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Risk Stratified Analysis Improves Risk Stratified Analysis Improves Prediction of Treatment Benefit Over Prediction of Treatment Benefit Over
Subgroup Analysis: Findings from Subgroup Analysis: Findings from Intergroup N9741Intergroup N9741
HK Sanoff, ME Campbell, HC Pitot, HK Sanoff, ME Campbell, HC Pitot, RM Goldberg, DJ SargentRM Goldberg, DJ Sargent
University of North Carolina at Chapel Hill, and University of North Carolina at Chapel Hill, and Mayo Clinic for the NCCTG, CALGB, ECOG, SWOG, Mayo Clinic for the NCCTG, CALGB, ECOG, SWOG,
NCICNCIC
ABSTRACT # 4018
Despite recent advances in therapy for metastatic Despite recent advances in therapy for metastatic colorectal cancer (MCRC), individuals’ responses to colorectal cancer (MCRC), individuals’ responses to treatment and clinical courses remain treatment and clinical courses remain heterogeneous. heterogeneous.
A substantial minority of patients progress rapidly, A substantial minority of patients progress rapidly, dying of disease within a year of diagnosis.dying of disease within a year of diagnosis.
Several baseline factors indicate a poor prognosis, Several baseline factors indicate a poor prognosis, i.e.:i.e.:– Performance status (PS) Performance status (PS) >> 2 2– Alkaline phosphatase (ALK) > twice upper limit of normal. Alkaline phosphatase (ALK) > twice upper limit of normal.
No baseline factors currently are used in treatment No baseline factors currently are used in treatment selectionselection
BACKGROUNDBACKGROUND
Risk stratified analysis (RSA) assesses Risk stratified analysis (RSA) assesses treatment effect according to baseline risktreatment effect according to baseline risk
–Uses pre-existing risk models to divide patients Uses pre-existing risk models to divide patients into risk groups.into risk groups.–Outcomes stratified based on these risk groupsOutcomes stratified based on these risk groups
RSA advocated as a better method for RSA advocated as a better method for predicting patient specific treatment predicting patient specific treatment benefit over subgroup analysis. benefit over subgroup analysis.
–RSA does not artificially divide according to RSA does not artificially divide according to one factor when many may coexist within one one factor when many may coexist within one patient.patient.
BACKGROUNDBACKGROUNDRisk Stratified AnalysisRisk Stratified Analysis
Kent & Hayward, JAMA 2007; 298: Kent & Hayward, JAMA 2007; 298: 12091209
Perform RSA of a large, phase III trial Perform RSA of a large, phase III trial of first-line chemotherapy for MCRCof first-line chemotherapy for MCRC
Compare RSA to subgroup analysis Compare RSA to subgroup analysis by PSby PS
Assess for differences in treatment Assess for differences in treatment benefit by risk group benefit by risk group
OBJECTIVESOBJECTIVES
Individual patient data from N9741, Phase III Individual patient data from N9741, Phase III trial of FOLFOX vs. IROX vs. IFLtrial of FOLFOX vs. IROX vs. IFL
N=1682N=1682 RSA based on risk model of Köhne et al.RSA based on risk model of Köhne et al. Köhne model developed in patients with Köhne model developed in patients with MCRC treated with 5FU. 3 risk groups based on:MCRC treated with 5FU. 3 risk groups based on:
– ECOG PSECOG PS– WBCWBC– Alkaline phosphataseAlkaline phosphatase– Number of sites of metastatic disease Number of sites of metastatic disease
METHODSMETHODS
KöhneKöhne et al. Ann Oncol 2002; 13: 308.
METHODSMETHODS
RISK GROUPS:RISK GROUPS:
OS and TTP were compared by risk group, PS. OS and TTP were compared by risk group, PS. Cox models assessed the relative predictive Cox models assessed the relative predictive utility of PS and risk group.utility of PS and risk group.
*WBC estimated from absolute granulocyte count (AGC) based on *WBC estimated from absolute granulocyte count (AGC) based on AGC= -0.7 + 0.8(WBC) [Benson, Cancer 1985]. AGC= -0.7 + 0.8(WBC) [Benson, Cancer 1985].
PS
# sites
# sitesWBC
High Risk
High Risk
Med
Alk 1
Low
High Risk
Med
0, 1> 1
<10 x 109>10 x 109
1>1
>300 <300
>1
RESULTSRESULTSOverall survival by Risk Overall survival by Risk GroupGroup
0
20
40
60
80
100
0 12 24 36 48 60
Time (M onths)
Low Median= 20.8 Mos
Intermediate Median= 17.4 Mos
High Median= 9.4 Mos
P-Value = <0.0001
RESULTSRESULTSOverall survival by Performance Overall survival by Performance StatusStatus
0
20
40
60
80
100
0 12 24 36 48 60
Time (M onths)
PS 0 Median= 20.4 Mos
PS 1 Median= 14.8 Mos
PS 2 Median= 9.1 Mos
P-Value = <0.0001
RESULTS: RESULTS: OS Multivariate OS Multivariate modelmodelPrediction improved by PS and Risk GroupPrediction improved by PS and Risk Group
Risk GroupRisk Group HR (95% CI)HR (95% CI) XX22 P-Value P-Value
PS 0PS 0 11
PS 1PS 11.4 (1.4 (1.3, 1.6)1.3, 1.6) 41.041.0 <0.0001<0.0001
PS 2PS 21.5 1.5 (1.2, 2.0)(1.2, 2.0) 10.310.3 0.00140.0014
LowLow 11
IntermediateIntermediate1.4 (1.4 (1.2, 1.5)1.2, 1.5) 31.731.7 <0.0001<0.0001
High High 2.3 2.3 (1.9, 2.8)(1.9, 2.8) 71.671.6 <0.0001<0.0001
Likelihood Ratio X2 for PS = 83.8, for Kohne = 114.1, Combined Model=157.6
RESULTS RESULTS OS by treatment arm, risk OS by treatment arm, risk groupgroupRisk GroupRisk Group Trt Trt
ArmArmNN Median Median
(Months)(Months)HR (95% CI)HR (95% CI) P-ValueP-Value
LowLow
FOLFOXFOLFOX 247247 27.527.5 11
IFLIFL 146146 18.218.2 1.7 1.7 (1.4, 2.1)(1.4, 2.1) <0.001<0.001
IROXIROX 135135 19.719.7 1.5 1.5 ( 12, 1.8)( 12, 1.8) <0.001<0.001
IntermediatIntermediatee
FOLFOXFOLFOX 384384 19.219.2 11
IFLIFL 227227 13.813.8 1.5 1.5 (1.3, 1.8)(1.3, 1.8) <0.001<0.001
IROXIROX 196196 17.817.8 1.3 1.3 (1.1, 1.6)(1.1, 1.6) 0.0050.005
HighHigh
FOLFOXFOLFOX 6060 10.710.7 11
IFLIFL 5555 9.49.4 1.3 1.3 (0.87, 1.9)(0.87, 1.9) 0.210.21
IROXIROX 4949 9.19.1 1.3 1.3 (0.87, 1.9)(0.87, 1.9) 0.220.22
Interaction p value risk group X treatment arm=0.08
CONCLUSIONSCONCLUSIONS
RSA using the Köhne model is prognostic RSA using the Köhne model is prognostic of survival in this cohort treated with of survival in this cohort treated with combination chemotherapy.combination chemotherapy.
FOLFOX is superior to IFL in all risk FOLFOX is superior to IFL in all risk groups.groups.
Trend towards less benefit in high risk Trend towards less benefit in high risk group.group.– Small # high risk patients supports need for Small # high risk patients supports need for
pooled analyses of these patients.pooled analyses of these patients.
CONCLUSIONSCONCLUSIONS
RSA adds predictive ability to a RSA adds predictive ability to a multivariate model above PS alone.multivariate model above PS alone.
RSA should be considered as a way to RSA should be considered as a way to present clinical trial data to better present clinical trial data to better inform pts and physicians of treatment inform pts and physicians of treatment benefitbenefit
RSA is useful for designing clinical RSA is useful for designing clinical trials to ensure balanced trials to ensure balanced randomizationrandomization
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