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吗啡-3-葡萄糖醛酸苷:支持其在大鼠对吗啡镇痛作用产生耐受性过程中假定作用的证据。

Morphine-3-glucuronide: evidence to support its putative role in the development of tolerance to the antinociceptive effects of morphine in the rat.

作者信息

Smith Gregg D, Smith Maree T

机构信息

Department of Pharmacy, The University of Queensland, Brisbane, Queensland 4072, Australia.

出版信息

Pain. 1995 Jul;62(1):51-60. doi: 10.1016/0304-3959(94)00228-7.

Abstract

Antinociceptive tolerance to morphine (MOR) was induced in groups of Sprague-Dawley rats receiving continuous intravenous infusions of morphine sulphate administered by 3 different MOR dosing regimes. At appropriate intervals throughout each infusion period, antinociceptive testing was performed using the tail-flick latency test and blood samples were collected. Groups of saline (SAL)-infused control rats also underwent antinociceptive testing and blood sample collection. Complete antinociceptive tolerance developed during each MOR infusion period and was characterized by a marked decline in the degree of antinociception from values greater than 90% of the maximum possible effect (%MPE) to pre-dosing baseline values. By contrast, %MPE values in SAL-infused control animals and in sham-operated rats were not significantly different from pre-dosing values throughout the infusion period, indicating that the experimental procedures themselves did not contribute to the development of antinociceptive tolerance to MOR. In addition, the rate of MOR tolerance development was inversely proportional to the MOR infusion rate. A very significant inverse relationship was observed between the mean degree of antinociception (%MPE) and the mean plasma molar concentration ratio, [morphine-3-glucuronide]/[MOR], for each of the 3 MOR dosing regimes and for the cumulated data. This relationship showed that near-maximum antinociception was attainable at ratio values less than approximately 0.50, whilst at ratio values above approximately 1.5, little or no antinociception was observed. Although %MPE was highly inversely correlated with the mean plasma morphine-3-glucuronide (M3G) concentrations for rats receiving regimes A and B, this was not the case for rats receiving regime C where antinociceptive tolerance was partially reversed by an increase in the morphine infusion rate part-way through the infusion period. In addition, a poor relationship was observed between %MPE and the mean plasma MOR concentration, possibly due to the confounding presence of M3G in all samples. Thus, we may conclude from this study in Sprague-Dawley rats that irrespective of the rate of antinociceptive tolerance development, the level of antinociception achievable appears to be highly inversely correlated with the mean [M3G]/[MOR] plasma molar concentration ratio and poorly correlated with the plasma MOR concentration, consistent with the notion that it is perhaps the balance between the excitatory effects of M3G and the inhibitory effects of MOR at the functional level which is the important determinant. Further research is required in carefully conducted studies in cancer patients to evaluate the possible contribution of the MOR metabolites, M3G and morphine-6-glucuronide (MbG), to increasing dosing requirements of MOR.(ABSTRACT TRUNCATED AT 400 WORDS)

摘要

对接受3种不同吗啡给药方案持续静脉输注硫酸吗啡的斯普拉格-道利大鼠组诱导了对吗啡(MOR)的抗伤害感受耐受性。在每个输注期的适当间隔,使用甩尾潜伏期试验进行抗伤害感受测试并采集血样。输注生理盐水(SAL)的对照大鼠组也进行了抗伤害感受测试和血样采集。在每个吗啡输注期均出现了完全的抗伤害感受耐受性,其特征是抗伤害感受程度从大于最大可能效应的90%(%MPE)显著下降至给药前基线值。相比之下,在整个输注期,输注生理盐水的对照动物和假手术大鼠的%MPE值与给药前值无显著差异,表明实验程序本身并未导致对吗啡的抗伤害感受耐受性的发展。此外,吗啡耐受性的发展速率与吗啡输注速率成反比。在3种吗啡给药方案中的每一种以及累积数据中,均观察到抗伤害感受的平均程度(%MPE)与平均血浆摩尔浓度比[吗啡-3-葡萄糖醛酸苷]/[MOR]之间存在非常显著的负相关关系。这种关系表明,在比值小于约0.50时可达到接近最大的抗伤害感受,而在比值高于约1.5时,几乎未观察到抗伤害感受。尽管对于接受方案A和B的大鼠,%MPE与平均血浆吗啡-3-葡萄糖醛酸苷(M3G)浓度高度负相关,但对于接受方案C的大鼠并非如此,在方案C中,在输注期中途通过增加吗啡输注速率部分逆转了抗伤害感受耐受性。此外,观察到%MPE与平均血浆MOR浓度之间的关系不佳,这可能是由于所有样本中均存在M3G的干扰。因此,从这项对斯普拉格-道利大鼠的研究中我们可以得出结论,无论抗伤害感受耐受性的发展速率如何,可达到的抗伤害感受水平似乎与平均[M3G]/[MOR]血浆摩尔浓度比高度负相关,与血浆MOR浓度相关性较差,这与以下观点一致,即在功能水平上,可能是M3G的兴奋作用与MOR的抑制作用之间的平衡是重要的决定因素。需要在精心开展的癌症患者研究中进行进一步研究,以评估MOR代谢物M3G和吗啡-6-葡萄糖醛酸苷(MbG)对增加MOR给药需求的可能贡献。(摘要截短至400字)

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