Frontiers in Molecular Biosciences,
Journal Year:
2022,
Volume and Issue:
9
Published: July 22, 2022
The
discovery
of
new
enzymes,
alongside
the
push
to
make
chemical
processes
more
sustainable,
has
resulted
in
increased
industrial
interest
use
biocatalytic
produce
high-value
and
chiral
precursor
chemicals.
Huge
strides
protein
engineering
methodology
silico
tools
have
facilitated
significant
progress
production
enzymes
for
processes.
However,
there
are
gaps
our
knowledge
relationship
between
enzyme
structure
function.
This
demonstrated
need
improved
computational
methods
model
mechanisms
understand
dynamics.
Here,
we
explore
efforts
rationally
modify
toward
changing
aspects
their
catalyzed
chemistry.
We
highlight
examples
where
links
function
been
made,
thus
enabling
rational
changes
give
predictable
outcomes.
look
at
future
directions
field
could
take
technologies
that
will
enable
it.
ChemSusChem,
Journal Year:
2022,
Volume and Issue:
15(9)
Published: March 3, 2022
The
role
and
power
of
biocatalysis
in
sustainable
chemistry
has
been
continuously
brought
forward
step
by
to
its
present
outstanding
position.
problem-solving
capabilities
have
realized
numerous
substantial
achievements
biology,
engineering.
Advances
breakthroughs
the
life
sciences
interdisciplinary
cooperation
with
clearly
accelerated
implementation
biocatalytic
synthesis
modern
chemistry.
Resource-efficient
manufacturing
processes
already
provided
benefits
as
well
customer-centric
value
creation
pharmaceutical,
food,
flavor,
fragrance,
vitamin,
agrochemical,
polymer,
specialty,
fine
chemical
industries.
Biocatalysis
can
make
significant
contributions
not
only
processes,
but
also
design
completely
new
value-creation
chains.
now
be
considered
a
key
enabling
technology
implement
Journal of the American Chemical Society,
Journal Year:
2021,
Volume and Issue:
144(1), P. 80 - 85
Published: Dec. 23, 2021
Propargyl
amines
are
versatile
synthetic
intermediates
with
numerous
applications
in
the
pharmaceutical
industry.
An
attractive
strategy
for
efficient
preparation
of
these
compounds
is
nitrene
propargylic
C(sp3)–H
insertion.
However,
achieving
this
reaction
good
chemo-,
regio-,
and
enantioselective
control
has
proven
to
be
challenging.
Here,
we
report
an
enzymatic
platform
amination
alkynes
using
a
hydroxylamine
derivative
as
precursor.
Cytochrome
P450
variant
PA-G8
catalyzing
transformation
was
identified
after
eight
rounds
directed
evolution.
A
variety
1-aryl-2-alkyl
accepted
by
PA-G8,
including
those
bearing
heteroaromatic
rings.
This
biocatalytic
process
selective
(up
2610
total
turnover
number
(TTN)
96%
ee)
can
performed
on
preparative
scale.
Journal of the American Chemical Society,
Journal Year:
2022,
Volume and Issue:
144(6), P. 2590 - 2602
Published: Feb. 2, 2022
The
biocatalytic
toolbox
has
recently
been
expanded
to
include
enzyme-catalyzed
carbene
transfer
reactions
not
occurring
in
Nature.
Herein,
we
report
the
development
of
a
strategy
for
synthesis
enantioenriched
α-trifluoromethyl
amines
through
an
asymmetric
N-H
insertion
reaction
catalyzed
by
engineered
variants
cytochrome
c552
from
Hydrogenobacter
thermophilus.
Using
combination
protein
and
substrate
engineering,
this
metalloprotein
scaffold
was
redesigned
enable
chiral
amino
esters
with
up
>99%
yield
95:5
er
using
benzyl
2-diazotrifluoropropanoate
as
donor.
When
diazo
reagent
varied,
enantioselectivity
enzyme
could
be
inverted
produce
opposite
enantiomers
these
products
99.5:0.5
er.
This
methodology
is
applicable
broad
range
aryl
amine
substrates,
it
can
leveraged
obtain
chemoenzymatic
access
β-trifluoromethyl-β-amino
alcohols
halides.
Computational
analyses
provide
insights
into
interplay
protein-
reagent-mediated
control
on
reaction.
work
introduces
first
example
carbenoid
acceptor-acceptor
donor,
offers
solution
enantioselective
α-trifluoromethylated
valuable
synthons
medicinal
chemistry
bioactive
molecules.
Journal of the American Chemical Society,
Journal Year:
2022,
Volume and Issue:
144(11), P. 4739 - 4745
Published: March 8, 2022
We
report
enantioselective
one-carbon
ring
expansion
of
aziridines
to
make
azetidines
as
a
new-to-nature
activity
engineered
"carbene
transferase"
enzymes.
A
laboratory-evolved
variant
cytochrome
P450BM3,
P411-AzetS,
not
only
exerts
unparalleled
stereocontrol
(99:1
er)
over
[1,2]-Stevens
rearrangement
but
also
overrides
the
inherent
reactivity
aziridinium
ylides,
cheletropic
extrusion
olefins,
perform
rearrangement.
By
controlling
fate
highly
reactive
ylide
intermediates,
these
evolvable
biocatalysts
promote
transformation
which
cannot
currently
be
performed
using
other
catalyst
classes.
Chemical Reviews,
Journal Year:
2023,
Volume and Issue:
123(6), P. 2832 - 2901
Published: Feb. 28, 2023
Many
successful
stories
in
enzyme
engineering
are
based
on
the
creation
of
randomized
diversity
large
mutant
libraries,
containing
millions
to
billions
variants.
Methods
that
enabled
their
evaluation
with
high
throughput
dominated
by
spectroscopic
techniques
due
speed
and
sensitivity.
A
proportion
studies
relies
fluorogenic
substrates
mimic
chemical
properties
target
or
coupled
enzymatic
assays
an
optical
read-out
assesses
desired
catalytic
efficiency
indirectly.
The
most
reliable
hits,
however,
achieved
screening
for
conversions
starting
material
product.
For
this
purpose,
functional
group
offer
a
general
approach
achieve
fast,
read-out.
They
use
chemoselectivity,
differences
electronic
steric
various
groups,
reduce
number
false-positive
results
analytical
noise
stemming
from
background
activities.
This
review
summarizes
developments
probes
chemoselective
derivatizations,
clear
focus
activity
protein
engineering.
Journal of the American Chemical Society,
Journal Year:
2024,
Volume and Issue:
146(12), P. 7876 - 7884
Published: March 15, 2024
Biocatalysis
is
becoming
an
indispensable
tool
in
organic
synthesis
due
to
high
enzymatic
catalytic
efficiency
as
well
exquisite
chemo-
and
stereoselectivity.
Some
biocatalysts
display
great
promiscuity
including
a
broad
substrate
scope
the
ability
catalyze
more
than
one
type
of
transformation.
These
promiscuous
activities
have
been
applied
individually
efficiently
access
numerous
valuable
target
molecules.
However,
systems
which
enzymes
possessing
multiple
different
are
less
developed.
Such
multifunctional
(MFBs)
would
simplify
chemical
by
reducing
number
operational
steps
enzyme
count,
simplifying
sequence
space
that
needs
be
engineered
develop
efficient
biocatalyst.
In
this
Perspective,
we
highlight
recently
reported
MFBs
focusing
on
their
synthetic
utility
mechanism.
We
also
offer
insight
into
origin
comment
potential
strategies
for
discovery
engineering.
