Download An Introduction to Metabolism

Survey
yes no Was this document useful for you?
   Thank you for your participation!

* Your assessment is very important for improving the workof artificial intelligence, which forms the content of this project

Document related concepts

Glycolysis wikipedia , lookup

Light-dependent reactions wikipedia , lookup

Amino acid synthesis wikipedia , lookup

Adenosine triphosphate wikipedia , lookup

Biosynthesis wikipedia , lookup

Basal metabolic rate wikipedia , lookup

Evolution of metal ions in biological systems wikipedia , lookup

Oxidative phosphorylation wikipedia , lookup

Photosynthetic reaction centre wikipedia , lookup

Enzyme inhibitor wikipedia , lookup

Biochemistry wikipedia , lookup

Metabolism wikipedia , lookup

Enzyme wikipedia , lookup

Transcript
Ch.8
An Introduction to
Metabolism
Flow of energy through life
• Life is built on chemical reactions
– transforming energy from one form to another
organic molecules  ATP &
organic molecules
sun
solar energy 
ATP & organic molecules
organic molecules 
ATP & organic molecules
Metabolism
– Is the totality of an organism’s chemical
reactions
Organization of the Chemistry of Life into
Metabolic Pathways
A metabolic
pathway begins
Enzyme 1
Enzyme 3
with a specific
Enzyme 2
C
A
molecule and
B
D
Product
ends with a
Starting
molecule
product
Each step is
catalyzed by a
specific enzyme
Metabolism
• Chemical reactions of life
– forming bonds between molecules
• dehydration synthesis
• synthesis
• anabolic reactions
– breaking bonds between molecules
• hydrolysis
• digestion
• catabolic reactions
That’s why
they’re called
anabolic steroids!
Thermodynamics
• Energy (E)~ capacity to do work; Kinetic energy~ energy of motion;
Potential energy~ stored energy
• Thermodynamics~ study of E transformations
• 1st Law: conservation of energy; E transferred/transformed, not
created/destroyed
• 2nd Law: transformations increase entropy (disorder, randomness)
Free energy
• Free energy: portion of system’s E that can perform work (at a
constant T)
• Exergonic reaction: net release of free E to surroundings
• Endergonic reaction: absorbs free E from surroundings
Change in free energy, ∆G
• The change in free energy, ∆G during a
biological process
– Is related directly to the enthalpy change
(∆H) and the change in entropy (∆S)
∆G = ∆H – T∆S
T = temp in Kelvin (K)
Chemical reactions & energy
• Some chemical reactions release energy
–
–
–
–
–
exergonic
∆G < 0
spontaneous
digesting polymers
hydrolysis = catabolism
digesting molecules=
LESS organization=
lower energy state
Free energy
Reactants
Amount of
energy
released
(∆G <0)
Energy
Products
Progress of the reaction
Figure 8.6 (a) Exergonic reaction: energy released
Chemical reactions & energy
• Some chemical reactions require input of energy
endergonic
∆G > 0
non-spontaneous
building polymers
dehydration synthesis = anabolism
building molecules=
MORE organization=
higher energy state
Products
Free energy
–
–
–
–
–
Energy
Reactants
Progress of the reaction
Figure 8.6 (b) Endergonic reaction: energy required
Amount of
energy
released
(∆G>0)
The energy needs of life
• Organisms are endergonic systems
– What do we need energy for?
• synthesis
– building biomolecules
•
•
•
•
reproduction
movement
active transport
temperature regulation
Where do we get the energy from?
• Work of life is done by energy coupling
– use exergonic (catabolic) reactions to fuel
endergonic (anabolic) reactions
digestion
+
synthesis
+
+
energy
+
energy
Living economy
• Fueling the body’s economy
– eat high energy organic molecules
• food = carbohydrates, lipids, proteins, nucleic acids
– break them down
• digest = catabolism
– capture released energy in a form the cell can use
• Need an energy currency
– a way to pass energy around
– need a short term energy
storage molecule
Whoa!
Hot stuff!
ATP
ATP
• Adenosine TriPhosphate
– modified nucleotide
• nucleotide =
adenine + ribose + Pi  AMP
• AMP + Pi  ADP
• ADP + Pi  ATP
– adding phosphates is endergonic
How efficient!
Build once,
use many ways
high energy bonds
I think
he’s a bit
unstable…
don’t you?
How does ATP store energy?
ADP
AMP
ATP
O– O– O– O – O–
–OP –OP
– –OP
––OP
–
O––OP
O–
O O O O O
• Each negative PO4 more difficult to add
– a lot of stored energy in each bond
• most energy stored in 3rd Pi
• 3rd Pi is hardest group to keep bonded to molecule
• Bonding of negative Pi groups is unstable
– spring-loaded
– Pi groups “pop” off easily & release energy
Instability of its P bonds makes ATP an excellent energy donor
How does ATP transfer energy?
ATP
ADP
O– O– O–
–OP –OP
– –OP
–
O–
O O O
O–
–OP O– +
O
• ATP  ADP
– releases energy
• ∆G = -7.3 kcal/mole
• Fuel other reactions
• Phosphorylation
– released Pi can transfer to other molecules
• destabilizing the other molecules
– enzyme that phosphorylates = “kinase”
7.3
energy
An example of Phosphorylation…
H H
C C
OHHO
• Building polymers from monomers
– need to destabilize the monomers
– phosphorylate!
H
C
OH
+
H
C
HO
H
It’s
C
never that
OH
+
simple!
H
C
+
P
H
C
HO
synthesis
+4.2 kcal/mol
“kinase”
enzyme
ATP-7.3 kcal/mol
-3.1 kcal/mol
enzyme
H H
C C
O
H
C
+
+
H2O
ADP
P
H H
C C
O
+
Pi
ATP / ADP cycle
Can’t store ATP
 good energy donor,
not good energy storage
ATP
cellular
respiration
7.3
kcal/mole
 too reactive
 transfers Pi too easily
 only short term energy storage
ADP + Pi
 carbohydrates & fats are
long term energy storage
A working muscle recycles over
10 million ATPs per second
Whoa!
Pass me
the glucose
(and O2)!
Another example of Phosphorylation…
• The first steps of cellular respiration
– beginning the breakdown of glucose to make ATP
Those
phosphates
sure make it
uncomfortable
around here!
glucose
C-C-C-C-C-C
hexokinase
phosphofructokinase
P
2
2
ATP
C
C
ADP
fructose-1,6bP
P-C-C-C-C-C-C-P
DHAP
P-C-C-C
G3P
C-C-C-P
H
C
P
activation
energy
Too much activation energy for life
• Activation energy
– amount of energy needed to destabilize the
bonds of a molecule
– moves the reaction over an “energy hill”
glucose
Reducing Activation energy
• Catalysts
– reducing the amount of energy to
start a reaction
uncatalyzed reaction
Pheeew…
that takes a lot
less energy!
catalyzed reaction
NEW activation energy
reactant
product
Catalysts
• So what’s a cell got to do to reduce
activation energy?
– get help! … chemical help…
ENZYMES
Call in the
ENZYMES!
G
Substrate Specificity of Enzymes
Substrate
• The substrate
– Is the reactant an enzyme acts on
Active site
• The enzyme
– Binds to its substrate, forming an
enzyme-substrate complex
Enzyme
• The active site
Figure 8.16
– Is the region on the enzyme where
the substrate binds
(a)
Naming conventions
• Enzymes named for reaction they catalyze
– sucrase breaks down sucrose
– proteases break down proteins
– lipases break
down lipids
– DNA polymerase builds DNA
• adds nucleotides
to DNA strand
– pepsin breaks down
proteins (polypeptides)
Factors Affecting Enzyme Function
•
•
•
•
•
•
•
Enzyme concentration
Substrate concentration
Temperature
pH
Salinity
Activators
Inhibitors
catalase
Factors affecting enzyme function
• Enzyme concentration
– as  enzyme =  reaction rate
• more enzymes = more frequently collide with substrate
– reaction rate levels off
reaction rate
• substrate becomes limiting factor
• not all enzyme molecules can find substrate
enzyme concentration
Factors affecting enzyme function
• Substrate concentration
– as  substrate =  reaction rate
• more substrate = more frequently collide with enzyme
– reaction rate levels off
reaction rate
• all enzymes have active site engaged
• enzyme is saturated
• maximum rate of reaction
substrate concentration
Factors affecting enzyme function
• Temperature
– Optimum T°
• greatest number of molecular collisions
• human enzymes = 35°- 40°C
– body temp = 37°C
– Heat: increase beyond optimum T°
• increased energy level of molecules disrupts bonds in
enzyme & between enzyme & substrate
– H, ionic = weak bonds
• denaturation = lose 3D shape (3° structure)
– Cold: decrease T°
• molecules move slower
• decrease collisions between enzyme & substrate
Enzymes and temperature
• Different enzymes function in different
organisms in different environments
reaction rate
human enzyme
hot spring
bacteria enzyme
37°C
temperature
70°C
(158°F)
Factors affecting enzyme function
• pH
– changes in pH
• adds or remove H+
• disrupts bonds, disrupts 3D shape
– disrupts attractions between charged amino acids
– affect 2° & 3° structure
– denatures protein
– optimal pH?
• most human enzymes = pH 6-8
– depends on localized conditions
– pepsin (stomach) = pH 2-3
– trypsin (small intestines) = pH 8
0 1 2 3 4 5 6 7 8 9 10 11
Factors affecting enzyme function
• Salt concentration
– changes in salinity
• adds or removes cations (+) & anions (–)
• disrupts bonds, disrupts 3D shape
– disrupts attractions between charged amino acids
– affect 2° & 3° structure
– denatures protein
– enzymes intolerant of extreme salinity
• Dead Sea is called dead for a reason!
Enzyme cofactors
• Cofactors
– Are non-protein enzyme helpers e.g. zinc,
iron, copper atoms
• Coenzymes
– Are organic cofactors e.g. vitamins
coenzyme
abbreviation
entity transfered
nicotine
adenine
dinucelotide
NAD - partly
composed of
niacin
electron
(hydrogen atom)
nicotine
adenine
dinucelotide
phosphate
NADP -Partly
composed of
niacin
electron
(hydrogen atom)
flavine
adenine
dinucelotide
FAD - Partly
composed of
riboflavin (vit.
B2)
electron
(hydrogen atom)
coenzyme A
CoA
Acyl groups
coenzymeQ
CoQ
electrons
(hydrogen atom)
coenzymes in group transfer
reactions
Enzyme Regulation
• Regulation of enzyme activity helps control
metabolism
• A cell’s metabolic pathways
– Must be tightly regulated
Enzyme Inhibitors
• Competitive
inhibitors
– Bind to the active
site of an enzyme,
competing with the
substrate
A substrate can
bind normally to the
active site of an
enzyme.
Substrate
Active site
Enzyme
(a) Normal binding
A competitive
inhibitor mimics the
substrate, competing
for the active site.
Figure 8.19
(b) Competitive inhibition
Competitive
inhibitor
Enzyme Inhibitors
• Noncompetitive inhibitors
– Bind to another part of an enzyme, changing
the function
A noncompetitive
inhibitor binds to the
enzyme away from
the active site, altering
the conformation of
the enzyme so that its
active site no longer
functions.
Noncompetitive inhibitor
Figure 8.19
(c) Noncompetitive inhibition
Allosteric regulation
• Conformational changes by regulatory
molecules
– inhibitors
• keeps enzyme in inactive form
– activators
• keeps enzyme in active form
Conformational changes
Allosteric regulation
Feedback inhibition
Active site
available
– The end product
of a metabolic
pathway shuts
down the pathway
Initial substrate
(threonine)
Threonine
in active site
Enzyme 1
(threonine
deaminase)
Isoleucine
used up by
cell
Intermediate A
Feedback
inhibition
Active site of
enzyme 1 no
longer binds
threonine;
pathway is
switched off
Enzyme 2
Intermediate B
Enzyme 3
Intermediate C
Isoleucine
binds to
allosteric
site
Enzyme 4
Intermediate D
Enzyme 5
Figure 8.21
End product
(isoleucine)
Cooperativity
• Substrate acts as an activator
– substrate causes conformational
change in enzyme
• induced fit
– favors binding of substrate at 2nd site
– makes enzyme more active & effective
• hemoglobin
Hemoglobin
 4 polypeptide chains
 can bind 4 O2;
 1st O2 binds
 now easier for other 3
O2 to bind