search
Back to results

Oral AMXT 1501 Dicaprate in Combination With IV DFMO

Primary Purpose

Cancer, Solid Tumor, Solid Carcinoma

Status
Recruiting
Phase
Phase 1
Locations
International
Study Type
Interventional
Intervention
AMXT1501
DFMO
Sponsored by
Aminex Therapeutics, Inc.
About
Eligibility
Locations
Arms
Outcomes
Full info

About this trial

This is an interventional treatment trial for Cancer focused on measuring DFMO IV, AMXT 1501, DFMO

Eligibility Criteria

12 Years - undefined (Child, Adult, Older Adult)All SexesDoes not accept healthy volunteers

4.2. Inclusion Criteria Patients will be eligible for study participation only if they meet ALL the inclusion criteria applicable to their diagnosis.

4.2.1. Patients Diagnosed with Advanced Solid Tumor(s)

  1. Understand and sign written IRB-approved informed consent form and be willing to comply with all study procedures. Refer to Section 9.4 for additional information on informed consent.
  2. Diagnosed with unresectable, locally advanced, or metastatic solid tumor for which no standard therapy is recognized or for which standard therapy has failed. Planned tumor types for evaluation include:

    • Platinum resistant* ovarian cancer (including - primary peritoneal cancer and fallopian tube cancer)

    • Breast cancer
    • Papillary thyroid cancer
    • Head and neck cancer
    • Gastric cancer
    • Non-small cell lung cancer (NSCLC)
    • Mesothelioma: Pleural and peritoneal
    • Esophageal
    • Endometrial cancer
    • Cervical
    • Melanoma
    • Colorectal cancers (colon, rectal)

      • Platinum-resistant is defined as disease that may have responded to a platinum-containing chemotherapy regimen, but there is documentation of demonstrated recurrence within 6 months following the completion of that platinum-containing regimen. Progressive disease of epithelial ovarian cancer (EOC) following platinum-based therapy can be documented by physical examination, computed tomography (CT) scans, or a doubling of cancer antigen 125 (CA-125) levels from either 1) upper limit of normal (ULN) or 2) most recent nadir value (per the Rustin criteria [Rustin et al., 2011]). For CA-125 to be used as a criterion for progressive disease, the CA-125 level nadir must have been above the ULN. In addition, the CA-125 nadir level must have been confirmed by a second measurement at least 1 week after the initial measurement.
  3. Must be >18 years of age.
  4. Histologically or cytologically documented disease.
  5. Has evaluable or measurable disease by RECIST v1.1 or mRECIST criteria.
  6. Provide tumor tissue from biopsy taken during Screening period.
  7. Performance status of 0 or 1 on the Eastern Cooperative Oncology Group (ECOG) scale.

    4.2.2. Patients Diagnosed with Diffuse Intrinsic Pontine Glioma or Diffuse Midline Glioma (Must also meet other generally noted criteria as noted within the protocol.

  8. For patients <18 years of age, the parents or legal guardians must understand and sign the written IRB-approved informed consent form (ICF). The patient, if able, must understand and sign the IRB-approved consent (assent) and be willing to comply with all study procedures.

    For patients ≥18 years of age, the patient must understand and sign written IRB-approved ICF and be willing to comply with all study procedures.

    Refer to Section 9.4 for additional information on informed consent.

  9. Diagnosed with DIPG or DMG.

    a. Any anatomic site of origin is acceptable.

  10. Must be ≥12 years of age and >40 kg in body weight.
  11. Radiologically documented disease.

    a. Patient with refractory or progressive DIPG or DMG, defined as tumors with a pontine epicenter and diffuse involvement of at least 2/3 of the pons, are eligible without histologic confirmation.

    b. Patients with brainstem tumors that do not meet radiographic criteria or are not considered to be typical DIPG or DMG will be eligible if the tumors have been biopsied and proven to be high-grade gliomas (such as anaplastic astrocytoma, glioblastoma, H3 K27M-mutant DMG).

  12. Has evaluable or measurable disease by RANO or RAPNO criteria.
  13. Provide cerebrospinal fluid (CSF) sample. Patients with pontine lesions for whom a radiological diagnosis of DIPG, DMG or high-grade gliomas is made will be eligible without a CSF sample, although CSF sample is strongly encouraged.
  14. Performance score:

    a. Patients >16 years of age, Karnofsky score ≥50%. b. Patients ≥12 and ≤16 years of age, Lansky ≥50%. Note: Patients who are unable to walk because of paralysis, but who are up in a wheelchair, will be considered ambulatory for the purpose of assessing the performance score.

  15. Patients must have fully recovered from the acute toxic effects of all prior anti-cancer chemotherapy:

    1. Myelosuppressive chemotherapy: At least 21 days after the last dose of myelosuppressive chemotherapy (42 days if prior nitrosourea).
    2. Hematopoietic growth factors: At least 14 days after the last dose of a long-acting growth factor (e.g., Neulasta) or 7 days for short-acting growth factor.
    3. Biologic (anti-neoplastic agent): At least 7 days after the last dose of a biologic agent. For agents that have known adverse events occurring beyond 7 days after administration, this period must be extended beyond the time during which adverse events are known to occur. The duration of this interval must be discussed with the study chair.
    4. Immunotherapy: At least 42 days after the completion of any type of vaccination.
    5. Monoclonal antibodies: >21 days must have elapsed from the infusion of last dose of antibody and toxicity related to antibody therapy must be recovered to Grade ≤1.
    6. Radiation therapy: Patients must have had their last fraction of craniospinal or focal irradiation a minimum of 8-12 weeks prior to enrollment.
    7. Stem cell transplant: Patients must be ≥3 months since autologous stem cell transplant. Patients who received allogenic stem cell transplant or solid organ transplant are not eligible for study.

    4.2.3. All Patients - All patients are required to meet these inclusion exclusion criteria to be considered eligible for the study:

  16. Patient is able to take oral medications and willing to use an at-home infusion pump.
  17. Must have adequate bone marrow and renal/hepatic function at the screening and baseline visits, defined as:

    a. Absolute neutrophil count (ANC) ≥1.5×109/L without granulocyte colony-stimulating factor (G-CSF) support within 7 days preceding the lab assessment.

    b. Platelet ≥100×109/L, without transfusion within 7 days preceding the lab assessment.

    c. Hemoglobin ≥9 g/dL, without transfusion support within 7 days preceding the lab assessment.

    d. Activated partial thromboplastin time/ partial thromboplastin time (aPTT/PTT) ≤1.5×ULN.

    e. Aspartate aminotransferase (AST) and alanine aminotransferase (ALT) ≤2.5×ULN (if liver metastases are present, then ≤5×ULN is allowed).

    f. Total serum bilirubin ≤1.5×ULN, (except for patients with known Gilbert's Syndrome in whom ≤3×ULN is permitted).

    Confirmation of Gilbert's diagnosis requires elevated unconjugated (indirect) bilirubin values; normal complete blood count in previous 12 months, blood smear, and reticulocyte count; normal aminotransferases and alkaline phosphatase in previous 12 months.

    g. The patient is clinically euthyroid. h. Renal: Serum creatinine <1.5×ULN or creatinine clearance ≥60 mL/min/1.73 m2 for patients with serum creatinine levels >1.5×ULN.

    i. Any Grade 3 or higher lab abnormalities should be discussed and approved by the Medical Monitor prior to enrollment (even if not considered clinically significant).

  18. Active secondary malignancies will not be allowed, with the exception of:

    1. Adequately treated basal cell carcinoma, SCC of the skin, or in situ cervical cancer;
    2. Adequately treated Stage 1 cancer from which the subject is currently in remission and has been in remission for ≥2 years;
    3. Low-risk prostate cancer with Gleason score <7 and prostate-specific antigen <10 ng/mL, or
    4. Any other cancer from which the patient has been disease-free for ≥3 years.
  19. Patient compliance and geographic proximity (as determined by the Principal Investigator [PI]) to allow adequate follow-up.
  20. Both male and female patients must be willing to consent to using highly effective contraception (refer to Section 5.7) prior to study entry, while on treatment, and at least 3 months thereafter.

4.3. Exclusion Criteria Patients will not be eligible for study participation if they meet ANY of the exclusion criteria.

4.3.1. Patients Diagnosed with Advanced Solid Tumor(s)

  1. Have a seizure disorder where >1 seizure has occurred within the last year.
  2. Patient with treated (surgically excised or irradiated) with stable brain metastases are eligible as long as the treatment was at least 4 weeks prior to initiation of study drug and baseline brain CT with contrast or magnetic resonance imaging (MRI) within 2 weeks of initiation of study drug is negative for new brain metastases. Patients with stable brain metastases must not require therapy with corticosteroids.
  3. Treatment with radiation therapy, surgery, chemotherapy, or immunotherapy within 4 weeks prior to study entry (6 weeks for nitrosoureas or Mitomycin C). Limited prior palliative radiation may be permissible no less than 2 weeks prior to C1D1 with approval from the Medical Monitor.

    4.3.2. Patients Diagnosed with Diffuse Intrinsic Pontine Glioma or Diffuse Midline Glioma

  4. Patients with seizure disorders may be enrolled if seizures are well-controlled, defined as no increase in seizure frequency in the prior 7 days.

    1. Anticonvulsants should be used as clinically indicated.
    2. The use of enzyme inducing anticonvulsants is not permitted.
  5. Patient with treated (surgically excised or irradiated) with stable brain metastases are eligible as long as the treatment was at least 8 to 12 weeks prior to initiation of study drug and baseline brain CT with contrast or MRI within 2 weeks of initiation of study drug is negative for new brain metastases. Patients receiving corticosteroids who have not been on a stable or decreasing dose of corticosteroid for at least 7 days prior to enrollment are not eligible.

4.3.3. All Patients 6. Have clinically significant cardiovascular disease (e.g., significant cardiac conduction abnormalities, uncontrolled hypertension, myocardial infarction, cardiac arrhythmia or unstable angina, New York Heart Association Grade 3 or greater congestive heart failure, serious cardiac arrhythmia requiring medication, Grade 2 or greater peripheral vascular disease, or history of cerebrovascular accident [CVA]) within 6 months of enrollment.

7. History or presence of an abnormal ECG that, in the Investigator's opinion, is clinically meaningful.

  1. Screening QTcF interval >480 ms is excluded. In the event that a single QTcF is >480 ms, the patient may enroll if the average QTcF for the 3 ECGs is <480 ms.
  2. For patients with an intraventricular conduction delay (QRS interval >120 ms), the JTc interval may be used in place of the QTcF with Sponsor approval. The JTc must be <340 ms if JTc is used in place of the QTcF.
  3. Patients with an intraventricular delay due to a left bundle branch block are excluded.

    Note: QTcF prolongation due to pacemaker may enroll if the JTc is normal. 8. Had major surgery, other than diagnostic surgery, within 4-weeks prior to Day 1.

    9. Have active bacterial, viral, or fungal infections requiring systemic therapy.

    10. Women who are pregnant or lactating. NOTE: Women of childbearing potential (WOCBP) must have a "negative" serum pregnancy test within 1 week prior to treatment.

a. Women not OCBP is defined as: i. Postmenopausal with >1 year since last menses and:

  1. If <65 years old, follicle-stimulating hormone (FSH) >40 mIU/mL.
  2. If ≥65 years old and not on hormone replacement therapy (HRT), FSH >30 mIU/mL.
  3. If ≥65 years old and on HRT, the FSH requirement in not applicable. Postmenopausal females on HRT will be allowed if HRT has been stable for ≥6 months prior to dosing of study drug(s).
  4. Written medical documentation of being sterilized (e.g., hysterectomy, double oophorectomy, bilateral salpingectomy) with the procedure performed ≥6 months prior to dosing study drug(s).

Note: Tubal ligation is not considered a form of permanent sterilization. 11. Patients may not have any unresolved toxicity >Grade 1 from previous anticancer therapy, except for stable chronic toxicities that are not expected to resolve (i.e., peripheral neuropathy, alopecia, etc.). Patients who have an ongoing requirement for thyroid replacement therapy from prior exposure to a checkpoint inhibitor but who are clinically euthyroid are permitted.

12. Have an unwillingness or inability to comply with procedures required in this protocol.

13. Current active liver disease from any cause, including hepatitis A (hepatitis A virus immunoglobulin M positive), hepatitis B (hepatitis B virus [HBV] surface antigen positive), or hepatitis C (hepatitis C virus [HCV] antibody positive, confirmed by HCV ribonucleic acid). Patients with HCV with undetectable virus after treatment are eligible. Patients with a prior history of HBV are eligible if quantitative polymerase chain reaction (PCR) for HBV DNA is negative. Note that elevated levels of biotin may interfere with viral serology testing.

14. Have a serious nonmalignant disease that, in the opinion of the Investigator or the Medical Monitor, could compromise protocol objectives.

15. Patients who are currently receiving any other investigational agent or who have received an investigational agent within the last 28 days, with the exception of any patient who participated in Study AMXT1501-101A.

16. Known GI disease or procedure that could interfere with the absorption of study drug, including inability to swallow whole capsules or conditions that may interfere with absorption. The Medical Monitor should be contacted for any questions regarding this exclusion criterion.

17. Patients who have exhibited allergic reactions to a similar structural compound, biological agent, or formulation.

18. Use of luteinizing hormone-releasing hormone (LHRH) agonist / antagonists are not permitted.

19. Use of biotin (i.e., Vitamin B7) or supplements containing biotin higher than the daily adequate intake of 30 µg (NIH-ODS 2020; Section 5.9.2.1).

Note: Patients who switch from a high dose to a dose of ≤30 µg/day are eligible for study entry.

20. Infection with human immunodeficiency virus (HIV)-1 or HIV-2. Exception: Patients with well-controlled HIV (e.g., CD4 >350/mm3 and undetectable viral load) are eligible.

Sites / Locations

  • Mayo Clinic - ArizonaRecruiting
  • Mayo Clinic - FloridaRecruiting
  • Mayo Clinic - MinnesotaRecruiting
  • Cincinnati Children's Hospital Medical CenterRecruiting
  • MD Anderson Cancer CenterRecruiting
  • Fred Hutch Cancer Center - Seattle Cancer Care AllianceRecruiting
  • Kids Cancer CentreRecruiting

Arms of the Study

Arm 1

Arm 2

Arm Type

Experimental

Experimental

Arm Label

Escalation

Expansion

Arm Description

Dose escalation of DFMO with AMXT1501 fixed dose will follow a 3 + 3 dose escalation design. The AMXT 1501 starting dose administered in the first cohort will be 1200mg total daily dose (200 mg capsules; 3 capsules in morning; 3 capsules in evening) along with IV DFMO administered in continuous infusion at 2mL/hr over a 28 days per cycle. The patient can be treated for additional 28 day treatment cycles as deemed appropriate by their study investigator. Dose escalation of DFMO alone will increase per cohort.

The expansion cohort will include up to 40 evaluable patients at a proposed RP2D level of AMXT1501 and DFMO defined by AMXT1501-101A study to further characterize safety at proposed RP2D dose level with repeat dosing, and characterize early anti-tumor activity.

Outcomes

Primary Outcome Measures

Determine DLTs and RP2Ds in AMXT 1501 in combination with IV DFMO
Indicate Number of patients with DLTs in AMXT1501 in combination with IV DFMO in patients with advanced cancer to determine the RP2D within the duration of the dose escalation period of the study as defined by the DLT definition of the protocol from baseline to end of Cycle 1
Determine safety and tolerability of AMXT1501 in combination with IV DFMO
To evaluate the safety and tolerability of AMXT1501 and IV DFMO combination in patients through collecting the number of patients with Treatment Related Adverse Events that occur in patients from first dose, AEs assessed by CTCAEv5.0

Secondary Outcome Measures

Determine the PK using AUC of AMXT 1501 and IV DFMO
To evaluate the pharmacokinetics (PK) of AMXT 1501 in combination with IV DFMO in patients
Determine the PK using Cmax of AMXT 1501 and IV DFMO
To evaluate the pharmacokinetics (PK) of AMXT 1501 and IV DFMO
Characterize investigator defined response Overall Response Rate (ORR) using RECIST v1.1
To characterize Investigator defined Overall Response Rate (ORR) using RECIST v1.1 response criteria.
Characterize investigator defined Duration of Response (DOR)
To characterize Investigator defined Duration of Response (DOR), using RECIST v1.1 response criteria and length of time (in days) from last study drug administration to time patient has progressive disease.
Characterize AMXT1501 and IV DFMO on the expression of immune related gene signatures
Evaluate the effects of AMXT1501 and IV DFMO on the expression of immune related gene signatures, immune cell phenotype by IHC, AMXT1501 and DFMO drug levels impact on polyamine levels

Full Information

First Posted
August 10, 2022
Last Updated
October 18, 2023
Sponsor
Aminex Therapeutics, Inc.
search

1. Study Identification

Unique Protocol Identification Number
NCT05500508
Brief Title
Oral AMXT 1501 Dicaprate in Combination With IV DFMO
Official Title
A Phase 1B/2A Study of the Safety, Tolerability and Initial Efficacy of Oral AMXT 1501 Dicaprate and Intravenous Difluoromethylornithine (DFMO) in Patients With Cancer
Study Type
Interventional

2. Study Status

Record Verification Date
October 2023
Overall Recruitment Status
Recruiting
Study Start Date
November 29, 2022 (Actual)
Primary Completion Date
June 30, 2024 (Anticipated)
Study Completion Date
September 30, 2024 (Anticipated)

3. Sponsor/Collaborators

Responsible Party, by Official Title
Sponsor
Name of the Sponsor
Aminex Therapeutics, Inc.

4. Oversight

Studies a U.S. FDA-regulated Drug Product
Yes
Studies a U.S. FDA-regulated Device Product
No
Data Monitoring Committee
Yes

5. Study Description

Brief Summary
A Phase 1B/2A study will be conducted to establish safety and dose level of AMXT 1501 dicaprate in combination with IV DFMO, in cancer patients.
Detailed Description
The objective of this study is to determine the safety and tolerability of oral AMXT 1501 dicaprate (AMXT1501) in combination with IV DFMO in patients with advanced solid tumors, or DIPG/DMG. Secondary objectives include characterization of plasma pharmacokinetics (PK), pharmacodynamic (PD), and other biomarker efficacy assessments of the impact of AMXT 1501 in combination with IV DFMO on polyamine uptake by circulating lymphocytes (blood cells). To these aims, the study will evaluate the safety, PK, PD, and other biomarker efficacy profiles of orally-administered AMXT 1501 and IV DFMO. Approximately, 56 patients will be enrolled to determine the maximum tolerated dose (MTD) and recommended phase 2 dose (RP2D) of AMXT 1501 and IV DFMO in combination. The MTD is defined as the highest dose level below at which dose escalation is stopped.

6. Conditions and Keywords

Primary Disease or Condition Being Studied in the Trial, or the Focus of the Study
Cancer, Solid Tumor, Solid Carcinoma, Advanced Cancer, DIPG Brain Tumor, Ovary Cancer, Breast Cancer, Papillary Thyroid Cancer, Head and Neck Cancer, Gastric Cancer, Nsclc, Mesotheliomas Pleural, Mesothelioma Peritoneum, Esophageal Cancer, Diffuse Midline Glioma, H3 K27M-Mutant, Endometrial Cancer, Cervical Cancer, Melanoma, Colorectal Cancer, Glioma, Malignant
Keywords
DFMO IV, AMXT 1501, DFMO

7. Study Design

Primary Purpose
Treatment
Study Phase
Phase 1, Phase 2
Interventional Study Model
Sequential Assignment
Masking
None (Open Label)
Allocation
Non-Randomized
Enrollment
56 (Anticipated)

8. Arms, Groups, and Interventions

Arm Title
Escalation
Arm Type
Experimental
Arm Description
Dose escalation of DFMO with AMXT1501 fixed dose will follow a 3 + 3 dose escalation design. The AMXT 1501 starting dose administered in the first cohort will be 1200mg total daily dose (200 mg capsules; 3 capsules in morning; 3 capsules in evening) along with IV DFMO administered in continuous infusion at 2mL/hr over a 28 days per cycle. The patient can be treated for additional 28 day treatment cycles as deemed appropriate by their study investigator. Dose escalation of DFMO alone will increase per cohort.
Arm Title
Expansion
Arm Type
Experimental
Arm Description
The expansion cohort will include up to 40 evaluable patients at a proposed RP2D level of AMXT1501 and DFMO defined by AMXT1501-101A study to further characterize safety at proposed RP2D dose level with repeat dosing, and characterize early anti-tumor activity.
Intervention Type
Drug
Intervention Name(s)
AMXT1501
Intervention Description
AMXT 1501 dicaprate is D-lys(palmitoyl)-spermine dicaprate salt in 200 mg (free base content) enterically-coated capsules
Intervention Type
Drug
Intervention Name(s)
DFMO
Other Intervention Name(s)
difluoromethyl ornithine monohydrochloride
Intervention Description
DFMO is DL-2-(difluoromethyl) ornithine monohydrochloride monohydrate provided as a 200 mg/mL aqueous solution in 20 mL vials.
Primary Outcome Measure Information:
Title
Determine DLTs and RP2Ds in AMXT 1501 in combination with IV DFMO
Description
Indicate Number of patients with DLTs in AMXT1501 in combination with IV DFMO in patients with advanced cancer to determine the RP2D within the duration of the dose escalation period of the study as defined by the DLT definition of the protocol from baseline to end of Cycle 1
Time Frame
1 year
Title
Determine safety and tolerability of AMXT1501 in combination with IV DFMO
Description
To evaluate the safety and tolerability of AMXT1501 and IV DFMO combination in patients through collecting the number of patients with Treatment Related Adverse Events that occur in patients from first dose, AEs assessed by CTCAEv5.0
Time Frame
1 year
Secondary Outcome Measure Information:
Title
Determine the PK using AUC of AMXT 1501 and IV DFMO
Description
To evaluate the pharmacokinetics (PK) of AMXT 1501 in combination with IV DFMO in patients
Time Frame
6 months
Title
Determine the PK using Cmax of AMXT 1501 and IV DFMO
Description
To evaluate the pharmacokinetics (PK) of AMXT 1501 and IV DFMO
Time Frame
6 months
Title
Characterize investigator defined response Overall Response Rate (ORR) using RECIST v1.1
Description
To characterize Investigator defined Overall Response Rate (ORR) using RECIST v1.1 response criteria.
Time Frame
6 months
Title
Characterize investigator defined Duration of Response (DOR)
Description
To characterize Investigator defined Duration of Response (DOR), using RECIST v1.1 response criteria and length of time (in days) from last study drug administration to time patient has progressive disease.
Time Frame
6 months
Title
Characterize AMXT1501 and IV DFMO on the expression of immune related gene signatures
Description
Evaluate the effects of AMXT1501 and IV DFMO on the expression of immune related gene signatures, immune cell phenotype by IHC, AMXT1501 and DFMO drug levels impact on polyamine levels
Time Frame
1 year
Other Pre-specified Outcome Measures:
Title
Evaluate AMXT1501 and DFMO on PD biomarker by evaluating the level/concentration of polyamine uptake.
Description
Will evaluate the effect of AMXT1501 and DFMO on pharmacodynamic (PD) biomarker of polyamine uptake in the blood starting at Cycle 1 through the end of Cycle 2 and again at the beginning of each new cycle.
Time Frame
6 months

10. Eligibility

Sex
All
Minimum Age & Unit of Time
12 Years
Accepts Healthy Volunteers
No
Eligibility Criteria
INCLUSION CRITERIA IMPORTANT NOTE- Younger 12-17 year old patients are also eligible for this study if they meet the noted DIPG or DMG criteria noted below, which is separate from Patient Diagnosed with Advanced Solid Tumors. Patients will be eligible for study participation only if they meet ALL the inclusion criteria applicable to their diagnosis. INCLUSION FOR PATIENTS DIAGNOSED WITH ADVANCED SOLID TUMORS Understand and sign written IRB-approved informed consent form and be willing to comply with all study procedures. Diagnosed with unresectable, locally advanced, or metastatic solid tumor for which no standard therapy is recognized or for which standard therapy has failed. Planned tumor types for evaluation include: Platinum resistant ovarian cancer (including - primary peritoneal cancer and fallopian tube cancer) Breast cancer Papillary thyroid cancer Head and neck cancer Gastric cancer Non-small cell lung cancer (NSCLC) Mesothelioma: Pleural and peritoneal Esophageal Endometrial cancer Cervical Melanoma Colorectal cancers (colon, rectal) Grade 4 Gliomas (including both IDH WT and IDH-mutant astrocytoma) Must be ≥18 years of age. Histologically or cytologically documented disease. Has evaluable or measurable disease by RECIST v1.1 or mRECIST criteria. o For patients with Grade 4 glioma, has evaluable or measurable disease by RANO (Appendix 5). Provide tumor tissue from biopsy taken during Screening period. Performance status of 0 or 1 on the Eastern Cooperative Oncology Group (ECOG) scale. INCLUSION FOR PATIENTS DIAGNOSED WITH DIPG OR DMG Patients must also meet other generally noted criteria as noted within the protocol For patients <18 years of age, the parents or legal guardians must understand and sign the written IRB-approved informed consent form (ICF). The patient, if able, must understand and sign the IRB-approved consent (assent) and be willing to comply with all study procedures. o For patients ≥18 years of age, the patient must understand and sign written IRB-approved ICF and be willing to comply with all study procedures. Diagnosed with DIPG or DMG. o Any anatomic site of origin is acceptable. Must be ≥12 years of age and >40 kg in body weight. Radiologically documented disease. (a) - Patient with refractory or progressive DIPG or DMG, defined as tumors with a pontine epicenter and diffuse involvement of at least 2/3 of the pons, are eligible without histologic confirmation. (b) - Patients with brainstem tumors that do not meet radiographic criteria or are not considered to be typical DIPG or DMG will be eligible if the tumors have been biopsied and proven to be high-grade gliomas (such as anaplastic astrocytoma, glioblastoma, H3 K27M-mutant DMG). Has evaluable or measurable disease by RANO or RAPNO criteria. o Has evaluable or measurable disease by RANO (for adults) or RAPNO (for children Provide cerebrospinal fluid (CSF) sample. Patients with pontine lesions for whom a radiological diagnosis of DIPG, or DMG is made will be eligible without a CSF sample, although CSF sample is strongly encouraged. Performance score: (a) Patients >16 years of age, Karnofsky score ≥50%. (b) Patients ≥12 and ≤16 years of age, Lansky ≥50%. Note: Patients who are unable to walk because of paralysis, but who are up in a wheelchair, will be considered ambulatory for the purpose of assessing the performance score. INCLUSION FOR ALL PATIENTS All patients are required to meet these inclusion exclusion criteria to be considered eligible for the study Patients must have fully recovered from the acute toxic effects of all prior anti-cancer chemotherapy: The following minimum periods from treatment apply: (a) Myelosuppressive chemotherapy: At least 21 days after the last dose of myelosuppressive chemotherapy (42 days if prior nitrosourea). (b) Hematopoietic growth factors: At least 14 days after the last dose of a long-acting growth factor (e.g., Neulasta) or 7 days for short-acting growth factor. (c) Biologic (anti-neoplastic agent): At least 7 days after the last dose of a biologic agent. For agents that have known adverse events occurring beyond 7 days after administration, this period must be extended beyond the time during which adverse events are known to occur. (d) Immunotherapy: At least 42 days after the completion of any type of vaccination. (e) Monoclonal antibodies: >21 days must have elapsed from the infusion of last dose of antibody and toxicity related to antibody therapy must be recovered to Grade ≤1. (f) Radiation therapy: Patients must have had their last fraction of craniospinal or focal irradiation a minimum of 8-12 weeks prior to enrollment. (g) Stem cell transplant: Patients must be ≥3 months since autologous stem cell transplant. Patients who received allogenic stem cell transplant or solid organ transplant are not eligible for study. Patient is able to take oral medications and willing to use an at-home infusion pump. Must have adequate bone marrow and renal/hepatic function at the screening and baseline visits, defined as: (a) Absolute neutrophil count (ANC) ≥1.5×109/L without granulocyte colony-stimulating factor (G-CSF) support within 7 days (b) Platelet ≥100×109/L, without transfusion within 7 days (c) Hemoglobin ≥9 g/dL, without transfusion support within 7 days (d) Activated partial thromboplastin time/ partial thromboplastin time (aPTT/PTT) ≤1.5×ULN. (e) Aspartate aminotransferase (AST) and alanine aminotransferase (ALT) ≤2.5×ULN (if liver metastases are present, then ≤5×ULN is allowed). (f) Total serum bilirubin ≤1.5×ULN, (except for patients with known Gilbert's Syndrome in whom ≤3×ULN is permitted). (g) The patient is clinically euthyroid. (h) Renal: Serum creatinine <1.5×ULN or creatinine clearance ≥60 mL/min/1.73 m2 for patients with serum creatinine levels >1.5×ULN. (i) Any Grade 3 or higher lab abnormalities should be discussed and approved by the Medical Monitor prior to enrollment (even if not considered clinically significant). Active secondary malignancies will not be allowed, with the exception of: (a) Adequately treated basal cell carcinoma, SCC of the skin, or in situ cervical cancer; (b) Adequately treated Stage 1 cancer from which the subject is currently in remission and has been in remission for ≥2 years; (c) Low-risk prostate cancer with Gleason score <7 and prostate-specific antigen <10 ng/mL, or (d) Any other cancer from which the patient has been disease-free for ≥3 years. Patient compliance and geographic proximity (as determined by the Principal Investigator [PI]) to allow adequate follow-up. Both male and female patients must be willing to consent to using highly effective contraception prior to study entry, while on treatment, and at least 3 months thereafter EXCLUSION CRITERIA Patients will not be eligible for study participation if they meet ANY of the exclusion criteria. Please note different criteria for patients with Advanced Solid Tumors (adults) vs patients with DIPG or DMG (pediatric) EXCLUSION FOR PATIENTS DIAGNOSED WITH ADVANCED SOLID TUMOR(S) Have a seizure disorder where >1 seizure has occurred within the last year. Patient with treated (surgically excised or irradiated) with stable brain metastases are eligible as long as the treatment was at least 4 weeks prior to initiation of study drug and baseline brain CT with contrast or magnetic resonance imaging (MRI) within 2 weeks of initiation of study drug is negative for new brain metastases. Patients with stable brain metastases must not require therapy with corticosteroids. Treatment with radiation therapy, surgery, chemotherapy, or immunotherapy within 4 weeks prior to study entry (6 weeks for nitrosoureas or Mitomycin C). Limited prior palliative radiation may be permissible no less than 2 weeks prior to C1D1 with approval from the Medical Monitor. EXCLUSION FOR PATIENTS WITH DIPG OR DMG - Patients with seizure disorders may be enrolled if seizures are well-controlled, defined as no increase in seizure frequency in the prior 7 days. Anticonvulsants should be used as clinically indicated. The use of enzyme inducing anticonvulsants is not permitted. EXCLUSION FOR ALL PATIENTS Patients with treated (surgically excised or irradiated) stable brain metastases are eligible as long as the treatment was at least 8 to 12 weeks prior to initiation of study drug and baseline brain CT with contrast or MRI within 2 weeks of initiation of study drug is negative for new brain metastases. Patients with brain metastases or who have Grade 4 glioma receiving corticosteroids who have not been on a stable or decreasing dose of corticosteroid for at least 7 days prior to enrollment are not eligible. Have clinically significant cardiovascular disease (e.g., significant cardiac conduction abnormalities, uncontrolled hypertension, myocardial infarction, cardiac arrhythmia or unstable angina, New York Heart Association Grade 3 or greater congestive heart failure, serious cardiac arrhythmia requiring medication, Grade 2 or greater peripheral vascular disease, or history of cerebrovascular accident [CVA]) within 6 months of enrollment. History or presence of an abnormal ECG that, in the Investigator's opinion, is clinically meaningful. Screening QTcF interval >480 ms is excluded. In the event that a single QTcF is >480 ms, the patient may enroll if the average QTcF for the 3 ECGs is <480 ms. For patients with an intraventricular conduction delay (QRS interval >120 ms), the JTc interval may be used in place of the QTcF with Sponsor approval. The JTc must be <340 ms if JTc is used in place of the QTcF. Patients with an intraventricular delay due to a left bundle branch block are excluded. Note: QTcF prolongation due to pacemaker may enroll if the JTc is normal Had major surgery, other than diagnostic surgery, within 4-weeks prior to Day 1. Have active bacterial, viral, or fungal infections requiring systemic therapy. Women who are pregnant or lactating: NOTE: Women of childbearing potential (WOCBP) must have a negative serum pregnancy test within 1 week prior to treatment. Women not OCBP is defined as (i) Postmenopausal with >1 year since last menses -- (a) If <65 years old, follicle-stimulating hormone (FSH) >40 mIU/mL. -- (b) If ≥65 years old and not on hormone replacement therapy (HRT), FSH >30 mIU/mL. -- (c)If ≥65 years old and on HRT, the FSH requirement is not applicable. Postmenopausal females on HRT will be allowed if HRT has been stable for ≥6 months prior to dosing of study drug(s). Written medical documentation of being sterilized (e.g., hysterectomy, double oophorectomy, bilateral salpingectomy) with the procedure performed ≥6 months prior to dosing study drug(s). Note: Tubal ligation is not considered a form of permanent sterilization. Patients may not have any unresolved toxicity >Grade 1 from previous anticancer therapy, except for stable chronic toxicities that are not expected to resolve (i.e., peripheral neuropathy, alopecia, etc.). Patients who have an ongoing requirement for thyroid replacement therapy from prior exposure to a checkpoint inhibitor but who are clinically euthyroid are permitted. Have an unwillingness or inability to comply with procedures required in this protocol. Current active liver disease from any cause, including hepatitis A (hepatitis A virus immunoglobulin M [Hep A IgM] positive), hepatitis B (hepatitis B virus [HBV] surface antigen positive), or hepatitis C (hepatitis C virus [HCV] antibody positive, confirmed by HCV ribonucleic acid). Patients with HCV with undetectable virus after treatment are eligible. Patients with a prior history of HBV are eligible if quantitative polymerase chain reaction (PCR) for HBV DNA is negative. Note that elevated levels of biotin may interfere with viral serology testing. Have a serious nonmalignant disease that, in the opinion of the Investigator or the Medical Monitor, could compromise protocol objectives. Patients who are currently receiving any other investigational agent or who have received an investigational agent within the last 28 days, with the exception of any patient who participated in Study AMXT1501-101A. Known GI disease or procedure that could interfere with the absorption of study drug, including inability to swallow whole capsules or conditions that may interfere with absorption. The Medical Monitor should be contacted for any questions regarding this exclusion criterion. Patients who have exhibited allergic reactions to a similar structural compound, biological agent, or formulation. Use of luteinizing hormone-releasing hormone (LHRH) agonist / antagonists are not permitted. Use of biotin (i.e., Vitamin B7) or supplements containing biotin higher than the daily adequate intake of 30 µg (NIH-ODS 2020; Section 5.9.2.1). NOTE: Patients who switch from a high dose to a dose of ≤30 µg/day are eligible for study entry. Infection with human immunodeficiency virus (HIV)-1 or HIV-2. o Exception: Patients with well-controlled HIV (e.g., CD4 >350/mm3 and undetectable viral load) are eligible.
Central Contact Person:
First Name & Middle Initial & Last Name or Official Title & Degree
Project Manager
Phone
910 240 3498
Email
priyanka.varma@iqvia.com
Overall Study Officials:
First Name & Middle Initial & Last Name & Degree
Sue Lee, MD
Organizational Affiliation
Aminex Therapeutics, Inc.
Official's Role
Study Chair
First Name & Middle Initial & Last Name & Degree
Michael Armstrong, MD
Organizational Affiliation
IQVIA Biotech
Official's Role
Study Director
Facility Information:
Facility Name
Mayo Clinic - Arizona
City
Phoenix
State/Province
Arizona
ZIP/Postal Code
85054
Country
United States
Individual Site Status
Recruiting
Facility Contact:
First Name & Middle Initial & Last Name & Degree
Cancer Center Clinical Trials Referral Office - from inside US (toll free)
Phone
855-776-0015
First Name & Middle Initial & Last Name & Degree
International patients
Phone
507-284-8884
Email
intl.mcr@mayo.edu
First Name & Middle Initial & Last Name & Degree
Jason S Starr, DO
Facility Name
Mayo Clinic - Florida
City
Jacksonville
State/Province
Florida
ZIP/Postal Code
32224
Country
United States
Individual Site Status
Recruiting
Facility Contact:
First Name & Middle Initial & Last Name & Degree
Cancer Center Clinical Trials Referral Office - from inside US (toll free)
Phone
855-776-0015
First Name & Middle Initial & Last Name & Degree
From Outside the US
Phone
507-284-8884
Email
intl.mcr@mayo.edu
Facility Name
Mayo Clinic - Minnesota
City
Rochester
State/Province
Minnesota
ZIP/Postal Code
55905
Country
United States
Individual Site Status
Recruiting
Facility Contact:
First Name & Middle Initial & Last Name & Degree
Cancer Center Clinical Trials Referral Office - from inside the US (toll free)
Phone
855-776-0015
First Name & Middle Initial & Last Name & Degree
Outside the US
Phone
507-284-8884
Email
intl.mcr@mayo.edu
First Name & Middle Initial & Last Name & Degree
Sani Kizilbash, MD, MPH
Facility Name
Cincinnati Children's Hospital Medical Center
City
Cincinnati
State/Province
Ohio
ZIP/Postal Code
45229
Country
United States
Individual Site Status
Recruiting
Facility Contact:
First Name & Middle Initial & Last Name & Degree
Clinical trials office
Phone
513-636-2799
Email
cancer@cchmc.org
First Name & Middle Initial & Last Name & Degree
Trent Hummel, MD
Facility Name
MD Anderson Cancer Center
City
Houston
State/Province
Texas
ZIP/Postal Code
77030
Country
United States
Individual Site Status
Recruiting
Facility Contact:
First Name & Middle Initial & Last Name & Degree
Rabia Khan
Phone
713-563-4667
Email
rkhan@mdanderson.org
First Name & Middle Initial & Last Name & Degree
Sarina Piha-Paul, MD
First Name & Middle Initial & Last Name & Degree
Wafik Zaky, MD
Facility Name
Fred Hutch Cancer Center - Seattle Cancer Care Alliance
City
Seattle
State/Province
Washington
ZIP/Postal Code
98109
Country
United States
Individual Site Status
Recruiting
Facility Contact:
First Name & Middle Initial & Last Name & Degree
LyTieng Huot
Email
phase1clinicaltrial@seattlecca.org
First Name & Middle Initial & Last Name & Degree
John Liao, MD
Facility Name
Kids Cancer Centre
City
Sydney
State/Province
New South Wales
Country
Australia
Individual Site Status
Recruiting
Facility Contact:
First Name & Middle Initial & Last Name & Degree
Sandra Montez
Phone
02-9382-1980
Email
sandra.montez@health.nsw.gov.au
First Name & Middle Initial & Last Name & Degree
David Ziegler, MD

12. IPD Sharing Statement

Plan to Share IPD
No

Learn more about this trial

Oral AMXT 1501 Dicaprate in Combination With IV DFMO

We'll reach out to this number within 24 hrs