Tumor Necrosis Factor Receptor-Associated Factor (TRAF)2 Represses the T Helper Cell Type 2 Response through Interaction with NFAT-Interacting Protein (NIP45)

Authors

Rebecca Lieberson, Harvard School of Public Health
Kerri A. Mowen, Harvard School of Public Health
Kathryn D. McBride, Harvard School of Public Health
Veronica Leautaud, Harvard School of Public Health
Xiankui Zhang, Medical University of South Carolina
Woong-Kyung Suh, Ontario Cancer Institute
Lin Wu
Laurie H. Glimcher, Harvard Medical School

Document Type

Article

Embargo Period

7-2-2001

Publication Date

7-2-2001

Abstract

Recently we have identified a novel protein NIP45 (nuclear factor of activated T cells [NFAT]-interacting protein) which substantially augments interleukin (IL)-4 gene transcription. The provision of NIP45 together with NFAT and the T helper cell type 2 (Th2)-specific transcription factor c-Maf to cells normally refractory to IL-4 production, such as B cells or Th1 clones, results in substantial IL-4 secretion to levels that approximate those produced by primary Th2 cells. In studies designed to further our understanding of NIP45 activity, we have uncovered a novel facet of IL-4 gene regulation. We present evidence that members of the tumor necrosis factor receptor–associated factor (TRAF) family of proteins, generally known to function as adapter proteins that transduce signals from the tumor necrosis factor receptor superfamily, contribute to the repression of IL-4 gene transcription and that this effect is mediated through their interaction with NIP45.

Journal

Journal of Experimental Medicine

Recommended Citation

Lieberson, Rebecca; Mowen, Kerri A.; McBride, Kathryn D.; Leautaud, Veronica; Zhang, Xiankui; Suh, Woong-Kyung; Wu, Lin; and Glimcher, Laurie H., "Tumor Necrosis Factor Receptor-Associated Factor (TRAF)2 Represses the T Helper Cell Type 2 Response through Interaction with NFAT-Interacting Protein (NIP45)" (2001). MUSC Faculty Journal Articles. 51.
https://medica-musc.researchcommons.org/facarticles/51