Discover @ Loyola University Chicago Health Sciences Division - Identification of a crucial residue required for Staphylococcus aureus LukAB cytotoxicity and receptor recognition.

Identification of a crucial residue required for Staphylococcus aureus LukAB cytotoxicity and receptor recognition. Journal Article

Local Library Link: Find It @ Loyola

Authors:	DuMont, AL; Yoong, P; Liu, X; Day, CJ; Chumbler, NM; James, DB; Alonzo, F; Bode, NJ; Lacy, DB; Jennings, MP; Torres, VJ
Article Title:	Identification of a crucial residue required for Staphylococcus aureus LukAB cytotoxicity and receptor recognition.
Abstract:	The bicomponent leukotoxins produced by Staphylococcus aureus kill host immune cells through osmotic lysis by forming ß-barrel pores in the host plasma membrane. The current model for bicomponent pore formation proposes that octameric pores, comprised of two separate secreted polypeptides (S and F subunits), are assembled from water-soluble monomers in the extracellular milieu and multimerize on target cell membranes. However, it has yet to be determined if all staphylococcal bicomponent leukotoxin family members exhibit these properties. In this study, we report that leukocidin A/B (LukAB), the most divergent member of the leukotoxin family, exists as a heterodimer in solution rather than two separate monomeric subunits. Notably, this property was found to be associated with enhanced toxin activity. LukAB also differs from the other bicomponent leukotoxins in that the S subunit (LukA) contains 33- and 10-amino-acid extensions at the N and C termini, respectively. Truncation mutagenesis revealed that deletion of the N terminus resulted in a modest increase in LukAB cytotoxicity, whereas the deletion of the C terminus rendered the toxin inactive. Within the C terminus of LukA, we identified a glutamic acid at position 323 that is critical for LukAB cytotoxicity. Furthermore, we discovered that this residue is conserved and required for the interaction between LukAB and its cellular target CD11b. Altogether, these findings provide an in-depth analysis of how LukAB targets neutrophils and identify novel targets suitable for the rational design of anti-LukAB inhibitors.
Journal Title:	Infection and immunity
ISSN:	1098-5522; 0019-9567
Publisher:	American Society for Microbiology. All Rights Reserved
Date Published:	2014

LUC Authors

28 Alonzo

Related LUC Article

Binary Toxin Cdt: Mechanism, Epidemiology, And Potential Clinical Importance

Gut microbes 2013
Clostridium Difficile Binary Toxin Cdt: Mechanism, Epidemiology, And Potential Clinical Importance

Gut microbes 2014
Staphylococcus Aureus Leukocidin Luk Ed And Hiv 1 Gp120 Target Different Sequence Determinants On Ccr5.

mBio 2016
The Relationship Between Glycan Binding And Direct Membrane Interactions In Vibrio Cholerae Cytolysin, A Channel Forming Toxin.

The Journal of biological chemistry 2015
The Bicomponent Pore Forming Leucocidins Of Staphylococcus Aureus.

Microbiology and molecular biology reviews : MMBR 2014