Literature DB >> 18656487

The exon-3-encoded domain of IL-15ralpha contributes to IL-15 high-affinity binding and is crucial for the IL-15 antagonistic effect of soluble IL-15Ralpha.

Grégory Bouchaud1, Laure Garrigue-Antar, Véronique Solé, Agnès Quéméner, Yvan Boublik, Erwan Mortier, Harmonie Perdreau, Yannick Jacques, Ariane Plet.   

Abstract

We previously showed that a natural soluble form of interleukin-15 (IL-15) Ralpha corresponding to the full-length ectodomain of IL-15Ralpha behaved as a potent antagonist of IL-15 action through IL-15Ralpha/beta/gamma, whereas a recombinant soluble IL-15Ralpha sushi domain did not, but instead acted as an agonist of IL-15 action through IL-15Rbeta/gamma. In order to determine precisely the molecular basis governing these antagonistic versus agonistic actions, we compared the binding properties and biological effects of recombinant soluble IL-15Ralpha (sIL-15Ralpha) species containing the sushi domain and different remaining parts of the ectodomain. We first demonstrate that the exon-3-encoded domain and, more particularly, its N-terminal 13-amino-acid (aa) peptide are important, in addition to the adjacent exon-2-encoded sushi domain, for the stabilization of the high-affinity IL-15.IL-15Ralpha complex by slowing down its dissociation rate and by contributing to about 10-20% of the free energy of interaction. We next show that all sushi-containing sIL-15Ralpha are agonists on IL-15Rbeta/gamma, coordinately increasing IL-15 binding and IL-15-induced proliferation. Their agonistic potencies are proportional to their respective affinities for IL-15. We then show that the antagonistic effect of sIL-15Ralpha in the context of IL-15Ralpha/beta/gamma is due to the 13-aa peptide that creates a sterical constraint impeding the binding of the sIL-15Ralpha.IL-15 complex to the membrane-anchored IL-15Ralpha/beta/gamma. In the frame of the soluble IL-15Ralpha sushi domain-IL-15 fusion protein that contains the 13-aa peptide, this constraint is alleviated as a result of a conformational effect due to the covalent linking of the 13-aa peptide to the N-terminus of IL-15. The soluble IL-15Ralpha sushi domain-IL-15 fusion protein is therefore able to bind and activate both the IL-15Rbeta/gamma and the IL-15Ralpha/beta/gamma receptors.

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Year:  2008        PMID: 18656487     DOI: 10.1016/j.jmb.2008.07.019

Source DB:  PubMed          Journal:  J Mol Biol        ISSN: 0022-2836            Impact factor:   5.469


  19 in total

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2.  A targeted IL-15 fusion protein with potent anti-tumor activity.

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Review 3.  IL-2 and Beyond in Cancer Immunotherapy.

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4.  Identification of a potent anti-IL-15 antibody with opposing mechanisms of action in vitro and in vivo.

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5.  NKTR-255 is a polymer-conjugated IL-15 with unique mechanisms of action on T and natural killer cells.

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6.  Novel human interleukin-15 agonists.

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7.  Design and characterization of a protein superagonist of IL-15 fused with IL-15Rα and a high-affinity T cell receptor.

Authors:  Jennifer D Stone; Adam S Chervin; Hans Schreiber; David M Kranz
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8.  Human fused NKG2D-IL-15 protein controls xenografted human gastric cancer through the recruitment and activation of NK cells.

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Journal:  Cell Mol Immunol       Date:  2015-09-14       Impact factor: 11.530

Review 9.  Immunobiology of the IL-15/IL-15Rα complex as an antitumor and antiviral agent.

Authors:  Yin Guo; Liming Luan; Naeem K Patil; Edward R Sherwood
Journal:  Cytokine Growth Factor Rev       Date:  2017-09-01       Impact factor: 7.638

10.  Highly potent anti-CD20-RLI immunocytokine targeting established human B lymphoma in SCID mouse.

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Journal:  MAbs       Date:  2014 Jul-Aug       Impact factor: 5.857
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