Neurotrophic factor receptor

Neurotrophic factor receptors or neurotrophin receptors are a group of growth factor receptors which specifically bind to neurotrophins (neurotrophic factors).

Two classes of neurotrophic factor receptors are the p75 and the "Trk" families of Tyrosine kinases receptors.

  • p75 is a low affinity neurotrophin receptor, to which all neurotrophins bind. It is a member of the tumour necrosis super family. In some contexts, the phrase "x" only applies to this receptor.[1]
  • The Trk family include TrkA, TrkB, and TrkC, and will only bind with specific neurotrophins, but with a much higher affinity. The Trks mediate the functional signals of the neurotrophins.
  • NGF binds to TrkA, BDNF and NT-4 bind to TrkB and NT-3 binds to TrkC. In addition NT-3 also binds to and activates TrkA and TrkB but it does so less efficiently.
  • Whilst the Trk receptors have a clearly defined trophic role, p75 receptors activate signalling pathways which can also result in apoptosis.

TrkA, B, and C receptors

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TrkA mediates its actions by causing the addition of phosphate molecules on certain tyrosines in the cell, activating cellular signaling.

There are other related Trk receptors (TrkB and TrkC), and there are other neurotrophic factors structurally related to NGF (BDNF, NT-3, and NT-4)

p75NTR receptor

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The Low affinity nerve growth factor receptor commonly known as "p75", can signal for apoptosis or promote neuronal survival. Neurotrophins that interact with p75NTR include NGF, NT-3, BDNF, and NT-4/5.[2] Neurotrophins activating p75NTR may initiate apoptosis (for example, via c-Jun N-terminal kinases signaling), and this effect can be counteracted by anti-apoptotic signaling by TrkA.[3] Neurotrophin binding to p75NTR can promote neuronal survival (for example, via NF-kB activation).[4]

Although NGF has been classically described as promoting neuron survival and differentiation, research performed in the early 2000s suggest that NGF with its prodomain attached (proNGF) can elicit apoptosis of cells that are positive for the LNGFR and negative for TrkA.[5]

Secreted proNGF has been demonstrated in a variety of neuronal and non-neuronal cell populations. It has been proposed that secreted proNGF can elicit neuron death in a variety of neurodegenerative conditions, including Alzheimer's disease, following the observation of an increase of proNGF in the nucleus basalis of postmortem Alzheimer's brains [citation needed].

References

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  1. ^ Nerve+Growth+Factor+Receptor+p75 at the U.S. National Library of Medicine Medical Subject Headings (MeSH)
  2. ^ Bibel, M.; Hoppe, E.; Barde, Y. A. (1999). "Biochemical and functional interactions between the neurotrophin receptors TRK and p75NTR". The EMBO Journal. 18 (3): 616–22. doi:10.1093/emboj/18.3.616. PMC 1171154. PMID 9927421.
  3. ^ Becker, E. B.; Howell, J.; Kodama, Y.; Barker, P. A.; Bonni, A. (2004). "Characterization of the c-Jun N-terminal kinase-BimEL signaling pathway in neuronal apoptosis". The Journal of Neuroscience. 24 (40): 8762–70. doi:10.1523/JNEUROSCI.2953-04.2004. PMC 6729963. PMID 15470142.
  4. ^ Hamanoue, M.; Middleton, G.; Wyatt, S.; Jaffray, E.; Hay, R. T.; Davies, A. M. (1999). "P75-mediated NF-kappaB activation enhances the survival response of developing sensory neurons to nerve growth factor". Molecular and Cellular Neurosciences. 14 (1): 28–40. doi:10.1006/mcne.1999.0770. PMID 10433815. S2CID 25648122.
  5. ^ Ibáñez C (2002). "Jekyll-Hyde neurotrophins: the story of proNGF". Trends Neurosci. 25 (6): 284–6. doi:10.1016/S0166-2236(02)02169-0. PMID 12086739. S2CID 9449831.

Further reading

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Review papers offer overviews and drawings of p75NTR pathways.[1][2]

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  1. ^ Reichardt, L. F. (2006). "Neurotrophin-regulated signalling pathways". Philosophical Transactions of the Royal Society of London. Series B, Biological Sciences. 361 (1473): 1545–64. doi:10.1098/rstb.2006.1894. PMC 1664664. PMID 16939974.
  2. ^ Kalb, R. (2005). "The protean actions of neurotrophins and their receptors on the life and death of neurons". Trends in Neurosciences. 28 (1): 5–11. doi:10.1016/j.tins.2004.11.003. PMID 15626491. S2CID 8468230.