PC30103 Biochemistry of Sports Lecture 3 - Carbohydrate Metabolism II PDF

Summary

These lecture notes cover carbohydrate metabolism, specifically focusing on glycolysis, the fate of pyruvate, and the tricarboxylic acid (TCA) cycle. Diagrams and explanations are included to illustrate these processes and related concepts.

Full Transcript

PC30103: Biochemistry of Sports

Lecture 3: Carbohydrate Metabolism II

24-10-2024
 Revision: Sources of ATPs in your body
Muscle cells (myocytes) have several
different ways to make ATPs. These
systems work together in 4 orders.

Limited ATP storage
3S

Phosphocreatine (PCr)
8-10S

Anaerobic respiration (glycolysis, lactic acid
metabolism and glycogenolysis)
90S

Aerobic respiration (TCA cycle and electron
transport chain, ETC)
Very long!
 Glycolysis (10 reactions)
1 2

How many
ATPs are being
Split one 6C *phosphofructokinase
3 produced via
molecule to two 4
3C molecules!
glycolysis?
Reaction ATP

Used 1, 3 -2

Produce (7, 10) X +4
from 2
6 molecules
5 7
Net +2

*2 molecules

10 9

8
Source: MacLaren, D., & Morton, J.
(2012). Biochemistry for sport and
exercise metabolism. UK: John
Wiley & Sons.
 The fate of pyruvate
Pyruvate - end product of glycolysis. Once it has been
formed, it passes into the mitochondria and is converted to
acetyl-CoA in the so-called ‘link’ reaction.

Key regulatory enzyme is known as pyruvate
dehydrogenase (PDH).

The formation of acetyl-CoA provides the crossroads
between carbohydrate and fat oxidation, and so the control
of PDH is seen as an important factor in the regulation of
fat and carbohydrate metabolism.
 The fate of pyruvate – “link” reaction

Enter TCA
cycle!

Source: MacLaren, D., & Morton, J.
(2012). Biochemistry for sport and
exercise metabolism. UK: John
Wiley & Sons.
Inside a myocyte (muscle cell): cytoplasm versus mitochondria –
aqueous environment

Glycolysis (anaerobic) takes place in the cytoplasm.
Pyruvate acetyl-CoA “link” reaction, mitochondrion.
Within the mitochondrion, the TCA cycle (aerobic) occurs in the
mitochondrial matrix.
ETC or oxidative phosphorylation (aerobic) occurs at the internal
folded mitochondrial membranes (cristae).
(Source: https://www.yourgenome.org/facts/what-is-a-cell; https://en.wikipedia.org/wiki/Myocyte#/media/File:Blausen_0801_SkeletalMuscle.png;
https://en.wikipedia.org/wiki/Inner_mitochondrial_membrane)
Inside a myocyte (muscle cell): cytoplasm versus mitochondria –
aqueous environment

Glycolysis (anaerobic) takes place in the
cytoplasm.
Pyruvate acetyl-CoA “link” reaction,
mitochondrion.
Within the mitochondrion, the TCA cycle
(aerobic) occurs in the mitochondrial
matrix.
ETC or oxidative phosphorylation
(aerobic) occurs at the internal folded
mitochondrial membranes (cristae). Why?

(Source: https://www.yourgenome.org/facts/what-is-a-cell; https://en.wikipedia.org/wiki/Myocyte#/media/File:Blausen_0801_SkeletalMuscle.png;
https://en.wikipedia.org/wiki/Inner_mitochondrial_membrane)
 Today – aerobic respiration to produce more ATPs
- TCA (citric acid cycle), ETC (oxidative phosphorylation)

Sources: Demetrius, L.,
Magistretti, P., & Pellerin, L.
(2014). Alzheimer's disease: The
amyloid hypothesis and the
Inverse Warburg effect. Frontiers
in physiology, 5, 522.
doi:10.3389/fphys.2014.00522.
 Tricarboxylic acid cycle (TCA cycle)
Acetyl-CoA (two-carbon) then enters the TCA cycle, where it attaches to a four-
carbon compound, oxaloacetic acid (OAA) to form citric acid/citrate (six-
carbon) – Citric acid cycle, Krebs cycle.

Citrate is then converted to isocitrate, then to succinyl-CoA and then to alpha-
ketoglutarate. The formation of alpha-ketogluterate produces NADH, as does the
next reaction to succinyl-CoA also produces NADH.

Succinyl-CoA then forms fumarate in a reaction that produces an FADH2.

Fumarate then forms malate, and then malate forms OAA again, with the
production of another NADH.

So the net effect of the TCA cycle from one Acetyl-CoA is to produce three
NADH, one FADH2 and one ATP.
 Tricarboxylic acid cycle (TCA cycle)
2C

4C 6C

8
enzymes 6C
are
involved
4C
in TCA
cycle!

4C

5C

4C Source: MacLaren, D.,
& Morton, J. (2012).
Biochemistry for sport
and exercise
4C metabolism. UK: John
Wiley & Sons.
 Electron transport chain (ETC)

Also known as electron transfer chain and oxidative
phosphorylation.

Inside the mitochondrion cristae (big area/luas permukaan) for the
reactions to occur efficiently.

NADH (from glycolysis and TCA cycle) and FADH2 (from TCA
cycle) will enter ETC and undergo oxidative phosphorylation to
produce ATPs.

Each NADH results in the formation
of three ATPs via oxidative
phosphorylation whilst the FADH2
is re-oxidized to form two ATPs
via oxidative phosphorylation.
Electron transport chain (ETC) – the concept of oxidation & reduction

The basics of electron transfer can be realized in reduction-oxidation - redox reactions
in which a molecule.

Molecule - when reduced, gains an electron. Once in its reduced form, the molecule
needs to become oxidized again to get rid of this electron.

Thus, the reduced form of a molecule gains an electron and an oxidized form loses an
electron.
Previously More modern term
Oxidation +O -H - e-

Reduction -O +H + e-

When NADH is formed from NAD, NADH is the reduced form and the NAD+ is the
oxidized form. For NADH to become NAD, it needs to donate an electron to another
molecule. If it does so, this other molecule then becomes reduced.
 Electron transport chain (ETC) – the process

Electron transfer chain occurs when electrons are donated from
NADH and FADH2 (with losing of H+ too) along a chain in the
inner mitochondrial membrane.

These are in effect a series of reduction-oxidation reactions.

Involves four complexes (I to IV) that temporarily accept the
electron, but then expel it until it meets the final electron
acceptor, O2.

H+ form a steep gradient in the intermembrane space and tend to
come back into the mitochondrion matrix through the enzyme ATP
synthetase (door) – create a great force – for the enzyme to work
(joining ADP and Pi to form ATP).
 Electron transport chain (ETC) - structure
Important elements
in this structure
Complex Real name e- e-
I NADH-Q e-
e-
reductase e-
e-
II coenzyme-Q
ATP
synthetase
III cytochrome
reductase e-
IV Cytochrome C
and
cytochrome
oxidase
ATP synthetase

iron-containing molecules -
iron deficiency in the human
body - impair aerobic energy
production.
Source: MacLaren & Morton, J. (2012).
Electron transport chain (ETC) – Oxidative phosphorylation
Mitochondrion matrix

Final electron receptor

ATP synthetase (door)
ADP + Pi ATP
phosphorylation

A great
force/
energy
is
formed
&
used!
(Source:
https://www.shutterstock.com/sear
ch/cartoon+door;
ATP synthetase (door) https://favpng.com/png_view/cart
oon-children-cartoon-child-
illustration-png/zHsBhV0V)
 Calculation of ATP generated in one glucose oxidation

Glycolysis - net production of two ATPs and two NADH
molecules.

‘link’ reaction (conversion of pyruvate to acetyl-CoA) produces
a further two NADH, don’t forget you have two pyruvates
generated from one glucose in glycolysis, so you will have two
acetyl-CoA to enter TCA and ETC.

TCA and ETC – 3 NADH, 1 FADH2, 1 ATP. Don’t forget you
have two acetyl-CoA molecules from two pyruvates.

1 NADH when oxidized can generate 3 ATPs.

1 FADH2 when oxidized can generate 2 ATPs.
Calculation of ATP generated in one glucose oxidation

2

“link” reaction
2

+ ETC
Sources of ATP - Primary energy sources (to generate ATPs)
for different running distances

ATP storage

3s
8-10s Glycogenolysis and Tricarboxylic acid cycle
glycolysis (TCA) and Electron
Transport Chain (ETC)
90s Several hours or more
We survive!
 Question?

Now, can you explain why O2 and
water are so important for our
survival?
 Next

Some general knowledges of
prolonged/endurance exercise
related to the body carbohydrate
(CHO) metabolism
 Endurance exercise on carbohydrate metabolism
Endurance exercise - defined as prolonged steady-state exercise performed for
durations between four minutes and four hours.

Middle distance events (e.g. track cycling, rowing, and swimming).

Long distance events (e.g. marathon running) and extended stages of road
cycling such as those of the Tour de France (‘Ironman triathlons’ -
ultraendurance).

(Sources: https://www.cartoonstock.com/directory/m/marathon.asp)
Endurance exercise related to carbohydrate metabolism

Increasing exercise intensity increases CHO utilization (from both muscle
glycogen and blood glucose) and reduces lipid oxidation (from both plasma
FFA and IMTG).

Increased CHO utilization with increasing exercise intensity is due to post-
transformational allosteric regulation of phosphorylase and transformation of
PDH (pyruvate dehydrogenase).

Increasing exercise duration increases lipid oxidation but reduces CHO
oxidation, as reflected by reduced glycogen and blood glucose utilization.

Carbohydrate loading is simply a nutritional strategy to increase the
glycogen stored in your body above its normal amount. This typically
involves several days of eating more CHO than usual while also decreasing
exercise to reduce the amount of CHO you are using.
Endurance exercise related to carbohydrate metabolism

CHO-loading increases muscle glycogen concentration and utilization during
exercise due to increased phosphorylase activity as a result of increased
substrate provision.

Increased pre-exercise muscle glycogen concentration increases PDH
activity and vice versa.

Reduced CHO oxidation following training is due to reduced glycogenolysis
(in turn regulated by reduced allosteric modulation of phosphorylase) and
PDH activity (likely due to reduced pyruvate production).

Liver glycogenolysis is reduced following training, as is muscle glucose
uptake.

The main cause of fatigue in prolonged endurance exercise is likely reduced
muscle glycogen and blood glucose availability, which reduces the
availability of substrate required to maintain the high CHO oxidation rates
necessary to sustain high power outputs.
 Next

Some general knowledges of high-
intensity intermittent exercise
(HIE) related to the body
carbohydrate (CHO) metabolism

(Source:
https://www.123rf.com/p
hoto_21157975_vector-
illustration-of-cartoon-
rugby-player.html)
 HIE related to carbohydrate metabolism
High-intensity intermittent exercise (HIE) is characterized by brief periods of
high-intensity activity (near maximal or supra-maximal) interspersed with
periods of low- to moderate intensity exercise or periods of inactivity (i.e. rest).

Eg. soccer, rugby, basketball.

Energy production during HIE may be fuelled by both anaerobic (PCr
hydrolysis, adenylate kinase, anaerobic glycolysis) and aerobic metabolism of
both carbohydrate and lipids.

It is a common misconception that “anaerobic metabolism” is the most
important energy producing pathway during HIE. Indeed, “oxidative
phosphorylation” becomes more important to ATP turnover with each
successive bout of high-intensity interval exercise and, in some cases, is the
main contributor to ATP production.
 HIE related to carbohydrate metabolism
CHO ingestion prior to HIE augments plasma insulin, glucose and CHO
oxidation and suppresses plasma glycerol, FFA and lipid oxidation.

CHO ingestion during HIE may spare muscle glycogen utilization, maintain
CHO oxidation rates and improve exercise capacity.

In the context of prolonged HIE that is relevant to sport, fatigue may be
related to depletion of substrates such as glycogen and PCr, especially in
type II fibres.
 Thank you

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