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开发并鉴定一种独特的抗 IgE 鼠单克隆抗体,可与人及犬 IgE 发生交叉反应。

Development and characterization of a unique anti-IgE mouse monoclonal antibody cross-reactive between human and canine IgE.

机构信息

Animal Allergy Clinical Laboratories Inc., Sagamihara, Kanagawa, Japan.

Vaccine Innovation Laboratory, RIKEN Cluster of Science, Technology and Innovation Hub, RIKEN Baton Zone Program, RIKEN, Yokohama Institute, Yokohama, Kanagawa, Japan.

出版信息

Immun Inflamm Dis. 2021 Dec;9(4):1740-1748. doi: 10.1002/iid3.531. Epub 2021 Sep 17.

Abstract

BACKGROUND

The efficacy assessment of human anti-IgE monoclonal antibodies (mAbs) in animal models before clinical trials is hampered due to the lack of cross-reactivity of anti-IgE mAbs between species.

OBJECTIVE

We developed CRE-DR (an anti-dog IgE monoclonal antibody), an anti-IgE mouse mAb that recognizes canine and human IgE, and then examined its IgE specificity and cross-reactivity between three animal and human species.

METHODS

After mouse immunization with a synthetic peptide derived from canine IgE ( NTNDWIEGETYYC ), we generated a hybridoma producing CRE-DR. The CRE-DR purified from the ascites of hybridoma-inoculated mice was used for ELISA and Western blot analysis to examine reactivity to dog, human, and rodent IgEs as well as recombinant bovine serum albumin (BSA)-conjugated to canine, human, and rodent IgE amino acid peptides corresponding to the immunizing sequence. We then performed enzyme-linked immunosorbent assays (ELISAs) for dog IgE using sera from dogs with atopic dermatitis (AD) after inhibition with canine IgE and IgG. The amino acid sequence recognized by CRE-DR was identified by ELISA using synthetic peptides.

RESULTS

CRE-DR is a monoclonal mouse IgG1κ specific for dog IgE, and the ELISA values in atopic dog sera were inhibited by dog IgE, but not dog IgG. The binding of CRE-DR to human IgE was relatively maintained, but not to rodent IgEs, which results were confirmed with the BSA-conjugated IgE peptides of the various species. The CRE-DR reactivity was supported by the comparison of amino acid sequence of CRE-DR epitope, DWIEGETYYC, in dog IgE; one, two, and three amino acids were substituted in the human, rat, and mouse IgE epitopes, respectively.

CONCLUSIONS AND CLINICAL RELEVANCE

CRE-DR is a mAb cross-reactive to dog and human IgEs, which can allow the use of a dog model of allergy to test the efficacy of a CRE-DR-derived anti-IgE therapeutic mAb before human clinical trials.

摘要

背景

在临床试验之前,由于抗 IgE 单克隆抗体(mAbs)在物种之间缺乏交叉反应性,因此动物模型中人类抗 IgE 单克隆抗体的疗效评估受到阻碍。

目的

我们开发了 CRE-DR(一种抗犬 IgE 单克隆抗体),这是一种识别犬和人 IgE 的抗 IgE 小鼠 mAb,然后检查了其 IgE 特异性和三种动物与人种之间的交叉反应性。

方法

用源自犬 IgE 的合成肽(NTNDWIEGETYYC)免疫小鼠后,我们生成了产生 CRE-DR 的杂交瘤。从小鼠杂交瘤接种的腹水上清液中纯化的 CRE-DR 用于 ELISA 和 Western blot 分析,以检查其对犬、人、和啮齿动物 IgE 以及与免疫序列相对应的犬、人、和啮齿动物 IgE 氨基酸肽偶联的重组牛血清白蛋白(BSA)的反应性。然后,我们使用特应性皮炎(AD)犬的血清进行了犬 IgE 的酶联免疫吸附测定(ELISA),并在抑制犬 IgE 和 IgG 后进行了测定。通过使用合成肽进行 ELISA 鉴定了 CRE-DR 识别的氨基酸序列。

结果

CRE-DR 是一种针对犬 IgE 的单克隆小鼠 IgG1κ,并且在特应性犬血清中的 ELISA 值被犬 IgE 抑制,但不受犬 IgG 抑制。CRE-DR 与人 IgE 的结合相对保持,但不与啮齿动物 IgE 结合,这一结果得到了各种物种的 BSA 结合 IgE 肽的证实。CRE-DR 反应性得到了 CRE-DR 表位 DWIEGETYYC 氨基酸序列在犬 IgE 中的比较的支持;人、大鼠和小鼠 IgE 表位分别有一个、两个和三个氨基酸被取代。

结论和临床相关性

CRE-DR 是一种与人、犬 IgE 发生交叉反应的 mAb,这可以允许在人类临床试验之前使用过敏犬模型来测试 CRE-DR 衍生的抗 IgE 治疗性 mAb 的疗效。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/18b3/8589357/6e2457cf8927/IID3-9-1740-g005.jpg

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