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Involvement of matrix metalloproteinase-9 in the development of morphine tolerance

机译:基质金属蛋白酶9参与吗啡耐受性的发展

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Matrix metalloproteinase-9 (MMP-9) is involved in tissue remodeling or neural plasticity in various clinical states (e.g. inflammation, neuropathic pain). We focused on the effect of MMP-9 on development of morphine tolerance after repeated morphine treatment. To develop morphine tolerance, mice were given morphine (10 mg/kg; s.c.) once daily for 5 days. The antinociceptive effect of morphine was measured by the tail flick method. Development of morphine tolerance was significantly inhibited by daily treatment of the non-specific MMP inhibitor GM6001 (5 μg/mouse, i.c.v.). A MMP-9 inhibitor (5 μg/mouse, i.c.v.) partially, yet significantly, inhibited the development of morphine tolerance. Intrathecal treatment of a MMP-9 inhibitor did not affect morphine tolerance. In MMP-9 (-/-) mice, the development of morphine tolerance was partially, yet significantly, inhibited compared with wild-type mice. MMP-9 protein expression levels in the midbrain gradually increased 12 h to 24 h after morphine treatment on day 1, but were unchanged on days 3-5. In the spinal cord, MMP-9 protein expression levels were unchanged. In gelatin zymography analyses, MMP-9 activity in the midbrain gradually increased 12 to 24 h after morphine treatment. Increment in MMP-9 activity in the midbrain was also observed on days 3-5. Our findings suggest that persistent MMP-9 activation observed after the transient increment in MMP-9 expression from the early phase of morphine treatment may contribute to the development of morphine tolerance.
机译:基质金属蛋白酶9(MMP-9)在各种临床状态(例如炎症,神经性疼痛)中参与组织重塑或神经可塑性。我们重点研究了MMP-9对吗啡反复治疗后对吗啡耐受性的影响。为了发展对吗啡的耐受性,每天一次给予小鼠吗啡(10 mg / kg; s.c.),持续5天。通过甩尾法测定吗啡的抗伤害感受作用。非特异性MMP抑制剂GM6001的每日治疗(5μg/小鼠,i.c.v.)显着抑制了吗啡耐受性的发展。 MMP-9抑制剂(5μg/小鼠,静脉内)部分但仍显着抑制吗啡耐受性的发展。鞘内注射MMP-9抑制剂不影响吗啡耐受性。在MMP-9(-/-)小鼠中,与野生型小鼠相比,吗啡耐受性的发展受到了部分(但显着)抑制。吗啡治疗后第1天,中脑中MMP-9蛋白表达水平在12h至24h逐渐增加,但在3-5天没有变化。在脊髓中,MMP-9蛋白表达水平未改变。在明胶酶谱分析中,吗啡处理后12至24小时,中脑MMP-9活性逐渐增加。在第3-5天也观察到中脑中MMP-9活性的增加。我们的发现表明,从吗啡治疗的早期开始,MMP-9表达瞬时增加后观察到的持久性MMP-9激活可能有助于吗啡耐受性的发展。

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