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首页> 外文期刊>Journal of pain and symptom management. >Intravenous ibandronate rapidly reduces pain, neurochemical indices of central sensitization, tumor burden, and skeletal destruction in a mouse model of bone cancer.
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Intravenous ibandronate rapidly reduces pain, neurochemical indices of central sensitization, tumor burden, and skeletal destruction in a mouse model of bone cancer.

机译:在骨癌小鼠模型中,静脉注射伊班膦酸可快速减轻疼痛,中枢敏化的神经化学指标,肿瘤负荷和骨骼破坏。

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摘要

Over half of all chronic cancer pain arises from metastases to bone and bone cancer pain is one of the most difficult of all persistent pain states to fully control. Currently, bone pain is treated primarily by opioid-based therapies, which are frequently accompanied by significant unwanted side effects. In an effort to develop nonopioid-based therapies that could rapidly attenuate tumor-induced bone pain, we examined the effect of intravenous administration of the bisphosphonate, ibandronate, in a mouse model of bone cancer pain. Following injection and confinement of green fluorescent protein-transfected murine osteolytic 2472 sarcoma cells into the marrow space of the femur of male C3H/HeJ mice, ibandronate was administered either as a single dose (300 microg/kg), at Day 7 post-tumor injection, when tumor-induced bone destruction and pain were first evident, or in three consecutive doses (100 microg/kg/day) at Days 7, 8, and 9 post-tumor injection. Intravenous ibandronate administered once or in three consecutive doses reduced ongoing and movement-evoked bone cancer pain-related behaviors, neurochemical markers of central sensitization, tumor burden, and tumor-induced bone destruction. These results support limited clinical trials that suggest the potential of ibandronate to rapidly attenuate bone pain and illuminate the mechanisms that may be responsible for limiting pain and disease progression.
机译:在所有慢性癌症疼痛中,有一半以上是由于转移至骨骼引起的,而骨癌疼痛是所有持续性疼痛状态中最难完全控制的疾病之一。当前,骨痛主要通过基于阿片样物质的疗法来治疗,该疗法经常伴有明显的不良副作用。为了努力开发基于非阿片类药物的疗法,可以迅速减轻肿瘤引起的骨痛,我们在骨癌痛的小鼠模型中检查了静脉给予双膦酸盐,伊班膦酸的效果。将绿色荧光蛋白转染的鼠溶骨性2472肉瘤细胞注射并封闭在雄性C3H / HeJ小鼠股骨的骨髓腔中后,在肿瘤发生后的第7天以单剂量(300 microg / kg)给予伊班膦酸首次发现肿瘤引起的骨破坏和疼痛时,或在肿瘤注射后第7、8和9天连续三剂(100微克/千克/天)注射。静脉注射伊班膦酸一次或连续三剂可减少正在进行的和运动诱发的骨癌疼痛相关行为,中枢敏化的神经化学标志物,肿瘤负荷以及肿瘤引起的骨破坏。这些结果支持有限的临床试验,这些试验表明伊班膦酸具有迅速减轻骨痛并挖掘可能限制疼痛和疾病进展的机制的潜力。

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