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Enhancing Antibody Fc Heterodimer Formation through Electrostatic Steering Effects

机译:通过静电转向效应增强抗体Fc异二聚体形成

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Naturally occurring IgG antibodies are bivalent and monospecific. Bispecific antibodies having binding specificities for two different antigens can be produced using recombinant technologies and are projected to have broad clinical applications. However, co-expression of multiple light and heavy chains often leads to contaminants and pose purification challenges. In this work, we have modified the CH3 domain interface of the antibody Fc region with selected mutations so that the engineered Fc proteins preferentially form heterodimers. These novel mutations create altered charge polarity across the Fc dimer interface such that coexpression of electrostatically matched Fc chains support favorable attractive interactions thereby promoting desired Fc heterodimer formation, whereas unfavorable repulsive charge interactions suppress unwanted Fc homodimer formation. This new Fc heterodimer format was used to produce bispecific single chain antibody fusions and monovalent IgGs with minimal homodimer contaminants. The strategy proposed here demonstrates the feasibility of robust production of novel Fc-based heterodimeric molecules and hence broadens the scope of bispecific molecules for therapeutic applications.
机译:天然存在的IgG抗体是二价和单特异性的。可以使用重组技术生产具有两种不同抗原的结合特异性的双特异性抗体,并预计具有广泛的临床应用。然而,多个轻链和重链的共同表达通常导致污染物和姿势净化挑战。在这项工作中,我们用选定的突变修饰了抗体Fc区的CH3结构域界面,使得工程化Fc蛋白优先形成异二聚体。这些新突变在Fc二聚体界面上产生改变的电荷极性,使得静电匹配的Fc链的共表达支持良好的有吸引力相互作用,从而促进所需的Fc异二聚体形成,而不利的排斥电荷相互作用抑制了不需要的Fc同型聚合物形成。这种新的Fc异二聚体形式用于产生具有最小同源过二聚体污染物的双特异性单链抗体融合和单价IgG。此处提出的策略显示了新型Fc基异二聚体分子的鲁棒生产的可行性,因此扩大了治疗应用的双特异性分子的范围。

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