Sortilin is Essential for ProNGF-induced Neuronal Cell Death

Overview

Journal Nature

Specialty Science

Date 2004 Feb 27

PMID 14985763

Citations 407

Authors

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

Claus M Petersen

Affiliations

Soon will be listed here.

Abstract

Sortilin (approximately 95 kDa) is a member of the recently discovered family of Vps10p-domain receptors, and is expressed in a variety of tissues, notably brain, spinal cord and muscle. It acts as a receptor for neurotensin, but predominates in regions of the nervous system that neither synthesize nor respond to this neuropeptide, suggesting that sortilin has additional roles. Sortilin is expressed during embryogenesis in areas where nerve growth factor (NGF) and its precursor, proNGF, have well-characterized effects. These neurotrophins can be released by neuronal tissues, 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 TrkA. 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.

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