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首页> 外文期刊>Evidence-based complementary and alternative medicine: eCAM >A Study on the Mechanism of Cinobufagin in the Treatment of Paw Cancer Pain by Modulating Localβ-Endorphin ExpressionIn Vivo
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A Study on the Mechanism of Cinobufagin in the Treatment of Paw Cancer Pain by Modulating Localβ-Endorphin ExpressionIn Vivo

机译:Cinobufagin通过调节体内β-内啡肽表达来治疗足爪癌痛的机制研究

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Background. Cinobufagin has been widely used in the treatment of carcinoma and plays an important role in the relief of cancer pain. But the involved mechanism remains unknown.Aim. To investigate the changes in thermal and mechanical hyperalgesia in paw cancer pain in mice and the action mechanism of cinobufagin using a paw cancer pain model.Methods. 60 female mice were randomly divided into 5 groups: control group, model group, cinobufagin group, cinobufagin +NAL-M group, and morphine group; except ones in control group, mice were inoculated with H22 hepatoma cells in the right hind paw. From the 9th day after inoculation, mice were administrated drug once daily lasting for 8 days. The pain behavior was determined on the 2nd, 4th, 6th, and 8th days before and after administration. On the last day, they were sacrificed. The levels ofβ-END, CRF, and IL-1βwere analyzed by ELISA; immunohistochemistry was performed to detect the expressions ofβ-END, POMC, andμ-OR in the tumor and adjacent tissue.Results. The thresholds of thermal pain and mechanical pain were significantly increased by cinobufagin. Moreover, the expressions ofβ-END, CRF, POMC, andμ-OR were significantly upregulated by cinobufagin. The analgesic effect of cinobufagin was blocked by the peripheral opioid receptor antagonist NAL-M.Conclusions. Cinobufagin significantly relieved cancer pain in mice and raised their pain threshold, mainly upregulating the expression levels ofβ-END andμ-OR in the hind paw tumor and adjacent tissue.
机译:背景。西诺蟾蜍精已被广泛用于治疗癌症,并在缓解癌症疼痛中起重要作用。但是涉及的机制仍然未知。利用爪癌疼痛模型研究小鼠爪癌疼痛热痛觉过敏和机械痛觉过敏的变化以及西诺蟾毒的作用机制。将60只雌性小鼠随机分为5组,分别为对照组,模型组,西蟾蜍精组,西蟾蜍精+ NAL-M组和吗啡组。除对照组外,小鼠右后爪均接种了H22肝癌细胞。从接种后第9天起,每天一次给小鼠施用药物,持续8天。在给药之前和之后的第2、4、6和8天确定疼痛行为。在最后一天,他们被牺牲了。 ELISA法检测β-END,CRF和IL-1β水平。免疫组织化学法检测肿瘤及癌旁组织中β-END,POMC和μ-OR的表达。烟蟾蜍精显着增加了热痛和机械痛的阈值。此外,烟蟾蜍精显着上调了β-END,CRF,POMC和μ-OR的表达。西诺蟾蜍精的镇痛作用被外周阿片受体拮抗剂NAL-M阻断。西诺蟾蜍精能明显减轻小鼠的癌痛并提高其疼痛阈值,主要是上调后爪肿瘤及附近组织中β-END和μ-OR的表达水平。

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