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INFORM2 Study Uses Nivolumab and Entinostat in Children and Adolescents With High-risk Refractory Malignancies (INFORM2 NivEnt)

Primary Purpose

CNS Tumor, Solid Tumor

Status
Recruiting
Phase
Phase 1
Locations
International
Study Type
Interventional
Intervention
Nivolumab and Entinostat
Sponsored by
University Hospital Heidelberg
About
Eligibility
Locations
Arms
Outcomes
Full info

About this trial

This is an interventional treatment trial for CNS Tumor focused on measuring high-risk solid tumors, high-risk CNS tumors

Eligibility Criteria

6 Years - 21 Years (Child, Adult)All SexesDoes not accept healthy volunteers

Inclusion Criteria:

  • Children and adolescents with refractory/relapsed/progressive high-risk

    • CNS tumors: medulloblastoma, ependymoma, ATRT, ETMR, pediatric high grade glioma (including DIPG) or other pediatric embryonal CNS tumors OR
    • solid tumors: neuroblastoma, nephroblastoma, rhabdoid tumor, embryonal or alveolar rhabdomyosarcoma, other embryonal small round blue cell tumors including pediatric type (bone) sarcoma or other pediatric type solid tumors OR
    • Children and adolescents with newly diagnosed high grade glioma (HGG) in the context of a constitutional mismatch repair deficiency syndrome after maximum safe surgical resection with no established standard of care treatment option with curative intention available. In addition in France: ineligible to radiotherapy
  • No standard of care treatment available
  • Age at registration ≥ 6 to ≤ 21 years
  • Molecular analysis for biomarker identification (SNV load, PDL1 mRNA expression, MYC/N amplification) in laboratories complying with DIN EN ISO/IEC 17025 or similar via INFORM molecular diagnostic platform or equivalently valid molecular pipeline
  • Biomarker determined using whole exome sequencing (SNV load), RNA-sequencing (PDL1 mRNA expression), whole genome- or whole exome sequencing (MYC/N amplification)
  • In case molecular analysis was not performed via INFORM Registry molecular pipeline: transfer of molecular data (whole exome and RNA sequencing)
  • Time between biopsy/puncture/resection of the current refractory/relapsed/progressive tumor and registration ≤ 24 weeks. In patients receiving therapy not impacting biomarker stratification, time between biopsy/puncture/resection of the current refractory/relapsed/progressive tumor and registration of ≤ 36 weeks is allowed
  • Disease that is measurable as defined by RANO criteria or RECIST v1.1 (as appropriate).
  • Life expectancy > 3 months, sufficient general condition score (Lansky ≥ 70 or Karnofsky ≥ 70). Transient states like infections can be accepted, and also stable disabilities resulting from disease/surgery (hemiparesis, amputations etc.) can be accepted and will not be considered for Lansky/Karnofsky assessments.
  • Laboratory requirements:

    • Hematology:

      • absolute granulocytes ≥ 1.0 × 109/l (unsupported)
      • platelets ≥ 100 × 109/l & stable
      • hemoglobin ≥ 8 g/dl or ≥ 4.96 mmol/L
    • Biochemistry:

      • Total bilirubin ≤ 1.5 x upper limit of normal (ULN)
      • AST(SGOT) ≤ 3.0 x ULN
      • ALT(SGPT) ≤ 3.0 x ULN
      • serum creatinine ≤ 1.5 x ULN for age
  • ECG: normal QTc interval according to Bazett formula < 440ms
  • Patient is able to swallow oral study medication
  • Ability of patient and/or legal representative(s) to understand the character and individual consequences of clinical trial
  • Females of childbearing potential must have a negative serum or urine pregnancy test within 7 days prior to initiation of treatment. Sexually active women of childbearing potential must agree to use acceptable and appropriate contraception during the study and for at least 6 months after the last study treatment administration. Sexually active male patients must agree to use a condom during the study and for at least 3 months after the last study treatment administration.
  • Absence of any psychological, familial, sociological or geographical condition potentially hampering compliance with the study protocol and follow-up schedule; those conditions should be discussed with the patient before registration in the trial
  • Before patient screening and registration, written informed consent, also concerning data and blood transfer, must be given according to ICH/GCP, and national/local regulations.
  • No prior therapy with the combination of immune checkpoint inhibitors and HDACi
  • BSA ≥ 0.9m2
  • Phase I: molecular analysis performed and biomarker status known (mutational load, PD-L1 mRNA expression AND MYC(N) amplification status).
  • Phase II: molecular analysis performed, biomarker status known (mutational load, PD-L1 mRNA expression AND MYC(N) amplification status) and stratification according to the following criteria:

    • Group A: high mutational load (defined as > 100 somatic SNVs/exome) based on whole exome sequencing OR
    • Group B: high PD-L1 mRNA expression (defined as reads per million total reads per kilobase of exon model (RPKM) > 3) based on RNA sequencing OR
    • Group C: Focal MYC(N) amplification based on whole genome sequencing or whole exome sequencing OR
    • Group D: Patients with biomarker low tumors according to the definitions of group A-C.

Exclusion Criteria:

  • Patients with CNS tumors or metastases who are neurologically unstable despite adequate treatment (e.g. convulsions).
  • Patients with low-grade gliomas or tumors of unknown malignant potential are not eligible
  • Evidence of > Grade 1 recent CNS hemorrhage on the baseline MRI scan.
  • Participants with bulky CNS tumor on imaging are ineligible; bulky tumor is defined as:

    • Tumor with any evidence of uncal herniation or severe midline shift
    • Tumor with diameter of > 6 cm in one dimension on contrast-enhanced MRI
    • Tumor that in the opinion of the investigator, shows significant mass effect
  • Previous allogeneic bone marrow, stem cell or organ transplantation
  • Diagnosis of immunodeficiency
  • Diagnosis of prior or active autoimmune disease
  • Evidence of interstitial lung disease
  • Any contraindication to oral agents or significant nausea and vomiting, malabsorption, or significant small bowel resection that, in the opinion of the investigator, would preclude adequate absorption.
  • Known history of human immunodeficiency virus (HIV) (HIV 1/2 antibodies). Known active hepatitis B (e.g., hepatitis B surface antigen-reactive) or hepatitis C (e.g., hepatitis C virus ribonucleic acid [qualitative]). Patients with past hepatitis B virus (HBV) infection or resolved HBV infection (defined as the presence of hepatitis B core antibody [HBc Ab] and absence of HBsAg) are eligible. HBV DNA test must be performed in these patients prior to study treatment. Patients positive for hepatitis C virus (HCV) antibody are eligible only if polymerase chain reaction is negative for HCV RNA.
  • Clinically significant, uncontrolled heart disease
  • Major surgery within 21 days of the first dose. Gastrostomy, ventriculo-peritoneal shunt, endoscopic ventriculostomy, tumor biopsy and insertion of central venous access devices are not considered major surgery, but for these procedures, a 48 hour interval must be maintained before the first dose of the investigational drug is administered.
  • Any anticancer therapy (e.g., chemotherapy, HDACi (including valproic acid), DNA methyltransferase inhibitors, other immunotherapy, targeted therapy, biological response modifiers, endocrine anticancer therapy or radiotherapy) within 2 weeks or at least 5 half- lives (whichever is longer) of study drug administration.
  • Radiologically confirmed radiotherapy induced pseudoprogression in CNS tumors
  • Traditional herbal medicines; these therapies are not fully studied and their use may result in unanticipated drug-drug interactions that may cause or confound the assessment of toxicity. As part of the enrollment/informed consent procedures, the patient will be counseled on the risk of interactions with other agents, and what to do if new medications need to be prescribed or if the patient is considering a new over-the- counter medicine or herbal product. For information on CYP substrates and P-gp inhibitors or inducers see section 5.8.
  • History of hypersensitivity to the investigational medicinal product or to any drug with similar chemical structure or to any excipient present in the pharmaceutical form (including benzamide) of the investigational medicinal product
  • Participation in other ongoing clinical trials.
  • Pregnant or lactating females.
  • Presence of underlying medical condition (e.g. gastrointestinal disorders or electrolyte disturbances) that in the opinion of the Investigator or Sponsor could adversely affect the ability of the subject to comply with or tolerate study procedures and/or study therapy, or confound the ability to interpret the tolerability of combined administration of entinostat and nivolumab in treated subjects
  • Patients receiving systemic steroid therapy or any other form of immunosuppressive therapy within 7 days prior to the first dose of study treatment. The use of physiologic doses of corticosteroids (up to 5 mg/m2/day prednisone equivalent) may be approved after consultation with the Sponsor. No patient will be allowed to enroll in this trial more than once.

Sites / Locations

  • Sydney Children's HospitalRecruiting
  • Children's Hospital at WestmeadRecruiting
  • Royal Children's HospitalRecruiting
  • Perth Children's HospitalRecruiting
  • St. Anna Children's HospitalRecruiting
  • Institut CurieRecruiting
  • Augsburg University HospitalRecruiting
  • Charité University Medicine BerlinRecruiting
  • Essen University HospitalRecruiting
  • Hannover Medical SchoolRecruiting
  • Hopp Children's Cancer Center Heidelberg (KiTZ)Recruiting
  • Prinses Máxima CentrumRecruiting
  • Karolinska InstituteRecruiting
  • Children's Hospital ZurichRecruiting

Arms of the Study

Arm 1

Arm Type

Experimental

Arm Label

Nivolumab and Entinostat

Arm Description

Combination Study of Nivolumab and Entinostat

Outcomes

Primary Outcome Measures

Phase I: Dose Limiting Toxicity (DLT) of the combination treatment.
A dose limiting toxicity (DLT) is defined as any AE according to the definitions and exceptions listed below that is related to the administration of the combination of investigational agents occurring during the priming week and first cycle of combination treatment (first 5 weeks) in phase I of the trial. A study participant will be considered evaluable for a DLT if at least 2 doses of nivolumab and 4 doses of entinostat were administered during the first 5 weeks (5 weeks normally incorporate the priming week and 1 cycle of planned combination treatment). Participants who discontinue treatment or have treatment delays preventing them from receiving the above defined minimal amount of treatment in the first cycle of combination treatment for reasons unrelated to study drug toxicity, are not evaluable for DLT and will be replaced in enrollment (maximum number of replacement subjects will be 3 per dose level).
Phase II: Best response (CR or PR)
Best response (CR or PR) will be based on RANO criteria for all primary CNS tumors and RECIST for non-CNS tumors, defined for each patient as the best response under study combination therapy during the first 6 cycles (assessment every 2 cycles). Calcified or intra-osseous (osteo)sarcoma target lesions which were progressive before initiation of treatment and show SD on response evaluation (confirmation through a subsequent scan at least 4 weeks later) will be considered as a responder.

Secondary Outcome Measures

Duration of Response (DOR)
DOR will be evaluated for all patients who experienced (confirmed) response. Starting time point will be the time when best response was determined.
Disease Control Rate (DCR)
DCR will be evaluated in addition, also using iRECIST and iRANO.
Stable disease (SD)
SD will be evaluated in addition, also using iRECIST and iRANO.
Progression-free survival (PFS)
The event-time endpoint PFS will be estimated using the Kaplan-Meier method, considering all the patients who started the treatment, whatever their compliance to treatment, including if the treatment was stopped prematurely for a reason other than disease progression. 95%-Confidence intervals will be provided for the Kaplan-Meier estimates.
Time to Response (TTR)
The event-time endpoint TTR will be estimated using the Kaplan-Meier method, considering all the patients who started the treatment, whatever their compliance to treatment, including if the treatment was stopped prematurely for a reason other than disease progression. 95%-Confidence intervals will be provided for the Kaplan-Meier estimates.
Overall Survival (OS)
The event-time endpoint OS will be estimated using the Kaplan-Meier method, considering all the patients who started the treatment, whatever their compliance to treatment, including if the treatment was stopped prematurely for a reason other than disease progression. 95%-Confidence intervals will be provided for the Kaplan-Meier estimates.
Immune related Response Rate (RR) measured by iRECIST criteria and iRANO criteria
As a secondary endpoint for patients who continued treatment beyond progression in case of clinical benefit, response as assessed by iRECIST or iRANO will be performed.
Maximum Plasma Time (Tmax)
Time to reach the maximum concentration (hr).
Maximum Plasma Concentration (Cmax)
The peak plasma concentration of a drug after Administration (ng/mL)
Half-life
The time required for the concentration of the drug to reach half of its original value (hr)
Area under the curve (AUC)
The integral of the concentration-time curve (ng/mL·hr)
total Clearance (CI/F)
The total body clearance will be equal to the renal clearance + hepatic clearance + lung clearance (L/h/m²)

Full Information

First Posted
February 4, 2019
Last Updated
November 8, 2022
Sponsor
University Hospital Heidelberg
Collaborators
German Cancer Research Center
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1. Study Identification

Unique Protocol Identification Number
NCT03838042
Brief Title
INFORM2 Study Uses Nivolumab and Entinostat in Children and Adolescents With High-risk Refractory Malignancies
Acronym
INFORM2 NivEnt
Official Title
INFORM2 Exploratory Multinational Phase I/II Combination Study of Nivolumab and Entinostat in Children and Adolescents With Refractory High-risk Malignancies
Study Type
Interventional

2. Study Status

Record Verification Date
November 2022
Overall Recruitment Status
Recruiting
Study Start Date
May 26, 2020 (Actual)
Primary Completion Date
June 30, 2024 (Anticipated)
Study Completion Date
June 30, 2025 (Anticipated)

3. Sponsor/Collaborators

Responsible Party, by Official Title
Principal Investigator
Name of the Sponsor
University Hospital Heidelberg
Collaborators
German Cancer Research Center

4. Oversight

Studies a U.S. FDA-regulated Drug Product
Yes
Studies a U.S. FDA-regulated Device Product
No
Product Manufactured in and Exported from the U.S.
Yes
Data Monitoring Committee
Yes

5. Study Description

Brief Summary
The aim of this trial is to determine preliminary activity of the combination treatment with nivolumab and entinostat in children and adolescents with high risk refractory/relapsed/progressive tumors harboring a high mutational load, high PD-L1 mRNA expression or focal MYC(N) amplification and explore activity in biomarker low tumors (low mutational load, low PD-L1 mRNA expression and non-MYC(N) amplified).
Detailed Description
Compared to adult cancers, most pediatric cancers carry a relatively low mutational burden. However, a small fraction of pediatric tumors in the INFORM registry cohort display a higher mutational burden. Truly hypermutated tumors, e.g. in the context of rare cancer predisposition syndromes, are reported to respond well to immune checkpoint inhibition. In addition to hypermutation, increased PD-L1 expression is associated with clinical responses to checkpoint inhibition. Increased PD-L1 mRNA expression is observed in a small fraction of pediatric patients in the INFORM registry cohort independent from mutational load. We hypothesize that pediatric tumors with a high mutational burden and/or high PD-L1 expression will respond to checkpoint inhibition. HDAC inhibition (HDACi) modifies T-cell regulation and can augment response to checkpoint inhibition by reducing the number of myeloid-derived suppressor cells and creating an immunogenic tumor microenvironment including induction of MHCI and neo-antigens. In vitro and in vivo models showed enhanced anti-tumor activity of the combination of checkpoint inhibition and HDACi compared to either agent alone. This provides a strong rationale to combine these drug classes. Furthermore, MYC- or NMYC-driven (referred to as MYC(N)) malignancies like very high-risk medulloblastomas or very high-risk neuroblastomas still have a dismal outcome. MYC is not only reported to upregulate PD-L1 and thereby a possible biomarker for checkpoint inhibition but also very compelling recent preclinical data strongly suggests that HDAC inhibitors are active against MYC amplified medulloblastoma in vitro and in vivo. In NMYC amplified neuroblastoma cell lines similar observations were made in vitro. Taken together, our results suggest that MYC(N)-driven tumors depend on HDAC and we hypothesize that MYC(N) status can serve as a biomarker for response prediction to a combinatorial treatment of checkpoint inhibition and HDAC inhibition. Pediatric patients aged 6-21 years with refractory/relapsed/progressive high-risk malignancies with a high mutational load (group A), with high PD-L1 mRNA expression (group B), with MYC(N) amplification (group C) and with a low mutational load, low PD-L1 mRNA expression and no MYC(N) amplification (Biomarker low group D) are eligible for this trial. Phase I determines the recommended phase 2 dose (RP2D) for the combination of the HDACi entinostat and the checkpoint inhibitor nivolumab for the age groups 6-11 and 12-21 years, respectively. Phase II investigates activity in 4 groups A, B, C, D. The duration of treatment is 12 cycles (1 cycle = 28 days), preceded by 1 priming week. In addition, a comprehensive accompanying research program investigates PD biomarkers for immune checkpoint and HDAC inhibition. Clinical trials investigating the combination of nivolumab and entinostat in children have not been reported so far.

6. Conditions and Keywords

Primary Disease or Condition Being Studied in the Trial, or the Focus of the Study
CNS Tumor, Solid Tumor
Keywords
high-risk solid tumors, high-risk CNS tumors

7. Study Design

Primary Purpose
Treatment
Study Phase
Phase 1, Phase 2
Interventional Study Model
Single Group Assignment
Model Description
Phase I: To determine the recommended phase II dose (RP2D) of the combination treatment with nivolumab and entinostat administered to adolescents 12-21 years with progressive, relapsed, refractory high-risk solid tumors and CNS tumors To determine the recommended phase II dose (RP2D) of the combination treatment with nivolumab and entinostat administered to children 6-11 years with progressive, relapsed, refractory high-risk solid tumors and CNS Tumors Phase II: To evaluate activity and safety of the combination treatment with nivolumab and entinostat in children and adolescents with refractory/relapsed/progressive high-risk solid tumors and CNS tumors with: Group A: a high mutational load (> 100 somatic SNVs/exome) Group B: high PD-L1 mRNA expression (RPKM by RNA-Seq > 3) Group C: Focal MYC(N) amplification Group D: Patients with biomarker low tumors according to the definitions of group A-C.
Masking
None (Open Label)
Allocation
N/A
Enrollment
128 (Anticipated)

8. Arms, Groups, and Interventions

Arm Title
Nivolumab and Entinostat
Arm Type
Experimental
Arm Description
Combination Study of Nivolumab and Entinostat
Intervention Type
Drug
Intervention Name(s)
Nivolumab and Entinostat
Intervention Description
Patients entering phase I will receive one week entinostat without nivolumab (priming phase) before receiving the combination treatment of nivolumab and entinostat.
Primary Outcome Measure Information:
Title
Phase I: Dose Limiting Toxicity (DLT) of the combination treatment.
Description
A dose limiting toxicity (DLT) is defined as any AE according to the definitions and exceptions listed below that is related to the administration of the combination of investigational agents occurring during the priming week and first cycle of combination treatment (first 5 weeks) in phase I of the trial. A study participant will be considered evaluable for a DLT if at least 2 doses of nivolumab and 4 doses of entinostat were administered during the first 5 weeks (5 weeks normally incorporate the priming week and 1 cycle of planned combination treatment). Participants who discontinue treatment or have treatment delays preventing them from receiving the above defined minimal amount of treatment in the first cycle of combination treatment for reasons unrelated to study drug toxicity, are not evaluable for DLT and will be replaced in enrollment (maximum number of replacement subjects will be 3 per dose level).
Time Frame
5 weeks
Title
Phase II: Best response (CR or PR)
Description
Best response (CR or PR) will be based on RANO criteria for all primary CNS tumors and RECIST for non-CNS tumors, defined for each patient as the best response under study combination therapy during the first 6 cycles (assessment every 2 cycles). Calcified or intra-osseous (osteo)sarcoma target lesions which were progressive before initiation of treatment and show SD on response evaluation (confirmation through a subsequent scan at least 4 weeks later) will be considered as a responder.
Time Frame
Change in 24 weeks
Secondary Outcome Measure Information:
Title
Duration of Response (DOR)
Description
DOR will be evaluated for all patients who experienced (confirmed) response. Starting time point will be the time when best response was determined.
Time Frame
Phase II: maximum of 48 weeks
Title
Disease Control Rate (DCR)
Description
DCR will be evaluated in addition, also using iRECIST and iRANO.
Time Frame
Phase II: maximum of 48 weeks
Title
Stable disease (SD)
Description
SD will be evaluated in addition, also using iRECIST and iRANO.
Time Frame
Phase II: maximum of 12 cycles (each cycle is 28 days)
Title
Progression-free survival (PFS)
Description
The event-time endpoint PFS will be estimated using the Kaplan-Meier method, considering all the patients who started the treatment, whatever their compliance to treatment, including if the treatment was stopped prematurely for a reason other than disease progression. 95%-Confidence intervals will be provided for the Kaplan-Meier estimates.
Time Frame
4 years
Title
Time to Response (TTR)
Description
The event-time endpoint TTR will be estimated using the Kaplan-Meier method, considering all the patients who started the treatment, whatever their compliance to treatment, including if the treatment was stopped prematurely for a reason other than disease progression. 95%-Confidence intervals will be provided for the Kaplan-Meier estimates.
Time Frame
Phase II: maximum of 12 cycles (each cycle is 28 days)
Title
Overall Survival (OS)
Description
The event-time endpoint OS will be estimated using the Kaplan-Meier method, considering all the patients who started the treatment, whatever their compliance to treatment, including if the treatment was stopped prematurely for a reason other than disease progression. 95%-Confidence intervals will be provided for the Kaplan-Meier estimates.
Time Frame
Phase II: maximum of 48 weeks
Title
Immune related Response Rate (RR) measured by iRECIST criteria and iRANO criteria
Description
As a secondary endpoint for patients who continued treatment beyond progression in case of clinical benefit, response as assessed by iRECIST or iRANO will be performed.
Time Frame
Phase II: maximum of 48 weeks
Title
Maximum Plasma Time (Tmax)
Description
Time to reach the maximum concentration (hr).
Time Frame
one week
Title
Maximum Plasma Concentration (Cmax)
Description
The peak plasma concentration of a drug after Administration (ng/mL)
Time Frame
one week
Title
Half-life
Description
The time required for the concentration of the drug to reach half of its original value (hr)
Time Frame
one week
Title
Area under the curve (AUC)
Description
The integral of the concentration-time curve (ng/mL·hr)
Time Frame
one week
Title
total Clearance (CI/F)
Description
The total body clearance will be equal to the renal clearance + hepatic clearance + lung clearance (L/h/m²)
Time Frame
one week
Other Pre-specified Outcome Measures:
Title
Exploratory: circulating tumor DNA (ctDNA)
Description
Assessment of circulating Tumor DNA in peripheral blood.
Time Frame
At baseline and every odd cycle (Cycle 3 - 12) and every third cycle (Cycle 13 - 24) (each cycle is 28 days).
Title
Exploratory: Response prediction
Description
Response prediction in a co-clinical PDX model and drug testing program
Time Frame
4 years
Title
Exploratory: Immune phenotyping (FACS Panel) and Luminex cytokine panel
Description
Immune phenotyping (FACS Panel) and Luminex cytokine panel in peripheral blood.
Time Frame
At baseline, after the priming week and after 5 weeks of initiation of therapy
Title
Exploratory: mRNA expression
Description
Analyze mRNA Expression data for Tumor infiltrating immune cell populations
Time Frame
4 years
Title
Exploratory: gene signatures
Description
Analyze gene signature in whole exome data
Time Frame
4 years
Title
Exploratory: cryptic transcription start sites
Description
Test induction of cryptic transcription start sites
Time Frame
At baseline, after priming week and after 5 weeks of initiation of therapy
Title
Exploratory: Single nucleotide variant (SNV) load
Description
Determination of SNV load by different methods (WES, Panel-Seq)
Time Frame
4 years

10. Eligibility

Sex
All
Minimum Age & Unit of Time
6 Years
Maximum Age & Unit of Time
21 Years
Accepts Healthy Volunteers
No
Eligibility Criteria
Inclusion Criteria: Children and adolescents with refractory/relapsed/progressive high-risk CNS tumors: medulloblastoma, ependymoma, ATRT, ETMR, pediatric high grade glioma (including DIPG) or other pediatric embryonal CNS tumors OR solid tumors: neuroblastoma, nephroblastoma, rhabdoid tumor, embryonal or alveolar rhabdomyosarcoma, other embryonal small round blue cell tumors including pediatric type (bone) sarcoma or other pediatric type solid tumors OR Children and adolescents with newly diagnosed high grade glioma (HGG) in the context of a constitutional mismatch repair deficiency syndrome after maximum safe surgical resection with no established standard of care treatment option with curative intention available. In addition in France: ineligible to radiotherapy No standard of care treatment available Age at registration ≥ 6 to ≤ 21 years Molecular analysis for biomarker identification (SNV load, PDL1 mRNA expression, MYC/N amplification) in laboratories complying with DIN EN ISO/IEC 17025 or similar via INFORM molecular diagnostic platform or equivalently valid molecular pipeline Biomarker determined using whole exome sequencing (SNV load), RNA-sequencing (PDL1 mRNA expression), whole genome- or whole exome sequencing (MYC/N amplification) In case molecular analysis was not performed via INFORM Registry molecular pipeline: transfer of molecular data (whole exome and RNA sequencing) Time between biopsy/puncture/resection of the current refractory/relapsed/progressive tumor and registration ≤ 24 weeks. In patients receiving therapy not impacting biomarker stratification, time between biopsy/puncture/resection of the current refractory/relapsed/progressive tumor and registration of ≤ 36 weeks is allowed Disease that is measurable as defined by RANO criteria or RECIST v1.1 (as appropriate). Life expectancy > 3 months, sufficient general condition score (Lansky ≥ 70 or Karnofsky ≥ 70). Transient states like infections can be accepted, and also stable disabilities resulting from disease/surgery (hemiparesis, amputations etc.) can be accepted and will not be considered for Lansky/Karnofsky assessments. Laboratory requirements: Hematology: absolute granulocytes ≥ 1.0 × 109/l (unsupported) platelets ≥ 100 × 109/l & stable hemoglobin ≥ 8 g/dl or ≥ 4.96 mmol/L Biochemistry: Total bilirubin ≤ 1.5 x upper limit of normal (ULN) AST(SGOT) ≤ 3.0 x ULN ALT(SGPT) ≤ 3.0 x ULN serum creatinine ≤ 1.5 x ULN for age ECG: normal QTc interval according to Bazett formula < 440ms Patient is able to swallow oral study medication Ability of patient and/or legal representative(s) to understand the character and individual consequences of clinical trial Females of childbearing potential must have a negative serum or urine pregnancy test within 7 days prior to initiation of treatment. Sexually active women of childbearing potential must agree to use acceptable and appropriate contraception during the study and for at least 6 months after the last study treatment administration. Sexually active male patients must agree to use a condom during the study and for at least 3 months after the last study treatment administration. Absence of any psychological, familial, sociological or geographical condition potentially hampering compliance with the study protocol and follow-up schedule; those conditions should be discussed with the patient before registration in the trial Before patient screening and registration, written informed consent, also concerning data and blood transfer, must be given according to ICH/GCP, and national/local regulations. No prior therapy with the combination of immune checkpoint inhibitors and HDACi BSA ≥ 0.9m2 Phase I: molecular analysis performed and biomarker status known (mutational load, PD-L1 mRNA expression AND MYC(N) amplification status). Phase II: molecular analysis performed, biomarker status known (mutational load, PD-L1 mRNA expression AND MYC(N) amplification status) and stratification according to the following criteria: Group A: high mutational load (defined as > 100 somatic SNVs/exome) based on whole exome sequencing OR Group B: high PD-L1 mRNA expression (defined as reads per million total reads per kilobase of exon model (RPKM) > 3) based on RNA sequencing OR Group C: Focal MYC(N) amplification based on whole genome sequencing or whole exome sequencing OR Group D: Patients with biomarker low tumors according to the definitions of group A-C. Exclusion Criteria: Patients with CNS tumors or metastases who are neurologically unstable despite adequate treatment (e.g. convulsions). Patients with low-grade gliomas or tumors of unknown malignant potential are not eligible Evidence of > Grade 1 recent CNS hemorrhage on the baseline MRI scan. Participants with bulky CNS tumor on imaging are ineligible; bulky tumor is defined as: Tumor with any evidence of uncal herniation or severe midline shift Tumor with diameter of > 6 cm in one dimension on contrast-enhanced MRI Tumor that in the opinion of the investigator, shows significant mass effect Previous allogeneic bone marrow, stem cell or organ transplantation Diagnosis of immunodeficiency Diagnosis of prior or active autoimmune disease Evidence of interstitial lung disease Any contraindication to oral agents or significant nausea and vomiting, malabsorption, or significant small bowel resection that, in the opinion of the investigator, would preclude adequate absorption. Known history of human immunodeficiency virus (HIV) (HIV 1/2 antibodies). Known active hepatitis B (e.g., hepatitis B surface antigen-reactive) or hepatitis C (e.g., hepatitis C virus ribonucleic acid [qualitative]). Patients with past hepatitis B virus (HBV) infection or resolved HBV infection (defined as the presence of hepatitis B core antibody [HBc Ab] and absence of HBsAg) are eligible. HBV DNA test must be performed in these patients prior to study treatment. Patients positive for hepatitis C virus (HCV) antibody are eligible only if polymerase chain reaction is negative for HCV RNA. Clinically significant, uncontrolled heart disease Major surgery within 21 days of the first dose. Gastrostomy, ventriculo-peritoneal shunt, endoscopic ventriculostomy, tumor biopsy and insertion of central venous access devices are not considered major surgery, but for these procedures, a 48 hour interval must be maintained before the first dose of the investigational drug is administered. Any anticancer therapy (e.g., chemotherapy, HDACi (including valproic acid), DNA methyltransferase inhibitors, other immunotherapy, targeted therapy, biological response modifiers, endocrine anticancer therapy or radiotherapy) within 2 weeks or at least 5 half- lives (whichever is longer) of study drug administration. Radiologically confirmed radiotherapy induced pseudoprogression in CNS tumors Traditional herbal medicines; these therapies are not fully studied and their use may result in unanticipated drug-drug interactions that may cause or confound the assessment of toxicity. As part of the enrollment/informed consent procedures, the patient will be counseled on the risk of interactions with other agents, and what to do if new medications need to be prescribed or if the patient is considering a new over-the- counter medicine or herbal product. For information on CYP substrates and P-gp inhibitors or inducers see section 5.8. History of hypersensitivity to the investigational medicinal product or to any drug with similar chemical structure or to any excipient present in the pharmaceutical form (including benzamide) of the investigational medicinal product Participation in other ongoing clinical trials. Pregnant or lactating females. Presence of underlying medical condition (e.g. gastrointestinal disorders or electrolyte disturbances) that in the opinion of the Investigator or Sponsor could adversely affect the ability of the subject to comply with or tolerate study procedures and/or study therapy, or confound the ability to interpret the tolerability of combined administration of entinostat and nivolumab in treated subjects Patients receiving systemic steroid therapy or any other form of immunosuppressive therapy within 7 days prior to the first dose of study treatment. The use of physiologic doses of corticosteroids (up to 5 mg/m2/day prednisone equivalent) may be approved after consultation with the Sponsor. No patient will be allowed to enroll in this trial more than once.
Central Contact Person:
First Name & Middle Initial & Last Name or Official Title & Degree
Melanie Heiss
Phone
+496221 56 7255
Email
melanie.heiss@kitz-heidelberg.de
First Name & Middle Initial & Last Name or Official Title & Degree
Ruth Witt
Email
ruth.witt@kitz-heidelberg.de
Facility Information:
Facility Name
Sydney Children's Hospital
City
Randwick
State/Province
New South Wales
ZIP/Postal Code
2031
Country
Australia
Individual Site Status
Recruiting
Facility Contact:
First Name & Middle Initial & Last Name & Degree
David Ziegler
Facility Name
Children's Hospital at Westmead
City
Westmead
State/Province
New South Wales
ZIP/Postal Code
2145
Country
Australia
Individual Site Status
Recruiting
Facility Contact:
First Name & Middle Initial & Last Name & Degree
Dinisha Govender
Facility Name
Royal Children's Hospital
City
Parkville
State/Province
Victoria
ZIP/Postal Code
3052
Country
Australia
Individual Site Status
Recruiting
Facility Contact:
First Name & Middle Initial & Last Name & Degree
Dong Anh Khuong Quang
Facility Name
Perth Children's Hospital
City
Nedlands
State/Province
Western Australia
ZIP/Postal Code
6009
Country
Australia
Individual Site Status
Recruiting
Facility Contact:
First Name & Middle Initial & Last Name & Degree
Nick Gottardo
Facility Name
St. Anna Children's Hospital
City
Vienna
ZIP/Postal Code
1090
Country
Austria
Individual Site Status
Recruiting
Facility Contact:
First Name & Middle Initial & Last Name & Degree
Caroline Hutter
Facility Name
Institut Curie
City
Paris
ZIP/Postal Code
75005
Country
France
Individual Site Status
Recruiting
Facility Contact:
First Name & Middle Initial & Last Name & Degree
Gudrun Schleiermacher
Facility Name
Augsburg University Hospital
City
Augsburg
ZIP/Postal Code
86156
Country
Germany
Individual Site Status
Recruiting
Facility Contact:
First Name & Middle Initial & Last Name & Degree
Michael Frühwald, Prof. Dr. Dr.
Facility Name
Charité University Medicine Berlin
City
Berlin
Country
Germany
Individual Site Status
Recruiting
Facility Contact:
First Name & Middle Initial & Last Name & Degree
Anne Thorwarth, Dr. med.
Facility Name
Essen University Hospital
City
Essen
Country
Germany
Individual Site Status
Recruiting
Facility Contact:
First Name & Middle Initial & Last Name & Degree
Uta Dirksen, Prof. Dr. med.
Facility Name
Hannover Medical School
City
Hannover
Country
Germany
Individual Site Status
Recruiting
Facility Contact:
First Name & Middle Initial & Last Name & Degree
Andreas Beilken, Dr. med.
Facility Name
Hopp Children's Cancer Center Heidelberg (KiTZ)
City
Heidelberg
ZIP/Postal Code
69120
Country
Germany
Individual Site Status
Recruiting
Facility Contact:
First Name & Middle Initial & Last Name & Degree
INFORM2 Team
Email
inform2@kitz-heidelberg.de
First Name & Middle Initial & Last Name & Degree
Olaf Witt, Prof. Dr. med.
Facility Name
Prinses Máxima Centrum
City
Utrecht
Country
Netherlands
Individual Site Status
Recruiting
Facility Contact:
First Name & Middle Initial & Last Name & Degree
Jasper van der Lugt
Facility Name
Karolinska Institute
City
Stockholm
Country
Sweden
Individual Site Status
Recruiting
Facility Contact:
First Name & Middle Initial & Last Name & Degree
Anna Nilsson
Facility Name
Children's Hospital Zurich
City
Zurich
ZIP/Postal Code
8032
Country
Switzerland
Individual Site Status
Recruiting
Facility Contact:
First Name & Middle Initial & Last Name & Degree
Nicolas Gerber

12. IPD Sharing Statement

Plan to Share IPD
Yes
IPD Sharing Plan Description
The pseudonymized data will be shared for transparency reasons in the context of publications and after publication with other physicians and scientists (national and international academia) to promote and accelerate research on causes and treatment development of oncological diseases. Requests for access to pseudonymized patient data for non-INFORM-related scientific purposes will be reviewed by a Data Access Committee consisting of the INFORM Board, and the participating investigators. A positive statement of the respective ethic committee and a signed data protection commitment are requested. Requests should be addressed to the coordinating investigator Prof. Olaf Witt. Results of scientific research based on the INFORM2 NivEnt data may be used for academic teaching, research and scientific publications or presentations at scientific meetings.
Citations:
PubMed Identifier
32503469
Citation
van Tilburg CM, Witt R, Heiss M, Pajtler KW, Plass C, Poschke I, Platten M, Harting I, Sedlaczek O, Freitag A, Meyrath D, Taylor L, Balasubramanian GP, Jager N, Pfaff E, Jones BC, Milde T, Pfister SM, Jones DTW, Kopp-Schneider A, Witt O. INFORM2 NivEnt: The first trial of the INFORM2 biomarker driven phase I/II trial series: the combination of nivolumab and entinostat in children and adolescents with refractory high-risk malignancies. BMC Cancer. 2020 Jun 5;20(1):523. doi: 10.1186/s12885-020-07008-8.
Results Reference
derived

Learn more about this trial

INFORM2 Study Uses Nivolumab and Entinostat in Children and Adolescents With High-risk Refractory Malignancies

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