Expression of α2‐adrenergic receptors in rat primary afferent neurones after peripheral nerve injury or inflammation

Abstract

1 Immunocytochemistry with polyclonal antibodies directed against specific fragments of intracellular loops of α_2A- and α_2C-adrenergic receptors (α_2A-AR, α_2C-AR) was used to explore the possibility that expression of these receptors in dorsal root ganglion (DRG) neurones of rat alters as a result of peripheral nerve injury or localized inflammation. 2 Small numbers of neurones with positive α_2A-AR immunoreactivity (α_2A-AR-IR) were detected in DRG from normal animals or contralateral to nerve lesions. In contrast, after complete or partial sciatic nerve transection the numbers of ipsilateral L₄ and L₅ DRG somata expressing α_2A-AR-IR sharply increased (>5-fold). There was no discernible change in the number of DRG neurones exhibiting α_2A-AR-IR innervating a region in association with localized chemically induced inflammation. 3 After nerve injury, double labelling with Fluoro-Gold, a marker of retrograde transport from transected fibres, or by immunoreactivity for c-jun protein, an indicator of injury and regeneration, suggested that many of the neurones expressing α_2A-AR-IR were uninjured by the sciatic lesions. 4 In general the largest proportionate increase in numbers of neurones labelled by α_2A-AR-IR after nerve lesions appeared in the medium-large diameter range (31–40 μm), a group principally composed of cell bodies of low threshold mechanoreceptors. The number of small diameter DRG neurones labelled by α_2A-AR-IR, a category likely to include somata of nociceptors, also increased but proportionately less. 5 Relatively few DRG neurones exhibited α_2C-AR-IR; this population did not appear to change after either nerve lesions or inflammation. 6 These observations are considered in relation to effects of nerve injury on excitation of primary afferent neurones by sympathetic activity or adrenergic agents, sympathetically related neuropathy and reports of sprouting of sympathetic fibres in DRG.