Post on 18-Jan-2016
The Combination of Bevacizumab (Bev) with capecitabine/irinotecan (CapIri/Bev) or capecitabine/oxaliplatin
(CapOx/Bev) is highly active in advanced colorectal cancer (ACRC): A randomized phase II study of the AIO Colorectal
Study Group (AIO trial 0604)
A. Reinacher-Schick1, S. Kubicka2, W. Freier3, D. Arnold4, G. Dietrich5, M. Geißler6, S. Hegewisch-Becker7, U. Graeven8, H.-J. Schmoll4 and W. Schmiegel1,
Ruhr University Bochum1, University Hannover2, Center of Oncology Hildesheim3, Martin-Luther-University Halle-Wittenberg4, Hospital Bietigheim, Bietigheim-Bissingen5, Community Hospital Esslingen6, Center of Oncology Eppendorf, Hamburg7, Maria Hilf Hospital Mönchengladbach8,
Germany
• Addition of Bevacizumab to 5FU/FA/irinotecan1 and 5FU/FA/oxaliplatin2,3 improves progression free survival (PFS) in advanced CRC (aCRC)
• Efficacy of Capecitabine/Oxaliplatin (CapOx) is similar to 5-FU/FA/Oxaliplatin
• Data on Capecitabine/Irinotecan (CapIri) combinations remains controversial, due to toxicity 4-7
1 Hurwitz, N Engl J Med 2004; 2 Giantonio, JCO 2007; 3 Saltz, JCO 2008; 4 Fuchs, JCO 2007; 5 Köhne, Ann Oncol 2008; 6 Grothey, ASCO 2003; 7 Koopman, Lancet 2007
Background
Aim
To investigate whether bevacizumab in combination with
CapOx or CapIri is effective for patients with aCRC
Study Design
Open-label, multicenter, randomized phase II study
Primary endpoint:Rate of pts. without disease progression at 6 months: Exclude insufficient activity (defined as rate < 60%)
Secondary endpoints:Overall survival, toxicity, resectability of liver/lung mets.
Main eligibility criteria
- written informed consent
- histologically proven aCRC, measurable lesion (RECIST)
- Age > 18 years
- ECOG performance status < 2
- Adequate haematological, renal and hepatic function
- no previous systemic immunotherapy or chemotherapy
(except (neo)adjuvant therapy for non-metastatic disease > 6 months)
- history of thrombosis or severe bleeding < 6 months, bleeding diathesis, therapeutic anticoagulation
- proteinuria < +1 by dipstick urin analysis
Treatment protocolArm A: d 1
d 15
Oxaliplatin130mg/m2, 120min i.v.Bevacizumab 7,5 mg/kg i.v. Capecitabine 1000mg/m2 p.o., 2x daily
Arm B: (*)Irinotecan200mg/m2, 30min i.v.Bevacizumab 7,5 mg/kg i.v. Capecitabine800mg/m2 p.o., 2x daily
q 3wks
note dose reduction of CapIri compared to previous trials for safety reasons
Patient accrualRekrutierungsbersicht
0
50
100
150
200
250
300
Jul05
Aug05
Sep05
Oct05
Nov05
Dec05
Jan06
Feb06
Mar06
Apr06
May06
Jun06
Jul06
Aug06
Sep06
Oct06
Soll
Ist
observedexpected
Baseline characteristics (n=247) No. Patients
Arm A127
Arm B120
Median age (range), years 64 (27-83) 64.5 (30-82) Distribution of age, % < 40 years 4 2 40-49 years 8 7 50-59 years 23 23 60-69 years 35 42 70-79 years 29 22 > 80 years 2 2 Male, female % 66 / 34 67 / 33 ECOG Performance status, %
0 52 52 1 45 46 2 3 2
Prior adjuvant therapy, % No 77 79 Yes 23 21
Treatment characteristics (n=247)
Number of pats.
Arm A127
Arm B120
Total247
Number of cycles (evaluable pats.)
1158 1269 2427
Mean no. of cycles (+/- SD)
9.1 (+/- 6.7) 10.6 (+/-7.1) 9.9 (+/-6.9)
Range 1-37 1-38 1-38
Median 8 9 9
Reasons for end of treatment, EOT (n=222)
Reason for EOT
n
Arm A
116
Arm B
108
Total
222
Disease Progression
46 (40%) 35 (32%) 81 (36%)
Progression free 70 (60%) 73 (68%) 143 (64%)
- toxicity 27 (39%) 12 (16%) 39 (27%)
- SAE 5 (7%) 8 (11%) 13 (9%)
- death, not tumor related
4 (6%) - 4 (3%)
- protocol violation 2 (3%) 5 (7%) 7 (5%)
- consent withdrawn 11 (16%) 14 (19%) 25 (17%)
- lost to follow-up 1 (1%) 2 (3%) 3 (2%)
- Resection/Ablation 4 (6%) 6 (8%) 10 (7%)
- Other 16 (23%) 26 (36%) 42 (29%)*end of treatment information available for n=222 pts.
CTC V. 3.0 Grade 3 and 4 Toxicities (n=247)
Related toxicities
Arm A (127)3°/4° [%]
Arm B (120)3°/4° [%]
Diarrhoea 21/0 16/0
Sensory neuropathy 24/1 0
Hand-Foot-Syndrome 11/0 8/0
Neutropenia 2/0 8/2
Thrombocytopenia 6/0 0
Fatigue 2/1 3/0
Ileus 2/1 2/0
Nausea 3/0 3/0
Vomiting 4/0 5/0
AEs of special interest (n=247)
AEs of special interest (Bev)
Arm A (127)3°/4° [%]
Arm B (120)3°/4° [%]
Thrombosis/Embolism - venous access thrombosis - other (incl. pulmonary emb.)
3/21/02/2
4/11/03/1
Hypertension 4/0 3/0
Cardiac ischemia/infarction 0 0/1
Hemorrhage/bleeding (GI) 1/0 0
Best overall response* (n=247)
Arm A
% of patients(n =127)
Arm B% of patients
(n =120)
CR 5 6 PR 48 49 SD 29 28 PD 5 6 NE/NA** 13 11
*ITT, RECIST criteria, investigator‘s assessment; **not evaluated/not available
PFS rate after 6 months: Primary endpoint
Arm A% of patients
(n =127)
Arm B% of patients
(n =120)
PFS rate/6 mo.
76 84
months
rate
with
out p
rogr
essi
on
0 6 12 18 24 30 36
0.0
0.2
0.4
0.6
0.8
1.0
Progression-free Survival by Treatment
Logrank test: p = 0.27
A : n = 127, 98 events, median = 10.4 monthsB : n = 120, 91 events, median = 12.1 months
Fig. 4.2_______
Progression free survival (PFS) - ITT analysis
months
rate
with
ou
t pro
gre
ssio
n
0 6 12 18 24 30 36
months
0.0
0.2
0.4
0.6
0.8
1.0
surv
ival
rat
e
Overall Survival by Treatment
Fig. 4.5_______
Logrank test: p = 0.55
A : n = 127, 46 events, median = 26.7 monthsB : n = 120, 40 events, median = NA
months
Su
rviv
al r
ate
Overall survival (OS) - ITT analysis
Conclusion• Both regimens, CapOx/Bev and CapIri/Bev,
are highly active in aCRC.
• The dose reduction of CapIri/Bev may lead to a favourable toxicity profile compared to previous capecitabine/irinotecan trials seemingly without compromising efficacy
• The CapIri/Bev arm - compared to the CapOx/Bev arm - seems to be associated with higher cycle numbers and a tendency towards longer PFS
Acknowledgements
We would like to thank
- the patients and their families- the co-investigators- the study nurses and data monitors- Roche Pharma AG and Sanofi-Aventis for financial support