
Experiments over the past decade in which NGF/TrkA signaling has been abolished by antibodies or targeted gene mutations have shown that 70- 85% of dorsal root ganglion (DRG) neurons require NGF for survival during development. There is consensus that many of the NGF-dependent neurons are small-diameter, peptidergic neurons subserving nociception. These neurons express the signaling receptor for NGF, TrkA. There is a major discrepancy, however, between the percentage of DRG neurons which require NGF for survival (70–85%) and percentage of DRG neurons expressing TrkA receptors (40–50%). The identity of these non-TrkA expressing, NGF-dependent neurons has not been established. A candidate group is a population of small DRG neurons with unmyelinated axons which bind BSI isolectins from the plant, Bandeiraea simplicifolia. We show here that most of these BSI-binding DRG neurons do not express TrkA in adult mice. However, in mutant mice in which NGF/TrkA signaling has been abolished by inactivation of the trkA gene, BSI-staining in the DRG and dorsal horn is completely eliminated. BSI-binding DRG cells are thus the first identified neuronal population in which cells do not express TrkA in maturity, but require NGF/TrkA signaling for survival during embryonic development. These neurons must either depend on NGF via a novel, indirect mechanism or alternatively, downregulate TrkA expression during development.
Mice, Knockout, Neurons, Heterozygote, Cell Survival, Homozygote, Neuropeptides, Nociceptors, Axons, Mice, Spinal Cord, Neurofilament Proteins, Ganglia, Spinal, Lectins, Mutation, Animals, Phosphorylation, Plant Lectins, Receptor, trkA
Mice, Knockout, Neurons, Heterozygote, Cell Survival, Homozygote, Neuropeptides, Nociceptors, Axons, Mice, Spinal Cord, Neurofilament Proteins, Ganglia, Spinal, Lectins, Mutation, Animals, Phosphorylation, Plant Lectins, Receptor, trkA
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