Transcript Ch6
Chapter 06 *Lecture Outline *See separate FlexArt PowerPoint slides for all figures and tables pre-inserted into PowerPoint without notes and animations. Copyright © The McGraw-Hill Companies, Inc. Permission required for reproduction or display. 1 A Glimpse of History Biologists had noticed that in vats of grape juice, alcohol and CO2 are produced while yeast cells increase in number • But idea not widely accepted, mocked by some • In 1850s, Louis Pasteur set out to prove • Simplified setup: clear solution of sugar, ammonia, mineral salts, trace elements • Added a few yeast cells—as they grew, sugar decreased, alcohol level increased • Strongly supported idea, but Pasteur failed to extract something from inside the cells that would convert sugar • In 1897, Eduard Buchner, a German chemist awarded Nobel Prize in 1907 showed that crushed yeast cells could convert sugar to ethanol and CO2; Microbial Metabolism All cells need to accomplish two fundamental tasks • Synthesize new parts • Cell walls, membranes, ribosomes, nucleic acids • Harvest energy to power reactions • Sum total of these is called metabolism • Human implications • • • • • Used to make biofuels Used to produce food Important in laboratory Invaluable models for study Unique pathways potential drug targets 6.1. Principles of Metabolism Copyright © The McGraw-Hill Companies, Inc. Permission required for reproduction or display. Can separate metabolism into two parts CATABOLISM ANABOLISM Energy source (glucose) • Catabolism Cell structures (cell wall, membrane, ribosomes, surface structures) • Processes that degrade compounds to release energy • Energy captured to make ATP Energy Macromolecules (proteins, nucleic acids, polysaccharides, lipids) Energy • Anabolism • Biosynthetic processes • Assemble subunits of macromolecules • Use ATP to drive reactions • Processes intimately linked Subunits (amino acids, nucleotides, sugars, fatty acids) Energy Precursor metabolites Waste products Nutrients (acids, carbon dioxide) (source of nitrogen, sulfur, etc.) Catabolic processes harvest the energy released during the breakdown of compounds and use it to make ATP. The processes also produce precursor metabolites used in biosynthesis. Anabolic processes (biosynthesis) synthesize and assemble subunits of macromolecules that make up the cell structures. The processes use the ATP and precursor metabolites produced in catabolism. Harvesting Energy Energy is the capacity to do work Two types of energy • Potential: stored energy (e.g., chemical bonds, rock on hill, water behind dam) • Kinetic: energy of movement (e.g., moving water) • Energy in universe cannot be created or destroyed, but it can be converted between forms • This is the 1st Law of Thermodynamics Harvesting Energy Photosynthetic organisms harvest energy in sunlight Copyright © The McGraw-Hill Companies, Inc. Permission required for reproduction or display. • Power synthesis of organic compounds from CO2 • Convert kinetic energy of photons to potential energy of chemical bonds Chemoorganotrophs obtain energy from organic compounds Radiant energy (sunlight) Photosynthetic organisms harvest the energy of sunlight and use it to power the synthesis of organic compounds from CO2. This converts radiant energy to chemical energy. Chemical energy (organic compounds) Chemoorganotrophs degrade organic compounds, harvesting chemical energy. • Depend on activities of photosynthetic organisms (top): © Photodisc Vol. Series 74, photo by Robert Glusie; (bottom): © Digital Vision/PunchStock Harvesting Energy Free energy is energy available to do work • E.g., energy released when chemical bond is broken • Compare free energy of reactants, products • Exergonic reactions: reactants have more free energy • Energy is released in reaction • Endergonic reactions: products have more free energy • Reaction requires input of energy • Change in free energy is same regardless of number of steps involved (e.g., converting glucose to CO2 + H2O) • Cells use multiple steps when degrading compounds • Energy released from exergonic reactions powers endergonic reactions Components of Metabolic Pathways Metabolic pathways • Series of chemical reactions that convert starting compound end product • May be linear, branched, cyclical Copyright © The McGraw-Hill Companies, Inc. 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Intermediatea Starting compound Intermediateb End product Intermediateb1 End product1 Intermediateb2 End product2 (a) Linear metabolic pathway Starting compound Intermediatea (b) Branched metabolic pathway Starting compound Intermediated End product Intermediatea Intermediatec Intermediateb (c) Cyclical metabolic pathway Components of Metabolic Pathways Role of Enzymes • Biological catalysts: accelerate conversion of substrate into product by lowering activation energy Relative energy • Highly specific: one at each step • Reactions would occur without, but extremely slowly Activation energy with an enzyme Energy of reactants Activation energy without an enzyme Energy of products Progress of reaction (a) Starting compound (b) Enzyme a Intermediatea Enzyme b Intermediateb Enzyme c End product Components of Metabolic Pathways Role of ATP • Adenosine triphospate (ATP) is energy currency • • • • Composed of ribose, adenine, three phosphate groups Adenosine diphospate (ADP) acceptor of free energy Cells produce ATP by adding Pi to ADP using energy Release energy from ATP to yield ADP and Pi Three processes to generate ATP • Substrate-level phosphorylation Unstable (high-energy) bonds • Exergonic reaction powers • Oxidative phosphorylation • Proton motive force drives • Photophosphorylation • Sunlight used to create proton motive force to drive P ~ P~ P ATP Pi Pi Energy used The energy comes from catabolic reactions. Energy released The energy drives anabolic reactions. P~ P ADP Components of Metabolic Pathways Role of the Chemical Energy Source and the Terminal Electron Acceptor Some atoms, molecules more electronegative than others H2S S0 Organic carbon compounds Energy release Organic carbon compounds CO2 SO4 FeOOH Fe2+ NH4+ NO2– ( to form NH4+) NO3– ( to form NH4+) Mn2+ MnO2 Relative tendency to give up electrons • (E.g., glucose to O2) H2 Relative tendency to give up electrons • Greater affinity for electrons • Energy released when electrons move from low affinity molecule to high affinity molecule Terminal electron acceptors Energy sources NO3– ( to form NH2) O2 (a) Energy is released when electrons are moved from an energy source with a low affinity for electrons to a terminal electron acceptor with a higher affinity. Components of Metabolic Pathways Role of the Chemical Energy Source and the Terminal Electron Acceptor (continued…) More energy released when difference in electronegativity is greater Copyright © The McGraw-Hill Companies, Inc. Permission required for reproduction or display. • Acceptor: • Terminal electron acceptor Pyruvate NO3– (to form NH4–) O2 (b) Three examples of chemoorganotrophic metabolism Terminal electron acceptors H2 H2S CO2 Fe2+ Relative tendency to give up electrons • Energy source Glucose Inorganic energy sources Relative tendency to give up electrons • Electron donor: Relative tendency to give up electrons Glucose Terminal as an electron energy source acceptors O2 (c) Three examples of chemolithotrophic metabolism Components of Metabolic Pathways Prokaryotes remarkably diverse in using energy sources and terminal electron acceptors • Organic, inorganic compounds used as energy source • O2, other molecules used as terminal electron acceptor • Electrons removed through series of oxidation-reduction reactions or redox reactions • Substance that loses electrons is oxidized • Substance that gains electrons is reduced • Electron-proton pair, or Transfer of electrons hydrogen, actually moves e • Dehydrogenation = oxidation Compound + Compound X Y • Hydrogenation = reduction X loses electron(s). – Y gains electron(s). X is the reducing agent. Y is the oxidizing agent. e– Compound X + Compound Y (reduced) (oxidized) X is oxidized by the reaction. Y is reduced by the reaction. Components of Metabolic Pathways Role of Electron Carriers • Energy harvested in stepwise process • Electrons transferred to electron carriers, which represent reducing power (easily transfer electrons to molecules) – Raise energy level of recipient molecule • NAD+/NADH, NADP+/NADPH, and FAD/FADH2 Precursor Metabolites Precursor metabolites are intermediates of catabolism that can be used in anabolism • Serve as carbon skeletons for building macromolecules • E.g., pyruvate can be converted into amino acids alanine, leucine, or valine Precursor Metabolites Recall that E. coli can grow in glucose-salts medium • Contains just glucose, inorganic salts • Glucose is energy source • Glucose is starting point for all cellular components Copyright © The McGraw-Hill Companies, Inc. Permission required for reproduction or display. • Includes proteins, lipids, carbohydrates, nucleic acids Glucose molecules To: Lipid synthesis To: Amino acid synthesis Carbohydrate synthesis To: Nucleic acid synthesis • Some glucose molecules completely oxidized for energy; others used in biosynthesis To: CO2 molecules + energy Overview of Catabolism Three central metabolic pathways • Oxidize glucose to CO2 • Catabolic, but precursor metabolites and reducing power can be diverted for use in biosynthesis • Termed amphibolic to reflect dual role • Glycolysis • Splits glucose (6C) to two pyruvates (3C) • Generates modest ATP, reducing power, precursors • Pentose phosphate pathway • Primary role is production precursor metabolites, NADPH • Tricarboxylic acid cycle • Oxidizes pyruvates from glycolysis • Generates reducing power, precursor metabolites, ATP Overview of Catabolism Copyright © The McGraw-Hill Companies, Inc. Permission required for reproduction or display. GLUCOSE Central metabolic pathways • Glycolysis • Pentose phosphate pathway • Tricarboxylic acid cycle Key outcomes • ATP • Reducing power • Precursor metabolites Electron Transport Chain 2 Pentose phosphate pathway Starts the oxidation of glucose Glycolysis Oxidizes glucose to pyruvate 1 Yields ~ ~ + Reducing power ATP by substrate-level phosphorylation Yields Reducing power Biosynthesis 5 Acids, alcohols, and gases Pyruvate Pyruvate 3a Fermentation Reduces pyruvate or a derivative Transition step CO2 CO2 Yields Reducing power AcetylCoA AcetylCoA X2 CO2 CO2 3b TCA cycle Incorporates an acetyl group and releases CO2 (TCA cycles twice) Yields ATP by substrate-level phosphorylation ~ ~ + Reducing power 4 Respiration Uses the electron transport chain to convert reducing power to proton motive force Yields ~ ATP by oxidative phosphorylation ~ Overview of Catabolism Respiration transfers electrons from glucose to electron transport chain • Electron transport chain generates proton motive force • Harvested to make ATP via oxidative phosphorylation i.e. “Builds a Battery • Aerobic respiration – O2 is terminal electron acceptor • Anaerobic respiration – Molecule other than O2 as terminal electron acceptor – Also use modified version of TCA cycle Overview of Catabolism Fermentation • If cells cannot respire, will run out of carriers available to accept electrons • Glycolysis will stop • Fermentation uses pyruvate or derivative as terminal electron acceptor to regenerate NAD+ • Glycolysis can continue 6.2. Enzymes Enzymes are biological catalysts • Name reflects function; ends in -ase • Has active site to which substrate binds weakly • • • • Causes enzyme shape to change slightly Existing substrate bonds destabilized, new ones form Enzymes are highly specific Enzyme not used up 6.2. Enzymes Enzymes are biological catalysts Enzyme-substrate complex formed Substrate Products released Enzyme Active site Enzyme unchanged (a) Substrate Substrate Enzyme Enzyme (b) (c) (b, c): From Voet: Biochemistry, 1/e, 0471617695, 1990, John Wiley & Sons 6.2. Enzymes Copyright © The McGraw-Hill Companies, Inc. Permission required for reproduction or display. Cofactors assist some enzymes • Cofactors can assist different enzymes; fewer types needed Enzyme • Include magnesium, zinc, copper, other trace elements • Coenzymes are organic cofactors • Include electron carriers FAD, NAD+, NADP+ Cofactor Substrate 6.2. Enzymes Environmental Factors Influencing Enzyme Activity • Enzymes have narrow range of optimal conditions • Temperature, pH, salt concentration • 10°C increase doubles speed of enzymatic reaction up until maximum • Proteins denature at higher temperatures Enzyme activity Optimum temperature Enzyme activity • Low salt, neutral pH usually optimal 1 2 3 4 5 6 7 8 9 10 11 12 13 Acidic Basic Temperature (a) Optimum pH (b) 6.2. Enzymes Allosteric Regulation • Enzyme activity controlled by binding to allosteric site • Distorts enzyme shape, prevents or enhances binding • Regulatory molecule is usually end product • Allows feedback inhibition Copyright © The McGraw-Hill Companies, Inc. Permission required for reproduction or display. Enzyme Enzyme Allosteric inhibitor Substrate Allosteric site Active site (b) (a) Allosteric inhibitor Starting compound (c) Enzyme a Intermediatea Enzyme b Enzyme c Intermediateb End product 6.2. Enzymes Enzyme Inhibition • Site to which inhibitor binds determines type • Competitive inhibitor binds to active site of enzyme • Chemical structure usually similar to substrate • Concentration dependent; blocks substrate • Example is sulfa drugs blocking folic acid synthesis Structural differences PABA (substrate) H HO N O C H O S O Sulfa (inhibitor) N H H PABA Enzyme (a) N (b) H H Sulfanilamide 6.2. Enzymes Enzyme Inhibition (continued…) • Non-competitive inhibitor binds to a different site • Allosteric inhibitors are one example; action is reversible • Some non-competitive inhibitors are not reversible – E.g., mercury oxidizes the S—H groups of amino acid cysteine, converts to cystine – Cystine cannot form important disulfide bond (S—S) – Enzyme changes shape, becomes nonfunctional 6.3. The Central Metabolic Pathways ATP Reducing power: NADH, FADH2, NADPH Precursor metabolites • Glucose molecules can have different fates • Can be completely oxidized to CO2 for maximum ATP • Can be siphoned off as precursor metabolite for use in biosynthesis 6.3. The Central Metabolic Pathways Copyright © The McGraw-Hill Companies, Inc. Permission required for reproduction or display. GLUCOSE 2 Glycolysis Pentose phosphate pathway Starts the oxidation of glucose Yields Glycolysis Oxidizes glucose to pyruvate 1 P~ P~ P + Reducing power ATP by substrate-level phosphorylation Yields Reducing power Biosynthesis 5 Fermentation Reduces pyruvate or a derivative Acids, alcohols, and gases • Converts 1 glucose to 2 pyruvates; yields net 2 ATP, 2 NADH • Investment phase: • 2 phosphate groups added • Glucose split to two 3-carbon molecules • Pay-off phase: • 3-carbon molecules converted to pyruvate • Generates 4 ATP, 2 NADH total Nets 2 ATP 3a Glucose Transition step CO2 CO2 Yields Reducing power Pyruvate Pyruvate x2 CO2 ATP ~ ~ CO2 3b TCA cycle Incorporates an acetyl group and releases CO2 (TCA cycles twice) ~ ADP Yields P~ P ~ P + ATP by substrate-level phosphorylation 1 ATP is expended to add a phosphate group. Reducing power 4 Respiration Uses the electron transport Chain to convert reducing power to proton motive force Yields P~ P~ P ATP by oxidative phosphorylation Glucose 6-phosphate 2 A chemical rearrangement occurs. Fructose 6-phosphate ~ ~ ATP 3 ATP is expended to add a phosphate group. 4 The 6-carbon molecule is split into two 3-carbon molecules. ~ ADP Fructose 1,6-bisphosphate Dihydroxyacetone phosphate A chemical rearrangement of one of the molecules occurs. 5 Glyceraldehyde 3-phosphate NAD+ NADH + H+ 1,3-bisphosphoglycerate ADP ATP ~ NAD+ 6 NADH + H+ ~ The addition of a phosphate group is coupled to a redox reaction, generating NADH and a high-energy phosphate bond. ~ ~ 7 ~ ~ ~ ~ ATP is produced by substrate-level phosphorylation. 3-phosphoglycerate 8 2-phosphoglycerate H2O A chemical rearrangement occurs. 9 H2O Phosphoenolpyruvate ADP ATP Pyruvate ~ ~ ~ ~ ~ ~ Water is removed, causing the phosphate bond to become high-energy. 10 ATP is produced by substrate-level phosphorylation. 6.3. The Central Metabolic Pathways Pentose Phosphate Pathway • Also breaks down glucose • Important in biosynthesis of precursor metabolites • Ribose 5-phosphate, erythrose 4-phosphate • Also generates reducing power: NADPH • Yields vary depending upon alternative taken 6.3. The Central Metabolic Pathways Transition Step GLUCOSE • CO2 is removed from pyruvate • Electrons reduce NAD+ to NADH + H+ • 2-carbon acetyl group joined to coenzyme A to form acetyl-CoA • Takes place in mitochondria in eukaryotes 2 Pentose phosphate pathway Starts the oxidation of glucose Yields Glycolysis Oxidizes glucose to pyruvate 1 ~ ~ + Reducing power ATP by substrate-level phosphorylation Pyruvate Yields CO2 Reducing power Biosynthesis Pyruvate 3a Pyruvate NAD+ Acids, alcohols, and gases CoA Transition step CO2 Yields Transition step: CO2 is removed, a redox reaction generates NADH, and coenzyme A is added. Fermentation Reduces pyruvate or a derivative 5 CO2 Reducing power AcetylCoA AcetylCoA NADH + H+ x2 CO2 CoA CO2 3b TCA cycle Incorporates an acetyl group and releases CO2 (TCA cycles twice) Acetyl-CoA 1 The acetyl group is transferred to oxaloacetate to start a new round of the cycle. Yields ~ ~ + Reducing power ATP by substrate-level phosphorylation CoA Respiration Uses the electron transport chain to convert reducing power to proton motive force 4 Yields ~ ~ ATP by oxidative phosphorylation NADH + H+ 2 A chemical rearrangement occurs. Oxaloacetate Citrate A redox reaction generates NADH. 8 NAD+ Isocitrate NAD+ Malate Water is added. 7 3 A redox reaction generates NADH and CO2 is removed. NADH + H+ H2 O CO2 Fumarate -ketoglutarate NAD+ 4 FADH2 6 CoA A redox reaction generates FADH2- NADH + H+ FAD 5 The energy released during CoA removal is harvested to produce ATP. CoA Succinyl-CoA Succinate CoA ~ ~ ATP ~ + Pi ADP CO2 A redox reaction generates NADH, CO2 is removed, and coenzyme A is added. 6.3. The Central Metabolic Pathways Tricarboxylic Acid (TCA) Cycle (Krebs) GLUCOSE 2 Pentose phosphate pathway Starts the oxidation of glucose • • • • • ~ ~ + Reducing power ATP by substrate-level phosphorylation Pyruvate Yields CO2 Reducing power Biosynthesis Pyruvate 3a Pyruvate NAD+ Acids, alcohols, and gases CoA Transition step CO2 Yields Transition step: CO2 is removed, a redox reaction generates NADH, and coenzyme A is added. Fermentation Reduces pyruvate or a derivative 5 CO2 Reducing power AcetylCoA AcetylCoA • Completes oxidation of glucose Produces Yields Glycolysis Oxidizes glucose to pyruvate 1 NADH + H+ x2 CO2 CoA CO2 3b TCA cycle Incorporates an acetyl group and releases CO2 (TCA cycles twice) Acetyl-CoA 1 The acetyl group is transferred to oxaloacetate to start a new round of the cycle. Yields ~ ~ + Reducing power ATP by substrate-level phosphorylation CoA Respiration Uses the electron transport chain to convert reducing power to proton motive force 4 Yields ~ ~ ATP by oxidative phosphorylation NADH + H+ 2 A chemical rearrangement occurs. Oxaloacetate Citrate A redox reaction generates NADH. 8 NAD+ 2 CO2 2 ATP 6 NADH 2 FADH2 Precursor metabolites Isocitrate NAD+ Malate Water is added. 7 3 A redox reaction generates NADH and CO2 is removed. NADH + H+ H2 O CO2 Fumarate -ketoglutarate NAD+ 4 FADH2 6 CoA A redox reaction generates FADH2- NADH + H+ FAD 5 The energy released during CoA removal is harvested to produce ATP. CoA Succinyl-CoA Succinate CoA ~ ~ ATP ~ + Pi ADP CO2 A redox reaction generates NADH, CO2 is removed, and coenzyme A is added. 6.4. Respiration Uses reducing power (NADH, FADH2) generated by glycolysis, transition step, and TCA cycle to synthesize ATP • Electron transport chain generates proton motive force • Drives synthesis of ATP by ATP synthase • Process proposed by British scientist Peter Mitchell in 1961 • Initially widely dismissed • Mitchell conducted years of self-funded research • Received a Nobel Prize in 1978 • Now called chemiosmotic theory The Electron Transport Chain—Generating Proton Motive Force Electron transport chain is membrane-embedded electron carriers • • • • • Pass electrons sequentially, eject protons in process Prokaryotes: in cytoplasmic membrane Eukaryotes: in inner mitochondrial membrane Energy gradually released Release coupled to ejection of protons • Creates electrochemical gradient (“Battery”) • Used to synthesize ATP • Prokaryotes can also power transporters, flagella Electrons from the energy source 2 e– Energy released is used to generate a proton motive force. High energy Low energy Electrons donated to the terminal electron acceptor. 2 H+ 1/ 2 H2O O2 The Electron Transport Chain—Generating Proton Motive Force Components of an Electron Transport Chain • Most carriers grouped into large protein complexes • Serve as proton pumps • Three general groups are notable • Quinones • Lipid-soluble molecules • Move freely, can transfer electrons between complexes • Cytochromes • Contain heme, molecule with iron atom at center • Several types • Flavoproteins • Proteins to which a flavin is attached • FAD, other flavins synthesized from riboflavin The Electron Transport Chain—Generating Proton Motive Force General Mechanisms of Proton Ejection • Some carriers accept only hydrogen atoms (protonelectron pairs), others only electrons • Spatial arrangement in membrane shuttles protons to outside of membrane • When hydrogen carrier accepts electron from electron carrier, it picks up proton from inside cell – or mitochondrial matrix • When hydrogen carrier passes electrons to electron carrier, protons released to outside of cell – or intermembrane space of mitochondria • Net effect is movement of protons across membrane • Establishes concentration gradient • Driven by energy released during electron transfer The Electron Transport Chain—Generating Proton Motive Force Electron Transport Chain of Mitochondria • Complex I (NADH dehydrogenase complex) • Accepts electrons from NADH, transfers to ubiquinone • Pumps 4 protons • Complex II (succinate dehydrogenase complex) • Accepts electrons from TCA cycle via FADH2, “downstream” of those carried by NADH • Transfers electrons to ubiquinone • Complex III (cytochrome bc1 complex) • Accepts electrons from ubiquinone from Complex I or II • 4 protons pumped; electrons transferred to cytochrome c • Complex IV (cytochrome c oxidase complex) • Accepts electrons from cytochrome c, pumps 2 protons • Terminal oxidoreductase, meaning transfers electrons to terminal electron acceptor (O2) The Electron Transport Chain of Mitochondria Copyright © The McGraw-Hill Companies, Inc. 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GLUCOSE 2 Pentose phosphate pathway Starts the oxidation of glucose Yields 1 Yields Glycolysis Oxidizes glucose to pyruvate P ~ P ~P + Reducing power ATP by substrate-level phosphorylation Reducing power Biosynthesis 5 Pyruvate Pyruvate Eukaryotic cell Fermentation Reduces pyruvate or a derivative Acids, alcohols, and gases 3a Transition step CO2 Yields CO2 Reducing power AcetylCoA AcetylCoA x2 CO2 CO2 TCA cycle 3b Incorporates an acetyl group and releases CO2 (TCA cycles twice) Yields Inner mitochondrial membrane Reducing power ATP by substrate-level phosphorylation 4 Respiration Uses the electron transport chain to convert reducing power to proton motive force Yields P P P ATP by oxidative phosphorylation Complex III Complex I 4 H+ 4 Ubiquinone + Complex II NAD+ Complex IV H+ 2 Proton motive force is used to drive: H+ ATP synthase (ATP synthesis) 10 H+ Cytochrome c Intermembrane space 2 e– Path of electrons NADH Use of Proton Motive Force Electron Transport Chain 1/ 2 H+ H2O 2 Mitochondrial matrix O2 Terminal electron acceptor H+ 3 ATP + 3 Pi 3 ADP The Electron Transport Chain—Generating Proton Motive Force Electron Transport Chain of Prokaryotes • Tremendous variation: even single species can have several alternate carriers • E. coli serves as example of versatility of prokaryotes • Aerobic respiration in E. coli • Can use 2 different NADH dehydrogenases – Proton pump equivalent to complex I of mitochondria • Can produce several alternatives to optimally use different energy sources, including H2 • Lack equivalents of complex III or cytochrome c – Quinones shuttle electrons directly to ubiquinol oxidase, a terminal oxidoreductase – Two versions for high or low O2 concentrations The Electron Transport Chain—Generating Proton Motive Force Electron Transport Chain of Prokaryotes (cont…) • Anaerobic respiration in E. coli • Harvests less energy than aerobic respiration – Lower electron affinities of terminal electron acceptors • Some components different • Can synthesize terminal oxidoreductase that uses nitrate as terminal electron acceptor – Produces nitrite – E. coli converts to less toxic ammonia • Sulfate-reducers use sulfate (SO42–) as terminal electron acceptor • Produce hydrogen sulfide as end product The Electron Transport Chain—Generating Proton Motive Force Copyright © The McGraw-Hill Companies, Inc. 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Prokaryotic cell Cytoplasmic membrane Electron Transport Chain NADH dehydrogenase Uses of Proton Motive Force Ubiquinol veoxidase force rive: H+ (2 or 4) H+ (0 or 4) Ubiquinone Path of electrons ATP synthase (ATP synthesis) Active transport (one mechanism) 10 H+ Rotation of a flagella H+ H+ Proton motive force is used to drive: Transported molecule Outside of cytoplasmic membrane 2 e– – Cytoplasm Succinate dehydrogenase NADH + NAD+ 2 H+ 1/ H2O 2 O2 Terminal electron acceptor H+ 3 ATP + 3 Pi 3 ADP The Electron Transport Chain—Generating Proton Motive Force ATP Synthase—Harvesting the Proton Motive Force to Synthesize ATP • Energy required to establish gradient • Released when gradient is eased • ATP synthase allows protons to flow down gradient in controlled manner • Uses Proton energy to add phosphate group to ADP • 1 ATP formed from entry of ~3 protons • Calculating yields • Based on experiments on rat mitochondria: ~2.5 ATP made per electron pair from NADH ~1.5 ATP made per electron pair from FADH2 The Electron Transport Chain—Generating Proton Motive Force Calculating theoretical maximum yields • In prokaryotes: • • • • Glycolysis: 2 NADH 6 ATP Transition step: 2 NADH 6 ATP TCA Cycle: 6 NADH 18 ATP; 2 FADH2 4 ATP Total maximum oxidative phosphorylation yield = 34 ATP • Slightly less in eukaryotic cells • NADH from glycolysis in cytoplasm transported across mitochondrial membrane to enter electron transport chain – Requires ~1 ATP per NADH generated The Electron Transport Chain—Generating Proton Motive Force ATP Yield of Aerobic Respiration in Prokaryotes • Substrate-level phosphorylation: • 2 ATP (from glycolysis; net gain) • 2 ATP (from the TCA cycle) • 4 ATP (total) • Oxidative phosphorylation: • • • • 6 ATP (from reducing power gained in glycolysis) 6 ATP (from reducing power gained in transition step) 22 ATP (from reducing power gained in TCA cycle) 34 (total) • Total ATP gain (theoretical maximum) = 38 ATP Yield of Aerobic Respiration in Prokaryotes Copyright © The McGraw-Hill Companies, Inc. 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GLUCOSE 2 Pentose phosphate pathway Starts the oxidation of glucose Yields Glycolysis Oxidizes glucose to pyruvate 1 Reducing power GLUCOSE ATP by substrate-level phosphorylation Glycolysis Oxidizes glucose to pyruvate Yields Reducing power Biosynthesis 5 Pyruvate 3a Pyruvate Fermentation Reduces pyruvate or a derivative ~ ~ Acids, alcohols, and gases Transition step CO2 Yield CO2 2 ATP net gain = 0 Reducing power AcetylCoA AcetylCoA x2 CO2 ~ ~ CO2 3b TCA cycle Incorporates an acetyl group and releases CO2 (TCA cycles twice) 2 ATP Yields Reducing power ATP by substrate-level phosphorylation 4 Respiration Uses the electron transport chain to convert reducing power to proton motive force Yields ATP by oxidative phosphorylation 2 NADH Oxidative phosphorylation ~ ~ 6 ATP ~ ~ Substrate-level phosphorylation Pyruvate 2 ATP Pyruvate 2 NADH AcetylCoA ~ ~ Oxidative phosphorylation 6 ATP Oxidative phosphorylation 18 ATP AcetylCoA 6 NADH x2 CO2 2 FADH2 CO2 TCA cycle Incorporates an acetyl group and releases CO2 (TCA cycles twice) ~ ~ ~ ~ Oxidative phosphorylation 4 ATP Substrate-level phosphorylation 2 ATP ~ ~ 6.5. Fermentation Fermentation used when respiration not an option • E. coli is facultative anaerobe • Aerobic respiration, anaerobic respiration, and fermentation GLUCOSE Pentose phosphate pathway Starts the oxidation of glucose 2 Yields Glycolysis Oxidizes glucose to pyruvate 1 P ~ ~P + P Reducing power ATP by substrate-level phosphorylation Yields Reducing power Biosynthesis Fermentation Reduces pyruvate or a derivative 5 Pyruvate Pyruvate Acids, alcohols, and gases 3a Transition step CO2 CO2 Yields Reducing power AcetylCoA AcetylCoA • Streptococcus pneumoniae lacks electron transport chain x CO2 2 CO2 3b TCA cycle Incorporates an acetyl group and releases CO2 (TCA cycles twice) Yields P ~ P ~ Reducing power P ATP by substrate-level phosphorylation + 4 • Fermentation only option Yields P ~ P ~ P ATP by oxidative phosphorylation • ATP-generating reactions are only those of glycolysis • Additional steps consume excess reducing power – Regenerate NAD+ Respiration Uses the electron transport chain to convert reducing power to proton motive force NADH + H+ NAD+ O H3C C O O– C H3C OH O C C O– H Lactate Pyruvate (a) Lactic acid fermentation CO2 O H3C C NADH + H+ O O C O– Pyruvate (b) Ethanol fermentation H3C C H Acetaldehyde NAD+ OH H3C C H Ethanol H 6.5. Fermentation Fermentation end products varied; helpful in identification, commercially useful • Ethanol • Butyric acid • Propionic acid • 2,3-Butanediol • Mixed acids Copyright © The McGraw-Hill Companies, Inc. Permission required for reproduction or display. Pyruvate Fermentation pathway Microorganisms End products Lactic acid Ethanol Butyric acid Propionic acid Mixed acids 2,3-Butanediol Streptococcus Lactobacillus Saccharomyces Clostridium Propionibacterium E. coli Enterobacter Lactic acid Ethanol CO2 Butyric acid Butanol Acetone Isopropanol CO2 H2 Propionic acid Acetic acid CO2 Acetic acid Lactic acid Succinic acid Ethanol CO2 H2 CO2 H2 (yogurt, dairy, pickle), b (wine, beer), (acetone): © Brian Moeskau/McGraw- Hill; (cheese): © Photodisc/McGraw-Hill; (Voges-Proskauer Test), (Methyl-Red Test): © The McGraw-Hill Companies, Inc./Auburn University Photographic Services 6.6. Catabolism of Organic Compounds Other than Glucose Microbes can use variety of compounds • Excrete hydrolytic enzymes; transport subunits into cell • Degrade further to appropriate precursor metabolites • Polysaccharides and disaccharides • Amylases digest starch; cellulases digest cellulose • Disaccharides hydrolyzed by specific disaccharidases • Lipids • Fats hydrolyzed by lipases; glycerol converted to dihydroxyacetone phosphate, enters glycolysis • Fatty acids degraded by β-oxidation to enter TCA cycle • Proteins • Hydrolyzed by proteases; amino group deaminated • Carbon skeletons converted into precursor molecules 6.6. Catabolism of Organic Compounds Other than Glucose Microbes can use variety of compounds (cont…) • Convert to precursor metabolites • Enter appropriate metabolic pathways POLYSACCHARIDES Starch Cellulose amylases lipases glycerol cellulases disaccharidases monosaccharides (simple sugars) Pentose phosphate pathway LIPIDS (fats) DISACCHARIDES Lactose Maltose Sucrose + GLUCOSE PROTEINS proteases Amino acids deamination fatty acids NH3 Glycolysis Applies to both branches In glycolysis Pyruvate Pyruvate AcetylCoA AcetylCoA X2 TCA cycle ß-oxidation removes 2-carbon units. 6.7. Chemolithotrophs Prokaryotes unique in ability to use reduced inorganic compounds as sources of energy • E.g., hydrogen sulfide (H2S), ammonia (NH3) • Produced by anaerobic respiration from inorganic molecules (sulfate, nitrate) serving as terminal electron acceptors • Important example of nutrient cycling • Four general groups 6.8. Photosynthesis Photosynthesis • Plants, algae, several groups of bacteria • General reaction is Light Energy 6 CO2 + 12 H2X C6H12O6 + 12 X + 6 H2O where X indicates element such as oxygen or sulfur • Can be considered in two distinct stages • Light reactions (light-dependent reactions) – Capture energy and convert it to ATP • Light-independent reactions (dark reactions) – Use ATP to synthesize organic compounds – Involves carbon fixation 6.8. Photosynthesis Photosynthesis (continued…) • Many variations found in approaches • Oxygenic and anoxygenic 6.8. Photosynthesis Capturing Radiant Energy • Colors observed are those of wavelength reflected • Pigments are located in photosystems within membranes • Chlorophylls (plants, algae, cyanobacteria) • Bacteriochlorophylls (anoxygenic bacteria) – Absorb different wavelengths than chlorophylls • Accessory pigments absorb at additional wavelengths – Carotenoids (many photosynthetic prokaryotes and eukaryotes) – Phycobilins (cyanobacteria, red algae) • Antennae pigments form complex • Funnel energy to reaction-center pigment 6.8. Photosynthesis Reaction-center pigments • Donate excited electrons to electron transport chain – Chlorophyll a (plants, algae, cyanobacteria) – Bacteriochlorophylls (anoxygenic bacteria) • Cyanobacteria: photosystems in membranes of stacked structures inside cell termed thylakoids • Plants, algae: thylakoids in stroma of chloroplast • Endosymbiotic theory explains • Purple bacteria: in cytoplasmic membrane, extensive infoldings • Green bacteria: specialized chlorosomes attached to cytoplasmic membrane Copyright © The McGraw-Hill Companies, Inc. Permission required for reproduction or display. Photosystem Radiant energy Electron transport chain Reaction-center chlorophyll e– Chlorophyll molecule Photosynthetic membrane Converting Radiant Energy into Chemical Energy Light-dependent reactions in cyanobacteria and photosynthetic eukaryotes • Two distinct photosystems (I and II) • Cyclic photophosphorylation – Photosystem I alone produces ATP – Reaction-center chlorophyll is terminal electron acceptor • Non-cyclic photophosphorylation – Used when cells need both ATP and reducing power • Electrons from photosystem II drive photophosphorylation – Are then donated to photosystem I – Photosystem II replenishes electrons by splitting water – Generates oxygen (process is oxygenic) • Electrons from photosystem I reduce NADP+ to NADPH Converting Radiant Energy into Chemical Energy Excited chlorophyll Proton gradient formed for ATP synthesis Excited chlorophyll H+ Electron carrier e– NADP reductase e– e– Energy of electrons NADPH NADP+ Proton pump Reactioncenter chlorophyll Radiant energy Electron carrier Electron carrier Reactioncenter chlorophyll e- Radiant energy Water-splitting enzyme Z 2 H2O e– 4 H Photosystem II + O2 Proton pump Photosystem I NADP reductase Converting Radiant Energy into Chemical Energy Light-dependent reactions in anoxygenic photosynthetic bacteria • Each has single photosystem • Cannot use water as electron donor, so anoxygenic • Use electron donors such as hydrogen gas (H2), hydrogen sulfide (H2S), organic compounds • Purple bacteria: photosystem similar to photosystem II • Energy of electrons insufficient to reduce NAD+ – Instead expend ATP to use reversed electron transport • Green bacteria: photosystem similar to photosystem I • Electrons can generate proton motive force or reduce NAD+ 6.9. Carbon Fixation Chemolithoautotrophs, photoautotrophs use CO2 to synthesize organic compounds: carbon fixation • In photosynthetic organisms: light-independent reactions • Consumes lots of ATP, reducing power • Reverse process of oxidizing compounds to CO2 liberates a lot of energy! • Calvin cycle most commonly used • Three essential stages • Incorporation of CO2 into organic compounds • Reduction of resulting molecule • Regeneration of starting compound • Six “turns” of cycle: net gain of one fructose-6-phosphate • Consumes 18 ATP, 12 NADPH per fructose molecule 6.9. Carbon Fixation Copyright © The McGraw-Hill Companies, Inc. Permission required for reproduction or display. 1 6 Carbon dioxide is added to ribulose 1,5-bisphosphate to start a new round of the cycle. CO2 12 molecules 3-phosphoglycerate ~ ~ 6 molecules ribulose 1,5-bisphosphate 12 ATP STAGE 1 ~ 12 ADP 12 molecules 1,3-bisphosphoglycerate ~ STAGE 3 6 ADP STAGE 2 ~ ~ 6 ATP 3 6 molecules ribulose 5-phosphate Ribulose 1,5-bisphosphate is regenerated so that the cycle Can continue. 12 NADPH + H+ 12 molecules glyceraldehyde 3-phosphate 12 NADP+ 12 Pi Series of complex reactions 2 1 molecule fructose 6-phosphate Cell components ATP and NADPH are used to reduce the product of stage1, producing glyceraldehyde 3-phosphate, which can be used in biosynthesis. 6.10. Anabolic Pathways—Synthesizing Subunits from Precursor Molecules Prokaryotes remarkably similar in biosynthesis • Synthesize subunits using central metabolic pathways • If enzymes lacking, end product must be supplied • Fastidious bacteria require many growth factors • Lipid synthesis requires fatty acids, glycerol • Fatty acids: 2-carbon units added to acetyl group from acetyl-CoA • Glycerol: dihydroxyacetone phosphate from glycolysis • Nucleotide synthesis • • • • DNA, RNA initially synthesized as ribonucleotides Purines: atoms added to ribose 5-phosphate to form ring Pyrimidines: ring made, then attached to ribose 5-phosphate Can be converted to other nucleobases of same type 6.10. Anabolic Pathways—Synthesizing Subunits from Precursor Molecules Copyright © The McGraw-Hill Companies, Inc. Permission required for reproduction or display. Glycolysis Pentose phosphate pathway Glucose 6-phosphate Fructose 6-phosphate Lipopolysaccharide (polysaccharide) Ribose 5-phosphate Erythrose 5-phosphate Nucleotides amino acids (histidine) Amino acids (phenylalanine, tryptophan, tyrosine) Peptidoglycan Dihydroxyacetone phosphate Lipids (glycerol component) 3-phosphoglycerate Amino acids (cysteine, glycine, serine) Phosphoenolpyruvate Amino acids (phenylalanine, tryptophan, tyrosine) Pyruvate Pyruvate Acetyl-CoA Acetyl-CoA Amino acids (alanine, leucine, valine) Lipids (fatty acids) Oxaloacetate Amino acids (aspartate, asparagine, isoleucine, lysine, methionine, threonine) X2 - ketoglutarate TCA cycle Amino acids (arginine, glutamate, glutamine, proline) 6.10. Anabolic Pathways—Synthesizing Subunits from Precursor Molecules Amino Acid Synthesis • Synthesis of glutamate provides mechanism for incorporation of nitrogen into organic material • Ammonium (NH4+) commonly used via glutamate synthesis • Transamination can generate other amino acids NH2 α-ketoglutarate Glutamate is synthesized by adding ammonia to the precursor metabolite α-ketoglutarate. Aspartate Oxaloacetate NH3 (ammonia) NH2 Glutamate The amino group (NH2) of glutamate can be transferred to other carbon compounds to produce other amino acids. 6.10. Anabolic Pathways—Synthesizing Subunits from Precursor Molecules Amino Acid Synthesis (continued…) • Aromatic amino acids: carefully regulated branch points • Tryptophan is feedback inhibitor of enzyme that directs branch to its synthesis – Pathway instead leads to tyrosine, phenylalanine – Tyrosine, phenylalanine likewise inhibit first enzyme of branch leading to their synthesis • The three amino acids also regulate formation of original 7-carbon compound (three different enzymes catalyze) From glycolysis Phenylalanine Compound a 3-C + 4-C From pentose phosphate pathway 7-C compound Branch point II Branch point I Tyrosine Compound b Tryptophan