单克隆抗体
抗体
药代动力学
转基因
转基因小鼠
免疫学
新生儿Fc受体
体内
主要组织相容性复合体
生物
医学
药理学
免疫球蛋白G
抗原
基因
遗传学
作者
Derry C. Roopenian,Gregory J. Christianson,Thomas J. Sproule
标识
DOI:10.1007/978-1-60761-058-8_6
摘要
Therapeutic monoclonal antibodies are widely recognized to be a most promising means to treat an increasing number of human diseases, including cancers and autoimmunity. To a large extent, the efficacy of monoclonal antibody treatment is because IgG antibodies have greatly extended persistence in vivo. However, conventional rodent models do not mirror human antibody pharmacokinetics. The key molecule responsible for the extended persistence antibodies is the major histocompatibility complex class I family Fc receptor, FcRn. We describe human FcRn transgenic mouse models and how they can be exploited productively for the preclinical pharmacokinetic evaluation of therapeutic antibodies.
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