CI-1017, a functionally M1-selective muscarinic agonist: design, synthesis, and preclinical pharmacology

H Tecle, R.D Schwarz, S.D Barrett, M.J Callahan, B.W Caprathe, R.E Davis, P Doyle, M Emmerling, D.J Lauffer, T Mirzadegan, D.W Moreland, W Lipiniski, C Nelson, C Raby, C Spencer, K Spiegel, A.J Thomas, J.C Jaen
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引用次数: 12

Abstract

The five muscarinic receptor subtypes (M1–M5) are characterized by seven helices that define a transmembrane cavity which serves as the binding pocket for agonists and antagonists. The five cavities appear to be topographically different enough to permit subtype selectivity among antagonists but not among classical agonists which tend to be smaller in size than antagonists. It was reasoned that synthesis of muscarinic agonists longer/larger than their classical counterparts might result in subtype selectivity. M1 subtype selectivity was found in a class of 1-azabicyclo[2.2.1]heptan-3-one, O-(3-aryl-2-propynyl) oximes. One of these, CI-1017, improved spatial memory of hippocampally deficient mice and nbM-lesioned rats at doses of 1.0–3.2 and 0.1–0.3 mg/kg, respectively, while producing parasympathetic side effects only at very high doses (100–178 mg/kg). Additionally, CI-1017 inhibited production of amyloidogenic Aβ and increased secretion of soluble APP. Thus, CI-1017, besides treating AD symptomatically, may also retard its progression. CI-1017 has recently completed phase I clinical trials.

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一种功能性m1选择性毒蕈碱激动剂CI-1017:设计、合成和临床前药理学
毒蕈碱受体的五种亚型(M1-M5)具有7个螺旋的特征,这些螺旋定义了一个跨膜腔,作为激动剂和拮抗剂的结合袋。这五种空腔似乎在地形上不同,足以允许拮抗剂之间的亚型选择性,但在传统激动剂之间却没有,因为它们的大小往往比拮抗剂小。认为合成比传统的毒蕈碱激动剂更长/更大的激动剂可能导致亚型选择性。在一类1-氮杂环[2.2.1]庚烷-3- 1,O-(3-芳基-2-丙基)肟中发现M1亚型选择性。其中,CI-1017分别在1.0-3.2 mg/kg和0.1-0.3 mg/kg剂量下改善了海马缺陷小鼠和nbn损伤大鼠的空间记忆,而只有在非常高剂量(100-178 mg/kg)时才产生副交感神经副作用。此外,CI-1017抑制淀粉样蛋白Aβ的产生,增加可溶性APP的分泌。因此,CI-1017除了对症治疗阿尔茨海默病外,还可能延缓其进展。CI-1017最近完成了I期临床试验。
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