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Introduction

Interleukin 33 is a cytokine member of the IL-1 superfamily. Cytokines are proteins involved in cell signaling. Their role is to regulate the function and the activity of other cells. IL-33 is involved in innate and adaptive immune responses.

In 2005, IL-33 was identified as a ligand for the transmembrane receptor ST2 and it IL-1 receptor accessory protein (IL-1RAcP), both members of the interleukin-1 receptor family. IL-33/ST2 signaling is involved in T-cell immune responses.

We will focuse on the interaction bewteen IL33 and the ST2 ectodomain (as you can see ).

Function

Caracteristics of IL-33:

IL-33 is constitutively expressed in several cells, such as epithelial or endothelial cells. IL-33 is also expressed in an inducible way by immune cells. In this case, the constitutive expression of IL-33 is very low or absent. In mast cells, the expression of IL-33 is induced by the calcium, but the mechanisms are still unclear. IL-33 is secreted in damaged tissues, where it activates the immune response.

Target cells:

ST2 exists in a soluble form (sST2) and a transmembrane form (ST2L). The both forms can interact with IL-33. ST2L are expressed in T lymphocytes, when they are specializing into Th2 cells (T helper type 2 cells, a specific type of T lymphocytes). This specialization occurs in the presence of IL4, expected to be secreted by polynuclear basophils.

IL-33 interacts with the ectodomain of ST2L. This interaction provokes the recruitment of the myeloid differentiation primary-response protein 88 (MYD88) complex, which is involved in the immune response against commune viral infections and some bacterial infections.

When IL-33 interacts with the sST2, it inhibits the fixation of IL-33 of the ectodomain of ST2.

Structure

Overall structure:

The understanding of the interaction of IL-33 with its receptors has been discovered thanks to the determination of the crystal structure of IL-33 in complex with ectodomain of ST2.

Besides, the combination of crystallography and small-angle X-ray-scattering methods reveal that ST2 has a very flexible conformation, contrary to IL-1RAcP. In fact, ST2 is constituted of three IgG-like domains (). D1 and D2 gather to form a single D1D2 module, connected through a linker with the D3 domain. ST2 contains also three residues linked with NAG.

This conformational specificity provides a capactity of ligand-binding with IL-33. Moreover, the rigidity of IL-1RAcP explains that it can not bind the IL-33 ligand directly.

In humans, IL-33 in its full length is composed of 270 residues and is biologically active.

The model includes IL-33 residues Ser117 to Ser268 and ST2 residues Ser21 to Arg317.

The structure of IL-33 consists in a forming a β-trefoil structure. Specific loops, such as the β4-β5 loop, are involved in the interaction with the accessory receptor IL-1RAcP when IL-33 is bound to ST2.

IL-33/ST2 interactions:

In the complex, IL-33 interacts with the three domains of ST2. The binding interface is very large and composed of two separate sites.

In the first binding site, thirteen IL-33 residues from β-loops are in contact with the D1D2 module of ST2: the four marked acids residues of IL-33 form a salt-bridge with five marked ST2 residues respectively. Besides, Glu144 and Asp149 form hydrogen bonds with main-chain atoms of ST2. IL-33 mutation of one of the acid residues (144, 148, 149 and 244) highly decreases the affinity of ST2 for IL-33.

In the second binding site, eight IL-33 residues from β-strands interact with the D3 domain of ST2.

There are both hydrophobic and hydrophilic interactions. Residues of IL-33 form an hydrophobic cluster (IL-33 residues Tyr163 and Leu182 and ST2 residues Leu246, Leu306, and Leu311). A salt-bridge interaction occurs between acidic residue Glu165 and Arg313 of ST2.