Three Loops of the Common γ Chain Ectodomain Required for the Binding of Interleukin-2 and Interleukin-7

Olosz, Ferenc; Malek, Thomas R.

doi:10.1074/jbc.m004976200

Cited by 22 publications

(33 citation statements)

References 32 publications

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“…Most strikingly, little specificity is conferred upon the IL-2͞␥ c interface due to the formation of only 2 hydrogen bonds, as opposed to 7 and 10 in the other two IL-2͞IL-2R interfaces. Our structural results also agree well with extensive mutagenesis work on defining the epitopes on ␥ c for various cytokines (25,26,35). Tyr-103 ␥ , Cys-160 ␥ , and Cys-209 ␥ , identified as hot-spot residues in all of the cytokine͞␥ c interfaces, form a hydrophobic patch in the center of the IL-2͞␥ c interface.…”

Section: Figsupporting

confidence: 75%

“…Tyr-103 ␥ , His-159 ␥ , and Leu-208 ␥ together with the disulfide (Cys-160 ␥ -Cys-209 ␥ ) contribute 53% of the buried surface on ␥ c and represent the major binding determinant. The importance of the disulfide bridge was previously appreciated from mutagenesis data (25,26), but its direct involvement in ligand binding was unexpected. With a buried surface area of 72 Å 2 and one hydrogen bond, IL2 is the most critical IL-2 residue that contacts ␥ c in accordance with biochemical data (27).…”

Section: Structure Of Il-2r␣ and Itsmentioning

confidence: 99%

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Crystal structure of the IL-2 signaling complex: Paradigm for a heterotrimeric cytokine receptor

Stauber

Debler

Horton

et al. 2006

Proc. Natl. Acad. Sci. U.S.A.

243

217

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IL-2 is a cytokine that functions as a growth factor and central regulator in the immune system and mediates its effects through ligand-induced hetero-trimerization of the receptor subunits IL-2R␣, IL-2R␤, and ␥c. Here, we describe the crystal structure of the trimeric assembly of the human IL-2 receptor ectodomains in complex with IL-2 at 3.0 Å resolution. The quaternary structure is consistent with a stepwise assembly from IL-2͞IL-2R␣ to IL-2͞IL-2R␣͞IL-2R␤ to IL-2͞IL-2R␣͞IL-2R␤͞␥c. The IL-2R␣ subunit forms the largest of the three IL-2͞IL-2R interfaces, which, together with the high abundance of charge-charge interactions, correlates well with the rapid association rate and high-affinity interaction of IL-2R␣ with IL-2 at the cell surface. Surprisingly, IL-2R␣ makes no contacts with IL-2R␤ or ␥c, and only minor changes are observed in the IL-2 structure in response to receptor binding. These findings support the principal role of IL-2R␣ to deliver IL-2 to the signaling complex and act as regulator of signal transduction. Cooperativity in assembly of the final quaternary complex is easily explained by the extraordinarily extensive set of interfaces found within the fully assembled IL-2 signaling complex, which nearly span the entire length of the IL-2R␤ and ␥c subunits. Helix A of IL-2 wedges tightly between IL-2R␤ and ␥c to form a three-way junction that coalesces into a composite binding site for the final ␥c recruitment. The IL-2͞␥c interface itself exhibits the smallest buried surface and the fewest hydrogen bonds in the complex, which is consistent with its promiscuous use in other cytokine receptor complexes.common ␥ chain ͉ cooperativity ͉ IL-2 receptor ͉ receptor assembly ͉ structure-activity relationship

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Section: Figsupporting

confidence: 75%

Section: Structure Of Il-2r␣ and Itsmentioning

confidence: 99%

Crystal structure of the IL-2 signaling complex: Paradigm for a heterotrimeric cytokine receptor

Stauber

Debler

Horton

et al. 2006

Proc. Natl. Acad. Sci. U.S.A.

243

217

View full text Add to dashboard Cite

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“…The available data about sites of interaction of cytokine receptors with their specific ligands indicated that the loop regions of FNIII domains rather than ␤ strands were the most likely ligand-binding sites (32)(33)(34)(35)(36). An alignment of Ig-like domains was used to predict the ␤ strands and loop regions of the G-CSF-R Ig-like domain.…”

Section: Mutation Of the Predicted Loop Regions Of The Ig-like Domain-mentioning

confidence: 99%

Identification of Ligand-binding Site III on the Immunoglobulin-like Domain of the Granulocyte Colony-stimulating Factor Receptor

Layton¹,

Hall²,

Connell³

et al. 2001

Journal of Biological Chemistry

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The granulocyte colony-stimulating factor receptor (G-CSF-R) forms a tetrameric complex with G-CSF containing two ligand and two receptor molecules. The Nterminal Ig-like domain of the G-CSF-R is required for receptor dimerization, but it is not known whether it binds G-CSF or interacts elsewhere in the complex. Alanine scanning mutagenesis was used to show that residues in the Ig-like domain of the G-CSF-R (Phe 75 , Gln 87 , and Gln 91 ) interact with G-CSF. This binding site for G-CSF overlapped with the binding site of a neutralizing anti-G-CSF-R antibody. A model of the Ig-like domain showed that the binding site is very similar to the viral interleukin-6 binding site (site III) on the Ig-like domain of gp130, a related receptor. To further characterize the G-CSF-R complex, exposed and inaccessible regions of monomeric and dimeric ligand-receptor complexes were mapped with monoclonal antibodies. The results showed that the E helix of G-CSF was inaccessible in the dimeric but exposed in the monomeric complex, suggesting that this region binds to the Ig-like domain of the G-CSF-R. In addition, the N terminus of G-CSF was exposed to antibody binding in both complexes. These data establish that the dimerization interface of the complete receptor complex is different from that in the x-ray structure of a partial complex. A model of the tetrameric G-CSF⅐G-CSF-R complex was prepared, based on the viral interleukin-6⅐gp130 complex, which explains these and previously published data. The granulocyte colony-stimulating factor receptor (G-CSF-R)1 is a transmembrane protein that is expressed predominantly on cells of the neutrophil lineage and is important in transmitting signals for their proliferation, differentiation, and function (1, 2). The extracellular region comprises six structural domains: an N-terminal Ig-like domain followed by five fibronectin type III (FNIII) domains (3) (Fig. 1A). The first two of the FNIII domains (called D2 and D3) form the cytokine receptor homology (CRH) module, which contains four cysteine residues in D2 and a WSXWS motif in D3. These features of the CRH module are conserved in members of the class 1 cytokine receptor family (4). This domain structure is also found in the closest homologue of the G-CSF-R, gp130, which is the shared signal transducing receptor chain of the interleukin (IL)-6 family of cytokines (5). The G-CSF-R and gp130 share 46% sequence similarity in the extracellular region (6). The ligands for the class 1 cytokine receptors have a conserved 4-␣-helical bundle structure but little sequence similarity (7).In the gp130 family of ligands and receptors, three binding interfaces have been identified (reviewed in Ref. 8). For example, IL-6 interacts with the IL-6 receptor at site I and gp130 at site II. A second gp130 receptor interacts at site III, resulting in a hexameric complex of two components each of IL-6, IL-6 receptor, and gp130 (9). On the IL-6 family of ligands, site I is located at the end of the D helix, site II on the A and C helices, and site III at the N...

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“…The pDC302 expression vector containing the full-length mouse IL-4R␣ (mIL-4R␣) cDNA was described previously (22) (provided by Immunex Corp., Seattle, WA). Site-directed mutagenesis of the m␥ c gene was performed by the QuikChange method (Stratagene, La Jolla, CA), as previously described (17). Mutations were verified by DNA sequencing.…”

Section: Methodsmentioning

confidence: 99%

“…Recent structure-function analysis of the mouse ␥ c (m␥ c ) ectodomain by site-directed mutagenesis (17), guided by predictions of theoretical models of the ␥ c structure (18 -20), identified four amino acids of ␥ c that are necessary for binding IL-2 and IL-7 (17). One of these residues, Tyr-103, may be directly involved in IL-2 and IL-7 binding.…”

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confidence: 99%

Structural Basis for Binding Multiple Ligands by the Common Cytokine Receptor γ-Chain

Olosz

Malek

2002

Journal of Biological Chemistry

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The common ␥-chain (␥ c ) that functions both in ligand binding and signal transduction is a shared subunit of the multichain receptors for interleukin (IL)-2, IL-4, IL-7, IL-9, IL-15, and IL-21. The structural basis by which the ectodomain of ␥ c contributes to binding six distinct cytokines is only partially defined. In the present study, epitope mapping of antagonistic anti-␥ c monoclonal antibodies led to the identification of Asn-128 of mouse ␥ c that represents another potential contact residue that is required for binding IL-2, IL-7, and IL-15 but not IL-4. In addition, Tyr-103, Cys-161, Cys-210, and Cys-211, previously identified to contribute to binding IL-2 and IL-7, were also found to be involved in binding IL-4 and IL-15. Collectively, these data favor a model in which ␥ c utilizes a common mechanism for its interactions with multiple cytokines, and the binding sites are largely overlapping but not identical. Asn-128 and Tyr-103 likely act as contact residues whereas Cys-161, Cys-210, and Gly-211 may stabilize the structure of the proposed ligandinteracting surface formed by the two extracytoplasmic domains.

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Three Loops of the Common γ Chain Ectodomain Required for the Binding of Interleukin-2 and Interleukin-7

Cited by 22 publications

References 32 publications

Crystal structure of the IL-2 signaling complex: Paradigm for a heterotrimeric cytokine receptor

Crystal structure of the IL-2 signaling complex: Paradigm for a heterotrimeric cytokine receptor

Identification of Ligand-binding Site III on the Immunoglobulin-like Domain of the Granulocyte Colony-stimulating Factor Receptor

Structural Basis for Binding Multiple Ligands by the Common Cytokine Receptor γ-Chain

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