Literature DB >> 30351237

A New Highly Thyrotropin Receptor-Selective Small-Molecule Antagonist with Potential for the Treatment of Graves' Orbitopathy.

Patrick Marcinkowski1, Inna Hoyer1, Edgar Specker1, Jens Furkert1, Claudia Rutz1, Martin Neuenschwander1, Sebastian Sobottka1, Han Sun1, Marc Nazare1, Utta Berchner-Pfannschmidt2, Jens Peter von Kries1, Anja Eckstein2, Ralf Schülein1, Gerd Krause1.   

Abstract

BACKGROUND: The thyrotropin receptor (TSHR) is the target for autoimmune thyroid stimulating antibodies (TSAb) triggering hyperthyroidism. Whereas elevated thyroid hormone synthesis by the thyroid in Graves' disease can be treated by antithyroid agents, for the pathogenic activation of TSHR in retro-orbital fibroblasts of the eye, leading to Graves' orbitopathy (GO), no causal TSHR directed therapy is available.
METHODS: Due to the therapeutic gap for severe GO, TSHR inhibitors were identified by high-throughput screening in Chinese hamster ovary cells expressing the TSHR. Stereo-selective synthesis of the screening hits led to the molecule S37, which contains seven chiral centers. Enantiomeric separation of the molecule S37 resulted in the enantiopure molecule S37a-a micro-molar antagonist of thyrotropin-induced cyclic adenosine monophosphate accumulation in HEK 293 cells expressing the TSHR.
RESULTS: The unique rigid bent shape of molecule S37a may mediate the observed high TSHR selectivity. Most importantly, the closely related follitropin and lutropin receptors were not affected by this compound. S37a not only inhibits the TSHR activation by thyrotropin itself but also activation by monoclonal TSAb M22 (human), KSAb1 (murine), and the allosteric small-molecule agonist C2. Disease-related ex vivo studies in HEK 293 cells expressing the TSHR showed that S37a also inhibits cyclic adenosine monophosphate formation by oligoclonal TSAb, which are highly enriched in GO patients' sera. Initial in vivo pharmacokinetic studies revealed no toxicity of S37a and a remarkable 53% oral bioavailability in mice.
CONCLUSION: In summary, a novel highly selective inhibitor for the TSHR is presented, which has promising potential for further development for the treatment of GO.

Entities:  

Keywords:  Graves’; antagonist; disease; hyperthyroidism; orbitopathy; small molecule; thyrotropin receptor

Mesh:

Substances:

Year:  2018        PMID: 30351237     DOI: 10.1089/thy.2018.0349

Source DB:  PubMed          Journal:  Thyroid        ISSN: 1050-7256            Impact factor:   6.568


  17 in total

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2.  Modulating TSH Receptor Signaling for Therapeutic Benefit.

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Review 3.  2021 update on thyroid-associated ophthalmopathy.

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4.  Novel Approaches for Immunosuppression in Graves' Hyperthyroidism and Associated Orbitopathy.

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6.  Proton pump inhibitors attenuate myofibroblast formation associated with thyroid eye disease through the aryl hydrocarbon receptor.

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9.  Novel Roles of Chloroquine and Hydroxychloroquine in Graves' Orbitopathy Therapy by Targeting Orbital Fibroblasts.

Authors:  Yan Guo; Hai Li; Xueying Chen; Huasheng Yang; Hongyu Guan; Xiaoying He; Yuxin Chen; Sunil Pokharel; Haipeng Xiao; Yanbing Li
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Review 10.  Is There Evidence for IGF1R-Stimulating Abs in Graves' Orbitopathy Pathogenesis?

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