Alpha-toxin Induces Programmed Cell Death of Human T cells, B cells, and Monocytes During USA300 Infection

dc.contributor.authorNygaard, Tyler K.
dc.contributor.authorPallister, Kyler B.
dc.contributor.authorDuMont, Ashley L.
dc.contributor.authorDeWald, Mark
dc.contributor.authorWatkins, Robert L.
dc.contributor.authorPallister, Erik Q.
dc.contributor.authorMalone, Cheryl L.
dc.contributor.authorGriffith, Shannon
dc.contributor.authorHorswill, Alexander R.
dc.contributor.authorTorres, Victor J.
dc.contributor.authorVoyich, Jovanka M.
dc.date.accessioned2019-04-22T19:34:15Z
dc.date.available2019-04-22T19:34:15Z
dc.date.issued2012-05
dc.description.abstractThis investigation examines the influence of alpha-toxin (Hla) during USA300 infection of human leukocytes. Survival of an USA300 isogenic deletion mutant of hla (USA300Δhla) in human blood was comparable to the parental wild-type strain and polymorphonuclear leukocyte (PMN) plasma membrane permeability caused by USA300 did not require Hla. Flow cytometry analysis of peripheral blood mononuclear cells (PBMCs) following infection by USA300, USA300Δhla, and USA300Δhla transformed with a plasmid over-expressing Hla (USA300Δhla Comp) demonstrated this toxin plays a significant role inducing plasma membrane permeability of CD14+, CD3+, and CD19+ PBMCs. Rapid plasma membrane permeability independent of Hla was observed for PMNs, CD14+ and CD19+ PBMCs following intoxication with USA300 supernatant while the majority of CD3+ PBMC plasma membrane permeability induced by USA300 required Hla. Addition of recombinant Hla to USA300Δhla supernatant rescued CD3+ and CD19+ PBMC plasma membrane permeability generated by USA300 supernatant. An observed delay in plasma membrane permeability caused by Hla in conjunction with Annexin V binding and ApoBrdU Tunel assays examining PBMCs intoxicated with recombinant Hla or infected with USA300, USA300Δhla, USA300Δhla Comp, and USA300ΔsaeR/S suggest Hla induces programmed cell death of monocytes, B cells, and T cells that results in plasma membrane permeability. Together these findings underscore the importance of Hla during S. aureus infection of human tissue and specifically demonstrate Hla activity during USA300 infection triggers programmed cell death of human monocytes, T cells and B cells that leads to plasma membrane permeability.en_US
dc.description.sponsorshipNational Institute of Health grants NIH-PAR98-072, NIH-RR020185; NIH-R01 award A1090046-01; Molecular Biosciences Fellowship; Montana State University Agricultural Experiment Station; New York University School of Medicine Development Funds; American Heart Association Scientist Development Grant 09SDG2060036; NIH Training Grant 5T32 AI007180-27en_US
dc.identifier.citationNygaard, Tyler K., Kyler B. Pallister, Ashley L. DuMont, Mark DeWald, Robert L. Watkins, Erik Q. Pallister, Cheryl Malone, Shannon Griffith, Alexander R. Horswill, Victor J. Torres, Jovanka M. Voyich. “Alpha-Toxin Induces Programmed Cell Death of Human T Cells, B Cells, and Monocytes During USA300 Infection.” PLoS ONE 7, no. 5 (May 4, 2012): e36532. doi:10.1371/journal.pone.0036532.en_US
dc.identifier.issn1932-6203
dc.identifier.urihttps://scholarworks.montana.edu/handle/1/15456
dc.language.isoenen_US
dc.rightsCC BY: This license lets you distribute, remix, tweak, and build upon this work, even commercially, as long as you credit the original creator for this work. This is the most accommodating of licenses offered. Recommended for maximum dissemination and use of licensed materials.en_US
dc.rights.urihttps://creativecommons.org/licenses/by/4.0/legalcodeen_US
dc.titleAlpha-toxin Induces Programmed Cell Death of Human T cells, B cells, and Monocytes During USA300 Infectionen_US
dc.typeArticleen_US
mus.citation.issue5en_US
mus.citation.journaltitlePLoS Oneen_US
mus.citation.volume7en_US
mus.data.thumbpage6en_US
mus.identifier.categoryHealth & Medical Sciencesen_US
mus.identifier.categoryLife Sciences & Earth Sciencesen_US
mus.identifier.doi10.1371/journal.pone.0036532en_US
mus.relation.collegeCollege of Letters & Scienceen_US
mus.relation.departmentMicrobiology & Immunology.en_US
mus.relation.researchgroupMT INBRE Bioinformatics and Biostatistics Core.en_US
mus.relation.universityMontana State University - Bozemanen_US

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