The Multiple Functions of IL-33

IL-33 was independently described by three different research groups interested in distinct biological topics. Onda et al. identified DVS27 as a protein that is upregulated in vasospastic cerebral arteries.¹ Baekkevold et al. identified NF-HEV as a nuclear factor in the endothelial cells of high endothelial venules.² Schmitz et al. identified IL-33 as an interleukin-1 family cytokine.³ DVS27, NF-HEV, and IL-33 all refer to the same multi-functional protein that is expressed primarily by endothelial and smooth muscle cells in the vasculature and airway.^{3, 4} IL-33 is upregulated by inflammatory stimulation in these cells, as well as keratinocytes and dermal fibroblasts, and by mechanical strain in cardiac fibroblasts.^{1, 5, 6}

IL-33 is synthesized as a 270 amino acid protein in humans and contains an N-terminal nuclear localization signal (NLS), a helix-turn-helix (HTH) motif, and a C-terminal region with structural homology to IL-1 family cytokines. It can be cleaved in vitro by caspase-1 to generate an 18 kDa C-terminal fragment, which serves as a cytokine.^{3, 5} The fate of the released N-terminal fragment has not yet been described. Full length IL-33 localizes to the nucleus where it associates with heterochromatin and mitotic chromosomes.^{1, 2, 5} Both of these interactions are mediated by the HTH motif but not the NLS.⁵ IL-33 functions in this context as a transcriptional repressor, although particular target genes have not been identified.⁵

The C-terminal fragment of IL-33 is the only cytokine that has been shown to bind the receptor ST2L.^{3, 7, 8, 9} The IL-33/ST2L complex subsequently associates with IL-1R AcP to enable IL-33-dependent activation of NFkB.^{3, 10} IL-1R AcP is a shared signaling subunit that also associates with IL-1 RI and IL-1 R6. Extracellular IL-33 promotes Th2-biased immune responses, resulting in eosinophilia and allergic inflammation. In Th2 cells, it upregulates the production of IL-4, IL-5, and IL-13 as well as ST2L.^{3, 10} In mast cells, it cooperates with TSLP in inducing the production of several cytokines and chemokines but does not trigger mast cell degranulation or eicosanoid production.⁷ Alternative splicing of ST2L generates ST2, a soluble decoy receptor that is elevated in the serum of asthma and heart failure patients.^{6, 8} ST2 association with IL-33 blocks ST2L-dependent signaling and the immunological and cardiac effects of IL-33.^{6, 7, 8} The IL-33/ST2L system has a distinct role in the heart. IL-33 counteracts cardiac myocyte hypertrophy, which is induced by angiotensin II or phenylephrine.⁶ This cardioprotective effect is reliant on ST2L-mediated signaling.⁶ In parallel to the induction of IL-33 in cardiac fibroblasts, ST2 is induced in cardiac myocytes by mechanical stress.⁶

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Full length IL-33 (Pro IL-33) localizes to the nucleus where it inhibits gene transcription. The C-terminal cytokine-like fragment of IL-33 is released and binds ST2L. Ternary complexes of IL-33/ST2/IL-1R AcP transduce signals that result in increased expression of proteins involved in allergic inflammation.

IL-33 shows similarities to IL-1 alpha and HMG-B1 in that it exhibits both nuclear and extracellular functions.⁴ Unlike those factors, however, little is known about the regulation of the full length and processed forms of IL-33. Further investigations will likely uncover relationships between its transcriptional targets, chromosome binding, immune and cardiac functions, and potential signaling crosstalk induced by other cytokines that utilize IL-1R AcP.

References

1. Onda, H. et al. (1999) J. Cereb. Blood Flow Metab. 19:1279.
2. Baekkevold, E.S. et al. (2003) Am. J. Pathol. 163:69.
3. Schmitz, J. et al. (2005) Immunity 23:479.
4. Gadina, M. & C.A. Jefferies (2007) Science STKE pe31.
5. Carriere, V. et al. (2007) Proc. Natl. Acad. Sci. USA 104:282.
6. Sanada, S. et al. (2007) J. Clin. Invest. 117:1538.
7. Allakhverdi, Z. et al. (2007) J. Immunol. 179:2051.
8. Hayakawa, H. et al. (2007) J. Biol. Chem. 282:26369.
9. Barksby, H.E. et al. (2007) Clin. Exp. Immunol. 149:217.
10. Chackerian, A.A. et al. (2007) J. Immunol. 179:2551.

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