Serial Testing for SARS-CoV-2 and Virus Whole Genome Sequencing Inform Infection Risk at Two Skilled Nursing Facilities with COVID-19 Outbreaks — Minnesota, April–June 2020

SARS-CoV-2, the virus that causes coronavirus disease 2019 (COVID-19), can spread rapidly in high-risk congregate settings such as skilled nursing facilities (SNFs) (1). In Minnesota, SNF-associated cases accounted for 3,950 (8%) of 48,711 COVID-19 cases reported through July 21, 2020; 35% of SNF-associated cases involved health care personnel (HCP*), including six deaths. Facility-wide, serial testing in SNFs has been used to identify residents with asymptomatic and presymptomatic SARS-CoV-2 infection to inform mitigation efforts, including cohorting of residents with positive test results and exclusion of infected HCP from the workplace (2,3). During April–June 2020, the Minnesota Department of Health (MDH), with CDC assistance, conducted weekly serial testing at two SNFs experiencing COVID-19 outbreaks. Among 259 tested residents, and 341 tested HCP, 64% and 33%, respectively, had positive reverse transcription–polymerase chain reaction (RT-PCR) SARS-CoV-2 test results. Continued SARS-CoV-2 transmission was potentially facilitated by lapses in infection prevention and control (IPC) practices, up to 12-day delays in receiving HCP test results (53%) at one facility, and incomplete HCP participation (71%). Genetic sequencing demonstrated that SARS-CoV-2 viral genomes from HCP and resident specimens were clustered by facility, suggesting facility-based transmission. Residents and HCP working in SNFs are at risk for infection with SARS-CoV-2. As part of comprehensive COVID-19 preparation and response, including early identification of cases, SNFs should conduct serial testing of residents and HCP, maximize HCP testing participation, ensure availability of personal protective equipment (PPE), and enhance IPC practices^† (4–5).

Interim guidance for HCP mask use and SNF visitor restriction was implemented statewide by March 31, 2020; however, during April, an increase in COVID-19 diagnoses and deaths among SNF residents in Minnesota occurred. In light of the release of CDC interim guidance on May 1 (6), and in an effort to improve IPC and implement facility-wide SARS-CoV-2 testing, two SNFs located in the Minneapolis-St. Paul metropolitan area contacted MDH after identifying multiple confirmed resident and HCP COVID-19 cases. During April 30–June 12, nasal, nasopharyngeal, or oral swabs were collected from residents and HCP and were tested to detect SARS-CoV-2 nucleic acid by RT-PCR, which was conducted at MDH Public Health Laboratory (MDH-PHL) and multiple commercial laboratories (6). After a first round of testing on April 30 and May 7 in facilities A and B, respectively, serial testing was conducted in residents every 7–10 days. HCP were offered testing services at the facility during serial testing of residents as well as whenever it was convenient to account for work schedules. Residents and HCP with positive test results were excluded from future serial testing. Starting in mid-March, HCP were screened daily for COVID-19–compatible symptoms, and symptomatic HCP were sent home per MDH and CDC guidance.^§ Symptomatic residents and HCP were tested outside of scheduled serial testing. Data on symptoms, demographic characteristics, and HCP work assignment were collected from resident charts, MDH COVID-19 case interviews, and SNF administrator interviews. MDH and CDC provided frequent onsite IPC assessment to both facilities, including review of cohorting, hand hygiene practices, and use of PPE. Residents with positive SARS-CoV-2 test results were moved to a COVID-19 care unit within each facility, and HCP with positive test results were excluded from work for at least 10 days (7). Whole genome sequencing was conducted by MDH-PHL on available^¶ specimens using previously described methods (8). Phylogenetic relationships, including distinct clustering of viral whole genome sequences, were inferred based on nucleotide differences via IQ-TREE, using general time reversible substitution models (9) as a part of the Nextstrain workflow (10). Descriptive analyses were conducted using R (version 3.6.1; The R Foundation). This activity was reviewed by CDC and was conducted consistent with applicable federal law and CDC policy.**

Acknowledgments

Kris Bisgard, Stephanie Rutledge, Diya Surie, Jennifer Hunter, Sarah Kabbani, Isaac Benowitz, Kelly Quinn, Deshella Dallas, CDC; Kirk Smith, staff members and leadership from the Minnesota Department of Health and State Emergency Operating Center COVID-19 response; all staff members and residents at facility A and B.

Corresponding author: Joanne Taylor, okp2@cdc.gov.

¹CDC COVID-19 Response Team; ²Minnesota Department of Health; ³Epidemic Intelligence Service, CDC.

References

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FIGURE 1. Date of serial testing round and daily specimen test results*^,†,§ for SARS-CoV-2 detection by reverse transcription–polymerase chain reaction (RT-PCR) testing — two skilled nursing facilities, Minnesota, April–June 2020

Abbreviation: HCP = health care personnel.

* In facility A, two residents had indeterminate results for specimens collected on April 30; one resident had a positive test result on May 7 and one resident had another indeterminate test result on May 11 before a negative test result on May 14.

^† In facility A, one HCP had an indeterminate test result on May 21 and was not retested.

^§ In facility B, one resident had an indeterminate result on May 7 and had a positive test result on May 14, one resident had an indeterminate result on May 28 and had a negative test result on June 4, and one resident had an indeterminate result on June 4 and had a negative test result on June 8.

Abbreviations: COVID-19 = coronavirus disease 2019; N/A = not applicable.
* Symptoms screening data incomplete for three residents at facility A and two residents at facility B. At facility A, one resident was discharged to another facility 2 days after a positive test result (presumed asymptomatic), one resident was evaluated at a hospital for abdominal pain and had a positive SARS-CoV-2 test result the following day (presumed asymptomatic), and one resident was evaluated at a hospital for severe chest pain and decreased oxygen saturation 4 days after a positive test result (presumed symptom onset ≤14 days after testing). At facility B, one resident was evaluated at a hospital for shortness of breath 7 days after positive SARS-CoV-2 test result (presumed symptom onset ≤14 days after testing), and one resident was admitted to hospital unresponsive with low oxygen saturation on date of testing (presumed symptomatic on date of testing).
^† Eight HCP at facility A and 41 HCP at facility B were not interviewed by Minnesota Department of Health. All HCP were screened for symptoms and temperature upon entering the facility and excluded if they had COVID-19–compatible symptoms; therefore, HCP with unknown or missing symptoms data who tested on the day of a facility-wide screening (six HCP at facility A and 39 HCP at facility B) were presumed asymptomatic on date of testing. HCP with unknown or missing symptoms data who were tested by their primary care provider (three HCP at facility A and three HCP at facility B) were presumed symptomatic on date of testing.
^§ Memory care unit was located on second floor or third floor.

FIGURE 2. Phylogenetic trees showing genetic distance between available* SARS-CoV-2 virus specimens collected from health care personnel (HCP) and residents at facility A^† and facility B^§— Minnesota, April–June 2020

* Genetic divergence based on nucleotide difference is indicated by length of branches. Available specimens included specimens tested and stored at Minnesota Public Health Laboratory and commercial labs where specimens could be retrieved and where RNA could be extracted.

^† Available specimens from facility A included HCP and residents diagnosed after April 29. At facility A, 17 resident and five HCP specimens had genetically similar virus strains, including one HCP with limited resident contact. Two HCP had virus sequences that were genetically different from the facility A cluster and were more similar to cases associated with community transmission in Minnesota. A third strain identified in a resident during the third testing round was genetically different from both HCP and resident strains.

^§ Available specimens from facility B included HCP diagnosed after May 6 and residents diagnosed after April 29, throughout the outbreak. At facility B, 75 resident specimens and five HCP specimens shared genetically related strains.