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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

1 Introduction
2 Overall Structure
3 Binding Interactions
4 See Also
5 Credits
6 References

Introduction

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.

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.

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

Here is another scene with a rainbow diagram description of the whole molecule

Overall Structure

The assembly composition of the 2yly protein is a homodimer. (Quaternary structure)

The DNA Binding domain is located in the C region, which is highly conserved. The ligand binding domain is located at the C terminus in the E and F regions. The ligand binding domain is often called the “three-layered anti-parallel α helical sandwich” because it contains 12 alpha helices along with one beta hairpin. Sites for dimerization and nuclear localization are located in the the D region, which is poorly conserved. Both ERα and ERβ have several splice variants, with ERα having over 20 and ERβ having 5.

The 2yly protein's secondary structure consists of mostly alpha helices (148 residues) and only two beta strands (6 residues) on the outside of the receptor shown below with the alpha helices showing polar and non-polar parts of the chain. The beta sheets are shown in yellow in the second green scene.

- , and

- Tertiary Structure

- Polar- Pink, Hydrophobic- Grey

- Surface groups (orange) vs. Buried groups (blue)

Binding Interactions

Among the series of p-hydroxybenzene sulfonamide ERβ receptor agonists discovered, protein 2yly has been identified for great selectivity over the related ERα receptor. Protein 2yly was originally designed to form an interaction with the His 475 through the tertiary hydroxyl group. However, the hydroxyl group serves as a conformational lock to form an internal hydrogen bond with the about 2.3 Å apart.^[1]

Internally packed against the phenyl group is the cyclopropyl group with large (shown in gray) between Ile 373 and both the benzyl and chiral methyl groups. The sulphonamide oxygens come in close contact with Met 336 and the benzyl group of the ligand comes near His 475 but there are no coulombic interactions formed. Depending on the functional group placed either next to the tertiary hydroxyl group or on the benzyl ring, further Van der Waals interactions can be seen within the lipophilic pocket. In other words, depending on the polarity of the group attached to the sulphonamide, interactions with His 475 will be varied.

Credits

Introduction - Benjamin Homyak

Overall Structure - Marissa Burgess

Drug Binding Site - Soo Lim Park

References

↑ Roberts LR, Armor D, Barker C, Bent A, Bess K, Brown A, Favor DA, Ellis D, Irving SL, MacKenny M, Phillips C, Pullen N, Stennett A, Strand L, Styles M. Sulfonamides as selective oestrogen receptor beta agonists. Bioorg Med Chem Lett. 2011 Oct 1;21(19):5680-3. Epub 2011 Aug 16. PMID:21885279 doi:10.1016/j.bmcl.2011.08.041

Retrieved from "http://52.214.119.220/wiki/index.php/Sandbox_Reserved_433"

@@ Line 11: / Line 11: @@
 ==Introduction==
-(Some sections below taken from primary paper) Further introduction for estrogen receptors later and why useful
+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.
-- "The gonadal steroid hormone estradiol, 1, exerts genomic actions through two oestrogen receptor subtypes, ERa and ERb. Emerging evidence has suggested that the function of ERb in contrast to ERa, potentially counteracts the proliferative effects of ERa on breast and endometrial tissue as well as being potentially responsible for the immunomodulatory as well as neuropharmacological behaviour of estradiol 1,2 There has been signiﬁcant interest in the potential therapeutic beneﬁt of selective ERb agonists to treat a variety of conditions including endometriosis3 and inﬂammatory bowel disease."
+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.
+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.
-- A series of p-hydroxybenzenesulphonamides ERb receptor agonists were discovered and several compounds identiﬁed had excellent selectivity over the related ERa receptor. One of these, compound 11, had an interesting binding conformation determined by X-ray and represents an excellent starting point in the quest for further selective ERb agonists.
-- There has been signiﬁcant interest in the potential therapeutic beneﬁt of selective ERb agonists to treat a variety of conditions including endometriosis3 and inﬂammatory bowel disease
-- The amino acid sequence of the ligand binding domains between ERa and ERb is very highly conserved with only minor differences; Leu384 and Met421 in ERa is replaced by Met336 and Ile373 in ERb. The overall molecule is shown here with the <scene name='48/483890/Met336_and_ile373_in_erb/1'>Met336 and Ile373</scene> in ERb in blue to show their location.
-. The amines were either purchased commercially or made via addition of a primary amine to an epoxide as shown in Scheme
-. The compounds were tested as racemates and those of interest were separated by chiral HPLC. A wide range of analogues were prepared utilising the approach described.
 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>
@@ Line 29: / Line 21: @@
 Here is another scene with a rainbow diagram description of the whole molecule
 <scene name='48/483890/2yly_overall_diagram/3'>Rainbow diagram</scene>
-Further scenes will be put in regarding more in depth focus on the estrogen receptor
 ==Overall Structure==
+The assembly composition of the 2yly protein is a homodimer. (Quaternary structure)
-- Secondary Structure
+The DNA Binding domain is located in the C region, which is highly conserved. The ligand binding domain is located at the C terminus in the E and F regions. The ligand binding domain is often called the “three-layered anti-parallel α helical sandwich” because it contains 12 alpha helices along with one beta hairpin. Sites for dimerization and nuclear localization are located in the the D region, which is poorly conserved. Both ERα and ERβ have several splice variants, with ERα having over 20 and ERβ having 5.
-- Mostly alpha helices with only two beta strands on the outside of the receptor shown below with the apla helices showing pollar and non-polar parts of the chain. The beta sheets are shown in yellow in the second green scene
+The 2yly protein's secondary structure consists of mostly alpha helices (148 residues) and only two beta strands (6 residues) on the outside of the receptor shown below with the alpha helices showing polar and non-polar parts of the chain. The beta sheets are shown in yellow in the second green scene.
 - <scene name='48/483890/2yly_alpha_helicies/1'>Alpha Helices</scene>, and <scene name='48/483890/2yly_beta_sheets/1'>Beta Sheets</scene>
@@ Line 49: / Line 39: @@
 ==Binding Interactions==
-- Complexes were originally designed to form an interaction with the His475 through the tertiary hydroxyl group
+Among the series of p-hydroxybenzene sulfonamide ERβ receptor agonists discovered, protein 2yly has been identified for great selectivity over the related ERα receptor. Protein 2yly was originally designed to form an interaction with the His 475 through the tertiary hydroxyl group. However, the hydroxyl group serves as a conformational lock to form an internal hydrogen bond with the <scene name='48/483890/Soolim_binding/1'>sulphonamide oxygen </scene> about 2.3 Å apart.<sup>[1]</sup>
-- Instead, the hydroxyl group acts as a conformational lock which forms an internal hydrogen bond with the sulphonamide oxygen about 2.3 A apart.
+Internally packed against the phenyl group is the cyclopropyl group with large <scene name='48/483890/Soolim_hydrophobic/1'>hydrophobic interactions</scene> (shown in gray) between Ile 373 and both the benzyl and chiral methyl groups. The sulphonamide oxygens come in close contact with Met 336 and the benzyl group of the ligand comes near His 475 but there are no coulombic interactions formed. Depending on the functional group placed either next to the tertiary hydroxyl group or on the benzyl ring, further Van der Waals interactions can be seen within the lipophilic pocket. In other words, depending on the polarity of the group attached to the sulphonamide, interactions with His 475 will be varied.
-- The sulphonamide oxygens pack against Met336 and the benzyl group at top of the pocket comes near His475 but does not form any coulombic interactions but Van der Waals interactions exist near the pocket.
-- Complexes make H-bonding interactions not only with Arg346 (yellow) and Glu305 (blue) but also His475 (green). Binding sites are shown <scene name='48/483890/2yly_binding2/1'>here</scene>

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

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Introduction

Overall Structure

Binding Interactions

See Also

Credits

References

Views

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Sandbox Reserved 433

From Proteopedia

Current revision

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

Contents

Introduction

Overall Structure

Binding Interactions

See Also

Credits

References

Views

Personal tools

Navigation

Search

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