首页> 外文期刊>The journal of pain: official journal of the American Pain Society >Analgesic efficacy of bradykinin B1 antagonists in a murine bone cancer pain model.
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Analgesic efficacy of bradykinin B1 antagonists in a murine bone cancer pain model.

机译:缓激肽B1拮抗剂在小鼠骨癌疼痛模型中的镇痛效果。

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Cancer pain is a significant clinical problem because it is the first symptom of disease in 20% to 50% of all cancer patients, and 75% to 90% of patients with advanced or terminal cancer must cope with chronic pain syndromes related to failed treatment and/or tumor progression. One of the most difficult to treat cancer pains is metastatic invasion of the skeleton that can generate ongoing and bone breakthrough pain, which represents one of the most debilitating cancer-related events. Because bradykinin has been shown to be released in response to tissue injury and plays a significant role in driving acute and chronic inflammatory pain, we focused on bradykinin antagonists in a model of bone cancer pain. In our model of bone cancer, which involves the injection and confinement of 2472 sarcoma cells to the mouse femur, pharmacologic blockade of the bradykinin B1 receptor is effective in reducing pain-related behaviors at both early and advanced stages of bone cancer. PERSPECTIVE: Bone cancer pain can be severe and difficult to control fully. With a mouse model of bone cancer pain we demonstrate that pharmacologic blockade of the bradykinin B1 receptor is effective in reducing bone cancer pain-related behaviors, suggesting that B1 antagonists might be useful in attenuating bone cancer pain in humans.
机译:癌症疼痛是一个重大的临床问题,因为它是所有癌症患者中20%至50%的疾病的首发症状,而75%至90%的晚期或晚期癌症患者必须应对与治疗失败和/或肿瘤进展。最难以治疗的癌症疼痛之一是骨骼的转移性侵袭,可产生持续性和骨穿透性疼痛,这是最使人衰弱的癌症相关事件之一。由于缓激肽已显示出可响应组织损伤而释放,并且在驱动急性和慢性炎性疼痛中起重要作用,因此我们将缓激肽拮抗剂集中在骨癌疼痛模型中。在涉及向小鼠股骨注射和限制2472个肉瘤细胞的骨癌模型中,缓激肽B1受体的药理阻断作用可有效减少骨癌早期和晚期的疼痛相关行为。观点:骨癌疼痛可能很严重,难以完全控制。使用骨癌疼痛的小鼠模型,我们证明了缓激肽B1受体的药理学阻断作用可有效减少与骨癌疼痛相关的行为,这表明B1拮抗剂可能对减轻人的骨癌疼痛有用。

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