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Neutrophil elastase, proteinase 3, and cathepsin G as therapeutic targets in human diseases.
[papillon-lefèvre syndrome]
Polymorphonuclear
neutrophils
are
the
first
cells
recruited
to
inflammatory
sites
and
form
the
earliest
line
of
defense
against
invading
microorganisms
.
Neutrophil
elastase
,
proteinase
3
,
and
cathepsin
G
are
three
hematopoietic
serine
proteases
stored
in
large
quantities
in
neutrophil
cytoplasmic
azurophilic
granules
.
They
act
in
combination
with
reactive
oxygen
species
to
help
degrade
engulfed
microorganisms
inside
phagolysosomes
.
These
proteases
are
also
externalized
in
an
active
form
during
neutrophil
activation
at
inflammatory
sites
,
thus
contributing
to
the
regulation
of
inflammatory
and
immune
responses
.
As
multifunctional
proteases
,
they
also
play
a
regulatory
role
in
noninfectious
inflammatory
diseases
.
Mutations
in
the
ELA
2
/
ELANE
gene
,
encoding
neutrophil
elastase
,
are
the
cause
of
human
congenital
neutropenia
.
Neutrophil
membrane-bound
proteinase
3
serves
as
an
autoantigen
in
Wegener
granulomatosis
,
a
systemic
autoimmune
vasculitis
.
All
three
proteases
are
affected
by
mutations
of
the
gene
(
CTSC
)
encoding
dipeptidyl
peptidase
I
,
a
protease
required
for
activation
of
their
proform
before
storage
in
cytoplasmic
granules
.
Mutations
of
CTSC
cause
Papillon-
Lefèvre
syndrome
.
Because
of
their
roles
in
host
defense
and
disease
,
elastase
,
proteinase
3
,
and
cathepsin
G
are
of
interest
as
potential
therapeutic
targets
.
In
this
review
,
we
describe
the
physicochemical
functions
of
these
proteases
,
toward
a
goal
of
better
delineating
their
role
in
human
diseases
and
identifying
new
therapeutic
strategies
based
on
the
modulation
of
their
bioavailability
and
activity
.
We
also
describe
how
nonhuman
primate
experimental
models
could
assist
with
testing
the
efficacy
of
proposed
therapeutic
strategies
.
Diseases
Validation
Diseases presenting
"large quantities in neutrophil"
symptom
papillon-lefèvre syndrome
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