Precursor cell survival and proliferation Numerous studies, both
in vivo and
in vitro, have shown that neurotrophins have proliferation and differentiation effects on CNS neuro-epithelial precursors,
neural crest cells, or precursors of the
enteric nervous system. TrkA that expresses NGF not only increase the survival of both C and A delta classes of nocireceptor neurons, but also affect the functional properties of these neurons.4 As mentioned before, BDNF improves the survival and function of neurons in CNS, particularly cholinergic neurons of the
basal forebrain, as well as neurons in the hippocampus and cortex. BDNF belongs to the neurotrophin family of growth factors and affects the survival and function of neurons in the central nervous system, particularly in brain regions susceptible to degeneration in AD. BDNF improves survival of cholinergic neurons of the basal forebrain, as well as neurons in the hippocampus and cortex. TrkC that expresses NT3 has been shown to promote proliferation and survival of cultured
neural crest cells, oligodendrocyte precursors, and differentiation of hippocampal neuron precursors.
Control of target innervation Each of the neurotrophins mentioned above promotes
neurite outgrowth. NGF/TrkA signaling regulates the advance of
sympathetic neuron
growth cones; even when neurons received adequate trophic (sustaining and nourishing) support, one experiment showed they did not grow into relating compartments without NGF. NGF increases the innervation of tissues that receive sympathetic or sensory innervation and induces aberrant innervation in tissues that are normally not innervated. NGF/TrkA signaling upregulates BDNF, which is transported to both peripheral and central terminals of nocireceptive sensory neurons. In the periphery, TrkB/BDNF binding and TrkB/
NT-4 binding acutely sensitizing nocireceptive pathway that require the presence of
mast cells.
Sensory neuron function Trk receptors and their ligands (neurotrophins) also affect neurons' functional properties. Both
NT-3 and BDNF are important in the regulation and development of
synapses formed between
afferent neurons and
motor neurons. Increased NT-3/trkC binding results in larger
monosynaptic excitatory postsynaptic potentials (EPSPs) and reduced
polysynaptic components. On the other hand, increased NT-3 binding to trkB to BDNF has the opposite effect, reducing the size of monosynaptic excitatory postsynaptic potentials (EPSPs) and increasing polysynaptic signaling.
Formation of ocular dominance column In the development of mammalian visual system, axons from each eyes crosses through the
lateral geniculate nucleus (LGN) and terminate in separate layers of
striate cortex. However, axons from each LGN can only be driven by one side of the eye, but not both together. These axons that terminate in layer IV of the striate cortex result in
ocular dominance columns. A study shows that The density of innervating axons in layer IV from LGN can be increased by exogenous BDNF and reduced by a scavenger of endogenous BDNF. Therefore, it raises the possibility that both of these agents are involved in some sorting mechanism that is not well comprehended yet. Previous studies with cat model has shown that
monocular deprivation occurs when input to one of the mammalian eyes is absent during the critical period (critical window). However, A study demonstrated that the infusion of NT-4 (a ligand of trkB) into the visual cortex during the critical period has been shown to prevent many consequences of
monocular deprivation. Surprisingly, even after losing responses during the critical period, the infusion of NT-4 has been shown to be able to restore them.
Synaptic strength and plasticity In mammalian
hippocampus, the axons of the
CA3 pyramidal cells project into
CA1 cells through the
Schaffer collaterals. The
long-term potentiation (LTP) may induce in either of these pathways, but it is specific only to the one that is stimulated with
tetanus. The stimulated axon does not impact spill over to the other pathway. TrkB receptors are expressed in most of these hippocampal neurons, including
dentate granule cells, CA3 and CA1 pyramidal cells, and inhibitory
interneurons. LTP can be greatly reduced by BDNF mutants. In a similar study on a mouse mutant with reduced expression of trkB receptors, LTP of CA1 cells reduced significantly. TrkB loss has also been linked to interfere with the memory acquisition and consolidation in many learning paradigm. ==Role of Trk oncogenes in cancer==