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快速的 IgE 和 FcεRIα 抗体多克隆脱敏。

Rapid polyclonal desensitization with antibodies to IgE and FcεRIα.

机构信息

Department of Research, Cincinnati Veterans Affairs Medical Center, Cincinnati, Ohio, USA.

出版信息

J Allergy Clin Immunol. 2013 Jun;131(6):1555-64. doi: 10.1016/j.jaci.2013.02.043. Epub 2013 Apr 28.

Abstract

BACKGROUND

Rapid desensitization, a procedure in which persons allergic to an antigen are treated at short intervals with increasing doses of that antigen until they tolerate a large dose, is an effective, but risky, way to induce temporary tolerance.

OBJECTIVE

We wanted to determine whether this approach can be adapted to suppress all IgE-mediated allergies in mice by injecting serially increasing doses of monoclonal antibodies (mAbs) to IgE or FcεRIα.

METHODS

Active and passive models of antigen- and anti-IgE mAb-induced IgE-mediated anaphylaxis were used. Mice were desensitized with serially increasing doses of anti-IgE mAb, anti-FcεRIα mAb, or antigen. Development of shock (hypothermia), histamine and mast cell protease release, cytokine secretion, calcium flux, and changes in cell number and FcεRI and IgE expression were evaluated.

RESULTS

Rapid desensitization with anti-IgE mAb suppressed IgE-mediated immediate hypersensitivity; however, some mice developed mild anaphylaxis during desensitization. Rapid desensitization with anti-FcεRIα mAb that only binds FcεRI that is not occupied by IgE suppressed both active and passive IgE-mediated anaphylaxis without inducing disease. It quickly, but temporarily, suppressed IgE-mediated anaphylaxis by decreasing mast cell signaling through FcεRI, then slowly induced longer lasting mast cell unresponsiveness by removing membrane FcεRI. Rapid desensitization with anti-FcεRIα mAb was safer and longer lasting than rapid desensitization with antigen.

CONCLUSION

A rapid desensitization approach with anti-FcεRIα mAb safely desensitizes mice to IgE-mediated anaphylaxis by inducing mast cell anergy and later removing all mast cell IgE. Rapid desensitization with an anti-human FcεRIα mAb may be able to prevent human IgE-mediated anaphylaxis.

摘要

背景

快速脱敏是一种将过敏者在短时间内间隔地用递增剂量的抗原进行治疗,直至其耐受大剂量抗原的方法,是一种有效但有风险的诱导暂时耐受的方法。

目的

我们想确定通过连续注射递增剂量的针对 IgE 或 FcεRIα 的单克隆抗体 (mAb),是否可以将这种方法用于抑制小鼠所有 IgE 介导的过敏反应。

方法

使用抗原和抗 IgE mAb 诱导的 IgE 介导的过敏反应的主动和被动模型。用递增剂量的抗 IgE mAb、抗 FcεRIα mAb 或抗原对小鼠进行脱敏。评估休克(低体温)、组胺和肥大细胞蛋白酶释放、细胞因子分泌、钙流以及细胞数量和 FcεRI 和 IgE 表达的变化。

结果

用抗 IgE mAb 进行快速脱敏可抑制 IgE 介导的即刻过敏反应;然而,一些小鼠在脱敏过程中出现轻度过敏反应。仅与未被 IgE 占据的 FcεRI 结合的抗 FcεRIα mAb 进行快速脱敏可抑制主动和被动 IgE 介导的过敏反应而不引起疾病。它通过降低通过 FcεRI 的肥大细胞信号传导,迅速但暂时抑制 IgE 介导的过敏反应,然后通过去除膜 FcεRI 缓慢诱导更长时间的肥大细胞无反应性。用抗 FcεRIα mAb 进行快速脱敏比用抗原进行快速脱敏更安全且更持久。

结论

用抗 FcεRIα mAb 进行快速脱敏可通过诱导肥大细胞失能,随后去除所有肥大细胞 IgE,安全地使小鼠对 IgE 介导的过敏反应脱敏。用抗人 FcεRIα mAb 进行快速脱敏可能能够预防人类 IgE 介导的过敏反应。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d8b4/4341981/e307957d06bb/nihms473898f1.jpg

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