Chapter 17

Question 1

Gluconeogenesis & pathway overview

Answer 1

• Pyruvate to glucose
• Gluconeogenesis = synthesis of glucose from non-carbohydrate precursors
• Gluconeogenesis = NOT a complete reversal of glycolysis

–> some enzymes for reversible steps of glycolysis will remain same during gluconeogenesis (reversible steps will utilize same enzymes as in glycolysis)

• Major site = liver, can occur in kidney
• Important during fasting/starvation
• Gluconeogenic pathway converts pyruvate into glucose from non-carbohydrate precursors: lactate, amino acids, and glycerol

 Pyruvate can be formed from muscle-derived lactate in liver by lactate dehydrogenase

 Carbon skeletons of some amino acids can be converted into gluconeogenic intermediates

 Glycerol (derived from hydrolysis of triacylglycerides) can be converted into dihydroxyacetone phosphate (DHAP), which can be processed by gluconeogenesis or glycolysis

Question 2

Glucose = primary fuel for _____ and only fuel for _____

Answer 2

brain; RBC

Question 3

List the 4-distinct enzymes in gluconeogenesis are needed to counter the irreversible steps of glycolysis

Answer 3

1. Pyruvate carboxylase
2. Phosphoenolpyruvate (PEP) carboxykinase (PEPCK)
3. Fructose 1,6-biphosphatase
4. Glucose-6-phosphatase

Question 4

Enzymes for gluconeogenesis located in cytoplasm EXCEPT …

Answer 4

• pyruvate carboxylase (in mitochondria)
• glucose-6-phosphatase (membrane bound in ER)

Question 5

Irreversible enzymes/steps of glycolysis and the enzymes/steps that bypass them in gluconceogensis

Answer 5

Irreversible steps and enzymes in glycolysis are hexokinase (glucose - G6P), PFK (F6P - F,16-BP), and pyruvate kinase (Phosphoenolpyruvate - pyruvate)

In gluconeogenesis, these 3 reactions are bypassed by the following steps & enzymes:

ENZYME Glucose 6-phosphatase converts glucose 6-phospahte plus H2O into glucose + Pi

ENZYME Fructose 1,6-biphosphatase converts fructose 1,6-biphosphate plus H2O into fructose 6-phosphte + Pi

ENZYME Phosphoenolpyruvate carboxykinase (PEPCK) converts oxaloacetate + GTP into phosphoenolpyruvate + GDP + CO2

ENZYME Pyruvate carboxylase converts pyruvate + CO2 + ATP + H2O into oxaloacetate + ADP + Pi

Question 6

1. Pyruvate to oxaloacetate via enzyme Pyruvate Carboxylase

Answer 6

• Conversion of pyruvate to oxaloacetate at expense of 1 ATP
• Pyruvate = 3 carbon molecule. Oxaloacetate = 4 carbon molecule. Three steps:

1. Bicarbonate (HCO3) is phosphorylated, 1 ATP is used
2. CO2 from biotin is transferred to biotin arm of enzyme, called carboxybiotin

–> requires vitamin B7 (biotin) as a cofactor

3. CO2 is added to pyruvate, allows for generation of oxaloacetate

** This step occurs in mitochondria, but ALL OTHER ENZYMES for gluconeogenesis exist in cytoplasm

** In aqueous solution, CO2 exists as bicarbonate

Question 7

Biotin as enzyme swing arm

Answer 7

Biotin = covalently attached prosthetic group that serves as the carrier of activated

• Pyruvate carboxylase requires vitamin B7 (biotin) as cofactor
• Biotin serves as carrier of activated CO2
• Carboxylate group of biotin is linked to lysine
• Biotin is covalently attached to biotin carboxylase carrier domain
• Biotin transports CO2 from biotin carboxylase active site to pyruvate carboxylase active site of an adjacent subunit (acting as swing arm, or tether)

–> biotin is NOT carboxylated UNLESS acetyl CoA is present (allosteric regulation)

Question 8

Oxaloacetate must be transported to the cytoplasm to complete the synthesis of phosphoenolpyruvate. Explain this process.

Answer 8

• There is no specific transport of oxaloacetate from mitochondria into cytoplasm, thus, to complete the synthesis to phosphoenolpyruvate, oxaloacetate is reduced to malate, then transported into cytoplasm
  • This involves enzyme malate dehydrogenase
• In cytoplasm, malate is re-oxidized to re-form oxalacetate, which alongside generates cytoplasmic NADH
  • NADH is utilized in subsequent steps of gluconeogenesis

Question 9

2. Oxaloacetate to phosphoenolpyruvate via enzyme phosphoenolpyruvate carboxykinase (PEPCK)

Answer 9

• Phosphoenolpyruvate carboxykinase (PEPCK) generates phosphoenolpyruvate from oxaloacetate in phosphorylation and decarboxylation reactions
• This step occurs at expense of 1 GTP
• Phosphoryl donor is GTP. CO2 that was added to pyruvate by by pyruvate carboxylase gets taken off

**addition of phosphoryl group to pyruvate is very unfavorable and an endergonic reaction

**carboxylation and decarboxylation reactions are favorable and used to power phosphorylation

**CO2 that was added by pyruvate carboxylate comes which helps set up the unfavorable reactions

** decarboxylations often drive reactions that are highly endergonic

Question 10

8. Fructose 1,6-BP to F6P via enzyme fructose 1,6-bisphosphatase

Answer 10

Phosphoenolpyruvate is metabolized by the enzymes of glycolysis in the reverse direction until the next irreversible step: hydrolysis of fructose 1,6-biphosphate)

• Enzyme for this reaction = fructose 1,6-biphosphatase (highly regulated allosteric enzyme)
• This step and activity is reciprocal of enzyme of PFK in glycolysis

Question 11

10. G6P to glucose via enzyme glucose 6-phosphatase

Answer 11

• F6P is converted into G6P by phosphoglucose isomerase (not regulated or irreversible step)
• Free glucose is generated from G6P via glucose 6-phosphotase (important control point)
• Takes place in liver and reverses the activity of glucokinase in liver
• Glucose 6-phosphotase is ER membrane anchored and reactions catalyzed by this enzyme take place on inner surface of ER

** this allows the phosphate to be removed and glucose to move out of the cell via GLUT transporters

• Other tissues (muscle) lack this phosphate; thus gluconeogenesis occurs up to point of generating G6P
• G6P is then added to top up tissue glycogen rather then export free glucose

Question 12

Net reaction of gluconcegenesis

Answer 12

• Net reaction for gluconeogenesis is energetically unfavorable unless it is coupled to favorable reactions
• Cost of gluconeogenesis = 4 ATP and 2 GTP w/ 6 high-transfer potential phosphoryl groups required in synthesis of glucose from pyruvate

2 pyruvate + 4 ATP + 2 GTP + 2 NADH + 2(H+) + 6 H2O –> glucose + 4 ADP + 2 GDP + 6 Pi + 2 NAD+

• Evidence of coupling (ATP/decarboxylation) drives unfavorable reactions
• Glycolysis: only 2 ATP net are generated
• Gluconeogenesis and glycolysis are reciprocally regulated so that within a cell, one pathway is relatively inactive while other is highly active

** The rationale for reciprocal regulation**

Glycolysis will predominate when glucose is abundant

Gluconeogenesis will be highly active when glucose is scarce

Question 13

The level of fructose 2,6-bisphosphate (F-2,6-BP) is ____ in the fed state and _____ in starvation

Answer 13

high; low

Question 14

The key regulation site in the gluconeogenesis pathway is the interconversion of

a) glucose and glucose 3-phosphate
b) fructose 3-phosphate and fructose 1,3-bisphosphate
c) fructose 6-phosphate and fructose 1,6-bisphosphate

Answer 14

c) fructose 6-phosphate and fructose 1,6-bisphosphate

Question 15

Fill in the blanks with regards to the key regulation site of the gluconeogenesis pathway.

Consider first a situation in which energy is needed. In this case, the concentration of AMP is _____. Under this condition, AMP stimulates _______ but inhibits _________. Thus, glycolysis is turned _____ and gluconeogenesis is ______

Answer 15

high; PFK; fructose 1,6-bisphosphatase; on; inhibited

Question 16

ATP and citrate inhibit _______, whereas citrate activates ____________

a) phosphofructokinase; fructose 1,6-bisphosphatase
b) fructose 1,6-bisphosphatase; phosoenolpyruvate
c) phosphofructokinase; fructose 1,3-bisphosphate

Answer 16

a) phosphofructokinase; fructose 1,6-bisphosphatase

Question 17

Liver glycolysis/gluconeogensis regulation: overview

Answer 17

• Key regulator: fructose 2,6-bisphosphate

–> activator of phosphofructokinase
–> inhibitor of fructose 1,6-bisphosphatase

• bifunctional enzyme: synthesis and hydrolysis of fructose 2,6-BP is facilitated by a bifunctional enzyme where both kinase and phosphatase activity are located on a single polypeptide chain

–> one domain is phosphofructokinase 2 (PFK2) (responsible for the synthesis of fructose 2,6-bisphosphate)
–> one domain is fructose 2,6-bisphosphatase (FBPase2) (responsible for hydrolysis)

• bifunctional enzyme regulated by glucagon signal

–> activity of the domains are regulated by blood glucose levels
–> When blood glucose is low, the hormone glucagon is degraded
–> glucagon signaling pathway leads to phosphorylation of bifunctional enzyme, which inhibits the kinase activity and stimulates phosphatase activity (turning off kinase automatically turns on phosphatase and vice versa)

Question 18

Liver glycolysis/gluconeogensis regulation: steps to the reciprocal control of the bifunctional enzyme PFK2/FBPase2

Answer 18

1. Glucagon signal through PKA leads to addition of phosphate to serine residue on PFK2-FBPase2 enzyme (bifunctional enzyme)

The activities of PFK2 and FBPase2 are reciprocally controlled by the phosphorylation of a single serine residue.

–> Turns off kinase and turns on phosphate (F-2,6-BP –> F6P)
–> no PFK stimulation –> gluconceogenesis predominates, glycolysis inhibited
–> Covalent modification activates FBPase2 and inhibits (restrains) PFK2, lowering the concentration of F-2,6-BP
–> Glucose formed by liver under these conditions is essential for viability of brain. Glucagon stimulation of PKA inactivates pyruvate kinase in liver

–> PFK activated –> glycolysis stimulated, gluconeogenesis inhibited
–> Covalent modification activates PFK2 and inhibits (restrains) FBPase2
–> The resulting increase in concentration of F-2,6-BP accelerates glycolysis
–> The coordinated control of glycolysis and gluconeogenesis is facilitated by the location of the kinase and phosphatase domains on the same polypeptide chain as the regulatory domain

Question 19

Type 2 Diabetes & Gluconeogenesis

Answer 19

• Insulin normally inhibits gluconeogenesis
• In type 2 diabetes, insulin fails to act (insulin resistance)
• Enzyme of gluconeogenesis, especially PEPCK (phosphoenolpyruvate carboxykinase), remain active, leading to abnormally high levels of blood glucose
• Treatment of type 2 diabetes includes weight loss, healthy diet, exercise, and drug treatment to enhance sensitivity to insulin

Question 20

Liver Carries a Metabolic Burden

Answer 20

• Liver supports the glucose needs of other tissues
• Lactate produced by muscle during concentration is released into blood
• Liver removes lactate and converts it into glucose, which can be released into blood
• Muscle-liver lactate exchange is called the cori cycle
• Muscle and erythrocytes are source of lactate

Question 21

WHEN does gluconeogenesis occur?

Answer 21

During fasting, starvation, and intense exercise

Question 22

Can humans make glucose from acetyl-CoA?

Answer 22

No

Question 23

Which organs do gluconeogenesis predominate in?

a) liver and intestines
b) liver and kidneys
c) brain and kidneys
d) lungs and heat

Answer 23

b) liver and kidneys

Question 24

Which non-carbohydrate compounds are converted into pyruvate for gluconeogenesis?

a) lactate
b) amino acids
c) glycerol
d) all of the above