Department of Endocrinology, The First Affiliated Hospital of Nanjing Medical University, No.300, Guangzhou Road, Gulou District, Nanjing, Jiangsu, China.
J Transl Med. 2024 Mar 29;22(1):318. doi: 10.1186/s12967-024-05129-3.
A subset of Graves' disease (GD) patients develops refractory hyperthyroidism, posing challenges in treatment decisions. The predictive value of baseline characteristics and early therapy indicators in identifying high risk individuals is an area worth exploration.
A prospective cohort study (2018-2022) involved 597 newly diagnosed adult GD patients undergoing methimazole (MMI) treatment. Baseline characteristics and 3-month therapy parameters were utilized to develop predictive models for refractory GD, considering antithyroid drug (ATD) dosage regimens.
Among 346 patients analyzed, 49.7% developed ATD-refractory GD, marked by recurrence and sustained Thyrotropin Receptor Antibody (TRAb) positivity. Key baseline factors, including younger age, Graves' ophthalmopathy (GO), larger goiter size, and higher initial free triiodothyronine (fT3), free thyroxine (fT4), and TRAb levels, were all significantly associated with an increased risk of refractory GD, forming the baseline predictive model (Model A). Subsequent analysis based on MMI cumulative dosage at 3 months resulted in two subgroups: a high cumulative dosage group (average ≥ 20 mg/day) and a medium-low cumulative dosage group (average < 20 mg/day). Absolute values, percentage changes, and cumulative values of thyroid function and autoantibodies at 3 months were analyzed. Two combined predictive models, Model B (high cumulative dosage) and Model C (medium-low cumulative dosage), were developed based on stepwise regression and multivariate analysis, incorporating additional 3-month parameters beyond the baseline. In both groups, these combined models outperformed the baseline model in terms of discriminative ability (measured by AUC), concordance with actual outcomes (66.2% comprehensive improvement), and risk classification accuracy (especially for Class I and II patients with baseline predictive risk < 71%). The reliability of the above models was confirmed through additional analysis using random forests. This study also explored ATD dosage regimens, revealing differences in refractory outcomes between predicted risk groups. However, adjusting MMI dosage after early risk assessment did not conclusively improve the prognosis of refractory GD.
Integrating baseline and early therapy characteristics enhances the predictive capability for refractory GD outcomes. The study provides valuable insights into refining risk assessment and guiding personalized treatment decisions for GD patients.
Graves 病(GD)患者中有一部分会发展为难治性甲状腺功能亢进症,这给治疗决策带来了挑战。确定高危人群的基线特征和早期治疗指标的预测价值是一个值得探索的领域。
这是一项前瞻性队列研究(2018-2022 年),共纳入 597 例新诊断的成年 GD 患者,均接受甲巯咪唑(MMI)治疗。根据抗甲状腺药物(ATD)剂量方案,利用基线特征和 3 个月治疗参数,建立预测难治性 GD 的模型。
在 346 例分析患者中,49.7%发生了 ATD 难治性 GD,表现为复发和持续的促甲状腺素受体抗体(TRAb)阳性。关键的基线因素,包括年龄较小、Graves 眼病(GO)、更大的甲状腺肿大小以及更高的初始游离三碘甲状腺原氨酸(fT3)、游离甲状腺素(fT4)和 TRAb 水平,均与难治性 GD 的风险增加显著相关,形成了基线预测模型(模型 A)。随后根据 3 个月时 MMI 累积剂量进行分析,分为高累积剂量组(平均≥20mg/天)和中低累积剂量组(平均<20mg/天)。分析了 3 个月时甲状腺功能和自身抗体的绝对值、百分比变化和累积值。基于逐步回归和多变量分析,根据 3 个月时的额外参数,建立了两个联合预测模型,模型 B(高累积剂量)和模型 C(中低累积剂量)。在这两个组中,这些联合模型在判别能力(以 AUC 衡量)、与实际结果的一致性(综合改善率为 66.2%)和风险分类准确性(尤其是基线预测风险<71%的 I 类和 II 类患者)方面均优于基线模型。通过使用随机森林进行的额外分析,证实了上述模型的可靠性。本研究还探讨了 ATD 剂量方案,发现难治性结局在预测风险组之间存在差异。然而,在早期风险评估后调整 MMI 剂量并不能显著改善难治性 GD 的预后。
整合基线和早期治疗特征可提高难治性 GD 结局的预测能力。本研究为细化 GD 患者的风险评估和指导个体化治疗决策提供了有价值的见解。
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