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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 span the lipid bilayer, and the calcium binding cavity.
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 span 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>Benjamin Lewin, 2007 - Cells - Jones & Bartlett Learning</ref>.
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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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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.
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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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.
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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>.

Revision as of 22:19, 2 January 2015

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

Drag the structure with the mouse to rotate

References

  1. 1.0 1.1 Benjamin Lewin, 2007 - Cells - Jones & Bartlett Learning
  2. Thomas D.Pollard and William C. Earnshaw, - Membrane, structure and function - Cell Biology (second edition), p.133-136
  3. 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
  4. 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.


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


Marisa Brini and Ernesto Carafoli, 2009 - Calcium Pumps in Health and Disease- Physiological Reviews

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