Phase II NKTR-102 In Bevacizumab-Resistant High Grade Glioma

NCT ID: NCT01663012

Last Updated: 2016-02-24

Basic Information

• Recruitment Status: COMPLETED
• Clinical Phase: PHASE2
• Total Enrollment: 20 participants
• Study Classification: INTERVENTIONAL
• Study Start Date: 2012-07-31
• Study Completion Date: 2015-02-28

Brief Summary

High Grade Gliomas, including anaplastic astrocytomas, anaplastic oligodendrogliomas and glioblastomas (GBM), are the most common and most aggressive primary brain tumors. Prognosis for patients with high-grade gliomas remains poor. The estimated median survival for patients with GBM is between 12 to 18 months. Recurrence after initial therapy with temozolomide and radiation is nearly universal. Since May 2009, the majority of patients in the US with an initial recurrence of high-grade glioma receive bevacizumab, a monoclonal antibody against vascular endothelial growth factor (VEGF), which is thought to prevent angiogenesis in these highly vascular tumors. BEV has response rates from 32-62% and has improved overall median survival in patients with recurrent high-grade gliomas1. However, the response is short lived, and nearly 100% of patients eventually progress despite bevacizumab. No chemotherapeutic agent administered following progression through bevacizumab has made a significant impact on survival. Patients progress to death within 1-5 months after resistance develops. Therefore, patients with high-grade gliomas who have progressed through bevacizumab represent a population in dire need of a feasible and tolerable treatment.

NKTR-102 is a topoisomerase I inhibitor polymer conjugate that was engineered by attaching irinotecan molecules to a polyethylene glycol (PEG) polymer using a biodegradable linker. Irinotecan released from NKTR-102 following administration is further metabolized to the active metabolite, 7-ethyl-10-hydroxy-camptothecin (SN38), that causes DNA damage through inhibition of topoisomerase. The goal in designing NKTR-102 was to attenuate or eliminate some of the limiting side effects of irinotecan while improving efficacy by modifying the distribution of the agent within the body. The size and structure of NKTR-102 results in marked alteration in pharmacokinetic (PK) profile for the SN38 derived from NKTR-102 compared to that following irinotecan: the maximal plasma concentration (Cmax) is reduced 5- to 10-fold and the half-life (t1/2 ) of SN38 is increased from 2 days to approximately 50 days. This altered profile leads to constant exposure of the tumor to the active drug. In addition, the large NKTR-102 molecule does not freely pass out of intact vasculature, which may account for relatively higher concentrations of the compound and the active metabolites in tumor tissues in in vivo models, where the local vasculature may be relatively more permeable. A 145 mg/m2 dose of NKTR-102, the dose intended for use in this phase II clinical trial (and being used in the phase III clinical program), results in approximately the same plasma exposure to SN38 as a 350 mg/m2 dose of irinotecan, but exposure is protracted, resulting in continuous exposure between dosing cycles and lower Cmax. NKTR-102 was therefore developed as a new chemotherapeutic agent that may improve the clinical outcomes of patients.

Conditions

Anaplastic Astrocytomas; Anaplastic Oligodendrogliomas; Glioblastomas (GBM)

Study Design

• Allocation Method: NA
• Intervention Model: SINGLE_GROUP
• Primary Study Purpose: TREATMENT
• Blinding Strategy: NONE

Study Groups

Drug: Etirinotecan pegol

145 mg/m2 dose

Group Type: EXPERIMENTAL

Etirinotecan pegol

Intervention Type: DRUG

Interventions

Etirinotecan pegol

Intervention Type: DRUG

Other Intervention Names

NKTR-102

Eligibility Criteria

Inclusion Criteria

• Pathologically proven high-grade glioma (WHO III or IV) with astrocytic component and must be in recurrence after treatment with bevacizumab
• Patients must have received conventional radiation therapy of total radiation dosage (ranging from 5400 to 6000 cGy administered in daily fractions of 150 to 200 cGy over 6 weeks) with concurrent temozolomide.

Patients must have received bevacizumab and be in recurrence after bevacizumab treatment.

• Patients must be at least 28 days from last administration of cytotoxic chemotherapy and at least 14 days from the last administration of bevacizumab.

• Patients must be >18 years of age.
• Patients must have a life expectancy > 6 weeks
• Patients must have a Karnofsky Performance Score (KPS) >=50
• If female, patients of childbearing potential must have a negative serum beta-hCG pregnancy test and must agree to use hormonal or barrier birth control with spermicidal gel to avoid pregnancy during the study
• Adequate organ function (obtained within 14 days prior to randomization and analyzed by the central laboratory) as evidenced by:

1. Absolute neutrophil count (ANC) >=1.5 X 10^9/L without myeloid growth factor support for 7 days preceding the lab assessment;

2. Hemoglobin (Hgb) >= 9 g/dL (90 g/L); < 9 g/dL (< 90 g/L) is acceptable if hemoglobin is corrected to >= 9 g/dL (90 g/L) as by growth factor or transfusion prior to randomization;

3. Platelet count >=100 X 10^9/L without blood transfusions for 7 days preceding the lab assessment;

4. Bilirubin <= 1.5 X upper limit of normal (ULN), except for patients with documented history of Gilbert's disease;

5. Alanine aminotransferase (ALT), and aspartate aminotransferase (AST) <= 2.5 X ULN

6. Alkaline phosphatase (AP) <= 3 X ULN

7. Serum creatinine <= 1.5 mg/dL (133 µmol/L) or calculated creatinine clearance >= 50 mL/min (using Cockcroft-Gault formula);

8. Women of childbearing potential (WCBP): negative serum pregnancy test (this test is required of all women unless post-menopausal, defined as 12 consecutive months since last regular menses, or surgically sterile).

• Patients must be willing and able to comply with the protocol and provide written informed consent prior to study-specific screening procedures.

Exclusion Criteria

Patients who meet any of the following criteria must not be permitted entry to the study.

• Patients who have had chemotherapy within 28 days, radiotherapy within 28 days, biological therapy within 14 days, and investigational therapy within 21 days prior to first dose of experimental drug.
• Patients who have received prior treatment for cancer with a camptothecin derivative (eg, irinotecan, topotecan, and investigational agents including but not limited to exatecan, rubitecan, gimatecan, karenitecan, SN38 investigational agents, EZN-2208, SN-2310, and AR-67).
• Patients with the following co-morbid disease or incurrent illness:

1. Patients with chronic or acute GI disorders resulting in diarrhea of any severity grade; patients who are using chronic anti-diarrheal supportive care (more than 3 days/week) to control diarrhea in the 28 days prior to first dose of investigational drug.

2. Patients with known cirrhosis diagnosed with Child-Pugh Class A or higher liver disease.

3. Prior malignancy except for non-melanoma skin cancer and carcinoma in situ (of the cervix or bladder), unless diagnosed and definitively treated more than 3 years prior to first dose of investigational drug.

4. Severe/uncontrolled inter-current illness within the previous 28 days prior to first dose of investigational drug.

5. Significant known cardiovascular impairment (NYHA CHF > grade 2, unstable angina, myocardial infarction within the previous 6 months prior to first dose of investigational drug, or existing serious cardiac arrhythmia).

6. Patients who require daily use of oxygen supplementation in the 28 days prior to first dose of investigational drug.

7. Any other significant co-morbid conditions that in the opinion of the Investigator would impair study participation or cooperation.

• Patients with a known allergy or hypersensitivity to any of the components of the investigational therapy, including PEG or topoisomerase inhibitors.
• Patients receiving the following medications at the time of first dose of investigational drug:

• Pharmacotherapy for hepatitis B or C, tuberculosis, or HIV.
• enzyme inducing anti-epileptic medications (EIAEDs)
• other chemotherapy, other investigational agents , or biologic agents for
• the treatment of cancer including antibodies(eg, bevacizumab,
• trastuzumab, or pertuzumab) or any investigational agent(s).
• Pregnant or nursing patients will be excluded from the study.
• Patients receiving active treatment for HIV will be excluded from this study because non-nucleoside reverse transcriptase inhibitors, protease inhibitors and maraviroc (a CCR5-antagonist) are extensively metabolized by the cytochrome P450 system. Interactions with these drugs may induce or inhibit irinotecan or SN38 metabolism, leading to over or under-dosing.

• Minimum Eligible Age: 18 Years
• Eligible Sex: ALL
• Accepts Healthy Volunteers: No

Sponsors

Nektar Therapeutics

INDUSTRY

Sponsor Role: collaborator

Lawrence Recht

OTHER

Sponsor Role: lead

Responsible Party

Lawrence Recht

Professor of Neurology and Neurological Sciences

Responsibility Role: SPONSOR_INVESTIGATOR

Principal Investigators

Lawrence Recht, MD

Role: PRINCIPAL_INVESTIGATOR

Stanford University

Locations

Stanford University School of Medicine

Palo Alto, California, United States

Countries

United States

Other Identifiers

SU-06212012-10228

Identifier Type: OTHER

Identifier Source: secondary_id

NCI-2012-01288

Identifier Type: OTHER

Identifier Source: secondary_id

BRN0021

Identifier Type: OTHER

Identifier Source: secondary_id

IRB-24833

Identifier Type: -

Identifier Source: org_study_id