Sandbox Reserved 1701

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=== Before Activation ===
=== Before Activation ===
The culmination of different motifs observed in MRGPRX2 compared to other class A GPCRs leads to external membrane ligand binding.The MRGPRX2 GPCR undergoes a much smaller conformational change upon ligand binding compared to other Class A GPCRs due to surface level binding versus deep helix binding. This contrast is represented in the photo below to show the unbound and bound transmembrane proteins of MRGPRX2 and 5-HT2A.
The culmination of different motifs observed in MRGPRX2 compared to other class A GPCRs leads to external membrane ligand binding.The MRGPRX2 GPCR undergoes a much smaller conformational change upon ligand binding compared to other Class A GPCRs due to surface level binding versus deep helix binding. This contrast is represented in the photo below to show the unbound and bound transmembrane proteins of MRGPRX2 and 5-HT2A.
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[[Image:Screen Shot 2022-03-282 at 6.59.44 PM.png|300px|center|thumb|Overlay of unbound (transparent) and bound (opaque) transmembrane proteins of both MRGRPX2 (left) and 5-HT2AR (right).]]
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[[Image:Screen Shot 2022-03-282 at 6.59.44 PM.png|500px|center|thumb|Overlay of unbound (transparent) and bound (opaque) transmembrane proteins of both MRGRPX2 (left) and 5-HT2AR (right).]]
=== After Activation ===
=== After Activation ===

Revision as of 00:00, 29 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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MRGPRX2 Human Itch G-Protein Coupled Receptor (GPCR)

Human Itch GPCR Structure. Transmembrane protein shown in red, alpha subunit in blue, beta subunit in magenta, and gamma subunit in yellow.

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