Nakatake Nobuhiro, Sanders Jane, Richards Tonya, Burne Peter, Barrett Carol, Pra Chiara Dal, Presotto Fabio, Betterle Corrado, Furmaniak Jadwiga, Smith Bernard Rees
FIRS Laboratories, RSR Ltd, Llanishen, Cardiff, United Kingdom.
Thyroid. 2006 Nov;16(11):1077-84. doi: 10.1089/thy.2006.16.1077.
We have used the human monoclonal TSH receptor (TSHR) autoantibody (M22) as a labeled ligand in competition with individual patient TSHR autoantibodies (TRAb) to estimate their serum concentrations and affinities. TSHR coated tubes, (125)I-labeled M22 IgG and Fab, and patient sera IgG and Fab were used in these studies. In 15 patients with Graves' disease, TRAb concentrations ranged from 50 to 500 ng/mL of serum (5- 60 parts per million of total serum IgG) and TRAb IgG affinities from 3.0 +/- 1.0-6.7 +/- 1.54-10(10) L/mol (mean +/- SD; n=3). Fab fragment affinities were similar to those of intact IgG. Serum TRAb with blocking (TSH antagonist; 4 patients) activity had similar affinities (3.0 +/- 0.25-7.2 +/- 2.2-10(10) L/mol) to TRAb IgG from patients with Graves' disease, but blocking TRAb concentrations were higher (1.7 - 27 mg/mL of serum). The concentrations of TRAb that we observed in the sera of the 15 Graves' patient (0.33 - 3.3 nmol/L) can be compared with that of circulating TSH. In particular, a serum TSH concentration of 100mU/L (0.7 nmol/L) is in the same range as the concentrations of TRAb we observed. Such a TSH concentration (similar to that observed after injection of 0.9 mg of recombinant human TSH) would be expected to cause a similar degree of thyrotoxicosis as seen in Graves' disease. Consequently, the thyroid-stimulating potencies (i.e., activity per mol) of patient serum TRAb and human TSH appear to be of a similar magnitude in vivo as well as in vitro. Overall, our results indicate that serum TRAb affinities are high and show only limited variations between different sera whereas concentrations of the autoantibodies vary widely.
我们使用人源单克隆促甲状腺激素受体(TSHR)自身抗体(M22)作为标记配体,与个体患者的TSHR自身抗体(TRAb)进行竞争,以估计其血清浓度和亲和力。在这些研究中使用了TSHR包被管、(125)I标记的M22 IgG和Fab以及患者血清IgG和Fab。在15例格雷夫斯病患者中,TRAb浓度范围为血清50至500 ng/mL(占总血清IgG的百万分之5至60),TRAb IgG亲和力为3.0±1.0至6.7±1.54×10¹⁰ L/mol(平均值±标准差;n = 3)。Fab片段亲和力与完整IgG相似。具有阻断(TSH拮抗剂;4例患者)活性的血清TRAb与格雷夫斯病患者的TRAb IgG具有相似的亲和力(3.0±0.25至7.2±2.2×10¹⁰ L/mol),但阻断性TRAb浓度更高(血清1.7至27 mg/mL)。我们在15例格雷夫斯病患者血清中观察到的TRAb浓度(0.33至3.3 nmol/L)可与循环TSH浓度相比较。特别是,血清TSH浓度为100 mU/L(0.7 nmol/L)与我们观察到的TRAb浓度处于同一范围。这样的TSH浓度(类似于注射0.9 mg重组人TSH后观察到的浓度)预计会引起与格雷夫斯病中所见相似程度的甲状腺毒症。因此,患者血清TRAb和人TSH的甲状腺刺激效力(即每摩尔活性)在体内和体外似乎具有相似的大小。总体而言,我们的结果表明血清TRAb亲和力较高,不同血清之间仅显示有限的差异,而自身抗体的浓度差异很大。
