International Journal of Molecular Sciences,
Journal Year:
2024,
Volume and Issue:
25(16), P. 8573 - 8573
Published: Aug. 6, 2024
Mucopolysaccharidosis
type
II
(MPS
II;
Hunter
syndrome)
is
a
rare,
X-linked
disorder
caused
by
deficient
activity
of
the
enzyme
iduronate-2-sulfatase.
Signs
and
symptoms
typically
emerge
at
1.5-4
years
age
may
include
cognitive
impairment,
depending
on
whether
patients
have
neuronopathic
or
non-neuronopathic
form
disease.
Treatment
available
in
replacement
therapy
(ERT)
with
recombinant
iduronate-2-sulfatase
(idursulfase).
A
systematic
literature
review
was
conducted
to
assess
evidence
regarding
efficacy,
effectiveness,
safety
ERT
intravenous
idursulfase
for
MPS
II.
Electronic
databases
were
searched
January
2023,
33
eligible
articles
found.
These
analyzed
evaluate
effects
overall
benefits
disadvantages
patient
subgroups.
Studies
showed
that
treatment
resulted
improved
short-
long-term
clinical
patient-centered
outcomes,
accompanied
favorable
profile.
Patients
had
more
pronounced
improvements
outcomes
than
those
In
addition,
identified
are
particularly
apparent
if
started
early
life,
strengthening
previous
recommendations
initiation
maximally
benefit
patients.
This
provides
comprehensive
summary
our
current
knowledge
efficacy
different
populations
will
help
inform
management
disease
an
evolving
landscape.
FEBS Journal,
Journal Year:
2024,
Volume and Issue:
291(15), P. 3331 - 3366
Published: March 18, 2024
Mammalian
glycosaminoglycans
(GAGs),
except
hyaluronan
(HA),
are
sulfated
polysaccharides
that
covalently
attached
to
core
proteins
form
proteoglycans
(PGs).
This
article
summarizes
key
biological
findings
for
the
most
widespread
GAGs,
namely
HA,
chondroitin
sulfate/dermatan
sulfate
(CS/DS),
keratan
(KS),
and
heparan
(HS).
It
focuses
on
major
processes
remain
be
deciphered
get
a
comprehensive
view
of
mechanisms
mediating
GAG
functions.
They
include
regulation
biosynthesis
postsynthetic
modifications
in
heparin
(HP)
HS,
composition,
heterogeneity,
function
tetrasaccharide
linkage
region
its
role
disease,
functional
characterization
new
PGs
recently
identified
by
glycoproteomics,
selectivity
interactions
mediated
chains,
display
chains
at
cell
surface
their
impact
availability
activity
soluble
ligands,
move
through
glycocalyx
layer
reach
receptors,
human
profile
health
roles
GAGs
particular
(syndecans,
decorin,
biglycan)
involved
cancer,
inflammation,
fibrosis,
possible
use
as
disease
biomarkers,
design
inhibitors
targeting
biosynthetic
enzymes
GAG-protein
develop
novel
therapeutic
approaches.
International Journal of Molecular Sciences,
Journal Year:
2023,
Volume and Issue:
24(4), P. 3887 - 3887
Published: Feb. 15, 2023
The
oxytocin
receptor
(OXTR),
encoded
by
the
OXTR
gene,
is
responsible
for
signal
transduction
after
binding
its
ligand,
oxytocin.
Although
this
signaling
primarily
involved
in
controlling
maternal
behavior,
it
was
demonstrated
that
also
plays
a
role
development
of
nervous
system.
Therefore,
not
surprise
both
ligand
and
are
modulation
behaviors,
especially
those
related
to
sexual,
social,
stress-induced
activities.
As
case
every
regulatory
system,
any
disturbances
structures
or
functions
may
lead
various
diseases
regulated
functions,
which
include
either
mental
problems
(autism,
depression,
schizophrenia,
obsessive-compulsive
disorders)
functioning
reproductive
organs
(endometriosis,
uterine
adenomyosis,
premature
birth).
Nevertheless,
abnormalities
connected
other
diseases,
including
cancer,
cardiac
disorders,
osteoporosis,
obesity.
Recent
reports
indicated
changes
levels
formation
aggregates
influence
course
some
inherited
metabolic
such
as
mucopolysaccharidoses.
In
review,
involvement
dysfunctions
polymorphisms
different
summarized
discussed.
analysis
published
results
led
us
suggest
expression
abundance
activity
specific
individual
but
rather
they
processes
(mostly
behavioral
changes)
might
modulate
disorders.
Moreover,
possible
explanation
discrepancies
effects
gene
methylation
on
proposed.
Human Mutation,
Journal Year:
2025,
Volume and Issue:
2025(1)
Published: Jan. 1, 2025
Mucopolysaccharidosis
Type
VI
(MPS
VI)
is
a
lysosomal
storage
disorder
associated
with
biallelic
pathogenic
variants
in
the
ARSB
gene.
Herein,
we
present
three
patients
biochemical
and
clinical
pictures
of
MPS
VI,
for
whom
routine
molecular
genetic
analysis
using
Sanger
sequencing
failed
to
identify
one
or
both
causative
variants.
RNA
patients’
samples
revealed
alterations
wild‐type
mRNA
isoform
all
cases,
case
required
further
whole
genome
sequencing.
As
result,
identified
complex
structural
variant,
which
52‐kb
insertion
LHFPL2
gene
fragment
Intron
4,
derived
from
nonallelic
homologous
recombination
leading
premature
transcription
termination,
recurrent
deep
intronic
variant
pseudoexon
activation
an
intragenic
deletion
altering
integrity
splicing
Exon
2.
Using
minigene‐based
cellular
model,
demonstrated
that
can
be
efficiently
blocked
by
antisense
molecules
incorporated
into
modified
U7
small
nuclear
RNAs
circular
RNAs.
The
same
approach
was
used
block
overlapping
polymorphic
increase
amount
approximately
twofold.
International Journal of Molecular Sciences,
Journal Year:
2025,
Volume and Issue:
26(3), P. 1273 - 1273
Published: Feb. 1, 2025
Mucopolysaccharidosis
type
IIIC
is
a
neurodegenerative
lysosomal
storage
disorder
(LSD)
characterized
by
the
accumulation
of
undegraded
heparan
sulfate
(HS)
due
to
lack
an
enzyme
responsible
for
its
degradation:
acetyl-CoA:α-glucosaminide
N-acetyltransferase
(HGSNAT).
Classical
treatments
are
ineffective.
Here,
we
attempt
new
approach
in
genetic
medicine,
substrate
reduction
therapy
(gSRT),
counteract
this
neurological
disorder.
Briefly,
used
synthetic
oligonucleotides,
particularly
gapmer
antisense
oligonucleotides
(ASOs),
target
synthesis
accumulated
compounds
at
molecular
level,
downregulating
specific
gene
involved
first
step
HS
biosynthesis,
XYLT1.
Our
goal
was
reduce
production
and,
consequently,
accumulation.
Initially,
five
ASOs
were
designed
and
their
potential
decrease
XYLT1
mRNA
levels
tested
patient-derived
fibroblasts.
Subsequent
analyses
focused
on
two
best
performing
molecules
alone.
The
results
showed
high
inhibition
(around
90%),
xylosyltransferase
I
(XT-I)
protein
6
10
days
after
transfection
(up
21%
32%,
respectively).
Overall,
our
highly
promising
may
represent
initial
towards
development
therapeutic
option
not
only
MPS
IIIC,
but
virtually
every
other
III
form.
Ultimately,
same
principle
also
apply
neuropathic
MPS.
Scientific Reports,
Journal Year:
2025,
Volume and Issue:
15(1)
Published: Feb. 10, 2025
Mucopolysaccharidosis
type
II
(MPS
II)
is
caused
by
a
deficiency
in
iduronate-2-sulfatase
(Ids),
an
enzyme
that
catabolizes
glycosaminoglycan
(GAG).
Ids
insufficiency
results
the
accumulation
of
GAG
various
organs,
ultimately
resulting
multisystemic
disease.
Trehalose,
non-reducing
disaccharide,
has
shown
protective
effects
against
diseases.
However,
its
potential
utility
through
oral
administration
MPS
not
yet
been
explored.
In
present
study,
to
investigate
efficacy
trehalose
Ids-knock-out
(KO)
mice,
Ids-KO
and
wild
(WT)
mice
were
treated
with
2%
dissolved
distilled
water
ad
libitum
for
24
weeks.
Histological
analysis
revealed
almost
all
tissues
from
exhibited
abnormal
changes,
including
large
vacuolization,
inflammatory
cell
infiltration,
deposition.
significantly
suppressed
levels,
inflammation
apoptosis
spleen
brain.
Additionally,
considerably
improved
cognitive
functions,
such
as
short-term
spatial
learning
working
memory,
alongside
limited
improvements
walking
capacity
mice.
These
suggest
can
reduce
accumulation,
vacuolization
number
apoptotic
cells
pathological
brain,
improving
spontaneous
alteration
behavior
could
be
promising
treatment
option
II.
The Italian Journal of Pediatrics/Italian journal of pediatrics,
Journal Year:
2025,
Volume and Issue:
51(1)
Published: March 18, 2025
Allogeneic
hematopoietic
stem
cell
transplantation
(HSCT)
has
proven
to
be
a
viable
treatment
option
for
patients
with
mucopolysaccharidoses
(MPS).
We
investigate
the
efficacy
and
improvements
in
quality
of
life
HSCT
pediatric
MPS.
A
retrospective
analysis
data
from
46
cases
MPS
single
institution
China
was
conducted.
The
cohort
included
9
I,
16
II,
15
IVA
6
VI.
median
age
at
diagnosis
2.59
years.
3.80
follow-up
time
3.1
years
(range,
0.8-8.1
years)
43
were
alive.
incidence
grades
II
IV
aGVHD
17.4%,
wherein
III
4.3%.
moderate-to-severe
cGVHD
6.5%.
GAGs
urinary
excretion
decreased
enzyme
activity
levels
reached
normal.
After
HSCT,
multiple
bone
dysplasia,
upper-airway
obstruction
recurrent
otitis
media
significantly
improved;
vision,
corneal
clouding,
cardiovascular
disease,
hepatosplenomegaly
hydrocephalus
improved
or
remained
stable;
neurological
symptoms
stable
most
but
progressed
others;
IH/S
nearly
normal
growth
rate
height
weight.
Meanwhile,
IH,
VI
poor
after
HSCT.
Activities
Daily
Living
(ADL)
scores
ADL
severe
phenotypes
lower
than
health
control
subjects
attenuated
phenotypes.
is
good
therapeutic
improves
patients.
provide
better
outcome
Orphanet Journal of Rare Diseases,
Journal Year:
2025,
Volume and Issue:
20(1)
Published: May 2, 2025
Abstract
This
systematic
review
of
randomized
controlled
trials
(RCT)
was
conducted
to
evaluate
the
efficacy
enzyme
replacement
therapy
(ERT)
for
patients
with
mucopolysaccharidosis
(MPS).
We
systematically
searched
PubMed,
Embase,
Web
Science,
and
Cochrane
databases
up
August
22,
2023.
Study
design,
interventions,
outcome
data
were
extracted.
Continuous
variable
random-effects
network
meta-analysis
performed.
The
included
23
studies
involving
1,047
people
MPS
I–VI.
In
I,
urinary
glycosaminoglycan
(uGAG)
level
significantly
reduced
in
who
took
2
mg/kg/week
pentosan
polysulfate
(-2.66,
95%
confidence
interval
(CI)[-3.86,
-1.46])
compared
those
1
mg/kg/week.
II,
placebo
group,
significant
reduction
observed
uGAG
(-270.77,
CI[-406.57,
-139.71])
cerebrospinal
fluid
(CSF)
GAG
(-1,385.29,
CI[-2493.33,
-392.65]).
IV,
6-min
walking
test
(6MWT)
(40.82,
CI[16.19,
64.92])
3-min
stair
climb
(3MSCT)
(16.07,
CI[12.16,
21.62])
increased
elosulfase
alfa
at
a
dose
4.0
group.
VI,
recombinant
human
arylsulfatase
B
(rhASB)
galsulfase
(1.0
mg/kg/week)
aggregation
group
(-217,
CI[-258,
-176])
(2.0
(-286.5,
CI[-436.5,
-136.5]),
respectively.
Moreover,
most
had
high
(34.8%)
or
unclear
(43.5%)
risk
bias
assessments
assessment
low.
ERT
alleviated
symptoms
some
extent,
but
current
evidence
insufficient.
Hence,
further
from
large-sample
RCT
is
needed.
International Journal of Nanomedicine,
Journal Year:
2025,
Volume and Issue:
Volume 20, P. 1443 - 1490
Published: Feb. 1, 2025
Abstract:
Given
the
complexity
of
central
nervous
system
(CNS)
and
diversity
neurological
conditions,
increasing
prevalence
disorders
poses
a
significant
challenge
to
modern
medicine.
These
disorders,
ranging
from
neurodegenerative
diseases
psychiatric
not
only
impact
individuals
but
also
place
substantial
burden
on
healthcare
systems
society.
A
major
obstacle
in
treating
these
conditions
is
blood-brain
barrier
(BBB),
which
restricts
passage
therapeutic
agents
brain.
Nanotechnology,
particularly
use
nanoparticles
(NPs),
offers
promising
solution
this
challenge.
NPs
possess
unique
properties
such
as
small
size,
large
surface
area,
modifiable
characteristics,
enabling
them
cross
BBB
deliver
drugs
directly
affected
brain
regions.
This
review
focuses
application
gene
therapy
enzyme
replacement
(ERT)
for
disorders.
Gene
involves
altering
or
manipulating
expression
can
be
enhanced
by
designed
carry
various
genetic
materials.
Similarly,
improve
efficacy
ERT
lysosomal
storage
(LSDs)
facilitating
delivery
brain,
overcoming
issues
like
immunogenicity
instability.
Taken
together,
explores
potential
revolutionizing
treatment
options
highlighting
their
advantages
future
directions
rapidly
evolving
field.
Keywords:
system,
nanoparticle,
therapy,
