Binding of the extracellular matrix laminin-1 to <i>Clostridioides difficile</i> strains

Santos, Mayara Gil de Castro; Trindade, Camilla Nunes dos Reis; Vommaro, Rossiane Cláudia; Domingues, Regina Maria Calvalcanti Pilotto; Ferreira, Eliane de Oliveira

doi:10.1590/0074-02760220035

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RESEARCH ARTICLE • Mem. Inst. Oswaldo Cruz 117 • 2022 • https://doi.org/10.1590/0074-02760220035 copy

Binding of the extracellular matrix laminin-1 to Clostridioides difficile strains

Authorship SCIMAGO INSTITUTIONS RANKINGS

BACKGROUND

Clostridioides difficile is the most common cause of nosocomial diarrhea associated with antibiotic use. The disease’s symptoms are caused by enterotoxins, but other surface adhesion factors also play a role in the pathogenesis. These adhesins will bind to components of extracellular matrix.

OBJECTIVE

There is a lack of knowledge on MSCRAMM, this work set-out to determine the adhesive properties of several C. difficile ribotypes (027, 133, 135, 014, 012) towards laminin-1 (LMN-1).

METHODS

A binding experiment revealed that different ribotypes have distinct adhesion capabilities. To identify this adhesin, an affinity chromatography column containing LMN-1 was prepared and total protein extracts were analysed using mass spectrometry.

FINDINGS

Strains from ribotypes 012 and 027 had the best adhesion when incubated with glucose supplementations (0.2%, 0.5%, and 1%), while RT135 had a poor adherence. The criteria were not met by RT014 and RT133. In the absence of glucose, there was no adhesion for any ribotype, implying that glucose is required and plays a significant role in adhesion.

MAIN CONCLUSIONS

These findings show that in the presence of glucose, each C. difficile ribotype interacts differently with LMN-1, and the adhesin responsible for recognition could be SlpA protein.

Key words:
Clostridioides difficile; adhesion; laminin-1; virulence

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[1] + Corresponding author: eliane_ferreirarj@micro.ufrj.br

Strains	Ribotypes	Toxigenic profile^b	Clinical conditions	References
SJ1	135^a	tcdA⁺/tcdB⁺/CDT^-	SH, DM, hemorrhagic EVA	²³23. Balassiano IT, Santos-Filho J, Oliveira MPB, Ramos MC, Japiassu AM, Reis AM, et al. An outbreak case of Clostridium difficile-associated diarrhea among elderly inpatients of an intensive care unit of a tertiary hospital in Rio de Janeiro. Diagn Microbiol Infect Dis. 2010; 68(4): 449-55.
HU09	133^a	tcdA⁺/tcdB⁺/CDT^-	Crohn’s disease	²⁴24. Balassiano, Santos-Filho J, Vital-Brazil JM, Nouér SA, Souza CRC, Brazier JS, et al. Detection of cross-infection associated to a Brazilian PCR-ribotype of Clostridium difficile in a university hospital in Rio de Janeiro, Brazil. Antonie van Leeuwenhoek. 2011; 99(2): 249-55.
1598	014	tcdA⁺/tcdB⁺/CDT^-	HIV⁺	²⁵25. Balassiano IT, Miranda KR, Boente RF, Pauer H, Oliveira ICM, Santos-Filho J, et al. Characterization of Clostridium difficile strains isolated from immunosuppressed inpatients in a hospital in Rio de Janeiro, Brazil. Anaerobe. 2009; 15(3): 61-4.
BI/NAP1^c	027	tcdA⁺/tcdB⁺ /CDT⁺	-	²⁶26. Warny M, Pepin J, Fang A, Killgore G, Thompson A, Brazier J, et al. Toxin production by an emerging strain of Clostridium difficile associated with outbreaks of severe disease in North America and Europe. Lancet. 2005; 366(9491): 1079-84.
630	012	tcdA⁺/tcdB⁺/CDT^-	Pseudomembranous colitis	²⁷27. Sebaihia M, Wren BW, Mullany P, Fairweather NF, Minton N, Stabler R, et al. The multidrug-resistant human pathogen Clostridium difficile has a highly mobile, mosaic genome. Nat Genet. 2006; 38(7): 779-86.