Garzón J, Sánchez-Blázquez P
Neuropharmacology, Cajal Institute, C.S.I.C., Madrid, Spain.
Life Sci. 1995;56(14):PL237-42. doi: 10.1016/0024-3205(95)00064-d.
The intracerebroventricular (i.c.v.) injection to mice of a polyclonal antibody raised against the peptide sequence 208-216 (TKYRQGSID) of cloned rat mu opioid receptor, reduced the analgesic potency of DAMGO, morphine and beta-endorphin-(1-31) when studied 48 h later in the tail-flick test. Antinociception elicited by delta agonists, DPDPE and [D-Ala2]-Deltorphin II, and by the kappa agonist U-50488H, was fully expressed in mice undergoing this treatment. The specific binding displayed by 0.6 nM [3H]-DAMGO was reduced in membranes preincubated with the antiserum, whereas no change could be detected for 3 nM [3H]-DPDPE or 2 nM [3H]-U-69593 labelling delta and kappa opioid receptors respectively. Naloxonazine, irreversible antagonist of the pharmacologically defined mu 1 opioid receptor, and beta-funaltrexamine (beta-FNA), that also displays irreversible antagonism at mu 1/2 receptors, when injected i.c.v. 24 h before the opioids significantly reduced the activity of DAMGO and morphine. In mice treated with naloxonazine, but not with beta-FNA, the antibody further reduced the remaining analgesic effect of DAMGO and morphine. Thus, both the antibody and beta-FNA blocked a wider population of mu opioid receptors than that tagged by naloxonazine.
向小鼠脑室内(i.c.v.)注射针对克隆大鼠μ阿片受体肽序列208 - 216(TKYRQGSID)产生的多克隆抗体,在48小时后进行甩尾试验研究时,降低了DAMGO、吗啡和β - 内啡肽 -(1 - 31)的镇痛效力。δ激动剂DPDPE和[D - Ala2]-Deltorphin II以及κ激动剂U - 50488H引起的抗伤害感受在接受该处理的小鼠中充分表现。用抗血清预孵育的膜中,0.6 nM [3H]-DAMGO显示的特异性结合减少,而分别标记δ和κ阿片受体的3 nM [3H]-DPDPE或2 nM [3H]-U - 69593的结合未检测到变化。纳洛酮嗪是药理学定义的μ1阿片受体的不可逆拮抗剂,β - 氟纳曲明(β - FNA)在μ1/2受体也表现出不可逆拮抗作用,在给予阿片类药物前24小时脑室内注射时,显著降低了DAMGO和吗啡的活性。在用纳洛酮嗪而非β - FNA处理的小鼠中,抗体进一步降低了DAMGO和吗啡剩余的镇痛作用。因此,抗体和β - FNA阻断的μ阿片受体群体比纳洛酮嗪标记的更广泛。
