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猴子在使用ABT - 418后延迟匹配样本任务表现的改善:一种用于增强记忆的新型胆碱能通道激活剂。

Improvement in performance of a delayed matching-to-sample task by monkeys following ABT-418: a novel cholinergic channel activator for memory enhancement.

作者信息

Buccafusco J J, Jackson W J, Terry A V, Marsh K C, Decker M W, Arneric S P

机构信息

Department of Pharmacology and Toxicology, Alzheimer's Research Center, Medical College of Georgia, Augusta, USA.

出版信息

Psychopharmacology (Berl). 1995 Aug;120(3):256-66. doi: 10.1007/BF02311172.

Abstract

ABT-418, a newly characterized centrally acting cholinergic channel activator (ChCA), was evaluated for its ability to improve performance in a delayed matching-to-sample (DMTS) task by mature macaques well trained in the task. Previous studies in rodents have indicated that ABT-418 shares the memory/cognitive enhancing actions of nicotine, but without many of nicotine's dose-limiting side effects. As DMTS provides a measure both of general cognitive function (the matching concept) and of recent memory, it was hypothesized that some doses of ABT-418 would enhance the monkeys' ability to correctly perform the DMTS task. Intramuscular administration of ABT-418 significantly enhanced DMTS performance at low (2-32.4 nmol/kg) doses. In fact, the drug was slightly more potent that nicotine in this regard, and all eight animals tested in this study exhibited enhanced performance at one or more doses. ABT-418 produced the greatest improvement in DMTS performance at the longest delay interval. In animals repeatedly tested with their individualized "Best Dose", DMTS performance increased on average by 10.1 +/- 3.5 percentage points correct, which was equivalent to an increase of 16.2% over baseline performance. ABT-418 did not significantly affect response times, i.e., latencies to make a choice between stimuli, or latencies to initiate new trials. Whereas nicotine enhanced DMTS performance both on the day of administration and on the following day (in the absence of drug), ABT-418-induced enhanced performance was detected only on the day of administration. Finally, single daily administration of the individualized best dose in three monkeys over a period of 8 days generally maintained enhancement of DMTS performance. Thus, the data were not consistent with the development of significant tolerance to the drug's mnemonic actions. In contrast to nicotine, no overt toxicity or side effects to acute or repeated administration of the drug were noted. Thus, ABT-418 represents a prototype of a new class of nicotinic agonists designed for the potential treatment of human dementias having a low profile of toxicity.

摘要

ABT - 418是一种新发现的中枢作用胆碱能通道激活剂(ChCA),研究人员通过对在延迟匹配样本(DMTS)任务中训练有素的成年猕猴进行测试,评估了其改善该任务表现的能力。此前对啮齿动物的研究表明,ABT - 418具有与尼古丁相同的记忆/认知增强作用,但没有尼古丁的许多剂量限制性副作用。由于DMTS既可以衡量一般认知功能(匹配概念),也可以衡量近期记忆,因此推测某些剂量的ABT - 418会提高猴子正确完成DMTS任务的能力。肌肉注射ABT - 418在低剂量(2 - 32.4 nmol/kg)时能显著提高DMTS表现。事实上,在这方面该药物比尼古丁的效力略强,本研究中测试的所有八只动物在一个或多个剂量下表现均有所提高。ABT - 418在最长延迟间隔时对DMTS表现的改善最大。在用各自的“最佳剂量”反复测试的动物中,DMTS表现平均正确提高了10.1±3.5个百分点,相当于比基线表现提高了16.2%。ABT - 418对反应时间没有显著影响,即在刺激之间做出选择的潜伏期或开始新试验的潜伏期。尼古丁在给药当天和第二天(无药物时)均能提高DMTS表现,而ABT - 418诱导的表现提高仅在给药当天被检测到。最后,在八天的时间里对三只猴子每日单次给予个体化最佳剂量,总体上维持了DMTS表现的提高。因此,数据与对该药物记忆作用产生显著耐受性的情况不一致。与尼古丁不同,未观察到该药物急性或反复给药的明显毒性或副作用。因此,ABT - 418代表了一类新型烟碱激动剂的原型,这类激动剂专为潜在治疗低毒性的人类痴呆症而设计。

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