Immunohistochemical study of opioid receptors after chronic morphine treatment in rats.

P L Tao, H S Niu, W M Lue, S D Wang
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Abstract

Previously, we have used the biochemical receptor binding method to investigate whether down-regulation of the opioid receptor is a mechanism for morphine tolerance, and we were led to a negative conclusion. In the current study, we further used immunohistochemistry to reinvestigate this issue. Male Sprague-Dawley rats (250-300 g) were chronically treated with morphine s.c. for 2, 4 or 6 days, using an escalating dosage paradigm (5-45 mg), which resulted in a 1.8 to 4.0-fold increase in AD50. Rat brains were removed, frozen, coronally sectioned (14 microm) and processed for mu- or delta-opioid receptor immunohistochemistry using the Avidin-Biotin Complex (ABC) method. No significant decrease in mu-opioid receptor (MOR) immunodensity was found in most of the brain regions, which were enriched with MOR after chronic treatment with morphine except for the anteroventral thalamic nucleus in the ventrolateral part (AVVL). No significant change in delta-opioid receptor (DOR) immunodensity after chronic treatment with morphine was found either. Therefore, our conclusion is that down regulation of opioid receptors may not be an important mechanism for morphine tolerance.

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大鼠慢性吗啡治疗后阿片受体的免疫组化研究。
此前,我们利用生化受体结合的方法研究阿片受体下调是否为吗啡耐受的机制,结果均为阴性结论。在本研究中,我们进一步利用免疫组织化学对这一问题进行了重新研究。雄性Sprague-Dawley大鼠(250-300 g)长期使用吗啡s.c.治疗2、4或6天,使用递增剂量模式(5-45 mg),导致AD50增加1.8 - 4.0倍。取大鼠脑,冷冻,冠状切片(14微米),用Avidin-Biotin Complex (ABC)法进行mu或delta阿片受体免疫组织化学处理。除腹侧丘脑前腹侧核(AVVL)外,经吗啡慢性治疗后,大部分脑区均出现了MOR的富集。慢性吗啡治疗后,δ -阿片受体(DOR)免疫密度也未见明显变化。因此,我们的结论是,阿片受体的下调可能不是吗啡耐受的重要机制。
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