Cre-loxP System-Based Mouse Model for Investigating Graves' Disease and Associated Orbitopathy

Yaru Bao; Daham Kim; Yoon Hee Cho; Cheol Ryong Ku; Jin Sook Yoon; Eun Jig Lee

doi:10.1089/thy.2023.0299

Cre-loxP System-Based Mouse Model for Investigating Graves' Disease and Associated Orbitopathy

Thyroid. 2023 Nov;33(11):1358-1367. doi: 10.1089/thy.2023.0299. Epub 2023 Sep 20.

Authors

Yaru Bao¹, Daham Kim², Yoon Hee Cho², Cheol Ryong Ku², Jin Sook Yoon³, Eun Jig Lee^{1

2}

Affiliations

¹ Graduate School of Medical Science, Brain Korea 21 Project, Severance Hospital, Institute of Vision Research, Yonsei University College of Medicine, Seoul, Republic of Korea.
² Department of Internal Medicine, Institute of Endocrine Research, Severance Hospital, Institute of Vision Research, Yonsei University College of Medicine, Seoul, Republic of Korea.
³ Department of Ophthalmology, Severance Hospital, Institute of Vision Research, Yonsei University College of Medicine, Seoul, Republic of Korea.

PMID: 37624749
DOI: 10.1089/thy.2023.0299

Abstract

Background: Graves' disease (GD), one of the most common forms of autoimmune thyroid disorders, is characterized by hyperthyroidism caused by antibodies (Abs) against the extracellular A-subunit of the thyrotropin receptor (TSHR). Various approaches have been used to create mouse models of GD, including transfected fibroblasts and immunization with plasmids or adenoviruses expressing human TSHR A-subunit (hTSHR A-subunit). These models, however, require repeated immunization and produce inconsistent results. In this study, we established a novel Cre-loxP system-based mouse model that is able to generate the hTSHR A-subunit, mimicking human GD, and characterized the histological changes in Graves' orbitopathy (GO) progression after a single injection. Materials and Methods: A Cre-loxP system-based mouse model was constructed by inserting the CAG-loxP-STOP-loxP-hTSHR A-subunit cassette into the Rosa26 locus of the mouse genome. Conditional expression of the hTSHR A-subunit was successfully achieved by intramuscular injection of the transactivator of transcription-Cre recombinase (GD mice). Blood tests for anti-TSHR Abs and the total thyroxine (T4) level were performed. Magnetic resonance imaging (MRI) was used to monitor morphological changes in the eyes. A histological examination of the thyroid gland and retrobulbar tissues was performed to observe pathological changes. Results: Twenty-four (8 control and 16 GD) mice were investigated. All GD mice exhibited higher levels of TSHR Abs compared with the control group. Moreover, more than 80% of the mouse models showed elevated T4 levels accompanied by thyroid goiter. MRI analysis revealed an increased volume of retrobulbar tissue, while immunohistochemical staining of orbital tissues exhibited macrophage infiltration and muscle fibrosis in the GD mice, contrasting with the control group. Conclusions: Our novel mouse model for GD, which showed the histological features of GO, was successfully established using the Cre-loxP system. This animal model offers improved insights and contributes to advancing methodological developments for GD and GO.

Keywords: Graves' disease; Graves' orbitopathy; TAT-Cre; TSHR A-subunit; site-specific recombination; transcription blocking sequence-floxed gene.

MeSH terms

Animals
Disease Models, Animal
Eye / pathology
Graves Disease*
Graves Ophthalmopathy*
Humans
Integrases / genetics
Mice
Receptors, Thyrotropin

Substances

Cre recombinase
Integrases
Receptors, Thyrotropin

Grants and funding

NO. 6-2021-0128/Yonsei University College of Medicine