Structure and function of Norrin in assembly and activation of a Frizzled 4–Lrp5/6 complex

  1. H. Eric Xu1,7,8
  1. 1Laboratory of Structural Sciences, Van Andel Research Institute, Grand Rapids, Michigan 49503, USA;
  2. 2Department of Molecular Pharmacology and Experimental Therapeutics, Mayo Clinic, Scottsdale, Arizona 85259, USA;
  3. 3Department of Biological Structure, University of Washington School of Medicine, Seattle, Washington 98195, USA;
  4. 4Center for Skeletal Disease Research,
  5. 5Laboratory of Cell Signaling and Carcinogenesis,
  6. 6Laboratory for Structural Biology and Biochemistry, Van Andel Research Institute, Grand Rapids, Michigan 49503, USA;
  7. 7Van Andel Research Institute/Shanghai Institute of Materia Medica Center, Key Laboratory of Receptor Research, Shanghai Institute of Materia Medica, Chinese Academy of Sciences, Shanghai 201203, China

    Abstract

    Norrin is a cysteine-rich growth factor that is required for angiogenesis in the eye, ear, brain, and female reproductive organs. It functions as an atypical Wnt ligand by specifically binding to the Frizzled 4 (Fz4) receptor. Here we report the crystal structure of Norrin, which reveals a unique dimeric structure with each monomer adopting a conserved cystine knot fold. Functional studies demonstrate that the novel Norrin dimer interface is required for Fz4 activation. Furthermore, we demonstrate that Norrin contains separate binding sites for Fz4 and for the Wnt ligand coreceptor Lrp5 (low-density lipoprotein-related protein 5) or Lrp6. Instead of inducing Fz4 dimerization, Norrin induces the formation of a ternary complex with Fz4 and Lrp5/6 by binding to their respective extracellular domains. These results provide crucial insights into the assembly and activation of the Norrin–Fz4–Lrp5/6 signaling complex.

    Keywords

    Footnotes

    • Received August 13, 2013.
    • Accepted October 3, 2013.

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