Volume 27, Number 12—December 2021
Research Letter
Wohlfahrtiimonas chitiniclastica Monomicrobial Bacteremia in a Homeless Man
, Paul M. Luethy, Mandee Noval, and Jonathan D. Baghdadi
Abstract
We report a case of septic shock attributable to monomicrobial bloodstream infection secondary to Wohlfahrtiimonas chitiniclastica infection. This case suggests that W. chitiniclastica likely possesses the virulence to cause severe disease. Culture-independent techniques were essential in the identification of this organism, which enabled selection of appropriate therapy.
In August 2020, a 63-year-old homeless man with a history of deep vein thrombosis and chronic venous insufficiency was found in his truck, unconscious and covered in feces and maggots. He reportedly had been parked in a single parking spot in rural Maryland, USA, for 3 days. His blood pressure in the field was too low to be quantified, and he was admitted to a community hospital in septic shock. Blood cultures were drawn before establishing intravenous access for administration of vancomycin, piperacillin/tazobactam, and crystalloid. After being stabilized, he was transferred to our hospital, a tertiary care center in Baltimore, Maryland, USA, where surgeons performed superficial surgical debridement of his lower extremities and removed maggots by using a scrub brush with the patient under anesthesia in the operating room. We discarded the maggots, and they were not submitted for identification.
The patient’s leukocyte count on arrival was 38.6 K/μL (reference range 4.5–11.0 K/μL), his creatinine 6.86 mg/dL (reference range 0.7–1.5 mg/dL), and his lactic acid 3.5 mmol/L (reference range 0.5–2.2 mmol/L). He had elevated transaminases, an aspartate aminotransferase level of 436 U/L (reference range 17–59 U/L) and alanine transaminase of 174 U/L (reference range 0–49 U/L). A computed tomography scan of the lower extremities showed ulceration of the anterior right lower leg with edema and fat stranding of the subcutaneous tissue without fluid collection or gas. A magnetic resonance imaging of his left foot showed no evidence of osteomyelitis.
On day 2 of hospitalization, transient hemodynamic instability necessitated initiation of vasopressor support and continuous renal replacement therapy; however, these treatments were rapidly tapered off. We identified gram-negative rods in the anaerobic blood culture from the community hospital, and we narrowed the patient’s antibiotics to piperacillin/tazobactam monotherapy. On hospital day 5, we identified the gram-negative rods as W. chitiniclastica by using matrix-assisted laser desorption/ionization time-of-flight (MALDI-TOF) mass spectrometry. We changed the patient’s intravenous antibiotics to 2 g of ceftriaxone daily and then, on hospital day 9, changed the regimen to 750 mg of oral levofloxacin daily to complete a 21-day course of treatment. We were unable to follow up with the patient after his discharge, but we proceeded with reporting about his case after it was deemed to be exempt by the Institutional Review Board at the University of Maryland Baltimore.
In 2008, W. chitiniclastica was first isolated from larvae of the parasitic fly Wohlfahrtia magnifica (1). Since 2008, a total of 11 cases of W. chitiniclastica bloodstream infections have been described (2–10; Appendix references 11,12) (Table). Our patient shares risk factors observed in other cases, including homelessness and chronic venous insufficiency (Appendix reference 13). The pathogenicity of W. chitiniclastica has remained uncertain in previous case reports secondary to its identification in polymicrobial infections. This severe case of monomicrobial W. chitiniclastica BSI is similar to a previous report of a 70-year-old man in Argentina who had septic shock with multiorgan failure secondary to the same bacteria (3). Taken together, these 2 cases challenge the hypothesis that other bacteria present in polymicrobial infections are primarily responsible for the disease associated with BSI attributable to W. chitiniclastica infection (9) and instead suggest that this pathogen may cause severe disease.
For our patient, W. chitiniclastica was first identified on MALDI-TOF mass spectrometry from a positive anaerobic blood culture. In all 9 cases for which detailed microbiologic methods are reported, W. chitiniclastica was identified from blood or tissue cultures by using MALDI-TOF mass spectrometry (5,8; Appendix reference 12), 16S rRNA sequencing (2,3,9), or both (4,7,10) (Table). This pattern demonstrates that W. chitiniclastica is extremely difficult to identify from clinical specimens without culture-independent techniques and highlights the utility of these techniques in clinical care.
Published case-reports demonstrate a heterogeneous approach to the clinical management of patients with W. chitiniclastica BSI. Often, selection of antibiotics was dictated by the other pathogens present in a polymicrobial infection. Generally, most studies report the use of β-lactams (2,3,5–10; Appendix reference 12) as initial therapy, with fluoroquinolones available as second-line or step-down therapy (3,7,8). The duration of treatment ranges from 7 days to 6 weeks (5–8; Appendix reference 12). Given that our patient rapidly improved and the presumed source of his infection had been controlled with debridement of his lower extremities, we opted for a 3-week course of treatment.
Dr. Harfouch is an infectious diseases fellow at the University of Maryland Medical Center. His primary research interests include the epidemiology and prevention of HIV among lesbian, gay, bisexual, and transgender persons.
Acknowledgment
We thank the healthcare team that participated in this patient’s care at the University of Maryland Medical Center and the University of Maryland Midtown Campus.
References
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Table
Cite This ArticleOriginal Publication Date: November 04, 2021
Table of Contents – Volume 27, Number 12—December 2021
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Please use the form below to submit correspondence to the authors or contact them at the following address:
Omar Harfouch, University of Maryland Medical Center, 725 W Lombard St, Baltimore MD 21211, USA
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