Advanced Synthesis & Catalysis,
Journal Year:
2022,
Volume and Issue:
364(8), P. 1488 - 1497
Published: March 1, 2022
Abstract
A
selective
Pd‐catalyzed
C(3)−H
cis
‐functionalization
of
piperidine
and
tetrahydropyran
carboxylic
acids
is
achieved
using
a
C(4)
aminoquinoline
amide
auxiliary.
High
mono‐
‐selectivity
attained
by
mesityl
acid
as
an
additive.
Conditions
are
developed
with
significantly
lower
reaction
temperatures
(≤50
°C)
than
other
reported
heterocycle
C(
sp
3
)−H
functionalization
reactions,
which
facilitated
DoE
optimization.
one‐pot
C−H
functionalization‐epimerization
procedure
provides
the
trans
‐3,4‐disubstituted
isomers
directly.
Divergent
removal
accomplished
installation
acid,
alcohol,
nitrile
functional
groups.
Overall,
fragment
compounds
suitable
for
screening
generated
in
3–4
steps
from
readily‐available
heterocyclic
acids.
magnified
image
Chemical Reviews,
Journal Year:
2018,
Volume and Issue:
119(3), P. 1855 - 1969
Published: Dec. 24, 2018
In
this
review,
we
summarize
the
origin
and
advancements
of
iridium-catalyzed
asymmetric
allylic
substitution
reactions
during
past
two
decades.
Since
first
report
in
1997,
Ir-catalyzed
have
attracted
intense
attention
due
to
their
exceptionally
high
regio-
enantioselectivities.
been
significantly
developed
recent
years
many
respects,
including
ligand
development,
mechanistic
understanding,
substrate
scope,
application
synthesis
complex
functional
molecules.
an
explicit
outline
ligands,
mechanism,
scope
nucleophiles,
applications
is
presented.
Accounts of Chemical Research,
Journal Year:
2019,
Volume and Issue:
52(9), P. 2657 - 2672
Published: June 19, 2019
ConspectusThe
catalytic,
asymmetric
synthesis
of
complex
molecules
has
been
a
core
focus
our
research
program
for
some
time
because
developments
in
the
area
can
have
an
immediate
impact
on
identification
novel
strategies
value-added
molecules.
In
concert
with
this
central
interest,
we
emphasized
design
ligand
scaffolds
as
tactic
to
discover
and
develop
chemistry
overcome
well-recognized
synthetic
challenges.
Based
group's
work
chiral
pool-derived
diolefin
ligands,
designed
implemented
class
hybrid
(phosphoramidite,olefin)
which
combines
properties
both
phosphoramidite
olefin
motifs
impact,
fine-tune,
even
override
inherent
reactivity
metal
center.
Specifically,
utilized
these
unique
modifying
ligands
address
several
recognized
limitations
field
iridium-catalyzed,
allylic
substitution.
The
methods
documented
typically
employ
branched,
unprotected
alcohols
substrates
obviate
need
rigorous
exclusion
air
moisture.Following
Takeuchi's
seminal
report
demonstrating
high
aptitude
Ir(I)-phosphite
catalysts
branch-selective
substitution,
concerted
efforts
from
numerous
laboratories
led
broadening
utility
reaction
class.
first
section
Account
outlines
process
leading
discovery
unprecedented
its
validation
iridium-catalyzed
amination
alcohols.
This
continues
involving
heteroatom-based
nucleophiles
within
inter-
intramolecular
etherification,
thioetherification
spiroketalization
processes.
second
highlights
use
readily
available
carbon
possessing
sp,
sp2,
sp3
hybridization
series
enantioselective
carbon–carbon
bond-forming
reactions.
We
describe
how
alkylzinc,
allylsilane,
classes
organotrifluoroborate
be
coupled
enantioselectively
enable
construction
key
including
1,5-dienes,
1,4-dienes,
1,4-enynes.
Since
electronic
steric
renders
(η3-allyl)-Ir(III)
intermediate
highly
electrophilic,
weak
such
alkyl
olefins
used.
also
show
that
more
nucleophilic
alkene
enamines
situ
generated
ketene
acetals
smoothly
participate
substitution
reactions
yield
valuable
piperidines
γ,δ-unsaturated
esters,
respectively.The
concept
stereodivergent
dual
catalysis,
synergistically
amine
catalysis
iridium
furnish
α-allylated
aldehydes
containing
two
independently
controllable
stereocenters
is
then
discussed.
enabled
independent,
stereoselective
all
four
possible
product
stereoisomers
single
set
starting
materials,
was
highlighted
Δ9-tetrahydrocannabinol.
concludes
overview
organometallic
mechanistic
studies
regarding
relevant
intermediates
catalytic
cycle
These
allowed
us
better
understand
origin
characteristics
exhibited
by
catalyst
comparison
related
systems.
Journal of the American Chemical Society,
Journal Year:
2018,
Volume and Issue:
140(6), P. 2080 - 2084
Published: Jan. 30, 2018
We
describe
a
fully
stereodivergent
synthesis
of
range
α,α-disubstituted
α-amino
acids
via
an
Ir/Cu-catalyzed
α-allylation
readily
available
imine
esters.
The
introduction
Cu-Phox
complex-activated
ester
into
the
chiral
iridium-catalyzed
allylic
allylation
process
is
crucial
for
its
high
reactivity
and
excellent
enantio-
diastereoselectivity
(up
to
>99%
ee
>20:1
dr).
Importantly,
two
catalysts
allow
full
control
over
configuration
stereocenters,
affording
all
stereoisomers
desired
products.
utility
this
methodology
was
demonstrated
by
synthesizing
dipeptides
analogues
bioactive
molecules
in
manner.
Journal of the American Chemical Society,
Journal Year:
2018,
Volume and Issue:
140(4), P. 1239 - 1242
Published: Jan. 10, 2018
We
report
stereodivergent
allylic
substitution
reactions
of
esters
with
prochiral
enolates
derived
from
azaaryl
acetamides
and
acetates
to
form
products
addition
the
at
most
substituted
carbon
an
allyl
moiety
two
catalysts,
a
chiral
metallacyclic
iridium
complex
bisphosphine-ligated
copper(I)
complex,
which
individually
control
configuration
electrophilic
nucleophilic
atoms,
respectively.
By
simple
permutations
enantiomers
all
four
stereoisomers
containing
stereogenic
centers
were
synthesized
high
diastereoselectivity
enantioselectivity.
A
variety
bearing
pyridyl,
benzothiazolyl,
benzoxazolyl,
pyrazinyl,
quinolinyl
isoquinolinyl
moieties
found
be
suitable
for
this
transformation.
Nature Communications,
Journal Year:
2019,
Volume and Issue:
10(1)
Published: June 20, 2019
Abstract
Catalytic
asymmetric
cycloadditions
via
transition-metal-containing
dipolar
intermediates
are
a
powerful
tool
for
synthesizing
chiral
heterocycles.
However,
within
the
field
of
palladium
catalysis,
compared
with
well-developed
normal
electron-demand
electrophilic
dipolarophiles,
general
strategy
inverse
ones
nucleophilic
dipolarophiles
remains
elusive,
due
to
inherent
linear
selectivity
in
key
palladium-catalyzed
intermolecular
allylations.
Herein,
based
on
switched
regioselectivity
iridium-catalyzed
allylations,
we
achieved
two
[4+2]
vinyl
aminoalcohols
aldehydes
and
β,γ-unsaturated
ketones
through
synergetic
iridium
amine
catalysis.
The
activation
by
catalysts
carbonyls
provide
foundation
subsequent
resulting
iridium-containing
1,4-dipoles
(di)enamine
dipolarophiles.
former
provides
straightforward
route
diverse
set
enantio-enriched
hydroquinolines
bearing
quaternary
stereocenters,
later
represent
an
enantio-
diastereodivergent
synthesis
hydroquinolines.
Angewandte Chemie International Edition,
Journal Year:
2019,
Volume and Issue:
59(5), P. 2039 - 2043
Published: Nov. 6, 2019
Abstract
The
stereodivergent
iridium‐catalyzed
allylic
alkylation
and
fluorination
of
acyclic
ketones
is
described.
α‐Pyridyl‐α‐fluoroketones
with
vicinal
tertiary
quaternary
stereocenters
were
obtained
in
moderate
to
excellent
yields
stereoselectivities.
Distinct
from
known
synthesis,
for
which
two
different
chiral
catalysts
are
required
general,
herein
we
report
a
sequence‐dependent
synthesis.
With
only
single
Ir
catalyst,
all
four
possible
stereoisomers
the
products
prepared
same
starting
materials
by
simply
adjusting
sequence
asymmetric
varying
absolute
configuration
catalyst.
Angewandte Chemie International Edition,
Journal Year:
2018,
Volume and Issue:
57(39), P. 12930 - 12934
Published: July 2, 2018
We
report
the
successful
generation
of
(diborylmethyl)zinc(II)
species
by
transmetallation
beteween
isolable
(diborylmethyl)lithium
and
zinc(II)
halide
(X=Br,
Cl)
their
application
in
synthesis
enantioenriched
gem-diborylalkanes
bearing
a
stereogenic
center
at
β-position
diboryl
groups
an
asymmetric
allylic
substitution
reaction.
The
reaction
has
broad
substrate
scope,
various
can
be
obtained
good
yields
with
excellent
enantioselectivity.
Further
elaboration
provides
access
to
diverse
set
valuable
chiral
building
blocks.
Organic Letters,
Journal Year:
2017,
Volume and Issue:
19(20), P. 5513 - 5516
Published: Oct. 6, 2017
A
one-step
enantioselective
and
diastereodivergent
α-allylation
of
unprotected
α-hydroxy
indanones
has
been
developed
using
an
Ir/Zn
dual
catalyst
system;
no
additional
base
is
required.
The
cyclic
tertiary
α-hydroxyketones
containing
vicinal
stereocenters
can
be
synthesized
with
excellent
enantioselectivity
(up
to
>99%
ee)
good
diastereoselectivity
12:1
dr).
By
a
simple
choice
the
appropriate
chiral
metal
combination,
all
four
product
stereoisomers
could
obtained
from
same
starting
materials
under
identical
conditions.
Journal of the American Chemical Society,
Journal Year:
2019,
Volume and Issue:
141(11), P. 4738 - 4748
Published: Feb. 20, 2019
The
inherent
difficulty
in
eliciting
facial
control
over
carbocations
has
limited
their
utility
as
intermediates
asymmetric
catalysis.
We
have
now
shown
that
a
docking
strategy
involving
the
reversible
coordination
of
substrate
to
chiral
transition-metal
catalyst
can
be
used
enable
highly
stereoselective
nucleophilic
attack
on
intermediate
tertiary
carbocations.
This
approach
been
implemented
achieve
first
example
enantioselective
reductive
deoxygenation
alcohols.
reduction
occurs
with
high
enantio-
(up
96%
ee)
and
regioselectivity
>50:1
rr)
by
applying
novel
Hantzsch
ester
analogue
convenient
hydride
source.
In-depth
mechanistic
studies
support
involvement
carbocation
is
coordinated
iridium
metal
center
via
key
allene
moiety.
Journal of the American Chemical Society,
Journal Year:
2019,
Volume and Issue:
141(6), P. 2228 - 2232
Published: Jan. 28, 2019
Ketones
and
aldehydes
are
employed
as
enol
O-nucleophiles
in
an
iridium-catalyzed
asymmetric
allylic
substitution
reaction.
The
reaction
proceeds
well
the
presence
of
a
well-defined
chiral
iridium
complex
under
mild
conditions.
A
series
2H-1,4-oxazine
skeletons
can
be
obtained
up
to
94%
yield
with
99%
ee.
utility
this
novel
method
has
been
demonstrated
by
its
implementation
first
enantioselective
synthesis
(+)-chelonin
A.
