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Extracellular traps released by antimicrobial TH17 cells contribute to host defense
George W. Agak, Alice Mouton, Rosane M.B. Teles, Thomas Weston, Marco Morselli, Priscila R. Andrade, Matteo Pellegrini, Robert L. Modlin
George W. Agak, Alice Mouton, Rosane M.B. Teles, Thomas Weston, Marco Morselli, Priscila R. Andrade, Matteo Pellegrini, Robert L. Modlin
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Research Article Immunology

Extracellular traps released by antimicrobial TH17 cells contribute to host defense

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Abstract

TH17 cell subpopulations have been defined that contribute to inflammation and homeostasis, yet the characteristics of TH17 cells that contribute to host defense against infection are not clear. To elucidate the antimicrobial machinery of the TH17 subset, we studied the response to Cutibacterium acnes, a skin commensal that is resistant to IL-26, the only known TH17-secreted protein with direct antimicrobial activity. We generated C. acnes–specific antimicrobial TH17 clones (AMTH17) with varying antimicrobial activity against C. acnes, which we correlated by RNA sequencing to the expression of transcripts encoding proteins that contribute to antimicrobial activity. Additionally, we validated that AMTH17-mediated killing of C. acnes and bacterial pathogens was dependent on the secretion of granulysin, granzyme B, perforin, and histone H2B. We found that AMTH17 cells can release fibrous structures composed of DNA decorated with histone H2B that entangle C. acnes that we call T cell extracellular traps (TETs). Within acne lesions, H2B and IL-17 colocalized in CD4+ T cells, in proximity to TETs in the extracellular space composed of DNA decorated with H2B. This study identifies a functionally distinct subpopulation of TH17 cells with an ability to form TETs containing secreted antimicrobial proteins that capture and kill bacteria.

Authors

George W. Agak, Alice Mouton, Rosane M.B. Teles, Thomas Weston, Marco Morselli, Priscila R. Andrade, Matteo Pellegrini, Robert L. Modlin

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Figure 8

Expression of T cell extracellular traps in acne lesions.

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Expression of T cell extracellular traps in acne lesions.
(A) Confocal i...
(A) Confocal images of IL-17 (red), histone H2B (green), and nuclei (DAPI, blue) in acne lesions. Dashed-line boxes identify the area further studied at higher power. Original magnification, ×63 with ×2 zoom from lower magnification in Supplemental Figure 9. (B) Higher-power magnification (×4 zoom of images in A) of the delineated regions marked in A showing H2B (green) and DAPI (red) only. White arrows indicate TETs in proximity to CD4+IL-17+H2B+ triple-positive cells within acne lesions. TETs are visualized as fibrous structures containing DNA (DAPI, blue) decorated with histone H2B (green) in the extracellular space. The images are projections of confocal Z-stacks generated from sections of 10-μm thickness. Data are from 3 individual samples. Scale bars: 10 μm (enlarged insets).

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