Characterizing Thyroid Hormone Replacement, Baseline Thyrotropin, and Survival in Immune Checkpoint Inhibitor-Associated Thyroid Dysfunction.

IF 5.8 1区医学 Q1 ENDOCRINOLOGY & METABOLISM

Thyroid Pub Date : 2025-06-18 DOI:10.1089/thy.2025.0076

Duaa Abdallah, Jake Johnson, Fang Qiu, Whitney Goldner, Apar Kishor Ganti, Anupam Kotwal

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引用次数: 0

Abstract

Background: Thyroid dysfunction (TD) occurs commonly from immune checkpoint inhibitors (ICI) cancer therapy, but questions remain regarding its predicting factors, appropriate dosing for thyroid hormone replacement, and the strength of association with overall survival (OS). We aim to address these three questions in our study. Methods: We performed a retrospective cohort study of adult patients with cancer who received ICIs from December 1, 2012, to December 31, 2019. After excluding 28 patients with preexisting primary hypothyroidism, 811 patients were evaluated for the development of new-onset ICI-TD. Kaplan-Meier survival and log-rank tests were used to compare OS distributions between ICI-TD status groups, following which Cox regression models addressed immortal time bias (ITB). Results: Of the 811 included patients with a median follow-up of 19.2 months, 122 (15.0%) patients developed ICI-TD. The median age at initiation of ICIs was 64.8 years; women comprised 42.8% of the cohort. There were no significant differences in age, sex, race, malignancy type, or personal history of autoimmunity in patients who developed ICI-TD versus those who did not. ICI-TD occurred most frequently after combination ICI therapy (32%) compared with CTLA-4 ICI and PD-1/PD-L1 ICI monotherapy (p = 0.002). The median levothyroxine dose was the highest, being 1.41 mcg/kg/day in the overt hypothyroidism group. Patients with ICI-TD had a higher median pre-treatment log2(thyrotropin or TSH) level (1.2, corresponding to TSH 2.3 mIU/L) versus those without (0.79, corresponding to TSH 1.7 mIU/L; p = 0.008); however, the area under the curve was <0.6, hence lacking predictive ability. The survival benefit of ICI-TD was not apparent after addressing ITB and adjusting for other variables affecting patient outcomes. Conclusions: The levothyroxine dose needed for overt hypothyroidism from ICI-TD is similar to athyreotic hypothyroidism. While baseline TSH in the upper normal range is associated with an increased risk of ICI-TD, there is no absolute baseline TSH value that accurately predicts ICI-TD in the clinical setting. The link between ICI-TD and OS needs further validation after accounting for ITB.

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免疫检查点抑制剂相关甲状腺功能障碍患者甲状腺激素替代、基线促甲状腺素和生存率的特征

背景：甲状腺功能障碍（TD）通常发生在免疫检查点抑制剂（ICI）癌症治疗中，但关于其预测因素、甲状腺激素替代的适当剂量以及与总生存期（OS）的关联强度仍存在疑问。我们的目标是在我们的研究中解决这三个问题。方法：对2012年12月1日至2019年12月31日接受ICIs治疗的成年癌症患者进行回顾性队列研究。在排除了28例既往存在原发性甲状腺功能减退的患者后，对811例患者进行了新发ICI-TD的评估。Kaplan-Meier生存和log-rank检验用于比较ICI-TD状态组之间的OS分布，随后Cox回归模型解决了不朽时间偏差（ITB）。结果：纳入的811例患者中位随访19.2个月，122例（15.0%）患者发生ICI-TD。开始使用ICIs时的中位年龄为64.8岁；女性占42.8%。发生ICI-TD的患者与未发生ICI-TD的患者在年龄、性别、种族、恶性肿瘤类型或自身免疫史方面没有显著差异。与CTLA-4 ICI和PD-1/PD-L1 ICI单药治疗相比，ICI- td在联合ICI治疗后发生率最高（32%）（p = 0.002）。明显甲状腺功能减退组左旋甲状腺素的中位剂量最高，为1.41微克/千克/天。ci - td患者的治疗前log2（促甲状腺激素或TSH）水平中位数（1.2，对应TSH 2.3 mIU/L）高于无ci - td患者（0.79，对应TSH 1.7 mIU/L）；P = 0.008)；结论：ci - td患者明显甲状腺功能减退所需的左旋甲状腺素剂量与甲状腺功能减退相似。虽然正常范围内的基线TSH与ci - td的风险增加有关，但在临床环境中，没有绝对的基线TSH值可以准确预测ci - td。考虑到ITB后，ICI-TD与OS之间的联系需要进一步验证。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Thyroid 医学-内分泌学与代谢

CiteScore

12.30

自引率

6.10%

发文量

195

审稿时长

6 months

期刊介绍： This authoritative journal program, including the monthly flagship journal Thyroid, Clinical Thyroidology® (monthly), and VideoEndocrinology™ (quarterly), delivers in-depth coverage on topics from clinical application and primary care, to the latest advances in diagnostic imaging and surgical techniques and technologies, designed to optimize patient care and outcomes. Thyroid is the leading, peer-reviewed resource for original articles, patient-focused reports, and translational research on thyroid cancer and all thyroid related diseases. The Journal delivers the latest findings on topics from primary care to clinical application, and is the exclusive source for the authoritative and updated American Thyroid Association (ATA) Guidelines for Managing Thyroid Disease.