Medication-associated thyroid eye disease: a review
摘要
To systematically review the literature surrounding medication-associated thyroid eye disease (TED).
MethodsA systematic search was conducted from inception to the 31st of March 2025 on PubMed, EMBASE and Web of Science. Studies describing medication-associated thyroid dysfunction and the subsequent development of TED were included. Articles without thyroid dysfunction and/or the absence of orbitopathy were excluded.
ResultsA total of 23 studies met the inclusion criteria. Implicated medications included alemtuzumab, immune checkpoint inhibitors (ICI), amiodarone and lenalidomide. The mean onset of thyroid dysfunction from commencement of alemtuzumab was 26.3 ± 12.2 months (Range: 7 to 53.3 months); and the mean onset of developing orbitopathy from thyroid dysfunction was 19.9 ± 21.4 months (Range: 0 to 96 months). Graves’ disease was the most common condition resulting in the development of alemtuzumab-associated TED. ICIs reported to cause TED included ipilimumab (anti-CTLA-4 drug), tremelimumab (anti-CTLA-4 drug), durvalumab (PD-1 inhibitor) and nivolumab (PD-1 inhibitor). Anti-CTLA4 drugs, such as ipilimumab and tremelimumab, were the most common agents implicated in the development of ICI-associated TED. ICIs may also incite orbital inflammation in the absence of thyroid dysfunction. A single case-report of amiodarone- and lenalidomide-associated TED was noted.
ConclusionMedication-associated TED is an important differential consideration in the work-up of orbital inflammatory disease. The clinico-radiological manifestations and the principles of management of medication-associated TED were similar to that of de novo TED. Certain medications, such as various ICIs, may demonstrate different clinical phenotypes of orbital inflammation, inciting either TED or a “TED-like” orbitopathy without evidence of underlying thyroid dysfunction.