The Journal of Cell Biology,
Год журнала:
2024,
Номер
224(3)
Опубликована: Дек. 17, 2024
The
tubulin
code
hypothesis
predicts
that
tails
create
programs
for
selective
regulation
of
microtubule-binding
proteins,
including
kinesin
motors.
However,
the
molecular
mechanisms
determine
and
their
relevance
in
cells
are
poorly
understood.
We
report
budding
yeast
kinesin-5
motors
by
β-tubulin
tail.
Cin8,
but
not
Kip1,
requires
tail
recruitment
to
mitotic
spindle,
creating
a
balance
both
spindle
efficient
progression.
identify
negatively
charged
patch
mediates
interaction
with
Cin8.
Using
vitro
reconstitution
genetically
modified
tubulin,
we
demonstrate
increases
Cin8
plus-end-directed
velocity
processivity.
Finally,
positively
amino-terminal
extension
coordinates
interactions
Our
work
identifies
mechanism
underlying
closely
related
how
this
promotes
proper
function
spindle.
Biochemical Society Transactions,
Год журнала:
2025,
Номер
53(01)
Опубликована: Фев. 5, 2025
Microtubule
(MT)
dynamic
instability,
a
cycle
of
growth,
catastrophe,
shrinkage
and
rescue,
is
driven
by
the
switching
tubulin
between
two
structural
states,
one
stabilised
GTP
other
GDP.
Recent
work
has
uncovered
ancient
origins
this
switch
revealed
further
fundamental
elements
microtubule
whereby
can
be
brought
about
range
allosteric
effectors,
propagate
deep
within
lattice
assembled
MTs,
profoundly
affect
MT
function.
Here,
we
review
evidence
for
discuss
current
ideas
its
mechanisms.
ABSTRACT
Sugars
are
important
both
as
an
energy
source
and
a
signaling
cue.
In
Arabidopsis
thaliana
,
SPINDLY
(SPY)
is
the
bona
fide
O
‐fucosylation
transferase
that
links
sugar
with
various
plant
growth
development
processes.
Previously,
spy
was
shown
to
display
strong
salt
drought
tolerance
phenotype.
Herein
we
confirmed
phenotype
further
studied
its
mechanism.
We
found
abscisic
acid
(ABA)
elevated
SPY
expression
in
guard
cells,
involved
ABA‐induced
stomatal
closure.
show
regulates
rearrangement
of
microtubule
cytoskeleton
cells.
Moreover,
reorganization
enhanced
mutants.
Mechanistically,
interacts
α‐tubulin1
(TUA1)
yeast‐two
hybrid,
bimolecular
fluorescence
complementation
split
luciferase
imaging
assays,
indicating
TUA1
may
be
‐fucosylated
by
SPY.
Our
work
line
notion
has
many
substrates
diverse
processes
plants,
also
unearths
key
mechanism
how
glycosylation
stomata
movement
via
cytoskeleton.
The Journal of Cell Biology,
Год журнала:
2024,
Номер
223(4)
Опубликована: Фев. 8, 2024
Microtubule-severing
enzymes
(MSEs),
such
as
Katanin,
Spastin,
and
Fidgetin
play
essential
roles
in
cell
division
neurogenesis.
They
damage
the
microtubule
(MT)
lattice,
which
can
either
destroy
or
amplify
MT
cytoskeleton,
depending
on
cellular
context.
However,
little
is
known
about
how
they
interact
with
their
substrates.
We
have
identified
microtubule-binding
domains
(MTBD)
required
for
Katanin
function
C.
elegans.
a
heterohexamer
of
dimers
containing
catalytic
subunit
p60
regulatory
p80,
both
are
female
meiotic
spindle
assembly.
Here,
we
report
that
p80-like(MEI-2)
dictates
binding
to
MTs
via
two
MTBDs
composed
basic
patches.
Substituting
these
patches
reduces
MTs,
compromising
its
meiotic-spindle
Structural
alignments
p80s
from
different
species
revealed
evolutionarily
conserved,
even
if
specific
amino
acids
involved
vary.
Our
findings
highlight
critical
importance
(p80)
providing
complex.
Frontiers in Neuroscience,
Год журнала:
2023,
Номер
17
Опубликована: Июль 26, 2023
Axons
are
processes
of
neurons,
up
to
a
metre
long,
that
form
the
essential
biological
cables
wiring
nervous
systems.
They
must
survive,
often
far
away
from
their
cell
bodies
and
century
in
humans.
This
requires
self-sufficient
biology
including
structural
proteins,
organelles,
membrane
trafficking,
metabolic,
signalling,
translational,
chaperone,
degradation
machinery—all
maintaining
homeostasis
energy,
lipids,
signalling
networks
reactive
oxygen
species
calcium.
Axon
maintenance
also
involves
specialised
cytoskeleton
cortical
actin-spectrin
corset,
bundles
microtubules
provide
highways
for
motor-driven
transport
components
organelles
virtually
all
above-mentioned
processes.
Here,
we
aim
conceptual
overview
key
aspects
axon
physiology,
homeostatic
they
form.
can
be
derailed,
causing
axonopathies
through
ageing,
trauma,
poisoning,
inflammation
or
genetic
mutations.
To
illustrate
which
malfunctions
lead
axonopathies,
focus
on
axonopathy-linked
subcellular
defects
caused
by
Based
these
descriptions
backed
our
comprehensive
data
mining
genes
linked
neural
disorders,
describe
‘dependency
cycle
local
homeostasis’
as
an
integrative
model
explain
why
very
different
causes
trigger
similar
providing
new
ideas
drive
quest
strategies
able
battle
devastating
diseases.
bioRxiv (Cold Spring Harbor Laboratory),
Год журнала:
2024,
Номер
unknown
Опубликована: Март 12, 2024
Abstract
Developmental
remodeling
shapes
neural
circuits
via
activity-dependent
pruning
of
synapses
and
axons.
The
cytoskeleton
is
critical
for
this
process,
as
microtubule
loss
enzymatic
severing
an
early
step
across
many
species.
However,
how
microtubule-severing
enzymes,
such
spastin,
are
activated
in
specific
neuronal
compartments
remains
unknown.
Here,
we
reveal
that
polyglutamylation,
a
posttranslational
tubulin
modification
enriched
neurons,
plays
instructive
role
developmental
by
tagging
microtubules
severing.
Motor
neuron-specific
gene
deletion
enzymes
add
or
remove
polyglutamylation—TTLL
glutamylases
vs.
CCP
deglutamylases—accelerates
delays
neuromuscular
synapse
neurotransmission-dependent
manner.
This
mechanism
not
to
peripheral
but
also
operates
central
circuits,
e.g.,
the
hippocampus.
Thus,
polyglutamylation
acts
rheostat
morphology
connectivity.
Cell Death and Disease,
Год журнала:
2024,
Номер
15(10)
Опубликована: Окт. 23, 2024
Lung
squamous
cell
carcinoma
(LUSC)
is
associated
with
high
mortality
and
has
few
therapeutic
options.
Chemotherapy
remains
the
main
treatment
for
LUSC
patients,
but
multi-drug
resistance
become
dominant
challenge
in
failure
of
chemotherapy
various
cancers.
Therefore,
effective
strategy
patients
an
urgent
unmet
need.
Here,
we
found
vasohibin-2
(VASH2)
was
a
prognostic
biomarker
VASH2
promoted
malignant
biological
behaviors
cells
chemoresistance
by
increasing
detyrosination
α-tubulin.
The
level
detyrosinated-tubulin
negatively
patient
prognosis.
Blocking
tubulin
carboxypeptidase
(TCP)
activity
inhibited
xenograft
tumor
growth
improved
efficacy
paclitaxel
vivo.
Results
revealed
that
VASH2-induced
increase
boosted
binding
kinesin
family
member
3C
(KIF3C)
to
microtubules
enhanced
KIF3C-dependent
endosomal
recycling
EGFR,
leading
prolonged
activation
PI3K/Akt/mTOR
signaling.
This
study
demonstrated
not
only
also
promising
target
LUSC,
which
offers
novel
insight
combination
EpoY,
TCP
inhibitor,
may
be
patients.
