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[[Image: Organic with clipped surface.png|100 px|left|thumb|Cross section view of mavoglurant in the binding pocket]] | [[Image: Organic with clipped surface.png|100 px|left|thumb|Cross section view of mavoglurant in the binding pocket]] | ||
| - | In the 7 transmembrane ( | + | In the 7 transmembrane domain (TMD), <scene name='72/721532/Mavoglurant_in_pocket/4'>Mavoglurant</scene> is in the 7TM domain pocket. Also, the lysozyme is attached to the intercellular region of the TMD. |
The variation can be seen in positioning of alpha helices. Class C has seemingly less space for mavoglurant to enter compared to Class A and F (Wu). The binding of mavoglurant is seen to be varied in different locations due to helix position (Dore). | The variation can be seen in positioning of alpha helices. Class C has seemingly less space for mavoglurant to enter compared to Class A and F (Wu). The binding of mavoglurant is seen to be varied in different locations due to helix position (Dore). | ||
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== Function and Pathway == | == Function and Pathway == | ||
| - | It all begins with glutamate binding to the venus fly trap domain. The signal transduction goes across the cystine-rich domain to the | + | It all begins with glutamate binding to the venus fly trap domain. The signal transduction goes across the cystine-rich domain to the TMD. Next the dimerization of the TMD occurs. This activates the Gq/11 pathway, which activates phspholipase Cβ. The active phospholipase Cβ performs hydrolysis on phosphotinositides and generates inositol 1,4,5-trisphosphate and diacyl-glycerol. This results in calcium mobilization and activation of protein kinase C. (Niswender, Colleen M..(2010). "Metabotropic Glutamate Receptors: Physiology, Pharmacology, and Disease." Annu. Rev. Pharmacol. Toxicol. Annual Review of Pharmacology and Toxicology 50.1: 295-322.) |
== Disease == | == Disease == | ||
Revision as of 02:31, 30 March 2016
Human metabotropic glutamate receptor 5 transmembrane domain
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