Hepatitis A Case Investigation

For all persons clinically diagnosed with hepatitis A, hospital and commercial laboratories were asked to forward available specimens to the FDOH Bureau of Public Health Laboratories (BPHL) for hepatitis A virus (HAV) genotyping based on the VP1-P2B junction region (17). Next-generation sequencing was performed on the MiSeq (Illumina) platform, and bioinformatics data processing used the Centers for Disease Control and Prevention (CDC) Global Hepatitis Outbreak Surveillance Technology (GHOST) platform (18). Investigation guidelines in Florida require that a case of hepatitis A in a food employee be further investigated to assess risk for possible food item or food preparation system contamination, which might also involve an environmental assessment. FDOH considered patron notification or suspension orders for food establishments, dependent upon the outcome of the risk assessments conducted.

IMD Case Investigation

For persons with diagnosed IMD, isolates of Neisseria meningitidis were forwarded to BPHL for serogrouping by slide agglutination, and further characterization by whole-genome sequencing on MiSeq or NextSeq550 (Illumina) systems. Select specimens were also forwarded to CDC laboratories for additional characterization or confirmation. We analyzed sequencing data by using BPHL’s FLAQ-AMR pipeline (https://github.com/BPHL-Molecular/flaq_amr) to assess sequence quality and identify the sequence type (ST) and submitted data to CDC’s Bacterial Meningitis Genome Analysis Platform (BMGAP; https://github.com/CDCgov/BMGAP) to identify the clonal complex (CC) and to verify serogroup for each isolate (19). We identified outbreak-associated cases by serogroup, ST, and CC, and constructed phylogenetic trees.

Mpox Case Investigation

In May 2022, FDOH notified healthcare providers and laboratories that mpox was considered reportable under existing rules. FDOH adopted the national surveillance case definition. That definition initially included clinical manifestations as a criterion, but on July 22, 2022, was modified to focus on laboratory results and epidemiologic risk factors for probable and confirmed cases (20).

Initially, all testing for orthopoxvirus and mpox virus infections was conducted at BPHL and CDC using previously described procedures (21,22). In July 2022, use of the nonvariola orthopoxvirus assay expanded to commercial laboratories (23). Molecular subtyping of isolates from mpox patients in Florida was not routinely done for surveillance purposes during the study period; however, CDC performed partial or full sequencing for a subset of samples (24,25).

Epidemiology and Analyses

FDOH Bureau of Epidemiology operates an electronic patient-based reportable disease surveillance system known as Merlin. Using data from Merlin, we identified persons meeting the outbreak case definition for >1 disease in the 3 concurrent outbreaks. We used data from other surveillance systems operated by the Bureau of Communicable Diseases for sexually transmitted infections (STIs) and HIV to ascertain history and risk factors for reportable STIs (e.g., chlamydia, gonorrhea, or syphilis) and HIV infection. We matched patient profiles between systems by using name, sex, date of birth, and address information.

We calculated descriptive statistics to characterize outbreak-related cases by person, place, and time. We assessed pairwise differences in median age via Dunn test and conducted χ² tests to compare cases of each disease by HIV infection, history of recent STI, and Orange County residency. We used 2-sided tests in all statistical analyses and considered p<0.05 statistically significant.

To assess the role of the public health response in controlling the concurrent outbreaks, we analyzed data from the statewide immunization registry by vaccine antigen and month of first dose administered. To distinguish outbreak response efforts from routine childhood or adolescent immunization, we limited data to vaccines administered to adults >18 years of age. We stratified data by persons receiving vaccine from a county health department (CHD) provider. To further characterize synergies in outbreak response efforts, we identified instances of vaccine administration to the same person, on the same day, against >1 of the diseases in the concurrent outbreaks. This activity was reviewed by the Ethics and Human Research Protection Program of FDOH and by CDC and was determined by both institutions to be public health practice, outbreak investigation, not requiring review and approval by an institutional review board.

Hepatitis A Cases

During the analysis period, a total of 322 hepatitis A cases among Florida residents were reported to FDOH; 153 (48%) met the outbreak case definition. Of nonoutbreak cases during that period, ≈50% had an identifiable risk factor for hepatitis A, among which 60% were associated with recent international travel. Among the 153 outbreak-associated cases, 95% were in male persons and 5% in female persons, 74% were in MSM, and 21% were in persons with HIV; 1 death occurred (Table 2). Among persons for whom sexual history was obtained, 25% reported no sexual contacts in the previous 3 months; 8% reported >5 sexual partners, and 22% reported recent sexual contact with a person whose identity was not known. Seventeen cases were identified among food employees, but no foodborne transmission was documented. Environmental assessments performed at food establishments where exposure might have occurred did not necessitate FDOH orders for patron notification or suspension of service.

Among outbreak-associated cases, 67 (44%) met the confirmed case classification, among which 60 cases had matching HAV genotype IA, GHOST cluster A17 cluster 21 (a.k.a. SC076 US-Mexican); the remaining 7 confirmed cases had an epidemiologic link to a laboratory-confirmed case. We excluded 4 cases from the outbreak that otherwise met the probable or suspected outbreak case classification because HAV sequencing results did not match the outbreak cluster type. Of the 60 cases with the matching HAV outbreak cluster type, 2 patients appear to be outliers and had no identifiable risk factors or recognized exposures to HAV. One case was in a 74-year-old heterosexual female person and the other was in a 9-year-old male child. Of the 7 confirmed cases not genotyped but confirmed through epidemiologic linkage, 2 were linked to the 9-year-old patient, his parents, who later became ill, likely because of secondary household transmission; the remaining 5 cases were sexual or household contacts of persons who identified as MSM.

IMD Cases

During the analysis period, 71 IMD cases among Florida residents were reported to FDOH. Of those, 44 (62%) cases were classified as outbreak associated. Among the outbreak cases, 72% were in persons who identified as MSM, 34% were in persons with HIV, and 20% of cases resulted in death (Table 2). The distribution of outbreak-associated cases by type of infection was 55% bacteremia, 20% meningitis, 5% septic arthritis, and 20% with >1 clinical syndrome. Case-fatality was highest (33%) among patients with bacteremia.

Among outbreak-associated cases, 40 (91%) met the confirmed case classification. Of those, 33 were caused by the ST11 CC11 outbreak strain; the other 7 confirmed cases were in persons who identified as MSM and had a serogroup C infection, but further strain characterization was not possible. Ten confirmed cases of the outbreak strain were in persons who did not identify as MSM, including a 77-year-old heterosexual woman with no known epidemiologic link to any other cases and 3 women who had no direct connection to one another but who were sexually active with the same male partner. Those 3 cases represent the only identified epidemiologic linkages among all the IMD cases in this outbreak.

Mpox Cases

During May 10­–November 30, 2022, Florida reported 2,845 confirmed or probable mpox cases among residents. Most cases were locally acquired, but 14% of patients reported out-of-state travel during the 3-week incubation period. Most cases were among adult (>99%) and male (98%) persons. Among cases in adults, 88% were in persons who identified as MSM, but transmission through sexual contact between heterosexual persons was also identified. Among Florida cases, uncommon transmission routes were identified and have been previously reported by FDOH (26–28), including nonsexual household contact (n = 8) and occupational exposure among healthcare workers (n = 2).

Among mpox cases, 52% were in persons living with HIV and 55% in persons who had a history of >1 STI in the previous 2 years (Table 2). For the 1,414 cases with information available regarding previous HIV diagnoses, 10% were diagnosed within the previous year; 93% of cases were in persons who received HIV care within the previous year, 81% were in persons whose HIV infections were virally suppressed, and 6% were in persons who had a recent CD4 count of <200 cells/µL. Few (6%) cases were hospitalized because of mpox; 3 deaths occurred for which mpox was considered a causative or contributing factor. All 3 deaths were in persons who had a previous AIDS diagnosis, and 2 were unhoused.

CDC sequenced 17 mpox virus isolates and identified 16 as clade IIb subclade B.1 (25). One isolate collected early in the outbreak, from a patient with exposure in the United Arab Emirates, was identified as clade IIb subclade A.2 (24).

Outbreak Overlap

We observed temporal overlap for the 3 outbreaks; hepatitis A cases occurred somewhat earlier, and peak incidence was during late March and early April 2022 (Figure 1). Peak incidence for IMD occurred a few weeks later, and 13 cases were reported over a 6-week period during May–June. The number of hepatitis A and IMD cases declined as mpox cases rapidly increased; mpox incidence peaked during late July to early August, then rapidly declined. We did not identify any instances of the same person being part of both the hepatitis A and IMD outbreaks. However, among mpox cases, 4 patients were also part of the hepatitis A outbreak, and 3 others were part of the IMD outbreak (Appendix Table 1).

The greatest concentration of outbreak-associated hepatitis A and IMD cases occurred in the central region of Florida (Figure 2). Orange County had the highest number of cases for both diseases: 53 (35%) cases of hepatitis A and 15 (34%) cases of IMD. On the basis of patient residence, we identified 12 postal (ZIP) codes with >1 case of both hepatitis A and IMD, 3 of which had >2 cases of each disease (Figure 2). For hepatitis A, several cases occurred in west-central Florida (Hillsborough and Pinellas Counties), where IMD was not observed. Several IMD cases occurred in southeastern Florida (Miami-Dade, Broward, and Palm Beach Counties), where outbreak-associated hepatitis A was not frequently observed.

Mpox cases in Florida were more widely dispersed; cases were reported in 45 of 67 counties. The highest concentration was observed in the southeast region, and 56% of all cases were reported in Broward and Miami-Dade Counties (Figure 3). Orange County reported the third highest (295; 10%) number of mpox cases. The 7 most populated counties in Florida accounted for 87% of mpox cases reported in the state. Exposure occurred exclusively outside the United States for 5% of Florida mpox cases, and an additional 2% of cases reported multiple exposure locations that included >1 location outside the United States.

Comparing cases by disease, the median age of IMD case-patients was 32 years, which was significantly younger than for hepatitis A (35 years; p = 0.0145) and mpox (36 years; p = 0.0043) case-patients. We detected statistically significant differences when comparing cases of each disease by HIV infection, history of recent STI, and Orange County residence (p<0.0001). HIV infection was more prevalent among mpox (52%) cases than among IMD (34%) or hepatitis A (21%) cases. In addition, STI in the previous 2 years was more prevalent among mpox (55%) cases than among hepatitis A (27%) or IMD (20%) cases. A lower percentage (10%) of mpox cases were among Orange County residents than were IMD (34%) and hepatitis A (35%) cases.

Control Measures

JYNNEOS (Bavarian Nordic) vaccine for preventing mpox became available in limited supplies in Florida in late May and June 2022. As the vaccine supply increased, persons vaccinated with their first dose increased markedly; in July and August, >53,000 adults in Florida received >1 dose (Appendix Table 2). Immunization against hepatitis A and IMD also increased markedly among adults during that timeframe (Figure 4). In August 2022, of the 28,592 persons receiving a first dose of JYNNEOS vaccine, 7,305 (26%) received >1 other vaccine against either hepatitis A or IMD on the same day; 2,979 (10%) received vaccines against all 3 diseases on the same day. More than half of adult immunizations for hepatitis A and IMD in August were administered by CHD providers. In contrast, during months outside the August–October period, <38% of adults receiving a vaccine for either disease received that dose from a CHD provider.

The hepatitis A and IMD outbreaks concluded by the end of 2022, but mpox cases continued to be reported in Florida as of January 2024. By that time, a total of 2,957 mpox cases had been reported since the start of the outbreak, which is considered ongoing.