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Therapeutic Strategies in Adjuvant Therapy of Colon Cancer. Mohamed Abdulla (M.D.) Prof. of Clinical Oncology, Kasr El-Aini School of Medicine, Cairo University. 01/04/2010. Colon Cancer; Challenging Issues:. Better Understanding of the Molecular Events. - PowerPoint PPT Presentation

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  • Therapeutic Strategies in Adjuvant Therapy of Colon CancerMohamed Abdulla (M.D.)Prof. of Clinical Oncology,Kasr El-Aini School of Medicine,Cairo University.01/04/2010

  • Colon Cancer; Challenging Issues:Better Understanding of the Molecular Events.Better Characterization of Prognostic Groups.Diagnosis in Younger Age Groups with Aggressive Behavior.Introduction of Pharmaceuticals Other Than Fluoropyremidines. Introduction of Targeted Therapies.

  • The Adenoma-Carcinoma Process:Kinzler KW, et al. New York, The genetic basis of human cancer. NY: McGraw-Hill, 1998:565-87. Vogelstein B, et al. N Engl J Med. 1988;319:525-532. Fearon ER, et al. Cell. 1990;61:759-767.Normal colonic epitheliumDysplastic aberrant crypt fociInitial adenoma developsIntermediate adenomaLate adenomaCarcinomaMetastasisMutation in APCMutation in K-rasMutation in DCCMutation in p53Other alteration?EGFR & VEGF

  • Who Should Receive Adjuvant Therapy?1. Staging System:OConnellJB, Maggard MA, Ko CY: Colon Cancer Survival Rates with The New American Joint Committee on Cancer, Sixth Edition Staging. J Natl Cancer Inst 2004;96:1423.LNs = > 12

  • Who Should Receive Adjuvant Therapy?2. Mesentric Nodules: (Contour Role):T-StageN-StageV1 (micro).V2 (macro)

    Isolated Tumor Cells & Micrometastases0 0.2 mm (N0)0.2 2 mm (N1mi)

    Stage III Not IVCancer 2008;112:504.

  • Who Should Receive Adjuvant Therapy?3. Peri-neural Invasion:An Under-Estimated Variable:15 25%JCO.2009.22.4949

  • 1/5 : Peritoneal Minimal Residual Disease.1/7 : Peritoneal Carcinomatois.Who Should Receive Adjuvant Therapy?3. Peritoneal Minimal Residual Disease:Surgical Techniques.Intraperitoneal & Intraportal Chemotherapy.HIPEC.Prevention of The Inflammatory Response.thelancet.com/oncology Vol 10 January 2009

  • Who Should Receive Adjuvant Therapy?4. Age Factor:Bouvier et al, CANCER August 15, 2008 / Volume 113 / Number 4

  • Who Should Receive Adjuvant Therapy?5. Timing of Chemotherapy Initiation:Hershman et al, CANCER December 1, 2006 / Volume 107 / Number 11

  • Accepted Standards of Care:Stage III Colon CancerLower Toxicity Profile & Better ComplianceNSABP Co1-6IMPACTNCCTGNCIC-CTG30%

  • Chemotherapeutics Other Than Fluoropyremidines:Stage III Colon Cancer:OxaliplatinUFTCapecitabineIrinotecanEffectiveness.Comparable Toxicity Profiles

  • Adjuvant FOLFOX4 in Stage II-III Colon Cancer: MOSAIC Study Schemade Gramont A, et al. ASCO 2007. Abstract 4007.FOLFOX4

    Leucovorin 200 mg/m2 IV + 5-FU 400 mg/m2 bolus + 5-FU 600 mg/m2 IV over 22 hrs +Oxaliplatin 85 mg/m2 IV(n = 1123)LV5FU2

    Leucovorin 200 mg/m2 IV + 5-FU 400 mg/m2 bolus + 5-FU 600 mg/m2 IV over 22 hrs(n = 1123)Patients with previously untreated, completely resected stage II-III colon cancer (N = 2246)

  • MOSAIC Study: 6-Y OAS; by Treatment Arm:J Clin Oncol. 2009,27:3109-3116

  • MOSAIC Study: 6-Y OAS; by Treatment Arm & Stage:J Clin Oncol. 2009,27:3109-3116

  • Final MOSAIC Results (contd)Rate of peripheral sensory neuropathy decreased over timeAt 4 yrsGrade 1: 12.0%Grade 2: 2.8%Grade 3: 0.7%Neutropenia grade 3 in 41.0% of patients receiving FOLFOX4 vs 4.7% of patients receiving LV5FU2Febrile neutropenia in 1.8% of patients receiving FOLFOX4de Gramont A, et al. ASCO 2007. Abstract 4007.

  • No Significant Survival Advantage for The Following Groups: Stage II Disease.Stage III Disease:Female Sex.> 65 Years old.T4 Tumors.N1 Disease.Poorly Differentiated Tumors.CEA > 5.Vascular Invasion.

    Final MOSAIC Results (contd)J Clin Oncol. 2009,27:3109-3116J Clin Oncol, Vol 27, No 19 (July 1), 2009: pp 3082-3084

  • Role of Irinotecan in Adjuvant Treatment of Stage III Colon Cancer PETACC-3 Study:J Clin Oncol.2009,27:3117-3125

  • Role of Irinotecan in Adjuvant Treatment of Stage III Colon Cancer PETACC-3 Study:J Clin Oncol.2009,27:3117-3125

  • Role of Irinotecan in Adjuvant Treatment of Stage III Colon Cancer PETACC-3 Study:J Clin Oncol.2009,27:3117-3125After Exclusion of Cases Developed Second Primary in Both Arms

  • Equivalent PFS in Head to Head Comparison in Metastatic Sitting.

    Biological Alteration in Metastatic or Recurrent Disease (Topoisomerase I).Oxaliplatin Versus Irinotecan:J Clin Oncol.2005, 23:4866-4875

  • IntestineLiverCapecitabine5'-DFCR5'-DFURCyD5'-DFCR5'-DFUR5-FUTumor >> healthy tissueCapecitabineCyDCE5'-DFCR = 5'-deoxy-5-fluorocytidine; 5'-DFUR = 5'-deoxy-5-fluorouridine;CyD = cytidine deaminase; CE = carboxylesteraseCapecitabine mode of action:TP-activation proof of concept at last?Thymidinephosphorylase (TP)

  • X-ACT: Xeloda (capecitabine) Adjuvant Chemotherapy Trial of stage III colon cancerPrimary endpoint: non-inferiority in DFSSecondary endpoint: OSBolus 5-FU/LV5-FU 425mg/m2 + LV 20mg/m2 days 15 q4wCapecitabine1,250mg/m2 b.i.d. days 114 q3w Chemonave stage III resection 8 weeks n=1, 004 n=983R A N D O M I SA T I O NData cut-off: January 2007b.i.d. = twice dailyTwelves C, et al. Eur J Cancer Suppl 2007;5:1 (Abstract 1LB)

  • X-ACT: Xeloda (capecitabine) Adjuvant Chemotherapy Trial of stage III colon cancerTwelves C, et al. Eur J Cancer Suppl 2007;5:1 (Abstract 1LB)5-year DFS (%)Capecitabine 1, 004 60.85-FU/LV983 56.71.00.80.60.40.200642487896MonthsHR=0.88 (95% CI: 0.771.01)NI margin 1.201218243036546066728490ITT populationEstimated probability102nTest of non-inferiority p
  • X-ACT: 5-year OS (median follow-up 6.8 years)HR=0.86 (95% CI: 0.741.01)NI margin 1.14064248789612182430365460667284901021.00.80.60.40.20Estimated probabilityTest of non-inferiority p=0.000116Test of superiority p=0.065-year OS (%)Capecitabine 1, 004 71.45-FU/LV983 68.4n0642487896Months1218243036546066728490102Twelves C, et al. Eur J Cancer Suppl 2007;5:1 (Abstract 1LB)

  • NeutropeniaNausea/ vomitingStomatitisDiarrhoeaFebrile neutropeniaHFSPatients (%)*****p
  • X-ACT and MOSAIC: projection of OS in stage III patientsITT populationEstimated probability024681.00.80.60.4YearsX-ACT1MOSAIC21Twelves C, et al. Eur J Cancer Suppl 2007;5:1 (Abstract 1LB)2De Gramont A, et al. J Clin Oncol 2007;25:(Suppl. 18):165s (Abstract 4007)Estimated probability1.00.80.60.4Years02468

  • Chemo/ radiotherapy-nave stage III colon cancer Bolus 5-FU/LV Mayo Clinic or Roswell ParkCAPOXCapecitabine 1,000mg/m2 b.i.d. days 115 Oxaliplatin 130mg/m2 day 1 q3wSchmoll HJ, et al. J Clin Oncol 2007;25:421723CAPOX: a new optionin the adjuvant setting:Primary endpoint: disease-free survivaln=944 n=942R A N D O M I SA T I O N

  • Grade 3/4 adverse eventsPatients (%)CAPOX1 (n=938) FOLFOX42 (n=1,108)FLOX3 (n=1,200)Cross-trial comparison*Not reportedNeutropeniaNauseaStomatitisDiarrhoeaFebrile neutropeniaHFSVomitingNeurosensory1Schmiegel WH, et al. J Clin Oncol 2007;25(Suppl. 18):172s (Abstract 4034) 2Andr T, et al. N Engl J Med 2004;350:234351 3Wolmark N, et al. J Clin Oncol 2005;23(Suppl. 16 Pt I):246s (Abstract LBA 3500)*Adjuvant CAPOX: favourable toxicity compared with FOLFOX and FLOX:**50403020100

  • Newly Emerged Strategies:Stage III Colon Cancer:NSABP-C0 - 6: 1608 ptsUFT5-Fu/LVDFSOAS66.9%68.3%78.7%78.7%Similar Toxicity Profile

  • Targeted Therapy in The Adjuvant Sitting

  • Stages at which angiogenesis plays a role in tumor progressionPremalignant stageMalignant tumorTumor growthVascular invasionDormant micrometastasisOvert metastasisAvascular tumorAngiogenic switchVascularized tumorTumor cell intravasationSeeding in distant organsSecondary angiogenesisAngiogenesis Is Involved Throughout Tumor Growth and MetastasisPoon RT, et al. J Clin Oncol. 2001;19:1207-1225. Reproduced with permission from the American Society of Clinical Oncology.

  • Trials of bevacizumab/capecitabine/Oxaliplatin in the adjuvant setting

    Trial

    n

    Cancer

    Treatment

    E5202(Cooperative)

    3,610

    Stage II colon

    FOLFOX bevacizumab (high risk)Observation (low risk)

    NSABP C-08(Cooperative)

    2,714

    Stage II/III colon

    FOLFOX bevacizumab

    QUASAR-2(Cooperative)

    2,240

    Stage II/III colon

    Capecitabine bevacizumab

    XELOXA(Cooperative)

    1,886

    Stage III colon

    CAPOX vs bolus 5-FU(Mayo Clinic or Roswell Park regimen)

    AVANT (Roche)

    3,450

    Stage II/III colon

    FOLFOX vs FOLFOX + bevacizumab vs XELOX + bevacizumab

  • Important adjuvant capecitabine/bevacizumab-based combination trials20042005200620072008200920102011XELOXA final safetyXELOXA 1 efficacyXELOXA survival follow-upQUASAR-2 1 efficacyAVANT 1 efficacyNSABP C-08 1 efficacy

  • NSABP Protocol C-08: mFOLFOX Bevacizumab in Stage II/III CRCWolmark N, et al. ASCO 2009. Abstract LBA4.Arm A: mFOLFOX6 Q2W x 26 (n = 1356)Arm B: mFOLFOX6 + Bevacizumab 5 mg/kg Q2W x 26 (n = 1354)Pts with stage II or III colon adenocarcinoma with ECOG PS of 0/11(N = 2710)Pts stratified by number of positive lymph nodes and randomized between Days 29 and 50 postoperativelymFOLFOX6 regimen: LV 400 mg/m2 IV, 5-FU 400 mg/m2 IV, 5-FU 2400 mg/m2 over 46 hours; oxaliplatin 85 mg/m2 IVPrimary endpoint: DFS

  • NSABP Protocol C-08: 3-Yr DFS Results:Wolmark N, et al. ASCO 2009. Abstract LBA4. DFS (%)Yrs02040608010000.51.01.52.02.53.03.5HR: 0.89 (P = .15)mFF6 + B mFF6Events 291 3123-Yr DFS 77.4 75.5

  • Anti-EGFR in Adjuvant ttt of Stage III Colon Cancer:Study Duration: 11/05 11/11.DFS, OAS & Safety.FOLFOX4+Cetuximab vs FOLFOX4.??

  • Stage II Disease:Stage IIStage IIIStage IIStage IIIStage IIStage IIStage IIIStage IIStage IIStage III

  • Issues to Be Considered:75 80% are cured with surgery alone.No current method to identify the subset of patients at higher risk of recurrence.Minimal benefit of adding chemotherapy.The associated significant morbidity.

  • Stage II Colon Cancer:QUASAR STUDY, 20043300 PTSSurgerySurgery +5-Fu/LV5% OAS1% Mortality5% OAS5% OAS1% Mortality5% OAS

  • Stage II Colon Cancer:Kerr D, et al. ASCO 2009. Abstract 4000.

  • Stage II Colon Cancer:QUASAR Validation Results: Recurrence score (per 25 units) predictive of DFS and OS DFS HR: 1.42 (95% CI: 1.09-1.84; P = .010) OS HR: 1.33 (95% CI: 1.01-1.76; P = .041) No significant differences in treatment score by treatment interaction in OS, DFS, or relapse-free intervalKerr D, et al. ASCO 2009. Abstract 4000.

    Clinical or Pathologic VariableHR (95% CI)P ValueMMR (deficient vs proficient)0.32 (0.15-0.69)< .001Tumor stage (T4 vs T3)1.83 (1.23-2.75).005Tumor grade (high vs low)0.62 (0.40-0.96).026Number of nodes examined (< vs 12)1.47 (1.01-2.14).040LVI (present vs absent)1.40 (0.88-2.23).175Recurrence score (continuous, per 25 units)1.61 (1.13-2.29).008

  • Study designed to compare the incidence of molecular biomarkers in pts with stage II/III CRC in the PETACC 3 trial (N = 3278).Frequency of MSI-H significantly higher in stage II (22%) vs stage III (12%) disease (P < .0001).Higher frequency of MSI detected in N0 tumors compared with N1 or N2 (P < .0001).Higher tumor stage correlated with increased frequency of MSI (T1/T2 vs T3 vs T4) (P = .037).

    Prognostic Value of CRC Biomarkers: Translational Study on PETACC 3Roth AD, et al. ASCO 2009. Abstract 4002.

  • Translational Study on PETACC 3: Results:Strong effect in stage II, decreases in stage III diseaseRoth AD, et al. ASCO 2009. Abstract 4002.

    Parameter, %HR95% CIP ValueBoth stage II and III (N = 1233) RFS0.5690.400-0.811.0018 OS0.5480.357-0.842.006Stage II (n = 391) RFS0.2650.107-0.661.0044 OS0.1590.039-0.659.011Stage III (n = 842) RFS0.6930.473-1.02.06 OS0.6990.446-1.09.12

  • Stage II Colon Cancer:Preoperative CEA Level:Journal of Surgical Oncology 2009;99:6570

  • Keep in Mind:Number of LNs > 12.Timing: 4-8 wks.Age.Molecular Markers.5-Fu/LV is the Backbone.Stage II Disease: Better Assessment.Stage III Disease: MOSAIC & X-ACT.The Role of Adjuvant Targeted Therapy.