Bigge C F, Malone T C, Hays S J, Johnson G, Novak P M, Lescosky L J, Retz D M, Ortwine D F, Probert A W, Coughenour L L
Department of Chemistry, Parke-Davis Pharmaceutical Research Division, Warner-Lambert Company, Ann Arbor, Michigan 48105.
J Med Chem. 1993 Jul 9;36(14):1977-95. doi: 10.1021/jm00066a007.
A novel series of octahydrophenanthrenamines and their heterocyclic analogues have been synthesized as potential noncompetitive antagonists of the N-methyl-D-aspartate (NMDA) receptor complex. The compounds were evaluated for their affinity at the phencyclidine (PCP) binding site by determining their ability to displace [3H]TCP from crude rat brain synaptic membranes. A wide range of affinities were observed, with the most potent analogs possessing IC50's equivalent to that of the reference agent MK-801 (3, dizocilpine). NMDA antagonist activity was demonstrated by prevention of glutamate-induced accumulation of [45Ca2+] in cultured rat cortical neurons. Selected compounds were also studied in vivo to determine their ability to prevent the lethal effects of systemically injected NMDA in the mouse. In general, the SAR of the phenanthrenamine series may be summarized as follows: (a) for the amino group at C4a, NHMe > NH2 > NHEt >> NC5H10; (b) for the B-ring substitution, X = CH2 > S > O; (c) unsaturation of the C ring decreases receptor affinity; (d) cis-ring fusion between the B and C rings is desirable; (e) 6-hydroxy or 6-methoxy substitution of the phenanthrenamine system identified an additional hydrogen bonding interaction that substantially increased receptor affinity; (f) spiro analogues (such as 55, IC50 = 3400 nM), which altered the point of attachment of the C ring, caused a substantial reduction in PCP-site affinity. Molecules from this series were useful for refining a pharmacophore model consistent with previous models of the PCP site. In this model, the (R)-(+)-phenanthrenamine 13 superimposes closely onto MK-801 (3), and the angular 4a-amino group is believed to hydrogen bond with a putative receptor site atom. In the phenanthrenamine and thiaphenanthrenamine series, the (R)-(+)-enantiomers (9, 13, and 44) are more potent by approximately 5-10-fold than their corresponding (S)-(-)-enantiomers with respect to their affinity for the PCP site, their ability to prevent accumulation of [45Ca2+] in cultured neuronal cells, and their protection against the lethal effects of NMDA in mice. In general, there was no separation between the dose that prevented NMDA lethality and the dose that produced ataxia in mice, except in the case of the thiaphenanthrenamines 41 and 43. We have not yet obtained evidence that this small separation in activity offers a therapeutic advantage in the treatment of cerebral ischemia or other neurodegenerative disorders.
已合成了一系列新型八氢菲胺及其杂环类似物,作为N-甲基-D-天冬氨酸(NMDA)受体复合物潜在的非竞争性拮抗剂。通过测定化合物从大鼠脑粗制突触膜中置换[3H]TCP的能力,评估它们在苯环利定(PCP)结合位点的亲和力。观察到了广泛的亲和力范围,最有效的类似物的IC50与参考药物MK-801(3,地佐环平)相当。通过预防谷氨酸诱导的培养大鼠皮层神经元中[45Ca2+]的积累,证明了NMDA拮抗剂活性。还对选定的化合物进行了体内研究,以确定它们预防小鼠全身注射NMDA致死效应的能力。一般来说,菲胺系列的构效关系可总结如下:(a)对于C4a位的氨基,NHMe > NH2 > NHEt >> NC5H10;(b)对于B环取代,X = CH2 > S > O;(c)C环的不饱和降低受体亲和力;(d)B环和C环之间的顺式环稠合是有利的;(e)菲胺体系的6-羟基或6-甲氧基取代确定了一种额外的氢键相互作用,该相互作用显著增加了受体亲和力;(f)螺环类似物(如55,IC50 = 3400 nM),其改变了C环的连接点,导致PCP位点亲和力大幅降低。该系列分子有助于完善与先前PCP位点模型一致的药效团模型。在该模型中,(R)-(+)-菲胺13与MK-801(3)紧密重叠,并且角形4a-氨基被认为与假定的受体位点原子形成氢键。在菲胺和硫代菲胺系列中,(R)-(+)-对映体(9、13和44)在对PCP位点的亲和力、预防培养神经元细胞中[45Ca2+]积累的能力以及对小鼠NMDA致死效应的保护方面,比其相应的(S)-(-)-对映体强约5-10倍。一般来说,除了硫代菲胺41和43的情况外,预防NMDA致死的剂量与在小鼠中产生共济失调的剂量之间没有区别。我们尚未获得证据表明这种活性上的微小差异在治疗脑缺血或其他神经退行性疾病方面具有治疗优势。
