SlideShare ist ein Scribd-Unternehmen logo

Biochemistry_Bioenergetics

Rengesh Balakrishnan
Rengesh Balakrishnan

The document discusses bioenergetics and several key concepts: 1) Photosynthesis captures energy from sunlight and converts it to chemical energy stored in glucose, which all animals obtain directly or indirectly. 2) Cellular respiration releases energy by combining oxygen and energy-rich compounds to produce ATP, the primary energy carrier in cells. 3) Metabolism consists of catabolic reactions that break down molecules and anabolic reactions that use energy from catabolism to build molecules. Metabolic pathways involve a series of reactions to produce a product.

Bildung
1 von 43
Bioenergetics Dr.B.RENGESH | M.Tech., Ph.D. Associate Professor, Department of Pharmaceutical Technology, Mahendra Engineering College (Autonomous), Namakkal District, Tamil Nadu, India
The Sun and Photosynthesis • The sun is the ultimate source of energy for all biological processes. This energy results from the fusion of hydrogen atoms to form helium atoms: • A portion of this energy reaches the Earth’s surface as sunlight, and is captured by the chlorophyll in plants. This energy drives the conversion of carbon dioxide and water to form glucose, and then into starch, triglycerides, and other forms of stored energy: • All animals obtain energy either directly or indirectly from these energy stores in plants
Cellular Respiration • During cellular respiration, plants and animals combine energy-rich compounds with oxygen from the air, producing CO2 and releasing energy. • Cellular respiration can be represented as: – A portion of the energy released during respiration is captured in the form of adenosine triphosphate (ATP), which stores energy for use in other processes. – The remainder of the energy from respiration is released as heat. An extremely simplified carbon cycle
Energy Flow in the Biosphere
Metabolism • Metabolism is the sum of all reactions occurring in an organism: – catabolism — the reactions involved in the breakdown of biomolecules. – anabolism — the reactions involved in the synthesis of biomolecules. • In general, energy is released during catabolism and required during anabolism. Metabolic Pathways • A metabolic pathway is a sequence of reactions used to produce one product or accomplish one process. – Each pathway consists of a series of chemical reactions that convert a starting material into an end product (e.g., the citric acid cycle and the electron transport chain). – Fortunately, there are a great many similarities among the major metabolic pathways in all life forms.
Catabolism of food • The catabolism of food is a three stage process. Stage I : The digestion of large, complex molecules into simpler ones. – The most common reaction in digestion is hydrolysis: Stage II : The small molecules from digestion are broken down into even simpler units, usually the two-carbon acetyl portion of acetyl coenzyme A (acetyl CoA): – Some energy is produced at this stage, but much more is produced during the oxidation of the acetyl units in Stage III.
Catabolism of food Stage III : This is referred to as the common catabolic pathway because the reactions are the same regardless of the type of food being degraded. – citric acid cycle – electron transport – oxidative phosphorylation • Energy released in Stage III appears in the form of energy-rich molecules of ATP. – The whole purpose of the catabolic pathway is to convert the chemical energy in foods into molecules of ATP, which carries energy to parts of the cell where energy is needed.
ATP – The primary energy carrier – Structure • Adenosine triphosphate, ATP, consists of: – the heterocyclic base adenine – the sugar ribose – a triphosphate group • At physiological pH, the protons on the triphosphate group are removed, giving ATP a charge of -4. – In the cell, it is complexed with Mg2+ in a 1:1 ratio, giving it a net charge of -2. adenine + ribose is called adenosine
ATP – The primary energy carrier – Hydrolysis • The triphosphate group is the part of the molecule that is important in the transfer of biochemical energy. The key reaction is the transfer of a phosphoryl group, —PO3 2-, from ATP to another molecule. – During the hydrolysis of ATP in water, a phosphoryl group is transferred from ATP to a water molecule: – The products are adenosine diphosphate (ADP) and a phosphate ion, often referred to as an inorganic phosphate, Pi, or just phosphate.
ATP – The primary energy carrier – Hydrolysis • The transfer of a phosphoryl group from ATP to water is accompanied by a release of energy. • Free energy, ΔG, is used as a measure of the energy change. – When energy is released, ΔG is negative. – When energy is absorbed, ΔG is positive. – When ΔG is measured under standard conditions, it is represented by ΔG º. – When ΔG º is measured under body conditions, it is represented by ΔG º’. • The liberated free energy is available for use by the cell to carry out processes requiring an input of energy:
ATP – The primary energy carrier – Hydrolysis • Compounds that liberate a large amount of free energy on hydrolysis are called high- energy compounds. • The hydrolysis of ATP to ADP is the principal energy-releasing reaction for ATP. Some other hydrolysis reaction occur under some conditions, such as the hydrolysis of ATP to adenosine monophosphate, AMP, and pyrophosphate, PPi:
ATP – The primary energy carrier – Hydrolysis – This is usually followed by immediate hydrolysis of the pyrophosphate, which releases even more energy: • The hydrolyses of ATP and related compounds are summarized below:
Important Coenzymes in the Common Catabolic Pathway Coenzyme-A • Coenzymes are weakly-bound organic groups that participate in enzyme-catalyzed reactions, often by acting as shuttle systems for the transfer of chemical groups (e.g., hydrogen transport). Many important coenzymes are formed from vitamins. • Coenzyme A is a central compound in metabolism. It is part of acetyl coenzyme A (acetyl CoA), the substance formed from all foods as they pass through Stage II of catabolism.
Important Coenzymes – Coenzyme-A – Components • Components of coenzyme A: – vitamin B5, pantothenic acid, in the center. – a phosphate derivative of ADP – β-mercaptoethylamine, which puts a reactive sulfhydryl group (—SH) at the end of the molecule (CoA—SH).
Important Coenzymes – Coenzyme-A – Nomenclature • The letter A is included in the name Coenzyme A to signify its participation in the transfer of acetyl groups, but Coenzyme A transfers all acyl groups. This is important in fatty acid oxidation and synthesis. • Acyl groups are linked to coenzyme A through the sulfur atom in a thioester bond:
Important Coenzymes – Ubiquinone (Q) • Also called coenzyme Q • A membrane-soluble low molecular weight compound • Long hydrophobic tail keeps Q anchored in the mitochondrial inner membrane • Q is a lipid soluble molecule that diffuses within the lipid bilayer, and shuttles electrons from • Complexes I and II and pass them to III • Not a part of any complex
Important Coenzyme – Nicotinamide Adenine Dinucleotide (NAD+) • NAD+, is an electron transporter which is a derivative of ADP and the vitamin nicotinamide (B3). • The reactive site of NAD+ is in the nicotinamide portion. – When oxidizing a substrate, the nicotinamide ring accepts two electrons and one proton, forming the reduced coenzyme NADH:
Important Coenzyme – Nicotinamide Adenine Dinucleotide (NAD+) • A typical cellular reaction in which NAD+ serves as an electron acceptor is the oxidation of an alcohol: • In this reaction, one hydrogen atom of the alcohol substrate is directly transferred to NAD+, whereas the other appears in solution as H+. Both electrons lost by the alcohol have been transferred to the nicotinamide ring in NADH. • Biochemical reactions involving coenzymes are often written more concisely: – This notation emphasizes the oxidation reaction and the involvement of the coenzyme.
Important Coenzymes – Flavin Adenine Dinucleotide (FAD) • FAD is another major electron carrier. It is a derivative of ADP & the vitamin riboflavin. • The active site is located within the riboflavin ring system. Unlike NAD+, FAD accepts both of the hydrogen atoms lost by the substrate, forming the reduced species FADH2:
Important Coenzymes – Flavin Adenine Dinucleotide (FAD) • The substrates for reactions involving FAD are often those in which a —CH2—CH2— portion of the substrate is oxidized to a double bond:
Mitochandria • The mitochondrion is the powerhouse of the cell. It is the organelle where many of the reactions of the common catabolic pathway occur. It consists of an outer membrane, which surrounds a inner membrane. – The folds of the inner membrane are called cristae. – The space that surrounds them is the matrix. • The enzymes for ATP synthesis (electron transport and oxidative phosphorylation) are located on the cristae. The enzymes for the citric acid cycle are found within the matrix, near the surface of the inner membrane.
An Animal Cell Schematic of typical animal cell: (1) Nucleolus (2) Nuclear membrane (3) Ribosomes (4) Vesicle (5) Rough endoplasmic reticulum (ER) (6) Golgi body (7) Cytoskeleton (8) Smooth ER (9) Mitochondria (10) Vacuole (11) Cytosol (12) Lysosome (13) Centrioles within centrosome
ELECTRON TRANSPORT CHAIN & OXIDATIVE PHOSPHORYLATION Mitochondrial Electron Transport How did we get here? • Summary of glycolysis • Summary of the citric acid cycle (including pyruvate dehydrogenase)
ELECTRON TRANSPORT CHAIN & OXIDATIVE PHOSPHORYLATION
• Final stages of aerobic oxidation of biomolecules in eukaryotes occur in the mitochondrion • Reduced coenzymes NADH and FADH2 from: (1) Aerobic oxidation of pyruvate by the citric acid cycle (2) Oxidation of fatty acids and amino acids Electron Transport Chain is the process by which NADH and FADH2 are oxidized and a proton gradient is formed. Oxidative phosphorylation is the process of making ATP by using the proton gradient generated by the ETC. Respiration by mitochondria: • Oxidation of substrates is coupled to the phosphorylation of ADP • Respiration (consumption of oxygen) proceeds only when ADP is present • The amount of O2 consumed depends upon the amount of ADP added ELECTRON TRANSPORT CHAIN & OXIDATIVE PHOSPHORYLATION
• Respiratory electron-transport chain (ETC) Series of enzyme complexes embedded in the inner mitochondrial membrane, which oxidize NADH and FADH2. Oxidation energy is used to transport protons creating a proton gradient – protons pumped from matrix to intermembrane space across IMM • ATP synthase uses the proton gradient energy to produce ATP; It is the release of the energy in the gradient back through the membrane through the protein ATP Synthase that drives ATP synthesis ELECTRON TRANSPORT CHAIN & OXIDATIVE PHOSPHORYLATION
• The electron transport chain is associated with the mitochondrial inner membrane • Complexes I-IV contain multiple cofactors, and are involved in electron transport • Overall transfer of 2 electrons from NADH through ETC to molecular oxygen: ELECTRON TRANSPORT CHAIN (ETC) – Overview
• Complexes I – where NADH electrons enter the chain • Complex II – Where FADH2 electrons enter the chain • Electrons passed from Complex I or II to Coenzyme Q • Coenzyme Q shuttles electrons to complex III • Complex III shuttles electrons to cytochrome C • Cytochrome C shuttles electrons to Complex IV • Complex IV transfers electrons to O2 which is then reduced to water • Flow through Complexes I, III and IV release energy which is used to pump protons across the IMM and form a “proton gradient” • Proton gradient has lots of potential energy • When the energy is released (protons flow back into matrix through ATP synthase), the energy drives ATP synthesis ELECTRON TRANSPORT CHAIN (ETC) – Overview
• Also called NADH-ubiquinone oxidoreductase • Complex I includes a flavoprotein (contains FMN – related to FAD) and proteins with Fe- S centers (iron-sulfur clusters) • These proteins provide two centers for oxidation reduction reactions ETC – Electron transfer and proton flow in Complex I • Transfers electrons from NADH to Coenzyme Q via FMN and iron-sulfur proteins • NADH transfers a two electrons as a hydride ion (H:-) to FMN • Reduction of Q to QH2 requires 2 e- • About 4 H+ translocated per 2 e- transferred
• Succinate-ubiquinone oxidoreductase • Same as succinate dehydrogenase, a component of the TCA cycle • Succinate dehydrogenase - Directs transfer of electrons from succinate to CoQ via FADH2. - Catalyzes the reduction of Q to QH2 • Acyl-CoA dehydrogenase - From β-oxidation of fatty acids. It also transfers electrons to CoQ via FADH2. • Complex II proteins provide two centers for oxidation reduction reactions - FAD → FADH2 - Fe3+ → Fe2+ (iron-sulfur cluster) • FAD of Complex II is reduced in a 2-electron transfer of a hydride ion from succinate • Complex II does NOT contribute to proton gradient, but supplies electrons from succinate **Note that all electrons from FADH2 and NADH must pass through CoQ.** ETC – Electron transfer in Complex II
ETC – Electron transfer in Complex II
ETC – Electron transfer and proton flow in Complex III • Ubiquinol-cytochrome c oxidoreductase • Transfers electrons to cytochrome c • Complex III contains several cytochromes (heme prosthetic group) and Fe-S center proteins which provide several centers for oxidation reduction reactions • Oxidation of one QH2 is accompanied by the translocation of 4 H+ across the inner mitochondrial membrane - Two H+ are from the matrix, two from QH2 - Regenerates Q for next round
ETC – Electron transfer and proton flow in Complex IV • Cytochrome c oxidase - Combination of cytochromes - A complex of 10 protein subunits that contains 2 cytochromes (a and a3) and proteins with copper centers that provide multiple centers for oxidation-reduction - Consists of, 2 types of prosthetic groups - 2 heme and 2 Cu. - Fe3+ → Fe2+ - Cu2+ → Cu1+ - Source of electrons is cytochrome c (links Complexes III and IV) - Catalyzes a four-electron reduction of molecular oxygen (O2) to water (H2O) - Cytochromes a and a3 are the only species capable of direct transfer of electrons to oxygen. - Translocates H+ into the intermembrane space and contributes to the proton gradient
ETC – Electron transfer and proton flow in Complex IV Net effect is transfer of four H+ for each pair of e- Proton translocation of 2 H+ for each pair of electrons transferred (each O atom reduced) However, for each pair of electrons (e.g. NADH), only get 2H+ transferred to intermembrane space in complex IV
SUMMARY OF ELECTRON TRANSPORT CHAIN
SUMMARY OF ELECTRON TRANSPORT CHAIN
ATP Synthase • F0F1 ATP Synthase uses the proton gradient energy for the synthesis of ATP • Large transmembrane protein complex • Faces into the mitochondrial matrix – spans the IMM • Composed of a “knob-and-stalk” structure • F0 (stalk) has a proton channel which spans the membrane. - Forms a proton pore. - Membrane-spanning portion – integral membrane protein - Made up of 4 different subunits - F0 subunit composition: a1b2c9-12 (c subunits form cylindrical, membrane- bound base)
ATP Synthase • F1 (knob) contains the catalytic subunits (ATP- synthesizing subunits) - Where ATP synthesis takes place - F1 knobs: inner face of the inner mitochondrial membrane - (subunit composition: α3β3γδε) - α3β3 oligomer of F1 is connected to c subunits by a multisubunit stalk of γ and ε chains • Passage of protons through the F0 (stalk) into the matrix is coupled to ATP formation • Estimated passage of 3 H+ / ATP synthesized • F0 is sensitive to oligomycin, an antibiotic that binds in the channel and blocks H+ passage, thereby inhibiting ATP synthesis
ATP Synthase – Mechanism • F1-F0 complex serves as the molecular apparatus for coupling H+ movement to ATP synthase. • There are 3 active sites, one in each β subunit • Passage of protons through the F0 channel causes the rotor to spin in one direction and the stator to spin in the opposite direction
Respiratory Inhibitors & Uncouplers Inhibitors are chemicals that can block electron transfer through specific complexes in the ETC - Complex I: blocked by rotenone, barbiturates - Complex III: blocked by antimycin A - Complex IV: blocked by cyanide, azide, carbon monoxide Uncouplers • In some special cases, the coupling of the two processes can be disrupted. • Uncouplers stimulate the oxidation of substrates in the absence of ADP • Large amounts of O2 are consumed but no ATP is produced. • Uncouplers are lipid-soluble weak acids • Both acidic and basic forms can cross the inner mitochondrial membrane
Respiratory Inhibitors & Uncouplers Uncouplers • Uncouplers deplete any proton gradient by transporting protons across the membrane • Do NOT affect electron transport • Allow protons back into the matrix without making ATP • Stimulate oxygen consumption 2,4-Dinitrophenol: an uncoupler • Used as a diet/weight loss drug • Hydrophobic low molecular weight substance that can diffuse through the mitochondrial inner membrane • Shuttles protons across the membrane and dissipates proton gradient • ATP synthesis goes down – ADP concentration in cells goes up and acts as a stimulator – Signals to turn on pathways to make ATP – Therefore, electron transport and O2 consumption turned on fully and is NOT regulated
Respiratory Inhibitors & Uncouplers 2,4-Dinitrophenol: an uncoupler • Energy produced by electron transport released as HEAT rather than harnessed into ATP synthesis • Fuels (carbs and fats) are consumed at great rates and get quick weight loss BUT – Get heavy breathing – using lots of oxygen – Excessive fever (heat generation) – BIG problem – no control over uncoupling – Brain, heart and muscles are affected as well • 2,4-dinitrophenol is extremely toxic and pulled from the market
Natural Uncouplers • In newborn and hibernating animals, brown fat oxidizes large amounts of substrate (mostly fatty acids) to generate heat • ‘Brown fat’- brown because of the large number of mitochondria and their associated cytochromes • In brown fat mitochondria oxidation of NADH and FADH2 is uncoupled from ATP synthesis – Mitochondria contain thermogenin (uncoupling protein). – Thermogenin allows the release of energy as heat instead of ATP. – Thermogenin dissipates proton electrochemical gradient • By providing another channel for return of protons - bypasses ATP synthase • Also called uncoupling protein (UCP) • In brown fat mitochondria, the energy that would have been used to make ATP is liberated as heat

Empfohlen

Carbohydrate metabolism & Interconnection of Metabolism with Respiratory chain
Carbohydrate metabolism & Interconnection of Metabolism with Respiratory chainCarbohydrate metabolism & Interconnection of Metabolism with Respiratory chain
Carbohydrate metabolism & Interconnection of Metabolism with Respiratory chain
Dr.Subir Kumar
 
Gluconeogenesis
GluconeogenesisGluconeogenesis
Gluconeogenesis
Ramesh Gupta
 
Co enzymes
Co enzymesCo enzymes
Co enzymes
Pulkit Agarwal
 
Metabolic processes
Metabolic processesMetabolic processes
Metabolic processes
Charilyn Cruz
 
Lipids: Structure and Functions
Lipids: Structure and FunctionsLipids: Structure and Functions
Lipids: Structure and Functions
vibhakhanna1
 
Gluconeogenesis
Gluconeogenesis Gluconeogenesis
Gluconeogenesis
Rajan Kumar
 
Regulation of enzyme activity
Regulation of enzyme activity Regulation of enzyme activity
Regulation of enzyme activity
International Medical School Malaysia
 
Carbohydrate metabolism
Carbohydrate metabolismCarbohydrate metabolism
Carbohydrate metabolism
WEEKLYMEDIC
 

Empfohlen

Carbohydrate metabolism & Interconnection of Metabolism with Respiratory chain
Carbohydrate metabolism & Interconnection of Metabolism with Respiratory chainCarbohydrate metabolism & Interconnection of Metabolism with Respiratory chain
Carbohydrate metabolism & Interconnection of Metabolism with Respiratory chain
Dr.Subir Kumar
 
Gluconeogenesis
GluconeogenesisGluconeogenesis
Gluconeogenesis
Ramesh Gupta
 
Co enzymes
Co enzymesCo enzymes
Co enzymes
Pulkit Agarwal
 
Metabolic processes
Metabolic processesMetabolic processes
Metabolic processes
Charilyn Cruz
 
Lipids: Structure and Functions
Lipids: Structure and FunctionsLipids: Structure and Functions
Lipids: Structure and Functions
vibhakhanna1
 
Gluconeogenesis
Gluconeogenesis Gluconeogenesis
Gluconeogenesis
Rajan Kumar
 
Regulation of enzyme activity
Regulation of enzyme activity Regulation of enzyme activity
Regulation of enzyme activity
International Medical School Malaysia
 
Carbohydrate metabolism
Carbohydrate metabolismCarbohydrate metabolism
Carbohydrate metabolism
WEEKLYMEDIC
 
Enzymes
EnzymesEnzymes
Enzymes
Ramesh Gupta
 
Electron transport chain( Oxidative phosphorylation)
Electron transport chain( Oxidative phosphorylation)Electron transport chain( Oxidative phosphorylation)
Electron transport chain( Oxidative phosphorylation)
Anup Shamsher Budhathoki
 
Fatty acid synthesis
Fatty acid synthesisFatty acid synthesis
Fatty acid synthesis
Namrata Chhabra
 
Oxidative phosphorylation and electron transport chain
Oxidative phosphorylation and electron transport chainOxidative phosphorylation and electron transport chain
Oxidative phosphorylation and electron transport chain
Dipesh Tamrakar
 
Biosynthesis of amino_acids
Biosynthesis of amino_acidsBiosynthesis of amino_acids
Biosynthesis of amino_acids
Prachee Rajput
 
Nucleotides metabolism
Nucleotides metabolismNucleotides metabolism
Nucleotides metabolism
Tapeshwar Yadav
 
Pentose phosphate pathway
Pentose phosphate pathway Pentose phosphate pathway
Pentose phosphate pathway
Rajan Kumar
 
HEXOSE MONOPHOSPHATE SHUNT
HEXOSE MONOPHOSPHATE SHUNTHEXOSE MONOPHOSPHATE SHUNT
HEXOSE MONOPHOSPHATE SHUNT
International Medicine School - Management and Science University
 
ELECTRON TRANSPORT AND OXIDATIVE PHOSPHORYLATION
ELECTRON TRANSPORT AND OXIDATIVE PHOSPHORYLATIONELECTRON TRANSPORT AND OXIDATIVE PHOSPHORYLATION
ELECTRON TRANSPORT AND OXIDATIVE PHOSPHORYLATION
Dr.M.Prasad Naidu
 
CHOLESTEROL BIOSYNTHESIS
CHOLESTEROL BIOSYNTHESISCHOLESTEROL BIOSYNTHESIS
CHOLESTEROL BIOSYNTHESIS
YESANNA
 
Calvin cycle
Calvin cycleCalvin cycle
Calvin cycle
Deepak Chawhan
 
Glycolysis
GlycolysisGlycolysis
Glycolysis
Dipesh Tamrakar
 
Role of ATP in Bioenergetics
Role of ATP in BioenergeticsRole of ATP in Bioenergetics
Role of ATP in Bioenergetics
HiraIftikhar9
 
Glycolipids
GlycolipidsGlycolipids
Glycolipids
Dr.M.Prasad Naidu
 
GLYCOLYSIS & ITS REGULATION
GLYCOLYSIS & ITS REGULATIONGLYCOLYSIS & ITS REGULATION
GLYCOLYSIS & ITS REGULATION
YESANNA
 
Enzyme catalysis mechanisms involved
Enzyme catalysis mechanisms involvedEnzyme catalysis mechanisms involved
Enzyme catalysis mechanisms involved
David Enoma
 
Pentose phosphate pathway (Hexose Monophosphate Pathway)
Pentose phosphate pathway (Hexose Monophosphate Pathway)Pentose phosphate pathway (Hexose Monophosphate Pathway)
Pentose phosphate pathway (Hexose Monophosphate Pathway)
Anup Bajracharya
 
Biosynthesis of phospholipids
Biosynthesis of phospholipidsBiosynthesis of phospholipids
Biosynthesis of phospholipids
Nusrat Sheikh
 
Bioenergetics
BioenergeticsBioenergetics
Bioenergetics
Princy Agarwal
 
Beta oxidation of fatty acid
Beta oxidation of fatty acidBeta oxidation of fatty acid
Beta oxidation of fatty acid
Santosh Kumar Sahoo
 
Biochemical energy production BIOCHEM.pptx
Biochemical energy production BIOCHEM.pptxBiochemical energy production BIOCHEM.pptx
Biochemical energy production BIOCHEM.pptx
JemimahJoyGuarin1
 
Bioenergetics
BioenergeticsBioenergetics
Bioenergetics
obanbrahma
 

Weitere ähnliche Inhalte

Was ist angesagt?

ELECTRON TRANSPORT AND OXIDATIVE PHOSPHORYLATION
ELECTRON TRANSPORT AND OXIDATIVE PHOSPHORYLATIONELECTRON TRANSPORT AND OXIDATIVE PHOSPHORYLATION
ELECTRON TRANSPORT AND OXIDATIVE PHOSPHORYLATION
Dr.M.Prasad Naidu
 

Was ist angesagt? (20)

Enzymes
EnzymesEnzymes
Enzymes
 
Electron transport chain( Oxidative phosphorylation)
Electron transport chain( Oxidative phosphorylation)Electron transport chain( Oxidative phosphorylation)
Electron transport chain( Oxidative phosphorylation)
 
Fatty acid synthesis
Fatty acid synthesisFatty acid synthesis
Fatty acid synthesis
 
Oxidative phosphorylation and electron transport chain
Oxidative phosphorylation and electron transport chainOxidative phosphorylation and electron transport chain
Oxidative phosphorylation and electron transport chain
 
Biosynthesis of amino_acids
Biosynthesis of amino_acidsBiosynthesis of amino_acids
Biosynthesis of amino_acids
 
Nucleotides metabolism
Nucleotides metabolismNucleotides metabolism
Nucleotides metabolism
 
Pentose phosphate pathway
Pentose phosphate pathway Pentose phosphate pathway
Pentose phosphate pathway
 
HEXOSE MONOPHOSPHATE SHUNT
HEXOSE MONOPHOSPHATE SHUNTHEXOSE MONOPHOSPHATE SHUNT
HEXOSE MONOPHOSPHATE SHUNT
 
ELECTRON TRANSPORT AND OXIDATIVE PHOSPHORYLATION
ELECTRON TRANSPORT AND OXIDATIVE PHOSPHORYLATIONELECTRON TRANSPORT AND OXIDATIVE PHOSPHORYLATION
ELECTRON TRANSPORT AND OXIDATIVE PHOSPHORYLATION
 
CHOLESTEROL BIOSYNTHESIS
CHOLESTEROL BIOSYNTHESISCHOLESTEROL BIOSYNTHESIS
CHOLESTEROL BIOSYNTHESIS
 
Calvin cycle
Calvin cycleCalvin cycle
Calvin cycle
 
Glycolysis
GlycolysisGlycolysis
Glycolysis
 
Role of ATP in Bioenergetics
Role of ATP in BioenergeticsRole of ATP in Bioenergetics
Role of ATP in Bioenergetics
 
Glycolipids
GlycolipidsGlycolipids
Glycolipids
 
GLYCOLYSIS & ITS REGULATION
GLYCOLYSIS & ITS REGULATIONGLYCOLYSIS & ITS REGULATION
GLYCOLYSIS & ITS REGULATION
 
Enzyme catalysis mechanisms involved
Enzyme catalysis mechanisms involvedEnzyme catalysis mechanisms involved
Enzyme catalysis mechanisms involved
 
Pentose phosphate pathway (Hexose Monophosphate Pathway)
Pentose phosphate pathway (Hexose Monophosphate Pathway)Pentose phosphate pathway (Hexose Monophosphate Pathway)
Pentose phosphate pathway (Hexose Monophosphate Pathway)
 
Biosynthesis of phospholipids
Biosynthesis of phospholipidsBiosynthesis of phospholipids
Biosynthesis of phospholipids
 
Bioenergetics
BioenergeticsBioenergetics
Bioenergetics
 
Beta oxidation of fatty acid
Beta oxidation of fatty acidBeta oxidation of fatty acid
Beta oxidation of fatty acid
 

Ähnlich wie Biochemistry_Bioenergetics

Ähnlich wie Biochemistry_Bioenergetics (20)

Biochemical energy production BIOCHEM.pptx
Biochemical energy production BIOCHEM.pptxBiochemical energy production BIOCHEM.pptx
Biochemical energy production BIOCHEM.pptx
 
Bioenergetics
BioenergeticsBioenergetics
Bioenergetics
 
bacterial metabolism.ppt
bacterial metabolism.pptbacterial metabolism.ppt
bacterial metabolism.ppt
 
Bioenergetics
BioenergeticsBioenergetics
Bioenergetics
 
09cellularrespiration 130311053359-phpapp02
09cellularrespiration 130311053359-phpapp0209cellularrespiration 130311053359-phpapp02
09cellularrespiration 130311053359-phpapp02
 
Metabolism
MetabolismMetabolism
Metabolism
 
Bioenergetics lecture sethu
Bioenergetics lecture sethuBioenergetics lecture sethu
Bioenergetics lecture sethu
 
Metabolism
MetabolismMetabolism
Metabolism
 
Plant metabolism and redox agents plant biochemistry ii
Plant metabolism and redox agents plant biochemistry iiPlant metabolism and redox agents plant biochemistry ii
Plant metabolism and redox agents plant biochemistry ii
 
Microbial respiration
Microbial respirationMicrobial respiration
Microbial respiration
 
Microbial respiration
Microbial respirationMicrobial respiration
Microbial respiration
 
Respiration for UG students
Respiration for UG studentsRespiration for UG students
Respiration for UG students
 
15_Photosynthesis.pdf
15_Photosynthesis.pdf15_Photosynthesis.pdf
15_Photosynthesis.pdf
 
BIOENERGETICS
BIOENERGETICSBIOENERGETICS
BIOENERGETICS
 
Mitochondria & choloroplat- Energy Harness Final old microsoft version.ppt
Mitochondria & choloroplat- Energy Harness Final old microsoft version.pptMitochondria & choloroplat- Energy Harness Final old microsoft version.ppt
Mitochondria & choloroplat- Energy Harness Final old microsoft version.ppt
 
Redox reactions in cellular respiration.pptx
Redox reactions in cellular respiration.pptxRedox reactions in cellular respiration.pptx
Redox reactions in cellular respiration.pptx
 
Metabolism and Redox coenzymes (1).pptx
Metabolism and Redox coenzymes (1).pptx Metabolism and Redox coenzymes (1).pptx
Metabolism and Redox coenzymes (1).pptx
 
B.Sc Micro II Microbial physiology Unit 2 Bacterial Respiration
B.Sc Micro II Microbial physiology Unit 2 Bacterial RespirationB.Sc Micro II Microbial physiology Unit 2 Bacterial Respiration
B.Sc Micro II Microbial physiology Unit 2 Bacterial Respiration
 
Bioenergetics
BioenergeticsBioenergetics
Bioenergetics
 
Respiration
RespirationRespiration
Respiration
 

Mehr von Rengesh Balakrishnan

Mehr von Rengesh Balakrishnan (14)

Biochemistry lecture notes proteins
Biochemistry lecture notes proteinsBiochemistry lecture notes proteins
Biochemistry lecture notes proteins
 
Biochemistry lecture notes nucleic acids
Biochemistry lecture notes nucleic acidsBiochemistry lecture notes nucleic acids
Biochemistry lecture notes nucleic acids
 
Biochemistry lecture notes metabolism_tca cycle; glyoxalate cycle
Biochemistry lecture notes metabolism_tca cycle; glyoxalate cycleBiochemistry lecture notes metabolism_tca cycle; glyoxalate cycle
Biochemistry lecture notes metabolism_tca cycle; glyoxalate cycle
 
Biochemistry lecture notes metabolism_glycolysis & pentose phosphate pathway
Biochemistry lecture notes metabolism_glycolysis & pentose phosphate pathwayBiochemistry lecture notes metabolism_glycolysis & pentose phosphate pathway
Biochemistry lecture notes metabolism_glycolysis & pentose phosphate pathway
 
Biochemistry lecture notes lipids
Biochemistry lecture notes lipidsBiochemistry lecture notes lipids
Biochemistry lecture notes lipids
 
Biochemistry lecture notes enzymes
Biochemistry lecture notes enzymesBiochemistry lecture notes enzymes
Biochemistry lecture notes enzymes
 
Biochemistry lecture notes carbohydrates
Biochemistry lecture notes carbohydratesBiochemistry lecture notes carbohydrates
Biochemistry lecture notes carbohydrates
 
Biochemistry lecture notes aminoacids
Biochemistry lecture notes aminoacidsBiochemistry lecture notes aminoacids
Biochemistry lecture notes aminoacids
 
Biochemistry lecture notes amino acids metabolism
Biochemistry lecture notes amino acids metabolismBiochemistry lecture notes amino acids metabolism
Biochemistry lecture notes amino acids metabolism
 
Fermentation Technology - Oxygen transfer, Antifoam Agents, Agitation, Aeration
Fermentation Technology - Oxygen transfer, Antifoam Agents, Agitation, AerationFermentation Technology - Oxygen transfer, Antifoam Agents, Agitation, Aeration
Fermentation Technology - Oxygen transfer, Antifoam Agents, Agitation, Aeration
 
Batch, Fed-Batch, Continuous Cultivation
Batch, Fed-Batch, Continuous CultivationBatch, Fed-Batch, Continuous Cultivation
Batch, Fed-Batch, Continuous Cultivation
 
Media Sterilisation
Media SterilisationMedia Sterilisation
Media Sterilisation
 
Media Formulation, Media Optimisation,
Media Formulation, Media Optimisation,Media Formulation, Media Optimisation,
Media Formulation, Media Optimisation,
 
Fermentation technology, Bioprocess Principles
Fermentation technology, Bioprocess PrinciplesFermentation technology, Bioprocess Principles
Fermentation technology, Bioprocess Principles
 

Kürzlich hochgeladen

Jual Obat Aborsi Hongkong ( Asli No.1 ) 085657271886 Obat Penggugur Kandungan...
Jual Obat Aborsi Hongkong ( Asli No.1 ) 085657271886 Obat Penggugur Kandungan...Jual Obat Aborsi Hongkong ( Asli No.1 ) 085657271886 Obat Penggugur Kandungan...
Jual Obat Aborsi Hongkong ( Asli No.1 ) 085657271886 Obat Penggugur Kandungan...
ZurliaSoop
 

Kürzlich hochgeladen (20)

How to setup Pycharm environment for Odoo 17.pptx
How to setup Pycharm environment for Odoo 17.pptxHow to setup Pycharm environment for Odoo 17.pptx
How to setup Pycharm environment for Odoo 17.pptx
 
Jual Obat Aborsi Hongkong ( Asli No.1 ) 085657271886 Obat Penggugur Kandungan...
Jual Obat Aborsi Hongkong ( Asli No.1 ) 085657271886 Obat Penggugur Kandungan...Jual Obat Aborsi Hongkong ( Asli No.1 ) 085657271886 Obat Penggugur Kandungan...
Jual Obat Aborsi Hongkong ( Asli No.1 ) 085657271886 Obat Penggugur Kandungan...
 
On National Teacher Day, meet the 2024-25 Kenan Fellows
On National Teacher Day, meet the 2024-25 Kenan FellowsOn National Teacher Day, meet the 2024-25 Kenan Fellows
On National Teacher Day, meet the 2024-25 Kenan Fellows
 
REMIFENTANIL: An Ultra short acting opioid.pptx
REMIFENTANIL: An Ultra short acting opioid.pptxREMIFENTANIL: An Ultra short acting opioid.pptx
REMIFENTANIL: An Ultra short acting opioid.pptx
 
Micro-Scholarship, What it is, How can it help me.pdf
Micro-Scholarship, What it is, How can it help me.pdfMicro-Scholarship, What it is, How can it help me.pdf
Micro-Scholarship, What it is, How can it help me.pdf
 
How to Add New Custom Addons Path in Odoo 17
How to Add New Custom Addons Path in Odoo 17How to Add New Custom Addons Path in Odoo 17
How to Add New Custom Addons Path in Odoo 17
 
Sociology 101 Demonstration of Learning Exhibit
Sociology 101 Demonstration of Learning ExhibitSociology 101 Demonstration of Learning Exhibit
Sociology 101 Demonstration of Learning Exhibit
 
Beyond_Borders_Understanding_Anime_and_Manga_Fandom_A_Comprehensive_Audience_...
Beyond_Borders_Understanding_Anime_and_Manga_Fandom_A_Comprehensive_Audience_...Beyond_Borders_Understanding_Anime_and_Manga_Fandom_A_Comprehensive_Audience_...
Beyond_Borders_Understanding_Anime_and_Manga_Fandom_A_Comprehensive_Audience_...
 
Key note speaker Neum_Admir Softic_ENG.pdf
Key note speaker Neum_Admir Softic_ENG.pdfKey note speaker Neum_Admir Softic_ENG.pdf
Key note speaker Neum_Admir Softic_ENG.pdf
 
Kodo Millet PPT made by Ghanshyam bairwa college of Agriculture kumher bhara...
Kodo Millet PPT made by Ghanshyam bairwa college of Agriculture kumher bhara...Kodo Millet PPT made by Ghanshyam bairwa college of Agriculture kumher bhara...
Kodo Millet PPT made by Ghanshyam bairwa college of Agriculture kumher bhara...
 
Wellbeing inclusion and digital dystopias.pptx
Wellbeing inclusion and digital dystopias.pptxWellbeing inclusion and digital dystopias.pptx
Wellbeing inclusion and digital dystopias.pptx
 
General Principles of Intellectual Property: Concepts of Intellectual Proper...
General Principles of Intellectual Property: Concepts of Intellectual Proper...General Principles of Intellectual Property: Concepts of Intellectual Proper...
General Principles of Intellectual Property: Concepts of Intellectual Proper...
 
Sensory_Experience_and_Emotional_Resonance_in_Gabriel_Okaras_The_Piano_and_Th...
Sensory_Experience_and_Emotional_Resonance_in_Gabriel_Okaras_The_Piano_and_Th...Sensory_Experience_and_Emotional_Resonance_in_Gabriel_Okaras_The_Piano_and_Th...
Sensory_Experience_and_Emotional_Resonance_in_Gabriel_Okaras_The_Piano_and_Th...
 
ICT role in 21st century education and it's challenges.
ICT role in 21st century education and it's challenges.ICT role in 21st century education and it's challenges.
ICT role in 21st century education and it's challenges.
 
HMCS Vancouver Pre-Deployment Brief - May 2024 (Web Version).pptx
HMCS Vancouver Pre-Deployment Brief - May 2024 (Web Version).pptxHMCS Vancouver Pre-Deployment Brief - May 2024 (Web Version).pptx
HMCS Vancouver Pre-Deployment Brief - May 2024 (Web Version).pptx
 
Food safety_Challenges food safety laboratories_.pdf
Food safety_Challenges food safety laboratories_.pdfFood safety_Challenges food safety laboratories_.pdf
Food safety_Challenges food safety laboratories_.pdf
 
Interdisciplinary_Insights_Data_Collection_Methods.pptx
Interdisciplinary_Insights_Data_Collection_Methods.pptxInterdisciplinary_Insights_Data_Collection_Methods.pptx
Interdisciplinary_Insights_Data_Collection_Methods.pptx
 
Accessible Digital Futures project (20/03/2024)
Accessible Digital Futures project (20/03/2024)Accessible Digital Futures project (20/03/2024)
Accessible Digital Futures project (20/03/2024)
 
UGC NET Paper 1 Mathematical Reasoning & Aptitude.pdf
UGC NET Paper 1 Mathematical Reasoning & Aptitude.pdfUGC NET Paper 1 Mathematical Reasoning & Aptitude.pdf
UGC NET Paper 1 Mathematical Reasoning & Aptitude.pdf
 
On_Translating_a_Tamil_Poem_by_A_K_Ramanujan.pptx
On_Translating_a_Tamil_Poem_by_A_K_Ramanujan.pptxOn_Translating_a_Tamil_Poem_by_A_K_Ramanujan.pptx
On_Translating_a_Tamil_Poem_by_A_K_Ramanujan.pptx
 

Biochemistry_Bioenergetics

  • 1. Bioenergetics Dr.B.RENGESH | M.Tech., Ph.D. Associate Professor, Department of Pharmaceutical Technology, Mahendra Engineering College (Autonomous), Namakkal District, Tamil Nadu, India
  • 2. The Sun and Photosynthesis • The sun is the ultimate source of energy for all biological processes. This energy results from the fusion of hydrogen atoms to form helium atoms: • A portion of this energy reaches the Earth’s surface as sunlight, and is captured by the chlorophyll in plants. This energy drives the conversion of carbon dioxide and water to form glucose, and then into starch, triglycerides, and other forms of stored energy: • All animals obtain energy either directly or indirectly from these energy stores in plants
  • 3. Cellular Respiration • During cellular respiration, plants and animals combine energy-rich compounds with oxygen from the air, producing CO2 and releasing energy. • Cellular respiration can be represented as: – A portion of the energy released during respiration is captured in the form of adenosine triphosphate (ATP), which stores energy for use in other processes. – The remainder of the energy from respiration is released as heat. An extremely simplified carbon cycle
  • 4. Energy Flow in the Biosphere
  • 5. Metabolism • Metabolism is the sum of all reactions occurring in an organism: – catabolism — the reactions involved in the breakdown of biomolecules. – anabolism — the reactions involved in the synthesis of biomolecules. • In general, energy is released during catabolism and required during anabolism. Metabolic Pathways • A metabolic pathway is a sequence of reactions used to produce one product or accomplish one process. – Each pathway consists of a series of chemical reactions that convert a starting material into an end product (e.g., the citric acid cycle and the electron transport chain). – Fortunately, there are a great many similarities among the major metabolic pathways in all life forms.
  • 6. Catabolism of food • The catabolism of food is a three stage process. Stage I : The digestion of large, complex molecules into simpler ones. – The most common reaction in digestion is hydrolysis: Stage II : The small molecules from digestion are broken down into even simpler units, usually the two-carbon acetyl portion of acetyl coenzyme A (acetyl CoA): – Some energy is produced at this stage, but much more is produced during the oxidation of the acetyl units in Stage III.
  • 7. Catabolism of food Stage III : This is referred to as the common catabolic pathway because the reactions are the same regardless of the type of food being degraded. – citric acid cycle – electron transport – oxidative phosphorylation • Energy released in Stage III appears in the form of energy-rich molecules of ATP. – The whole purpose of the catabolic pathway is to convert the chemical energy in foods into molecules of ATP, which carries energy to parts of the cell where energy is needed.
  • 8. ATP – The primary energy carrier – Structure • Adenosine triphosphate, ATP, consists of: – the heterocyclic base adenine – the sugar ribose – a triphosphate group • At physiological pH, the protons on the triphosphate group are removed, giving ATP a charge of -4. – In the cell, it is complexed with Mg2+ in a 1:1 ratio, giving it a net charge of -2. adenine + ribose is called adenosine
  • 9. ATP – The primary energy carrier – Hydrolysis • The triphosphate group is the part of the molecule that is important in the transfer of biochemical energy. The key reaction is the transfer of a phosphoryl group, —PO3 2-, from ATP to another molecule. – During the hydrolysis of ATP in water, a phosphoryl group is transferred from ATP to a water molecule: – The products are adenosine diphosphate (ADP) and a phosphate ion, often referred to as an inorganic phosphate, Pi, or just phosphate.
  • 10. ATP – The primary energy carrier – Hydrolysis • The transfer of a phosphoryl group from ATP to water is accompanied by a release of energy. • Free energy, ΔG, is used as a measure of the energy change. – When energy is released, ΔG is negative. – When energy is absorbed, ΔG is positive. – When ΔG is measured under standard conditions, it is represented by ΔG º. – When ΔG º is measured under body conditions, it is represented by ΔG º’. • The liberated free energy is available for use by the cell to carry out processes requiring an input of energy:
  • 11. ATP – The primary energy carrier – Hydrolysis • Compounds that liberate a large amount of free energy on hydrolysis are called high- energy compounds. • The hydrolysis of ATP to ADP is the principal energy-releasing reaction for ATP. Some other hydrolysis reaction occur under some conditions, such as the hydrolysis of ATP to adenosine monophosphate, AMP, and pyrophosphate, PPi:
  • 12. ATP – The primary energy carrier – Hydrolysis – This is usually followed by immediate hydrolysis of the pyrophosphate, which releases even more energy: • The hydrolyses of ATP and related compounds are summarized below:
  • 13. Important Coenzymes in the Common Catabolic Pathway Coenzyme-A • Coenzymes are weakly-bound organic groups that participate in enzyme-catalyzed reactions, often by acting as shuttle systems for the transfer of chemical groups (e.g., hydrogen transport). Many important coenzymes are formed from vitamins. • Coenzyme A is a central compound in metabolism. It is part of acetyl coenzyme A (acetyl CoA), the substance formed from all foods as they pass through Stage II of catabolism.
  • 14. Important Coenzymes – Coenzyme-A – Components • Components of coenzyme A: – vitamin B5, pantothenic acid, in the center. – a phosphate derivative of ADP – β-mercaptoethylamine, which puts a reactive sulfhydryl group (—SH) at the end of the molecule (CoA—SH).
  • 15. Important Coenzymes – Coenzyme-A – Nomenclature • The letter A is included in the name Coenzyme A to signify its participation in the transfer of acetyl groups, but Coenzyme A transfers all acyl groups. This is important in fatty acid oxidation and synthesis. • Acyl groups are linked to coenzyme A through the sulfur atom in a thioester bond:
  • 16. Important Coenzymes – Ubiquinone (Q) • Also called coenzyme Q • A membrane-soluble low molecular weight compound • Long hydrophobic tail keeps Q anchored in the mitochondrial inner membrane • Q is a lipid soluble molecule that diffuses within the lipid bilayer, and shuttles electrons from • Complexes I and II and pass them to III • Not a part of any complex
  • 17. Important Coenzyme – Nicotinamide Adenine Dinucleotide (NAD+) • NAD+, is an electron transporter which is a derivative of ADP and the vitamin nicotinamide (B3). • The reactive site of NAD+ is in the nicotinamide portion. – When oxidizing a substrate, the nicotinamide ring accepts two electrons and one proton, forming the reduced coenzyme NADH:
  • 18. Important Coenzyme – Nicotinamide Adenine Dinucleotide (NAD+) • A typical cellular reaction in which NAD+ serves as an electron acceptor is the oxidation of an alcohol: • In this reaction, one hydrogen atom of the alcohol substrate is directly transferred to NAD+, whereas the other appears in solution as H+. Both electrons lost by the alcohol have been transferred to the nicotinamide ring in NADH. • Biochemical reactions involving coenzymes are often written more concisely: – This notation emphasizes the oxidation reaction and the involvement of the coenzyme.
  • 19. Important Coenzymes – Flavin Adenine Dinucleotide (FAD) • FAD is another major electron carrier. It is a derivative of ADP & the vitamin riboflavin. • The active site is located within the riboflavin ring system. Unlike NAD+, FAD accepts both of the hydrogen atoms lost by the substrate, forming the reduced species FADH2:
  • 20. Important Coenzymes – Flavin Adenine Dinucleotide (FAD) • The substrates for reactions involving FAD are often those in which a —CH2—CH2— portion of the substrate is oxidized to a double bond:
  • 21. Mitochandria • The mitochondrion is the powerhouse of the cell. It is the organelle where many of the reactions of the common catabolic pathway occur. It consists of an outer membrane, which surrounds a inner membrane. – The folds of the inner membrane are called cristae. – The space that surrounds them is the matrix. • The enzymes for ATP synthesis (electron transport and oxidative phosphorylation) are located on the cristae. The enzymes for the citric acid cycle are found within the matrix, near the surface of the inner membrane.
  • 22. An Animal Cell Schematic of typical animal cell: (1) Nucleolus (2) Nuclear membrane (3) Ribosomes (4) Vesicle (5) Rough endoplasmic reticulum (ER) (6) Golgi body (7) Cytoskeleton (8) Smooth ER (9) Mitochondria (10) Vacuole (11) Cytosol (12) Lysosome (13) Centrioles within centrosome
  • 23. ELECTRON TRANSPORT CHAIN & OXIDATIVE PHOSPHORYLATION Mitochondrial Electron Transport How did we get here? • Summary of glycolysis • Summary of the citric acid cycle (including pyruvate dehydrogenase)
  • 25. • Final stages of aerobic oxidation of biomolecules in eukaryotes occur in the mitochondrion • Reduced coenzymes NADH and FADH2 from: (1) Aerobic oxidation of pyruvate by the citric acid cycle (2) Oxidation of fatty acids and amino acids Electron Transport Chain is the process by which NADH and FADH2 are oxidized and a proton gradient is formed. Oxidative phosphorylation is the process of making ATP by using the proton gradient generated by the ETC. Respiration by mitochondria: • Oxidation of substrates is coupled to the phosphorylation of ADP • Respiration (consumption of oxygen) proceeds only when ADP is present • The amount of O2 consumed depends upon the amount of ADP added ELECTRON TRANSPORT CHAIN & OXIDATIVE PHOSPHORYLATION
  • 26. • Respiratory electron-transport chain (ETC) Series of enzyme complexes embedded in the inner mitochondrial membrane, which oxidize NADH and FADH2. Oxidation energy is used to transport protons creating a proton gradient – protons pumped from matrix to intermembrane space across IMM • ATP synthase uses the proton gradient energy to produce ATP; It is the release of the energy in the gradient back through the membrane through the protein ATP Synthase that drives ATP synthesis ELECTRON TRANSPORT CHAIN & OXIDATIVE PHOSPHORYLATION
  • 27. • The electron transport chain is associated with the mitochondrial inner membrane • Complexes I-IV contain multiple cofactors, and are involved in electron transport • Overall transfer of 2 electrons from NADH through ETC to molecular oxygen: ELECTRON TRANSPORT CHAIN (ETC) – Overview
  • 28. • Complexes I – where NADH electrons enter the chain • Complex II – Where FADH2 electrons enter the chain • Electrons passed from Complex I or II to Coenzyme Q • Coenzyme Q shuttles electrons to complex III • Complex III shuttles electrons to cytochrome C • Cytochrome C shuttles electrons to Complex IV • Complex IV transfers electrons to O2 which is then reduced to water • Flow through Complexes I, III and IV release energy which is used to pump protons across the IMM and form a “proton gradient” • Proton gradient has lots of potential energy • When the energy is released (protons flow back into matrix through ATP synthase), the energy drives ATP synthesis ELECTRON TRANSPORT CHAIN (ETC) – Overview
  • 29. • Also called NADH-ubiquinone oxidoreductase • Complex I includes a flavoprotein (contains FMN – related to FAD) and proteins with Fe- S centers (iron-sulfur clusters) • These proteins provide two centers for oxidation reduction reactions ETC – Electron transfer and proton flow in Complex I • Transfers electrons from NADH to Coenzyme Q via FMN and iron-sulfur proteins • NADH transfers a two electrons as a hydride ion (H:-) to FMN • Reduction of Q to QH2 requires 2 e- • About 4 H+ translocated per 2 e- transferred
  • 30. • Succinate-ubiquinone oxidoreductase • Same as succinate dehydrogenase, a component of the TCA cycle • Succinate dehydrogenase - Directs transfer of electrons from succinate to CoQ via FADH2. - Catalyzes the reduction of Q to QH2 • Acyl-CoA dehydrogenase - From β-oxidation of fatty acids. It also transfers electrons to CoQ via FADH2. • Complex II proteins provide two centers for oxidation reduction reactions - FAD → FADH2 - Fe3+ → Fe2+ (iron-sulfur cluster) • FAD of Complex II is reduced in a 2-electron transfer of a hydride ion from succinate • Complex II does NOT contribute to proton gradient, but supplies electrons from succinate **Note that all electrons from FADH2 and NADH must pass through CoQ.** ETC – Electron transfer in Complex II
  • 31. ETC – Electron transfer in Complex II
  • 32. ETC – Electron transfer and proton flow in Complex III • Ubiquinol-cytochrome c oxidoreductase • Transfers electrons to cytochrome c • Complex III contains several cytochromes (heme prosthetic group) and Fe-S center proteins which provide several centers for oxidation reduction reactions • Oxidation of one QH2 is accompanied by the translocation of 4 H+ across the inner mitochondrial membrane - Two H+ are from the matrix, two from QH2 - Regenerates Q for next round
  • 33. ETC – Electron transfer and proton flow in Complex IV • Cytochrome c oxidase - Combination of cytochromes - A complex of 10 protein subunits that contains 2 cytochromes (a and a3) and proteins with copper centers that provide multiple centers for oxidation-reduction - Consists of, 2 types of prosthetic groups - 2 heme and 2 Cu. - Fe3+ → Fe2+ - Cu2+ → Cu1+ - Source of electrons is cytochrome c (links Complexes III and IV) - Catalyzes a four-electron reduction of molecular oxygen (O2) to water (H2O) - Cytochromes a and a3 are the only species capable of direct transfer of electrons to oxygen. - Translocates H+ into the intermembrane space and contributes to the proton gradient
  • 34. ETC – Electron transfer and proton flow in Complex IV Net effect is transfer of four H+ for each pair of e- Proton translocation of 2 H+ for each pair of electrons transferred (each O atom reduced) However, for each pair of electrons (e.g. NADH), only get 2H+ transferred to intermembrane space in complex IV
  • 36. SUMMARY OF ELECTRON TRANSPORT CHAIN
  • 37. ATP Synthase • F0F1 ATP Synthase uses the proton gradient energy for the synthesis of ATP • Large transmembrane protein complex • Faces into the mitochondrial matrix – spans the IMM • Composed of a “knob-and-stalk” structure • F0 (stalk) has a proton channel which spans the membrane. - Forms a proton pore. - Membrane-spanning portion – integral membrane protein - Made up of 4 different subunits - F0 subunit composition: a1b2c9-12 (c subunits form cylindrical, membrane- bound base)
  • 38. ATP Synthase • F1 (knob) contains the catalytic subunits (ATP- synthesizing subunits) - Where ATP synthesis takes place - F1 knobs: inner face of the inner mitochondrial membrane - (subunit composition: α3β3γδε) - α3β3 oligomer of F1 is connected to c subunits by a multisubunit stalk of γ and ε chains • Passage of protons through the F0 (stalk) into the matrix is coupled to ATP formation • Estimated passage of 3 H+ / ATP synthesized • F0 is sensitive to oligomycin, an antibiotic that binds in the channel and blocks H+ passage, thereby inhibiting ATP synthesis
  • 39. ATP Synthase – Mechanism • F1-F0 complex serves as the molecular apparatus for coupling H+ movement to ATP synthase. • There are 3 active sites, one in each β subunit • Passage of protons through the F0 channel causes the rotor to spin in one direction and the stator to spin in the opposite direction
  • 40. Respiratory Inhibitors & Uncouplers Inhibitors are chemicals that can block electron transfer through specific complexes in the ETC - Complex I: blocked by rotenone, barbiturates - Complex III: blocked by antimycin A - Complex IV: blocked by cyanide, azide, carbon monoxide Uncouplers • In some special cases, the coupling of the two processes can be disrupted. • Uncouplers stimulate the oxidation of substrates in the absence of ADP • Large amounts of O2 are consumed but no ATP is produced. • Uncouplers are lipid-soluble weak acids • Both acidic and basic forms can cross the inner mitochondrial membrane
  • 41. Respiratory Inhibitors & Uncouplers Uncouplers • Uncouplers deplete any proton gradient by transporting protons across the membrane • Do NOT affect electron transport • Allow protons back into the matrix without making ATP • Stimulate oxygen consumption 2,4-Dinitrophenol: an uncoupler • Used as a diet/weight loss drug • Hydrophobic low molecular weight substance that can diffuse through the mitochondrial inner membrane • Shuttles protons across the membrane and dissipates proton gradient • ATP synthesis goes down – ADP concentration in cells goes up and acts as a stimulator – Signals to turn on pathways to make ATP – Therefore, electron transport and O2 consumption turned on fully and is NOT regulated
  • 42. Respiratory Inhibitors & Uncouplers 2,4-Dinitrophenol: an uncoupler • Energy produced by electron transport released as HEAT rather than harnessed into ATP synthesis • Fuels (carbs and fats) are consumed at great rates and get quick weight loss BUT – Get heavy breathing – using lots of oxygen – Excessive fever (heat generation) – BIG problem – no control over uncoupling – Brain, heart and muscles are affected as well • 2,4-dinitrophenol is extremely toxic and pulled from the market
  • 43. Natural Uncouplers • In newborn and hibernating animals, brown fat oxidizes large amounts of substrate (mostly fatty acids) to generate heat • ‘Brown fat’- brown because of the large number of mitochondria and their associated cytochromes • In brown fat mitochondria oxidation of NADH and FADH2 is uncoupled from ATP synthesis – Mitochondria contain thermogenin (uncoupling protein). – Thermogenin allows the release of energy as heat instead of ATP. – Thermogenin dissipates proton electrochemical gradient • By providing another channel for return of protons - bypasses ATP synthase • Also called uncoupling protein (UCP) • In brown fat mitochondria, the energy that would have been used to make ATP is liberated as heat