| Chem 431 |
Biochemistry |
Fall 2001 |
| Lecture Notes:: 8 October |
© R. Paselk 2001 |
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INTRODUCTION TO ENZYMES
Specificity
Models for Enzyme Specificity:
- Lock & Key model of Fischer: diagram; Hexokinase example:
reaction, methanol and water as ineffective picks. [overhead
8-13, S]
- Induced-fit model of Koshland: diagram; space-filling models
of HK with and without substrate. (Figure 14.2, p386) [overhead
8-13, S; 16-5, V&V{HK}]
Types of specificity:
- Geometric specificity: shape (overhead 12-1, V&V]
- Chiral specificity: most chirally specific enzymes are absolutely
stereospecific.
- Prochirality, because of their own chiral nature enzymes
can often hold substrates in such a way that on one chiral product
is made, distinguishing between seemingly identical groups. [overhead
12.3, V&V]
- Chemical specificity: functional groups, types of chemical
reaction.
Enzyme Kinetics
CHEMICAL REACTION KINETICS
Gives information on dynamic systems.
Sets the parameters for catalytic mechanisms such as:
- Number of species in rate determining step, which species
involved in Transition State.
- Order of steps: Thus for A + B Æ
C + D can have many mech.:
A Æ C + X;
B + X Æ D etc.
Review some Kinetics from General Chemistry:
- First Order: r = k[S] for S Æ
P; & r =-d[S]/dt = d[P]/dt.
- Example - SN1 from organic chemistry: A
+ B Æ C + D as 1st order reaction,
as in the hydroxylation of t-alkylchloride:
- First order because rate depends only on the formation
of the carbocation, which in turn depends only on [R3CCl]
Review some Kinetics from General Chemistry:
-
- Second order: r = k[A][B] for A + B Æ
P; or can have r = k[A]2 ;
- Example - SN2 from organic chemistry: A
+ B Æ C + D as 2nd order reaction,
as in the hydroxylation of primary alkylchlorides:
- Now 2nd order because both RH2CCl and
OH- (reverse of figure above) are involved in slow
step.
-
- Higher order reactions occur, but uncommon.
- Zero order: r = k: Only occurs with catalysts, important
in enzyme catalysis. 0 order also only occurs above a minimum
[A].
ENZYME KINETICS
We have now reviewed kinetics as tools. Before we go to enzymes
a few comments:
- Note: r = -d[S]/dt = d[P]/dt
- Note that for all cases with fixed initial concentrations
except zero order as [A] decreases r decreases, so need to look
at initial rates, that is rate of reaction before a significant
amount of reactant is used up. Biochem vi = ri
- With enzymes can get very high apparent orders due to allosteric
effects.
Plots of vi = d[P]/dt vs. [S] for 0 - 3rd order
Now look at enzymes:
For simple enzyme, S Æ P get
rectangular hyperbola type plot for vi vs [S], similar
to Mb binding curve.
Let's look at a mathematical model and attempt to generate
curve. This was first done by Michaelis and Menten for an equilibrium
model. Better is the steady state model of Haldane and Briggs
(more general), which we will derive.
For S Æ P assume
And for initial reaction conditions [P] = 0 & therefore
k4 = 0, so have
Now vi = d[P]/dt = k3[ES] (Note that
kcat is often used instead of k3);
Assume steady state (steady state assumption: d[ES]/dt= 0):
d[ES]/dt= 0; Thus: 0 = d[ES]/dt= k1[E][S]
- k2[ES] - k3[ES].
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- Last modified 8 October 2001
Pathway Diagrams
