Title: Fuel Usage During the FeastStarve Cycle
1Fuel Usage During the Feast-Starve Cycle
2Glucose Homeostasis !!
3Hyperglycemia Osmotic diuresis
Importance of glucose homeostasis
4No more food coming from gut
EARLY FASTED
FED
5Formation and Degradation of Glycogen
6Review of glycogen structure
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9Some dietary background info
- Calorie kcal
- Typical daily expenditure 2500 Cal
- Typical source of calories for Americans
- 40 fat
- 45 CHO
- 15 protein
10Glycogen content, liver
- Maximum 742 kcal
- Typically after a meal 300 kcal
- After O.N. fast 200 kcal
- After 24-36 hr fast 15 kcal
Rule of thumb Liver stores are gone in 24 hr.
11Glycogen content, muscle
- After O.N. Fast 500 kcal
- After a meal 600 -700 kcal
- After CHO Loading 1000 kcal
- After prolonged fast 250 kcal
12Structure-Function
- Why store glucose as a polymer?
- What is the advantage of branching?
13Physiological Importance ofGlycogen
14In regulating blood glucose
Physiological importance
- During absorptive phase glycogenesis in liver
and muscle prevents hyperglycemia - Glcblood Glycogenliver, muscle
- During fasting phase and exercise
glycogenolysis in liver prevents hypoglycemia - Glcblood
15Allows muscle to performstrenuous exercise
Physiological importance
16Clinical Aspects
Physiological importance
- Inborn errors of metabolism
- Diabetes
17Illustration of metabolic regulation
Significance regarding basic biochemical concepts
- Different pathways for synthesis and degradation
- Reciprocal regulation
- Role of hormones -- signal transduction
18Catabolism of Glycogen
19 Pi
20Phosphorylytic cleavage (Step 4 in Fig 1)
Enzyme Glycogen phosphorylase
21Phosphorylase attacks nonreducing termini
22Reducing end
23Fates of G1P in liver and muscle
24Liver only!
25Debranching
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29Birds-eye view of glycogenolysis
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32Glycogen Synthesis(glycogenesis)
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34Key concepts
- Synthesis cannot be a reversal glycogenolysis--
thermodynamically unfavorable - Synthesis requires activated building block
UDP-glucose - Separate pathways allow for reciprocal regulation.
35Synthesis of UDP-Glucose
Subsequent hydrolysis of PP drives rx to
completion
pyrophosphatase
2 Pi
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37Addition of new glucosyl residue
- Occurs at non-reducing terminus
- Enzyme glycogen synthase
- requires a primer
- if no primer exists, one is made by the enzyme
glycogenin. - some primer is usually available.
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39Formation of the branches
- Requires a branching enzyme
- Block of 7 residues is transfered from terminus
to interior
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41Summary of synthesis and degradation
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43Energetics of Storage
(1) Glucose ATP ÿ Glucose 6-phosphate (2)
Glucose 6-phosphate ÿ glucose 1-phosphate (3)
Glucose 1-phosphate UTP ÿ UDP-glucose
PPi (4) PPi H2O ÿ 2 Pi (5) UDP-glucose
glycogenn ÿ glycogenn1 UDP (6) UDP ATP ÿ
UTP ADP (nucleoside diphosphate kinase)
_________________________________
_______________________________ Sum
Glucose 2 ATP glycogenn H2O ÿ glycogenn1
2 ADP 2 Pi
Requires 2 ATP to store 1 glucose residue as
glycogen
44Energy cost of storage, cont
- Glucose Glycogen 6 loss
- Glucose Fatty acids 25 loss
45Regulation of Glycogen Synthesis and Degradation
46The general problem in metabolic regulation --
futile cycles
47Examples of potential futile cycles
481. In glycolysis-gluconeogenesis
F-6-P ATP ? F16BP ADP (PFK-1) F16BP H2O
? F-6-P Pi (F1,6-bisphosphatase) Net ATP
H2O ? ADP Pi
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502. In glycogen synthesis-degradation
Overall synthesis of glucosyl residue from G6P
(1) G6P ATP glycogenn H2O ?
glycogenn1 ADP 2 Pi Breakdown of glycogen
to G6P (2) glycogenn1 Pi ? glycogenn
G1P (3) G1P ? G6P _________________
_________________________________________ Net
reaction ATP H2O ? ADP Pi
51General solution coordinated control
reciprocal regulation
- One pathway switched on other off
- Usual target committed enzymes
- Mechanisms of regulating committed enzymes
- phosphorylation
- allosteric activation/inhibition
52Example of committed enzyme glycogen synthase
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54Phosphorylase is the key regulatory enzyme in
glycogenolysis
Glycogen synthase is the key regulatory enzyme in
glycogenesis
55Phosphorylation/DephosphorylationThe most
important mechanism of regulation in fuel
metabolism
Regulation of committed step
56Regulatory scheme...
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58Pi
Pi
59Key hormones in fuel metabolism
- Insulin
- Counter-regulatory hormones
- glucagon
- catecholamines (epinephrine, norepinephrine)
- cortisol
60Liver vs MusclePhysiological considerations
rationale for regulatory effects
61Tissue ObjectivesMuscle vs Liver
- Use glycogen as fuel for intense exercise
- Replenish stores when possible (fed, rest)
- Do NOT release Glc for other tissues
- Buffer blood glucose
- remove Glc from blood after meal
- release Glc into blood during fast or heavy
exercise
62Therefore...
63RegulationMuscle vs
Liver
- Signals for glycogenolysis
- nerve impulse
- epinephrine
- Signal for glycogenesis
- insulin
- Signals for glycogenolysis
- glucagon
- epinephrine
- Signal for glycogenesis
- insulin
64Therefore...
- Liver has receptors for
- insulin
- glucagon
- epinephrine
- Muscle has receptors for
- insulin
- epinephrine
- NOT GLUCAGON
65To complete the picture...
66Adipose tissue
- Mobilizes fat in fasting state
- stimulated by glucagon, epinephrine
- Deposits fat in well fed state
- stimulated by insulin
- Therefore...adipose has receptors for insulin,
glucagon, and epinephrine.
67Details of Glycogen RegulationA
Signal-TransductionAmplification Cascade
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69Transduction of Signal
- Glucagon or epinephrine is the first messenger
(extracellular) - cyclic AMP is the second messenger (intracellular)
70Structure of cyclic AMP
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72 Step 2 of Cascade Detail of Protein
Kinase A Activation
73Effect of insulin dephosphorylation
Activates protein phosphatase -1
(PP-1)
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75Amplification
One definition Effect of one first-messenger
molecule on the ratio of active/inactive forms of
target protein
Theoretical amplification is astronomical. In
vivo amplification in this system is
about 10-fold.
76Epinephrine also acts at alpha-receptors
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78Details of Glycogen Regulation
79Key Exercise Signals
- Epinephrine (external)
- flight or fight response
- Ca2 (internal)
- from neuronal impulse
- AMP (internal)
- from ATP hydrolysis for contraction
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81Glycogen Storage Diseases
82Andersens
McCardles
83PompesA Lysosomal Storage Disease
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85McCardles Disease (muscle phosphorylase
deficiency)Clinical Features
- Exercise Intolerance
- Cramps
- Blood in urine after exercise
- Second wind
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