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硫酰胺类药物和高氯酸盐对格雷夫斯病中促甲状腺素免疫球蛋白的类似作用:反对硫酰胺类药物免疫抑制作用的证据

Similar effects of thionamide drugs and perchlorate on thyroid-stimulating immunoglobulins in Graves' disease: evidence against an immunosuppressive action of thionamide drugs.

作者信息

Wenzel K W, Lente J R

出版信息

J Clin Endocrinol Metab. 1984 Jan;58(1):62-9. doi: 10.1210/jcem-58-1-62.

Abstract

Previous studies have shown that serum titers of thyroid-specific antibodies such as thyroid-stimulating immunoglobulins (TSI), TSH-displacing antibodies (TDA), or microsomal antibodies (MAb) decrease in patients with Graves' disease during therapy with thionamide drugs (TD). In keeping with some in vitro results it was postulated that TD have an immunosuppressive action which may be partly responsible for the beneficial effects. To further elucidate this theory, we compared the changes in TSI during treatment with TD such as methimazole (MMI) and propylthiouracil (PTU) as well as with perchlorate (PC), an unrelated compound with a different mode of therapeutic action. Of 69 patients with hyperthyroidism due to Graves' disease, serum from 62 (90%) was positive for TSI, as measured by cAMP accumulation in a thyroid tissue culture assay. Six patients had to be excluded due to noncompliance. Of the remaining 56 patients, those 41 subjects (73%) with good control of the disease were followed up to 24 months during dose-adjusted antithyroid treatment. All patients with an uncomplicated course of treatment had a decline in the initially increased TSI values on either drug regimen. Five of 10 patients receiving PTU and 8 of 13 patients receiving MMI reached normal TSI levels; so did 11 of 18 patients receiving PC. There was no individual correlation between TSI decrease and drug dosages or the serum T4 and T3 levels. In all 3 groups, however, a decrease in mean T4 and T3 levels preceded the fall in TSI. By grouping the patients according to whether they had more than a 20% decrease in the initial TSI values after either 2 months or more than 4 months of treatment, it could be shown that the late responders had significantly higher T4 and T3 levels after 2 months of treatment. The similar patterns of change in TSI during treatment with TD and PC are strong evidence against an immunosuppressive effect of TD. If any direct interference occurs, a toxic effect on intrathyroidal lymphocytes by intrathyroidal drug accumulation could be the cause of the disappearance of TSI with both drug types. On the other hand, the data provide indirect evidence for the theory that the restoration of the euthyroid state is the cause of decreasing TSI levels and normalization of the immune regulation in many patients during treatment with antithyroid drugs.

摘要

以往研究表明,在硫脲类药物(TD)治疗格雷夫斯病患者的过程中,甲状腺特异性抗体如促甲状腺素受体抗体(TSI)、促甲状腺素置换抗体(TDA)或微粒体抗体(MAb)的血清滴度会降低。与一些体外实验结果一致,有人推测TD具有免疫抑制作用,这可能是其产生有益效果的部分原因。为了进一步阐明这一理论,我们比较了在使用甲巯咪唑(MMI)、丙硫氧嘧啶(PTU)等TD以及高氯酸盐(PC,一种治疗作用方式不同的无关化合物)治疗期间TSI的变化。在69例格雷夫斯病所致甲亢患者中,通过甲状腺组织培养试验中cAMP积累测定,62例(90%)患者的血清TSI呈阳性。6例患者因不依从被排除。在其余56例患者中,41例(73%)病情得到良好控制的患者在调整剂量的抗甲状腺治疗期间随访了24个月。所有治疗过程无并发症的患者,无论采用哪种药物治疗方案,其最初升高的TSI值均下降。接受PTU治疗的10例患者中有5例、接受MMI治疗的13例患者中有8例以及接受PC治疗的18例患者中有11例TSI水平恢复正常。TSI降低与药物剂量或血清T4和T3水平之间无个体相关性。然而,在所有3组中,平均T4和T3水平的降低均先于TSI的下降。通过根据患者在治疗2个月或4个月以上后初始TSI值是否下降超过20%进行分组,可以发现反应较慢的患者在治疗2个月后T4和T3水平显著更高。TD和PC治疗期间TSI的相似变化模式有力地证明TD不存在免疫抑制作用。如果存在任何直接干扰,甲状腺内药物蓄积对甲状腺内淋巴细胞的毒性作用可能是两种药物类型导致TSI消失的原因。另一方面,这些数据为以下理论提供了间接证据:在许多患者接受抗甲状腺药物治疗期间,甲状腺功能正常状态的恢复是TSI水平降低和免疫调节正常化的原因。

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