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= Clinical Relevance =
= Clinical Relevance =
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MRGPRX2 initiates IgE-mediated anaphylactic reactions.<ref name="porebski">DOI: 10.3389/fimmu.2018.03027</ref> MRGPRX2-mediated anaphylactic responses occur more quickly than IgE-mediated responses, but the responses also tended to be more transient.<ref name="porebski"/> Common commercial drugs, like icatibant and cetrorelix, as well as neuromuscular blocking agents activate mast cells through the MRGPRX2 pathway.
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<scene name='90/904324/Mrgprx2/5'>MRGPRX2</scene> initiates IgE-mediated anaphylactic reactions.<ref name="porebski">DOI: 10.3389/fimmu.2018.03027</ref> MRGPRX2-mediated anaphylactic responses occur more quickly than IgE-mediated responses, but the responses also tended to be more transient.<ref name="porebski"/> Common commercial drugs, like icatibant and cetrorelix, as well as neuromuscular blocking agents activate mast cells through the MRGPRX2 pathway.
Many mutations also affect the actions of MRGPRX2. For example, a single residue mutation in sub-pocket 1 (Glu164Arg) prevented interactions between the receptor and ligands like C48/80.<ref name="porebski"/> In addition, single nucleotide polymorphisms (SNPs) have been linked to many variations of MRGPRX2 which predispose patients to hyperactivation of the receptors. Two of the most common SNPs are Asn62Thr which affects the cytoplasmic domain and Asn16His which affects the extracellular domain.<ref name="porebski"/> These mutations have been theorized to potentially protect patients from drug-induced mast cell degranulation and hypersensitivity reactions.
Many mutations also affect the actions of MRGPRX2. For example, a single residue mutation in sub-pocket 1 (Glu164Arg) prevented interactions between the receptor and ligands like C48/80.<ref name="porebski"/> In addition, single nucleotide polymorphisms (SNPs) have been linked to many variations of MRGPRX2 which predispose patients to hyperactivation of the receptors. Two of the most common SNPs are Asn62Thr which affects the cytoplasmic domain and Asn16His which affects the extracellular domain.<ref name="porebski"/> These mutations have been theorized to potentially protect patients from drug-induced mast cell degranulation and hypersensitivity reactions.

Revision as of 23:23, 17 April 2022

Human Itch G-Coupled Protein Receptors

Cryo-EM structure of Gq coupled MRGPRX2.

Drag the structure with the mouse to rotate


Student contributors

Madeline Beck

Joey Gareis

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