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10 th PBL in calcium- and phospholipid signaling May 3-14, 2010 Md. Shahidul Islam, M.D., Ph.D. Associate Professor Department of Clinical Sciences and Education, Södersjukhuset Karolinska Institutet Forskningscentrum, Södersjukhuset 118 83 Stockholm, Sweden Shaisl@ki.se
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Sydney Ringer (1883) Survival of Fish Muscle contraction Fertilization of eggs Development of tadpole Locke and Overton (1894) Impulse transmission
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Why Ca 2+ is chosen by nature for diverse regulations?
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Specific and tight binding to effector proteins Suitable coordination chemistry Larger diameter and flexible coordination number Can bind in to irregularly shaped protein cavities
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Evolutionary history of calcium Ancient sea water was free of calcium Water contaminated by rocks Protection against calcium toxicity evolved Cells chose calcium as a signaling ion
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Total Ca 2+ and free Ca 2+ Total cell calcium: 2.5 mmol/Kg wet weight. Higher total calcium in tumors 60-80% of it is bound to the extracellular coat Large amount of calcium in secretory granules and ER Free Ca 2+ concentration is important for regulatory purposes
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What are the functions of Ca 2+ ? Structural. –Bone –Membrane fluidity and integrity (Ca 2+ phospholipid) –Protein structure and function –Chromatin structure
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What are the functions of Ca 2+ ? Co-factor for enzymes –Protein Kinase C –Phospholipase A 2 –Prothrombin –Calpain –DNAse 1 Electrical –Ca 2+ current during action potential
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Intracellular Regulation Second messenger Muscle contraction Secretion Metabolism Gene expression
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Ca 2+ is a two-edged sword Excessive rise of [Ca 2+ ] i –Activation of Proteases Phosphatases Endonucleases
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Excessive rise of [Ca 2+ ] i Impaired mitochondrial function Perturbation of cytoskeletal organization Apoptosis, cell death
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Cellular components that determine Ca 2+ fluxes and Ca 2+ homeostasis: Plasma membrane Ca 2+ channels –Voltage-gated –Receptor operated –TRPs Plasma membrane Ca 2+ ATPase Na + /Ca 2+ Exchanger
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Na + /Ca 2+ exchanger vs PM Ca 2+ ATPase Na + /Ca 2+ exchanger: Low affinity, high capacity. Takes care of large Ca 2+ loads PM Ca2+ ATPase. High affinity low capacity Three Na + /Ca 2+ exchanger genes. Gene products NCX1, NCX2, NCX3; several splice variants
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PM Ca2+ ATPase P-type family of transport ATPases Four genes PMCA1, PMCA2, PMCA3, PMCA4 Four splice variants Calmodulin-dependent
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Cellular components that determine Ca 2+ fluxes and Ca 2+ homeostasis: ER Serco-Endoplasmic Reticulum Ca 2+ ATPase (SERCA) IP3 Recepotors Ryanodine receptors TRIC (trimeric intracellular cation) channel (Yazawa M, Nature 2007) Luminal Ca 2+ -binding proteins
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Cellular components that determine Ca 2+ fluxes and Ca 2+ homeostasis: Mitochondria –Ca2+ Uniporter –Na + /Ca 2+ exchanger Cytoplasm –Calmodulins –Parvalbumin –Other Ca 2+ -binding proteins
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Calcium Channels Voltage Dependent –Slow, fast Intracellular Ca2+ channel
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Receptor-operated Ca 2+ channels
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Ca 2+ Channels Receptor-operated Ca 2+ channels –Nicotinic cholinergic receptor –NMDA receptor ion channel –Purinergic receptor P2X
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Voltage-gated Ca 2+ channels
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Gene Superfamily of Voltage- Gated Ion Channels Voltage-gated Na + channels Voltage-gated K + channels Voltage-gated Ca 2+ channels
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Distinct classes of Ca 2+ curents L-type –High activation voltage –Large conductance –Long lasting –Blocked by dihydropyridine, phenylalkylamine, benzothiazepine
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Other high-voltage-activated Ca 2+ channels N-type –Neuronal P/Q-type R-type Not blocked by DHPs, blocked by polypeptide toxins
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Low-voltage activated Ca 2+ current T-type –Tiny conductance –Transient current –
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Nomenclature Ion conducted Main regularor Alpha-1 subunit gene family Cav1.1
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EA Ertel Neuron 25:533, 2000.
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Molecules and curents Cav1.1 Cav1.2 Cav1.3 Cav1.4 Cav2.1 Cav2.2 Cav2.3 Cav3.1 Cav3.2 Cav3.3 L-type P/Q-type N-type R-type T-type
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Blockers Cav1.1 Cav1.2 Cav1.3 Cav1.4 Cav2.1 Cav2.2 Cav2.3 Cav3.1 Cav3.2 Cav3.3 DHP Not known -Agatoxin IVA Conotoxin None
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Fluorescence
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Jablonski Diagram
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Fluorescence Resonance Energy Transfer
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What is FRET It is a distance-dependent interaction between the electronic excited states of two dye molecules in which excitation is transferred from a donor molecule to an acceptor molecule without emission of a photon.
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Conditions for FRET Proximity (10-100Å) Absorption spectrum of acceptor overlaps emission spectrum of donor Donor and acceptor transition dipole orientation is parallel
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Excitation and emission spectra of different ”GFP”
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Cameleons
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Miyawaki A. 1997, Nature 388:6645
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