Angewandte Chemie International Edition,
Journal Year:
2024,
Volume and Issue:
63(32)
Published: May 24, 2024
Abstract
Synthesis
of
bicyclic
scaffolds
has
gained
significant
attention
in
drug
discovery
due
to
their
potential
mimic
benzene
bioisosteres.
Here,
we
present
a
mild
and
scalable
Sc(OTf)
3
‐catalyzed
[3+2]
cycloaddition
bicyclo[1.1.0]butanes
(BCBs)
with
ynamides,
yielding
diverse
array
polysubstituted
2‐amino‐bicyclo[2.1.1]hexenes
good
excellent
yields.
These
products
offer
valuable
starting
materials
for
the
construction
novel
functionalized
bicyclo[1.1.0]butanes.
Preliminary
mechanistic
studies
indicate
that
reaction
involves
nucleophilic
addition
ynamides
bicyclo[1.1.0]butanes,
followed
by
an
intramolecular
cyclization
situ
generated
enolate
keteniminium
ion.
We
expect
these
findings
will
encourage
utilization
complex
bioisosteres
foster
further
investigation
into
BCB‐based
chemistry.
Journal of Agricultural and Food Chemistry,
Journal Year:
2023,
Volume and Issue:
71(47), P. 18087 - 18122
Published: March 24, 2023
The
design
of
bioisosteres
represents
a
creative
and
productive
approach
to
improve
molecule,
including
by
enhancing
potency,
addressing
pharmacokinetic
challenges,
reducing
off-target
liabilities,
productively
modulating
physicochemical
properties.
Bioisosterism
is
principle
exploited
in
the
bioactive
compounds
interest
both
medicinal
agricultural
chemists,
this
review,
we
provide
synopsis
applications
where
kind
molecular
editing
has
proved
be
advantageous
molecule
optimization.
examples
selected
for
discussion
focus
on
carboxylic
acids,
fluorine
fluorinated
motifs
compound
design,
some
sulfoximine
functionality,
drug-H2O
complexes,
phenyl
ring.
Journal of the American Chemical Society,
Journal Year:
2024,
Volume and Issue:
146(4), P. 2789 - 2797
Published: Jan. 18, 2024
Dearomative
photocycloaddition
of
monocyclic
arenes
is
an
appealing
strategy
for
comprehending
the
concept
"escape
from
flatland".
This
brings
replacement
readily
available
planar
aromatic
hydrocarbon
units
with
a
3D
fused
bicyclic
core
sp3-enriched
carbon
units.
Herein,
we
outline
intermolecular
approach
dearomative
phenols.
In
order
to
circumvent
ground-state
aromaticity
and
construct
conformationally
restrained
building
blocks,
bicyclo[1.1.0]butanes
were
chosen
as
coupling
partners.
renders
straightforward
access
bicyclo[2.1.1]hexane
unit
cyclic
enone
moiety,
which
further
contributed
synthetic
linchpin
postmodifications.
Mechanistic
experiment
advocates
plausible
onset
both
reactants,
depending
on
redox
potential.
Journal of Medicinal Chemistry,
Journal Year:
2024,
Volume and Issue:
67(10), P. 7668 - 7758
Published: May 7, 2024
Covalent
inhibitors
and
other
types
of
covalent
modalities
have
seen
a
revival
in
the
past
two
decades,
with
variety
new
targeted
drugs
having
been
approved
recent
years.
A
key
feature
such
molecules
is
an
intrinsically
reactive
group,
typically
weak
electrophile,
which
enables
irreversible
or
reversible
formation
bond
specific
amino
acid
target
protein.
This
often
called
"warhead",
critical
determinant
ligand's
activity,
selectivity,
general
biological
properties.
In
2019,
we
summarized
emerging
re-emerging
warhead
chemistries
to
cysteine
acids
(Gehringer,
M.;
Laufer,
S.
A.
J.
Med.
Chem.
62,
5673−5724;
DOI:
10.1021/acs.jmedchem.8b01153).
Since
then,
field
has
rapidly
evolved.
Here
discuss
progress
on
warheads
made
since
our
last
Perspective
their
application
medicinal
chemistry
chemical
biology.
Angewandte Chemie International Edition,
Journal Year:
2024,
Volume and Issue:
63(13)
Published: Jan. 30, 2024
Abstract
Herein,
we
have
synthesized
multifunctionalized
2‐oxa‐3‐azabicyclo[3.1.1]heptanes,
which
are
considered
potential
bioisosteres
for
meta
‐substituted
arenes,
through
Eu(OTf)
3
‐catalyzed
formal
dipolar
[4π+2σ]
cycloaddition
of
bicyclo[1.1.0]butanes
with
nitrones.
This
methodology
represents
the
initial
instance
fabricating
bicyclo[3.1.1]heptanes
adorned
multiple
heteroatoms.
The
protocol
exhibits
both
mild
reaction
conditions
and
a
good
tolerance
various
functional
groups.
Computational
density
theory
calculations
support
that
mechanism
likely
involves
nucleophilic
addition
nitrones
to
bicyclo[1.1.0]butanes,
succeeded
by
an
intramolecular
cyclization.
synthetic
utility
this
novel
has
been
demonstrated
in
concise
synthesis
analogue
Rupatadine.
Chemistry - A European Journal,
Journal Year:
2023,
Volume and Issue:
29(29)
Published: Feb. 14, 2023
The
use
of
metalated
(aza)bicyclo[1.1.0]butanes
in
synthesis
is
currently
experiencing
a
renaissance,
as
evidenced
by
the
numerous
reports
last
5
years
that
have
relied
on
such
intermediates
to
undergo
unique
transformations
or
generate
novel
fragments.
Since
their
discovery,
these
species
been
demonstrated
participate
wide
range
reactions
with
carbon
and
heteroatom
electrophiles,
well
metal
complexes,
facilitate
rapid
diversification
(aza)bicyclo[1.1.0]butane-containing
compounds.
Key
this
relative
acidity
bridgehead
C-H
bonds
which
promotes
facile
deprotonation
subsequent
functionalization
an
unsubstituted
position
framework
via
intermediacy
(aza)bicyclo[1.1.0]butane.
Additionally,
late-stage
incorporation
deuterium
atoms
strained
fragments
has
led
elucidation
reaction
mechanisms
involve
bicycles.
continued
investigation
into
inimitable
reactivity
bicycles
will
cement
importance
within
field
organometallic
chemistry.
Journal of the American Chemical Society,
Journal Year:
2024,
Volume and Issue:
146(29), P. 19621 - 19628
Published: May 13, 2024
For
nearly
60
years,
significant
research
efforts
have
been
focused
on
developing
strategies
for
the
cycloaddition
of
bicyclobutanes
(BCBs).
However,
higher-order
and
catalytic
asymmetric
BCBs
long-standing
formidable
challenges.
Here,
we
report
Pd-catalyzed
ligand-controlled,
tunable
cycloadditions
divergent
synthesis
bridged
bicyclic
frameworks.
The
dppb
ligand
facilitates
formal
(5+3)
vinyl
oxiranes,
yielding
valuable
eight-membered
ethers
with
scaffolds
in
100%
regioselectivity.
Cy-DPEphos
promotes
selective
hetero-[2σ+2σ]
to
access
pharmacologically
important
2-oxabicyclo[3.1.1]heptane
(O-BCHeps).
Furthermore,
corresponding
O-BCHeps
94–99%
ee
has
achieved
using
chiral
(S)-DTBM-Segphos,
representing
first
cross-dimerization
two
strained
rings.
obtained
are
promising
bioisosteres
ortho-substituted
benzenes.
Chemical Science,
Journal Year:
2023,
Volume and Issue:
14(36), P. 9696 - 9703
Published: Jan. 1, 2023
Ring-opening
of
bicyclo[1.1.0]butanes
(BCBs)
is
emerging
as
a
powerful
strategy
for
1,3-difunctionalized
cyclobutane
synthesis.
However,
reported
radical
strain-release
reactions
are
typically
plagued
with
diastereoselectivity
issues.
Herein,
an
atom-economic
protocol
the
highly
chemo-
and
diastereoselective
polar
ring-opening
BCBs
hydroxyarenes
catalyzed
by
π-acid
catalyst
AgBF4
has
been
developed.
The
use
readily
available
starting
materials,
low
loading,
high
selectivity
(up
to
>98
:
2
d.r.),
broad
substrate
scope,
ease
scale-up,
versatile
functionalizations
products
make
this
approach
very
attractive
synthesis
1,1,3-trisubstituted
cyclobutanes.
Moreover,
control
experiments
theoretical
calculations
were
performed
illustrate
reaction
mechanism
selectivity.
Angewandte Chemie International Edition,
Journal Year:
2024,
Volume and Issue:
63(21)
Published: March 5, 2024
Abstract
Synthesis
of
bicyclic
scaffolds
has
emerged
as
an
important
research
topic
in
modern
drug
development
because
they
can
serve
saturated
bioisosters
to
enhance
the
physicochemical
properties
and
metabolic
profiles
candidates.
Here
we
report
a
remarkably
simple
silver‐enabled
strategy
access
polysubstituted
3‐azabicyclo[3.1.1]heptanes
single
operation
from
readily
accessible
bicyclobutanes
(BCBs)
isocyanides.
The
process
is
proposed
involve
formal
(3+3)/(3+2)/retro‐(3+2)
cycloaddition
sequence.
This
novel
protocol
allows
for
rapid
generation
molecular
complexity
starting
materials,
products
be
easily
derivatized,
further
enriching
BCB
chemistry
growing
set
valuable
sp
3
‐rich
building
blocks.
Journal of the American Chemical Society,
Journal Year:
2024,
Volume and Issue:
146(27), P. 18565 - 18575
Published: June 27, 2024
Bridged
bicyclic
scaffolds
are
emerging
bioisosteres
of
planar
aromatic
rings
under
the
concept
"escape
from
flatland".
However,
adopting
this
into
exploration
pyridines
remains
elusive
due
to
challenge
incorporating
a
N
atom
such
bridged
structures.
Herein,
we
report
practical
routes
for
divergent
synthesis
2-
and
3-azabicyclo[3.1.1]heptenes
(aza-BCHepes)
as
potential
readily
accessible
vinyl
azides
bicyclo[1.1.0]butanes
(BCBs)
via
two
distinct
catalytic
annulations.
The
reactivity
tailored
with
BCBs
is
key
achieving
transformations.
Ti
Angewandte Chemie International Edition,
Journal Year:
2024,
Volume and Issue:
63(29)
Published: May 11, 2024
Abstract
The
exploration
of
the
complex
chemical
diversity
bicyclo[n.1.1]alkanes
and
their
use
as
benzene
bioisosteres
has
garnered
significant
attention
over
past
two
decades.
Regiodivergent
syntheses
thiabicyclo[4.1.1]octanes
(S‐BCOs)
highly
substituted
bicyclo[2.1.1]hexanes
(BCHs)
using
a
Lewis
acid‐catalyzed
formal
cycloaddition
bicyclobutanes
(BCBs)
3‐benzylideneindoline‐2‐thione
derivatives
have
been
established.
first
hetero‐(4+3)
BCBs,
catalyzed
by
Zn(OTf)
2
,
was
achieved
with
broad
substrate
scope
under
mild
conditions.
In
contrast,
less
electrophilic
BCB
ester
undergoes
Sc(OTf)
3
‐catalyzed
[2π+2σ]
reaction
1,1,2‐trisubstituted
alkenes,
yielding
BCHs
spirocyclic
quaternary
carbon
center.
Control
experiments
preliminary
theoretical
calculations
suggest
that
diastereoselective
product
formation
may
involve
concerted
between
zwitterionic
intermediate
E
‐1,1,2‐trisubstituted
alkenes.
Additionally,
nucleophilic
ring‐opening
mechanism.
