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Document Description
Title
Human
kallikrein-related
peptidase
6
(KLK6)
and
13
(KLK13)
are
involved
in
ovarian
carcinoma
pathogenesis
Author
White
,
Nicole
,
1978-
Description
Thesis
(Ph.D.)--Memorial
University
of
Newfoundland
,
2010.
Medicine
Date
2010
Pagination
xvii, 5-212 leaves : ill. (some col.)
Subject
Kallikrein;
Ovaries--Cancer--Diagnosis;
Ovaries--Cancer--Genetic
aspects;
Subject.MESH
Kallikreins;
Ovarian
Neoplasms--diagnosis;
Ovarian
Neoplasms--etiology;
Degree
Ph.D.
Degree Grantor
Memorial University of Newfoundland. Faculty of Medicine
Discipline
Medicine
Language
Eng
Notes
Includes
bibliographical
references
Abstract
It
is
estimated
in
2009
that
2500
Canadian
women
were
diagnosed
and
1750
women
lost
their
lives
to
epithelial
ovarian
cancer.
This
malignancy
has a
high
mortality
rate
because
the
majority
of
women
are
diagnosed
in
late
stage
disease
where
the
5
year
survival
rate
is
only
20%.
Late
diagnosis
is
a
result
of the
lack
of an
effective
screening
marker.
Currently
,
CA125
is
the
only
marker
that
is
used
for
ovarian
cancer
patients
and
it
is
used
primarily
to
monitor
disease
recurrence
after
treatment.
Unfortunately
,
CA125
lacks
the
sensitivity
and
specificity
to be
used
for
early
detection
of
ovarian
cancer.
Recently
, a
new
group
of
genes
, the
human
kallikrein-related
peptidase
(KLK)
family
, has been
implicated
in
ovarian
cancer
and are
being
investigated
as
potential
new
biomarkers
for the
malignancy.
In
particular
,
KLK
13
has been
shown
to have
increased
expression
in
ovarian
cancer.
KLK13
has
increased
expression
in the
ovarian
cancer
cell
lines
CAOV-3
,
OVCAR-3
, and
SKOV-3
when
compared
to the
IOSE
cell
line
and
is
involved
in
cell
motility.
Increased
KLK13
expression
increases
migration
in the
epithelial
cell
lines
IOSE
and
Mv1Lu.
Also
,
when
KLK13
expression
was
decreased
in the
ovarian
cancer
cell
line
SKOV-3
,
which
has
high
endogenous
KLK13
expression
levels
, there was a
decrease
in
cellular
migration.
Increased
KLK13
expression
in
IOSE
cells
increased
cellular
invasion
through
the
basement
membrane.
These
data
together
suggest
KLK
13
plays
a
role
in
ovarian
carcinogenesis
and
may
be a
potential
therapeutic
target.
In
order
to
see
if
KLK
expression
had any
prognostic
significance
in
ovarian
cancer
patients
,
paraffin
embedded
ovarian
cancer
samples
were
analyzed
for
KLK6
and
KLK13
mRNA
expression.
High
expression
levels
of
both
KLK6
and
KLK13
were
associated
with
invasive
ovarian
cancer.
Also
,
high
KLK6
expression
was
associated
with
late
stage
ovarian
cancer
and
serous
histological
type.
Both
KLK6
and
KLK13
were also
shown
to be
markers
of
poor
prognosis
as
patients
with
high
kallikrein
expression
were
more
likely
to have a
recurrence
than
patients
with
low
KLK
expression.
When
KLK6
,
KLK13
and
Mucl6
were
assessed
for the
ability
to
detect
ovarian
cancer
, the
genes
detected
56%
,
50%
, and
56%
,
respectively
,
early
stage
(Stage
I
and
II)
ovarian
cancer
patients.
When
all
three
markers
were
used
in
combination
, the
sensitivity
of the
test
improved
to
84%.
There was
no
significant
change
in the
specificity
or
positive
predictive
value
, but the
negative
predictive
value
increased
from
33%
using
the
individual
markers
to
58%
when
all
three
markers
were
combined.
These
data
together
suggest
KLK6
and
KLK
13
are
involved
in
ovarian
cancer
tumorigenesis.
Both
KLK6
and
KLK13
are
potential
new
markers
and
possible
therapeutic
targets
for
ovarian
carcinoma.
Type
Text
Resource Type
Electronic
thesis
or
dissertation
Format
Image/jpeg;
Application/pdf
Source
Paper copy kept in the Centre for Newfoundland Studies, Memorial University Libraries
Local Identifier
a3497942
Rights
The author retains copyright ownership and moral rights in this thesis. Neither the thesis nor substantial extracts from it may be printed or otherwise reproduced without the author's permission.
Collection
Electronic
Theses
and
Dissertations
Scanning Status
Completed
PDF File
(25.81
MB)
--
http://collections.mun.ca/PDFs/theses/White_Nicole.pdf
CONTENTdm file name
50833.cpd