Treating Patients With Metastatic Prostate Cancer Not Responding to Hormone and Chemotherapy
NCT ID: NCT00331344
Last Updated: 2017-10-31
Study Results
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View full resultsBasic Information
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COMPLETED
PHASE1/PHASE2
100 participants
INTERVENTIONAL
2006-04-30
2010-11-30
Brief Summary
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Detailed Description
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I. Determine the maximum tolerated dose (MTD) and dose-limiting toxicities of the combination of ixabepilone, mitoxantrone hydrochloride, and prednisone in patients with hormone-refractory metastatic prostate cancer that progressed during or after taxane-based chemotherapy. (Phase I) II. Assess the efficacy, as measured by reduction in prostate-specific antigen, of this regimen in these patients. (Phase II)
SECONDARY OBJECTIVES:
I. Evaluate the overall safety of this regimen as second-line chemotherapy in these patients.
II. Evaluate the objective response rate in patients treated with this regimen.
OUTLINE: This is a multicenter, phase I, open label, dose-escalation study of mitoxantrone hydrochloride and ixabepilone followed by a phase II study.
PHASE I: Patients receive mitoxantrone hydrochloride intravenously (IV) over 30 minutes and ixabepilone IV over 3 hours on day 1 and oral prednisone twice daily on days 1-21. Treatment repeats every 21 days for ≥ 3 courses in the absence of disease progression or unacceptable toxicity. Cohorts of 3-6 patients receive escalating doses of mitoxantrone hydrochloride and ixabepilone until the maximum tolerated dose (MTD) is determined. The MTD is defined as the dose preceding that at which 2 of 6 patients experience dose-limiting toxicity.
PHASE II: Patients receive mitoxantrone hydrochloride and ixabepilone at the MTD determined in phase I and prednisone as in phase I.
After completion of study treatment, patients are followed every 3 months.
Conditions
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Study Design
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SEQUENTIAL
TREATMENT
NONE
Study Groups
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Treatment (combination chemotherapy)
Patients receive mitoxantrone hydrochloride IV over 30 minutes and ixabepilone IV over 3 hours on day 1 and oral prednisone twice daily on days 1-21. Treatment repeats every 21 days for ≥ 3 courses in the absence of disease progression or unacceptable toxicity.
mitoxantrone hydrochloride
Given IV
ixabepilone
Given IV
prednisone
Given orally
Interventions
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mitoxantrone hydrochloride
Given IV
ixabepilone
Given IV
prednisone
Given orally
Other Intervention Names
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Eligibility Criteria
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Inclusion Criteria
* Progressive metastatic disease (i.e., positive bone scan or measurable disease) despite castrate levels of testosterone (either from orchiectomy or luteinizing hormone-releasing hormone \[LHRH\] agonist therapy)
* Progressive disease after discontinuing hormonal therapy
* Progressive disease is based on any of the following\*:
* Transaxial imaging
* Rise in prostate-specific antigen (PSA)
* Radionuclide bone scan (must show new metastatic lesions)
* Nonmeasurable or measurable disease
* For measurable disease, progression is defined by RECIST criteria
* Positive bone scan and elevated PSA required for nonmeasurable disease
* PSA evidence of progressive prostate cancer during or after first-line chemotherapy consists of a PSA level ≥ 2 ng/mL that has risen on ≥ 2 successive occasions ≥ 1 week apart
* Received ≥ 3 prior courses of paclitaxel- or docetaxel-based therapy, with disease progression documented during therapy or after cessation of therapy
* No more than 1 prior chemotherapy regimen
* Re-treatment with the same taxane-based regimen allowed
* Changes in prior chemotherapy regimen (addition of other agents) for disease progression are considered 2 chemotherapy regimens, and are not allowed
* PSA ≥ 2 ng/mL
* Testosterone \< 50 ng/dL
* Patients must continue primary androgen deprivation with LHRH analogue if they have not undergone orchiectomy
* No known active brain metastases
* ECOG performance status 0-2
* Life expectancy ≥ 12 weeks
* Creatinine ≤ 1.5 times upper limit of normal (ULN) OR creatinine clearance \> 40 mL/min
* ALT and AST \< 2.5 times ULN
* Granulocyte count ≥ 2,000/mm³
* Platelet count ≥ 100,000/mm³
* Bilirubin \< 1.5 times ULN
* Ejection fraction normal by MUGA scan or echocardiogram
* No significant cardiovascular disease, including any of the following:
* Congestive heart failure (New York Heart Association class III-IV heart disease)
* Active angina pectoris
* Myocardial infarction within the past 6 months
* No serious infections or nonmalignant medical illnesses that are uncontrolled or whose control may be jeopardized by study therapy
* No psychiatric illness or social situation that would preclude study compliance
* No pre-existing motor or sensory peripheral neuropathy \> grade 1
* No known prior severe hypersensitivity reactions to agents containing Cremophor® EL
* No "currently active" second malignancy other than nonmelanoma skin cancer
* Patients are not considered to have a "currently active" malignancy if they have completed therapy and are considered to be at \< 30% risk of relapse
* Fertile patients must use effective contraception prior to, during, and for 3 months after completion of study treatment
* See Disease Characteristics
* No prior mitoxantrone hydrochloride, ixabepilone, or other epothilones
* At least 4 weeks since prior hormonal therapy (i.e., any dose of megestrol, finasteride, or any herbal product known to decrease PSA levels \[e.g., saw palmetto or PC-SPES\]) other than LHRH agonist or a stable dose of corticosteroids from a prior chemotherapy regimen
* More than 4 weeks since other prior systemic therapies for prostate cancer
* At least 4 weeks since prior radiation therapy
* More than 8 weeks since prior radiopharmaceuticals (e.g., strontium chloride Sr 89 or samarium Sm 153 lexidronam pentasodium)
* No concurrent moderate to strong CYP3A4 inhibitors
* No concurrent prophylactic colony-stimulating factors
* No concurrent radiotherapy
18 Years
MALE
No
Sponsors
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National Cancer Institute (NCI)
NIH
Responsible Party
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Principal Investigators
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Andrea Harzstark
Role: PRINCIPAL_INVESTIGATOR
University of California San Francisco Medical Center-Mount Zion
Locations
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UCSF Helen Diller Family Comprehensive Cancer Center
San Francisco, California, United States
University of Wisconsin Hospital and Clinics
Madison, Wisconsin, United States
Countries
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References
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Rosenberg JE, Ryan CJ, Weinberg VK, Smith DC, Hussain M, Beer TM, Ryan CW, Mathew P, Pagliaro LC, Harzstark AL, Sharib J, Small EJ. Phase I study of ixabepilone, mitoxantrone, and prednisone in patients with metastatic castration-resistant prostate cancer previously treated with docetaxel-based therapy: a study of the department of defense prostate cancer clinical trials consortium. J Clin Oncol. 2009 Jun 10;27(17):2772-8. doi: 10.1200/JCO.2008.19.8002. Epub 2009 Apr 6.
Harzstark AL, Rosenberg JE, Weinberg VK, Sharib J, Ryan CJ, Smith DC, Pagliaro LC, Beer TM, Liu G, Small EJ. Ixabepilone, mitoxantrone, and prednisone for metastatic castration-resistant prostate cancer after docetaxel-based therapy: a phase 2 study of the Department Of Defense Prostate Cancer Clinical Trials Consortium. Cancer. 2011 Jun 1;117(11):2419-25. doi: 10.1002/cncr.25810. Epub 2010 Dec 29.
Other Identifiers
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055513
Identifier Type: -
Identifier Source: secondary_id
CDR0000481121
Identifier Type: REGISTRY
Identifier Source: secondary_id
NCI-2009-00155
Identifier Type: -
Identifier Source: org_study_id
NCT01648374
Identifier Type: -
Identifier Source: nct_alias