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前带现象干扰胰岛细胞抗体检测:糖尿病高危人群及初发胰岛素依赖型糖尿病患者两种方法的直接比较

A prozone phenomenon interferes in islet cell antibody detection: direct comparison of two methods in subjects at risk of diabetes and in insulin dependent diabetics at onset.

作者信息

Colman P G, Di Mario U, Rabizadeh A, Dotta F, Anastasi E, Eisenbarth G S

机构信息

Joslin Diabetes Center, Brigham and Women's Hospital, Harvard Medical School, New England Deaconess Hospital, Boston, Massachusetts 02215.

出版信息

J Autoimmun. 1988 Apr;1(2):109-17. doi: 10.1016/0896-8411(88)90019-4.

Abstract

A recent international workshop documented marked interlaboratory variation in end point titers of standard islet cell antibody (ICA) positive sera. End titers were lower using a modified assay which utilizes fluorescein labeled protein A (ICA-pA) rather than fluoresceinated anti-IgG (ICA-IgG) to detect antibody binding to islets. In this study we sought to compare directly two ICA assays with respect to future development of IDDM. Sera were obtained from 26 prospectively evaluated high risk subjects identified by family screening or history of transient hyperglycemia and 12 normal controls. As expected, end point titers for ICA positive sera were 10 times greater using the ICA-IgG assay than with the ICA-pA assay. However, despite higher end point titers, the ICA-IgG assay failed to detect more 'prediabetics' and showed a prozone effect. Fourteen subjects were positive at a 1:2 dilution using the ICA-pA assay. Only 10 of these 14 were positive at a 1:2 dilution using the ICA-IgG assay but all became positive at greater sera dilutions. No normal controls were positive using either assay. A similar prozone was observed with anti-islet monoclonal antibodies A2B5 and 4F2. Sera from 14 long-standing IDDM patients (where titers of ICA may have decreased relative to time of onset of diabetes) which were negative using ICA-pA were also assayed using ICA-IgG. Five sera positive for ICA-IgG but negative for ICA-pA were identified. In addition two sera in which a prozone effect was seen with ICA-pA were identified.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

最近的一次国际研讨会记录了标准胰岛细胞抗体(ICA)阳性血清终点滴度在不同实验室间存在显著差异。使用改良检测方法时终点滴度较低,该改良检测方法利用荧光素标记的蛋白A(ICA-pA)而非荧光素化抗IgG(ICA-IgG)来检测抗体与胰岛的结合。在本研究中,我们试图就IDDM的未来发展直接比较两种ICA检测方法。血清取自26名通过家族筛查或短暂高血糖病史确定的前瞻性评估高危受试者以及12名正常对照。正如预期的那样,使用ICA-IgG检测时ICA阳性血清的终点滴度比ICA-pA检测高10倍。然而,尽管终点滴度较高,但ICA-IgG检测未能检测出更多“糖尿病前期患者”,并显示出前带效应。使用ICA-pA检测时,14名受试者在1:2稀释度下呈阳性。在这14名受试者中,使用ICA-IgG检测时只有10名在1:2稀释度下呈阳性,但在更高血清稀释度下均呈阳性。两种检测方法均未检测出正常对照呈阳性。使用抗胰岛单克隆抗体A2B5和4F2时也观察到类似的前带现象。还使用ICA-IgG检测了14名长期IDDM患者(其ICA滴度相对于糖尿病发病时间可能已降低)的血清,这些血清使用ICA-pA检测为阴性。确定了5份ICA-IgG阳性但ICA-pA阴性的血清。此外,还确定了两份使用ICA-pA检测出现前带效应的血清。(摘要截短于250字)

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