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评估候选治疗性抗IL21R抗体的激动潜力。

Assessing agonistic potential of a candidate therapeutic anti-IL21R antibody.

作者信息

Guo Yongjing, Hill Andrew A, Ramsey Renee C, Immermann Frederick W, Corcoran Christopher, Young Deborah, Lavallie Edward R, Ryan Mark, Bechard Theresa, Pfeifer Richard, Warner Garvin, Bologna Marcia, Bloom Laird, O'Toole Margot

机构信息

Pfizer, BioTherapeutics Clinical Translational Medicine, Cambridge, MA, USA.

出版信息

J Transl Med. 2010 May 26;8:50. doi: 10.1186/1479-5876-8-50.

Abstract

BACKGROUND

Selective neutralization of the IL21/IL21R signaling pathway is a promising approach for the treatment of a variety of autoimmune diseases. Ab-01 is a human neutralizing anti-IL21R antibody. In order to ensure that the activities of Ab-01 are restricted to neutralization even under in vitro cross-linking and in vivo conditions, a comprehensive assessment of agonistic potential of Ab-01 was undertaken.

METHODS

In vitro antibody cross-linking and cell culture protocols reported for studies with a human agonistic antibody, TGN1412, were followed for Ab-01. rhIL21, the agonist ligand of the targeted receptor, and cross-linked anti-CD28 were used as positive controls for signal transduction. In vivo agonistic potential of Ab-01 was assessed by measuring expression levels of cytokine storm-associated and IL21 pathway genes in blood of cynomolgus monkeys before and after IV administration of Ab-01.

RESULTS

Using a comprehensive set of assays that detected multiple activation signals in the presence of the positive control agonists, in vitro Ab-01-dependent activation was not detected in either PBMCs or the rhIL21-responsive cell line Daudi. Furthermore, no difference in gene expression levels was detected in blood before and after in vivo Ab-01 dosing of cynomolgus monkeys.

CONCLUSIONS

Despite efforts to intentionally force an agonistic signal from Ab-01, none could be detected.

摘要

背景

选择性中和IL21/IL21R信号通路是治疗多种自身免疫性疾病的一种有前景的方法。Ab-01是一种人源中和抗IL21R抗体。为确保即使在体外交联和体内条件下Ab-01的活性也仅限于中和作用,对Ab-01的激动潜力进行了全面评估。

方法

针对Ab-01,遵循了已报道的用于人源激动性抗体TGN1412研究的体外抗体交联和细胞培养方案。将靶向受体的激动剂配体rhIL21和交联的抗CD28用作信号转导的阳性对照。通过测量食蟹猴静脉注射Ab-01前后血液中细胞因子风暴相关基因和IL21通路基因的表达水平,评估Ab-01的体内激动潜力。

结果

使用一套全面的检测方法,在存在阳性对照激动剂的情况下检测多个激活信号,在PBMC或rhIL21反应性细胞系Daudi中均未检测到体外Ab-01依赖性激活。此外,食蟹猴体内注射Ab-01前后血液中的基因表达水平没有差异。

结论

尽管有意努力促使Ab-01产生激动信号,但未检测到任何激动信号。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e3cd/2896924/eb29b8f6e204/1479-5876-8-50-1.jpg

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