User:Felipe de Melo Santana/Sandbox 1

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You may include any references to papers as in: the use of JSmol in Proteopedia ^[1] or to the article describing Jmol ^[2] to the rescue.

1 General information
2 Structure
3 OxyR activation
4 Protein activity in different forms
5 Purification and crystallization

General information

OxyR is a protein that functions as a transcription factor. The OxyR we are analyzing is that of Escherichia Coli. In this perspective, the protein works by regulating the transcription of specific genes, being sensitive to H2O2. This transcription factor belongs to the LysR family, with 34 kDa, which forms homotetramers. Under this focus, the members of this family present a domain linked to DNA in their N-terminal region, called helix-loop-helix, a central domain responsible for recognizing H2O2 that is sensitive to the regulation signal and, finally, a domain in C-terminal region responsible for activation and mutimerization.

Structure

This protein its a transcription factor, at that time its shows two different structures when its reduced or oxidized. The reduced form monomer of the OxyR regulatory domain consists of two α/β domains that are linked by two interdomain strands. Residues in the middle of a folded domain form the majority of the N-terminal a/b domain. The C-terminal a/b Results and Discussion domain II is made of residues . The remaining C-terminal 30 Structure Determination residues come back to domain I to form an edge of the domain . The two domains exhibit a similar folding pattern consisting of a central b sheet flanked by helices and loops.

OxyR activation

The OxyR transcription factor is activated by the formation of an intramolecular disulfide bond (Zheng et al 1998).

The OxyR activation, by H2O2, begins with the oxidation of the residue into a sulfenic acid intermediate, which causes destabilization of the Cys199 side chain in the hydrophobic binding pocket, due to its increased size and charge. The destabilization leads to expulsion of the side chain of Cys199 out of the interdomain pocket, resulting in a flexible loop around Cys199 (Lee et al 2004).

This change in the regulatory domain of OxyR allows the formation of an intramolecular disulfide bond between Cys199 and Cys208, responsible for keeping OxyR in the active form. Thus, OxyR is deactivated by the reduction of the disulfide bond, that leads OxyR back to its reduced form (Zheng et al. 1998).

Figure 1. Intermediates in the structural transitions of OxyR.

Protein activity in different forms

The OxyR transcription factor regulate the expression of genes involved in redox-homeostasis (Stroz et al. 1990).

OxyR protein is able to DNA-binding in its two different forms, oxidized and reduced. In your oxidized form, OxyR binds to four adjacent major grooves in DNA, while in the reduced form, OxyR binds to two pairs of adjacent major grooves separated by one helical turn (Toledano et al 1994). These two modes of binding allow OxyR to regulate different promoters, under different cell conditions.

Both forms of OxyR act as repressors, regulating its own expression by oxyR transcription repression, while only oxidized OxyR is able to activate gene expression, inducing the expression of oxyS (a small regulatory RNA), hydroperoxidase I (katG), alkyl hydroperoxide reductase (ahpCF), glutathione reductase (gorA), glutaredoxin 1 (grxA) and other genes involved in redox-homeostasis, that protect the cell against oxidative stress (Zheng et al 1998).

Figure 2. Tetrameric Structure and a Plausible Model of DNA Interactions.

The tetramers observed in crystals of the reduced (A) and oxidized (B) forms are shown with the DNA positioned on the tetramers with plausible orientations. The tetramers are shown as ribbons (red, green, blue, and yellow for each monomer) and the model of DNA is represented as helical coils (cyan).

Purification and crystallization

This is a sample scene created with SAT to by Group, and another to make of the protein. You can make your own scenes on SAT starting from scratch or loading and editing one of these sample scenes.

References

Zheng, M., Aslund, F., and Storz, G. (1998). Activation of the OxyR transcription factor by reversible disulfide bond formation. Science 279, 1718–1721.

Choi H, Kim S, Mukhopadhyay P, et al. Structural basis of the redox switch in the OxyR transcription factor. Cell. 2001;105(1):103-113. doi:10.1016/s0092-8674(01)00300-2

Toledano, M.B., Kullik, I., Trinh, F., Baird, P.T., Schneider, T.D., and Storz, G. (1994). Redox-dependent shift of OxyR-DNA contacts along an extended DNA-binding site: a mechanism for differential promoter selection. Cell 78, 897–909.

Storz, G., Tartaglia, L.A., and Ames, B.N. (1990). Transcriptional regulator of oxidative stress-inducible genes: direct activation by oxidation. Science 248, 189–194

Kullik, I., Toledano, M.B., Tartaglia, L.A., and Storz, G. (1995a). Mutational analysis of the redox-sensitive transcriptional regulator OxyR: regions important for oxidation and transcriptional activation. J. Bacteriol. 177, 1275–1284.

Lee C, Lee SM, Mukhopadhyay P, et al. Redox regulation of OxyR requires specific disulfide bond formation involving a rapid kinetic reaction path. Nat Struct Mol Biol. 2004;11(12):1179-1185. doi:10.1038/nsmb856

↑ Hanson, R. M., Prilusky, J., Renjian, Z., Nakane, T. and Sussman, J. L. (2013), JSmol and the Next-Generation Web-Based Representation of 3D Molecular Structure as Applied to Proteopedia. Isr. J. Chem., 53:207-216. doi:http://dx.doi.org/10.1002/ijch.201300024
↑ Herraez A. Biomolecules in the computer: Jmol to the rescue. Biochem Mol Biol Educ. 2006 Jul;34(4):255-61. doi: 10.1002/bmb.2006.494034042644. PMID:21638687 doi:10.1002/bmb.2006.494034042644

Proteopedia Page Contributors and Editors (what is this?)

Felipe de Melo Santana

Retrieved from "http://52.214.119.220/wiki/index.php/User:Felipe_de_Melo_Santana/Sandbox_1"

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-==1I69==
+ŕ==1I69==
 <StructureSection load='1I69' size='340' side='right' caption='Caption for this structure' scene=''>
 This is a default text for your page '''Felipe de Melo Santana/Sandbox 1'''. Click above on '''edit this page''' to modify. Be careful with the &lt; and &gt; signs.
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 == OxyR activation ==
-The OxyR transcription factor is activated by the formation of an intramolecular disulfide bond.
+The OxyR transcription factor is activated by the formation of an intramolecular disulfide bond (Zheng et al 1998).
-The Oxyr activation, by H2O2, begins with the oxidation of the <scene name='84/844928/Cys_199/1'>Cys199</scene> residue into a sulfenic acid intermediate, which causes destabilization of the Cys199 side chain in the hydrophobic binding pocket, due to its increased size and charge. This destabilization lead to expulsion of the side chain of Cys199 out of the interdomain pocket, resulting in a flexible loop around Cys199.
-These changes in the regulatory domain of OxyR allow the formation of an intramolecular disulfide bond between Cys199 and Cys208, separated by 17 Å in reduced form,  which maintain OxyR in the active form.
+The OxyR activation, by H2O2, begins with the oxidation of the <scene name='84/844928/Cys_199/1'>Cys199</scene> residue into a sulfenic acid intermediate, which causes destabilization of the Cys199 side chain in the hydrophobic binding pocket, due to its increased size and charge. The destabilization leads to expulsion of the side chain of Cys199 out of the interdomain pocket, resulting in a flexible loop around Cys199 (Lee et al 2004).
+This change in the regulatory domain of OxyR allows the formation of an intramolecular disulfide bond between Cys199 and Cys208, responsible for keeping OxyR in the active form. Thus, OxyR is deactivated by the reduction of the disulfide bond, that leads OxyR back to its reduced form (Zheng et al. 1998).
 [[Image:Pasted_image_1.png]]
@@ Line 25: / Line 28: @@
 == Protein activity in different forms ==
+The OxyR transcription factor regulate the expression of genes involved in redox-homeostasis (Stroz et al. 1990).
+OxyR protein is able to DNA-binding in its two different forms, oxidized and reduced. In your oxidized form, OxyR binds to four adjacent major grooves in DNA, while in the reduced form, OxyR binds to two pairs of adjacent major grooves separated by one helical turn (Toledano et al 1994). These two modes of binding allow OxyR to regulate different promoters, under different cell conditions.
+Both forms of OxyR act as repressors, regulating its own expression by oxyR transcription repression, while only oxidized OxyR is able to activate gene expression, inducing the expression of oxyS (a small regulatory RNA), hydroperoxidase I (katG), alkyl hydroperoxide reductase (ahpCF), glutathione reductase (gorA), glutaredoxin 1 (grxA) and other genes involved in redox-homeostasis, that protect the cell against oxidative stress (Zheng et al 1998).
-The OxyR transcription factor regulate the expression of genes involved in redox-homeostasis.
-OxyR protein is able to DNA-binding in its two different forms, oxidized and reduced. In your oxidized form, OxyR binds to four adjacent major grooves in DNA, while in the reduced form, OxyR binds to two pairs of adjacent major grooves separated by one helical turn (figure X). These two modes of binding allow OxyR to regulate different promoters, under different cell conditions.
-Both forms of OxyR act as repressors, regulating its own expression by oxyR transcription repression, while only oxidized OxyR is able to activate gene expression, inducing the expression of oxyS, hydroperoxidase I (katG), alkyl hydroperoxide reductase (ahpCF), glutathione reductase (gorA), glutaredoxin 1 (grxA) and other genes involved in redox-homeostasis, that protect the cell against oxidative stress.
 [[Image:Pasted_image_0.png]]

User:Felipe de Melo Santana/Sandbox 1

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Revision as of 21:33, 18 June 2020

Contents

General information

Structure

OxyR activation

Protein activity in different forms

Purification and crystallization

References

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