2011
DOI: 10.1074/jbc.m111.262014
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Additional Acetylcholine (ACh) Binding Site at α4/α4 Interface of (α4β2)2α4 Nicotinic Receptor Influences Agonist Sensitivity

Abstract: Nicotinic acetylcholine receptor (nAChR) ␣4 and ␤2 subunits assemble in two alternate stoichiometries to produce (␣4␤2) 2 ␣4 and (␣4␤2) 2 ␤2, which display different agonist sensitivities. Functionally relevant agonist binding sites are thought to be located at ␣4(؉)/␤2(؊) subunit interfaces, but because these interfaces are present in both receptor isoforms, it is unlikely that they account for differences in agonist sensitivities. In contrast, incorporation of either ␣4 or ␤2 as auxiliary subunits produces i… Show more

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Cited by 117 publications
(217 citation statements)
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“…The biphasic effect arises from the high and low sensitivity component. The high sensitivity component is appointed to the unaltered α2(+)/β2(−) interfaces, whereas the low sensitivity component is due to the impaired α2(+)/α2(−) interface (29). To the contrary, this mutation had no effect on either the EC 50 or the desensitization kinetics of the α2 W84A β2 HS subtype compared with the WT HS receptor (Tables S2 and S3 and Fig.…”
Section: Resultsmentioning
confidence: 76%
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“…The biphasic effect arises from the high and low sensitivity component. The high sensitivity component is appointed to the unaltered α2(+)/β2(−) interfaces, whereas the low sensitivity component is due to the impaired α2(+)/α2(−) interface (29). To the contrary, this mutation had no effect on either the EC 50 or the desensitization kinetics of the α2 W84A β2 HS subtype compared with the WT HS receptor (Tables S2 and S3 and Fig.…”
Section: Resultsmentioning
confidence: 76%
“…For that reason, we constructed the α2 mutant W84A and coexpressed it in Xenopus oocytes with the β2 WT nAChR subunit in 10:1 or in 1:10 RNA ratios, thus expressing solely the LS or the HS subtype, respectively (27). Trp84 is a highly conserved residue on the complementary side of the ligand binding site that in the α2-Epi structure was found to interact with the ligand directly and its role in the binding site of other nAChRs has been evaluated in numerous studies (29,39,40) (Fig. 4 A and B).…”
Section: Resultsmentioning
confidence: 99%
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“…4 G and H, Right). Notably, previous studies show that expressing the heteromeric α4β2 nAChR under conditions that favor an (α4β2) 2 α4 stoichiometry (three α4 and two β2 subunits) results in a receptor having two α4(+)/β2(−) interfaces with high agonist sensitivity and a third binding site at the α4(+)/α4(−) interface that displays low agonist sensitivity (59)(60)(61).…”
Section: Discussionmentioning
confidence: 99%
“…This is reflected by the biphasic ACh concentration-response curves in in vitro assays at cells expressing a heterogeneous population of a4b2 nAChRs [13][14][15][16]. The lower ACh sensitivity of the LS receptor is believed to arise from a recently discovered low-sensitivity ACh binding site located in the a4/a4 interface only present in this stoichiometry [17,18]. Intriguingly, the high-and low-sensitive ACh binding sites in the LS receptor display differential responses to various nAChR ligands [19][20][21].…”
Section: Molecular Aspects Of Nachrsmentioning
confidence: 99%