摘要
曲妥单抗(TZM)治疗可引起心脏毒性的发展,对这种必要风险的最佳识别可能损害治疗依从性和危害长期康复。为了更好的了解和预测心脏毒性,引起这种毒性作用的分子机制不断被发现。心肌细胞的细胞表面存在HER2。神经调节蛋白是由心脏内皮细胞产生的,且结合在HER4上,从而引起HER2的二聚化和随后的正常心脏功能所必须的细胞信号传导的发生。HER2活性的渐减主要对心肌细胞的共存产生影响。但是,TZM诱导的新功能障碍的大致分子机制仍然不清楚。这篇短篇综述旨在总结遗传、药理和医学数据以帮助识别这些可以解释引起心脏毒性的机制。此外,这些机制凸显了HER2遗传多态性(Val655Ile)在病人识别TZM诱导的心脏作用的风险发展的重要性。
关键词: 心脏毒性,遗传多态性,人类表皮生长因子受体2,个体化治疗,曲妥单抗
图形摘要
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Advanced Pharmacy
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