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==Introduction==
==Introduction==
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Estrogen receptors are proteins found on and inside of the cell. When activated by estrogen these receptors are important in sexual maturation and gestation. There are two types of estrogen receptors that exist which include nuclear estrogen receptors (ERa and ERb), which are included in the nuclear receptor family of intracellular receptors, and membrane estrogen receptors.
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Estrogen receptors are proteins found on and inside of the cell. When activated by estrogen these receptors are important in sexual maturation and gestation. There are two types of estrogen receptors that exist which include nuclear estrogen receptors (ERα and ERβ), which are included in the nuclear receptor family of intracellular receptors, and membrane estrogen receptors.
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A series of p-hydroxybenzenesulphonamides ERb receptor agonists discovered along with various compounds listed showed selectivity over the ERa receptor. Overall, they found that compound 11 showed better binding conformation determined by X-ray, and presents a better starting point for the journey to find a more selective ERb agonist.
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A series of p-hydroxybenzenesulphonamides ERβ receptor agonists discovered along with various compounds listed showed selectivity over the ERα receptor. Overall, they found that compound 11 showed better binding conformation determined by X-ray, and presents a better starting point for the journey to find a more selective ERβ agonist.
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Looking at the gonadal steroid hormone estradiol,1, action is performed through estrogen subtypes, ERa and ERb. The detrimental effects of ERb in comparison to the proliferative effects ERa are found to inhibit breast and endometrial tissue compared to ERa and could potentially be responsible for the immunomodulatory and neuropharmacalogical behavior of estradiol 1,2. The interest in the therapeutic benefits of selective ERb agonists to combatant various conditions including endometriosis and inflammatory bowel disease.
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Looking at the gonadal steroid hormone estradiol,1, action is performed through estrogen subtypes, ERα and ERβ. The detrimental effects of ERβ in comparison to the proliferative effects ERα are found to inhibit breast and endometrial tissue compared to ERα and could potentially be responsible for the immunomodulatory and neuropharmacalogical behavior of estradiol 1,2. The interest in the therapeutic benefits of selective ERβ agonists to combatant various conditions including endometriosis and inflammatory bowel disease.
This is an overall scene with the beta sheets in purple and the alpha helices in ball and stick figures <scene name='48/483890/Ben_homyak_overall_structure/1'>Overall Structure</scene>
This is an overall scene with the beta sheets in purple and the alpha helices in ball and stick figures <scene name='48/483890/Ben_homyak_overall_structure/1'>Overall Structure</scene>

Revision as of 00:38, 11 April 2016


This Sandbox is Reserved from January 19, 2016, through August 31, 2016 for use for Proteopedia Team Projects by the class Chemistry 423 Biochemistry for Chemists taught by Lynmarie K Thompson at University of Massachusetts Amherst, USA. This reservation includes Sandbox Reserved 425 through Sandbox Reserved 439.


Estrogen receptor beta/p-hydroxybenzene sulfonamide complexes (2yly)[1]

by Benjamin Homyak, Soo Lim Park, Marissa Burgess

Student Projects for UMass Chemistry 423 Spring 2016

p-hydroxybenzenesulphonamides ERb receptor (PDB entry 2yly)

Drag the structure with the mouse to rotate
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