Ovarian Neoplasms Clinical Trial
Official title:
ANG-001 Pelvic Mass Training Study: Evaluation of Multiple Circulating Tumor Cell-derived RNA Markers to Estimate Risk of Ovarian Cancer in Patients Presenting With a Pelvic Mass.
ANGLE has developed the Parsortix™ Cell Separation System (Parsortix), an automated system
capable of harvesting rare circulating cells for analysis from a sample of peripheral blood
based on cellular size and deformability. In a small pilot study, scientists at the Medical
University of Vienna demonstrated that measurement of a combination of mRNA markers extracted
from CTCs captured using the Parsortix system could be used to identify women with ovarian
cancer. This study is designed to provide specimens for optimization of an assay using
clinical and biomarker information (i.e. demographics, imaging results and/or serum tumor
markers) in combination with mRNA extracted from rare cells in the blood of women presenting
with a pelvic mass for the detection of malignancy.
Primary Objective: Optimization of an assay for the differentiation of women with benign
pelvic masses from those with malignant pelvic masses using mRNA markers extracted from CTCs
isolated from whole blood. Multiple serum tumor markers and mRNA markers will be measured,
and the results will be compared to the actual clinical diagnosis made for each patient
through other recognized methods (e.g. histopathology). The blood samples collected in the
course of this study will be used to finalize the selection of mRNA and/or serum tumor
markers to be evaluated in future prospective studies.
Exploratory Objective: Use statistical modeling to determine the need for and/or preliminary
design of a mathematical algorithm to combine the multiple serum tumor and/or mRNA markers
for estimation of the risk of ovarian cancer.
This study is exploratory in nature and is designed to be hypothesis generating to support
the design of future studies. A total of 200 women diagnosed with a pelvic mass (defined as a
simple, complex or a solid ovarian cyst / pelvic mass) who are scheduled for a laparotomy or
laparoscopy for removal of the pelvic mass will be enrolled for evaluation of the primary and
exploratory endpoints. An initial evaluation of the data will be conducted after
identification of 15 evaluable subjects with histopathologically confirmed ovarian cancer. It
is estimated that 50 - 100 subjects will be required to obtain a minimum of 15 evaluable
subjects with histopathologically confirmed ovarian cancer. The remainder of the women
enrolled (expected to be ~100 - 150 subjects) will be used to verify the findings from the
initial evaluation (i.e. correlation of the markers with the absence or presence of
malignancy) and to refine the assay/algorithm.
Within 60 days prior to surgery, each subject must have a pelvic imaging study (e.g.
ultrasound, CT scan, MRI, etc.) conducted and read to visualize the pelvic mass according to
the current standard of care. Results of the pelvic imaging study(ies) will be recorded.
Within 60 days prior to, or on the day of the pelvic mass surgery, collect up to 35mL of
peripheral blood into one 5mL SST tube, which must be drawn first, followed by three separate
10mL EDTA tubes. Serum from SST tube will be prepared at the local study center and used for
protein biomarker testing. The EDTA tubes will be shipped to the Medical University of
Vienna, where the blood will be pooled and equal volumes processed using two different
separation methods on the Parsortix™ system to capture and harvest rare cells. The harvested
material from the EDTA tubes will be lysed, and total RNA will be extracted from the cell
lysate for evaluation of multiple gene targets using quantitative PCR (qPCR).
Laparotomy or laparoscopy for removal of the pelvic mass will be performed by a qualified
individual. Tissue samples will be sent to the local pathology department for histological
examination in accordance with standard institutional practices. Results of the
histopathological evaluation will be recorded, including the final diagnosis along with
histological sub-type, and if available, stage and grade of ovarian cancer where disease is
identified.
Subjects will be considered negative for ovarian cancer:
- if the subject undergoes surgery and no mass is identified, or;
- if the histopathological findings are negative for cancer (i.e. benign conditions).
Subjects will be considered positive for ovarian cancer:
- if the histological examination of the tissue taken at the time of surgery confirms the
presence of ovarian, primary peritoneal and/or fallopian tube cancers.
For the purposes of enrollment, subjects diagnosed with a malignancy other than an ovarian
cancer as well as those diagnosed with low malignant potential (LMP) / borderline tumors will
not be counted as an ovarian cancer. However, two separate analyses of the final study data
will be conducted: one where subjects diagnosed with other cancers are excluded from the
analysis of the primary endpoint and the subjects diagnosed with LMP / borderline tumors are
classified as being negative for malignancy, and a second where subjects diagnosed with other
cancers and those diagnosed with LMP / borderline tumors are classified as being positive for
malignancy.
Demographical and clinical data may be summarized using descriptive statistics. Continuous
variables may be summarized using the number of observations, mean, standard deviation,
coefficient of variation, median, and range as appropriate. Categorical values may be
summarized using the number of observations and percentages as appropriate.
The association of the markers (i.e. serum protein markers and mRNA markers) with the
histopathological diagnosis will be assessed using appropriate statistical methods (e.g.,
logistic regression, analysis of variance [ANOVA], etc.), depending on the endpoints.
Analyses may be performed within and between various histopathological diagnosis sub-groups.
Other clinical covariates (such as imaging results and subject demographics) may also be
included in the modeling.
An initial evaluation of the correlation of the markers with the histopathological diagnosis
will be performed after the identification of 15 subjects with histopathologically verified
ovarian cancer. The final cohort of patients will be used to verify the findings from the
initial evaluation (i.e. correlation of the markers with the absence or presence of
malignancy) and to refine the assay/algorithm. Bootstrap analyses may be utilized on the
entire set of 200 subjects to finalize an assay/algorithm for further study.
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