancy room or were cohorted with another patient with concurrent or prior MRSA carriage; subsequent to the intervention, MRSA carriage did not affect bed placement. Other infection prevention approaches potentially affecting MRSA outcome ascertainment and transmission did not change in the study period (Supplemental Table 1).

Study design

This study measures MRSA HAI outcomes before and after DcCP in December 2020, including a pre-intervention period January 2019 through November 2020 and a post-intervention period December 2020 through December 2022. Contact precautions—using gown and gloves for all care involving patient contact and in patient’s environment—were used for patients identified as MRSA carriers until December 2020 after which they were no longer required for care of patients with prior or current MRSA infections or colonization. No units were excluded from DcCP. Before and after the intervention, as part of standard precautions, use of gowns and gloves were recommended for any potential contact with blood or body fluids including draining wounds. The use of CP for vancomycin-resistant enterococci (VRE) among carriers, and VRE active surveillance for all patients, was employed during the entire study period. During the post-intervention period, VRE and MRSA co-infection was noted in two patients, hence requiring use of CP.

We measured two co-primary outcomes: National Healthcare Safety Network (NHSN) reported MRSA HAI rates and the frequency of WGS-confirmed MRSA transmission events. NSHN HAI were defined for all HAI types using NHSN procedures. ^12,13 WGS surveillance was performed on MRSA isolates from clinical specimens identified ≥3 days after hospitalization or within 30 days of a prior healthcare exposure. Isolates from asymptomatic screening were not included. DNA was extracted from patient isolates using MagMAX DNA extraction kit on King Fisher Apex and sequencing libraries were prepared using Illumina DNA Prep Tagmentation kit on an Eppendorf EpMotion liquid handler per manufacturer’s instructions. Samples were pooled in equimolar concentration and then sequenced on an Illumina NextSeq 550 using the v2.5, 300 cycle kit. The resulting WGS reads were assembled using Unicycler v0.5.0, ^{Reference Wick, Judd, Gorrie and Holt14} annotated using Prokka v1.14, ^{Reference Seemann15} and species were determined using Kraken2. ^{Reference Wood, Lu and Langmead16} Transmission clusters were determined by computing the pairwise single nucleotide polymorphisms (SNPs) among the patient isolates of the same species in the database (restricted to the period WGS was performed) using Snippy v4.3.0 ¹⁷ or SKA v1.0. ^{Reference Harris18} Isolate pairs with 15 or fewer pairwise core genome SNP differences were considered genetically related, representing transmission. ^{Reference Sundermann, Chen and Kumar19} WGS events were considered attributable to the study period if the isolate was the second or subsequent genetically related isolate with a “source” isolate during the study period (including pre-DcCP or post-DcCP periods). The related isolates were also examined for geo-temporal and procedural commonalities: transmission events for which the patient pair were cared for on the same unit with at least one day of overlap on the unit, or who received care from a specific healthcare worker concomitantly, were considered epidemiologically linked.

WGS was performed as part of a preexisting research investigation in two different stages: Isolates were banked and analyzed retrospectively until August 2019, and from January 2022 onward WGS was performed in “real time” with infection preventionist notification of genetically related pairs. ^{Reference Sundermann, Chen and Kumar19,Reference Sundermann, Srinivasa and Waggle20} At the time of the current analysis, isolates from September 2019 to December 2021 were not sequenced. Therefore, the analysis periods for WGS-confirmed transmission were restricted to the availability of WGS data during the study periods: January through August 2019 during the use of CP and January through December 2022 after DcCP (Figure 1).

Figure 1. The frequency of co-primary outcomes of methicillin-resistant Staphylococcus aureus healthcare-associated infections and whole genome sequencing-defined transmission events before and after discontinuation of contact precautions. Note: WGS, whole genome sequencing. Arrow indicates date of study intervention.

This investigation was approved (Project 4222) as a quality improvement project by the UPMC Quality Improvement Review Committee.

Statistical analysis

To evaluate the impact of DcCP on HAI rates, we performed a time series analysis of MRSA HAI rates before and after DcCP, using a linear regression model to calculate the step change and change in slope. The frequency of subcategories of HAI in each study period were descriptive in nature. To compare the change in HAI and WGS-defined attributable transmission events, we calculated an incidence rate ratio (IRR), 95% confidence intervals (95%CI), and P values using a median-unbiased estimation. Characteristics of WGS-defined transmission events were descriptive. Each co-primary outcome was calculated per 10,000 patient days; as a sensitivity analysis, we calculated these outcomes per 1,000 patient admissions.

We also performed several exploratory analyses. Because MRSA transmission and HAI is more common in ICUs than non-ICUs, ^{Reference Evans, Kralovic, Simbartl, Jain and Roselle21} we analyzed HAI attributed to ICU locations per 10,000 critical care patient days. One estimate of transmission is acquisition of asymptomatic carriage in individuals without prior MRSA carriage; therefore, we calculated the new acquisition rate per 10,000 patient days as measured using by routine active surveillance. Since CP did not change for VRE during the study period, we calculated the rate of VRE HAI per 10,000 patient days to serve as a non-intervention comparison. These rates were evaluated as time series analyses as described for the primary HAI outcome and qualitatively compared to the findings for the primary HAI outcome. All analyses were performed using Stata version 16.0 software (StataCorp, College Station, TX).