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由隔区损伤或慢性阿托品治疗引起的毒蕈碱超敏反应。

Muscarinic supersensitivity induced by septal lesion or chronic atropine treatment.

作者信息

Westlind A, Grynfarb M, Hedlund B, Bartfai T, Fuxe K

出版信息

Brain Res. 1981 Nov 23;225(1):131-41. doi: 10.1016/0006-8993(81)90323-1.

Abstract

Nine days after medial septal lesion a 20% increase in the number of muscarinic antagonist binding sites in rat hippocampus was observed without any change in the affinity for agonist or antagonist. Chronic atropine treatment (s.c. 5 mg/kg, twice a day for 14 days, 20 mg/kg once a day for 14 days or 100 mg/kg for 4 days and 20 mg/kg for 10 days, once daily) led to an increase in the number of muscarinic antagonist binding sites in rat hippocampus with 35, 80 and 80% respectively and also lowered the affinity for 3H-antagonists in a dose dependent manner. Agonist binding studies also indicated an increase in receptor number and a decrease in affinity. The latter change can possibly be explained by the presence of residual atropine 24 h after the last injection. If this is taken into account we may conclude that muscarinic supersensitivity evoked either by severing the input or by chronic pharmacologic blockade both produced "new receptors' with ligand binding properties similar to the original receptors.

摘要

内侧隔区损伤9天后,观察到大鼠海马中毒蕈碱拮抗剂结合位点数量增加20%,而对激动剂或拮抗剂的亲和力没有任何变化。慢性阿托品治疗(皮下注射5mg/kg,每天两次,共14天;20mg/kg,每天一次,共14天;或100mg/kg,共4天,随后20mg/kg,每天一次,共10天)导致大鼠海马中毒蕈碱拮抗剂结合位点数量分别增加35%、80%和80%,并且还以剂量依赖性方式降低了对3H-拮抗剂的亲和力。激动剂结合研究也表明受体数量增加而亲和力降低。后一种变化可能可以通过最后一次注射24小时后仍存在残留阿托品来解释。如果考虑到这一点,我们可以得出结论,无论是通过切断传入神经还是通过慢性药理阻断引起的毒蕈碱超敏反应,都会产生“新受体”,其配体结合特性与原始受体相似。

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