Pyritinol facilitates the recovery of cortical cholinergic deficits caused by nucleus basalis lesions.

A Toledano, M L Bentura
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引用次数: 13

Abstract

The effect of a nootropic, Pyritinol, on the recovery of cortical cholinergic deficits induced by injury of the nucleus basalis has been tested on two groups of unilateral quisqualic acid nbM-lesioned rats. The first group had a 30 nmol lesion producing a cortical cholinergic impairment at 21 days, with a spontaneous recovery at 45 days. The second group had a 50 nmol lesion that produced a deeper cholinergic deficit, which did not recover at 45 days. Pyritinol enhanced the recovery in the 30 nmol group of animals on the 21st day after surgery. The recovery was measured as an increase in the activities of acetylcholinesterase (AChE), choline acetyltransferase (ChAT) and the high affinity choline uptake system, and the histochemical densities of the cortical AChE network and the M2 receptor. Histochemical analysis of the nbM enabled cortical recovery to be related to the number of surviving neurons and also to their hypertrophy and AChE-ChAT hyperactivity. Pyritinol enhanced recovery in 30 nmol lesioned animals but in the other group, with a lower number of surviving neurons and a lower ability of the cells to become hypertrophic, the drug was unable to promote cortical recovery.

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吡啶醇促进基底核损伤引起的皮质胆碱能缺陷的恢复。
在两组单侧准质酸nbm损伤大鼠身上,研究了益智药吡啶醇对基底核损伤引起的皮质胆碱能缺损的恢复作用。第一组有30 nmol的损伤,在21天产生皮质胆碱能损伤,在45天自然恢复。第二组有50 nmol的损伤,产生更深的胆碱能缺陷,在45天没有恢复。30 nmol吡啶醇组动物术后第21天恢复较好。恢复测量为乙酰胆碱酯酶(AChE)、胆碱乙酰转移酶(ChAT)和高亲和力胆碱摄取系统活性的增加,以及皮质AChE网络和M2受体的组织化学密度的增加。nbM的组织化学分析表明,皮层恢复与存活神经元的数量有关,也与它们的肥大和AChE-ChAT多动有关。Pyritinol促进了30只nmol损伤动物的恢复,但在另一组中,由于存活神经元数量较少,细胞变得肥大的能力较低,该药物无法促进皮质恢复。
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