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CHAPTER 5. Aerobic Respiration and the Mitochondrion. Introduction. The early Earth was populated by anarobes , which captured and utilized energy by oxygen-independent metabolism. Oxygen accumulated in the primitive atmosphere after cyanobacteria appeared.
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CHAPTER 5 Aerobic Respiration and the Mitochondrion
Introduction • The early Earth was populated by anarobes, which captured and utilized energy by oxygen-independent metabolism. • Oxygen accumulated in the primitive atmosphere after cyanobacteria appeared. • Aerobes evolved to use oxygen to extract more energy from organic molecules. • In eukaryotes, aerobic respiration takes place in the mitochondrion.
5.1 Mitochondrial Structure and Function (1) • Mitochondria have characteristic morphologies despite variable appearance. • Typical mitochondria are bean-shaped organelles but may be round or threadlike. • The size and number of mitochondria reflect the energy requirements of the cell.
Mitochondrial Structure and Function (2) • Mitochondria can fuse with one another, or split in two. • The balance between fusion and fission is likely a major determinant of mitochondrial number, length, and degree of interconnection.
Mitochondrial Structure and Function (3) • Inner and outer mitochondrial membranes enclose two spaces: the matrix and intermembrane space. • The outer mitochondrial membrane serves as its outer boundary. • The inner mitochondrial membrane is subdivided into two interconnected domains: • Inner boundary membrane • Cristae – where the machinery for ATP is located
Mitochondrial Structure and Function (4) • Mitochondrial Membranes • The outer membrane is about 50%; the inner membrane is more than 75% protein. • The inner membrane contains cardiolipin but not cholesterol, both are true of bacterial membranes. • The outer membrane contains a large pore-forming protein called porin. • The inner membrane is impermeable to even small molecules; the outer membrane is permeable to even some proteins.
Mitochondrial Structure and Function (5) • The mitochondrial matrix • Contains a circular DNA molecule, ribosomes, and enzymes. • RNA and proteins can be synthesized in the matrix.
5.2 Oxidative Metabolism in the Mitochondrion (1) • The first steps in oxidative metabolism are carried out in glycolysis. • Glycolysis produces pyruvate, NADH, and two molecules of ATP. • Aerobic organisms use O2 to extract more than 30 additional ATPs from pyruvate and NADH. • Pyruvate is transported across the inner membrane and decarboxylated to form acetyl CoA, which enters the next stage.
Oxidative Metabolism in the Mitochondrion (2) • The tricarboxylic acid (TCA) cycle • It is a stepwise cycle where substrate is oxidized and its energy conserved. • The two-carbon acetyl group from acetyl CoA is condensed with the four-carbon oxaloacetate to form a six-carbon citrate. • During the cycle, two carbons are oxidized to CO2, regenerating the four-carbon oxaloacetate needed to continue the cycle.
Oxidative Metabolism in the Mitochondrion (3) • The TCA cycle (continued) • Four reactions in the cycle transfer a pair of electrons to NAD+ to form NADH, or to FAD+ to form FADH2. • Reaction intermediates in the TCA cycle are common compounds generated in other catabolic reactions making the TCA cycle the central metabolic pathway of the cell.
Catabolic pathways generate compounds that are fed into the TCA cycle
Oxidative Metabolism in the Mitochondrion (4) • The Importance of Reduced Coenzymes in the Formation of ATP • The reduced coenzymes FADH2 and NADH are the primary products of the TCA cycle. • NADH formed during glycolysis enters the mitochondria via malate-aspartate or glycerol phosphate shuttles.
Oxidative Metabolism in the Mitochondrion (5) • The Importance of Reduced Coenzymes • As electrons move through the electron-transport chain, H+ are pumped out across the inner membrane. • ATP is formed by the controlled movement of H+ back across the membrane through the ATP-synthesizing enzyme.
Oxidative Metabolism in the Mitochondrion (6) • Reduced coenzymes (continued) • The coupling of H+ translocation to ATP synthesis is called chemiosmosis. • Three molecules of ATP are formed from each pair of electrons donated by NADH; two molecules of ATP are formed from each pair of electrons donated by FADH2.
The Human Perspective: The Role of Anaerobic and Aerobic Metabolism in Exercise (1) • ATP hydrolysis increases 100-fold during exercise, quickly exhausting ATP available. • Muscles used stored creatine phosphate (CrP) to rapidly generate but must rely on aerobic or anaerobic synthesis of new ATP for sustained activity. CrP + ADP Cr + ATP
The Human Perspective: The Role of Anaerobic and Aerobic Metabolism in Exercise (2) • Fast-twitch muscle fibers contract rapidly, have few mitochondria ad produce ATP anaerobically. • Anaerobic metabolism produces fewer ATPs per glucose but produces them very fast. • Anaerobic metabolism rapidly depletes available glucose and builds up lactic acid which reduces cellular pH.
The Human Perspective: The Role of Anaerobic and Aerobic Metabolism in Exercise (3) • Slow-twitch fibers contract slowly, have many mitochondria and produce most of their ATP by aerobic metabolism. • Aerobic metabolism initially uses glucose as a substrate. • Free fatty acids are oxidized during prolonged exercise. • Ratio of fast- to slow-twitch fibers is variable and depends on the normal function of the muscle.
5.3 The Role of Mitochondria in the Formation of ATP (1) • ATP can be formed by substrate-level phosphorylation or oxidative phosphorylation. • Accounts for > 160 kg of ATP in our bodies per day
The Role of Mitochondria in the Formation of ATP (2) • Oxidation-Reduction (Redox) Potentials • Strong oxidizing agents have a high affinity for electrons; strong reducing agents have a weak affinity for electrons • Redox reactions are accompanied by a decrease in free energy. • The transfer of electrons causes charge separation that can be measured as a redox potential.
The Role of Mitochondria in the Formation of ATP (3) • Electron Transport • Electrons move through the inner membrane via a series of carriers of decreasing redox potential. • Electrons associated with either NADH or FADH2 are transferred through specific electron carriers that make up the electron transport chain.
The Role of Mitochondria in the Formation of ATP (4) • Types of Electron Carriers • Flavoproteins are polypeptides bound to either FAD or FMN. • Cytochromes contain heme groups bearing Fe or Cu metal ions. • Three cooper atoms are located within a single protein complex and alternate between Cu2+/Cu3+ • Ubiquinone (coenzyme Q) is a lipid-soluble molecule made of five-carbon isoprenoid units.
The Role of Mitochondria in the Formation of ATP (5) • Types of Electron Carriers (continued) • Iron-sulfur proteins contain Fe in association with inorganic sulfur. • These carriers are arranged in order of increasingly positive redox potential. • Sequence of carriers determined by use if inhibitors.
The Role of Mitochondria in the Formation of ATP (6) • Electron-Transport Complexes • Complex I (NADH dehydrogenase) catalyzes transfer of electrons from NADH to ubiquinone and transports four H+ per pair. • Complex II (succinatedehydrogenase) catalyzes transfer of electrons from succinate to FAD to ubiquinone without transport of H+. • Complex III (cytochrome bc1) catalyzes the transfer of electrons from ubiquinone to cytochrome c and transports four H+ per pair.
The electron-transport chain of the inner mitochondrial membrane
The electron-transport chain of the inner mitochondrial membrane
The Role of Mitochondria in the Formation of ATP (7) • Electron-Transport Complexes (continued) • Complex IV (cytochrome c oxidase) catalyzes transfer of electrons to O2 and transports H+ across the inner membrane. • Cytochrome oxidase is a large complex that adds four electrons to O2 to form two molecules of H2O. • The metabolic poisons CO, N3–, and CN– bind catalytic sites in Complex IV.
The Role of Mitochondria in the Formation of ATP (8) • Cytochrome oxidase • Electrons are transferred one at a time. • Energy released by O2 reduction is presumably used to drive conformational changes. • These changes would promote the movement of H+ ions and through the protein.
5.4 Translocation of Protons and the Establishment of a Proton-Motive Force (1) • There are two components of the proton gradient: • The concentration gradient between the matrix and intermembrane space creates a pH gradient (ΔpH). • The separation of charge across the membrane creates an electric potential (Ψ). • The energy present in both components of the gradients is proton-motive force (Δp).
Translocation of Protons and the Establishment of a Proton-Motive Force (2) • Dinitrophenol (DNP) uncouples glucose oxidation and ATP formation by increasing the permeability of the inner membrane to H+, thus eliminating the proton gradient. • Differences in uncoupling proteins (UCPs) account for differences in metabolic rate.
5.5 The Machinery for ATP Formation (1) • Isolation of coupling factor 1, or F1, showed that it hydrolyzed ATP. • Under experimental conditions, it behaves as an ATP synthase. • Led to conclusion that an ionic gradient establishes a proton-motive force to phosphorylate ADP.
An experiment to drive ATP formation in membrane vesicles reconstituted with the Na+/K+-ATPase
The Machinery for ATP Formation (2) • The structure of the ATP synthase: • The F1 particle is the catalytic subunit, and contains three catalytic sites for ATP synthesis. • The F0 particle attaches to the F1 and is embedded in the inner membrane. • The F0 base contains a channel through which protons are conducted from the intermembrane space to the matrix–demonstrated in experiments with submitochondrial particles.
ATP formation in experiments with submitochondrial particles
The Machinery for ATP Formation (3) • The Basis of ATP Formation According to the Binding Change Mechanism • The binding change mechanism states the following: • Movement of protons through ATP synthase alters the binding affinity of the active site. • Each active site goes through distinct conformations that have different affinities for substrates and product.
