A Study of Therapeutic Iobenguane (131-I) and Vorinostat for Recurrent or Progressive High-Risk Neuroblastoma Subjects (OPTIMUM)

• ClinicalTrials.gov Identifier: NCT03561259
• Recruitment Status: Recruiting
• First Posted: June 19, 2018
• Last Update Posted: February 16, 2023
• Sponsor: Jubilant DraxImage Inc.
• Information provided by (Responsible Party): Jubilant DraxImage Inc.

Study Description

Brief Summary:

The purpose of this study is to evaluate the efficacy and safety of 131I-MIBG in combination with Vorinostat in patients with Recurrent or Progressive neuroblastoma

Condition or disease	Intervention/treatment	Phase
Neuroblastoma; Neuroectodermal Tumors; Neoplasms	Drug: 131I-MIBG; Drug: 131-MIBG + Vorinostat	Phase 2

Expanded Access : An investigational treatment associated with this study is available outside the clinical trial.   More info ...

Detailed Description:

OPTIMUM (MIBG 2014-01) is a Phase II, Two arm, non-randomized, open-label study of therapeutic 131I-iobenguane (131I-MIBG) as single agent or in combination with Vorinostat for the treatment of neuroblastoma. The study will be conducted in male and female subjects, greater than 1 year of age, with iobenguane avid, who have recurrent or progressive disease, regardless of overall response to frontline therapy, where frontline therapy includes a minimum of 4 cycles of induction therapy at any time prior to enrollment, high-risk neuroblastoma.

Subjects who are eligible for combination treatment will receive vorinostat 180 mg/m2/dose (maximum dose 400 mg) once daily for 14 days (Day -1 to Day 12) continuously.

Subjects will receive 18 mCi/kg of 131I-MIBG intravenously on Day 1.

If the subject qualifies, the subject will receive the second treatment course of 131I-MIBG in combination with vorinostat or 131I-MIBG alone (no sooner than 6 weeks following first treatment course). Subject must have an overall response of stable disease or better, as assessed by the Investigator, and meet certain predefined criteria to receive the second course of treatment.

Following a screening period of up to 4 weeks, the duration in the study treatment phase for an individual subject, who receives two treatments, is up to 26 weeks. For an individual subject, who receives one treatment only, the duration of the treatment phase is 16 weeks. In addition, there is a 2-year follow-up after the treatment phase, during which assessments will be performed to assess disease progression, as well as record adverse events.

Study Design

• Study Type: Interventional (Clinical Trial)
• Estimated Enrollment: 60 participants
• Allocation: Non-Randomized
• Intervention Model: Single Group Assignment
• Intervention Model Description: Two-arm, non-randomized, open-label study.
• Masking: None (Open Label)
• Primary Purpose: Treatment
• Official Title: A Phase II, Open Label, Two-Arm Study of Therapeutic Iobenguane (131I) as Single Agent or in Combination With Vorinostat for Recurrent or Progressive High- Risk Neuroblastoma Subjects (OPTIMUM TRIAL)
• Actual Study Start Date: October 21, 2019
• Estimated Primary Completion Date: December 1, 2023
• Estimated Study Completion Date: April 2025

Arms and Interventions

Arm	Intervention/treatment
Experimental: 131I-MIBG; 131I-MIBG	Drug: 131I-MIBG; Subjects will receive 18 mCi/kg of 131I-MIBG administered over 1.5 to 2 hours on Day 1 either a central line or a peripheral intravenous catheter. The maximum absolute dose of 131I-MIBG is determined by institution therapeutic limits and will not exceed 1,000 mCi. Subjects with an overall response of stable disease or better as assessed by the Investigator, and who meet certain protocol predefined criteria, may receive a second 18 mCi/kg 131I-MIBG treatment no sooner than 6 weeks following the first treatment.; Other Names: I-131 meta-iodobenzylguanidine; Iobenguane I-131 MIBG Injection
Experimental: 131I-MIBG + Vorinostat; 131I-MIBG + Vorinostat	Drug: 131-MIBG + Vorinostat; Subjects will receive vorinostat 180 mg/m2/dose (maximum dose 400 mg) once daily by mouth, NG, or G-tube on days -1 to +12 (14 total doses) for 14 days continuously. The 131I-MIBG treatment will be administered on day 1 via either a central line or a peripheral intravenous catheter over 1.5 to 2 hours. On day 1 of therapy, vorinostat should be taken 1 hour prior to the start of the 131I-MIBG infusion. Subjects with an overall response of stable disease or better, as assessed by the Investigator and who meet certain predefined criteria, may receive a second course of 18 mCi/kg 131I-MIBG combined with vorinostat (180 mg/m2) no sooner than 6 weeks following the first therapeutic 131I-MIBG treatment.

Outcome Measures

Primary Outcome Measures :

1. Overall Response [ Time Frame: 6 weeks after the last 131I-MIBG treatment which will either be the first or the second treatment course (131I-MIBG + vorinostat) and a confirmatory assessment at least 6 weeks thereafter (at least 12 weeks from the end of treatment) ]
   Overall response (Yes/No) is based on the International Neuroblastoma Response Criteria (INRC, published 2017). The INRC will be calculated based on 123I-iobenguane scans, CT/MRI, and bone marrow biopsies and aspirates. A "Yes" is defined as complete response, partial response or minor response. A "No" response is defined as stable disease or progressive disease.

Secondary Outcome Measures :

1. Overall Response at 6 weeks after 131I-MIBG treatment [ Time Frame: 6 weeks after the last 131I-MIBG treatment (first or second treatment of 131I-MIBG + vorinostat). ]
   The Revised INRC overall response (yes/no) defined as complete response, partial response, or minor response 6 weeks after the last131I-MIBG treatment which will either be the first treatment or the second treatment.
2. Durability of Effect of Overall Response (Yes/No) [ Time Frame: For all tumour assessment data collected throughout the study (up to the end of the 2-year follow-up)(131I-MIBG + vorinostat). ]
   Durability of effect with the INRC will be assessed as INRC for all tumor assessment data available including any data collected beyond 12 weeks after the last 131I-MIBG treatment which will either be the first treatment or the second treatment.
3. Relative Curie Extension Score [ Time Frame: 6 weeks after the last 131I-MIBG treatment which will either be the first or the second treatment course (131I-MIBG + vorinostat) ]
   Relative Curie Extension Score 6 weeks after the last MIBG 131I treatment, which will either be the first treatment or the second treatment.
4. Durability of Effect of Relative Curie Extension Score [ Time Frame: For all tumour assessment data collected throughout the study for both arms (up to the end of the 2-year follow-up). ]
   Durability of effect with the Relative Curie Extension Score will be assessed as the score for all tumor assessment data available including any data collected beyond 12 weeks after the last MIBG 131I treatment, which will either be the first treatment or the second treatment. The Relative Curie Extension Score will be calculated using the Baseline (Visit 2) Absolute Curie Extension Score. The Curie Extension Scores will be calculated from the results of the (123I) iobenguane scans.

Other Outcome Measures:

1. Incidence of Adverse Events (CTCAE Version 5.0) [ Time Frame: Up to 22 weeks ]
   Adverse events as graded according to the Common Terminology Criteria for Adverse Events (CTCAE) Version 5.0
2. Incidence of Serious Adverse Events [ Time Frame: Through study completion, up to 2.5 years. ]
   Percentage of subjects with hematological and nonhematological toxicities. Any relationship between the whole body radiation absorbed dose and nonhematological SAEs will also be assessed;
3. Whole Body Radiation Dose [ Time Frame: After each 131I-MIBG treatment for up to 120 hours. ]
   To assess radiation safety in terms of any potential relationship between the whole body radiation absorbed dose and nonhematological serious adverse events (SAEs)

Eligibility Criteria

• Ages Eligible for Study: 1 Year and older (Child, Adult, Older Adult)
• Sexes Eligible for Study: All
• Accepts Healthy Volunteers: No

Criteria

Inclusion Criteria:

1. Subjects with a diagnosis of iobenguane avid, high-risk neuroblastoma based on Revised INRC criteria at the time of study enrollment with recurrent or progressive disease at any time prior to enrollment, regardless of overall response to frontline therapy, where frontline therapy includes a minimum of 4 cycles of induction therapy at any time prior to enrollment.

2. May have had prior 131I-MIBG therapy, provided:

   1. It has been at least 6 months from the date of last 131I-MIBG ;
   2. Response was other than progressive disease on first restaging after 131I-MIBG ;
   3. Prior 131I-MIBG was given as monotherapy and not in combination with systemic anticancer agents;
   4. Cumulative lifetime dose of 131I-MIBG at enrollment does not exceed 18 mCi/kg.

3. All soft tissue lesions identified on CT/MRI scans must be iobenguane avid lesions on an (123I)-iobenguane scan, or

   1. any progressive non-iobenguane avid lesion is proven by biopsy to be a non-neuroblastoma lesion.
   2. any other non-avid lesion is comprised of a fibrotic or scarred mass as shown by routine imaging and confirmed by the investigator.
4. Adequate cryopreserved autologous peripheral blood stem cells or bone marrow (at least 2 aliquots of 2.0 × 10exp6 CD34/kg at the time of study enrollment).
5. If a male, must agree to use an adequate contraception method as deemed appropriate by the Investigator (e.g., vasectomy, condoms) or partner using effective contraception and to not donate sperm during the study and for 90 days after receiving the last dose of study drug.
6. If a female of childbearing potential, have a negative serum pregnancy test result prior to each dosing and, if sexually active, be practicing an effective method of birth control [e.g., intrauterine device, double-barrier method (i.e., diaphragm, or a cervical cap) with intravaginal spermicidal foam, cream or gel], or male partner sterilization throughout the study.
7. Age at study entry ≥1 year.
8. Previous platelet transfusions are permitted, as long as the subject has a platelet count ≥50,000/μL without transfusion support for at least 1 week.
9. Subjects must have a minimum pulse oximetry measurement of at least 94% at baseline.
10. An absolute neutrophil count ≥750/μL without growth factor for 5 days.
11. Liver function parameter results: total bilirubin ≤2 × upper limit of normal for age, and Serum alanine aminotransferase (glutamic-pyruvic transaminase) and serum aspartate aminotransferase (glutamic-oxaloacetic transaminase) ≤ 10 times the upper limit of normal (for all sites, the upper limit of normal for alanine aminotransferase is defined as 45 U/L).
12. Normal thyroid function as measured by T4 or TSH or have abnormal results that are not considered clinically important by the Investigator or may be receiving levothyroxine.
13. Cardiac Function: shortening fraction of ≥ 27% by echocardiogram or ejection fraction ≥ 50% documented by echocardiogram or radionuclide angiogram within 1 month prior to Visit 1 (Baseline).
14. Karnofsky Performance Status (for subjects >16 years of age) or the Lansky Performance Status Performance Status (for subjects 1 to 16 years of age) ≥50%.
15. Full recovery from the toxic effects of any prior therapy.

16. Coagulation Function:

    1. International Normalized Ratio (INR) < 1.5
    2. Partial thromboplastin time (PTT) < 1.5 times upper limit of normal.

Exclusion Criteria:

1. Subjects within 5 half-lives after any antibody-based immunotherapy, or have not recovered from effects of any biologic therapy.
2. Subjects <12 weeks after myeloablative therapy with autologous stem cell transplant.
3. Subjects who have had an allogeneic stem cell treatment less than 4 months from Visit 1 are excluded. Those who have received allogeneic stem cell treatment more than 4 months from Visit 1 must have recovered and have no active graft versus host disease (GVHD) to be eligible.
4. Subjects must not have received radiation for a minimum of 2 weeks prior to study enrollment. Subjects whose only site(s) of disease have been radiated are eligible as long as the subject has MIBG avidity 2 weeks after completion of radiation. A minimum of 12 weeks prior to study enrollment is required following prior large field radiation therapy (ie, craniospinal, whole abdominal, total lung, > 50% marrow space)
5. History of total body irradiation.
6. Subjects do not have adequate renal function defined as GFR ≥ 70 mL/min/1.73 m2 either by creatinine clearance or radioisotope direct measurement or by calculation with the Schwartz formula
7. Subjects who are on hemodialysis.
8. Pregnancy or breastfeeding.
9. Significant active infections including active hepatitis B, or hepatitis C infection, or known infection with human immunodeficiency virus (HIV) (testing for HIV is not required prior to study entry).
10. Clinically important cardiac, pulmonary, and hepatic impairment.

11. Vorinostat treatment exclusion criteria (subjects, who meet any one of these criteria and otherwise meet eligibility criteria, are still eligible for 131I-MIBG monotherapy)

    1. Since valproic acid has HDAC inhibitory activity, patients must not have received valproic acid within 30 days of study entry.
    2. Since vorinostat may prolong the QT interval, patients must not be receiving other medications known to prolong the QT interval at the time of study entry . Pentamidine must not have been received within 1 week of study enrollment.
    3. Patients with a history of deep venous thrombosis that was not associated with the presence of a central venous catheter.
    4. Patients who are receiving Coumadin.

Contacts and Locations

Contacts

Contact: Melda Dolan, MD; 1-215-930-4550; melda.dolan@jubl.com

Contact: Suzanne Bissonnette; 215-406-0127; SBissonnette@jubl.com

Locations

United States, California

Stanford University; Not yet recruiting

Palo Alto, California, United States, 94304

Contact: Elizabeth Reichert, PhD 650-724-8842 lreichert@stanford.edu

Principal Investigator: Robbie Majzner, MD

UCSF Pediatric Hematology/Oncology; Recruiting

San Francisco, California, United States, 94158

Contact: Debbie Lara 415-476-2218 Debbie.deLara@ucsf.edu

Principal Investigator: Kieuhoa Vo, MD

United States, Colorado

Children's Hospital Colorado; Recruiting

Aurora, Colorado, United States, 80045

Contact: Astrid Eder 720-777-8531 astrid.eder@coloradochildrens.org

Principal Investigator: Margaret Macy, MD

United States, Florida

Nemours Children's Specialty Care; Recruiting

Jacksonville, Florida, United States, 32207

Contact: Manisha M Bansal, MD 904-697-3793 Manisha.Bansal@nemours.org

Principal Investigator: Manisha Bansal, MD

United States, Illinois

University of Chicago Medical Center; Recruiting

Chicago, Illinois, United States, 60637

Contact: Melissa Z Marx, MPH 773-702-2927 lzeilner@peds.bsd.uchicago.edu

Principal Investigator: Ami V Desai, MD

United States, Iowa

University of Iowa Hospitals and Clinics; Recruiting

Iowa City, Iowa, United States, 52242

Contact: Roxane Mitten 319-356-1212 roxanne-mitten@uiowa.edu

Principal Investigator: David Dickens, MD

United States, Massachusetts

Dana-Farber Cancer Institute; Recruiting

Boston, Massachusetts, United States, 02215

Contact: Catherine M Clinton, MS 617-632-5556 Catherine_clinton@dfci.harvard.edu

Principal Investigator: Suzanne Shusterman, MD

United States, Minnesota

University of Minnesota; Recruiting

Minneapolis, Minnesota, United States, 55455

Contact: Ashley Schempp, MPH 612-625-9340 john3587@umn.edu

Principal Investigator: Emily Greengard, MD

United States, Missouri

Washington University Medical Center in St. Louis; Recruiting

Saint Louis, Missouri, United States, 63110

Contact: Sally Jones, MA, CCRP 314-454-4353 jones_s@wustl.edu

Principal Investigator: Frederick Huang, MD

United States, New York

Northwell Health /Cohen Children's Medical Center; Recruiting

New Hyde Park, New York, United States, 11040

Contact: Eva Atsidaftos eatsidaf@northwell.edu

Contact: Yusuf Sattar YSattar@northwell.edu

Principal Investigator: Julie Krystal, MD

Memorial Sloan Kettering Cancer Center; Recruiting

New York, New York, United States, 10065

Contact: Ellen M Basu, MD, PhD 212-639-5204

Principal Investigator: Ellen Basu, MD, PhD

United States, North Carolina

Carolinas Medical Center/Levine Children's Hospital (Atrium Health); Recruiting

Charlotte, North Carolina, United States, 28203

Contact: Katherine Farmer 704-641-7350 Katherine.Farmer@atriumhealth.org

Principal Investigator: Javier E Osterheld, MD

United States, Ohio

Cincinnati Children's Hospital Medical Center; Recruiting

Cincinnati, Ohio, United States, 45229

Contact: Lori Backus 513-636-2047 lori.backus@cchmc.org

Principal Investigator: Brian Weiss, MD

United States, Pennsylvania

The Children's Hospital of Philadelphia; Recruiting

Philadelphia, Pennsylvania, United States, 19104

Contact: Yael Mosse, MD 215-590-0965 mosse@email.chop.edu

Contact: Jennifer Saggio SAGGIO@email.chop.edu

Principal Investigator: Yael Mosse, MD

Children's Hospital of Pittsburgh; Recruiting

Pittsburgh, Pennsylvania, United States, 15224

Contact: Doreen Snelsire 412-692-8864 Doreen.Snelsire@chp.edu

Principal Investigator: Andrew Bukowinski, MD

UPMC Children's Hospital of Pittsburgh; Recruiting

Pittsburgh, Pennsylvania, United States, 15224

Contact: Doreen Snelsire Doreen.Snelsire@chp.edu

Principal Investigator: Andrew Bukowinski, MD

United States, Texas

University of Texas Southwestern Medical Center, Children's Health; Recruiting

Dallas, Texas, United States, 75235

Contact: Beverly Kleiber, PhD, CCRP 214-456-1003 beverly.kleiber@childrens.com

Principal Investigator: Tanya Watt, MD

Cook Children's Hematology/Oncology Center; Recruiting

Fort Worth, Texas, United States, 76104

Contact: Juli Ramirez 682-885-2580 juli.ramirez@cookchildrens.org

Principal Investigator: Meaghan Granger, MD

Texas Children's Hospital; Recruiting

Houston, Texas, United States, 77030

Contact: Akudo Anyanwu: 832-824-4167 aanyanw@texaschildrens.org

Principal Investigator: Jennifer Foster, MD

United States, Washington

Seattle Children's Hospital; Recruiting

Seattle, Washington, United States, 98105

Contact: Christine Goetz, BA,CCRC 206-884-1149 christine.goetz@seattlechildrens.org

Principal Investigator: Navin R Pinto, MD

United States, Wisconsin

University of Wisconsin, American Family Children's Hospital and Clinical Science Center; Recruiting

Madison, Wisconsin, United States, 53792

Contact: Jenny Weiland 608-890-8070 jlweiland@pediatrics.wisc.edu

Contact: Celeste Matsuchima 608-890-8069 camatsus@pediatrics.wisc.edu

Principal Investigator: Kenneth DeSantes, MD

Sponsors and Collaborators

Jubilant DraxImage Inc.

Investigators

• Study Director: Melda Dolan; Jubilant DraxImage Inc., dba Jubilant Radiopharma

More Information

• Responsible Party: Jubilant DraxImage Inc.
• ClinicalTrials.gov Identifier: NCT03561259
• Other Study ID Numbers: MIBG 2014-01
• First Posted: June 19, 2018
• Last Update Posted: February 16, 2023
• Last Verified: February 2023

Individual Participant Data (IPD) Sharing Statement:

• Plan to Share IPD: No

• Studies a U.S. FDA-regulated Drug Product: Yes
• Studies a U.S. FDA-regulated Device Product: No

Keywords provided by Jubilant DraxImage Inc.:

Iobenguane Avid High-risk Neuroblastoma; 3-Iodobenzylguanidine; Radiopharmaceutical

Additional relevant MeSH terms:

Neuroblastoma; Neuroectodermal Tumors; Neuroectodermal Tumors, Primitive; Neuroectodermal Tumors, Primitive, Peripheral; Neoplasms, Neuroepithelial; Neoplasms, Germ Cell and Embryonal; Neoplasms by Histologic Type; Neoplasms; Neoplasms, Glandular and Epithelial; Neoplasms, Nerve Tissue; Vorinostat; 3-Iodobenzylguanidine; Antineoplastic Agents; Histone Deacetylase Inhibitors; Enzyme Inhibitors; Molecular Mechanisms of Pharmacological Action; Radiopharmaceuticals