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<Structure load='1SU4' size='350' frame='true' align='right' caption='Insert caption here' scene='Insert optional scene name here' />
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== '''Calcium ATPase''' ==
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<StructureSection load='1SU4' size='350' side='right' caption='3D Structure of the SERCA pump resolved with x-ray cristallography' scene='Insert optional scene name here'>
== Introduction ==
== Introduction ==
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All living organisms depend on P-type ATPase to pump cation across the membrane. They play a fundamental role in their metabolism and physiology. Ca2+ ATPase, a P-type ATPase, transports calcium ions across the membrane against a concentration gradient. These pumps clear cytoplasm of the second messenger, the calcium. It's very important to keep a low concentration of calcium in the cell for a good cell signaling.
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We can found the PMCA (Plasma Membrane Ca2+ ATPase) which remove the calcium from the cell and the SERCA (Sarcoplasmic Endoplasmic Reticulum Ca2+ ATPase) which pumps calcium into the endoplasmic reticulum.
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All living organisms depend on P-type ATPase to pump cations across membranes. P-type ATPases are distinct from other ATPases because there is an autophosphorylation step in their catalytic cycle. They play a fundamental role in organisms metabolism and physiology. Ca2+ ATPase is one type of P-type ATPases which transports calcium ions across membranes against a concentration gradient. These pumps clear the cytoplasm of the calcium, which is a second messenger. It's very important to keep a low concentration of calcium in the cell for a good cell signaling. The hydrolysis of ATP is necessary for the pump's functioning. For each ATP hydrolyzed, it transfers two calcium ions through the membrane, and two or three hydrogen ions in the opposite direction.
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The hydrolysis of one adenosine triphosphate (ATP) is essential for the functioning of the pump and the transport of one calcium ion.
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== Structural Highlights ==
== Structural Highlights ==
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The calcium ATPase is a protein composed of 1001 aminoacids.
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The calcium ATPase is a protein composed of 994 aminoacids.
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The protein is composed of many <scene name='60/604489/Alpha_regions/1'>alpha helices regions</scene>, including 10 transmembrane alpha helices. It also contains a lot of beta strands.
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The <scene name='60/604489/Secondary_structure/1'>secondary structure</scene> of the protein is composed of helical regions (47%), beta sheet regions (16%) and loops. There are <scene name='60/604489/10_transmembrane_helices/1'>10 transmembrane alpha helices</scene>, and three of them line a channel that spans the lipid bilayer and that allows calcium to pass through membranes. It also contains too cytoplasmic loops between the transmembrane helices. When the protein is not phosphorylated, two of the transmembrane helices are disrupted and form a cavity that can bind two molecules of calcium.
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The protein is divided in <scene name='60/604489/The_4_domains_of_the_pump/1'>4 regions</scene>. The <scene name='60/604489/Transmembrane_domain/1'>transmembrane region</scene> of the protein contains the channel that spans the lipid bilayer, and the calcium binding cavity.
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The two cytoplasmic loops form three separate domains. The <scene name='60/604489/Nucleotide_binding_domain/1'>nucleotide binding domain (N)</scene> contains the site where ATP binds to the protein. The <scene name='60/604489/P_domain/1'>phosphorylation domain (P)</scene> contains an Aspartate residue (<scene name='60/604489/Asp_351/1'>Asp 351</scene>) that can be phosphorylated. Finally, the <scene name='60/604489/Actuator_domain/1'>actuator domain (A)</scene> is involved in the transmission of major conformational changes. The phosphorylation and the nucleotide binding domains form the <scene name='60/604489/Catalytic_site/1'>catalytic site</scene> of the protein<ref name="first">Benjamin Lewin, 2007 - Cells - Jones & Bartlett Learning</ref>.
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== Mechanism of action ==
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The architecture of calcium ATPase (determined by X-Ray crystallography) allows to understand mechanisms by which the energy of ATP is coupled to the calcium transport across a membrane.
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The first step of the calcium pump catalytic cycle is the cooperative binding of <scene name='60/604489/Calcium_molecules/1'>two calcium ions</scene> in the calcium binding cavity. Then, ATP binds to the ATP binding site (nucleotide binding domain) and transfers its γ-phosphate to the aspartic acid 351 (phosphorylation domain). That creates a acid-stable aspartyl phosphate intermediate. The phosphorylation of Asp351 allows a large conformational changes in cytoplasmic domains: the nucleotide binding domain and the phosphorylation domain are brought into close proximity. This rearrangement causes a 90° rotation of the actuator domain, which leads to a rearrangement of the transmembrane helices. This rearrangement alters the affinity of the protein for the calcium and disrupts the calcium binding cavity. Calcium is released in the lumen of the endoplasmic reticulum/Golgi Apparatus or outside the cell. After releasing calcium, two or three protons bind to the transport sites (charges compensation) and the aspartyl phosphate is hydrolyzed to complete the cycle. <ref name = "four">Marisa Brini , Ernesto Carafoli, 2009 - ''Calcium pumps in health and disease'' - Physiological Reviews</ref>
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[[Image:51-TheCalciumPumps-calcium-pumps.jpg|400px|center|]]
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The structure on the left is the empty state (free from calcium). Two calcium ions are shown in blue and Asp351 is shown in red.<ref name="second"> David Goodsell, 2004 - Calcium pump molecul of the month - PDB, doi: 10.2210/rcsb_pdb/mom_2004_3</ref>
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To sum up, calcium pumps have two conformations, E1 and E2. These two conformations are characterized by different specificity for ion binding. When the pump is in the E1 state, it has high calcium affinity and interacts with calcium at one side of the membrane. In the E2 state, the enzyme has a lower calcium affinity and that leads to the release of the ion at the opposite side. E1 has the calcium binding site oriented toward the cytoplasm. E2 has the calcium binding site oriented toward the lumen of the endoplasmic reticulum or toward the extracellular space<ref name="third">Thomas D.Pollard and William C. Earnshaw, - ''Membrane, structure and function'' - Cell Biology (second edition), p.133-136</ref>. The phosphorylated intermediate, E1 can phosphorylate ADP, whereas E2 can only react with water<ref>David H.MacLennan, William J.Rice and N. Michael Green, 1997 - ''The Mechanism of Ca2+ Transport by Sarco(Endo)plasmic Reticulum Ca2+-ATPases'' - The Journal of Biological Chemistry, p.272, 28815-28818, http://www.jbc.org/content/272/46/28815.full.html</ref>. In the absence of calcium, calcium pumps are mainly in E1 state.
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[[Image:Etat.jpg|center|]]<ref name = "four">Marisa Brini , Ernesto Carafoli, 2009 - ''Calcium pumps in health and disease'' - Physiological Reviews</ref>
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== Ligand and Interaction ==
 
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The architecture of calcium ATPase (determined by X-Ray crystallography) allow to understand mechanisms by which the energy of ATP is coupled to the calcium transport across a membrane.
 
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Structurally, the pump contains 10 transmembrane domains (α helices), two large intracellular loops and amino/carboxy-terminal cytoplasmic tails.
 
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In the cytoplasm, the ATP binds to the cytosolic loop that connects transmembrane domains four and five (ATP binding site). It transfers its γ-phosphate to the aspartic acide 351 (phosphorylation site) and creates a acid-stable aspartyl phosphate intermediate. The binding of ATP is initiated by the cooperative fixing of two calcium ions to the transport site. The phosphorylation of Asp351 allows a large conformational changes in cytoplasmic domains which closes the ion gates from the cytoplasm and alters the affinity of the protein for the calcium. After releasing calcium (in the lumen of cytoplasm or out side the cell), two protons are bound to the transport sites (charges compensation) and the aspartyl phosphate is hydrolyzed to complete the cycle.
 
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To sum up, calcium pumps have two conformations, E1 and E2. E1 has the calcium binding site oriented toward the cytoplasm . E2 has the calcium binding site oriented toward the lumen of the endoplasmic reticulum or toward the extracellular background. These two conformations are characterized by different specificity for ion binding.
 
== Biological Function and Localisation ==
== Biological Function and Localisation ==
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The pumps exist in two major conformational states : E1 and E2. When the pump is in the E1 state, it has high calcium affinity and interacts with calcium at one side of the membrane. In the E2 state, the enzyme has a lower calcium affinity and that leads to the release of the ion at the opposite side.
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There are 3 types of calcium ATPases depending on their localization. The '''SERCA''' (Sarco/Endoplasmic Reticulum Calcium ATPase) is localized in the endoplasmic reticulum membranes, including the nuclear envelope. Only the structure of the SERCA has been resolved by x-ray crystallography. The '''PMCA''' (Plasma Membrane Calcium ATPase) is localized in plasma membranes. The '''SPCA''' (Secretory Pathway Calcium ATPase) is localized in the Golgi apparatus membranes. The particularity of this pump is that it is also able to transport Mn2+ ions.
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Recently, some structural work on the SERCA pump has shown that the mechanism of the pump is a little bit more complex. When the calcium pump is unphosphorylated, two of the helices are disrupted, forming a cavity accessible from the cytosol. This cavity binds two calcium ions. When ATP binds to the pump, it allows the phosphorylation of the enzyme on its phosphorylation domain. The hydrolysis of ATP causes conformational changes that bring the nucleotide binding domain and the phosphorylation domain of the enzyme into close proximity. The activator domain rotates and the transmembrane helices 4 and 6 rearrange. Calcium is released into the lumen of the sarcoplasmic reticulum.
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[[Image:ATPases.jpg|500px|center|]]
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More recent structural work on the SERCA pump has increased the complexity of the conformational transitions that occur during the catalytic cycle. Upon binding of Ca2+, a series of structural changes occur that involve both the protruding cytoplasmic sector and the transmembrane domains, permitting the phosphorylation of the catalytic D-residue by the γ-phosphate of ATP. The dissociation of Ca2+ from the enzyme follows the transition of the high Ca2+ affinity E1∼P(Ca2+) enzyme to the lower affinity E2-P enzyme, the hydrolysis of which then regenerates the Ca2+-free E2 ATPase, completing the catalytic cycle.
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Calcium is a very important molecule for cell signalling. Eucaryotic cells need to maintain a very low calcium concentration in their cytosol. The extracellular calcium concentration is much higher. That difference of concentrations across the membrane creates a gradient of concentration and allows the signalling to be very effective. Indeed, even a very small influx of calcium significantly increases the concentration of calcium inside the cell. Therefore, calcium pumps are very important to maintain the calcium concentration gradient and to remove calcium from the cell after signalling.
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== Regulations ==
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Calcium is involved in many physiological processes such as programmed cell death, fertilization, gene transcription, secretion (including neurotransmitter secretion) etc. For example, the SERCA pump is mainly found in skeletal muscle cells and cardiac cells. It is involved in the relaxation of skeletal muscle cells. Those cells contain a special endoplasmic reticulum called the sarcoplasmic reticulum which is the place of calcium storage. After contraction, calcium ions are transported from the cytoplasm into the sarcoplasmic reticulum through the SERCA pump. This causes the relaxation of the muscle cells because the cytosolic concentration of calcium decreases. The SERCA pump works together with the PMCA pump to export calcium ions from the cytosol and to set the resting level of the cytosolic calcium concentration<ref name="first">Benjamin Lewin, 2007 - Cells - Jones & Bartlett Learning</ref>.
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There are different kind of calcium ATPase regulations. For example, the phospholamban (PLN or PLB) is a membrane protein that regulates the calcium pump in cardiac muscle and skeletal muscle cells. This small phosphoprotein is a pentamer. The phospholamban can be phosphorylated at three distinct sites by various protein kinases (PKA, PKC, CamK...). The phosphorylation state is mediatedthrough beta-adrenergic stimulation. In unphosphorylate state, the phospholamban inhibits the activity of calcium pump in cardiac and skeletal muscle cells by decreasing the apparent affinity of the ATPase for calcium. The phosphorylation of the protein results in the dissociation of the protein from the ATPase. The phosphoprotein binds just downstream of the active ATPase site (asp351).
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The activity of the calcium pump is also regulated by by calmodulin, acidic phospholipids and phosphorylation by kinases A and C. Most of the activation mechanisms implicate the C-terminal region of the pump containing the high affinity calmodulin binding domain, which is involved in the autoinhibition of the pump.
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== Dysfunctions and Diseases ==
 
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== References ==
 
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David H.MacLennan, William J.Rice and N. Michael Green, 1997 - ''The Mechanism of Ca2+ Transport by Sarco(Endo)plasmic Reticulum Ca2+-ATPases'' - The Journal of Biological Chemistry, p.272, 28815-28818
 
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== Regulations ==
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There are different kinds of calcium ATPase regulations. For example, the <scene name='60/604489/Phospholamban/2'>phospholamban</scene> (PLN or PLB) and the <scene name='60/604489/Sarcolipin/1'>sarcolipin</scene> are membrane proteins that regulate the calcium pump in the cardiac muscle and in skeletal muscle cells. These two proteins are close homologous and play the same role. The phospholamban is a phosphoprotein that can be phosphorylated at three distinct sites by various protein kinases (PKA, PKC, CamK...). The phosphorylation state is mediated through beta-adrenergic stimulation. In unphosphorylated state, the phospholamban inhibits the activity of the calcium pump in cardiac and skeletal muscle cells by decreasing the apparent affinity of the ATPase for calcium. The phosphorylation of the protein results in the dissociation of the protein from the ATPase<ref>Marianela G.Dalghi, Marisa M.Fernández, Mariela Ferreira-Gomes, Irene C.Mangialavori, Emilio L.Malchiodi, Emanuel E.Strehler and Juan Pablo F.C.Rossi, 2013 - ''Plasma Membrane Calcium ATPase Activity Is Regulated by Actin Oligomers through Direct Interaction'' - The Journal of Biological Chemistry, p.288, 23380-23393, http://www.jbc.org/content/288/32/23380.full.</ref>.
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Marianela G.Dalghi, Marisa M.Fernández, Mariela Ferreira-Gomes, Irene C.Mangialavori, Emilio L.Malchiodi, Emanuel E.Strehler and Juan Pablo F.C.Rossi, 2013 - ''Plasma Membrane Calcium ATPase Activity Is Regulated by Actin Oligomers through Direct Interaction'' - The Journal of Biological Chemistry, p.288, 23380-23393
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Another example of regulation is the plasma membrane calcium pump carboxy-terminal tail that contains the calmodulin binding domain (regulatory domain) which acts as an auto-inhibitory domain. The binding of the calmodulin frees the pump from autoinhibition<ref>Marisa Brini and Ernesto Carafoli, 2010 - ''The plasma membrane Ca2+ ATPase and the Plasma Membrane Sodium Calcium Exchanger Cooperate in the Regulation of Cell Calcium'' - Cold Spring Harbor Perspectives in Biology, http://cshperspectives.cshlp.org/content/3/2/a004168.full</ref>.
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Marisa Brini and Ernesto Carafoli, 2010 - ''The Plasma Membrane Ca2+ ATPase and the Plasma Membrane Sodium Calcium Exchanger Cooperate in the Regulation of Cell Calcium'' - Cold Spring Harbor Perspectives in Biology
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== Dysfunctions and Diseases ==
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Marisa Brini and Ernesto Carafoli, 2009 - ''Calcium Pumps in Health and Disease''- Physiological Reviews
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Two human genetic diseases caused by mutations in the SERCA pump have been identified : Brody's disease and Darier's disease.<ref name = "four">Marisa Brini , Ernesto Carafoli, 2009 - ''Calcium pumps in health and disease'' - Physiological Reviews</ref> Brody's disease is caused by 2 mutations in the SERCA1 gene called ATP2A1: <scene name='60/604489/Ile_235/1'>Ile235Asn</scene> and <scene name='60/604489/Glu982/1'>Glu982Lys</scene>. <ref>Nyamkhishig Sambuughin, Elena Zvaritch, Natasha Kraeva, Olga Sizova, Erica Sivak, Kelley Dickson, Margaret Weglinski, John Capacchione, Sheila Muldoon, Sheila Riazi, Susan Hamilton, Barbara Brandom and David H. MacLennan, 2014 - ''Exome analysis identifies Brody myopathy in a family diagnosed with malignant hyperthermia susceptibility'' - Molecular Genetics & Genomic Medicine</ref>. Brody's disease is an autosomal recessive myopathy. The symptoms are muscle stiffness, cramps and progressive impairment of muscle relaxation during exercise. Darier's disease is a rare, dominantly inherited disorder that affects the skin producing a variety of types of lesions. It is caused by mutations in the SERCA2 gene (ATP2A2). Defects in the activity or expression level of the pump can cause other dysfunctions such as heart failure or cancer.
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Thomas D.Pollard and William C. Earnshaw, - ''Membrane, structure and function'' - Cell Biology (second edition), p.133-136
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</StructureSection>
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== References ==
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<references/>

Current revision

Calcium ATPase

3D Structure of the SERCA pump resolved with x-ray cristallography

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References

  1. 1.0 1.1 Benjamin Lewin, 2007 - Cells - Jones & Bartlett Learning
  2. 2.0 2.1 2.2 Marisa Brini , Ernesto Carafoli, 2009 - Calcium pumps in health and disease - Physiological Reviews
  3. David Goodsell, 2004 - Calcium pump molecul of the month - PDB, doi: 10.2210/rcsb_pdb/mom_2004_3
  4. Thomas D.Pollard and William C. Earnshaw, - Membrane, structure and function - Cell Biology (second edition), p.133-136
  5. David H.MacLennan, William J.Rice and N. Michael Green, 1997 - The Mechanism of Ca2+ Transport by Sarco(Endo)plasmic Reticulum Ca2+-ATPases - The Journal of Biological Chemistry, p.272, 28815-28818, http://www.jbc.org/content/272/46/28815.full.html
  6. Marianela G.Dalghi, Marisa M.Fernández, Mariela Ferreira-Gomes, Irene C.Mangialavori, Emilio L.Malchiodi, Emanuel E.Strehler and Juan Pablo F.C.Rossi, 2013 - Plasma Membrane Calcium ATPase Activity Is Regulated by Actin Oligomers through Direct Interaction - The Journal of Biological Chemistry, p.288, 23380-23393, http://www.jbc.org/content/288/32/23380.full.
  7. Marisa Brini and Ernesto Carafoli, 2010 - The plasma membrane Ca2+ ATPase and the Plasma Membrane Sodium Calcium Exchanger Cooperate in the Regulation of Cell Calcium - Cold Spring Harbor Perspectives in Biology, http://cshperspectives.cshlp.org/content/3/2/a004168.full
  8. Nyamkhishig Sambuughin, Elena Zvaritch, Natasha Kraeva, Olga Sizova, Erica Sivak, Kelley Dickson, Margaret Weglinski, John Capacchione, Sheila Muldoon, Sheila Riazi, Susan Hamilton, Barbara Brandom and David H. MacLennan, 2014 - Exome analysis identifies Brody myopathy in a family diagnosed with malignant hyperthermia susceptibility - Molecular Genetics & Genomic Medicine
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