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Cutting edge: Identification of a pre-ligand assembly domain (PLAD) and ligand binding site in the IL-17 receptor

  • Jill M. Kramer
  • , Walter Hanel
  • , Fang Shen
  • , Nilgun Isik
  • , James P. Malone
  • , Amarnath Maitra
  • , Wade Sigurdson
  • , David Swart
  • , Joel Tocker
  • , Tian Jin
  • , Sarah L. Gaffen
  • SUNY Buffalo
  • National Institutes of Health
  • Amgen Incorporated

Research output: Contribution to journalArticlepeer-review

42 Scopus citations

Abstract

IL-17 is the hallmark cytokine of the newly described "Th17" lymphocyte population. The composition, subunit dynamics, and ligand contacts of the IL-17 receptor are poorly defined. We previously demonstrated that the IL-17RA subunit oligomerizes in the membrane without a ligand. In this study, computational modeling identified two fibronectin-III-like (FN) domains in IL-17RA connected by a nonstructured linker, which we predicted to mediate homotypic interactions. In yeast two-hybrid, the membrane-proximal FN domain (FN2), but not the membrane-distal domain (FN1), formed homomeric interactions. The ability of FN2 to drive ligand-independent multimerization was verified by coimmunoprecipitation and fluorescence resonance energy transfer microscopy. Thus, FN2 constitutes a "pre-ligand assembly domain" (PLAD). Further studies indicated that the FN2 linker domain contains the IL-17 binding site, which was never mapped. However, the FN1 domain is also required for high affinity interactions with IL-17. Therefore, although the PLAD is located entirely within FN2, effective ligand binding also involves contributions from the linker and FN1.

Original languageEnglish
Pages (from-to)6379-6383
Number of pages5
JournalJournal of Immunology
Volume179
Issue number10
DOIs
StatePublished - Nov 15 2007

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