2. - Also known as Respiration.
- Comprises of these different processes
depending on type of organism:
I. Anaerobic Respiration
II. Aerobic Respiration
3. Comprises of these stages:
glycolysis:
glucose 2 pyruvate + NADH
fermentation:
pyruvate lactic acid
or
ethanol
cellular respiration:
4. Comprises of these stages:
Oxidative decarboxylation of pyruvate
Citric Acid cycle
Oxidative phosphorylation/ Electron Transport
Chain(ETC)
5. Brief overview of STARCHY
catabolism of FOOD
glucose to generate
α – AMYLASE ; MALTASES
energy
Glucose Glucose converted to glu-6-PO4
Start of cycle
Glycolysis in
Cycle : anaerobic cytosol
Aerobic condition;
2[Pyruvate+ATP+NADH] in mitochondria
Anaerobic condition Pyruvate enters as AcetylcoA
- Krebs Cycle
Lactic Acid fermentation in
muscle. - E transport chain
Only in yeast/bacteria
Anaerobic respiration or
Alcohol fermentation
7. 1st stage of glucose metabolism → glycolysis
An anaerobic process, yields 2 ATP (additional energy
source)
Glucose will be metabolized via gycolysis; pyruvate as
the end product
The pyruvate will be converted to lactic acid (muscles
→ liver)
Aerobic conditions: the main purpose is to feed
pyruvate into TCA cycle for further rise of ATP
8. The breakdown of glucose to pyruvate as summarized:
Glucose (six C atoms) → 2 pyruvate (three C atoms)
2 ATP + 4 ADP + 2 Pi → 2 ADP + 4 ATP (phosphorylation)
Glucose + 2 ADP + 2 Pi → 2 Pyruvate + 2 ATP (Net reaction)
Fig. 17-1, p.464
37. Gluconeogenesis
Conversion of pyruvate to glucose
Biosynthesis and the degradation of many important biomolecules follow
different pathways
There are three irreversible steps in glycolysis and the differences bet.
glycolysis and gluconeogenesis are found in these reactions
Different pathway, reactions and enzyme
ST
E P1
p.495
38. is the biosynthesis of new glucose from non-CHO precursors.
this glucose is as a fuel source by the brain, testes, erythrocytes and
kidney medulla
comprises of 9 steps and occurs in liver and kidney
the process occurs when quantity of glycogen have been depleted -
Used to maintain blood glucose levels.
Designed to make sure blood glucose levels are high enough to meet
the demands of brain and muscle (cannot do gluconeogenesis).
promotes by low blood glucose level and high ATP
inhibits by low ATP
occurs when [glu] is low or during periods of fasting/starvation, or
intense exercise
pathway is highly endergonic
*endergonic is energy consuming
40. The oxalocetate formed in the mitochondria
have two fates:
- continue to form PEP
- turned into malate by malate dehydrogenase
and leave the mitochondria, have a reaction
reverse by cytosolic malate dehydrogenase
Reason?
41.
42. Controlling glucose
metabolism
• found in Cori cycle
• shows the cycling of
glucose due to
gycolysis in muscle and
gluconeogenesis in
liver
• This two metabolic
pathways are not active
simultaneously. As energy store for
• when the cell needs next exercise
ATP, glycolisys is more
active
•When there is little
need for ATP,
gluconeogenesis is
more active
Fig. 18-12, p.502
43. Cori cycle requires the net
hydrolysis of two ATP and two
GTP.
glu cos e + 2 NAD + + 2 ADP + 2 Pi →
+
2 Pyruvate + 2 NADH + 4 H + 2 ATP + 2 H 2O
+
2 Pyruvate + 2 NADH + 4 H + 4 ATP + 2GTP + 6 H 2O →
Glu cos e + 2 NAD + + 4 ADP + 2GDP + 6 Pi
2 ATP + 2GTP + 4 H 2O →
2 ADP + 2GDP + 4 Pi
45. The Citric Acid cycle
Cycle where 30 to 32 molecules of ATP can be produced from
glucose in complete aerobic oxidation
Amphibolic – play roles in both catabolism and anabolism
The other name of citric acid cycle: Krebs cycle and
tricarboxylic acid cycle (TCA)
Takes place in mitochondria
66. Overall production from glycolysis, oxidative
decarboxylation and TCA:
Oxidative Glycolysis TCA cycle
decarboxylation
- 2 ATP 2 ATP
2 NADH 2 NADH 6 NADH , 2 FADH2
2 CO2 2 Pyruvate 4 CO2
Electron transportation system
Notes de l'éditeur
FIGURE 17.1 One molecule of glucose is converted to two molecules of pyruvate. Under aerobic conditions, pyruvate is oxidized to CO2 and H2O by the citric acid cycle (Chapter 19) and oxidative phosphorylation (Chapter 20). Under anaerobic conditions, lactate is produced, especially in muscle. Alcoholic fermentation occurs in yeast. The NADH produced in the conversion of glucose to pyruvate is reoxidized to NAD+ in the subsequent reactions of pyruvate.
FIGURE 17.2 The glycolytic pathway.
Louis Pasteur (1822–1895). His research on fermentation led to important discoveries in microbiology and chemistry.
FIGURE 17.3 In the first phase of glycolysis, five reactions convert a molecule of glucose to two molecules of glyceraldehyde-3-phosphate.
FIGURE 17.3 In the first phase of glycolysis, five reactions convert a molecule of glucose to two molecules of glyceraldehyde-3-phosphate.
FIGURE 17.4 A comparison of the conformations of hexokinase and the hexokinase–glucose complex.
FIGURE 17.6 At high [ATP], phosphofructokinase behaves cooperatively, and the plot of enzyme activity versus [fructose-6-phosphate] is sigmoidal. High [ATP] thus inhibits PFK, decreasing the enzyme’s affinity for fructose-6-phosphate.
FIGURE 17.7 The second phase of glycolysis.
FIGURE 17.7 The second phase of glycolysis.
FIGURE 17.8 Schematic view of the binding site of an NADH-linked dehydrogenase. There are specific binding sites for the adenine nucleotide portion of the coenzyme (shown in red to the right of the dashed line) and for the nicotinamide portion of the coenzyme (shown in yellow to the left of the dashed line), in addition to the binding site for the substrate. Specific interactions with the enzyme hold the substrate and coenzyme in the proper positions. Sites of interaction are shown as a series of pale green lines.
FIGURE 17.10 Control points in glycolysis.
FIGURE 17.11 The recycling of NAD and NADH in anaerobic glycolysis.
FIGURE 17.11 The recycling of NAD and NADH in anaerobic glycolysis.
FIGURE 17.12 The structures of thiamine (vitamin B1) and thiamine pyrophosphate (TPP), the active form of the coenzyme.
FIGURE 18.6 The pathways of gluconeogenesis and glycolysis. Species in blue, green, and pink shaded boxes indicate other entry points for gluconeogenesis (in addition to pyruvate).
FIGURE 18.9 Pyruvate carboxylase catalyzes a compartmentalized reaction. Pyruvate is converted to oxaloacetate in the mitochondria. Because oxaloacetate cannot be transported across the mitochondrial membrane, it must be reduced to malate, transported to the cytosol, and then oxidized back to oxaloacetate before gluconeogenesis can continue.
FIGURE 18.12 The Cori cycle. Lactate produced in muscles by glycolysis is transported by the blood to the liver. Gluconeogenesis in the liver converts the lactate back to glucose, which can be carried back to the muscles by the blood. Glucose can be stored as glycogen until it is degraded by glycogenolysis. (NTP stands for nucleoside triphosphate.)
Gerty and Carl Cori, codiscoverers of the Cori cycle.
FIGURE 18.13 Control of liver pyruvate kinase by phosphorylation. When blood glucose is low, phosphorylation of pyruvate kinase is favored. The phosphorylated form is less active, thereby slowing glycolysis and allowing pyruvate to produce glucose by gluconeogenesis.
FIGURE 19.1 The central relationship of the citric acid cycle to catabolism. Amino acids, fatty acids, and glucose can all produce acetyl-CoA in stage 1 of catabolism. In stage 2, acetyl-CoA enters the citric acid cycle. Stages 1 and 2 produce reduced electron carriers (shown here as e-). In stage 3, the electrons enter the electron transport chain, which then produces ATP.
FIGURE 19.2 The structure of a mitochondrion. (a) Colored scanning electron microscope image showing the internal structure of a mitochondrion (green, magnified 19,200 x). (b) Interpretive drawing of the scanned image. (c) Perspective drawing of a mitochondrion. (For an electron micrograph of mitochondrial structure, see Figure 1.13.)
FIGURE 19.3 An overview of the citric acid cycle. Note the names of the enzymes. The loss of CO2 is indicated, as is the phosphorylation of GDP to GTP. The production of NADH and FADH2 is also indicated.
FIGURE 19.3 An overview of the citric acid cycle. Note the names of the enzymes. The loss of CO2 is indicated, as is the phosphorylation of GDP to GTP. The production of NADH and FADH2 is also indicated.
FIGURE 19.6 Three-point attachment to the enzyme aconitase makes the two -CH2-COO - ends of citrate stereochemically nonequivalent.
FIGURE 19.7 The isocitrate dehydrogenase reaction.
FIGURE 19.8 Control points in the conversion of pyruvate to acetyl-CoA and in the citric acid cycle.
FIGURE 19.10 A summary of catabolism, showing the central role of the citric acid cycle. Note that the end products of the catabolism of carbohydrates, lipids, and amino acids all appear. (PEP is phosphoenolpyruvate; -KG is ketoglutarate; TA is transamination; is a multistep pathway.)
FIGURE 19.11 How mammals keep an adequate supply of metabolic intermediates. An anabolic reaction uses a citric acid cycle intermediate ( - ketoglutarate is transaminated to glutamate in our example), competing with the rest of the cycle. The concentration of acetyl-CoA rises and signals the allosteric activation of pyruvate carboxylase to produce more oxaloacetate. * Anaplerotic reaction. **Part of glyoxylate pathway.
FIGURE 19.12 Transfer of the starting materials of gluconeogenesis from the mitochondrion to the cytosol. Note that phosphoenolpyruvate (PEP) can be transferred from the mitochondrion to the cytosol, as can malate. Oxaloacetate is not transported across the mitochondrial membrane. (1 is PEP carboxykinase in mitochondria; 2 is PEP carboxykinase in cytosol; other symbols are as in Figure 19.10.)
FIGURE 19.15 A summary of anabolism, showing the central role of the citric acid cycle. Note that there are pathways for the biosynthesis of carbohydrates, lipids, and amino acids. OAA is oxaloacetate, and ALA is -aminolevulinic acid. Symbols are as in Figure 19.10.)