4.6 Article

Effect of Intrahippocampal Administration of α7 Subtype Nicotinic Receptor Agonist PNU-282987 and Its Solvent Dimethyl Sulfoxide on the Efficiency of Hypoxic Preconditioning in Rats

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MOLECULES
卷 26, 期 23, 页码 -

出版社

MDPI
DOI: 10.3390/molecules26237387

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hypoxic preconditioning; hippocampus; CA1 area; intrahippocampal injections; nicotinic alpha 7 receptors (alpha 7nAChRs); PNU-282987 (PNU); dimethyl sulfoxide (DMSO)

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  1. Institute of General Pathology and Pathophysiology

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The study confirms the key role of the hippocampus in the mechanism of hypoxic preconditioning, as well as the importance of alpha 7nAChR activation in hypoxic preconditioning. It was found in the experiment that the activation of alpha 7nAChRs is not involved in the cholinergic signaling initiated by HBH or DMSO via any route of administration.
We have previously suggested a key role of the hippocampus in the preconditioning action of moderate hypobaric hypoxia (HBH). The preconditioning efficiency of HBH is associated with acoustic startle prepulse inhibition (PPI). In rats with PPI > 40%, HBH activates the cholinergic projections of hippocampus, and PNU-282987, a selective agonist of alpha 7 nicotinic receptors (alpha 7nAChRs), reduces the HBH efficiency and potentiating effect on HBH of its solvent dimethyl sulfoxide (DMSO, anticholinesterase agent) when administered intraperitoneally. In order to validate the hippocampus as a key structure in the mechanism of hypoxic preconditioning and research a significance of alpha 7nAChR activation in the hypoxic preconditioning, we performed an in vivo pharmacological study of intrahippocampal injections of PNU-282987 into the CA1 area on HBH efficiency in rats with PPI & GE; 40%. We found that PNU-282987 (30 mu M) reduced HBH efficiency as with intraperitoneal administration, while DMSO (0.05%) still potentiated this effect. Thus, direct evidence of the key role of the hippocampus in the preconditioning effect of HBH and some details of this mechanism were obtained in rats with PPI & GE; 40%. The activation of alpha 7nAChRs is not involved in the cholinergic signaling initiated by HBH or DMSO via any route of administration. Possible ways of the potentiating action of DMSO on HBH efficiency and its dependence on alpha 7nAChRs are discussed.

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