1998
DOI: 10.1083/jcb.140.4.911
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The p75 Neurotrophin Receptor Mediates Neuronal Apoptosis and Is Essential for Naturally Occurring Sympathetic Neuron Death

Abstract: Abstract. To determine whether the p75 neurotrophin receptor (p75NTR) plays a role in naturally occurring neuronal death, we examined neonatal sympathetic neurons that express both the TrkA tyrosine kinase receptor and p75NTR. When sympathetic neuron survival is maintained with low quantities of NGF or KCl, the neurotrophin brain-derived neurotrophic factor (BDNF), which does not activate Trk receptors on sympathetic neurons, causes neuronal apoptosis and increased phosphorylation of c-jun. Function-blocking a… Show more

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Cited by 464 publications
(494 citation statements)
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References 63 publications
(101 reference statements)
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“…Importantly, NGF does not cause significant cell death, despite the fact that subplate neurons do not express the Trk receptor for NGF, TrkA. These observations differ significantly from results in sympathetic neurons and oligodendrocytes, in which p75NTR signaling promotes cell death in the absence of activated TrkA receptors (Bamji et al, 1998;Yoon et al, 1998). Coaddition of saturating amounts of both BDNF and NT3 does not increase subplate neuron survival above that with either factor alone (Fig.…”
Section: P75ntr Promotes Survival Of Cultured Subplate Neuronscontrasting
confidence: 47%
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“…Importantly, NGF does not cause significant cell death, despite the fact that subplate neurons do not express the Trk receptor for NGF, TrkA. These observations differ significantly from results in sympathetic neurons and oligodendrocytes, in which p75NTR signaling promotes cell death in the absence of activated TrkA receptors (Bamji et al, 1998;Yoon et al, 1998). Coaddition of saturating amounts of both BDNF and NT3 does not increase subplate neuron survival above that with either factor alone (Fig.…”
Section: P75ntr Promotes Survival Of Cultured Subplate Neuronscontrasting
confidence: 47%
“…Studies of mice carrying a gene deletion of p75NTR reveal that it is necessary for survival of sensory and basal forebrain cholinergic neurons, although, conversely, it is necessary for naturally occurring cell death in sympathetic, motor, and retinal neurons (Lee et al, 1992;Bamji et al, 1998;Brennan et al, 1999;Frade and Barde, 1999;Peterson et al, 1999). However, because both neuronal and non-neuronal cells express p75NTR, it is unclear from these studies, as well as studies of unpurified neurons in vitro, whether or not p75NTR functions in a cellautonomous manner for all of these neuronal populations.…”
Section: Discussionmentioning
confidence: 99%
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“…The co-presence of Trk on a neuron silences pro-apoptotic pathways by activation of the pro-survival transcription factor, NF-κB, which subsequently activates Akt (Bibel & Barde, 2000;Kaplan & Miller, 2000;Khursigara et al, 1999). Sympathetic neurons and basal forebrain neurons that were p75-deficient in p75-/-mice underwent robust axonal sprouting, hypertrophy, or target innervation with naturally-occurring developmental apoptosis being significantly delayed (Kaplan & Miller, 2000;Walsh et al, 1999;Yeo et al, 1997;Bamji et al, 1998). Without intrinsic catalytic activity, the p75 ICD appears to rely on docking of adaptor www.intechopen.com Aloyz et al, 1998;Salehi, et al, 2002;Muller, et al, 1998;de Chaves et al, 1997;Casademunt, et al, 1999;2 Chittka & Chao, 1999;3 Domeniconi et al, 2005;4 Khursigara et al, 1999;5 Susen, et al, 1999;Lad & Neet, 2003.…”
Section: P75 Signalingmentioning
confidence: 99%
“…The role of p75 during development is time-and area-dependent. For example, p75 can mediate cell death in specific populations, including oligodendrocytes and sympathetic neurons (e.g., Casaccia-Bonnefil et al, 1996;Bamji et al, 1998). In other models, e.g., cultured hippocampal neurons or PC12 cells, p75 mediates survival (Roux et al, 2001;Bui et al, 2002;Culmsee et al, 2002).…”
Section: Role Of Neurotrophinsmentioning
confidence: 99%