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关于格雷夫斯病患者抗甲状腺药物治疗后复发预测的前瞻性多中心研究。

Prospective multicentre study on the prediction of relapse after antithyroid drug treatment in patients with Graves' disease.

作者信息

Schleusener H, Schwander J, Fischer C, Holle R, Holl G, Badenhoop K, Hensen J, Finke R, Bogner U, Mayr W R

机构信息

Endocrine Department, Medical Clinic, Free University, Berlin, FRG.

出版信息

Acta Endocrinol (Copenh). 1989 Jun;120(6):689-701. doi: 10.1530/acta.0.1200689.

Abstract

Graves' disease is an autoimmune disease characterized by a course of remission and relapse. Since the introduction of antithyroid drug treatment, various parameters have been tested for their ability to predict the clinical course of a patient with Graves' disease after drug withdrawal. Nearly all these studies were retrospective [corrected] and often yielded conflicting results. In a prospective multicentre study with a total of 451 patients, we investigated the significance of a variety of routine laboratory and clinical parameters for predicting a patient's clinical course. Patients who had positive TSH receptor antibodies activity at the end of therapy showed a significantly higher relapse rate than those without (P less than 0.001). However, the individual clinical course cannot be predicted exactly (sensitivity 0.49, specificity 0.73, N = 391). The measurement of microsomal (P = 0.99, sensitivity 0.37, specificity 0.63, N = 275) or thyroglobulin antibodies (P = 0.76, sensitivity 0.18, specificity 0.84, N = 304) at the end of antithyroid drug therapy did not show a statistically significant difference in the antibody titre between the patients of the relapse and those of the remission group. Additionally, HLA-DR typing (HLA-DR3: P = 0.37, sensitivity 0.36, specificity 0.58, N = 253) was proven to be unsuitable for predicting a patient's clinical course. Patients with abnormal suppression or an abnormal TRH test at the end of antithyroid drug therapy relapse significantly more often (P less than 0.001) than patients with normal suppression or normal TRH test. Patients with a large goitre also have a significantly (P less than 0.001) higher relapse rate than those with only a small enlargement. The sensitivity and specificity values of all these parameters, however, were too low to be useful for daily clinical decisions in the treatment of an individual patient. This is also true for the combinations of different parameters. Though the highest sensitivity value (0.94) was found for a combination of the suppression and the TRH test at the end of therapy, the very low specificity value (0.13) for this combination reduced its clinical usefulness.

摘要

格雷夫斯病是一种以缓解和复发为病程特点的自身免疫性疾病。自从引入抗甲状腺药物治疗以来,人们对各种参数进行了测试,以评估其预测格雷夫斯病患者停药后临床病程的能力。几乎所有这些研究都是回顾性的[已修正],且结果常常相互矛盾。在一项共有451例患者的前瞻性多中心研究中,我们调查了各种常规实验室和临床参数对于预测患者临床病程的意义。治疗结束时促甲状腺激素受体抗体活性呈阳性的患者复发率显著高于抗体活性阴性的患者(P<0.001)。然而,无法准确预测个体的临床病程(敏感性0.49,特异性0.73,N = 391)。抗甲状腺药物治疗结束时,微粒体抗体(P = 0.99,敏感性0.37,特异性0.63,N = 275)或甲状腺球蛋白抗体(P = 0.76,敏感性0.18,特异性0.84,N = 304)的检测结果显示,复发组和缓解组患者的抗体滴度在统计学上无显著差异。此外,HLA-DR分型(HLA-DR3:P = 0.37,敏感性0.36,特异性0.58,N = 253)被证明不适用于预测患者的临床病程。抗甲状腺药物治疗结束时抑制试验异常或促甲状腺激素释放激素(TRH)试验异常的患者复发频率显著高于抑制试验或TRH试验正常的患者(P<0.001)。甲状腺肿大明显的患者复发率也显著高于仅轻度肿大的患者(P<0.001)。然而,所有这些参数的敏感性和特异性值都过低,无法用于个体患者治疗的日常临床决策。不同参数组合的情况也是如此。虽然治疗结束时抑制试验和TRH试验组合的敏感性值最高(0.94),但该组合的特异性值极低(0.13),降低了其临床实用性。

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