Cancer of Ovary Clinical Trial
Official title:
Olympia-MITO13-validation of a Laparoscopic Score to Predict the Chance of Optimal Cytoreduction in Advanced Ovarian Cancer Patients: an Open-label Prospective Multicentric-trial.
Prospective multicenter study that aims to evaluate the learning curve of a laparoscopic
score to predict possibility of optimal cytoreduction in patients with ovarian / tubal /
peritoneal advanced at the time of first surgery. The study consists of subjecting all
patients with a clinical suspicion and / or radiological diagnostic laparoscopy (SLPs).
Laparoscopy should be described and recorded in electronic form. After the procedure each
patient will have a Laparoscopic-evaluation-form filled up with a laparoscopic score (PI).
The minimum number of cases to be enrolled is 10 patients, in a minimum time of 1 year. The
data collected and the video should be sent to the Center Coordinator, who will determine the
adequacy of the procedure and the accuracy of the score enrollment is completed for each
center. All eligible subjects will be considered by intention-to-treat population (ITT). For
this phase of the study, it is not necessary know the outcome of the surgical patient (RT) or
if it was then subjected to exploratory laparotomy or less.
Results from large but retrospective studies clearly demonstrated that RT after primary
surgery is the most important prognostic factor in AOC patients. Subsequently, several
studies have shown a complete cytoreduction (RT=0) is associated with a statistically
significant longer survival rate than minimal residual disease (RT=1-2 cm). As a consequence,
a maximal surgical effort is considered the main goal to pursue in these patients.
However, data from the literature have shown that a certain percentage of AOC patients,
variable between 10 and 80%, are still considered inoperable at time of primary surgery, and
they are submitted to an unnecessary xipho-pubic laparotomy. This approach, beside affecting
QoL, can be related to some complications and delay in starting chemotherapy. This result can
be related to a series of variables, including patient's performance status, philosophy of
the centre and skillness of the surgeon. Finally, the anatomic diffusion of the disease is
described as one of the most limiting factor to an optimal cytoreduction.
In order to preoperatively identify patients with unresectable tumors, which can be spared an
unnecessary exploratory laparotomy, several approaches have been attempted, including CA 125
serum levels and CT-scan. However, the accuracy of those parameters has been unsatisfactory,
and limited by the retrospective nature of the studies and the highly variable rates of
optimal cytoreduction in different series.
Laparoscopy is well-known to offer a direct and magnified vision of the peritoneal cavity and
a better view of the upper abdomen. It allows the pathological assessment of the disease
without an open surgical procedure, with a shorter operating time and better results in terms
of post-operative morbidity. We first demonstrated in a pilot study that laparoscopy alone is
able to provide the same information regarding the chance of optimal cytoreduction (RT<= 1cm)
than standard laparotomy in clinically AOC patients. Since then, other investigators have
confirmed the role of laparoscopy in the evaluation of the possibility of achieving optimal
residual disease in the same clinical subset.
However, one of the major criticism to these studies was represented by the surgeon
subjectivity in evaluating optimal debulking in relation to surgical team and operating room
performances. Consequently, on the basis of previous published papers, we set up a
quantitative predictive model, which provides each patient with a score, taking into account
several laparoscopically-assessed sites of disease to objectively predict the chance of
achieving optimal cytoreduction. This model gives each parameter (omental cake, diaphragmatic
carcinosis, peritoneal carcinosis, superficial liver metastases, stomach infiltration, bowel
infiltration and mesenteric retraction) a value of 2 (see "Statistical considerations").
Finally, we undertook a study to validate the performance of the model in a larger
prospective series of AOC patients. For each laparoscopic parameter we have discussed and
agreed the characteristics able to define a positive evaluation, especially those identifying
the critical areas of surgical resection. This study confirmed that with a PI cut-off > 8,
the percentage of inappropriate "no exploration" is 0, while the percentage of unnecessary
exploration equals to 40.5%. In conclusion the laparoscopic subjective ability to predict
optimal cytoreduction was definitively turned into an objective score.
Moreover, the laparoscopic score (Fagotti's score) has been validated externally in a centre
different from the one where it was developed [19,20], demonstrating that predictive
qualities of PI remain unchanged even if applied on a different population centre, with own
surgical background. This report suggests that the limit of subjectiveness, characterizing
the evaluation of ovarian cancer spread, tend to a solution.
Study design Phase I
1. Patients with a clinical/radiological suspicious primary advanced ovarian/peritoneal
cancer should undergo the following pre-operative staging examinations: haematological
and chemical parameters, including CA 125 serum levels, thorax-abdomen-pelvis CT-scan.
2. If inclusion criteria will be satisfied, an informed consent has to be signed before any
surgical procedure.
3. Patients will be then submitted to an open laparoscopy with at least one ancillary
trocar to evaluate the seven parameters previously described, assigning each one a score
to obtain a global predictive index. PI score is calculated based on. A video has to be
registered.
4. Patients'characteristics, including histological diagnosis, should be reported in the
enclosed summarizing schedule. On the other hand, no additional information regarding
the following treatment of the patient, i.e. abandoned vs. upfront surgery, RT or follow
up are required during the preliminary phase 1.
5. Send Laproscopic form, pre-operative documents and Video to the coordinating centre.
For preliminary phase 1, a minimum number of 10 patients has to be enrolled in one year. Time
and number of cases can be increased to reach the established accuracy rate > 80%.
The fairness of the laparoscopic PI value obtained in each specific centre will be
established through the revision of film material by the coordinating centre and the accuracy
will be calculated after realizing 10 cases. The centres achieving an accuracy rate > 80% can
enter in the second phase of the study. Other centres will require further cases until the
achievement of the objective.
All enrolled patients who receive the expected treatment will be considered
intention-to-treat-population (ITT).
Participation to preliminary Phase I of the study is a necessary but not sufficient
pre-requisite to adhere to Phase II. A new approval from the Ethical Committee is needed to
enter into the Phase II.
Centres can withdraw from the study in any time, but a written explanation is required.
Phase II Only centres participating to Phase I can enter into Phase II trial, after achieving
an accuracy rate >75%. A new approval from the Ethical Committee is needed to enter into the
Phase II.
1. Patients with a clinical/radiological suspicious primary advanced ovarian/peritoneal
cancer should undergo the following pre-operative staging examinations: haematological
and chemical parameters, including CA 125 serum levels, thorax-abdomen-pelvis CT-scan.
2. If inclusion criteria will be satisfied, an informed consent has to be signed before any
surgical procedure (Appendix 1).
3. Patients will be then submitted to an open laparoscopy with at least one ancillary
trocar to evaluate the seven parameters previously described, assigning each one a score
to obtain a global predictive index. PI score is calculated based on Appendix 2. No
videos need to be registered.
4. Patients'characteristics, including histological diagnosis, should be reported in the
enclosed summarizing schedule (Appendix 3). In this case additional information
regarding the following treatment of the patient, i.e. abandoned vs. upfront surgery, RT
and site, type of surgical procedures needed to obtain optimal cytoreduction, and follow
up data are required (Appendix 4).
5. Send Appendices 2 and 3 to the coordinating centre. For phase 2 study, a minimum number
of 100 patients should be enrolled in two years, overall.
Results regarding the primary objective of the study can be obtained immediately after the
enrolment of all the patients. Secondary objectives of the study need at least a minimum
follow-up of 3 years.
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