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This Sandbox is Reserved from Jan 06, 2014, through Aug 22, 2014 for use by the Biochemistry II class at the Butler University at Indianapolis, IN USA taught by R. Jeremy Johnson. This reservation includes Sandbox Reserved 911 through Sandbox Reserved 922.

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Monoglyceride Lipase

Introduction

Image:MGLProt.jpg

Monomer of MGL created in PYMOL (PDB:3PE6)

Monoglyceride Lipase (MGL, MAGL, MGLL) is a 33 kDa protein found mostly in the cell membrane. It is a serine hydrolase enzyme that exhibits an α/β hydrolase fold. In addition, MGL possesses amphitropic character, where the area around the active site of MGL is polar while the site itself is non-polar. This characteristic allows the protein to be present both in the membrane and in the cytosol. MGL plays a key role in the hydrolysis of 2-arachidonoylglycerol (2-AG), an endocannabinoid produced by the the central nervous system. The α/β fold allows 2-AG to selectively bind to the active site and be broken down into arachidonic acid and glycerol. Upon breakdown, glycerol leaves via an "exit tunnel" found perpendicular to the α/β fold. 2-AG itself has been found to possess anti-nociceptive, immunomodulatory, anti-inflammatory and tumor-reductive character when it binds to cannabinoid receptors. Due to the vast medical and therapeutic utility of 2-AG, the inhibition of MGL is a high interest target in pharmaceutical research. ^[1]

Structure

Bertrand, et al, created the first crystal structure of MGL in its . MGL is a part of the α-β hydrolase family of enzymes. This category of proteins contains an eight-stranded beta sheet, specifically containing seven parallel and one antiparallel constituent strand (), surrounded by alpha-helices. ^[1]

MGL has a characteristic lid domain comprised of two large loops that surround . This region of the enzyme is the putative membrane-interacting moiety of the protein, which is consistent with its amphipathic nature and outward-facing hydrophobic residues. It has been proposed that 2-AG and other lipids suspended in the hydrophobic section of the cell membrane associate with this region before entering the active tunnel. Interestingly, MGL’s lid domain may be more flexible than its analogs in other α-β hydrolases, due to the various conformations it assumed in crystallographic studies. ^[1] Currently, there is no consensus about the quaternary arrangement of MGL. Some researchers claim that it is found as a monomer ^[1] ^[2], whereas others believe it to be a physiologically active dimer. ^[3]

MGL contains an active site tunnel roughly 25Å long and 8Å wide residing beneath its lid region. Like its substrate, 2-AG and other monoacylglycerols, the tunnel is largely amphipathic. Hydrophobic residues dominate the tunnel except for the terminal occluded region, which houses the catalytic triad. In its apo form, the catalytic region is not solvent-exposed, unlike the wide opening of the tunnel. ^[1]^[3] A unique structural motif in MGL is a 5Å solvent-exposed hole connecting the exterior to the catalytic site. It is proposed to act as an “exit hole” through which the glycerol product leaves MGL. The fatty acid product, namely arachidonic acid, presumably travels back through the active site tunnel. ^[1]^[2]^[3]

MGL’s serine hydrolase chemistry is executed by a (Ser132-His279-Asp249) and seems to utilize the same mechanism as the much-studied chymotrypsin. In this mechanism, an activated serine nucleophile cleaves the ester bond of the substrate. The subsequent tetrahedral intermediate is stabilized by the , formed by the main-chain nitrogens of Ala61 and Met (or Se-Met) 133.

Biological/Medical Relevance

2-AG activates the same cannabinoid receptors (CB1 and CB2) for both anandamide and the main psychoactive compound found in Cannabis sativa, Δ9-Tetrahydrocannabinol (THC), via retrograde signaling. It is the most abundant endocannabinoid found in the brain, and it is believed to possess analgesic, anti-inflammatory, immunomodulating, neuroprotective, and hypotensive effects, as well as being capable of inhibiting growth of cancer cells in prostate and breast tissue. ^[3]^[4]

Studies have shown that around 85% of 2-AG in the rat brain is metabolized by MGL, while other lipases such as fatty acid amide hydrolase (FAAH) process the remainder of the metabolite (Blankman). This evidence indicates that MGL is the primary enzyme for the metabolism of 2-AG in humans, making it a highly desirable target molecule for the modulation of 2-AG concentration in the body. Most MGL is found in the cell membrane, although it has been discovered in the cytosol as well. (Bertrand, Labar, Schalk) Although the most-studied role of MGL is the degradation of 2-AG in the brain, MGL may also play a role in adipose tissue to complete the hydrolysis of triglycerides into fatty acids and glycerol as well as working in the liver to mobilize triglycerides for secretion. (Labar, Schalk)

Three general MGL inhibitor classes have been observed: noncompetitive, partially irreversible inhibitors such as URB602; irreversible serine-reactive inhibitors such as JZL184 and SAR629 (SAR-629); and cysteine-reactive inhibitors such as N-arachidonoylmaleimide (NAM). (Bertrand) Despite the existence of such compounds, there is a strong demand for the creation of more highly-specific and more potent inhibitors that could be used as anti-pain drugs for their ability to keep 2-AG active in the neuronal synapses. (Labar)

MGL is an enzyme of immense interest for cancer research, with the potential to shed light on the role of fatty acids in malignancy, the varying efficacy of endocannabinoids as anti-cancer agents in different body tissues, and the multifarious influences on the PI-3k/Akt signaling pathway in carcinogenesis.

MGL exerts a twofold influence on cancer growth; endocannabinoids such as 2-AG have been shown to have anti-tumorigenic properties (Labar, Nomura) and a high fatty-acid concentration may play a role in the promotion of cancer aggressiveness and malignancy. One study showed that in aggressive breast, melanoma, ovarian, and prostate cancer cells, MGL activity was higher than in nonaggressive malignant cells. (Nomura) Subsequently, the creation of effective MGL inhibitors may help to treat highly aggressive cancers in addition to their proposed use as analgesics.

Contrary to this evidence, however, a recent study found that in lung, breast, ovary, stomach, and colorectal cancer, MGL expression was reduced. It was found that in addition to the previously-discussed control over the 2-AG degradation and fatty acid synthesis pathways, MGL also interacted with key phospholipids (specifically, the 3-phosphorylated phosphoinositide products of PI-3K) in the PI3K/Akt signaling and tumor growth pathway. In this role, it serves as a negative effector. Indeed, decreased concentrations of MGL were found to increase Akt phosphorylation. (Hong)

Further research into MGL’s role in different body tissues is necessary to more fully elucidate its complex role in cancer pathology. A specific research topic for exploration is MGL’s effect on exogenous cannabinoid medications given to cancer patients as a palliative medication. (Nomura)

References

↑ ^1.0 ^1.1 ^1.2 ^1.3 ^1.4 ^1.5 Bertrand T, Auge F, Houtmann J, Rak A, Vallee F, Mikol V, Berne PF, Michot N, Cheuret D, Hoornaert C, Mathieu M. Structural basis for human monoglyceride lipase inhibition. J Mol Biol. 2010 Feb 26;396(3):663-73. Epub 2009 Dec 3. PMID:19962385 doi:10.1016/j.jmb.2009.11.060
↑ ^2.0 ^2.1 Schalk-Hihi C, Schubert C, Alexander R, Bayoumy S, Clemente JC, Deckman I, Desjarlais RL, Dzordzorme KC, Flores CM, Grasberger B, Kranz JK, Lewandowski F, Liu L, Ma H, Maguire D, Macielag MJ, McDonnell ME, Haarlander TM, Miller R, Milligan C, Reynolds C, Kuo LC. Crystal structure of a soluble form of human monoglyceride lipase in complex with an inhibitor at 1.35 A resolution. Protein Sci. 2011 Feb 3. doi: 10.1002/pro.596. PMID:21308848 doi:10.1002/pro.596
↑ ^3.0 ^3.1 ^3.2 ^3.3 Labar G, Bauvois C, Borel F, Ferrer JL, Wouters J, Lambert DM. Crystal structure of the human monoacylglycerol lipase, a key actor in endocannabinoid signaling. Chembiochem. 2010 Jan 25;11(2):218-27. PMID:19957260 doi:10.1002/cbic.200900621
↑ Nomura DK, Lombardi DP, Chang JW, Niessen S, Ward AM, Long JZ, Hoover HH, Cravatt BF. Monoacylglycerol lipase exerts dual control over endocannabinoid and fatty acid pathways to support prostate cancer. Chem Biol. 2011 Jul 29;18(7):846-56. doi: 10.1016/j.chembiol.2011.05.009. PMID:21802006 doi:http://dx.doi.org/10.1016/j.chembiol.2011.05.009

Retrieved from "http://52.214.119.220/wiki/index.php/Sandbox_Reserved_919"

@@ Line 20: / Line 20: @@
 MGL contains an active site tunnel roughly 25Å long and 8Å wide residing beneath its lid region.  Like its substrate, 2-AG and other [http://en.wikipedia.org/wiki/Monoglyceride monoacylglycerols], the tunnel is largely amphipathic. Hydrophobic residues dominate the tunnel except for the terminal occluded region, which houses the [http://en.wikipedia.org/wiki/Catalytic_triad#Ser-His-Asp catalytic triad].  In its apo form, the catalytic region is not solvent-exposed, unlike the wide opening of the tunnel. <ref name="bert" /><ref name="labar" /> A unique structural motif in MGL is a 5Å solvent-exposed hole connecting the exterior to the catalytic site. It is proposed to act as an “exit hole” through which the glycerol product leaves MGL. The fatty acid product, namely arachidonic acid, presumably travels back through the active site tunnel. <ref name="bert" /><ref name="shalk" /><ref name="labar" />
-===Active Site===
+MGL’s serine hydrolase chemistry is executed by a <scene name='57/573134/Catalytic_triad/3'>Catalytic Triad</scene> (Ser132-His279-Asp249) and seems to utilize the same mechanism as the much-studied [http://en.wikipedia.org/wiki/Chymotrypsin chymotrypsin]. In this mechanism, an activated serine nucleophile cleaves the ester bond of the substrate. The subsequent tetrahedral intermediate is stabilized by the <scene name='57/573134/Oxyanion_hole/2'>Oxyanion Hole</scene>, formed by the main-chain nitrogens of Ala61 and Met (or Se-Met) 133.
-<scene name='57/573133/Ligand_showing/1'>Ligand Bound</scene>
-<p><scene name='57/573134/Catalytic_triad/2'>Catalytic Triad</scene></p>
-<p><scene name='57/573134/Oxyanion_hole/1'>Oxyanion Hole</scene></p>
+==Biological/Medical Relevance==
+-AG activates the same cannabinoid receptors (CB1 and CB2) for both [http://en.wikipedia.org/wiki/Anandamide anandamide] and the main psychoactive compound found in Cannabis sativa, [http://en.wikipedia.org/wiki/Tetrahydrocannabinol Δ9-Tetrahydrocannabinol] (THC), via [http://en.wikipedia.org/wiki/Retrograde_signaling retrograde signaling]. It is the most abundant endocannabinoid found in the brain, and it is believed to possess analgesic, anti-inflammatory, immunomodulating, neuroprotective, and hypotensive effects, as well as being capable of inhibiting growth of cancer cells in prostate and breast tissue. <ref name="labar" /><ref name="nomura"> PMID:21802006 </ref>
+Studies have shown that around 85% of 2-AG in the rat brain is metabolized by MGL, while other lipases such as [http://en.wikipedia.org/wiki/Fatty_acid_amide_hydrolase fatty acid amide hydrolase] (FAAH) process the remainder of the metabolite (Blankman). This evidence indicates that MGL is the primary enzyme for the metabolism of 2-AG in humans, making it a highly desirable target molecule for the modulation of 2-AG concentration in the body. Most MGL is found in the cell membrane, although it has been discovered in the cytosol as well. (Bertrand, Labar, Schalk) Although the most-studied role of MGL is the degradation of 2-AG in the brain, MGL may also play a role in adipose tissue to complete the hydrolysis of triglycerides into fatty acids and glycerol as well as working in the liver to mobilize triglycerides for secretion. (Labar, Schalk)
+Three general MGL inhibitor classes have been observed: noncompetitive, partially irreversible inhibitors such as [http://en.wikipedia.org/wiki/URB602 URB602]; irreversible serine-reactive inhibitors such as [http://en.wikipedia.org/wiki/JZL184 JZL184] and SAR629 (SAR-629); and cysteine-reactive inhibitors such as [http://www.chemspider.com/Chemical-Structure.24774833.html N-arachidonoylmaleimide] (NAM). (Bertrand) Despite the existence of such compounds, there is a strong demand for the creation of more highly-specific and more potent inhibitors that could be used as anti-pain drugs for their ability to keep 2-AG active in the neuronal synapses. (Labar)
+MGL is an enzyme of immense interest for cancer research, with the potential to shed light on the role of fatty acids in malignancy, the varying efficacy of endocannabinoids as anti-cancer agents in different body tissues, and the multifarious influences on the PI-3k/Akt signaling pathway in [http://en.wikipedia.org/wiki/Carcinogenesis carcinogenesis].
+MGL exerts a twofold influence on cancer growth; endocannabinoids such as 2-AG have been shown to have anti-tumorigenic properties (Labar, Nomura) and a high fatty-acid concentration may play a role in the promotion of cancer aggressiveness and malignancy. One study showed that in aggressive breast, melanoma, ovarian, and prostate cancer cells, MGL activity was higher than in nonaggressive malignant cells. (Nomura) Subsequently, the creation of effective MGL inhibitors may help to treat highly aggressive cancers in addition to their proposed use as analgesics.
+Contrary to this evidence, however, a recent study found that in lung, breast, ovary, stomach, and colorectal cancer, MGL expression was reduced. It was found that in addition to the previously-discussed control over the 2-AG degradation and fatty acid synthesis pathways, MGL also interacted with key phospholipids (specifically, the 3-phosphorylated phosphoinositide products of PI-3K) in the [http://en.wikipedia.org/wiki/PI3K/AKT/mTOR_pathway PI3K/Akt signaling and tumor growth pathway]. In this role, it serves as a negative effector. Indeed, decreased concentrations of MGL were found to increase [http://en.wikipedia.org/wiki/AKT Akt] phosphorylation. (Hong)
+Further research into MGL’s role in different body tissues is necessary to more fully elucidate its complex role in cancer pathology. A specific research topic for exploration is MGL’s effect on exogenous cannabinoid medications given to cancer patients as a palliative medication. (Nomura)
 </StructureSection>
 ===References===
 {{reflist}}

Sandbox Reserved 919

From Proteopedia

Revision as of 19:07, 3 April 2014

Monoglyceride Lipase

Introduction

Structure

Biological/Medical Relevance

References

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