COVID-19–Associated Fusobacterium nucleatum Bacteremia, Belgium

We report 4 cases of Fusobacterium nucleatum bacteremia associated with coronavirus disease (COVID-19). Three cases occurred concomitantly with COVID-19 diagnosis; 1 occurred on day 15 of intensive care. None of the patients had known risk factors for F. nucleatum bacteremia. F. nucleatum infection could represent a possible complication of COVID-19.

In March and April 2020, 2 major hospitals in Brussels, Belgium, observed 4 cases of monomicrobial F. nucleatum bacteremia, all associated with severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) infection among patients with coronavirus disease . In contrast, the same hospitals reported a total of 4 F. nucleatum cases in 2019, 3 in 2018, 2 in 2017, 1 in 2016, and 2 in 2015. However, the hospital emergency plan initiated on March 14 during the first wave of the COVID-19 pandemic in Belgium prohibited all nonurgent medical care. Thus, the 2020 F. nucleatum incidence cannot be extrapolated and compared with previous years because of modifications of patient characteristics.
F. nucleatum was cultured from patients' blood specimens by using a BD BACTEC FX blood culture system (Becton Dickinson, https://www.bd.com) and pure isolates were successfully identified by using matrix-assisted laser desorption/ionization time-offlight mass spectrometry (Bruker Daltonics, https:// www.bruker.com). Cross-contamination was formally excluded because blood cultures became positive on different days and bacterial identifications were performed on separate sets of experiments (Table 1).
Nasopharyngeal swab samples were collected from the 4 patients. Three patients tested positive for SARS-CoV-2 by reverse transcription PCR (RT-PCR) using the RealStar SARS-CoV-2 RT-PCR kit (Altona Diagnostics, https://www.altona-diagnostics.com) and 1 by a COVID-19 Ag Respi-Strip rapid antigen test (Coris Bioconcept, https:// www.corisbio.com). All 4 patients had concomitant pneumonia compatible with COVID-19 on chest computed tomography (CT) scans. The patients were 34, 51, 52, and 70 years of age (median 51.5 years); the median age was lower than in previously reported F. nucleatum bacteremia (1,2), but the sample size is too small for statistical analysis. None of the patients had any classical risk factors for F. nucleatum bacteriemia. The youngest patient had no underlying conditions. Three patients had abdominal symptoms and 2 underwent abdominal CT with contrast, but both had unremarkable results. Three patients had symptoms of bacteremia at the time of COVID-19 diagnosis; bacteremia was diagnosed in the other patient after 15 days in the hospital intensive care unit (ICU). The ICU patient received a single 800-mg intravenous dose of tocilizumab (TCZ) to treat COVID-19-associated hyperinflammatory syndrome. Increased risk for severe infection, including bacteremia, has been associated with long-term TCZ treatment when administered for non-COVID-19 indications (3). To our knowledge, no previous F. nucleatum infection has been reported with TCZ use in general. The patient died of COVID-19-related severe respiratory failure on day 21 in the ICU, but the other 3 patients were discharged to home without complications.
Although SARS-CoV-2 infection initially was described as an agent of severe pneumonia, other organ involvements are now well described. Other studies among hospitalized COVID-19 patients have shown that 18%-48% had digestive complaints ranging from anorexia to diarrhea and abdominal pain (4,5). RT-PCR detected the virus in the feces of 48%-53% of patients with abdominal complaints and feces remained positive in 20%-33% of patients even after respiratory samples converted from RT-PCR-positive to negative (4,6). The propensity of SARS-CoV-2 to infect digestive organs might be explained by the fact that angiotensin converting enzyme 2, a known receptor used by the virus to enter human cells, has been found to be highly expressed in enterocytes (4,7).
The reservoir of F. nucleatum is generally considered to be the oral cavity (8). Only 1 of these patients had oral symptoms, but no oral lesions were observed. The 3 other patients had abdominal symptoms, suggesting that bacteremia might be the consequence of translocation from the digestive tract (9). F. nucleatum has been shown to colonize colon mucus with associated mucosal inflammation (10).
In conclusion, digestive tract invasion by SARS-CoV-2 and secondary inflammatory response might promote translocation of opportunistic pathogens, such as F. nucleatum, and further research could elucidate this interaction. Nonetheless, our observations suggest that anaerobe bacteremia should be considered as a complication of COVID-19. T uberculosis (TB) is an ancient disease affecting a plethora of domestic and wild animals, including humans. In primates, TB can cause severe multisystemic disease. The prevalence of TB in lemurs within Madagascar is unknown; the most recent documented case occurred in 1973 (1). Reverse zoonotic transmission of TB can occur when nonhuman primates are in close contact with humans (1). We report a clinical case and genomic analysis of TB infection in a female subadult ring-tailed lemur (Lemur catta) held at a nongovernmental organization facilty in Southwestern Madagascar. The University of San Diego (San Diego, CA, USA) provided ethics authorization (no. IACUC 0619-01).
The lemur was born in the wild in September or October 2018 and was surrendered to the facility in April 2019. On July 12, the animal was emaciated, anorexic, and lethargic; it had a large fistulated mass on the left cervical region. The mass was surgically removed and found to be caseous and necrotic (Figure). Despite rehydration and systemic antimicrobial therapy, the lemur died on July 16.

RESEARCH LETTERS
We diagnosed tuberculosis in an illegally wild-captured pet ring-tailed lemur manifesting lethargy, anorexia, and cervical lymphadenopathy. Whole-genome sequencing confirmed the Mycobacterium tuberculosis isolate belonged to lineage 3 and harbored streptomycin resistance. We recommend reverse zoonosis prevention and determination of whether lemurs are able to maintain M. tuberculosis infection.