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. 2020 Sep;108(3):967-981.
doi: 10.1002/JLB.4MA0420-497R. Epub 2020 Jun 12.

Targeting NLRP3 and Staphylococcal pore-forming toxin receptors in human-induced pluripotent stem cell-derived macrophages

Seong H Chow  1 Pankaj Deo  1 Amy T Y Yeung  2 Xenia P Kostoulias  3 Yusun Jeon  1 Mei-Ling Gao  4   5 Azadeh Seidi  1 Françios Alwyn Benson Olivier  1 Sushmita Sridhar  2 Cara Nethercott  3 David Cameron  3 Avril A B Robertson  6 Remy Robert  1 Charles R Mackay  3 Ana Traven  1 Zi-Bing Jin  4   5 Christine Hale  2 Gordon Dougan  2   7 Anton Y Peleg  3   8 Thomas Naderer  1
Affiliations

Targeting NLRP3 and Staphylococcal pore-forming toxin receptors in human-induced pluripotent stem cell-derived macrophages

Seong H Chow et al. J Leukoc Biol. 2020 Sep.

Abstract

Staphylococcus aureus causes necrotizing pneumonia by secreting toxins such as leukocidins that target front-line immune cells. The mechanism by which leukocidins kill innate immune cells and trigger inflammation during S. aureus lung infection, however, remains unresolved. Here, we explored human-induced pluripotent stem cell-derived macrophages (hiPSC-dMs) to study the interaction of the leukocidins Panton-Valentine leukocidin (PVL) and LukAB with lung macrophages, which are the initial leukocidin targets during S. aureus lung invasion. hiPSC-dMs were susceptible to the leukocidins PVL and LukAB and both leukocidins triggered NLPR3 inflammasome activation resulting in IL-1β secretion. hiPSC-dM cell death after LukAB exposure, however, was only temporarily dependent of NLRP3, although NLRP3 triggered marked cell death after PVL treatment. CRISPR/Cas9-mediated deletion of the PVL receptor, C5aR1, protected hiPSC-dMs from PVL cytotoxicity, despite the expression of other leukocidin receptors, such as CD45. PVL-deficient S. aureus had reduced ability to induce lung IL-1β levels in human C5aR1 knock-in mice. Unexpectedly, inhibiting NLRP3 activity resulted in increased wild-type S. aureus lung burdens. Our findings suggest that NLRP3 induces macrophage death and IL-1β secretion after PVL exposure and controls S. aureus lung burdens.

Keywords: NLRP3; inflammation; macrophage; pneumonia; staphylococcus; toxin.

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References

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