Tamoxifen for Progressive Transitional Cell Carcinoma Following Previous Chemotherapy Treatment
Information source: Baylor College of Medicine
Information obtained from ClinicalTrials.gov on November 03, 2008
Link to the current ClinicalTrials.gov record.
Condition(s) targeted: Urinary Bladder Neoplasms
Intervention: Tamoxifen (Drug)
Phase: Phase 2
Status: Recruiting
Sponsored by: Baylor College of Medicine Official(s) and/or principal investigator(s):
Seth P. Lerner, M.D., Principal Investigator, Affiliation: Baylor College of Medicine
Overall contact:
Joy Banerjee, Phone: 713-798-4479, Email: banerjee@bcm.edu
Summary
The major objective of this two-stage phase II study is to determine whether tamoxifen is
deserving of further study in metastatic bladder cancer. Tamoxifen is expected to function as
a cytostatic (and not cytotoxic) agent, and may produce more disease stability than
regression. Sustained stable disease is considered to be clinically important and the more
likely event. Hence, 4-month freedom from progression is chosen as the primary end-point
instead of response rate. Freedom from progression is defined as the period from start of
therapy to the time of objective radiologic progression. A total of 25 subjects will be
enrolled, 15 during stage 1 and 10 during stage 2 of a two-stage minimax design phase II
study.
Pre-therapy evaluation (within 3 weeks of initiation of therapy):
- History and physical examination (H and P)
- Performance status (PS) assessment
- CBC (complete blood counts)
- CMP (complete metabolic profile)
- Pregnancy test (in women younger than 50)
- Computed tomography (CT) scan of the chest, abdomen and pelvis
- Bone scan if bone pain or raised alkaline phosphatase
- Biopsy (may use previous biopsy specimen)
- Samples of plasma from the routine CBC and CMP will be banked indefinitely for future
biomarker studies at the Scott Department of Urology.
Treatment plan: Therapy will be administered as an outpatient. Tamoxifen is administered at
20 mg/day as a single daily oral dose. Clinical assessment of patients by a history and
physical examination will be performed every 4 weeks (one cycle). Objective radiological
assessment of response will be made every 8 weeks or earlier if clinically indicated. A CT
(computerized tomography) scan of the abdomen, pelvis and chest will be performed at baseline
and every 2 cycles. A response is confirmed by repeating the scans in 4 weeks. Bone scan is
performed if the patient complains of new bone pain or has raised alkaline phosphatase. A
radiologist who is blinded to the treatment regimen reads the scans. The RECIST criteria are
used to define response. Tamoxifen is continued until progressive disease or intolerable side
effects occur.
Clinical Details
Official title: H-16848 - Phase II Pilot Study With Correlative Markers of Tamoxifen for Progressive Transitional Cell Carcinoma Following Previous Chemotherapy
Study design: Treatment, Non-Randomized, Open Label, Uncontrolled, Single Group Assignment, Safety/Efficacy Study
Primary outcome: Sustained stable disease is considered to be clinically important. Hence, 4-month freedom from progression (FFP) (Stable disease + Partial response + Complete response) is chosen as the primary end-point instead of response rate.
Eligibility
Minimum age: 18 Years.
Maximum age: N/A.
Gender(s): Both.
Criteria:
Inclusion Criteria:
- Patients previously diagnosed with bladder cancer who have already received 1-2
systemic therapy regimens (chemotherapy or biological therapy or both) but including
at least one chemotherapy regimen.
- Patients who have had the cancer spread to other parts of the body.
- Patients must have adequate liver function.
Exclusion Criteria:
- Patients who have uncontrolled nervous system metastasis
- Patients who are pregnant
- Patients who have had systemic therapies within the past 4 weeks
- Patients who plan to have major surgery within 2 weeks
- Patients who have Grade III/IV heart problems
- Patients who have severe and/or uncontrolled medical disease.
- Patients who might be at high risk for deep vein thrombosis
Locations and Contacts
Joy Banerjee, Phone: 713-798-4479, Email: banerjee@bcm.edu
San Camillo and Forlanini Hospitals, Rome, Italy; Recruiting
Cora N. Sternberg, MD, FACP
Baylor College Of Medicine, Houston, Texas 77030, United States; Recruiting
Seth P. Lerner, M.D., Principal Investigator
Guru Sonpavde, M.D., Sub-Investigator
Daniel E. Epner, MD, Sub-Investigator
Additional Information
Baylor College of Medicine's Clinical Trials Scott Department of Urology, Baylor College of Medicine Bladder Cancer Advocacy Network
Related publications: Kim HT, Kim BC, Kim IY, Mamura M, Seong DH, Jang JJ, Kim SJ. Raloxifene, a mixed estrogen agonist/antagonist, induces apoptosis through cleavage of BAD in TSU-PR1 human cancer cells. J Biol Chem. 2002 Sep 6;277(36):32510-5. Epub 2002 Jun 25. Shen SS, Smith CL, Hsieh JT, Yu J, Kim IY, Jian W, Sonpavde G, Ayala GE, Younes M, Lerner SP. Expression of estrogen receptors-alpha and -beta in bladder cancer cell lines and human bladder tumor tissue. Cancer. 2006 Jun 15;106(12):2610-6.
Starting date: January 2007
Ending date: January 2013
Last updated: September 4, 2008
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