JAMA Neurol:α-突触核蛋白单抗PRX002 I期临床结果喜人

2018-06-19 zhangfan MedSci原创

研究认为,PRX002治疗具有极高的耐受性,与外周α-突触核蛋白结合率高。脑脊液药物浓度高于外周,可结合脑细胞外聚集α-突触核蛋白达到预期的治疗效果

α-突触核蛋白被认为是导致帕金森病理过程的核心因素。单克隆抗体PRX002/RG7935 (PRX002)通过靶向α-突触核蛋,抑制α-突触核蛋白神经元间转移,具有潜在的神经元保护和延缓PD疾病进展的效果。近日研究人员公布了PRX002治疗特发性PD患者的I期临床结果。

40-80岁的,轻微至中度特发性PD患者参与(Hoehn-Yahr分期1-3期),患者接受6个剂量的PRX002 (0.3 mg/kg, 1.0 mg/kg, 3.0 mg/kg, 10 mg/kg, 30 mg/kg或 60 mg/kg)或安慰剂,每4周3次,随后接受24周的观察。研究的主要终点为安全性、耐受性及药代动力学研究。

80名患者参与研究,男性占80%,平均年龄58岁。研究中未发生治疗相关的严重不良事件。治疗组患者不良事件率较对照组高5%,包括便秘、输液反应、腹泻、头痛、周围水肿、腰穿后综合征以及上呼吸道感染。未检出抗药抗体。血浆药物浓度按近似剂量成比例增加,平均消除半衰期在所有剂量下相近,均为10.2天。最大剂量条件下,与安慰剂相比游离血清α-突触核蛋白水平下降了97%。脑脊液中药物浓度存在剂量依赖性,较血清浓度增加0.3%。

研究认为,PRX002治疗具有极高的耐受性,与外周α-突触核蛋白结合率高。脑脊液药物浓度高于外周,可结合脑细胞外聚集α-突触核蛋白达到预期的治疗效果。

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    2018-09-25 yinhl1978
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    2018-06-19 1ddf0692m34(暂无匿称)

    学习了.长知识

    0