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High levels of type VII collagen expression in recessive dystrophic epidermolysis bullosa cutaneous squamous cell carcinoma keratinocytes increases PI3K and MAPK signalling, cell migration and invasion.
[dystrophic epidermolysis bullosa]
Epidermolysis
bullosa
is
a
group
of
inherited
skin
fragility
diseases
varying
in
severity
from
mild
scarring
to
infant
mortality
.
Great
efforts
are
being
undertaken
to
develop
therapeutic
strategies
to
treat
the
more
pernicious
forms
of
this
disease
,
particularly
those
associated
with
recessive
,
loss
-of-function
mutations
.
In
such
cases
significant
effort
is
directed
toward
delivering
recombinant
protein
at
levels
sufficient
to
demonstrate
clinical
benefit
.
Recessive
dystrophic
epidermolysis
bullosa
(
RDEB
)
predisposes
patients
to
a
high
incidence
of
life-threatening
cutaneous
squamous
cell
carcinoma
(
cSCC
)
.
Mutations
in
the
gene
encoding
type
VII
collagen
,
COL
7
A
1
,
are
the
sole
cause
of
this
disease
and
conflicting
reports
concerning
type
VII
collagen
and
COL
7
A
1
in
carcinogenesis
exist
.
To
investigate
potential
oncogenic
effects
of
expressing
recombinant
type
VII
collagen
in
patient
cells
.
We
used
retroviral
transduction
to
introduce
type
VII
collagen
into
keratinocytes
derived
from
patients
with
and
without
RDEB
.
Retroviral
expression
of
type
VII
collagen
in
cSCC
keratinocytes
established
from
patients
with
RDEB
resulted
in
increased
cell
adhesion
,
migration
and
invasion
coupled
with
a
concurrent
increase
in
PI
3
K
and
MAPK
signalling
.
Our
data
suggest
caution
when
formulating
strategies
where
delivery
of
type
VII
collagen
is
likely
to
exceed
levels
seen
under
normal
physiological
conditions
in
a
patient
group
with
a
higher
inherent
risk
of
developing
skin
cancer
.