Post on 24-Dec-2014
description
2. Starts in the prostate gland
Wraps around the urethra (the tube that carries urine out of the
body.)
Third common cause of death from cancer in man of all ages.
First most common cause of death from cancer in man over 75 of
age.
Rarely found in man younger than 40.
Highest risk: Man over 60.
Prostate cancer:
3. Prostate cancer:
4. patient specific therapeutic cancer vaccine for prostate
cancer.
Manufactured by a company named Dendreon.
Was approved by the FDA on April 29, 2010 to treat asymptomatic or
minimally symptomatic metastatic Hormone refractory prostate
cancer.
Sipuleucel-T:
5.
1. Patients own white blood cells with antigen presenting cells
(APC) are extracted. (Those cells called Dentritic therefore the
company name is Dendreon).
Preparation of treatment vaccine Sipuleucel-T
6. 2. The cells are incubated with fusion protein (PA2024) consist
of:
7. immune signaling factor(GM-CSF) that helps the APCs to
mature.Preparation of Sipuleucel-T:
8. 9. ClinicalTrials.gov Identifier:NCT01133704
Purpose:
stimulate T-cell immunity against prostatic acid phosphatase.
evaluate the safety and efficacy of sipuleucel-T in a
placebo-controlled study.
Clinical trial overview:
10. PAP- not found in non prostate tissue.
Patients who developed a natural immune response to PAP had a
longer disease progression: 34 weeks vs 13 weeks
Background to trial design:
11. 1. Overall Time to Disease Progression
Time frame: 36 months
Asymptomatic patients compare to placebo.
2. Overall Survival
Subjects were followed for 3 years from the time of randomization
or until death.
Primary Outcome Measures:
12. 127 patients with asymptomatic metastatic hormone refractory
prostate cancer.
2:1 ratio to receive three infusions of sipuleucel-T (n = 82) or
placebo (n = 45) every 2 weeks.
PATIENTS AND METHODS:
13. 19 centers in the United States.
Patients with histologically confirmed adenocarcinomaof the
prostate.
Radiologic evidence of metastases.
Serum testosterone less than 50 ng/dL.
Expected survival of at least 3 months.
Recruitment for trial:
14. Prior radiation must be completed at least one month
beforetrial treatment.
Radiation is prohibited within 1 year of treatment.
Patients with prior immunotherapy were not eligible to
participate.
Patients with cancer-related bone pain or with visceral metastasis
were not permitted.
Recruitment for trial continuous:
15. 2:1 ration T cells- placebo.
Treatment was given on weeks: 0, 2, 4
Freshly prepared T cells and placebo vaccine for each
treatment.
Acetaminophen (650 mg) was given 30 minutes prior to
injection.
Treatment administration:
16. Patients were observed every 8-12 weeks after treatment.
Examination performed:
Physical examination.
Adverse event assessment.
Laboratory tests.
Radiographic imaging.
Painassessment.
Following up with patients:
17. progressive disease on serial radiographic imaging tests.
new cancer-related pain associated with a radiographic anatomic
correlation.
progression such as spinal cord compression, nerve root
compression, or pathologic fracture.
Trial End Points:
18. Increase greater than 50% in measurable disease.
Clear worsening of nonmeasurable disease.
Appearance of at least two new lesions on a bone scan.
Development of cancer-related pain that correlated with a site of
metastasis.
Development of other clinical events consistent with
progression.
Progressive disease defined:
19. Attaining a power of 80%.
Two-sided .05 significance level.
Assumption: sipuleucel-T result in an increase in median TTP to 7.7
months.
Loss to follow-up rate of 5%.
Enrollment of approximately 120 patients was targeted to achieve
the required 80 events.
Statistical Considerations:
20. Patient Disposition:
21. Clinical Results:
Primary end point, time to disease progression
22. Final overall survival
Clinical Results:
23. Immune Monitoring:
The PA2024 T-cell stimulation index is a measure of specific T-cell
responsiveness against the target antigen.
Toxicity:
significantly more common in sipuleucel-T treated patients.
*No patient discontinued the trial because of toxicity.
Other measurments:
24. Of the 127 patients, 115 patients had progressive disease at
the time of data analysis.
The median for time to disease progression (TTP) for sipuleucel-T
was 11.7 weeks vs 10.0 weeks for placebo.
Median survival was 25.9 months for sipuleucel-T and 21.4 months
for placebo.
Final results:
25. The improvement in the primary end point TTP did not achieve
statistical significance.
Study suggests that sipuleucel-T may provide a survival advantage
to asymptomatic HRPC patients.
Need for further supportive studies.
Conclusion
26. At 36 months, the estimated survival rate in the sipuleucel-T
group was 34 weeks compared with 11 weeks in the placebo
group.
The real numbers were 25.9 vs 21.4.
provide a survival advantage to asymptomatic HRPC patients.
no patients were removed from the trial for toxicity.
no treatment-related deaths.
Need for supportive studies?
27. Feel free to contact me:
a_ostrovski@yahoo.com
917-478-1063
Questions?