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首页> 外文期刊>Current opinion in biotechnology >Enlarging the repertoire of therapeutic monoclonal antibodies platforms: domesticating half molecule exchange to produce stable IgG4 and IgG1 bispecific antibodies
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Enlarging the repertoire of therapeutic monoclonal antibodies platforms: domesticating half molecule exchange to produce stable IgG4 and IgG1 bispecific antibodies

机译:扩大治疗性单克隆抗体平台的范围:驯化半分子交换以产生稳定的IgG4和IgG1双特异性抗体

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Half molecule exchange is the process whereby two IgG4 molecules exchange a heavy chain-light chain unit to form a new IgG4 entity with specificity towards two different antigens. While this unique property of IgG4 molecules confers anti-inflammatory properties in nature, it is not a desirable feature for a therapeutic mAb. Engineering of the IgG4 hinge region making it resemble that of an IgG1 is sufficient to dramatically reduce half molecule exchange in vitro and in vivo. The S228P modification of the hinge confers pharmaceutical properties to IgG4 equivalent to those of standard IgG1, while retaining the inability to trigger ADCC and CDC. Application of the molecular precepts underlying half molecule exchange between IgG4 molecules to IgG1 scaffolds offers the possibility to produce bispecific antibodies in vitro.
机译:半分子交换是两个IgG4分子交换重链-轻链单元以形成对两种不同抗原具有特异性的新IgG4实体的过程。尽管IgG4分子的这种独特性质赋予了自然抗炎特性,但对于治疗性mAb而言却不是理想的功能。 IgG4铰链区的工程使其类似于IgG1,足以显着减少体内外的半分子交换。对铰链的S228P修饰赋予了与标准IgG1等效的IgG4药物特性,同时保留了无法触发ADCC和CDC的能力。 IgG4分子与IgG1支架之间的半分子交换所基于的分子规则的应用提供了在体外产生双特异性抗体的可能性。

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