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首页> 外文期刊>Insect Biochemistry and Molecular Biology >Amino acids within loops D, E and F of insect nicotinic acetylcholine receptor beta subunits influence neonicotinoid selectivity.
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Amino acids within loops D, E and F of insect nicotinic acetylcholine receptor beta subunits influence neonicotinoid selectivity.

机译:昆虫烟碱样乙酰胆碱受体β亚基的D,E和F环中的氨基酸影响新烟碱的选择性。

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摘要

Nicotinic acetylcholine (ACh) receptors (nAChRs) are ligand-gated ion channels which mediate fast cholinergic synaptic transmission in insect and vertebrate nervous systems. The nAChR agonist-binding site is present at the interface of adjacent subunits and is formed by loops A-C present in alpha subunits together with loops D-F present in either non-alpha subunits or homomer-forming alpha subunits. To investigate the mechanism of neonicotinoid selectivity, we have examined the effects of altering insect-specific loops D, E and F in hybrid nAChRs containing insect and mammalian subunits (Nlalpha1 from the brown planthopper Nilaparvata lugens and beta2 from rat). Introduction of the insect-specific loops D, E and F, singly or together, into rat beta2 subunit resulted in a leftward shift of the imidacloprid dose-response curves for nAChRs Nlalpha1-beta2 chimeras, reflecting decreases in EC(50), compared to wildtype nAChRs Nlalpha1-beta2. By contrast, the influences on ACh potency were minimal or negligible. The effects of loop D could be interpreted by the earlier findings of Shimomura et al. [2006. Role in the selectivity of neonicotinoids of insect-specific basic residues in loop D of the nicotinic acetylcholine receptor agonist-binding site. Mol. Pharmacol. 70, 1255-1263.], in which T77R and E79V were shown to be responsible for neonicotinoid selectivity. In the present study, S131Y(R) and D133N in loop E and T191W and P192K in loop F were found to contribute to the neonicotinoid selectivity of insect-specific loops E and F. These results indicated the insect-specific loops D, E and F each play important roles in neonicotinoids selectivity. This study contributes to our understanding of the molecular mechanism underlying selectivity of neonicotinoids against insects over vertebrates.
机译:烟碱乙酰胆碱(ACh)受体(nAChRs)是配体门控离子通道,可在昆虫和脊椎动物神经系统中介导快速胆碱能突触传递。 nAChR激动剂结合位点存在于相邻亚基的界面上,并由存在于α亚基中的环A-C和存在于非α亚基或形成同聚物的α亚基中的环D-F形成。为了研究新烟碱选择性的机理,我们研究了改变昆虫特异性环D,E和F在含有昆虫和哺乳动物亚基(褐飞虱Nilaparvata lugens的Nlalpha1和大鼠β2)的杂交nAChRs中的作用。将昆虫特异性环D,E和F单独或一起引入大鼠beta2亚基中导致nAChRs Nlalpha1-beta2嵌合体的吡虫啉剂量反应曲线向左移动,反映出EC(50)的减少野生型nAChRs Nlalpha1-beta2。相比之下,对ACh效力的影响微乎其微或微不足道。 Shimomura等人的早期发现可以解释D环的作用。 [2006。昆虫特异性碱性残基新烟碱在烟碱样乙酰胆碱受体激动剂结合位点环D中的作用。大声笑Pharmacol。 70,1255-1263。],其中表明T77R和E79V负责新烟碱的选择性。在本研究中,发现环E中的S131Y(R)和D133N以及环F中的T191W和P192K有助于昆虫特异性环E和F的新烟碱选择性。这些结果表明昆虫特异性环D,E和F它们各自在新烟碱选择性中起重要作用。这项研究有助于我们了解新烟碱类化合物对脊椎动物上昆虫的选择性的分子机制。

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