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首页> 外文期刊>Current drug discovery technologies >Transgenic mouse strains as platforms for the successful discovery and development of human therapeutic monoclonal antibodies.
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Transgenic mouse strains as platforms for the successful discovery and development of human therapeutic monoclonal antibodies.

机译:转基因小鼠品系作为成功发现和开发人类治疗性单克隆抗体的平台。

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摘要

Transgenic mice have yielded seven of the ten currently-approved human antibody drugs, making them the most successful platform for the discovery of fully human antibody therapeutics. The use of the in vivo immune system helps drive this success by taking advantage of the natural selection process that produces antibodies with desirable characteristics. Appropriately genetically-engineered mice act as robust engines for the generation of diverse repertoires of affinity- matured fully human variable regions with intrinsic properties necessary for successful antibody drug development including high potency, specificity, manufacturability, solubility and low risk of immunogenicity. A broad range of mAb drug targets are addressable in these mice, comprising both secreted and transmembrane targets, including membrane multi-spanning targets, as well as human target antigens that share high sequence identity with their mouse orthologue. Transgenic mice can routinely yield antibodies with sub-nanomolar binding affinity for their antigen, with lead candidate mAbs frequently possessing affinities for binding to their target of less than 100 picomolar, without requiring any ex vivo affinity optimization. While the originator transgenic mice platforms are no longer broadly available, a new generation of transgenic platforms is in development for discovery of the next wave of human therapeutic antibodies.
机译:转基因小鼠已经产生了十种目前批准的人类抗体药物中的七种,使其成为发现完全人类抗体疗法的最成功平台。体内免疫系统的使用通过利用产生具有所需特征的抗体的自然选择过程来帮助推动这一成功。适当地,经基因工程改造的小鼠可充当强大的引擎,以生成具有亲和力成熟的完整人类可变区的各种库,这些库具有成功开发抗体药物所必需的内在特性,包括高效力,特异性,可制造性,溶解性和低免疫原性风险。在这些小鼠中可寻址的mAb药物靶标范围很广,既包括分泌的靶标,也包括跨膜靶标,包括跨膜靶标,以及与它们的小鼠直系同源物具有高度序列同一性的人靶标抗原。转基因小鼠可以常规产生对其抗原具有亚纳摩尔结合亲和力的抗体,而领先的候选单克隆抗体通常具有小于100皮摩尔的结合力,而无需任何离体亲和力优化。尽管始祖转基因小鼠平台已不再广泛可用,但新一代转基因平台正在开发中,以发现下一波人类治疗性抗体。

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