Homogeneous Catalyst

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Homogeneous catalysis plays an important role in industries like pharmaceuticals and polymers though its contribution is smaller compared to heterogeneous catalysis. Organometallic complexes have revolutionized homogeneous processes.

Advantages include no pore diffusion limitations and better understood mechanisms. Disadvantages include difficulty in catalyst separation and stability only under mild conditions.

Condensation, dehydration, hydrolysis and halogenations. Examples given are manufacture of bisphenol A and ethyl acetate, and dehydration of ethanol to ethylene.

NPTEL Chemical Engineering Catalyst Science and Technology

Lecture 31
Homogeneous catalysis
Contribution of homogeneous catalytic process in chemical industry is significantly
smaller compared to heterogeneous catalytic process, it is only about 17-20 %. But
importance of homogeneous catalysis is increasing significantly. The significance of
homogeneous catalysis is growing rapidly particularly in the area of pharmaceutical and
polymer industry. Some of the important industrial processes include:
1. Oxidations of alkenes such as production of acetaldehyde, propylene oxide etc.
2. Polymerization such as production of polyethylene, polypropylene or polyesters.

A new major development in homogeneous catalysis is the application of organometallic


complexes as catalysts. The use of organometallic catalysts has revolutionized the
homogeneous processes increasing economic viability. Another new area is bio-catalysis
involving enzymes catalysts. Enzyme catalysts are highly selective and active for
production of fine chemicals, pharmaceuticals etc. Enzyme catalysts are discussed in a
separate section.
In homogeneous catalysis, all the reactants and catalysts are present in a single fluid
phase and usually in the liquid phase. Homogeneous catalysts are the simple molecules or
ions such as HF, H2SO4, Mn+2 as well as complex molecules such as organometallic
complexes, macrocyclic compounds and large enzyme molecules.
Advantages
Advantages of homogeneous processes can be summarized as follows:

In many reactions, homogeneous catalysts are more active and/or selective


compared to heterogeneous catalysts.

In homogeneous catalysis, the catalysts are molecularly dispersed within the


fluid. Hence, pore diffusion limitations are absent. However, bulk phase mass
transfer limitation may occurs.

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Catalytic chemistry and mechanism for homogeneous catalysis are better studied
and understood. Therefore, it is easier to control and manipulate the process
parameters.

Disadvantages
However, homogeneous processes are also associated with some major disadvantages
which result in limited use of these processes. These disadvantages are summarized
below:
Homogeneous catalysts are stable only in relatively mild conditions which limit their
applicability.
Since the catalysts are molecularly dispersed in the phase as the reactant, products and
solvents, the separation at end of the process is difficult and expensive. In many cases, it
is not possible to recover the catalyst.
Types of reactions
Several homogeneous catalytic systems are :
1. Acid base catalysis
2. Catalysis by metal ions
3. Catalysis by organometallic complexes
4. Catalysis by Lewis acids
5. Catalysis by porphyrin complexes
6. Catalysis by enzymes

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1. Catalysis by acids or bases


Acid base catalysts are used in the following types of reactions:
i. Condensation
ii. Dehydration
iii. Hydrolysis
iv. Halogenations
Examples
a) Acid catalyzed condensation

i.

Acid catalyzed condensation of phenol and acetone to bisphenol which is


an important intermediate in the manufacture of epoxy resin and
polycarbonates.

CH 3COCH 3 + 2 OH + 2 H +
OH C ( CH 3 ) 2 OH + H 2O

= benzyl group

ii. Acid catalyzed synthesis of ethyl acetate ester from ethanol and acetic acid.
CH 3CH 2OH + CH 3COOH CH 3COOCH 2CH 3 + H 2O

b) Acid catalyzed dehydration of ethyl alcohol to ethylene


+

H
CH 3CH 2OH
CH
=
CH 2 + H 2O
2

c) Hydrolysis of esters

i.

Hydrolyses of carboxylic esters to form the parent carboxylic acid and an


alcohol.
O

H 2O
heat

C
R

OR'

C
R

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ROH

OH

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d) Acid or base catalyzed halogenation

Ketones can be halogenated in the presence of acid or base and X2(X= Cl, Br).
O

C
C

H3C
H

Br2
CH3

Base

H3C

Br

C
Br

H Br

CH3
Br

2. Catalysis

by

Metal ion
Metal ions can act as catalysts. Metal ions function in different ways :
1. Metal ion can act as a super acid. It introduces positive charge into the
substrate, making it more susceptible toward nucleophilic attack.
2. Metal ions can also act as templates. Metal ions are able to coordinate to more
than 2 ligands and thereby bring the molecules together.
3. Metal ions can act as redox catalysts. Many metal ions can accept or donate
electrons by changing their oxidation state and thereby participate in redox
reactions.
Examples
a) Catalysis by Cu2+ ions
Cu2+ ions are very effective catalysts for the hydrolysis of -amino acid esters.
2+

Cu
CHRNH 2 COOCH 3
CHRNH 2 COOH + CH 3OH
H 2O

b) Catalysis by Mg2+ ions


Hydrolysis of phosphate esters is catalyzed by metal ions, usually Mg2+.
2+

Mg
CH 3 COOPO3
CH 3COOH + H 3 PO4
H 2O

3.

Catalysis by organometallic complexes

Presently, organometallic catalysts play major role in homogeneous catalysis.


Organometallic complex consist of a central transition metal ion bonded to organic
ligands such as R2C=CR2, RCO, R3P, R3N, CO etc. Catalysis occurs through dissociation
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of ligands followed by co-ordination of reactant molecule to the metal ion. The transition
metal ions react through exchange of d electrons. Organometallic complexes usually have
octahedral or tetrahedral geometry. Reactions catalyzed by organometallic complexes
include

hydrogenation,

hydroformylation,

carbonylation

and

decarbonylation,

hydrocarbon rearrangement, partial oxidations etc.


Effect of ligands
The nature of surrounding ligands is very important in organometallic catalysis and
known as ligand effect. The product distribution depends on the ligand environment
around the metal center. Using the same metal center, different products can be obtained
with the same substrate when associated ligands are changed around the metal center.
Ligand types
Phosphine based ligands ( PR3 ; where R= t-Bu, n-Bu, Ph, CH3O, CF3CH2O, Cl, CF3) are
most widely used. The alkyl phosphines are strong bases and are donor ligands while
the organophosphites, P(OR)3 , are strong acceptors and form stable complexes with
electron rich transition metal by accepting electrons.
Other ligands that are used are discussed below :
1. Hydrocarbyl group : Cyclopentadieneyl ligands (Cp) are associated with metals
such as Ti, Zr, Hf . The Cp2TiCl2 catalyst is used in ethylene polymerization.
Ruthenium complexes containing aromatic ligands are used for hydrogen transfer
reactions such as transfer of hydrogen from alcohol to ketone producing another
alcohol.
2. Alkoxide, imides and imido are used as anionic ligands in zirconium and titanium
catalysts for the polymerization of alkene. These are mostly used in combination
with cyclopentadienyl ligands.
3. Nitrogen ligands include pyridine and imidazole ligands. They are more stable
than phosphine based ligands. Enzyme catalysts contains mostly nitrogen ligands
in the form of imidazoles or porphyrins binding to metals such as copper or iron.

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Some other nitrogen based ligands such as amido ligands, diimine ligand are
shown in Fig 2.
4. Some other ligands such as phosphine with nitrogen substituents, carbon based
ligands are also shown in Fig. 2.
i-Pr

i-Pr

N
P

i-Pr

Ph

i-Pr

Ph

i-Pr

i-Pr

N
Ph

N
P

P
O

Ph

NMe2

i-Pr

OPh

i-Pr

Fig. 2. Examples of phosphorous, nitrogen and carbon based ligands

4. Catalysis by Lewis acids


a.

Diels alder reactions

Reaction of diene with a mono-ene form cyclohexene derivativeis shown below.


AlCl3

AlCl3

AlCl3
O

OCH 3

OCH 3
OCH3

b. Epoxidation
Epoxidation reaction is important reaction for producing organic intermediates.
Alkenes can be transformed to epoxide by hyperoxides and catalysts. Catalysts
are often titanium or molybdenum complex acting as Lewis acid.

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tBu
tBu

O
+

O
H

OH

+
Ti

Ti

5. Catalysis by porphyrin complexes


Porphyrin complexes are used to catalyze epoxidation and hydroxylation reactions. The
porphyrins are macrocyclic compound. The porphyrin molecule contains fourpyrrole
rings linked via methine bridges.The structure of porphyrin macro molecule is shown in
Fig. 3. The porphyrin ring system is very stable and exhibits aromatic character. The
porphyrin nucleus is a tetradentate ligand inwhich the space is available for a
coordinating metal and has a maximum diameter of approximately 3.7 A0. When
coordination occurs, two protons are removed from the pyrrole nitrogen atoms,
leavingtwo negative charges. Various metals such as Na, K, Li Co, Ni, Cu, Fe, Mn form
complexes.

N
H
H
N

Fig 3.Structure of porphyrin macro molecule

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Epoxidation
The Ru(II)porphyrin complexes is used as epoxidation catalyst of olefins.Ruthenium(II)
carbonyl tetraphenylporphyrinscatalyze epoxidation of olefins in the presence
ofmetachloroperbenzoic acid as oxidants.

Hydroxylation
The hydroxylation of unactivated alkanes can be done inthe presence of iodosylbenzene
and iron porphyrins catalyst. The oxidation of cyclohexane in presence of
iodosylbenzenewith chloro(5,10,15,20-tetra-o-tolylporphyrinato)iron(III) [Fe(TTP)CI]
producescyclohexanol andcyclohexanone as shown below.

H
H

OH
H

iron porphyrins

Text reference

Piet W.N.M. van Leeuwen, Homogeneous catalysis: Understanding the Art,


Springer, 2004

Piet W.N.M. van Leeuwen, and John C. Chadwick, Homogeneous catalysis:


Activity-stability deactivation, Wiley, VCH, 2011

H. Bartholomew and R. J. Farrauto, Fundamentals of Industrial catalytic


Processes, Wiley, VCH, 2006

M. Biesaga, K. Pyrzynska, M. Trojanowicz, Porphyrins in analytical chemistry: A


review, Talanta 51 (2000) 209224

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Lecture 32
Mechanism and reaction rate
Activity
The homogeneous catalyst precursors are added in the reaction system in different forms
and are transformed into the active form insitu. During one catalytic cycle, the catalyst
may pass through several intermediate forms and finally produce the products. After end
of each catalytic cycle, the catalyst itself should be regenerated without any change.
A catalyst should be able to pass through the catalytic cycle multiple times. Higher the
number of times the catalyst passes through this cycle, higher is the activity of the
catalyst. The number of times that a catalyst can go through this cycle converting
substrate molecule to product molecules is defined as the turnover number. In other
words, the turnover number, TON, is the total number of substrate molecules that a
catalyst can convert into product molecules. In homogeneous systems, the turnover
frequency is defined as the number of molecules of substrate converted per second which
is the turnover number in a certain period of time.
Selectivity
Following type of selectivities are defined :
1. Chemoselectivity
When two chemically different functionalities are present in same molecule, then the
selective reaction of one functional group in presence of the other is known as
chemoselectivity. As shown below, the alkene and aldehyde groups present in the same
molecule can undergo hydrogenation resulting in products I, II or III as a result of
hydrogenation of both groups, only aldehyde or only alkene respectively. Selectively
hydrogenating any one of the two functional groups and maximizing the corresponding
product is known as chemoselectivity.

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2.

Hydrogenation

OH

OH

II

III

Regioselectivity

When the functional group can attach to multiple sites, then the selectivity determining
the site of attachment is known as regioselectivity. As in the example shown, for the
hydroformylation reaction of styrene, the formyl group can attach to either terminal
carbon atom or secondary internal carbon atom resulting in linear or branched product,
respectively.
O

Hydroformylation

3. Diastereoselectivity

The isomeric molecules having similar molecular formula but differing in the threedimensional orientation of atoms are known as stereoisomers. Diastereomers are two or
more stereoisomers of a compound that are not mirror images of each other. When
stereoisomers are mirror images of each other that are non-superimposable, they are
called enantiomers.
For a substrate containing a stereogenic centre, the catalyst can direct the addition of
atoms to give two diastereomers.

The selectivity for either diastereomer is called

diastereoselectivity. For example, the addition of dihydrogen as shown below gives two
diastereomers.

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OH

OH

OH

Hydrogenation

4. Enantioselectivity
When substrate is achiral, that is the molecule is superimposable on its mirror image,
catalyst may give rise to the formation of specific product enantiomer as shown in the
example below. This is known as enantioselectivity.
COOR 1

COOR 1

R3

Hydrogenation

R3

NHCOR2

NHCOR 2

COOR 1

R3

NHCOR 2

Homogeneous catalysis mechanism is often represented by catalytic cycles. In catalytic


cycles, usually catalysts are shown as member of cycle and all reactants and products are
placed outside the cycle and connected to it by arrows.

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For example, the cycle of a catalytic reaction A+B P, having intermediates K and L
can be represented as
P

cat

The stable metal complex added to the reaction at the beginning is called catalyst
precursor or precatalyst. Turnover frequency in terms of catalytic cycle can be defined as
number of times the cycles is completed in unit time.
The intermediates species can be studied using various spectroscopic studies such as
FTIR, NMR, UV-Vis etc.
Acid -base catalysis
Mechanism
In acid-base catalysis, both acid and bases may act as catalysts in solution. The H+ is
used for protonating the intermediates and a base or solvent is used for removing the
proton at a later stage. The rate of acid base reactions depends on pH since the rate is a
function of both H+ and OH concentrations. The proton transfer mechanism in general
can be represented as

B + H A [ B H A] B H + A

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Kinetics
In acid catalysis, the proton transfer step is slower and is the rate determining step.
Subsequently, the protonated substrate rapidly reacts to give the product(s) as shown
below :

SH + + A
S + HA
slow

fast
SH +
products

Reaction rate is dependent on all acids/bases present in solution. Rate constant for
reaction is function of concentrations of H+, OH, HA and A . First order rate constant
can be calculated from

k=
k0 + k H + CH + + kOH COH + k HACHA + k A C A
where k0 = rate constant for uncatalyzed reaction (small relative to other terms)
Activity of acid-base catalyst
Activity of an acid depends on its acid strength and molecular structure. Acids of higher
strength are more catalytically active. Strength is defined in terms of equilibrium constant

H + + A
(KHA) for dissociation. HA

K HA =

a H + a A
aHA

where ai is the respective activity

For general acid catalyst, rate constant depends on its acid strength as :

=
log k HA log K HA + constant
Where,

k HA

= rate constant of the catalytic step

K HA = dissociation constant of acid HA

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= Bronsted coefficient (normally 0<

<1)

indicates the sensitivity of catalytic step for changes in acid strength of HA.Similarly,
Brnsted relation for general base catalysis is

=
log k B log K HB + constant
The coefficient has the same meaning as for general acid catalysis.
Mechanisms of few acid-base catalyzed processes are discussed below.
Ester hydrolysis : The hydrolysis of esters is catalyzed by both acids and bases. H2O
acts as the proton donor. The mechanism for acid and base catalyzed hydrolysis can be
represented as :
Acid catalyzed hydrolysis :
O

OH

OH
H 2O

H+
H 3C

OCH3

H 3C

H 3C

OCH3

OCH3

C
OH2

OH

CH3COOH

H 3C

CH3OH

OHCH3

C
OH

Base catalyzed hydrolysis :

OH

O
H3C

OCH3

H2O

O
OH -

H3C

OCH3

H 3C

OH

CH3O -

H 2O

OH

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Dehydration: Acid catalyzed dehydration mechanism is illustrated by dehydration of


ethyl alcohol to ethene. Alcohol is initially protonated. Then, a water molecule leaves
forming a carbocation. Then, -elimination occurs producing the alkene.
+

HA
A
CH 3 CH 2 O H 2
CH 3 C H 2 + H 2O
CH
=
CH 3 CH 2 OH
CH 2 + HA
2

Halogenation :

For base catalyzed halogenation reactions,

the probable reaction

mechanism is illustrated below. The ionization of the ketonic substrate in the presence of
basic catalyst is the rate determining step.
O

C
H3C

s lo w

C
C

Base

CH3

O
C

H 3C

CH3

H 3C

Br
Br

Br2

C
CH3

C
Br

Br

Fast

H 3C

CH3

Br-

Br

Catalysis by Metal ion


The metal ions can coordinate simultaneously to electron donating atoms, such as N
and/or oxygen, present in the reactant. The probable mechanisms of Cu2+ and Mg2+: ion
catalyzed hydrolysis are shown below.

Cu2+

Cu2+
O
H2 N

C u2+

H2N

C
C

OHH2N

C
C

O CH 3
H

OCH3
H

O
C
C
R

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OCH3
OH

H+

H2N

C
C

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CH3OH

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Mg2+
O

Mg2+
O

H 3C

O
H 3C

O
P
O

H 2O
H 2PO 4Fast

CH3COO -

Catalysis by Organometallic complexes


As discussed, for heterogeneous catalysts the reaction starts with the adsorption of
reactant on a vacant site on the

catalyst surface. Similarly, for homogeneous

organometallic complex catalysts, the reaction begins with the reactant molecule getting
attached to a metal centre in the catalyst. Hence, the metallic centers must have vacant
coordination sites. However, it is difficult to maintain vacant sites on the metallic center
as the molecules are always in solvated conditions. Over all, the mechanism can be
described as removal of ligand from the metallic center and addition of reactant to the
vacant site. This mechanism is similar to substitution reaction. There is always
competition for vacant sites between ligand, reactant or solvent molecules. The process is
proposed to occur by associative or dissociative mechanism.
1. Dissociative mechanism
In dissociative ligand exchange mechanism, initially there is breaking of bond between
the metal and leaving ligand. This is the slowest and rate controlling step. A solvent
molecule occupies the open site. Subsequently, the solvent is replaced by reactant in a
fast step.
L
M

L
L

L
L

SOLVENT

solvent +

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L
M

solvent

R = Reactant
2. Associative mechanism
In associative ligand exchange process, bond breaking of ligand from metal and bond
formation between metal and reactant occurs simultaneously as shown below.
L
M

L
L

+ R

Elementary steps
The basic elementary steps that are involved in organometallic chemistry are discussed
briefly.
1. Insertion
In insertion mechanism an unsaturated molecule inserts into a metal- anion bond. In the
shown example, the CO inserts into the metal (Pt)-methyl bond and acyl bond formed (RCO) takes position of methyl group. The vacant position on metal is filled in solvent (S)
molecule.

Me

Me

+
P

Pt
P

Pt

C
O

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2. Migration
In migration mechanism, atom or group of atoms migrates from metal to hydrocarbon. In
the shown example, hydride migrates from metal atom to ethene. The vacant position on
metal is filled in by ligand (L) molecule.
H
M

CH2

CH2

H
M

M
CH 2

H2C

H2C

CH3

3. elimination
This reaction is reverse of migration. The -elimination requires a vacant site at the
complex.
L

-L

H
M

M
CH2-CH2-H

CH2

H 2C

4. Oxidative addition
In this reaction, a compound XY adds to a metal complex during which the XY bond is
broken and two new bonds MX and MY are formed
Y
M

X
X

5. Reductive elimination
It is reverse of oxidative addition
L

CH3

CH3

Pd
L

Pd

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CH3
CH3

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6. Cycloaddition reaction involving metal


In presence of multivalent metal, alkene/alkynes form metallacyclic compounds .

7. Activation of substrate toward nucleophilic attack


Co-ordination of alkene to electronegative metal (may carry a positive charge), activates
the alkene toward attack of nucleophiles.

+
OH-

OH

Pd2+
Pd
K

L
K

Text reference

Piet W.N.M. van Leeuwen, Homogeneous catalysis: Understanding the Art,


Springer, 2004

Piet W.N.M. van Leeuwen, and John C. Chadwick, Homogeneous catalysis:


Activity-stability deactivation, Wiley, VCH, 2011

B. Cornils and W.A. Hermann (Ed.),

Applied homogeneous catalysis with

organometallic compounds, Wiley-VCH, 2000

H. Bartholomew and R. J. Farrauto, Fundamentals of Industrial catalytic


Processes, Wiley, VCH, 2006

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Lecture 33
Reaction rate
An organometallic catalysis reaction is proposed to occur in two steps involving
formation of an intermediate. A typical hydrogenation reaction is shown below where the
first step involves the reversible formation of reactive intermediates.

The second

hydrogenation step is irreversible.


k1

M + S
MS
k
1

k2
M + products
MS + H 2

=
M catalyst
=
S substrate
Usually, it is assumed that the concentration of reactive intermediate, MS, is small and
constant compared to the total concentration of M. The rate of production of products for
the given scheme can be written as follows.

r = k2CMS CH 2 ------------(3)
where Ci is the concentration of component i. A steady state approximation assumes
that the amount of MS being formed and reacting are the same. Equation 4 gives the
steady state approximation as :

dCMS
=
0=
k1CM CS k1CMS k2CMS CH 2 ------------ (4)
dt
The total amount of M ( CM T ) can be obtained from equation 5 as summation of
concentration CM and CMS.

C=
CM + CMS --------------- (5)
MT
By substitution the overall rate is given by equation 6.

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r=

k1k2CM T CS CH 2
k1CS + k2CH 2 + k1

------------- (6)

Consider two conditions:


Case A : Reaction 1 is much slower than reaction 2

1
2

MS
M+S
Product

Case A can be represented by the above scheme which shows that the activation energy
for the forward step 1 is much higher compared to the backward reaction of step 1 or step
2. Hence it implies that k2 > k-1 >> k1 . Then, the rate equation can be simplified as

r = k1CM T CS
Here reaction 1 is slower (higher activation energy) and hence the rate determining step.
As soon as the MS is formed via the slow forward reaction 1 it is converted to products.
In this case, rate of reaction is independent of hydrogen concentration.

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Case B : Reaction 2 much slower than 1


2

M+S

MS
Products

As shown in the above figure , energy barriers for both forward and backward reaction of
step 1 are much lower than that of step 2. The rate determining step is therefore step 2.
That is k, k-1 >> k2 .
Hence ,equation 6 can be simplified and the rate equation is given as

r=

k1k2CM T CS CH 2
k1CS + k1

Selectivity
In a multistep reaction scheme, selectivity is determined as soon as an irreversible step
occurs. It can be understood by the following examples.
Case 1 : Selectivity determining step coinciding with rate determining step

Reactant

Product 1

Product 2
Path A

Path B

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In the proposed scheme shown above, the reaction can proceed by two paths, A and B.
Activation energy barrier for path 1B is lower compared to path 1A. Hence product 2 is
formed preferentially over product 1 and rate of formation of 2 is determined by step
1B.
Case 2 : Selectivity determined by first step while second step is rate determining
1A
1B

2A

2B

Reactant

Product a

Intermediate
state

Intermediate
state

Path A

Product b

Path B

In the above scheme, two products a and b are formed from a reactant in two steps by
path A and B , respectively. Activation energy for step 2 is higher than step 1 for
formation of both products. Hence, barrier 2 is the rate determining step. Again,
activation energy barrier of step 1A in path A is more than step 1B in path B. Hence
product b by path B will be formed preferentially. Thus, the selectivity is determined
before the rate determining step, provided that the activation energy of the backward
reaction from the intermediate state is higher compared to forward reaction.

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Case 3 : Selectivity determined after the rate-controlling step


1

Reactant
Intermediate
state

Product A
Product B

In the above figure, the step 1 has the higher energy barrier and is the rate determining
step. The intermediate formed by step 1 can transform to product A or B via two
pathways. The ratio of products A and B is controlled by the heights of the respective
energy barriers. Since activation energy barrier is lower for product B, it has higher
selectivity. Thus, in this case selectivity is determined in by the second competing steps
after the initial rate -determining step which is same for both products.
Rate equations of homogeneous catalyzed reactions often refer to the liquid phase
concentrations. In most cases, the rate equations are non-linear with respect to the
concentration of the reactant. The concentration of reacting species or products formed
can be measured during reaction using several techniques such as chromatography, UVvisible spectroscopy , IR spectroscopy etc. Homogeneous catalyzed reactions are often
carried out in multiphase systems. Gaseous reactants such as H2, CO, O2 have to be
transferred from the gas phase to the organic liquid phase where the reaction takes place.
When one of the reactants is in the gas phase, such as in hydrogenation reaction, fast
dissolving of the gas into the liquid is required to avoid any external mass transfer
limitations. Mass transfer limitations in a batch reactor can be checked by measuring the
rate as a function of stirring rate. When mass transfer limitation is absent, there should be
no change in reaction rate with stirring rate. However, in the presence of mass transfer
limitations, rate increases with stirring upto an extent then become constant when mixing
is sufficient. Further, to increase the solubility of the gas into liquid, high pressure has to
be used. Any type of reactor such as batch, CSTR or plug flow reactor can be used. For
elucidation of mechanism, rate data at low conversions are highly desirable. These can be
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obtained more easily in a batch reactor. However, maintaining constant temperature by


effective removal or supply of heat is difficult in a batch reactor. To effectively control
the heat and mass transfer limitations, stirring is essential in a batch reactor. If the
reaction is highly exothermic or endothermic, cooling or heating coils are needed,
respectively. Most homogeneous hydrogenations, halogenations, hydro-halogenations,
hydro-formylation and hydro-cynation reactions are first order in olefin reactant. Intrinsic
rate equations of few homogeneous catalyzed reactions are discussed below.
1.

Hydroformylation of propene

Hanna et al. [1] investigated the kinetics of propene hydroformylation over a silicasupported Rhsulfoxantphos complex stabilized by the ionic liquid [bmim][OctSO4]. The
hydroformylation of propene is proposed to be initiated by the loss of a CO ligand from
Rh complex (step 1) followed by coordination to propene (step 2). Migratory insertion
into RhH bond forms a propyl-Rh complex (step 3). For alkene insertion into RhH
bond as rate determining step following rate expression was proposed.
r=

K 1 K 2 k3 PC3 H 6 [ Rh]
PCO + K 1 + K 1 K 2 PC3 H 6

where k3 is the rate coefficient of alkene insertion step 3, K1 and K2 are equilibrium
constants for step 1 and 2 , respectively. PCO and PC3H6 are the partial pressures of CO
and propene, respectively. The [Rh] is the total moles of Rh.
2.

Hydrogenation of cyclohexene

The kinetics of homogeneous hydrogenation of cyclohexene in the presence of the


catalytic system consisting of Rh2Cl2(C8H14)4

and 2-aminopyridine

has been

investigated by Zuber et al. [2]. The proposed mechanism is described below.


+

S
Rh2Cl2 (C8 H14 ) 4 + 4ampy
2 Rh(ampy ) x S y + 2Cl + 4C8 H14
+

K1
Rh(ampy ) x S y + H 2
RhH 2 (ampy ) x S y
+

K2
Rh(ampy ) x S y + C6 H10
Rh ( C6 H10 ) (ampy ) x S y 1

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+

k
RhH 2 (ampy ) x S y + C6 H10
RhH 2 ( C6 H10 ) (ampy ) x S y 1
+

fast
RhH 2 ( C6 H10 ) (ampy ) x S y 1
C6 H12 + Rh(ampy ) x S y

Here ampy is 2-aminopyridine and S is the solvent (EtOH). It is assumed that the catalyst
forms complexes both with cyclohexene (equilibrium constant K1) and with hydrogen
(equilibrium constant K2). The rate of reaction is expressed as:

r=

kK1CcyclohexeneCH 2
1 + K1CH 2 + K 2Ccyclohexene

Ccat

At 40 0C, the rate of hydrogenation of cyclohexene, catalyzed by CoH3(PPh3)3 was


described by Hendrikse et al. [3]. Addition of cyclohexene to the catalyst was proposed
as the rate-limiting step and the following mechanism was proposed.

3
1

A + H 2
AH 3
2
2

AH 3 + P
AH 3 P
AP
A + P
3

r
AH 3 + S
AH 3 S

A = Co(PPh3)2 or its solvated species.

r=

kr C A K1CS CH3/2
1 + K1CH3/2 + K1K 2CH3/2CP + K3CP

[5]

Where, CA, CS, CH and CP are the concentrations of catalyst, cyclohexene, hydrogen and
triphenylphosphine, respectively, in solution. Equation shows that triphenylphosphine is
an inhibitor for the hydrogenation reaction.

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3.

Carbonylation of methanol

The homogeneous rhodium complex catalyzing methanol carbonylation in the presence


of methyl iodide can be described as follows [4]. First, the oxidative addition of methyl
iodide to the active rhodium species occurs. Then, insertion of carbon monoxide to CRh bond occurs. It is followed by the elimination of methyl acetate by methanolysis,
reductive dissociation of HI from the rhodium species and the regeneration of methyl
iodide. The first step, the oxidative addition of methyl iodide, is believed to be the ratedetermining step.

RhLn + CH 3 I CH 3 RhILn
CH 3 RhILn + CO CH 3CO RhILn
CH 3CO RhILn + CH 3OH CH 3COOCH 3 + HRhILn
HRhILn HI + RhLn
HI + CH 3OH CH 3 I + H 2O
The corresponding rate expression is given as
0
0
r = kCMeI CCO
CMeOH

The formation rate has first order dependence on methyl iodide concentration and is
approximately zero order with respect to concentration of both carbon monoxide and
methanol.
4.

Oxidation of cyclohexane

On oxidation of cyclohexane with PhIO in presence of

meso-tetra(3-pyridyl)

porphynatemanganese

meso-tetra(4-pyridyl)

(III)

[Mn(3-TRPyP)]

and

porphynatemanganese(III) [Mn(4-TRPy-P)] species, at 25 0C, was found to yield


cyclohexanol and cyclohexanone as major products.

+ PhIO

Mn(3-TRPyP)

OH +

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O + PhI

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The mechanism for cyclohexane oxidation by PhIO catalyzed by Mn(3-TRPyP) or Mn(4TRPyP) complexes as proposed by Nunes et al. [5] is as follows :
1
< Mn > + PhIO
< Mn O IPh >
fast

I Ph

C 6 H 12 + < Mn O IPh >


< Mn O >
k2

k 2

H C 6 H 11

I Ph
< Mn O >

k
Slow
3

< Mn OH C 6 H 11 > + PhI

H C 6 H 11
4
< Mn O H C 6 H 11 >
< Mn > + C 6 H 11OH
fast

Corresponding rate of equation is given as r = kcat C

Mn

CC6 H12

Text reference

Piet W.N.M. van Leeuwen, Homogeneous catalysis: Understanding the Art,


Springer, 2004

Piet W.N.M. van Leeuwen, and John C. Chadwick, Homogeneous catalysis:


Activity-stability deactivation, Wiley, VCH, 2011

B. Cornils and W.A. Hermann (Ed.)

Applied homogeneous catalysis with

organometallic compounds, Wiley-VCH,2000

H. Bartholomew and R. J. Farrauto, Fundamentals of Industrial catalytic


Processes, Wiley, VCH, 2006

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Journal reference
1. D. G. Hanna, S. Shylesh, S. Werner, A. T. Bell, Journal of Catalysis 292 (2012)
166
2. M. Zuber, B. Bana and F. Pruchnik, Journal of Molecular Catalysis 10 (1981)
143
3.

J. L. Hendrikse and J. W. E. Coenen, Journal of Catalysis 30 (1973) 72

4. N. Takahashi, Y. Orikasa and T. Yasiiima, Journal of Catalysis 50 (1979) 61


5. G. S. Nunes, I. Mayer, H.E. Toma, K. Araki, Journal of Catalysis 236 (2005) 55

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Lecture 34
Industrial homogeneous processes
Hydrogenation
Homogeneous hydrogenation is one of the earliest developed industrial homogeneous
processes.

The most effective homogeneous hydrogenation catalyst is Wilkinsons

catalyst having composition RhCl (PPh3)3 ,where PPh3 is tridentate phosphine ligand.
Both monomeric and dimer [Rh2Cl2(PPh3)4 ] forms are active catalyst. Since Rh can exist
in two oxidation states, it readily catalyzes oxidative addition and reductive elimination
reactions. The functional groups attached to the phosphine ligands also affect the
catalytic activity significantly. Activity is increased significantly by adding methoxy
group to the phosphine ligands.
In hydrogenation process, the first step is dissociation of one ligand L, which is replaced
by a solvent molecule. After ligand dissociation, oxidative addition reaction of H2 takes
place. This is followed by migration of hydride from metal to ethane, forming the ethyl
group. Finally, reductive elimination of ethane completes the cycle. The general reaction
sequence can be represented as follows :

RhClL3 + S RhClL2 S + L
RhClL2 S + H 2 RhH 2ClL2 S
=
RhH 2ClL2 S + H 2C CH 2 RhH 2ClL2 (C2 H 4 ) + S
RhH 2ClL2 (C2 H 4 ) + S RhH (C2 H 5 )ClL2 S
RhH (C2 H 5 )ClL2 S C2 H 6 + RhClL2 S
Here L=tri-arylphosphines ; S= solvent ( ethanol , toluene )
In general, homogeneous hydrogenation processes are industrially of less importance
compared to heterogeneous hydrogenation processes. However, interest is growing in
homogeneous hydrogenation processes particularly in the area of asymmetric
hydrogenation. In pharmaceutical industry, asymmetric hydrogenation is used to produce
enantiomerically pure compounds having desirable clinical properties. The main

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advantage of this process is the high selectivity, which eliminates the production of nondesired enantiomer which is non active or can cause undesirable side effects.
Example of asymmetric hydrogenation
1. Synthesis of L-dopa :
The asymmetric hydrogenation of cinnamic acid derivatives involves synthesis of LDopa. L-Dopa is a drug for treating Parkinsons disease. It is one of the recently
developed industrial processes. L-Dopa structure is shown below. The C atom bonded to
the NH2 group is the chiral center. The enantiomer D-Dopa is ineffective form.
CH 2

COOH
C

NH 2

HO
OH

The reaction is carried out in the presence of rhodium complex having asymmetric
diphosphine ligand which induces enantio-selectivity. The hydrogenation reaction is
carried out with a substituted cinnamic acid. The main step in L-Dopa synthesis, the
hydrogenation of prochiral alkene to a specific optical isomer, is shown below.
COOH
CH

CH 2

NHAc

H2

COOH
C
H

NHAc

AcO

AcO

OCH3

OCH 3

Fig. 1. Critical step in hydrogenation of prochiral alkene to specific enantiomer.

Catalyst is prepared by reacting Rh salt with an alkene chloride, such as hexadiene


chloride or cyclooctadiene chloride, producing a cationic Rh species.

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In the first step, alkene co-ordinates to rhodium species. The next step is hydrogenation
involving oxidative addition of hydrogen to the alkene complex. The oxidative addition
of hydrogen is irreversible and determines the enantioselectivity. Migration of hydride
locks the configuration of the enantiomeric center. In this system, the same
hydrogenation step determines the rate as well as selectivity.
The difference between this catalytic step and step involving Wilkinson catalyst lies in
the sequence of the oxidative addition and the alkene complexation. For rhodium
complex catalysts , the intermediate alkene complex has been spectroscopically observed.
Subsequently, oxidative addition of H2 and insertion of the alkene occurs, followed by
reductive elimination of the hydrogenation product.
Process
In a typical industrial process, the alcohol soluble catalyst along with soluble alkene
prochiral compound is introduced in an autoclave under reaction conditions of 50 0C and
3 atm H2. Since the products obtained are insoluble, separation is easier. The optical yield
is 95%.
Hydroformylation
The hydroformylation reaction involves conversion of alkene to aldehyde in the presence
of CO and hydrogen. The reaction is given as
O
R

H2 +

CO

Linear product

Branched product

The process is carried out over cobalt or rhodium complex based catalysts. Both linear
and branched chain products can be produced. Linear aldehydes are more valuable feed
stock for plasticizers and linear alcohols. Hence, the main objective is to have high
selectivity for more useful linear products.
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Cobalt complex catalysts


In cobalt complex catalyzed hydroformylation reaction, the catalytically active form is
HCo(CO)4 complex. The sequence of hydroformylation process for linear aldehyde
formation is shown below.

HCo ( CO )4 + CH 2 = CHR HCo(CH 2 =CHR) ( CO )3 + CO


HCo(CH 2 =CHR) ( CO )3 + CO Co(CH 2 CH 2 R) ( CO )4

Co(CH 2 CH 2 R) ( CO )4 + CO Co ( CO ) (CH 2 CH 2 R) ( CO )4

Co ( CO ) (CH 2 CH 2 R) ( CO )4 + H 2 CHO(CH 2 CH 2 R) + HCo ( CO )4


The first step is the replacement of CO ligand by an alkene. In the next step, hydride
migration to alkene occurs producing alkyl cobalt complex in which alkyl may be either
linear or branched. In the subsequent step, one incoming CO occupies the vacant site. It is
followed by migration of the alkyl to a co-ordinated CO to give an acyl-complex. In the
final step, dihydrogen reacts with acyl complex to form aldehyde product and regenerate
the starting hydrido-cobalt-carbonyl complex. In cobalt catalyzed hydroformylation, the
hydrogenation step is rate determining.
Phosphine modified Co catalysts
The performance of the cobalt complex is significantly modified when associated with
tertiary alkyl phosphines ligands. The selectivity to linear products is increased
significantly. But the reaction becomes slower, and as a result reaction needs to be
carried out at a higher temperature. The intermediate carbonyl complex formed is more
stable and hence the process can be carried out at lower pressure. In case of tetra cobalt
carbonyl complex HCo(CO)4 , high pressure is needed to prevent decomposition of
carbonyls to metal and CO. The phosphine complexed catalysts can also catalyze
hydrogenation and consequently cocurrent hydrogenation of aldehyde to alcohol, which
is usually the desired final form.

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Process
Hydroformylation of both higher and lower alkenes can be carried out using HCo(CO)3L
complex. Reaction is done in two stages as shown in Fig. 1, to limit the hydrogenation of
alkene. In the first reactor, low hydrogen partial pressure is used, and in the second
reactor high hydrogen partial pressure is used to ensure hydrogenation of aldehyde to
alcohol. The unreacted alkenes and gases are recycled back to the first reactor. Multiple
distillation columns are used to separate the unreacted reactants and catalysts. Catalysts
remain in the bottom phase of the distillation column and recycled back. The aldehydes
and alcohols are collected as overhead products from the distillation tower.

alkene

Heavy ends

Fig 1. Process flow diagram of hydroformylation process.

Rhodium complex catalysts


The rhodium complex catalysts contain triphenylphosphine ligand [P(C6H5)3 , TPP]
groups. The composition of rhodium complex catalysts is HRh(CO)(P(C6H5)3)3 . This
catalyst is highly active resulting in better utilization of feed stock. The most important
example of

industrial hydroformylation process is the synthesis of aldehydes,

particularly conversion of propylene to butylaldehyde. Rhodium complexes are the best


catalyst for low molecular weight alkene conversion however, cobalt complex catalysts
are better for conversion of high molecular weight alkenes.

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The overall reaction is given as :


CH 3CH= CH 2 + CO + H 2 nCH 3CH 2CH 2CHO + (1 n)CH 3CHCHOCH 3
linear

branched

The Rh complex catalyzed process is carried out at lower temperature and pressure of 80
-100 0C and 15-30 atm, respectively.
The catalyst is produced insitu from different starting materials such as Rh acetylacetate
carbonyl , CO, H2, TPP group. The HRh(CO)(P(C6H5)3)3 form gives 99 % selectivity
for linear aldehyde. At higher pressure , HRh(CO)3P(C6H5)3 species are formed that
favors the branched aldehyde which is an undesirable product. Hence, high CO partial
pressure is undesirable.
Moreover, at high partial pressure of CO, the reaction rate is inhibited by CO. On the
other hand, at very low partial pressures of CO, the concentration of active carbonyl as
well as CO reactant concentration are low, hence reaction rate is lowered. Rate of
hydroformylation is also dependent on phosphine concentration. At low TPP: Rh wt ratio,
the reaction rate increases with increasing concentration. However, at higher TPP:Rh wt
ratio, the rate decreases greatly with increasing TPP concentration. Hence, at high
concentration, TPP acts as inhibitor similar to CO.
In hydroformylation reaction, efficient mass transfer between gas (H2 and CO) and
organic liquid phase is obtained by gas liquid sparging and rapid stirring. Catalyst
separation is usually done by distillation. Product aldehydes are separated and Rh catalyst
remains in aqueous solution, which is recycled back to the reactor.
Rh complex catalysts can be deactivated by various ways. Free carboxylic acids,
produced as byproduct, can coordinate with Rh deactivating it. Further, traces of chlorine
or oxygen can also react with Rh decreasing its activity. When Rh catalysts are recovered
at the bottom of distillation column, some of the heavy high boiling products remain with
the catalyst, leading to faster deactivation. Rhodium is recovered from the deactivated
catalyst and used for new catalyst preparation.

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Carbonylation of methanol
Carbonylation of methanol produces acetic acid. Acetic acid is used in the production of
vinyl acetate, cellulose acetate, acetic anhydride, acetyl chloride and solvent acetates.
Reaction can be cobalt or rhodium complex catalyzed. The reaction is given as

CO + CH 3OH CH 3COOH
For cobalt carbonyl complex, catalytically active form is HCo(CO)4 . The cobalt
complex, CH3OH and CO are dissolved in a suitable solvent, such as butane, and reacted
to obtain acetic acid at 250 0C and 475 atm pressure. High pressure is required to dissolve
the CO and to stabilize the catalyst complex in the active form.
Rhodium catalysts involve milder conditions of 175 0C and 15-25 atm pressure which is
advantageous. Rhodium catalyzed process is used for large scale operation. The rhodium
precursors salt is RHI3 . The two catalysts components are rhodium and iodide. Under
reaction conditions, the CO and water reduce RhI3 to monovalent rhodium complex [Rh
(CO)2 I2 ]-1 which is the active form. In the presence of a large excess of iodide , methyl
iodide is formed. CH3I is reported to participate in the mechanism and the rate is
determined by the reaction of CH3I with Rh complex. The mechanism proposed is as
follows :

CH 3OH + HI CH 3 I + H 2O
CH 3 I + RhI 2 (CO) 2 CH 3 RhI 3 (CO) 2
CO + CH 3 RhI 3 (CO) 2 CH 3C (O) RhI 3 (CO) 2
CH 3C (O) RhI 3 (CO) 2 RhI 2 (CO) 2 + CH 3COI
CH 3COI + H 2O CH 3COOH + HI
The corresponding rate is given as r = kCRh complex CCH 3 I

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Fig 2. Process flow diagram for acetic acid production

Process
The flow diagram of the process is given in Fig 2. The liquid mixture from the reactor is
first depressurized. The separation of acetic acid from catalyst components is done by
distillation. In the first distillation column, the light ends are removed. In the second
distillation column, the acetic acid product is removed at the top and the heavy end at the
bottom, containing Rh catalysts, is recycled back to the reactor. Catalyst deactivation is
associated with high solution acidity caused by increasing free HI leading to formation of
an inactive complex [Rh(CO)2I4]-.
In this process, the following side reactions occur reducing the selectivity of the process.
i.

Water is essential for the reaction to occur ,but at high concentrations, it can react
with CO resulting in loss of one of the reactants.

CO + H 2O H 2 + CO 2
ii.

The other side reaction involves HI which oxidizes Rh(I) to Rh(III) iodide which
may precipitate from the reaction. It has to be converted back to Rh (I) complex.

CH3 Rh I3 (CO) 2 + HI CH 4 + Rh I 4 (CO) 2


Rh I 2 (CO) 2 + 2HI H 2 + Rh I 4 (CO) 2

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Text Reference

Piet W.N.M. van Leeuwen, Homogeneous catalysis: Understanding the Art,


Springer, 2004

Piet W.N.M. van Leeuwen, and John C. Chadwick, Homogeneous catalysis:


Activity-stability deactivation, Wiley, VCH, 2011

B. Cornils and W.A. Hermann (Ed.)

Applied homogeneous catalysis with

organometallic compounds, Wiley-VCH,2000

H. Bartholomew and R. J. Farrauto, Fundamentals of Industrial catalytic


Processes, Wiley, VCH, 2006

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Lecture 35
Enzyme catalytic processes
Enzyme catalytic processes are extensively used in food industries for centuries such as
in production of bread, beverages, yoghurt, cheese, vinegar etc. Enzymes have properties
similar to homogeneous catalysts. New enzymes are continuously being discovered. At
present, more than 3000 enzymes are reported.

Enzyme catalyst
Enzymes are large macromolecular polypeptide (polymers of amino acid monomers)
proteins. Molecular weight is in the range of 104-106 . Each enzyme has a unique threedimensional structure with a binding site or active site that is chemically and
geometrically compatible with a particular reactant molecule and thereby can give upto
100 % selectivity.
Enzymes are formed in living systems by condensation and/or dehydration of amino
acids that have the composition of H2N-CHR-COOH, to form peptide C-N bonds. Large
structure contains hundreds of amino acids and there is enormous number of possible
structures. Only few are characterized and well known. Naturally occurring metal ions in
enzymes reported are Mg, Zn, Ca, Ni, Fe, Co, Mo.
Example :
Lysozyme enzyme

Catalyze splitting of polysaccharide chains

129 amino acids residues joined by peptide linkage

Glutamic acid and aspartic acid are important functional groups at the
active sites

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Glutamic acid

Aspartic acid

Enzymes are synthesized by living organisms and can be extracted from their biological
source, purified and used in laboratory and industrial processes. Enzymes can also be
synthesized in vitro that is in an artificial environment outside the living organism.
Enzymes are only active within a limited range of pH and temperature.
Enzyme catalysis
Enzyme catalyze a variety of biological reactions such as :

Breakdown of proteins and sugars

Photosynthesis

Oxidation reduction that converts food to CO2, water and energy

Production of hormones

Enzymes are classified into six different groups based on the type of reactions catalyzed:
i.

Oxidoreductases : oxidation-reduction

ii.

Transferases : functional group transfer

iii.

Hydrolases : hydrolysis

iv.

Lyases : addition or formation of double bonds

v.

Isomerases : isomerization

vi.

Ligases : bond formations

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Activity
Enzymes generally function only under mild conditions of temperature and pH. Activity
of a typical enzyme increases with temperature upto 50-60

C passes through a

maximum and then declines. Enzymes catalyze biochemical reactions with very high
rates, 10-10000 molecules /enzyme/second compared to one or less for conventional
catalysts. High activity of enzyme is illustrated in Table 1
Table 1. Comparison of activation energies and relative rates of acid catalyzed and enzyme catalyzed hydrolysis reactions

Reactions

Hydrolysis

Activation energies

Relative rates

Conventional

Enzyme

Conventional

Enzyme

catalysis

catalysis

catalysis

catalysis

Urease

1012

of Acid catalyzed:

urea

104 kJ/mol

catalyzed : 29
kJ/mole

Selectivity of enzyme
Major advantage of enzymes is their selectivity. Enzymes are characterized by their
ability to catalyze biochemical reactions with high selectivity (essentially 100 %). Most
enzymes are only active for a single reaction i.e. stereochemical specificity of enzymes is
absolute. Three types of selectivity are exerted by enzymes :
1. Chemoselectivity
2. Regioselectivity
3. Stereoselectivity
1.Chemoselectivity
Enzyme can catalyze transformation of one type of functional group in the presence of
other sensitive groups in the substrate molecule . This reduces undesired reactions to a
great extent. The lipase of Burkholderia cepacia catalyzes acylation of 1-phenylethanol
hundred times faster than of the corresponding amine using methyl butyrate as acyl
donor.

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As shown in the figure, in a transacylation reaction , Burkholderia cepacia lipase ( Bcl)


prefer the alcohol over the amine as acyl acceptor by a factor of 100.
2. Regioselectivity
Enzymatic catalytic center has a complicated 3D structure that can distinguish between
two or more identical functional groups located in different sites of the substrate
molecule. As a result only one group participates in the reaction resulting in selective
products.
Example :
During deacylation of polyacylated sugar, high yield (80-90 %) of the product as shown
in following reaction is obtained. The other minor derivatives are products of deacylation
at other positions.
OH

OR
RO
RO

Lipase

RO
RO

O
OR

OR

OMe

OMe

R= COC4H9

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3. Stereoselectivity
Stereoisomers are defined as isomers of a substrate whose chemical compositions are
same but their structure differ such that their mirror images are non-superimposable.
Each one of the two stereoisomers is known as optical isomer or enantiomer. Production
of only one enantiomer with 100 % selectivity is important as activity depends on
stereochemistry. For the same substrate, one stereoisomer may be active while the other
stereoisomer may be inactive or active for an undesirable reaction. This enantioselectivity
is the most important feature of enzymes. Enzymes are capable of recognizing any type
of chirality of substrate and synthesizing one particular enatiomers. There are three
approaches to synthesis of enantiomerically enriched compounds using enzymes.
1. Kinetic resolution
2. Desymmetrization
3. Deracemization
R

fast

(S)

(P)

R, S = enntiomers of a racemic substrate


P , Q = enantiomers of a product

+
slow

(Q)

yield = 50% ( P ) ; 50% ( S )

Kinetic resolution of a racemic mixture rests upon chiral discrimination of enantiomers.


Each enantiomer is transformed into a product at a different rate. The theoretical yield is
then 50% of the product (P) and the unreacted substrate (S).
1. Desymmetrization
In desymmetrization process, a prochiral mesosubstrate is preferentially transformed into
one enantiomers of the product. In the ideal case, the yield of the product may be 100 %.

(P)
A
slow

P , Q enantiomers of a product
A prochiralor mesosubstate

yield = 100% ( P )

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2. Deracemization
Racemic mixture is defined as equal amounts of enantiomers of a chiral molecule. In this
process racemic substrate is transformed into one enantiomer of the product.

R, S = enntiomers of a racemic substrate


P = enantiomeric product
yield = 100% ( P )

retention
R
( P)

(S)

Kinetics

Inversion

Some functional groups on enzymes such as carboxylic COO- group can act as Bronsted
base. Some acidic functional groups are also proton donors. Proton bounded to one of the
functional groups result in most active enzyme form. The addition or removal of proton
to a critical functional group redistributes the charge on the active site and affects its
binding with the substrate. Accordingly, the rate of an enzymatic reaction is a strong
function of pH.
Most enzymes follow the kinetics proposed by Michaelis and Menten. Enzyme (E) and
substrate (S) first form an enzyme-substrate complex [ES], called the Michaelis-Menten
complex. The complex [ES] can then either dissociate back to substrate or cross the
energy barrier to form enzyme and product (P).
1

E + S
[ ES ]

k
E + P
[ ES ]

E = enzyme

; S = substrate; P=

product
The Michaelis-Menten equation gives the rate of formation of products as :

r k=
=
2 C ES
K
=
m

k2CE0 CS

( K m + CS )
( k1 + k2 ) / k1

Where CS is the concentration of substrate and CEO is the initial concentration of enzyme.

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Km is known as Michaelis constant. The rate law is derived from following basic
assumptions:
1. The first step of binding of substrate to enzyme is faster compared to second step
of dissociation of enzyme-substrate complex [ES] to products. Hence 2nd step is
the rate determining step.
2. At initial stages of reaction, concentration of product is assumed to be zero.
3. At steady state, the concentration of the intermediate ES is constant.
Rate of formation of product P is given as

=
r k2CES k2CE CP -------------(1)
At initial stage of reaction, concentration of product, CP = 0
Hence,

r = k2CES ------------- (2)


Now at steady state condition,
Rate of formation of [ES] = Rate of breakdown of [ES]

k1CE CS + k2CE CP =
k1CES + k2CES
Substituting CP = 0

k1C
=
k1CES + k2CES
E CS
Or CES
=

C E CS
k1
-----------------(3)
=
C E CS
k1 + k2
Km

where K m =

k1 + k2
k1

The ratio of rate constants, Km is known as Michaelis constant.


Substituting concentration CES from equation (3) in equation (2), rate expression is
obtained as

=
r k=
k2
2C ES

C E CS
----------------(4)
Km

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The total concentration of enzyme is summation of concentration of free enzyme CE and


concentration of enzyme bound to substrate CES. Hence total concentration of enzyme CE0
is given as

CE=
CE + CES
0
Substituting value of CES from equation (3) we obtain

CE 0 =
CE +

Or CE =

C
C E CS
=
CE 1 + S
Km
Km

CES =

C E CS
Km

CE 0

CS
1 +

Km

Substituting CE in equation (4)

k 2 CS
k 2CS C E 0
k C K mCE 0
=
CE
= 2 S

Km
K m CS K m ( K m + CS )
1 +

Km

=
r k=
2 C ES

Or r =

k 2 C E 0 CS
( K m + CS )

The rate expression is often referred as Michaelis-Menten rate law. This is valid for many
enzyme reactions at constant pH.
Stability & deactivation
If exposed to severe conditions of temperature and pH, enzyme catalysts can undergo

Loss or modification of functional groups or amino acid residues

Change in conformations which alter and deactivate the site

The deactivation rate is extremely high with slight increases in temperature for e.g 50%
loss of activity in 5 min at 65-70

C. Because of their high deactivation, enzymes are

shipped and stored under refrigeration (0 - 4 0C). Some enzymes are active and stable at
higher temperature. The -amylase catalyzes starch liquefaction at 105-115 deg 0C.
Catalysts stability can be improved by the following methods:
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Immobilizing enzymes on inert support

Covalent binding to a support

Adsorption on solid surface

Entrapment in gel

Immobilization of enzymes also facilitates recovery of the catalysts.


Enzyme catalysts : limitations
Major limitations for industrial applications are :
1.

Expense of isolating and purifying the catalysts

2.

Lack of stability when removed from cell or living extra-cellular environment

3.

Difficulty and expense of separation in batch operations

Second and third difficulties can be reduced by immobilized enzyme technology


mentioned above. Separation of enzymes from the product is difficult, expensive and can
cause deactivation.
Industrial bio-catalytic process
Over 300 enzymes are available commercially. About 20 of these enzymes are used in
large and moderately large scale production of chemicals, food products and
pharmaceuticals. Enzymes used in largest quantities include amylase, glucoamylase,
glucose isomerase, lipase, prolease and rennet. Applications of these include starch
processing, production of detergents, beverage, milk products and medicine.

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Table 2 : Examples of different types of enzymes used in industry

Enzyme type

Enzyme

applications

Oxidoreductase

catalase

sterilization of milk

glucose oxidase

removal of glucose from


food

lipoxidase

bleach in white bread

peroxidase

paper manufacturing

and amylase

brewing

cellulase

wine making

glucoamylase

starch processing

penicillin amidase

antibiotics

keratinase

leather manufacturing

Lyase

fumerate hydratase

malic acid

Isomerase

glucose isomerase

fructose syrup production

Hydrolase

Example of industrial processes


1.

Glucose isomerization

Glucose is produced from starch using glucoamylase catalyst. The conversion of glucose
to its sweeter form , fructose, is an important enzymatic process. For this reaction,
conventional acid base catalysis is ineffective. This can be done using glucose
isomerase catalysts. It is the largest commercial application of immobilized enzymes.

Commercial glucose isomerase catalysts are produced from : Actinoplanes missouriensis,


Bacillus coagulans, Flavobacterium aborescens
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Commercial immobilized form of the catalyst is relatively insensitive to temperature and


is effective at high substrate concentration. They require Co2+, Mn2+ or Mg2+ cofactors
and are inhibited by Ca2+, Cu2+, Zn2+, and Hg2+ as well as sugar alcohols such as sorbitol
and xylitor.
Reported immobilization methods include :
1. Occlusion in gelatin followed by crosslinking with glutaraldehyde
2. Adsorption of purified enzyme on silica followed by crosslinking with
glutaraldehyde
3. Binding with polystyrene or resin
However, the third method has been less successful as the catalyst is distorted during
processing. Immobilized catalyst forms are granulated to particle size of 0.1 -1.5 mm.

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Process
The process is carried out in continuous flow fixed bed reactors at 55-60 0C temperature.
The pH is maintained at 7.5 to 8 by adding Na2CO3. MgSO4 is added as catalyst
activator and also helps to adjust the pH. Multiple reactors are used to control the product
quality. The catalyst has a half-life of 50-175 years at 55 0C. The schematics in Fig. 1
shows the major steps involved in glucose isomerise process.

Filter removes the

materials that can plug the catalysts pores. Carbon adsorbent bed is used to remove the
impurities that can poison the catalysts. The feed evaporator concentrate the feed to 35-45
%.

Fig.1.

Schematics showing major steps in glucose isomerise process

2. Chiral synthesis of L-aspartic acid


L-aspartic acid is widely used in food and pharmaceutical industries, for example in
production of low calorific sweetener aspartame and in treatment of leukemia. It is
produced by the reaction of fumaric acid with ammonia over L-aspartase

HOOC CH = CH COOH + NH 3 HOOC CH 2 CH ( NH 2 ) COOH

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Isolated enzymes are highly unstable. It is prepared by trapping E.colli cell in matrix of
polyacryl amide or poly urethane. The immobilized cells are very active at 35-40 0C
achieving 95% conversion. The half-life of these immobilized cells is 120-680 days.
Reaction is conducted in a column reactor at 37 0C at pH 8.5 using a feed of ammonium
fumarate. MgCl2 is added for catalyst stability.
3. Enzymatic hydrolysis : production of 6 aminopenicillanic acid (6-APA)
The 6 aminopenicillanic acid is produced by penicillin-acylase catalyzed acetal
hydrolysis of penicillins G and U. It is used to produce a large family of highly effective
antibiotics such as ampicillin and amoxicillin. Acylase catalyzed hydrolysis of penicillin
G involves the removal of the phenyacetyl side chain to produce phenylacetic acid and 6APA as shown below.

NH2
CH2

CO

NH

CH 3
CH3

H 2O

CH 2

COOH

CH 3

+
N

COOH

N
COOH
O

Penicillin G

Phenylacetic acid

6-APA

Reaction occurs at 35 0C at pH 7-8. The pencillin acylase can be obtained from bacterial
and fungal organisms. Bacterial acylase are best for penicillin G and fungal acylase
most active for penicillin U.
Production of 6-APA is conducted in a stirred batch reactor or continuous stirred tank
reactor (CSTR) at 35-40 0C and 7-8 pH using a feed of 4-15 wt% penicillin G. The pH of
the reactor is controlled at 7-8 by continuous addition of alkali to compensate for
production of phenylacetic acid.

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CH3

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Text reference

Piet W.N.M. van Leeuwen, Homogeneous catalysis: Understanding the Art,


Springer, 2004

Piet W.N.M. van Leeuwen, and John C. Chadwick, Homogeneous catalysis:


Activity-stability deactivation, Wiley, VCH, 2011

H. Bartholomew and R. J. Farrauto, Fundamentals of Industrial catalytic


Processes, Wiley, VCH, 2006

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