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Transcript 
HTA OF TRASTUZUMAB IN
ADJUVANT TREATMENT
FOR HER2 POSITIVE BREAST CANCER
Karianne Johansen, PhD, Senior Advisor,
Torbjørn Wisløff , Researcher
Inger Natvig Norderhaug , Research Director
Norwegian Health Service Research
Centre
Expert Group
ƒ Professor dr.med. Per Eystein Lønning, University of Bergen,
Haukeland University hospital, Bergen
ƒ Professor dr.med. Ivar Sønbø Kristiansen, HERO, University of
Oslo
ƒ Overlege dr.med. Bjørn Naume, The National hospital, Oslo
ƒ Professor dr. med. Jan Norum, Cancer Unit, University hospital
Northen Norway, Tromsø
ƒ Professor dr.philos. Jan Abel Olsen, HERO, Universitetet i Tromsø
ƒ Professor dr. med. Erik Wist, Cancer department, Ullevaal
University Hospital, Oslo
Background and Issues
ƒ
Promising interim data from large trials of Herceptin in treatment of
HER2 positive adjuvant breast cancer published Q4 2005 /Q1 2006
ƒ
Manufacturing authorization expected in Norway soon
ƒ
HER2 amplification recognized in 20-30% of breast cancers
ƒ
Associated with an aggressive form of the disease and shortened diseasefree survival and overall survival
ƒ
Pressure was put on an HTA of the new treatment prior to regulatory
approval
ƒ
Part 1. A systematic review of the existing data to evaluate the effect and
safety was performed
ƒ
Part 2. A cost-effectiveness model for Norway was developed
Search for literature
ƒ
All relevant databases were searched according to a predefined protocol
(Medline, Embase,the Cochrane Database of Systematic Reviews (CDSR), the
Cochrane Controlled Trials Register (CCTR), the Science Citation index og the NHS
Centre for Reviews and Dissemination databases (DARE, NHS EED, HTA)and OHE
HEED)
ƒ
Web sites for conferences and international clinical trial databases
ƒ
Manufacturer's were asked to submit relevant documentation according to
the protocol
Results from the systematic review
Search result
ƒ
ƒ
5 trials included - rated to medium quality
Event driven interim analysis focusing on disease-free survival (DFS)
Direction of effect
Disease Free Survival
ƒ A highly significant effect compared with the control group were found in all trials
ƒ
A meta-analysis of the hazard ratio for a risk of an event in the trastuzumab group
compared with the control group were 0.5 (95% CI, 0.4 to 0.6)
The absolute differences
– 7.5 % to 8.4 % at 2 years
– 11.0 % to 19.0 % at 4 years
Overall Survival
ƒ All reported results were in favor of trastuzumab
ƒ Only one analysis (JOINT) of two trials showed statistical significant effect
ƒ
We concluded
There is not enough data available to draw certain conclusions regarding overall
survival due to short follow-up
*HERA, NSABP B-31, NCCTG- N9831, BCIRG 006 , FinHER
Results from the systematic review
Direction of adverse events
ƒ
Trastuzumab was associated with increased risk of cardio toxicity, despite very strict
cardiovascular exclusion criteria in the protocols
ƒ
NYHA Class III or IV congestive heart failure or death from cardiac causes
– Trastuzumab group:
0.5 % to 4.1 %
– Control group:
0.0 % to 1.0 %
ƒ
Decrease in LVEF
– Trastuzumab group:
– Control group:
7.1 % to 17.3 %
2.2 % to 9.0 %
Discontinuations of trastuzumab :
8.5 % - 31.4 %.
ƒ
We concluded
Long term follow-up of patients is needed, with a special focus on cardio toxicity
Further need for evaluation – Issues ?
ƒ
A Hazard Ratio of 0.5 for a risk of a disease-free event in the trastuzumab
group compared with the control group is a relative number
ƒ
How effective is today's adjuvant treatment of breast cancer in Norway?
ƒ
What is the incremental risk of death for HER2 positive patients?
ƒ
Treatment with trastuzumab is costly with potentially serious adverse
event – whom are eligible for treatment?
ƒ
Is the incremental effect of trastuzumab reasonable relative to the
incremental cost?
ƒ
How sustainable is the effect beyond the interim data?
Patients eligible for treatment
Mean age 50 years - less patients above 55 - none above 70
Incidence of
Breast Cancer
Age
Eligible for
adjuvant chemotherapy
HER2 positive and
eligible for trastuzumab
20 - 54
845
676
203
1078
344
103
771
0
0
2694
1021
306
55 - 69
70 +
Total
*Age 55-70 years, eligibility for adjuvant chemotherapy depend on hormone receptor status
Not women who have an LVEF of 55% or less, or any of the following:
•
•
•
•
•
•
a history of documented congestive heart failure
high-risk uncontrolled arrhythmias
angina pectoris requiring medication
clinically significant valvular disease
evidence of transmural infarction on electrocardiograph (ECG)
poorly controlled hypertension.
Health Economic evaluation
Standard treatment:
FEC100 + observation
New treatment:
FEC100 + 1 year trastuzumab every 3 weeks
ƒ
A markow model, one year cycles was constructed
Inputs were based on
ƒ
The results from the clinical trials (Event rates and Hazard ratios)
ƒ
Data from the Norwegian Cancer Registry used for breast cancer survival
ƒ
Different assumptions were made together with the expert group to show different
variations on extending the effect beyond the clinical trials
ƒ
Both cost and LYG were discounted at 3 %
ƒ
In the base case costs are presented from a health care perspective
ƒ
Average age in the model, 50 years, time horizon - life time perspective
*FEC100 = 5-flurouracil, epirubicin-og cyklofosfamid
(locoregional radiotheraoy and systemic hormonal therapy is used were appropriate)
Model Structure
1. Disease free
2. Local recurrence
3. Distant recurrence
4. Death*
*Dead from metastatic breast cancer or from non-cancer causes while in any
of the first 3 disease states.
Patient die from breast cancer only after distant recurrence
Base case Scenarios A and B
Scenario A
ƒ Stadium I and II from the Cancer Registry as a total sum of survival
ƒ
ƒ
Events
– Years 0 - 4:
– Years 5 – 10:
– Years 11 + :
Probability of death from breast cancer
Comparator arm
– Years 0 – 10: Survival taken from the Norwegian Cancer Registry
– HER2 additional risk factor of 1.3 was applied for the first 10 years
Trastuzumab
– Years 0 to 4:
– Years 5 – 10 :
– Years 11 + :
ƒ
Results from clinical trials
Results gradually decline
=0
HR from the JOINT analysis used (0.67)
The cancer registry with equal risk
Patients alive follow normal survival in the population
Probability of death from other causes than breast cancer
– Survival rates from Norwegian Statistics
Scenario B
ƒ Stadium IV from the Cancer Registry used for risk of death from metastatic phase
ƒ In all other stages risk of dying follow normal survival in the population)
Survival Curves Scenario A and B
1
Kontroll Scenario A
0,9
Overlevelse
Survival
Herceptin Scenario A
0,8
Kontroll Scenario B
0,7
Herceptin Scenario B
0,6
0,5
0,4
0,3
0,2
0,1
0
0
5
10
15
20
25
År
Years
30
35
40
45
50
Results (discounted 3%)
Scenario A
Strategy
Cost
(EUR)
Trastuzumab
59 000
Standard
29 625
Incremental
Cost (EUR)
Effectiveness
(LY)
Incremental
Effectiveness
(LYG)
ICER
18,7
29 375
17,2
1,5
19 580 EUR/LYG
Scenario B
Strategy
Cost
(EUR)
Trastuzumab
54 875
Standard
21 500
Incremental
Cost (EUR)
Effectiveness
(LY)
Incremental
Effectiveness
(LYG)
ICER
17,7
33 375
15,5
Cost-effectiveness in favor of trastzumab
2,2
15 170 EUR/LYG
Results (undiscounted)
Scenario A
Strategy
Cost
(EUR)
Trastuzumab
72 625
Standard
48 000
Incremental
Cost (EUR)
Effectiveness
(LY)
Incremental
Cost-Effectiveness
Ratio
(ICER)
Incremental
Effectiveness
(LYG)
30,2
24 625
27,5
2,7
9120 EUR/LYG
Scenario B
Strategy
Cost
(EUR)
Trastuzumab
65 125
Standard
34 000
Incremental
Cost (EUR)
Effectiveness
(LY)
Incremental
Effectiveness
(LYG)
Incremental
Cost-Effectiveness
Ratio
(ICER)
28,5
31 125
24,5
Cost-effectiveness in favor of trastzumab
3,9
7980 NOK/LYG
Conclusion
ƒ
ICER presented below most common thresholds
ƒ
Treatment with trastuzumab per patient is estimated at 40 600 EUR the
first year in the model
ƒ
In a cohort of 300 females there will be 11 less local recurrence and 44 less
metastatic events in the trastuzumab arm
ƒ
The largest uncertainty is the extrapolation of long term benefit from the
interim results, with a short follow-up
ƒ
Careful follow-up of patients focusing on recurrence, survival and long
term adverse events needed
ƒ
A special focus should be put on long term follow up of cardio toxicity.
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