Cutaneous tuberculosis-ambiguous transmission, bacterial diversity with biofilm formation in humoral abnormality: case report illustration

Przemysław Zdziarski; Mariola Paściak; Anna Chudzik; Monika Kozińska; Ewa Augustynowicz-Kopeć; Andrzej Gamian

doi:10.3389/fpubh.2023.1091373

Cutaneous tuberculosis-ambiguous transmission, bacterial diversity with biofilm formation in humoral abnormality: case report illustration

Front Public Health. 2023 Apr 21:11:1091373. doi: 10.3389/fpubh.2023.1091373. eCollection 2023.

Authors

Przemysław Zdziarski¹, Mariola Paściak², Anna Chudzik², Monika Kozińska³, Ewa Augustynowicz-Kopeć³, Andrzej Gamian²

Affiliations

¹ Department of Clinical Immunology, Tuberculosis and Pulmonary Disease, Lower Silesian Oncology Center, Wroclaw, Poland.
² Department of Immunology of Infectious Diseases, Hirszfeld Institute of Immunology and Experimental Therapy, Polish Academy of Sciences, Wroclaw, Poland.
³ Department of Microbiology, National Tuberculosis and Lung Diseases Research Institute, Warsaw, Poland.

Abstract

Background: Cutaneous tuberculosis (CTB) and its paucibacillary forms are rare and difficult to diagnose, especially in immunocompromised patients with significant comorbidity. The aim of the study was to introduce the modern concept of the microbiome and diagnostic chain into clinical practice (patient-centered care) with the presentation of an atypical form of cutaneous tuberculosis with necrotizing non-healing ulcers leading to polymicrobial infection.

Methods: The study material included samples from sputum, broncho-alveolar lavage and skin ulcer, taken from a patient developing cutaneous tuberculosis. The microbiological investigation was performed, and identification of the isolates was carried out using genotyping and the matrix-assisted laser desorption ionization-time of flight mass spectrometry.

Results: The immunocompromised patient with humoral abnormality (plasma cell dyscrasia) and severe paraproteinemia developed multiorgan tuberculosis. Although cutaneous manifestation preceded systemic and pulmonary symptoms (approximately half a year), the mycobacterial genotyping confirmed the same MTB strain existence in skin ulcers and the respiratory system. Therefore, the infectious chain: transmission, the portal of entry, and bacterial spreading in vivo, were unclear. Microbial diversity found in wound microbiota (among others Gordonia bronchialis, Corynebacterium tuberculostearicum, Staphylococcus haemolyticus, and Pseudomonas oryzihabitans) was associated with the spread of a skin lesion. The in vitro biofilm-forming capacity of strains isolated from the wound may represent the potential virulence of these strains. Thus, the role of polymicrobial biofilm may be crucial in ulcer formation and CTB manifestation.

Conclusions: Severe wound healing as a unique biofilm-forming niche should be tested for Mycobacterium (on species and strain levels) and coexisting microorganisms using a wide range of microbiological techniques. In immunodeficient patients with non-typical CTB presentation, the chain of transmission and MTB spread is still an open issue for further research.

Keywords: Actinobacteria; biofilm; cutaneous tuberculosis; diagnostic chain; microbiome; paraproteinemia; portal of entry/exit; translational medicine.

Publication types

Case Reports
Research Support, Non-U.S. Gov't

MeSH terms

Biofilms
Humans
Tuberculosis*

Grants and funding

This study was supported by private funds of PZ, from the statutory activity of the Hirszfeld Institute and the National Tuberculosis and Lung Diseases Research Institute. The study is part of the PZ's project: Analysis of the structural properties of a microbial biofilm matrix.