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strategic reasons (not due to lack of efficacy or safety issues)
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This is a modular, first time in patient, open-label, multicentre study of OMO-1, administered orally, alone and in combination with anti-cancer treatments, in patients with locally advanced, unresectable or metastatic solid malignancies.
The study will consist of a number of study modules. The initial Module 1 will evaluate OMO-1 as monotherapy to provide dose(s) and schedule(s) for further Modules of combination therapy.
Module 2 will evaluate OMO-1 in combination with small molecule EGFR-TKIs.
Study modules will consist of a Part A (dose finding) and an optional Part B (cohort expansion). The option to start Part B and add further modules will be the decision of the safety review committee, based on emerging preclinical anti-tumour data and, safety and tolerability information from the study as a whole.
For all modules, Part A cohorts may be expanded by up to 12 additional patients at doses (at or above the MBAD) that have been confirmed to be tolerated. These patients will have mandatory paired biopsies to assess the tumour for relevant PDc biomarkers, and to explore further the tolerability, safety and PK activity at these doses.
In all combination modules, the dose of each combination agent investigated will not exceed their current recommended dose. The starting dose of OMO-1 in combination modules will not exceed the one currently tolerated in Module 1 (monotherapy). For cohorts in which OMO-1 is dosed in combination with cytotoxic chemotherapy, dosing will not continue once the cycles of chemotherapy have been completed.
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| Label | Type | Description | Intervention Names |
|---|---|---|---|
| Module 1 Monotherapy Multiple Ascending Dose | Experimental | Multiple ascending dose cohorts dosing OMO-1 (bid) monotherapy in all comer patients up to a maximally tolerated or maximally feasible dose |
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| Module 1 Monotherapy Paired Biopsy | Experimental | Paired biopsy cohort(s) dosing OMO-1 (bid) monotherapy in patients selected for MET dependent tumours at minimally biologically active doses and above |
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| Module 1 Monotherapy Expansion Cohort(s) | Experimental | Expansion cohort(s) dosing OMO-1 (bid) monotherapy in patients selected for MET dependent tumours at recommended phase 2 dose (RP2D) |
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| Module 2 Combination with EGFR-TKI Multiple Ascending Dose | Experimental | Multiple ascending dose cohorts dosing OMO-1 (bid) in combination with EGFR-TKI in MET amplified patients up to a maximally tolerated or maximally feasible dose |
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| Module 2 Combination with EGFR-TKI Paired Biopsy | Experimental | Paired biopsy cohort(s) dosing OMO-1 (bid) in combination with EGFR-TKI in MET amplified patients at minimally biologically active doses and above |
| Name | Type | Description | Arm Group Labels | Other Names |
|---|---|---|---|---|
| OMO-1 | Drug | OMO-1 is a small molecule inhibitor of the enzymatic activity of the MET receptor tyrosine kinase |
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| Measure | Description | Time Frame |
|---|---|---|
| Incidence of treatment-emergent adverse events including dose-limiting toxicities | The proportion of patients with treatment-emergent (serious) adverse events including dose-limiting toxicity (DLT) | Baseline (C1D1) until 28 days after last administration of OMO-1 |
| Incidence of clinically significant abnormal measurements in physical examination, ophthalmological examination, vital signs, electrocardiogram (ECG), pregnancy test, lab tests and ECOG performance status | Physical examination and ophthalmological examination, vital signs; electrocardiogram (ECG); pregnancy test; haematology; clinical chemistry; urinalysis; plasma/renal makers; tumour markers; ECOG performance status | Screening until 28 days after last administration of OMO-1 |
| Measure | Description | Time Frame |
|---|---|---|
| Objective Response Rate | Objective response rate (ORR) by RECIST 1.1 - the proportion of patients with a confirmed reduction in tumour burden of a predefined amount (this will include short lived responses). | Screening until 28 days after last administration of OMO-1 |
| Percentage change in tumour size |
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Inclusion Criteria:
Aged at least 18 years
Provision of signed and dated, written informed consent.
Histological or cytological confirmation of locally advanced, unresectable or metastatic solid malignancy.
Performance status: Eastern Co-operative Oncology Group (ECOG) ≤1 and life expectancy ≥3 months.
Ability to swallow and retain oral medication.
Adequate organ functions.
Females of child-bearing potential:
Sexually active male patients must be willing to use barrier contraception
Exclusion Criteria:
In addition to the main core eligibility criteria, Module specific eligibility criteria include:
Module 1:
Patient recruited into the paired biopsy cohorts of Part A must have:
Patients recruited into Part B cohorts must have:
Module 2:
Patients recruited into Part A and Part B cohorts must have:
In addition, patients recruited into Module 2 Part B cohorts must have:
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| Name | Affiliation | Role |
|---|---|---|
| Martijn Lolkema, MD, PhD | Erasmus Medical Center | Principal Investigator |
| Facility | Status | City | State | ZIP | Country | Contacts |
|---|---|---|---|---|---|---|
| Mary Crowley Cancer Research | Dallas | Texas | 75251 | United States | ||
| University Hospital Antwerp |
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| ID | Term |
|---|---|
| D009369 | Neoplasms |
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A modular, multi-arm, multi-part, first time in patient study
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| Module 2 Combination with EGFR-TKI Expansion Cohort | Experimental | Expansion cohort dosing OMO-1 (bid) monotherapy in combination with EGFR-TKI in MET amplified patients at recommended phase 2 (combination) dose (RP2D) |
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Percentage change in tumour size will be determined for patients with measurable disease at baseline and is derived at each visit by the percentage change from baseline in the sum of the diameters of target lesions. The best percentage change in tumour size will be the patient's value representing the largest decrease (or smallest increase) from baseline in tumour size. |
| Screening until 28 days after last administration of OMO-1 |
| Maximal OMO-1 plasma concentration Cmax | Measurement of OMO-1 levels in plasma over time to calculate Cmax | Baseline (C1D1) and D1 in even cycles (C) until end of treatment (Part A) ; Baseline and C2D1 (Part B) |
| Area under the OMO-1 plasma concentration curve (AUC) | Measurement of OMO-1 levels in plasma over time to calculate AUC | Baseline (C1D1) and D1 in even cycles (C) until end of treatment (Part A) ; Baseline and C2D1 (Part B) |
| 'Proof of mechanism' and 'proof of principle' pharmacodynamic biomarkers, including markers of tumour cell proliferation and apoptosis. | Measurement of levels of 'Proof of mechanism' and 'proof of principle' pharmacodynamic biomarkers, including markers of tumour cell proliferation and apoptosis. | Screening until end of treatment |
| Edegem |
| Belgium |
| Institut Bergonie | Bordeaux | France |
| Hôpital La Timone | Marseille | France |
| lnstitut Gustave Roussy | Villejuif | France |
| Erasmus MC | Rotterdam | Netherlands |
| UMCU Universitair Medisch Centrum Utrecht | Utrecht | Netherlands |
| University College London Hospitals NHS Foundation Trust | London | United Kingdom |
| The Christie NHS Foundation Trust | Manchester | United Kingdom |
| The Newcastle Upon Tyne Hospitals NHS Foundation Trust | Newcastle upon Tyne | United Kingdom |
| University of Oxford, Department of Oncology | Oxford | United Kingdom |