Adrenomedullary chromaffin cells express at least two subtypes of acetylcholine nicotinic receptors, which differ in their sensitivity to the snake toxin α-bungarotoxin. One subtype is involved in the activation step of the catecholamine secretion process and is not blocked by the toxin. The other is α-bungarotoxin-sensitive, and its functional role has not yet been defined. The α7 subunit is a component of this subtype. Autoradiography of bovine adrenal gland slices with α-bungarotoxin indicates that these receptors are restricted to medullary areas adjacent to the adrenal cortex and colocalize with the enzyme phenylethanolamine N-methyl transferase (PNMT), which confers the adrenergic phenotype to chromaffin cells. Transcripts corresponding to the α7 subunit also are localized exclusively to adrenergic cells. To identify possible transcriptional regulatory elements of the α7 subunit gene involved in the restricted expression of nicotinic receptors, we isolated and characterized its 5' flanking region, revealing putative binding sites for the immediate early gene transcription factor Egr- 1, which is known to activate PNMT expression. In reporter gene transfection experiments, Egr-1 increased α7 promoter activity by up to sevenfold. Activation was abolished when the most promoter-proximal of the Egr-1 sites was mutated, whereas modification of a close upstream site produced a partial decrease of the Egr-1 response. Because Egr-1 was found to be expressed exclusively in adrenergic cells, we suggest that this transcription factor may be part of a common mechanism involved in the induction of the adrenergic phenotype and the differential expression of α-bungarotoxin-sensitive nicotinic receptors in the adrenal gland.
CITATION STYLE
Criado, M., Toro, E. D. D., Carrasco-Serrano, C., Smillie, F. I., Juíz, J. M., Viniegra, S., & Ballesta, J. J. (1997). Differential expression of α-bungarotoxin-sensitive neuronal nicotinic receptors in adrenergic chromaffin cells: A role for transcription factor Egr-1. Journal of Neuroscience, 17(17), 6554–6564. https://doi.org/10.1523/jneurosci.17-17-06554.1997
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