Frontiers in Immunology (Jun 2021)

NLRP3 Regulates IL-4 Expression in TOX+ CD4+ T Cells of Cutaneous T Cell Lymphoma to Potentially Promote Disease Progression

  • Enrique Huanosta-Murillo,
  • Enrique Huanosta-Murillo,
  • Marcela Alcántara-Hernández,
  • Brenda Hernández-Rico,
  • Brenda Hernández-Rico,
  • Georgina Victoria-Acosta,
  • Patricia Miranda-Cruz,
  • María Antonieta Domínguez-Gómez,
  • Fermín Jurado-Santacruz,
  • Genaro Patiño-López,
  • Vadim Pérez-Koldenkova,
  • Alam Palma-Guzmán,
  • Paula Licona-Limón,
  • Ezequiel M. Fuentes-Pananá,
  • Alicia Lemini-López,
  • Laura C. Bonifaz

DOI
https://doi.org/10.3389/fimmu.2021.668369
Journal volume & issue
Vol. 12

Abstract

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In cutaneous T cell lymphoma (CTCL), a dominant Th2 profile associated with disease progression has been proposed. Moreover, although the production and regulation of IL-4 expression during the early stages of the disease may have important implications in later stages, these processes are poorly understood. Here, we demonstrate the presence of TOX+ CD4+ T cells that produce IL-4+ in early-stage skin lesions of CTCL patients and reveal a complex mechanism by which the NLRP3 receptor promotes a Th2 response by controlling IL-4 production. Unassembled NLRP3 is able to translocate to the nucleus of malignant CD4+ T cells, where it binds to the human il-4 promoter. Accordingly, IL-4 expression is decreased by knocking down and increased by promoting the nuclear localization of NLRP3. We describe a positive feedback loop in which IL-4 inhibits NLRP3 inflammasome assembly, thereby further increasing its production. IL-4 induced a potentially malignant phenotype measured based on TOX expression and proliferation. This mechanism of IL-4 regulation mediated by NLRP3 is amplified in late-stage CTCL associated with disease progression. These results indicate that NLRP3 might be a key regulator of IL-4 expression in TOX+ CD4+ T cells of CTCL patients and that this mechanism might have important implications in the progression of the disease.

Keywords