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Sortilin is essential for proNGF-induced neuronal cell death

Author

Listed:
  • Anders Nykjaer

    (Aarhus University
    ReceptIcon Aps)

  • Ramee Lee

    (Weill Medical College of Cornell University)

  • Kenneth K. Teng

    (Weill Medical College of Cornell University)

  • Pernille Jansen

    (Aarhus University
    Max-Delbrück-Center for Molecular Medicine)

  • Peder Madsen

    (Aarhus University)

  • Morten S. Nielsen

    (Aarhus University)

  • Christian Jacobsen

    (Aarhus University)

  • Marco Kliemannel

    (Martin-Luther-Universität)

  • Elisabeth Schwarz

    (Martin-Luther-Universität)

  • Thomas E. Willnow

    (ReceptIcon Aps
    Max-Delbrück-Center for Molecular Medicine)

  • Barbara L. Hempstead

    (Weill Medical College of Cornell University)

  • Claus M. Petersen

    (Aarhus University)

Abstract

Sortilin1 (∼95 kDa) is a member of the recently discovered family of Vps10p-domain receptors2,3, and is expressed in a variety of tissues, notably brain, spinal cord and muscle. It acts as a receptor for neurotensin4,5, but predominates in regions of the nervous system that neither synthesize nor respond to this neuropeptide6, suggesting that sortilin has additional roles. Sortilin is expressed during embryogenesis7 in areas where nerve growth factor (NGF) and its precursor, proNGF, have well-characterized effects6,7. These neurotrophins can be released by neuronal tissues8,9, and they regulate neuronal development through cell survival and cell death signalling. NGF regulates cell survival and cell death via binding to two different receptors, TrkA and p75NTR (ref. 10). In contrast, proNGF selectively induces apoptosis through p75NTR but not TrkA11. However, not all p75NTR-expressing cells respond to proNGF, suggesting that additional membrane proteins are required for the induction of cell death. Here we report that proNGF creates a signalling complex by simultaneously binding to p75NTR and sortilin. Thus sortilin acts as a co-receptor and molecular switch governing the p75NTR-mediated pro-apoptotic signal induced by proNGF.

Suggested Citation

  • Anders Nykjaer & Ramee Lee & Kenneth K. Teng & Pernille Jansen & Peder Madsen & Morten S. Nielsen & Christian Jacobsen & Marco Kliemannel & Elisabeth Schwarz & Thomas E. Willnow & Barbara L. Hempstead, 2004. "Sortilin is essential for proNGF-induced neuronal cell death," Nature, Nature, vol. 427(6977), pages 843-848, February.
    • Handle: RePEc:nat:nature:v:427:y:2004:i:6977:d:10.1038_nature02319
    DOI: 10.1038/nature02319
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    Cited by:

    1. Michael W Pankhurst & Christine A Clark & Judith Zarek & Carl A Laskin & Ian S McLennan, 2016. "Changes in Circulating ProAMH and Total AMH during Healthy Pregnancy and Post-Partum: A Longitudinal Study," PLOS ONE, Public Library of Science, vol. 11(9), pages 1-13, September.
    2. Christine Bee & Yasmina N Abdiche & Donna M Stone & Sierra Collier & Kevin C Lindquist & Alanna C Pinkerton & Jaume Pons & Arvind Rajpal, 2012. "Exploring the Dynamic Range of the Kinetic Exclusion Assay in Characterizing Antigen-Antibody Interactions," PLOS ONE, Public Library of Science, vol. 7(4), pages 1-13, April.

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