Hannah Miller scite author profile

SUMMARY The excretion of steroid hormone metabolites was studied in normal, thyrotoxic and myxoedematous subjects. Corticosteroid excretion was increased in thyrotoxicosis and reduced in myxoedema. In myxoedema there was also a fall of total androgen excretion due principally to a reduction of the androsterone component. There was no change in total androgen excretion in thyrotoxic subjects, but there was a fall of aetiocholanolone excretion.

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TREM2is thyroid hormone regulated making the TREM2 pathway druggable with ligands for thyroid hormone receptor

Ferrara

Chaudhary

DeBell

et al. 2021

Preprint

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Triggering receptor expressed on myeloid cells-2 (TREM2) is a cell surface receptor on macrophages and microglia that senses and responds to disease associated signals to regulate the phenotype of these innate immune cells. The TREM2 signaling pathway has been implicated in a variety of diseases ranging from neurodegeneration in the central nervous system to metabolic disease in the periphery. We report here that TREM2 is a thyroid hormone regulated gene and its expression in macrophages and microglia is stimulated by thyroid hormone. Both endogenous thyroid hormone and sobetirome, a synthetic thyroid hormone agonist drug, suppress pro-inflammatory cytokine production from myeloid cells including macrophages that have been treated with the SARS-CoV-2 spike protein which produces a strong, pro-inflammatory phenotype. Thyroid hormone agonism was also found to induce phagocytic behavior in microglia, a phenotype consistent with activation of the TREM2 pathway. The thyroid hormone antagonist NH-3 blocks the anti-inflammatory effects of thyroid hormone agonists and suppresses microglia phagocytosis. Finally, in a murine experimental autoimmune encephalomyelitis (EAE) multiple sclerosis model, treatment with Sob-AM2, a CNS-penetrating sobetirome prodrug, results in increased Trem2 expression in disease lesion resident myeloid cells which correlates with therapeutic benefit in the EAE clinical score and reduced damage to myelin. Our findings represent the first report of endocrine regulation of TREM2 and provide a unique opportunity to drug the TREM2 signaling pathway with orally active small molecule therapeutic agents.

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Anti-Thyroid Activity of 2-Carbethoxythio-1-Methylglyoxaline

Macgregor¹,

Miller²

1953

The Lancet

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Hannah Miller

Myelin repair stimulated by CNS-selective thyroid hormone action

TREM2 is thyroid hormone regulated making the TREM2 pathway druggable with ligands for thyroid hormone receptor

Thyroid Function and Steroid Hormone Excretion

TREM2is thyroid hormone regulated making the TREM2 pathway druggable with ligands for thyroid hormone receptor

Anti-Thyroid Activity of 2-Carbethoxythio-1-Methylglyoxaline

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