Sandbox Reserved 1702

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===Inactive===
===Inactive===
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A few hallmarks of the inactive structure of mGlu2 are the Venus FlyTrap Domain in the open conformation, well separated Cysteine-Rich Domains, and distinct orientation of the 7 Transmembrane Domains (7TM). Perhaps the most critical component of the inactive form is the <scene name='90/904307/Tmd_helices/3'>asymmetric TM3-TM4 interface</scene> formed by both of the 7 alpha helices in the alpha and beta chains in the transmembrane domain. The transmembrane domain is mediated mainly by helix IV on the alpha chain and helix lll on the beta chain of the dimer through hydrophobic interactions. These hydrophobic interactions between both transmembrane helices stabilize inactive conformation of mGlu2.
[[Image:TM4_hydrophobic_interactions.png|300 px|left|thumb|'''Figure 1.''' Hydrophobic interactions of transmembrane helices III and IV that stabilize the inactive form of mGlu2.]]
[[Image:TM4_hydrophobic_interactions.png|300 px|left|thumb|'''Figure 1.''' Hydrophobic interactions of transmembrane helices III and IV that stabilize the inactive form of mGlu2.]]
===Positive Allosteric Modulator(PAM) Bound===
===Positive Allosteric Modulator(PAM) Bound===

Revision as of 22:58, 28 March 2022

This Sandbox is Reserved from February 28 through September 1, 2022 for use in the course CH462 Biochemistry II taught by R. Jeremy Johnson at the Butler University, Indianapolis, USA. This reservation includes Sandbox Reserved 1700 through Sandbox Reserved 1729.
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Metabotropic Glutamate Receptor 2

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