Strategies to evaluate potential effector function of glycan variants: a case study of ordesekimab (AMG 714 or PRV-015).

IF 2.4 4区 医学 Q3 TOXICOLOGY Journal of Immunotoxicology Pub Date : 2022-12-01 DOI:10.1080/1547691X.2022.2113841
Yu-Ling Wei, Teresa Wegesser, Scott Kuhns, Jonathan Werner, Hervé Lebrec, Xiaoting Wang
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Abstract

The potential for effector functions of therapeutic antibodies, including antibody-dependent cell-mediated cytotoxicity (ADCC), is a biological activity of interest for characterization, regardless of if ADCC is an intended primary pharmacological effect. The composition of the conserved antibody Fc glycan can vary as a function of post-translational processing which may affect the binding affinity to Fc receptors, leading to a change of effector activity. Ordesekimab (AMG 714 or PRV-015), a fully human immunoglobulin G1-kappa anti-interleukin (IL)-15 monoclonal antibody, is in clinical development for celiac disease. The binding of ordesekimab to IL-15 inhibits the interaction of IL-15 with the IL-2Rβ and common γ chain of the IL-15 receptor complex, but not with the IL-15Rα chain. Therefore, the simultaneous binding of ordesekimab to the F receptor (R) IIIα expressed on natural killer (NK) cells and to the IL-15/IL-15Rα complex on cells such as monocytes may theoretically enable ADCC toward the IL-15Rα-expressing cells. The high mannose (HM) levels on the Fc glycan were found to vary in different lots of ordesekimab resulting from refinements to the manufacturing process, and the impact on ordesekimab-mediated ADCC activity was evaluated in in vivo and in vitro studies. A review of nonclinical and clinical data found no evidence of ordesekimab-induced depletion of monocytes, or cytotoxicity in organs with wide IL-15Rα expression, suggesting a lack of in vivo ADCC activity. In addition, in vitro peripheral blood mononuclear cells-based ADCC assay did not reveal any cytolytic effect of ordesekimab with various levels of HM content when cocultured with recombinant human IL-15. Taken together, these data demonstrate that ADCC is not a potential liability for ordesekimab and does not contribute to the reduction of IL-15-mediated inflammation, the intended pharmacological effect.

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评估聚糖变体潜在效应功能的策略:以orderekimab (AMG 714或PRV-015)为例
治疗性抗体的潜在效应功能,包括抗体依赖细胞介导的细胞毒性(ADCC),是表征感兴趣的生物活性,无论ADCC是否是预期的主要药理作用。保守抗体Fc聚糖的组成可以随着翻译后加工的变化而变化,这可能会影响其与Fc受体的结合亲和力,从而导致效应物活性的变化。Ordesekimab (AMG 714或PRV-015)是一种全人免疫球蛋白G1-kappa抗白细胞介素(IL)-15单克隆抗体,目前正处于乳糜泻的临床开发中。ordesekimab与IL-15结合抑制IL-15与IL-2Rβ和IL-15受体复合物的公共γ链的相互作用,但不与IL-15Rα链相互作用。因此,ordesekimab同时结合自然杀伤细胞(NK)上表达的Fcγ受体(R) IIIα和细胞(如单核细胞)上表达的IL-15/IL-15Rα复合物,理论上可能使ADCC作用于表达IL-15Rα的细胞。由于制造工艺的改进,在不同批次的orderekimab中发现Fc聚糖上的高甘露糖(HM)水平有所不同,并且在体内和体外研究中评估了对orderekimab介导的ADCC活性的影响。一项对非临床和临床数据的回顾发现,在IL-15Rα广泛表达的器官中,没有证据表明ordesekimab诱导单核细胞耗损或细胞毒性,这表明缺乏体内ADCC活性。此外,在体外外周血单核细胞ADCC实验中,不同HM含量的orderekimab与重组人IL-15共培养均未显示出任何细胞溶解作用。综上所述,这些数据表明ADCC不是ordesekimab的潜在责任,也不会减少il -15介导的炎症,这是预期的药理作用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Journal of Immunotoxicology
Journal of Immunotoxicology 医学-毒理学
CiteScore
6.70
自引率
3.00%
发文量
26
审稿时长
1 months
期刊介绍: The Journal of Immunotoxicology is an open access, peer-reviewed journal that provides a needed singular forum for the international community of immunotoxicologists, immunologists, and toxicologists working in academia, government, consulting, and industry to both publish their original research and be made aware of the research findings of their colleagues in a timely manner. Research from many subdisciplines are presented in the journal, including the areas of molecular, developmental, pulmonary, regulatory, nutritional, mechanistic, wildlife, and environmental immunotoxicology, immunology, and toxicology. Original research articles as well as timely comprehensive reviews are published.
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