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Article

Shared Long-Range Regulatory Elements Coordinate Expression of a Gene Cluster Encoding Nicotinic Receptor Heteromeric Subtypes

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Pages 5636-5649 | Received 15 Mar 2006, Accepted 13 May 2006, Published online: 27 Mar 2023
 

Abstract

The nicotinic acetylcholine receptor (nAChR) β4/α3/α5 gene cluster encodes several heteromeric transmitter receptor subtypes that are essential for cholinergic synaptic transmission in adrenal gland, autonomic ganglia, pineal gland, and several nuclei in the central nervous system. However, the transcriptional mechanisms coordinating expression of these subunit genes in different cell populations are unknown. Here, we used transgenic methods to investigate long-range transcriptional control of the cluster. A 132-kb P1-derived artificial chromosome (PAC) encoding the rat cluster recapitulated the neurally- and endocrine-restricted expression patterns of the endogenous β4/α3/α5 genes. Mutation of ETS factor binding sites in an enhancer, β43′, embedded in the β4 3′-untranslated exon resulted in greatly diminished β4, α3, and α5 expression in adrenal gland and to a lesser extent in the superior cervical ganglion (SCG) but not in other tissues. Phylogenetic sequence analyses revealed several conserved noncoding regions (CNRs) upstream of β4 and α5. Deletion of one of them (CNR4) located 20 kb upstream of β4 resulted in a dramatic decrease in β4 and α3 expression in the pineal gland and SCG. CNR4 was sufficient to direct LacZ transgene expression to SCG neurons, which express the endogenous β4α3α5 subunits, and pineal cells, which express the endogenous β4α3 combination. Finally, CNR4 was able to direct transgene expression to major sites of expression of the endogenous cluster in the brain. Together, our findings support a model in which cell type-specific shared long-range regulatory elements are required for coordinate expression of clustered nAChR genes.

Supplemental material for this article may be found at http:://mcb.asm.org/.

We thank Neal Copeland for the EL250 bacterial strain. We thank Richard Zigmond for important comments on the final draft.

This work was supported by Public Health Service grant R01NS29123 from the NINDS.

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