the hinge region of human thyroid-stimulating hormone (tsh) receptor operates as a tunable switch between hormone binding and receptor activation人类的铰链区促甲状腺激素(tsh)受体是一个可调开关之间的绑定和激素受体激活.pdfVIP
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the hinge region of human thyroid-stimulating hormone (tsh) receptor operates as a tunable switch between hormone binding and receptor activation人类的铰链区促甲状腺激素(tsh)受体是一个可调开关之间的绑定和激素受体激活
The Hinge Region of Human Thyroid-Stimulating
Hormone (TSH) Receptor Operates as a Tunable Switch
between Hormone Binding and Receptor Activation
Ritankar Majumdar, Rajan R. Dighe*
Department of Molecular Reproduction, Development and Genetics,Indian Institute of Science, Bangalore, Karnataka, India
Abstract
The mechanism by which the hinge regions of glycoprotein hormone receptors couple hormone binding to activation of
downstream effecters is not clearly understood. In the present study, agonistic (311.62) and antagonistic (311.87)
monoclonal antibodies (MAbs) directed against the TSH receptor extracellular domain were used to elucidate role of the
hinge region in receptor activation. MAb 311.62 which identifies the LRR/Cb-2 junction (aa 265–275), increased the affinity
of TSHR for the hormone while concomitantly decreasing its efficacy, whereas MAb 311.87 recognizing LRR 7–9 (aa 201–
259) acted as a non-competitive inhibitor of Thyroid stimulating hormone (TSH) binding. Binding of MAbs was sensitive to
the conformational changes caused by the activating and inactivating mutations and exhibited differential effects on
hormone binding and response of these mutants. By studying the effects of these MAbs on truncation and chimeric
mutants of thyroid stimulating hormone receptor (TSHR), this study confirms the tethered inverse agonistic role played by
the hinge region and maps the interactions between TSHR hinge region and exoloops responsible for maintenance of the
receptor in its basal state. Mechanistic studies on the antibody-receptor interactions suggest that MAb 311.87 is an allosteric
insurmountable antagonist and inhibits initiation of the hormone induced conformational changes in the hinge region,
whereas MAb 311.62 acts as a partial agonist that recognizes a conformational epitope critical for c
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