2. Objectives of Adjuvant�Endocrine Therapy of Breast Cancer What is the primary objective of adjuvant endocrine therapy?
To reduce risk of recurrence?
To reduce risk of developing distant metastases?
To reduce the risk of dying?
To improve QOL?�
3. Multitude of Endpoints �in Adjuvant Endocrine Trials OS, DFS, DDFS, TTP, time to distant metastases
Regulatory bodies do not necessarily agree on common definition for end points
DFS has generally been the primary end point for adjuvant endocrine therapy trials
There is no standard definition of DFS
Differences in events included
Nonrecurrence cancer events included (eg, new contralateral breast primary cancer; second nonbreast cancer; death from any cause)
Challenge for cross-trial comparisons �
4. Definition of DFS or Event-Free �Survival in Adjuvant AI Trials
5. BIG 1-98: Secondary Efficacy �End Points Protocol-defined1
Overall survival (OS)
Time from randomisation to death from any cause
Systemic disease-free survival (SDFS)
Time from randomisation to systemic recurrence (excluding local and contralateral breast events), a second nonbreast cancer, or death from any cause
Prospectively defined in statistical analysis plan
Time to recurrence
Time to distant recurrence
Time from randomisation to first recurrence at a distant sitea
6. ATAC: Protocol-Defined�Secondary Efficacy End Points Time to recurrence (TTR)
Including new contralateral breast cancer �(invasive and DCIS)
Time to distant recurrence (TTDR)
Contralateral breast cancer
Time to breast cancer death (death after recurrence)
OS
7. Impact of Distant Metastases �in Breast Cancer More than two thirds of all breast cancer recurrences are distant metastases1,2
Based on data for the tamoxifen arms in the ATAC and BIG 1-98 trials
Distant recurrences are strongly associated with the highest risk of death3
3-4 times higher risk than locoregional recurrences or contralateral occurrences
8. QOL Considerations in Adjuvant Endocrine Therapy Trials Long-term side effects of therapy vs efficacy benefits
Distant metastases worsen QOL more than locoregional recurrences or occurrences of new contralateral breast cancers1,2
9. Distant Metastases: Different �Definitions Used Across Trials SDFS
Time from randomisation to systemic recurrence (excluding local and contralateral breast events), a second nonbreast cancer, or death from any cause
TTDR
Time from randomisation to a recurrence at a distant sitea
Distant disease–free survival (DDFS)
Time from randomisation to first recurrence at a distant site or death from any cause
10. Proposal for Standardised Definitions of Efficacy End Points
11. Proposed Standardised Definition of End Points in Adjuvant Breast Cancer Trials Events that have been inconsistently included, as well as inconsistently defined, within the definition of breast cancer DFS
Contralateral breast cancer: only invasive lobular (LCIS) or invasive ductal cancer (DCIS), or both
In situ carcinomas: DCIS only, or both DCIS and LCIS
Second primary cancers: including or excluding contralateral breast cancer, including or excluding nonbreast cancers or unknown cancers at nonbreast sites
Death from other causes: known to be other than breast cancer
12. Proposed Standardised Definition of End Points in Adjuvant Breast Cancer Trials (cont’d) “Invasive disease–free survival” (IDFS) includes
Ipsilateral invasive breast tumour recurrence (IBTR)
Locoregional invasive breast cancer recurrence (invasive breast cancer in the breast, axilla, regional lymph nodes, chest wall)
Distant recurrence (biopsy-confirmed or clinically diagnosed)
Death attributable to any cause, including breast cancer, nonbreast cancer, or unknown cause
Contralateral invasive breast cancer
Second primary nonbreast invasive cancer
13. Proposed Standardised Definition of End Points in Adjuvant Breast Cancer Trials (cont’d) DDFS includes
Distant recurrence
Death attributable to any cause including breast cancer, nonbreast cancer, or unknown cause
OS includes
Death attributable to any cause including breast cancer, nonbreast cancer, or unknown cause
14. DDFS as Surrogate for OS�(or “Breast Cancer Death”)
15. Meta-Analysis: DFS Not Strongly Correlated With OS Meta-analysis of 118 adjuvant breast cancer trials explored correlation between 2-y DFS and 5-y OS
DFS predictor of OS (P<0.001)
However, for a hypothetical trial of N=1000, the 95% prediction interval of 5-y OS ranges from -0.2% to 11.3% even if 2-y DFS difference is 10% in favor of the experimental arm
Therefore, despite a moderately strong correlation, 2-y DFS is not strong enough to be used as a surrogate for 5-y OS
16. DDFS as a Surrogate for OS in �Adjuvant AI Breast Cancer Trials? MA.17 (node+, 30-mo FU): letrozole vs placebo
DDFS (HR 0.53, P=0.001) and OS (HR 0.61, P=0.04)
MA.17 (late extended adjuvant, 5.3-y FU): placebo-to-letrozole vs placebo
DDFS (HR 0.39, P=0.004) and OS (HR 0.30, P<0.0001)
IES: tamoxifen ? exemestane vs tamoxifen
DDFS (HR 0.66, P=0.0004) at 30.6-mo FU
Trend for OS (HR 0.83, P=0.08) at 37.4-mo FU
ABCSG-8/ARNO 95 and ITA meta-analysis: tamoxifen ? anastrozole �vs tamoxifen
DDFS (HR 0.61, P=0.002); OS (HR 0.71, P=0.04)
17. What Should Be the Primary End Point for Adjuvant Cancer Trials in Good-Prognosis Patients?
18. DFS and OS as End Points Traditionally, DFS (however defined) and OS have been the key end points
Used by medical journals and regulatory bodies
Adapted when most patients died of their treated cancer �(now only 30% die of breast cancer)
Provided reliable and rapid results
DFS and OS include all deaths, even those unrelated to treated cancer
DFS may also include occurrence of any new unrelated cancer
Major drawback with DFS and OS is lack of disease-specific outcome
19. Problems With OS in Adjuvant Studies in Early Breast Cancer Only 30% of women with breast cancer die of their disease
In current adjuvant trials half of the deaths are in women without recurrence
Situation is particularly important for stage I patients1
Addition of deaths without recurrence dilutes ability to detect effect of treatment on breast cancer control
20. Proposed Primary End Points for Trials of Good-Prognosis Breast Cancer Patients TTR
Very sensitive to early treatment effects
Includes all breast cancer-related outcomes (ie, local, regional, and distant recurrence, and any contralateral breast cancers)
TTDR
Only includes distant recurrences for which the likelihood of death within the next 5 years is high
Other cancer occurrences and deaths from other causes properly belong in a safety analysis
Combining them with breast cancer-specific events and deaths will only confuse interpretation of treatment efficacy
