Test 3 Unit 3-Energy and Cellular Respiration

Question 1

What is the law of Thermodynamics and define all variables.

Answer 1

ΔG = ΔH - TΔS
ΔG: Free energy, spontaneous reactions
ΔH: Enthalpy, potential energy
ΔS: Entropy, disorder
T: Temperature

Question 2

Explain how enthalpy (ΔH) works.

Answer 2

Transformations that absord energy (endothermic) result in the products having MORE potential energy. (+ΔH)
Transformations that release energy (exothermic) result in the products having LESS potential energy. (-ΔH)

*If you gain potential energy (+ΔH), reaction is NOT spontaneous.

Question 3

Explain how enthropy (ΔS) works.

Answer 3

The measure of wheter a reaction gains disorder.
Gas > Liquid > Solid.
*Reactions that gain disorder (+ΔS) tend to be spontaneous.

Question 4

Explain free energy (ΔG).

Answer 4

-ΔG = spontaneous (exergonic)
\+ΔG = NOT spontaneous (endergonic)

Question 5

Explain how exergonic and endergonic reactions relate to catabolic and anabolic reactions.

Answer 5

• Catabolic = energy released = exergonic = spontaneous

- Anabolic = energy required = endergonicc = not spontaneous

Question 6

Why does ATP hydrolysis release free energy?

Answer 6

ATP hydrolysis releases free energy, so it is exergonic (spontaneous) because:

1. decrease in potential energy
2. increase in entropy

Question 7

Why is there less potential energy in ADP than in ATP?

Answer 7

Because the loss of the terminal phosphate has decreased the electrical repulsion among the negatively charged oxygen atoms of the phosphate groups.

Question 8

Explain how ATP hydrolysis can make other reactions spontaneous in the cell
.

Answer 8

Through energy coupling: an endergonic reaction occurs by being coupled to an exergonic reaction. the energy is provided by the exergonic breakdown of ATP.

Question 9

Explain the concept of activation energy for enzymes

Answer 9

For chemical reactions to occur, bonds need to be broken and this requires a small input of energy called ACTIVATION ENERGY. Enzymes can accelerate reactions by lowering the activation energy.

Question 10

Explain how enzymes reduce the amount of activation energy required to start a reaction

Answer 10

Enzymes reduce the activation energy by inducing the transition state. The binding of substrate(s) to an active site results in the substrate’s acquiring the transition state conformation. Enzymes can:

1. Bring reacting molecules together (reacting molecules can assume the transition state only when they collide)
2. Charge interactions: expose the reactant to altered charges that promote catalysis
3. Change the shape of a substrate into a conformation that mimics the transition state.

Question 11

What is a cofactor?

Answer 11

A nonprotein group that binds very precisely to the enzyme. Cofactors are often metals, such as iron, copper, zinc, or manganese. The cofactor binds to the enzyme and activates it.

Question 12

Give an example of an enzymatic cofactor.

Answer 12

ATP, vitamins (nonprotein groups), Retinal, Ascorbic acid, or vitamin C, is used as a cofactor in hydroxylases.

Question 13

How can 
1.substrate concentration
2.enzyme concentration 
3.pH 
4.temperature 
affect the rate of reaction?

Answer 13

1. In the presence of excess substrate, the rate of catalysis is proportional to the amount of enzyme. At some point, it reaches a saturation level if the enzyme concentration is constant (↑ substrate = not so efficient!)
2. As enzyme concentration increases, the rate of product formation increases. (↑ enzyme = very efficient!)
3. An enzyme has an optimal pH at which it is most active
4. An enzyme has an optimal temperature at which it is most active. Heat-sensitive enzymes can be activated/inhibited with temperature changes.

Question 14

Explain how enzymes can be regulated through competitive and non competitive interactions

Answer 14

• Competitive regulation: the competitive inhibiter molecule competes with the substrate for the active site and the substrate is unable to bind when the inhibitor is bound to active site.
• Non-competitive (allosteric) regulation: Can be activation or inhibition

Question 15

Explain how allosteric activation/inhibition works.

Answer 15

1. Activation:
   Enzyme binds to allosteric activator and converts it to a HIGH-affinity state = the substrate can bind.
2. Inhibition:
   Enzyme binds to allosteric inhibitor and converts it to a LOW-affinity state = the substrate is released.

Question 16

What is the difference in efficiency of aerobic and anaerobic pathways?

Answer 16

• Aerobic respiration: 1 glucose = 36-38 ATPS (MOST EFFICIENT!)
• Anaerobic respiration: 1 glucose = 2-36 ATPS
• Fermentation: 1 glucose = 2 ATPS

Question 17

Why is anaerobic respiration and fermentation less efficient than aerobic?

Answer 17

Because it uses non-O2 compounds as electron acceptors which are less efficient because they are less electronegative than O2, so they have less affinity for electrons.
Fermentation is a back-up that uses organic compounds as electron acceptors.

Question 18

Where and why in cellular respiration does fermentation occur?

Answer 18

Why? If oxygen is absent or in short supply

Where? In the cytosol. Pyruvate remains in the cytosol and is reduced using the NADH generated by glycolysis.

Question 19

What are the 2 types of fermentation?

Answer 19

1. Alcohol (in microorganisms such as yeasts, which are single-celled fungi)
2. Lactate (in many bacteria and some plant and animal tissues)

Question 20

Explain oxidation and reduction.

Answer 20

-Oxidation is the loss of electrons by a molecule, atom, or ion. (oxidized)
-Reduction is the gain of electrons by a molecule, atom, or ion (reduced)
The reducing agent (oxidized) gives its electron to the oxidizing agent (reduced).

Question 21

Give examples of oxidation and reduction.

Answer 21

Glucose is oxidized to CO2 (CO2 is oxidized form).
O2 is reduced into H2O. (H2O is reduced form)
NAD+ is oxidized form
NADH is reduced form
FAD is oxidized form
FADH2 is reduced form

Question 22

Explain how redox processes lead to ATP production

Answer 22

• Glycolysis: oxidation of glucose, converted into 2 pyruvate
• Pyruvate oxidation: Oxidation of pyruvate forms Acetyl-CoA, which is oxidized to CO2. ATP and NADH is synthesized.
• Oxidative phosphorylation: NADH oxidized and electrons are passed along ETC to create a proton gradient that is used to synthesize ATP

C6H12O6 + 6O2 → 6CO2 + 6H2O +ATP (glucose is oxidized, O2 is reduced)

Question 23

Illustrate how NAD+ and NADH serve as a transport for electrons in cellular respiration

Answer 23

1) In the energy releasing phase of Glycolysis, NAD+ accepts some electrons and 1 proton is reduced to NADH.
2) In Pyruvate Oxidation, the conversion of pyruvate to acetly-CoA leads to the transfer of 2 electrons and 1 proton to NAD+ which forms NADH.
3) In CAC, NAD+ is reduced 3 times to NADH
4) In Oxidative Phosphorylation, the potential energy resides in NADH that will be oxidized to NAD+ and the electrons released will start the ETC (proton-motive-force)

Question 24

What are the major pathways of cellular respiration?

Answer 24

Glycolysis, Pyruvate oxidation, Citric acid cycle, Oxidative phosphorylation (ETC + chemiosmosis).

Question 25

Which molecules do the transition/link between the 3-4 major pathways of cellular respiration?

Answer 25

Glycolysis –> PYRUVATE–> Pyruvate oxidation–> ACETYL-COA–>Citric acid cycle–>NADH and FADH2–> Oxidative phosphorylation (ETC + chemiosmosis).

Question 26

Explain the difference between the energy requiring phase and the energy releasing phase of glycolysis

Answer 26

Energy requiring phase uses 2 ATPs to transform glucose into 2 molecules of G3P
Energy releasing phase releases 4 ATPs and 2 NADH and transforms 2 G3P into 2 Pyruvate molecules.
Each reaction in glycolysis is catalyzed by its own enzyme (one of them being phosphofructokinase).

Question 27

What is substrate level phosphorylation?

Answer 27

ATP is generated by substrate-level phosphorylation, which is mediated by a specific enzyme called pyruvate kinase, is a mode of ATP synthesis. A phosphate group is transferred from a high-energy donor (PEP) directly to ADP, forming ATP.

Question 28

What is chemiosmosis?

Answer 28

The ability of cells to use the proton-motive force to do work. The protons move through the ATP synthase and make it spin and results in ATP synthesis.

Question 29

What is the difference between substrate level phosphorylation and chemiosmosis?

Answer 29

Chemiosmosis uses the enzyme ATP synthase and a proton-motive force whereas SLP uses the enzyme pyruvate-kinase and a high-energy donor.

Question 30

Why is O2 the best electron acceptor?

Answer 30

By being highly electronegative, O2 has greater affinity for electrons than any other electron acceptor.

Question 31

Where are the carbon atoms of a glucose molecule released in cellular respiration?

Answer 31

-2 CO2 in pyruvate oxidation
-4 CO2 in citric acid cycle
total of 6 carbons (CO2)

Question 32

How and where can different monosaccharides, amino acids and fatty acids enter cellular respiration to be converted to energy?

Answer 32

• Glycerol can be converted to G3P and be phosphorylated and enter glycolysis
• Carbohydrates are broken down and can enter glycolysis (like fructose)
• Fatty acids can undergo fatty acid oxidation (split onto 2-carbon segments) and transform into Acetyl-CoA and therefore enter the CAC
• Proteins are hydrolyzed to amino acids and NH2 is removed and the remainder of the molecule enters as pyruvate or acetyl-coA.

Question 33

Give an example of an amino acid that can enter cellular respiration to be converted to energy?

Answer 33

Alanine is converted into pyruvate, which can undergo pyruvate oxidation, CAC and oxidative phosphorylation.

Question 34

How many ATP/NADH are released in Glycolysis?

Answer 34

2 ATPs by substrate-level phosphorylation.

2 NADH.

Question 35

How many ATP/NADH are released in Pyruvate oxidation?

Answer 35

2 NADH.

Question 36

How many ATP/NADH/FADH2 are released in Citric acid cycle?

Answer 36

2 ATPs by substrate-level phosphorylation.
6 NADH.
2 FADH2.

Question 37

How many ATP/NADH/FADH2 are released in Oxidative phosphorylation?

Answer 37

None. the NADH and FADH released is used to create a proton gradient that will induce ATP synthesis where 10p+/NADH and 6p+/FADH2.

Question 38

How is the free energy released in the ETC used to synthesize ATP?

Answer 38

In the electron transport chain, electrons are passed from one molecule to another through 4 complexes, and energy released in these electron transfers is used to form an electrochemical gradient (proton gradient in the intermembrane space). In chemiosmosis, the energy stored in the gradient is used by ATP synthase to make ATP.

Question 39

How is cellular respiration regulated?

Answer 39

The rate of ATP generation matches the requirements of the cell for chemical energy.
It is mainly regulated by the allosteric enzyme phosphofructokinase, which catalyses the conversion of fructose 6-phosphate to fructose 1,6-bisphosphate.

Question 40

What are phosphofructokinase’s inhibitor/activator?

Answer 40

Activator: ADP
Inhibitor: ATP

Question 41

How does phosphofructokinase regulate cellular respiration in ATP excess?

Answer 41

When there is excess ATP, it binds to phosphofructokinase and inhibits its activity. This slows or stops the reactions after glycolysis.

Question 42

How does phosphofructokinase regulate cellular respiration when there is no enough ATP?

Answer 42

When there is no enough ATP, ADP accumulates and binds to phosphofructokinase. It activates the enzyme to produce ATP.

Question 43

Briefly explain how the ETC works and how NADH and FADH2 are related to it.

Answer 43

It extracts the potential energy in NADH and FADH2. Electrons move spontaneously down a potential energy gradient from 1 complex to the next (4 complexes total). The release of energy is used to pump protons into the intermembrane space. There is also smaller electron carriers, ubiquinone and cytosol c, that act as shuttles between major complexes. The transport is done by prosthetic groups (cofactors).

Question 44

Describe the # protons pumped by each complex for NADH and FADH2.

Answer 44

NADH:
1 pumps 4 p+
2 pumps 0 p+
3 pumps 4 p+
4 pumps 2 p+
FAHD2:
1 pumps 0 p+
2 pumps 0 p+
3 pumps 4 p+
4 pumps 2 p+

Question 45

Describe the electron flow during ETC.

Answer 45

Electron flow is spontaneous from high to low potential energy (down free energy gradient)