Aldrich Jane V, Patkar Kshitij A, McLaughlin Jay P
Department of Medicinal Chemistry, University of Kansas, Lawrence, KS 66045, USA.
Proc Natl Acad Sci U S A. 2009 Oct 27;106(43):18396-401. doi: 10.1073/pnas.0910180106. Epub 2009 Oct 19.
The cyclic peptide zyklophin {[N-benzylTyr(1),cyclo(D-Asp(5),Dap(8))-dynorphin A-(1-11)NH(2), Patkar KA, et al. (2005) J Med Chem 48: 4500-4503} is a selective peptide kappa opioid receptor (KOR) antagonist that shows activity following systemic administration. Systemic (1-3 mg/kg s.c.) as well as central (0.3-3 nmol intracerebroventricular, i.c.v.) administration of this peptide dose-dependently antagonizes the antinociception induced by the selective KOR agonist U50,488 in C57BL/6J mice tested in the 55 degrees C warm water tail withdrawal assay. Zyklophin administration had no effect on morphine- or SNC-80-mediated antinociception, suggesting that zyklophin selectively antagonizes KOR in vivo. Additionally, the antagonism of antinociception induced by centrally (i.c.v.) administered U50,488 following peripheral administration of zyklophin strongly suggests that the peptide crosses the blood-brain barrier to antagonize KOR in the CNS. Most importantly, the antagonist activity of zyklophin (3 mg/kg s.c.) lasts less than 12 h, which contrasts sharply with the exceptionally long duration of antagonism reported for the established small-molecule selective KOR antagonists such as nor-binaltorphimine (nor-BNI) that last weeks after a single administration. Systemically administered zyklophin (3 mg/kg s.c.) also prevented stress-induced reinstatement of cocaine-seeking behavior in a conditioned place preference assay. In conclusion, the peptide zyklophin is a KOR-selective antagonist that exhibits the desired shorter duration of action, and represents a significant advance in the development of KOR-selective antagonists.
环肽齐考诺肽{[N-苄基酪氨酸(1),环(D-天冬氨酸(5),二氨基丙烷(8))-强啡肽A-(1-11)NH₂,帕特卡尔·K·A等人(2005年)《药物化学杂志》48卷:4500 - 4503页]}是一种选择性肽κ阿片受体(KOR)拮抗剂,全身给药后显示出活性。在55℃温水甩尾试验中对C57BL/6J小鼠进行测试时,该肽全身(1 - 3毫克/千克皮下注射)以及中枢(0.3 - 3纳摩尔脑室内注射,i.c.v.)给药均剂量依赖性地拮抗选择性KOR激动剂U50,488诱导的抗伤害感受。齐考诺肽给药对吗啡或SNC - 80介导的抗伤害感受没有影响,这表明齐考诺肽在体内选择性拮抗KOR。此外,在外周给予齐考诺肽后,对中枢(i.c.v.)给予U50,488诱导的抗伤害感受的拮抗作用强烈表明该肽可穿过血脑屏障以拮抗中枢神经系统中的KOR。最重要的是,齐考诺肽(3毫克/千克皮下注射)的拮抗剂活性持续时间不到12小时,这与已确立的小分子选择性KOR拮抗剂如去甲纳曲酮(nor - BNI)单次给药后持续数周的异常长的拮抗持续时间形成鲜明对比。在条件性位置偏爱试验中,全身给予齐考诺肽(3毫克/千克皮下注射)还可预防应激诱导的可卡因觅药行为的恢复。总之,肽齐考诺肽是一种KOR选择性拮抗剂,具有所需的较短作用持续时间,代表了KOR选择性拮抗剂开发方面的重大进展。