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Lysosomal multienzyme complex: pros and cons of working together.
[gm1 gangliosidosis]
The
ubiquitous
distribution
of
lysosomes
and
their
heterogeneous
protein
composition
reflects
the
versatility
of
these
organelles
in
maintaining
cell
homeostasis
and
their
importance
in
tissue
differentiation
and
remodeling
.
In
lysosomes
,
the
degradation
of
complex
,
macromolecular
substrates
requires
the
synergistic
action
of
multiple
hydrolases
that
usually
work
in
a
stepwise
fashion
.
This
catalytic
machinery
explains
the
existence
of
lysosomal
enzyme
complexes
that
can
be
dynamically
assembled
and
disassembled
to
efficiently
and
quickly
adapt
to
the
pool
of
substrates
to
be
processed
or
degraded
,
adding
extra
tiers
to
the
regulation
of
the
individual
protein
components
.
An
example
of
such
a
complex
is
the
one
composed
of
three
hydrolases
that
are
ubiquitously
but
differentially
expressed
:
the
serine
carboxypeptidase
,
protective
protein
/
cathepsin
A
(
PPCA
)
,
the
sialidase
,
neuraminidase-
1
(
NEU
1
)
,
and
the
glycosidase
β-galactosidase
(
β-
GAL
)
.
Next
to
this
'
core
'
complex
,
the
existence
of
sub-complexes
,
which
may
contain
additional
components
,
and
function
at
the
cell
surface
or
extracellularly
,
suggests
as
yet
unexplored
functions
of
these
enzymes
.
Here
we
review
how
studies
of
basic
biological
processes
in
the
mouse
models
of
three
lysosomal
storage
disorders
,
galactosialidosis
,
sialidosis
,
and
GM
1
-
gangliosidosis
,
revealed
new
and
unexpected
roles
for
the
three
respective
affected
enzymes
,
Ppca
,
Neu
1
,
and
β-
Gal
,
that
go
beyond
their
canonical
degradative
activities
.
These
findings
have
broadened
our
perspective
on
their
functions
and
may
pave
the
way
for
the
development
of
new
therapies
for
these
lysosomal
storage
disorders
.
Diseases
Validation
Diseases presenting
"canonical degradative activities"
symptom
gm1 gangliosidosis
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