Phase I Study of Cantrixil in Patients With Ovarian Cancer, Fallopian Tube Cancer or Primary Peritoneal Cancer.



Status:Recruiting
Conditions:Ovarian Cancer, Cervical Cancer, Cancer
Therapuetic Areas:Oncology
Healthy:No
Age Range:18 - Any
Updated:1/23/2019
Start Date:November 2016
End Date:December 2019
Contact:Dr James Garner, MBBS MBA
Email:james.garner@kaziatherapeutics.com
Phone:+612 94724101

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Phase I Study of Intra-peritoneal Cantrixil in Patients With Persistent or Recurrent Ovarian Cancer, Fallopian Tube Cancer or Primary Peritoneal Cancer.

The main purpose of this study is to determine the safety and feasibility of weekly
intra-peritoneal administration of Cantrixil to women with persistent or recurrent ovarian
cancer, Fallopian tube cancer or primary peritoneal cancer. The study also aims to determine
the maximum tolerated dose of Cantrixil in these patients when administered as a monotherapy
or a combination therapy.

This study is a progressive design with 2 discrete Parts (Part A: Dose escalation, Part B:
Dose expansion. Cycle 1/Part A is a dose-finding assessment (dose escalation) to establish
the MTD of Cantrixil when administered as a single dose once a week for 3 weeks. Cycle2/Part
A continues with 3 additional weekly doses of Cantrixil as a monotherapy before an assessment
of disease response. In Cycles 3 to 8/Part A, patients will be administered the same once
weekly dose of Cantrixil they tolerated in Cycles 1 and 2 (tolerance defined as no dose
limiting toxicities [DLTs] or unacceptable treatment-related adverse events [AEs]) in
combination with a limited range of standard chemotherapy agent(s), in order to assess the
safety and tolerability of Cantrixil in combination therapy. Standard chemotherapy drugs will
be administered at the standard efficacious doses to maintain optimum benefit of known drug
combinations for patients.

Once the MTD has been determined in Part A, an additional 12 patients will be recruited in an
expansion cohort for Part B. These patients will receive 2 cycles of Cantrixil monotherapy at
the MTD, followed by up to 6 cycles of combination therapy.

Patients enrolled into the respective parts of the study may not receive treatments under
different parts of the protocol.

To accommodate the intraperitoneal administration of Cantrixil, an in-dwelling, closed
catheter or port will be inserted if the patient does not already have one. For
intraperitoneal ports, the minimum period between port placement and the first administration
of Cantrixil must not be shorter than 7 days.

Patients should begin protocol treatment within a maximum of 28 days of enrolment (i.e.,
signing of consent form).

Patients will start at Dose Level 0 which is calculated to be the human equivalent of 10% of
the STD10 dose in rats (dose is 1/10 the severely toxic dose in 10% of rats tested). Dose
levels -1 and -2 will only be activated if there are 2 DLTs at the Dose Level 0 and -1,
respectively. Single patient cohorts will be treated with increasing doses of Cantrixil until
an AE is observed that meets the definition of a Dose Limiting Toxicity (DLT) or, in the
opinion of the Data Safety Monitoring Committee (DSMC) and the Investigator, is causally
related to study treatment and warrants observing additional patients at this dose level; at
this point the study will revert to a 3+3 rules based dose escalation study. Once the study
enters a 3+3 rules-based design, the study will not revert back to single patient cohorts.

If any unacceptable treatment-related AE or DLT is observed in any cycle, patients may be
dose reduced to the next lower dose level of Cantrixil for subsequent doses of therapy. If a
second unacceptable treatment-related AE or DLT is observed during any cycle within the same
patient, treatment for the patient with Cantrixil will be discontinued. Investigators may
continue with the standard chemotherapy at their discretion and if it is considered safe and
in the patient's best interest.

If any of the following unacceptable treatment-related AEs or DLTs are observed and unless
clearly unrelated to study treatment (e.g., disease progression), treatment at the allocated
Cantrixil dose will be discontinued and dose escalation may be considered:

- Hematologic toxicity

- Grade 4 neutropenia, lasting at least 5 days,

- Grade 3 or Grade 4 neutropenia associated with fever >38.5°C,

- Grade 4 thrombocytopenia lasting at least 5 days,

- Grade 3 thrombocytopenia associated with severe bleeding in the opinion of the
Investigator,

- Dose delay of ≥3 weeks due to failure to recover counts.

- Any Common Terminology Criteria for Adverse Events (CTCCTCAE) version 4.03 Grade 3 or
Grade 4 non haematological toxicity except:

- Alopecia

- Grade 3 abdominal pain deemed related to the port or catheter as determined by the
treating physician

- Grade 3 anorexia

- Grade 3 fatigue

- Grade 3 nausea and/or vomiting, or diarrhoea, lasting ≤48 hours with or without
maximal medical management.

- Grade 3 dehydration as a result of nausea and vomiting

- Grade 3 constipation

- Grade 3 metabolic abnormalities [hypokalaemia, hypomagnesemia, hypocalcaemia,
hypophosphatemia]) that recovers to Grade 1 or less within 48 hours with or without
medical management o• Other serious adverse events (SAEs) which, in the opinion of
the treating Investigator, are related to investigational product and necessitate
temporary or permanent cessation of administration o• Treatment delays of ≥3 weeks
due to any treatment-related non-haematological toxicity will constitute a DLT All
patients who discontinued from the study (i.e. are now Off Therapy/ End of Therapy)
treatment will progress to follow-up unless the patient withdraws consent.

The initiation of each new cycle of Cantrixil will be at the discretion of the Investigator
and will depend on the potential or measurable benefit to the patient assuming continued
tolerability and adequate organ function.

Cantrixil treatment will be stopped due to RECIST version 1.1 defined disease progression
observed after at least 4 cycles of therapy, recurrence of unacceptable toxicity after 1
Cantrixil dose reduction or patient consent withdrawal. Note that patients with progressive
disease at the end of 2 cycles of Cantrixil monotherapy will not be taken off therapy if
Cantrixil has been well tolerated. Pre-clinical data would suggest that the maximum benefit
from Cantrixil will be realised as a combination therapy, hence all patients will have the
opportunity to continue receiving Cantrixil as a combination therapy. Additionally, patients
receiving combination therapy that are observed to have progressive disease as identified by
RECIST version 1.1 criteria but who, in the opinion of the Investigator, continued to derive
clinical benefit may continue Cantrixil treatment. Patients may also be discontinued from
study treatment if the Investigator considers continuing therapy is not in the patient's best
interest. All patients discontinued from study treatment will progress to follow-up unless
the patient withdraws consent.

Tumour assessment via radiological imaging will be conducted during screening and every 6
weeks after the start of therapy, i.e. at the end of monotherapy and then after every 2
cycles of combination therapy. Either contrast-enhanced magnetic resonance imaging (MRI) or
contrast-enhanced computed tomography (CT) may be used, but once a modality is used at
baseline this must be used consistently for that patient throughout their participation on
the study. Other imaging is not mandatory, but may be performed if clinically indicated.

Adverse events will be monitored for the duration of the study from the time of informed
consent. Blood samples will be collected weekly for standard safety testing, or more
frequently if clinically relevant, during the study. Additional volumes of blood will be
collected before and after administration of Cantrixil for PK analysis (4 mL per time point
as per the proposed PK schedule and for any exploratory studies (at baseline, end of Cycle 2
and end of treatment, 15 to 20 mL at each time-point).

Inclusion Criteria:

1. Patients must have recurrent or persistent epithelial ovarian, fallopian tube, or
primary peritoneal cancer. The original diagnosis must be verified by a histology
report. All histological sub-types and all grades of disease are eligible to
participate; grade, histological sub-type and breast cancer susceptibility gene (BRCA)
status must be recorded at study entry.

2. Patients must be female and at least 18 years old.

3. Patients with malignant ascites are eligible to participate; paracentesis will be
conducted before the administration of Cantrixil. Drainage of the maximum volume of
ascites necessary for symptomatic relief should be performed according to local
standard operating procedures before administration of Cantrixil.

4. Patients must have completed at least two (2) or more prior therapies (including
adjuvant therapy) for their ovarian, Fallopian tube or primary peritoneal cancer prior
to participation in the current study; all prior therapies must be recorded at
baseline. Patients that have received prior intraperitoneal therapy are eligible for
this study.

5. Patients must have platinum-resistant relapsed disease, platinum refractory disease,
or have documented intolerance to platinum therapy. Patients will not be eligible
based on rising CA-125 levels alone, patients must have other clinical symptoms (such
as malignant ascites) or radiological tumour measurements that support disease
recurrence or progression.

6. At least 4 weeks must have passed from any previous therapy and any toxicities from
prior therapies (6 weeks for bevacizumab, nitrosoureas or mitomycin C treatment) must
have resolved to less than or equal to Common Terminology Criteria for Adverse Events
(CTCAE version 4.03) Grade 1 with the exception of alopecia, Grade 2 prior
platinum-therapy related neuropathy and Grade 2 anaemia.

7. Patients must have a performance status of Eastern Cooperative Oncology Group (ECOG) 0
to 2 and, in the Investigator's opinion, be able to complete at least a major part of
the study.

8. Patients must be willing and able to undergo insertion of a port or catheter for
intraperitoneal access; the type of port or catheter used will be recorded.

9. Patients may have measurable or non-measurable disease; disease response and
progression will be measured and assessed according to RECIST version 1.1 criteria
using contrast CT, MRI and CA 125 measurements.

10. Patients must have acceptable hepatic and marrow function as defined below:

- Absolute neutrophil count >1.5 x 109/L

- Platelets >100 x 109/L

- Total bilirubin; <2.5 times the institutional upper limit of normal (ULN)

- Haemoglobin (Hb) of >10 g/dL; patients with Hb >9g/dL will be considered for this
study if they have not received a transfusion or other bone marrow support.
Patients with Hb >10 g/dL that have received a recent transfusion will only be
eligible if there has been a wash-out period of 7 days for rhesus factor and 10
days for platelet transfusions, respectively.

- Aspartate aminotransferase (AST) (serum glutamic oxaloacetic transaminase
[SGOT])/ alanine aminotransferase (ALT) (serum glutamic pyruvate transaminase
[SGPT]) ≤2.5 x institutional ULN.

- Serum creatinine <1.5 x ULN

- Prothrombin time (PT) or international normalised ratio (INR) ≤1.5 x ULN and
activated partial thromboplastin time (aPTT) ≤1.5 x ULN if not on anticoagulation
treatments.

11. Patients must be willing and able to comply with all study requirements, including
treatment timing and/or nature of required assessments and treatment at designated
study centre.

12. Each participant must be adequately informed about the purpose of the study; potential
benefits and risks; their right to refuse participation or to withdraw consent at any
time; institutional affiliation and potential competing interests of the researcher;
and sources of study funding and have signed and dated a written informed consent
form.

Exclusion Criteria:

1. Patients who have had chemotherapy, biologic therapy, immunotherapy, or radiotherapy
within 4 weeks (6 weeks for bevacizumab, nitrosoureas or mitomycin C) prior to
entering the study.

2. Patients must not have had major surgery within 4 weeks prior to screening.

3. Patients may not have received any other investigational medicinal products (IMPs) or
participated in any other interventional clinical research studies within 3 months of
the first Cantrixil administration.

4. Patients receiving any medications or substances that are strong inhibitors or
inducers of cytochrome P450 (CYP)1A2, CYP2B6 and CYP3A4 or those substances with
narrow therapeutic index are not to be enrolled. These compounds are prohibited from
screening until completion of end of therapy or first post-treatment follow-up visit.
For a list of prohibited medications see the University of Indiana Clinical
Pharmacology Department's P450 Drug Interaction Table
(http://medicine.iupui.edu/clinpharm/ddis/main-table/). Note: the use of paclitaxel is
allowed, but only 24 hours after Cantrixil administration.

5. Patients at high risk of bowel perforation are excluded, including but not limited to
any one or more of the following;

- Patients with a recent history (previous 12 months) of bowel obstruction prior to
study entry

- Patients with CT scans that suggest invasion of bowel by tumour

- Patients with symptoms to suggest impending bowel obstruction

- Patients with prior whole abdominal radiotherapy

- Patients with chronic inflammatory bowel diseases such as Crohn's disease or
ulcerative colitis

6. Patients may not have uncontrolled or severe systemic diseases or psychiatric
conditions, which in the treating physician's opinion makes it unsafe for the patient
to participate in the study or would hinder compliance with the protocol. Screening
for chronic conditions is not required.

7. Patients that are pregnant, lactating, or unable to adopt adequate contraception are
excluded. Women of childbearing potential must have a negative pregnancy test within 7
days prior to screening.

8. Patients with a known history of hepatitis B or C.

9. Patients known to have tested positive for human immunodeficiency virus (HIV)

10. Patients with a known hypersensitivity to or serious reaction to benzopyrans are
excluded.
We found this trial at
4
sites
Providence, Rhode Island 02903
Principal Investigator: Don Dizon, MD FACP
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from
Providence, RI
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Dallas, Texas 75246
Principal Investigator: Minal Barve, MD
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from
Dallas, TX
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800 Northeast 10th Street
Oklahoma City, Oklahoma 73104
Principal Investigator: Dr K Moore
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from
Oklahoma City, OK
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Westmead, New South Wales 2145
Principal Investigator: Prof Paul Harnett, MBBS FRACP PhD
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from
Westmead,
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