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Biological membranes, cell compartments

Biological membranes, cell compartments. Bruno Sopko. Content. Introduction Plasma membrane Lipid rafts Nucleus Mitochondria Endopla smic reti c ulum Golgi ap paratus Lysosom s Peroxisom s Cytoplasm a nd cytoskelet on. Introduction - Advantages of the compartmentalisation.

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Biological membranes, cell compartments

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  1. Biological membranes, cell compartments Bruno Sopko

  2. Content • Introduction • Plasma membrane • Lipid rafts • Nucleus • Mitochondria • Endoplasmicreticulum • Golgi apparatus • Lysosoms • Peroxisoms • Cytoplasm andcytoskeleton

  3. Introduction - Advantages of the compartmentalisation • Maintaining of the high local concentration of the chemical components in one compartment – higher reaction rates • Controlling the transport of intermediates among compartments is other effective regulation system of metabolic pathways, localized in more than one compartment • Protection from the environment • Protection from the “aggressive” compartment interior

  4. Introduction – subcellular compartments • Nucleus • Nucleolus • Golgi apparatus • Mitochondrion • Lysosoms • Peroxisoms • Cytoskeleton • Cytosol • Centriols • Plasma membrane • Endoplasmic reticulum

  5. Introduction – Transport across membrane • Diffusion • Assisted diffusion • Active transport

  6. Plasma membrane • Plasma membrane (plasmalemma) is biologic membrane separating inner parts of the cell from the environment. • Plasma membrane is the surface of all cells and is selectively-permeable. This is the regulation part for the intake and excretion of the chemical substances. • Composed of lipids (phospholipids, glycolipids and cholesterol esters) and proteins, participating in many cell processes as, for instance, cell adhesion, ion channels transport and cell signaling. • Inner part contains specific sites, binding components of intercellular cytoskeleton. • Organized in subcompartments – microdomains, rafts

  7. Plasmamembrane - forming

  8. Lipid Rafts Lipid rafts are small (10-200nm), heterogeneous, highly dynamic, sterol- and sphingolipid-enriched domains that compartmentalize cellular processes.

  9. Lipid Rafts • Cholesterol and sphingolipid-enriched membrane microdomains or platforms • Cholesterol of double concentration • Sphingomyelin concentration elevated by 50% • Concentrate and segregate proteins within the membrane • More ordered and tightly packed than surrounding bilayer • Float freely in the surrounding membrane

  10. Types of lipid rafts • Caveolae: small, flask-shaped invaginations of the plasma membrane enriched in caveolin • Planar lipid rafts: found in neurons and enriched in flotillin • Caveolin and flotillin recruit signaling proteins • Signaling can be promoted or dampened

  11. Lipid Raft Proteins • “True resident proteins” • GPI-anchored proteins-prion protein (PrPc) • Caveolin • Flotillin • Signaling proteins • G-protein, non-receptor tyrosine kinases • Cytoskeletal/Adhesion proteins • actin, myosin, vinculin, cofilin, cadherin, ezrin

  12. GPI-anchored proteins

  13. Lipid Raft formation

  14. Lipid Rafts and Viruses • HIV virus • Budding may occur from lipid rafts • Influenza virus • Raft-associated glycoproteins in envelope

  15. Nucleus • DNA replication • Transcription, synthesis of mRNA, tRNA, rRNA, ribosomes • Surrounded by double membrane connected to ER • Transport of cytosolic compounds (active and passive) only via nuclear pores • Specialized subcompartments (nucleolus –ribosomes formation, DNA replication is localized etc.)

  16. Nucleus

  17. Nucleus – transport across nuclearenvelope

  18. Nucleus –protein transfer Transferintonucleus Transfer fromnucleus

  19. Nucleus –RNA export

  20. Mitochondria • Two membranes – inner and outer are highly different in composition and enzymatic activity • Matrix of the mitochondria (mitosol) exhibits different biochemical functions • Majority of the mitochondrial proteins is coded in nucleolar DNA (and synthesized by free ribosomes in cytosol), but 13 mitochondrial proteins and some RNA are coded in circular mitochondrial DNA (mtDNA)

  21. Mitochondria • Synthesis of more then 90% ATP – oxidative phosphorylation (inner membrane) • Heat production • Apoptosis – inner mitochondrial pathway • Oxidative decarboxylation of pyruvate (pyruvatedehydrogenase complex) • ß-oxidation of fatty acids (shorter then 24-C) • Kreb’scyclus - mitosol • P450 - in inner membrane

  22. Mitochondria –protein import

  23. Mitochondria –elektronimport fromcytosolic NADH Michael W. King, Ph.D / IU SchoolofMedicine / mikingatiupui.edu

  24. Mitochondria – ATP export to cytosol

  25. Mitochondria – import of fatty acidsfor-oxidation

  26. Mitochondria –acetyl-CoA export forsynthesis of lipids and cholesterol Michael W. King, Ph.D / IU SchoolofMedicine / mikingatiupui.edu

  27. Mitochondria – the urea cycle • Only ornithintranscarbamoylase is located in mitosol • Carbamoylphosphate is synthetized in mitochondria from bicarbonate and ammonia, utilizing 2 ATP • Citrullin is exported via antiport with ornithine

  28. Endoplasmicreticulum • Proteosynthesis (rough ER = RER) • Primal steps of polysaccharides chains synthesis (N-bound glycoproteins (RER)) • Synthesis (smooth ER = SER) - phospholipids, triglycerides • Cholesterol and steroids (SER) synthesis (on thesurface) • Hydroxylation of endogenous a exogenous compounds by cytochromes P450 (SER) • Calcium ions storage (SER , sarcoplasmic reticulum) • Connected with nucleolar envelope

  29. Golgi apparatus • Cooperates with endoplasmic reticulum • Enzymatic postranslation protein modifications (glycosylation, sulfatation) • Synthesis of new plasma membrane and participation in creation of primal lysosoms and peroxisoms

  30. Lysosoms • Hydrolysis of intracellular material – proteins nucleic acids, lipids together with organelles – autofagia • Extracellular material is hydrolyzed after the transport into the cell by endocytosis (pinocytosis and phagocytosis) - heterofagia • Intracellular digestion of intracellular, and extracellular compounds • Lysosomal enzymes are hydrolases with maximal activity at pH 5 (inside of lysosoms)

  31. Lysosoms • Substances are in membrane enclosed vesicle • By fusion of the vesicle with primal lysosom secondary lysosom is formed • Lysosomal hydrolases digest the content of secondary lysosoms • Digested parts of the hydrolysate are transferred to cytosol for reuse • Non-digested material is accumulated in residual body and is excreted by exocytose • Remaining (nonexocytosed) residual bodies contain lipofuscin („age pigment“)

  32. Peroxisoms • Produce or use hydrogen peroxide • Differ in function and in number in different types of cell • More then 50 types of enzyme catalyzing oxidative and reductive biosynthetic reactions • oxidation of very long fatty acids chains (a- and b-oxidation) • synthesis glycerolipids, glycerol ether lipids (plasmalogens) and isoprenoids • enzymes for oxidation of D-aminoacids, 2-hydroxy acids and uric acid (uricase is absent at higher apes) • catalasa • Known more then 25 perixosomes biogenesis disorders (Zellweger‘s syndrome = absence of peroxisomes and death occurs by age 6 months) • Some xenobiotics induce peroxisom proliferation

  33. Peroxisoms - -oxidationoflongfattyacids

  34. Peroxisoms –plasmalogenssynthesis

  35. Cytoplasm/cytoskeleton • Keeps phenotype (morphology) of the cell and participate in intracellular transport, cell mobility and cell division • Is formed by microtubules, intermedial filaments and actin filaments (microfilaments)

  36. Cytoplasm/cytoskeleton - microtubules • diameter 25 nmandlengthfrom 200 nm to 25 mm • Polymersofα- andβ-tubulin dimmers, polymerizedend to end to protofilaments. Protofilamentsformhollowmicrotubules

  37. Cytoplasm/cytoskeleton - intermedialfilaments • diameter 10 nm • Domain structure of IF is conserved. Each protein contains non-a-helix domain at N and C-ends, which frame a-helix domain of the „stick“ • Basic unit of the intemedial filaments (IF) is dimmer • Known more then 70 gensforsix basic types(I - VI) IF : • I a II - keratins (epithelialandhigher) • III – e.g. desmin (sarcomersofmusclecells) andvimentin (e.g. fibroblasts - correctlocalizationoforganelles • V - nucleolar IF

  38. Cytoplasm/cytoskeleton - intermedialfilaments

  39. Cytoplasm/cytoskeleton - microfilaments • The most dynamic part of cytoskeleton are microfilaments (actin filaments). • Diameter is 6nm • Formed by two linear polymers of actin subunits

  40. Cytoplasm/cytoskeleton - Centrosom and centriols • Centrosom is organell, main organisation centre of microtubules and regulates cell cycle • Centrosom is the cell region, forming microtubules • Centrioles are important parts of centrosomes.

  41. Cytoplasm/cytosol • 54% cell volume • Many reaction chains are located in parts of cytosol • glycolysis (NAD+/ NADH) • PPP - pentosophosphate pathway (NADPH) • glycogenolysis • glycogenesis (synthesa glykogenu) • biosynthesis of fatty acids (fatty acid synthase) • synthesis of active saccharides • Proteosynthesis support • Forming „subcompartments“ with different enzyme concentrations-> many reactions are carried out only in certain parts of cytosol

  42. Examples of pathways localized in a single compartment only • Kreb’s cycle • Glycolysis • Proteosynthesis • DNA replication

  43. Literature • Gabriel Schlenstedt, Protein import into the nucleus, FEBS Letters 389 (1996) 75-79 • Walter Nickel and Catherine Rabouille, Mechanisms of regulatedunconventional protein secretion, NATURE Reviews, Molecular cell Biology volume 10, february 2009 • Marks´ Basic Medical Biochemistry, A Clinical Approach, third edition, 2009 (M. Lieberman, A.D. Marks) • David A. Jans, Chong-Yun Xiao, and Mark H.C. Lam, Nuclear targeting signalrecognition: a key control pointin nuclear transport?, BioEssays 22:532-544, 2000 John Wiley & Sons, Inc • The Cell: A Molecular Approach, Fourth Edition, GEOFFREY M. COOPER , ROBERT E. HAUSMAN, 2007, ASM Press, Washington, D.C. USA • YoshihiroYoneda, How Proteins Are Transported from Cytoplasm to the Nucleus, J. Biochem. 121, 811-817 (1997) • AlwinKöhler and Ed Hurt, Exporting RNA from the nucleus • to the cytoplasm, NATURE Reviews, Molecular cell Biology volume 8, october 2007

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