Article

  • The EMBO Journal (2005) 24, 2265 - 2283
  • doi:10.1038/sj.emboj.7600688

Published online: 9 June 2005

Essential role of Hrs in a recycling mechanism mediating functional resensitization of cell signaling

Aylin C Hanyaloglu1, Emma McCullagh1 and Mark von Zastrow1

  1. University of California, San Francisco, CA, USA

Correspondence to:

Mark von Zastrow, Department of Psychiatry and Department of Cellular and Molecular Pharmacology, UCSF, N212 Genentech Hall, San Francisco, CA 94143-2140, USA. Tel.: +1 415 476 7855; Fax: +1 415 514 0169; E-mail: zastrow@itsa.ucsf.edu

Received 8 October 2004; Accepted 28 April 2005


Hepatocyte growth factor-regulated tyrosine kinase substrate (Hrs) is well known to terminate cell signaling by sorting activated receptors to the MVB/lysosomal pathway. Here we identify a distinct role of Hrs in promoting rapid recycling of endocytosed signaling receptors to the plasma membrane. This function of Hrs is specific for receptors that recycle in a sequence-directed manner, in contrast to default recycling by bulk membrane flow, and is distinguishable in several ways from previously identified membrane-trafficking functions of Hrs/Vps27p. In particular, Hrs function in sequence-directed recycling does not require other mammalian Class E gene products involved in MVB/lysosomal sorting, nor is receptor ubiquitination required. Mutational studies suggest that the VHS domain of Hrs plays an important role in sequence-directed recycling. Disrupting Hrs-dependent recycling prevented functional resensitization of the beta2-adrenergic receptor, converting the temporal profile of cell signaling by this prototypic G protein-coupled receptor from sustained to transient. These studies identify a novel function of Hrs in a cargo-specific recycling mechanism, which is critical to controlling functional activity of the largest known family of signaling receptors.

  • Keywords:

    • GPCR,
    • Hrs,
    • recycling,
    • resensitization,
    • ubiquitin
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