自身免疫性疾病和eb病毒相关疾病患者可溶性FcϵRII/CD23:可溶性FcϵRII/CD23 ELISA分析

Yoshikawa Tsutomu, Nanba Toshihiko, Kato Hironori, Hori Kotari, Inamoto Takashi, Kumagai Shunichi, Yodoi Junji
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引用次数: 17

摘要

IgE的低亲和力Fc受体(FcϵRII/CD23)及其可溶性形式(sCD23, IgE结合因子)具有多种功能,其水平升高与各种免疫疾病有关。我们建立了酶偶联单抗和生物素化单抗两种灵敏的ELISA系统。ELISA系统的检出限分别为0.03和1.0 ng/ml,在1.0 ~ 10 ng/ml范围内具有良好的相关性。在酶偶联mAb ELISA系统中,303名正常健康志愿者的sCD23平均浓度为1.4±0.3 ng/ml。在使用生物素化单抗的ELISA系统中,正常健康志愿者的sCD23水平显示几乎相同的值。在类风湿性关节炎、系统性红斑狼疮、Sjögren综合征、进行性系统性硬化症、混合性结缔组织病等自身免疫性疾病患者中,sCD23水平明显高于正常人。此外,在伴有免疫抑制的肝移植后Epstein-Barr病毒相关疾病中,当临床症状明显时,血浆sCD23水平迅速升高至12 ng/ml以上。此外,sCD23值仍然很高,尽管升高的GOT水平逐渐下降到标准值,EBV肝炎得到改善。这些数据表明,sCD23水平是自身免疫性疾病和ebv相关疾病以及过敏性疾病的敏感标志物。sCD23的ELISA系统可能是估计这些疾病临床病程的额外诊断工具。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Soluble FcϵRII/CD23 in Patients with Autoimmune Diseases and Epstein-Barr Virus-Related Disorders: Analysis by ELISA for Soluble FcϵRII/CD23

The low-affinity Fc receptor for IgE (FcϵRII/CD23) and its soluble form (sCD23, IgE-binding factor) have multiple functions, and enhanced levels of these are associated with various immunological diseases. We established two sensitive ELISA systems using enzyme-conjugated mAb and biotinylated mAb. The detection limits of the ELISA systems were 0.03 and 1.0 ng/ml, which showed good correlation in the range 1.0-10 ng/ml. In the ELISA system using enzyme-conjugated mAb, the average sCD23 concentration in 303 normal healthy volunteers was 1.4 ± 0.3 ng/ml. In the ELISA system using biotinylated mAb, sCD23 levels in normal healthy volunteers showed almost the same values. In patients with autoimmune diseases such as rheumatoid arthritis, systemic lupus erythematosus, Sjögren syndrome, progressive systemic sclerosis, and mixed connective tissue disease, the sCD23 levels were significantly higher than those in normal individuals. Furthermore, in Epstein-Barr virus-related disorders after liver transplantation with immunosuppression, plasma levels of sCD23 rapidly Increased to more than 12 ng/ml when clinical symptoms were evident. In addition, the sCD23 values remained high, although elevated GOT levels gradually decreased to standard values and EBV hepatitis improved. These data suggest that sCD23 levels are a sensitive marker of autoimmune diseases and EBV-related disorders in addition to allergic disorders. The ELISA system for sCD23 may be an additional diagnostic tool in estimating the clinical courses of these diseases.

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