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Acyl-Coenzyme Cholesterol Acetyltransferase (ACAT)

1 Introduction
2 Structural Overview
- 2.1 Tunnels
3 Active Site
4 Mechanism
5 Inhibitor
6 Diseases
- 6.1 Neurodegenerative Diseases and Cancers
- 6.2 Alzheimer's Disease

Introduction

Acyl-Coenzyme A Cholesterol Acyltransferase (), or also known as Sterol O-Acyltransferase (SOAT), is an important enzyme in the body. Cholesterol esters were found in arterial lesions in 1910, but the first ACAT activity was discovered in the mid 1900's. This led to the inhibition of ACAT as being looked at as a possible strategy of preventing or treating atherosclerosis. Between 1980-1995, the interest in ACAT inhibitors grew, but some of the compounds looked at exhibited toxicity. As they were looking into the function of the ACAT1 gene, ACAT2 was discovered. In 1993, an ACAT gene was successfully cloned. This discovery led to more studies with ACAT and atherosclerosis. Some of these studies used mice and showed cellular toxicity. ACAT inhibition is still being looked into as a strategy for treatment or prevention of atherosclerosis and related diseases. ^[1]

Figure 1. Mechanism overview for Acyltransferase of ACAT1

ACAT is an important enzyme that catalyzes the esterification of cholesterol to form cholesterol esters, and it belongs to the class of enzymes called acyltransferases. It is also a member of the MBOAT family because it is key in lipid metabolism. This enzyme is biologically important because it affects the solubility of cholesterol in the cell membrane and promotes accumulation of cholesterol ester in the cytoplasm as fat droplets. Accumulation of cholesterol ester as these lipid droplets is a main characteristic of macrophage foaming, which can lead to atherosclerotic diseases ^[2].

Structural Overview

ACAT was experimentally determined as a tetramer, yet is functionally active as a dimer. This is about 260 kDa and is composed of helices and loops, with each monomer containing 9 transmembrane helices (Figure 3). The was found to be the active arrangement.

Figure 2. The grey shaded region illustrates the lipid bilayer, oriented with the lumen side upward and cytosolic side on the bottom. The tunnels allowing access to the catalytic site are labeled

The is mobile and mostly hydrophobic, and the residues interact in a shape-complementary manner. It was also found that the reaction chamber is shielded by a lid from the cytosolic side, which leads to low catalytic activity. The binding of acyl-CoA and cholesterol induce conformational changes that activate the tunnels. Work is still being done to fully determine the mechanism of this reaction, but this is the proposed pathway.

Figure 3. Monomer in the Membrane. This shows the 9 transmembrane helices. Each helix is labeled and colored according to the different domains. The ligand is shown as ball and stick.

Tunnels

The catalytic site is accessed through three different tunnels that lead from the center catalytic domain of the monomer, to the [lumen], cytosol, and transmembrane space. The tunnels allow the entrance of reactants into the acyl transferase mechanism and the exit of the products to the correct location depending on their function.^[3] The is open to the cytosolic side of the protein in which the Acyl CoA enters into the catalytic domain. The is the transmembrane tunnel in which the cholesterol enters into the catalytic domain space. Important of the T tunnel include Arg262, Phe263, and Leu306. These residues are important for the proper entrance and orientation of the cholesterol to allow for its deprotonation in the mechanism. Upon mutation of these residues, the tunnel function was inhibited.^[4] The is used for the cholesterol ester product to be able to leave the lumen of the cell yet this exit mechanism is still unknown in addition to the cholesterol leaving to the transmembrane space through the T tunnel. The cholesterol enters through the T tunnel while the acyl-CoA enters through the C tunnel. The reaction is catalyzed at the intersection of the two tunnels, where the His460 residue is located. The CoASH is released to the cytosol from the C tunnel, but the cholesterol ester either exits from the T tunnel to the membrane or through the L tunnel to the lumen.^[5]

Active Site

The catalytic site contains that are essential to the mechanism of the ACAT1 mechanism. These residues include His460 to function as a base catalyst and Asn421 which functions as transition state stabilization with hydrogen bonding. Also important for orientation of the Acyl CoA ligand is the presence of hydrophobic residues to stabilize the fatty acid (Trp407,Trp420). The active site is at the intersection of all three tunnels to allow a central position for the acyltransferase to occur. The H460 is positioned to deprotonate the cholesterol upon entering through the T tunnel: Acyl CoA upon entering is positioned to where the sulfur bonded to the carboxyl carbon is at the direct intersection of the T tunnel into the active site.

Mechanism

The mechanism of the [acyltransferace]reaction occurs in the catalytic site one of the monomers in the dimer of ACAT1. The T tunnel and and C tunnel converge to the same space to allow the proper orientation of the Acyl CoA and the incoming cholesterol from the transmembrane. The Acyl CoA is oriented in a way to allow the His460 to act as a base catalyst to begin the reaction by deprotonation of the cholesterol which allows it to attack the carbonyl carbon which breaks the sulfur carbonyl bond (figure 2). The Acyl CoA is held in place by the of Asn 421. This mechanism produces Acyl-CoASH and cholesteryl ester. The Acyl-CcASH leaves through the C tunnel to the cytosol.

Figure 4: Acyltransferase mechanism of ACAT1 with conserved MBOAT family catalytic residues.

Inhibitor

is known as a small molecule inhibitor that is part of the fatty acyl amide analog family, and functions as a competitive inhibitor of Acyl-CoA ^[6]^[7]. Guan discussed that this inhibitor in previous studies had shown that CI-976 reduced the size of atherosclerotic plaques and cholesterol levels in plasma ^[7] .

The illustrates how CI-976 can act as a competitive inhibitor of Acyl-CoA. Structurally, Acyl-CoA and CI-976 are both largely hydrophobic, each with long hydrophobic tails. As evident in this image, the hydrophobic tail of CI-976, mimics that of Acyl-CoA. This allows for the CI-976 inhibitor to be recognized by ACAT1 and to bind tightly in the active site pocket, blocking Acyl-CoA from binding, thus rendering ACAT1 unable to perform its reaction.

Figure 5. CI-976 Inhibitor

Diseases

Neurodegenerative Diseases and Cancers

ACAT1 is involved in diseases such as Alzheimer's Disease and Parkinson’s Disease and other neurodegenerative diseases due to the accumulation of Aβ plaques in the brain. After research on glioma, prostate cancer, pancreatic cancer, leukemia, and breast cancer, it has been noted that ACAT1 plays a role in the progression of cancer over time. Recently, it was discovered that there was a significant increase in ACAT1 expression in ovarian cancer cell lines ^[8]. ACAT-2 is believed to be upregulated in Nephrotic Syndrome which can lead to cardiovascular disease and renal diseases ^[9]. Because of ACAT1's activity in tissues such as the aorta, intestine, and liver, it plays a role in atherosclerosis. Studies have shown that the inhibition of ACAT2 can slow the progression of Atherosclerosis ^[10]. Guan discussed a previous study which found that CI-976 decreased the size of atherosclerosis plaques and the overall concentration of cholesterol in the blood plasma of animals that had been fed a high cholesterol diet ^[7]

Alzheimer's Disease

Alzheimer's Diseaseis a neurodegenerative disease characterized by accumulation of extracellular plaques that cause interferences with memory retrieval. These plaques are made up of Amyloid Beta (Aβ) peptides which are products of the cleavage of Human Amyloid-Beta Precursor Protein (hAPP) ^[6] ^[11]. Within the cells, there is an accumulation of hyperphosphorylated Tau protein. Research has shown that the concentration of cholesterol within cells can affect the production of Aβ ^[6]. As the concentration of cholesterol in the endoplasmic reticulum of neurons increases, hAPP is downregulated ^[6]. Inhibition of ACAT1 would lead to higher concentrations of cholesterol in the cells, signaling downregulation of hAPP. Less hAPP available decreases the amount of Aβ peptides being produced which then reduces the available Aβ peptides that form the extracellular plaques associated with Alzheimer's Disease ^[6] ^[11].

References

ACAT article ^[12] SOAT Article ^[13]

↑ Farese RV Jr. The nine lives of ACAT inhibitors. Arterioscler Thromb Vasc Biol. 2006 Aug;26(8):1684-6. doi:, 10.1161/01.ATV.0000227511.35456.90. PMID:16857957 doi:http://dx.doi.org/10.1161/01.ATV.0000227511.35456.90
↑ Qian H, Zhao X, Yan R, Yao X, Gao S, Sun X, Du X, Yang H, Wong CCL, Yan N. Structural basis for catalysis and substrate specificity of human ACAT1. Nature. 2020 May;581(7808):333-338. doi: 10.1038/s41586-020-2290-0. Epub 2020 May, 13. PMID:32433614 doi:http://dx.doi.org/10.1038/s41586-020-2290-0
↑ Qian H, Zhao X, Yan R, Yao X, Gao S, Sun X, Du X, Yang H, Wong CCL, Yan N. Structural basis for catalysis and substrate specificity of human ACAT1. Nature. 2020 May;581(7808):333-338. doi: 10.1038/s41586-020-2290-0. Epub 2020 May, 13. PMID:32433614 doi:http://dx.doi.org/10.1038/s41586-020-2290-0
↑ Qian H, Zhao X, Yan R, Yao X, Gao S, Sun X, Du X, Yang H, Wong CCL, Yan N. Structural basis for catalysis and substrate specificity of human ACAT1. Nature. 2020 May;581(7808):333-338. doi: 10.1038/s41586-020-2290-0. Epub 2020 May, 13. PMID:32433614 doi:http://dx.doi.org/10.1038/s41586-020-2290-0
↑ Qian H, Zhao X, Yan R, Yao X, Gao S, Sun X, Du X, Yang H, Wong CCL, Yan N. Structural basis for catalysis and substrate specificity of human ACAT1. Nature. 2020 May;581(7808):333-338. doi: 10.1038/s41586-020-2290-0. Epub 2020 May, 13. PMID:32433614 doi:http://dx.doi.org/10.1038/s41586-020-2290-0
↑ ^6.0 ^6.1 ^6.2 ^6.3 ^6.4 Guan C, Niu Y, Chen SC, Kang Y, Wu JX, Nishi K, Chang CCY, Chang TY, Luo T, Chen L. Structural insights into the inhibition mechanism of human sterol O-acyltransferase 1 by a competitive inhibitor. Nat Commun. 2020 May 18;11(1):2478. doi: 10.1038/s41467-020-16288-4. PMID:32424158 doi:http://dx.doi.org/10.1038/s41467-020-16288-4
↑ ^7.0 ^7.1 ^7.2 Guan C, Niu Y, Chen SC, Kang Y, Wu JX, Nishi K, Chang CCY, Chang TY, Luo T, Chen L. Structural insights into the inhibition mechanism of human sterol O-acyltransferase 1 by a competitive inhibitor. Nat Commun. 2020 May 18;11(1):2478. doi: 10.1038/s41467-020-16288-4. PMID:32424158 doi:http://dx.doi.org/10.1038/s41467-020-16288-4
↑ Ayyagari VN, Wang X, Diaz-Sylvester PL, Groesch K, Brard L. Assessment of acyl-CoA cholesterol acyltransferase (ACAT-1) role in ovarian cancer progression-An in vitro study. PLoS One. 2020 Jan 24;15(1):e0228024. doi: 10.1371/journal.pone.0228024., eCollection 2020. PMID:31978092 doi:http://dx.doi.org/10.1371/journal.pone.0228024
↑ Vaziri ND, Liang KH. Acyl-coenzyme A:cholesterol acyltransferase inhibition ameliorates proteinuria, hyperlipidemia, lecithin-cholesterol acyltransferase, SRB-1, and low-denisty lipoprotein receptor deficiencies in nephrotic syndrome. Circulation. 2004 Jul 27;110(4):419-25. doi: 10.1161/01.CIR.0000136023.70841.0F. , Epub 2004 Jul 19. PMID:15262831 doi:http://dx.doi.org/10.1161/01.CIR.0000136023.70841.0F
↑ Willner EL, Tow B, Buhman KK, Wilson M, Sanan DA, Rudel LL, Farese RV Jr. Deficiency of acyl CoA:cholesterol acyltransferase 2 prevents atherosclerosis in apolipoprotein E-deficient mice. Proc Natl Acad Sci U S A. 2003 Feb 4;100(3):1262-7. doi: 10.1073/pnas.0336398100., Epub 2003 Jan 21. PMID:12538880 doi:http://dx.doi.org/10.1073/pnas.0336398100
↑ ^11.0 ^11.1 Shibuya Y, Chang CC, Chang TY. ACAT1/SOAT1 as a therapeutic target for Alzheimer's disease. Future Med Chem. 2015;7(18):2451-67. doi: 10.4155/fmc.15.161. Epub 2015 Dec 15. PMID:26669800 doi:http://dx.doi.org/10.4155/fmc.15.161
↑ Qian H, Zhao X, Yan R, Yao X, Gao S, Sun X, Du X, Yang H, Wong CCL, Yan N. Structural basis for catalysis and substrate specificity of human ACAT1. Nature. 2020 May;581(7808):333-338. doi: 10.1038/s41586-020-2290-0. Epub 2020 May, 13. PMID:32433614 doi:http://dx.doi.org/10.1038/s41586-020-2290-0
↑ Guan C, Niu Y, Chen SC, Kang Y, Wu JX, Nishi K, Chang CCY, Chang TY, Luo T, Chen L. Structural insights into the inhibition mechanism of human sterol O-acyltransferase 1 by a competitive inhibitor. Nat Commun. 2020 May 18;11(1):2478. doi: 10.1038/s41467-020-16288-4. PMID:32424158 doi:http://dx.doi.org/10.1038/s41467-020-16288-4

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@@ Line 35: / Line 35: @@
 ==Inhibitor==
-The <scene name='87/877626/Overlay/10'>overlay</scene> illustrates the competitive inhibition of Acetyl-CoA and the inhibitor CI-976. Structurally, Acetyl-CoA and CI-976 are both largely hydrophobic, each with long hydrophobic tails and aromatic heads. As evident in this image, the hydrophobic tail of CI-976, mimics that of Acetyl-CoA. This allows for the inhibitor to be recognized by ACAT and to bind tightly in the active site pocket, blocking Acetyl-CoA from binding, thus rendering ACAT unable to perform its reaction. [[Image: CI-976_chemdraw.jpg|300 px|right|thumb|Figure 5. CI-976 Inhibitor]]
+<scene name='87/877626/Inhibitor/7'>CI-976</scene> is known as a small molecule inhibitor that is part of the fatty acyl amide analog family, and functions as a competitive inhibitor of Acyl-CoA <ref name "Shengcheng">PMID:32424158</ref><ref name="Guan"> doi:10.1038/s41467-020-16288-4</ref>. Guan discussed that this inhibitor in previous studies had shown that CI-976 reduced the size of atherosclerotic plaques and cholesterol levels in plasma <ref name="Guan"> doi:10.1038/s41467-020-16288-4</ref> .
+The <scene name='87/877626/Overlay/13'>overlay</scene> illustrates how CI-976 can act as a competitive inhibitor of Acyl-CoA. Structurally, Acyl-CoA and CI-976 are both largely hydrophobic, each with long hydrophobic tails. As evident in this image, the hydrophobic tail of CI-976, mimics that of Acyl-CoA. This allows for the CI-976 inhibitor to be recognized by ACAT1 and to bind tightly in the active site pocket, blocking Acyl-CoA from binding, thus rendering ACAT1 unable to perform its reaction. [[Image: CI-976_chemdraw.jpg|300 px|right|thumb|Figure 5. CI-976 Inhibitor]]
+==Diseases==
+===Neurodegenerative Diseases and Cancers===
+ACAT1 is involved in diseases such as [https://www.mayoclinic.org/diseases-conditions/alzheimers-disease/symptoms-causes/syc-20350447 Alzheimer's Disease] and [https://www.mayoclinic.org/diseases-conditions/parkinsons-disease/symptoms-causes/syc-20376055 Parkinson’s Disease] and other neurodegenerative diseases due to the accumulation of Aβ plaques in the brain. After research on [https://www.mayoclinic.org/diseases-conditions/glioma/symptoms-causes/syc-20350251 glioma], [https://www.mayoclinic.org/diseases-conditions/prostate-cancer/symptoms-causes/syc-20353087 prostate cancer], [https://www.mayoclinic.org/diseases-conditions/pancreatic-cancer/symptoms-causes/syc-20355421 pancreatic cancer], [https://www.mayoclinic.org/diseases-conditions/leukemia/symptoms-causes/syc-20374373 leukemia], and [https://www.mayoclinic.org/diseases-conditions/breast-cancer/symptoms-causes/syc-20352470 breast cancer], it has been noted that ACAT1 plays a role in the progression of cancer over time. Recently, it was discovered that there was a significant increase in ACAT1 expression in ovarian cancer cell lines <ref name="Ayyagari"> doi:10.1371/journal.pone.0228024</ref>. ACAT-2 is believed to be upregulated in Nephrotic Syndrome which can lead to cardiovascular disease and renal diseases <ref name="Vaziri"> doi:10.1161/01.CIR.0000136023.70841.0F</ref>. Because of ACAT1's activity in tissues such as the aorta, intestine, and liver, it plays a role in atherosclerosis. Studies have shown that the inhibition of ACAT2 can slow the progression of Atherosclerosis <ref name="Willner"> doi:10.1073/pnas.0336398100</ref>. Guan discussed a previous study which found that CI-976 decreased the size of atherosclerosis plaques and the overall concentration of cholesterol in the blood plasma of animals that had been fed a high cholesterol diet <ref name="Guan"> doi:10.1038/s41467-020-16288-4</ref>
-===Disease===
+===Alzheimer's Disease===
-==Alzheimer's Disease==
+[https://www.mayoclinic.org/diseases-conditions/alzheimers-disease/symptoms-causes/syc-20350447 Alzheimer's Disease]is a neurodegenerative disease characterized by accumulation of extracellular plaques that cause interferences with memory retrieval. These plaques are made up of [https://en.wikipedia.org/wiki/Amyloid_beta Amyloid Beta] (Aβ) peptides which are products of the cleavage of [https://en.wikipedia.org/wiki/Amyloid-beta_precursor_protein#:~:text=Amyloid%2Dbeta%20precursor%20protein%20(APP,antimicrobial%20activity%2C%20and%20iron%20export. Human Amyloid-Beta Precursor Protein] (hAPP) <ref name "Chang">doi:10.1002/iub.305</ref> <ref name="Shibuya"> PMID:26669800</ref>. Within the cells, there is an accumulation of hyperphosphorylated [https://en.wikipedia.org/wiki/Tau_protein Tau] protein. Research has shown that the concentration of cholesterol within cells can affect the production of Aβ <ref name "Chang">doi:10.1002/iub.305</ref>. As the concentration of cholesterol in the endoplasmic reticulum of neurons increases, hAPP is downregulated <ref name "Chang">doi:10.1002/iub.305</ref>. Inhibition of ACAT1 would lead to higher concentrations of cholesterol in the cells, signaling downregulation of hAPP. Less hAPP available decreases the amount of Aβ peptides being produced which then reduces the available Aβ peptides that form the extracellular plaques associated with Alzheimer's Disease <ref name "Chang">doi:10.1002/iub.305</ref> <ref name="Shibuya"> PMID:26669800</ref>.
-Alzheimer's Disease is a neurodegenerative disease characterized by accumulation of extracellular plaques that cause interferences with memory retrieval. These plaques are made up of amyloid beta (Aβ) peptides which are products of the cleavage of human Amyloid Precursor Protein (hAPP) <ref name "Chang">doi:10.1002/iub.305</ref> <ref name="Shibuya"> PMID:26669800</ref>. Within the cells, there is an accumulation of hyperphosphorylated tau <ref name "Chang">doi:10.1002/iub.305</ref> <ref name="Shibuya"> PMID:26669800</ref>. Research has shown that the concentration of cholesterol within cells can affect the production of Aβ <ref name "Chang">doi:10.1002/iub.305</ref> <ref name="Shibuya"> PMID:26669800</ref>. As the concentration of cholesterol in the endoplasmic reticulum of neurons increases, hAPP is downregulated <ref name "Chang">doi:10.1002/iub.305</ref><ref name="Shibuya"> PMID:26669800</ref>. Inhibition of ACAT1 would lead to higher concentrations of cholesterol in the cells, signaling downregulation of hAPP. Less hAPP available decreases the amount of Aβ peptides being produced and decreases the available Aβ peptides that could form the extracellular plaques associated with Alzheimer's Disease <ref name "Chang">doi:10.1002/iub.305</ref> <ref name="Shibuya"> PMID:26669800</ref>.
-==Other Diseases==
-ACAT is also involved in diseases such as Parkinson’s and other neurodegenerative diseases due to the accumulation of Aβ plaques in the brain. After research on glioma, prostate, pancreatic, leukemia, and breast cancers, it has been noted that ACAT plays a role in the progression of cancer over time. Recently, Ayyagari et al. found that there was a significant increase in ACAT-1 expression in ovarian cancer cell lines <ref name="Ayyagari"> doi:10.1371/journal.pone.0228024</ref>. ACAT-2 is believed to be upregulated in Nephrotic Syndrome (NS) which can lead to cardiovascular disease and renal diseases <ref name="Vaziri"> doi:10.1161/01.CIR.0000136023.70841.0F</ref>. Because of ACAT's activity in tissues such as the aorta, intestine, and liver, it plays a role in Atherosclerosis <ref name="Willner"> doi:10.1073/pnas.0336398100</ref>. Studies have shown that the inhibition of ACAT-2 can slow the progression of Atherosclerosis <ref name="Willner"> doi:10.1073/pnas.0336398100</ref>.