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Prospective administration of anti-nerve growth factor treatment effectively suppresses functional connectivity alterations after cancer-induced bone pain in mice

机译:抗神经生长因子治疗前瞻性施用有效抑制癌症癌骨疼痛后的功能性连体改变

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Cancer-induced bone pain is abundant among advanced-stage cancer patients and arises from a primary tumor in the bone or skeletal metastasis of common cancer types such as breast, lung, or prostate cancer. Recently, antibodies targeting nerve growth factor (NGF) have been shown to effectively relieve neuropathic and inflammatory pain states in mice and in humans. Although efficacy has been shown in mice on a behavioral level, effectiveness in preventing pain-induced functional rearrangements in the central nervous system has not been shown. Therefore, we assessed longitudinal whole-brain functional connectivity using resting-state functional magnetic resonance imaging in a mouse model of cancer-induced bone pain. We found functional connectivity between major hubs of ascending and descending pain pathways such as the periaqueductal gray, amygdala, thalamus, and cortical somatosensory regions to be affected by a developing cancer pain state. These changes could be successfully prevented through prospective administration of a monoclonal anti-NGF antibody (mAb911). This indicates efficacy of anti-NGF treatment to prevent pain-induced adaptations in brain functional networks after persistent nociceptive input from cancer-induced bone pain. In addition, it highlights the suitability of resting-state functional magnetic resonance imaging readouts as an indicator of treatment response on the basis of longitudinal functional network changes.
机译:癌症诱导的骨疼痛在晚期癌症患者中丰富,并且来自骨骼,肺或前列腺癌等常见癌症类型的骨骼或骨骼转移中的主要肿瘤。最近,已显示针对神经生长因子(NGF)的抗体有效地缓解小鼠和人类的神经病和炎症疼痛状态。虽然小鼠在行为水平上显示了功效,但尚未显示在预防中枢神经系统中疼痛引起的功能重排的有效性。因此,我们在癌症诱导的骨疼痛的小鼠模型中评估纵向全脑功能连通性。我们发现了升序和下降疼痛途径的主要中心之间的功能连通性,例如Periaquenceal Grey,amygdala,丘脑和皮质体传感区域受到发展癌症疼痛状态的影响。通过预期施用单克隆抗NGF抗体(MAB911)可以成功地防止这些变化。这表明抗NGF治疗患者在癌症诱导的骨疼痛的持续伤害性投入后预防脑功能网络中疼痛诱导的适应性的疗效。此外,它突出了静止状态功能磁共振成像读数作为基于纵向功能网络变化的治疗响应指示的适用性。

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