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| ID | Type | Description | Link |
|---|---|---|---|
| 2023-503451-94 | Other Identifier | EU-CTR |
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| Name | Class |
|---|---|
| National Cancer Institute, France | OTHER_GOV |
| AstraZeneca | INDUSTRY |
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Multicentric, prospective, multi-indication, single-treatment arm, open-label phase II trial assessing the efficacy of MEDI5752
Multicentric, prospective, multi-indication, single-treatment arm, open-label phase II trial assessing the efficacy of MEDI5752.
Patients with mature tertiary lymphoid structures advanced solid tumors will be included in two independent cohorts:
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| Label | Type | Description | Intervention Names |
|---|---|---|---|
| Cohort A: patients with TLS+ IO-naïve solid tumors | Experimental | Participants with TLS+ IO-naïve solid tumors will be treated by MEDI5752 |
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| Cohort B: patients with TLS+ PD1/PDL1-experienced solid tumors | Experimental | Participants with TLS+ PD1/PDL1-experienced solid tumors will be treated by MEDI5752 |
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| Name | Type | Description | Arm Group Labels | Other Names |
|---|---|---|---|---|
| MEDI5752 | Drug | A treatment cycle consists of 3 weeks. MEDI5752 will be administered by intravenous infusion at a fixed dose on Day 1 of each cycle |
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| Measure | Description | Time Frame |
|---|---|---|
| Assessment of the antitumor activity of MEDI5752 (independently for eah cohort) | Antitumor activity will be assessed in terms of objective response rate within 24 weeks based on RECIST v1.1, independently for each cohort, and based on centralized radiological review. Objective response under treatment is defined as patients with confirmed complete response or confirmed partial response, as per RECIST v1.1, observed during treatment with the investigational product. Objective response rate is defined as the proportion of patients alive with objective response based on RECIST v1.1. Objective response is recorded from study treatment initiation until the end of treatment. | an expected average of 6 months |
| Measure | Description | Time Frame |
|---|---|---|
| 24-weeks clinical benefit rate (CBR) independently for each cohort | CBR is defined as the proportion of patients with clinical benefit at 6 months. Clinical benefit is defined as confirmed complete response, confirmed partial response or stable disease more than 24 weeks, defined as per RECIST v1.1. | 24 weeks |
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Inclusion Criteria:
Histologically confirmed solid tumor
IO-naïve patients (cohort A) OR patients with secondary resistance to PD1/PDL1 inhibitors (cohort B),
Patients in cohort B:
Presence of mature tertiary lymphoid structures (TLS) by IHC as described in protocol section 3.2.4. Except if presence of TLS has been already confirmed by Biopathological platform at Bergonié Institute, presence of TLS should be confirmed by central review based on FFPE tumor tissue sample,
Advanced unresectable or metastatic solid disease,
Measurable disease according to RECIST v1.1
At least one tumor site that can be biopsied for research purpose,
Age ≥ 18 years,
Body weight > 35 kg,
ECOG ≤ 1,
Life expectancy > 3 months,
Adequate hematological, renal, metabolic, hepatic and cardiac functions:
Disease progression on prior treatment, or previously untreated disease with no available acceptable treatment. Note that no more than three lines of systemic treatment for metastatic disease are allowed and that patients with oncogenic addiction must have progressed on prior approved regimens),
Recovery to grade ≤ 1 from any adverse event derived from previous treatment (excluding alopecia of any grade (according to the NCI-CTCAE, version 5.0),
Women of childbearing potential must have a negative serum pregnancy test within 7 days prior to study entry.
Women and men must agree to use at least one medically highly effective method of contraception from screening, throughout the treatment period
Voluntary signed and dated written informed consents prior to any specific study procedure,
Patients with a social security in compliance with the French law.
Exclusion Criteria:
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| Name | Role | Phone | Extension | |
|---|---|---|---|---|
| Antoine ITALIANO, MD, PhD | Contact | +33556333333 | a.italiano@bordeaux.unicancer.fr | |
| Simone MATHOULIN-PELISSIER, MD, PhD | Contact | s.mathoulin@bordeaux.unicancer.fr |
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| Facility | Status | City | State | ZIP | Country | Contacts |
|---|---|---|---|---|---|---|
| Institut Bergonie | Bordeaux | 33076 | France |
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| ID | Term |
|---|---|
| D000072717 | Tertiary Lymphoid Structures |
| ID | Term |
|---|---|
| D020763 | Pathological Conditions, Anatomical |
| D013568 | Pathological Conditions, Signs and Symptoms |
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2 independent single-arm, multicenter, phase II trials, based on a two-stage three-outcome design as described in Sargent et al.
Cohort A : patients with TLS+ IO-naïve solid tumor (miscellaneous) Cohort B: patients with TLS+ PD1/PDL1-experienced solid tumor (miscellaneous)
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| Best overall response (BoR) independently for each cohort |
BoR is defined as the best response recorded from the start of the study treatment until the end of treatment taking into account any requirement for confirmation. The best overall response is determined once all the data for the participant is known (RECIST v1.1). |
| Throughout the treatment period, an expected average of 6 months |
| Duration of response (DoR) independently for each cohort | DoR is defined as the time from documentation of tumor response (complete response/partial response whichever is first recorded) to disease progression, according to RECIST v1.1. DoR will be assessed in responder (confirmed CR / PR) patients only. | Throughout the treatment period, an expected average of 6 months |
| 1-year progression-free survival (PFS), independently for each cohort | PFS is defined as the time from study treatment initiation to the first occurrence of disease progression or death (of any cause), whichever occurs first | 1 year |
| 2-year progression-free survival (PFS), independently for each cohort | PFS is defined as the time from study treatment initiation to the first occurrence of disease progression or death (of any cause), whichever occurs first | 2 year |
| 1-year overall survival (OS), independently for each cohort | OS is defined as the time from study treatment initiation to death (of any cause) | 1 year |
| 2-year overall survival (OS), independently for each cohort | OS is defined as the time from study treatment initiation to death (of any cause) | 2 year |
| Safety profile, independently for each cohort: Common Terminology Criteria for Adverse Events version 5 | Number of participants with toxicity graded using the Common Terminology Criteria for Adverse Events version 5 | Throughout the treatment period, an expected average of 6 months |
| 24-weeks clinical benefit rate (iCBR) independently for each cohort as per iRECIST | iCBR is defined as the rate of patients with iCR, iPR or immune stable disease (iSD) | 24 weeks |
| Duration of response (iDoR) independently for each cohort as per iRECIST | iDoR is defined as the time from the date of the first response iCR/iPR (whichever is first recorded) to the date of PD (iUPD confirmed as iCPD) as per iRECIST. iDOR is defined for subjects with iCR or iPR. If a patient has iPR (#1) followed by a iUPD (#1) which is not confirmed, then a iPR (#2) followed by a iUPD (#2) which is confirmed at the next assessment, then the iDOR is calculated from iPR1 until iUPD2 | Throughout the treatment period, an expected average of 6 months |
| 1-year progression-free survival (iPFS), independently for each cohort as per iRECIST | o iPFS is defined as the time from study treatment initiation to the first occurrence of disease progression as per iRECIST or death (of any cause), whichever occurs first. The event date to be used for calculation of progression-free survival (iPFS) should be the first date at which progression criteria are met (ie, the date of iUPD) provided that iCPD is confirmed at the next assessment. If iUPD occurs, but is disregarded because of later iSD, iPR, or iCR, that iUPD date should not be used as the progression event date. If progression is not confirmed and there is no subsequent iSD, iPR, or iCR, then the iUPD date should still be used in the following scenarios: if the patient stops protocol treatment because they were not judged to be clinically stable, or no further response assessments are done (because of patient refusal, protocol noncompliance, or patient death); the next timepoint responses are all iUPD, and iCPD never occurs | 1 year |
| 2-year progression-free survival (iPFS), independently for each cohort as per iRECIST | o iPFS is defined as the time from study treatment initiation to the first occurrence of disease progression as per iRECIST or death (of any cause), whichever occurs first. The event date to be used for calculation of progression-free survival (iPFS) should be the first date at which progression criteria are met (ie, the date of iUPD) provided that iCPD is confirmed at the next assessment. If iUPD occurs, but is disregarded because of later iSD, iPR, or iCR, that iUPD date should not be used as the progression event date. If progression is not confirmed and there is no subsequent iSD, iPR, or iCR, then the iUPD date should still be used in the following scenarios: if the patient stops protocol treatment because they were not judged to be clinically stable, or no further response assessments are done (because of patient refusal, protocol noncompliance, or patient death); the next timepoint responses are all iUPD, and iCPD never occurs | 2 year |
| iORR independently for each cohort | iORR is defined as the rate of patients with immune complete or partial responses (iCR, iPR) as per iRECIST. iCR and iPR can be assigned after iUPD (immune unconfirmed progressive disease) has been documented as per iRECIST (Seymour et al) | Throughout the treatment period, an expected average of 6 months |