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SUT-8701,一种胆囊收缩素类似物,可预防大鼠基底前脑损伤后大脑皮质中的胆碱能神经变性。

SUT-8701, a cholecystokinin analog, prevents the cholinergic degeneration in the rat cerebral cortex following basal forebrain lesioning.

作者信息

Takahashi M, Sugaya K, Kojima K, Katoh T, Ueki M, Kubota K

机构信息

Area of Aging and Intractable Diseases, Science University of Tokyo, Chiba, Japan.

出版信息

Jpn J Pharmacol. 1993 Apr;61(4):341-9. doi: 10.1254/jjp.61.341.

Abstract

SUT-8701 is a cholecystokinin octapeptide (CCK8) analog and a more lipophilic peptide than CCK8. We previously demonstrated that intra-ventricularly administered CCK8 protected against the degeneration of the cholinergic neurons in the cortex of the nucleus basalis magnocellularis (nbm)-lesioned rat. We determined whether SUT-8701 and CCK8 have the ability to protect against cholinergic degeneration in the cerebral cortex of nbm-lesioned rats. Systemically administered SUT-8701 (0.1-1 micrograms/day/animal, s.c.) preserved choline acetyltransferase activity and K(+)-evoked acetylcholine release in nbm-lesioned rats. SUT-8701 was more potent than CCK8. However, SUT-8701 was much less potent than CCK8 in satiety action. The affinity of SUT-8701 to the cholecystokinin (CCK) receptors assessed by using [125I]-CCK8 was almost the same as that of CCK8 in the mouse cerebral cortex, but was 107 times less than that of CCK8 in guinea pig pancreas. These results suggest that SUT-8701 may be effective in slowing down the degenerative processes in Alzheimer's disease by preserving the integrity of cholinergic neurons in the nucleus basalis.

摘要

SUT - 8701是一种胆囊收缩素八肽(CCK8)类似物,且比CCK8具有更强的亲脂性。我们之前证明,脑室内注射CCK8可保护基底核大细胞部(nbm)损伤大鼠皮质中的胆碱能神经元免于退化。我们确定了SUT - 8701和CCK8是否有能力保护nbm损伤大鼠大脑皮质中的胆碱能神经元免于退化。全身给药SUT - 8701(0.1 - 1微克/天/动物,皮下注射)可保留nbm损伤大鼠的胆碱乙酰转移酶活性和钾离子诱发的乙酰胆碱释放。SUT - 8701比CCK8更有效。然而,SUT - 8701在饱腹感作用方面比CCK8弱得多。通过使用[125I] - CCK8评估,SUT - 8701对胆囊收缩素(CCK)受体的亲和力在小鼠大脑皮质中与CCK8几乎相同,但在豚鼠胰腺中比CCK8低107倍。这些结果表明,SUT - 8701可能通过保持基底核中胆碱能神经元的完整性,有效减缓阿尔茨海默病的退化进程。

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