Volume 30, Number 1—January 2024
Research Letter
Mycobacterium senegalense Infection in Kidney Transplant Patient with Diabetes, Memphis, Tennessee, USA
, Reeti Khare, and Shirin Mazumder
Abstract
Fewer than 30 cases of Mycobacterium senegalense infection have been reported. We report a complicated case of M. senegalense infection in Memphis, Tennessee, in the southeastern United States. The patient's comorbidities of past organ transplant and insulin-dependent diabetes required delicate consideration of those health conditions to guide treatment.
Mycobacterium senegalense, also referred to as M. conceptionense, is a nonpigmented rapid-growing mycobacterium belonging to the M. fortuitum group, which was first isolated in 2006 from a posttraumatic osteitis inflammation in France (1,2). Only a handful of M. conceptionense cases are readily identifiable in existing literature. Infections can manifest with pulmonary involvement but more commonly manifest as skin or subcutaneous infection, such as after face rejuvenation surgery, breast augmentation surgery, gastric carcinoma resection, or subcutaneous ankle infection (3–6). Mycobacterial species like M. senegalense have been found in irrigation systems, soil, domestic and wild animals, and dairy products (7,8). Cases of M. senegalense infection have been observed in France, Iran, Taiwan, South Korea, Japan, and the United States, demonstrating an unidentifiable pattern of regional bacterial prevalence.
Establishing an accurate diagnosis of M. senegalense infection is incredibly difficult, requiring histological examination and extensive mycobacterial cultures (9). The limited susceptibility data also mean an optimal therapy has not been completely established, which leaves certain patient populations, particularly the elderly and immunocompromised, susceptible to increased illness and death from M. senegalense infection (10). We report a complicated case of M. senegalense infection in a patient with a previous kidney transplant and insulin-dependent diabetes mellitus in Memphis, Tennessee, USA.
A 70-year-old Black woman with end-stage kidney disease sought care for a painful, swollen, abdominal wall abscess. She had first noticed the lesion ≈3 weeks before in the left mid-abdomen, where she frequently injected insulin. The patient denied any recent travel, drainage at the site, or fever. The 7- × 4-cm abscess was drained the next day without complications, and we sent the custard-like purulent material for laboratory testing.
The patient had undergone a right-sided cadaveric renal transplant 8 years before; her immunosuppressive regimen consisted of tacrolimus, mycophenolate, and prednisone. The patient’s past diagnoses at the time of infection included type 2 diabetes mellitus, lupus, hypertension, hyperlipidemia, sleep apnea, and coronary artery disease. Insulin injections create small open wounds where pathogens can enter and cause infection. An environmental source of the infection was not sought. The hospital microbiology laboratory detected acid-fast bacilli on direct AFB smear. The patient immediately began empiric antimicrobial drugs, including doxycycline (100 mg 2×/d) and levofloxacin (250 mg 1×/d), adjusted for her creatinine clearance.
The isolate was sent to the National Jewish Mycobacteriology Reference Laboratory (Denver, Colorado, USA) for confirmation and susceptibility testing. Sanger sequencing analysis was performed; BLAST (https://blast.ncbi.nlm.nih.gov/Blast.cgi) testing of the rpoB sequence results against the public GenBank database identified M. senegalense (>99% homology to existing sequences). A line probe assay for common nontuberculous mycobacteria, GenoType NTM-DR (Hain Lifescience, https://www.hain-lifescience.de), was performed first to differentiate qualitatively and in vitro species of several strains of mycobacteria, such as M. avium complex, M. abscessus, M. chelonae, M. intracellulare, M. chimaera, M. massiliense, M. bolletii, and M. chelonae, but did not yield a species-level identification. Those tests supported identification as M. senegalense, and the sequence was deposited in GenBank (accession no. OR644277). In vitro susceptibility testing demonstrated the antibiotics to which the isolate was susceptible, intermediate, and resistant, according to Clinical and Laboratory Standards Institute guidelines (https://clsi.org) (Table).
The patient continued taking doxycycline. Levofloxacin was stopped after the patient reported nausea and vomiting. Because of increasing creatinine levels, trimethoprim/sulfamethoxazole was not used. The isolate was susceptible to clarithromycin, but it was not selected because of ongoing tacrolimus treatment. Amoxicillin/clavulanate was chosen, despite the isolate’s intermediate susceptibility, because of better patient tolerance. The final drug regimen was doxycycline (100 mg 2×/d) and amoxicillin/clavulanate (250/125 mg 2×/d) adjusted for renal function; expected treatment course was 4–6 months. At the 3-month clinic follow-up, the lesion had notably shrunk to a 3- × 0.8-cm open wound with no drainage, foul odor, or tenderness. By 6-month follow-up, the lesion had closed and was hyperpigmented and flat, without fluctuance or signs of active infection.
We achieved identification of M. senegalense through rpoB gene sequencing, and treatment was guided by antibiotic susceptibility options. Separating M. senegalense from the rest of the M. fortuitum complex species helps guide appropriate treatment and epidemiologic analysis of mycobacterial species by geographic location. This patient presented a unique and delicate case in which adequate treatment required thorough consideration of other medications, diagnoses, and comorbidities. Overall, this complicated, interesting case of M. senegalense infection at the site of insulin injections for a diabetic patient in the southeastern United States adds to the limited body of M. senegalense infection and treatment knowledge. This case highlights that M. senegalense is present in this region, suggesting a higher index of suspicion is needed for patients in those areas.
Ms. Singh is a third-year medical student at the University of Tennessee whose research interests include topics in dermatology or specialties of internal medicine, particularly infectious disease, rheumatology, and oncology. Dr. Mazumder is an associate professor of medicine in the Division of Infectious Diseases, Department of Internal Medicine, at the University of Tennessee Health Science Center, and the laboratory director at the Methodist LeBonheur Healthcare Ambulatory Clinics. Her research interests include infectious diseases, particularly HIV, transplant infections, and fungal infections.
Acknowledgment
R.K. has laboratory-contracted research with Insmed, Paratek Pharmaceuticals, AN2 Therapeutics, Spero Therapeutics, and Mannkind Corporation.
References
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Cite This ArticleOriginal Publication Date: December 16, 2023
Table of Contents – Volume 30, Number 1—January 2024
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Please use the form below to submit correspondence to the authors or contact them at the following address:
Nupur Singh, University of Tennessee Health Science Center, 910 Madison Ave, Memphis, TN, 38103, USA
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