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Management of
Metastatic Colorectal
      Cancer
         Dr Sujay Susikar
      Post Graduate Student
  Department of Surgical Oncology
  Government Royapettah Hospital
The challenges of metastatic CRC
        • A significant number of
          patients present with          ~40%
          metastatic disease



 ~50%               • Many newly diagnosed patients
                      eventually develop metastatic
                      disease


5-year survival rate —
    2% (if unresectable) to 50% (if resectable)
Management of synchronous metastasis
                                      Non               Systemic
              Synchronous          obstructing           therapy
              addominal/
               peritoneal                             Colon resection/
                 mets             Obstructing or
                                                         diverting            Systemic
                                    imminent
                                                        colostomy/             therapy
                                   obstruction
                                                      bypass/ stenting
Synchronous
 Metastatic
 colorectal
 carcinoma                                                     Colectomy with
                                                            synchronous or staged
                                                          resection OR neoadjuvant
                                         Resectable         chemo OR colectolmy
                                                                                             Adjuvant
                                                                                             therapy
                                                            F/B chemo and staged
                                                                   resection
              Synchronous liver
              and /or lung only
                    mets
                                                                              Converted to resectable
                                                                                – synchronous or
                                                                                 staged resection
                                      Unresectable            Systemic
                                                               therapy         Remains unresectable –
                                                                                 continuum of care
Management of metachronous
       metastasis
Management of potentially resectable
     colorectal cancer liver metastases
Regional treatments for hepatic metastases from CRC
 Surgical resection
 Local tumor ablation
       Percutaneous injection
       Cryotherapy,
       Radiofrequency ablation
   Regional hepatic intraarterial chemotherapy
   Chemoembolization,
   Radiation therapy (RT).

     Only surgery is associated with a survival advantage
Management of potentially resectable
     colorectal cancer liver metastases

   Resection offers the greatest likelihood of cure
    for patients with liver-isolated CRC.
   Five -year survival rates after resection range
    from 24 to 58 percent, averaging 40 percent
   Surgical mortality rates are generally <5 %
Patient selection for resection
Criteria for absolute unresectability
 Nontreatable extrahepatic disease,
 Unfit for surgery
 Involvement of more than 70 percent of the liver or six
  segments
 Radiographic evidence of involvement of the hepatic artery,
  major bile ducts, main portal vein, or celiac/paraaortic
  lymph nodes

Modern multidisciplinary consensus defines resectable CRC
 liver metastases simply as tumors that can be resected
 completely, leaving an adequate liver remnant
CRITERIA FOR RESECTABILITY
    General criteria for fitness
1.   Good performance status
2.   Absence of extra hepatic disease

    Specific Criteria that decides the outcome
1.   Risk of recurrence- Clinical Risk Score for CRC

    Anatomical criteria for resectability
1.   Number of metastases
2.   Precise location
3.   Relationship with the portal pedicle and the hepatic veins
Clinical Risk Score

5 clinical criteria each assigned 1 point:

1) Node-positive primary
2)<12 month disease-free interval
3) >1 liver tumors
4) Largest tumor >5 cm
5) CEA >200 ng/mL.
Principles of Resection in Colorectal Liver
                    Metastases
   An R0 resection of both the intra- and extrahepatic
    disease sites must be feasible.
   At least two adjacent liver segments need to be spared.
   Vascular inflow and outflow, as well as biliary drainage
    to the remaining segments, must be preserved.
   The volume of the liver remaining after resection (i.e.,
    the future liver remnant) must be adequate
Preoperative Patient Evaluation
   Colonoscopy
   Chest / abdominal/ pelvic CT
   CBC, Platelets, Chemistry
   CEA
   Determination of tumor K- RAS status
   Needle biopsy – if clinically indicated
   PET – CT only if potentially surgically curable M1 disease
Conversion therapy for initially
       unresectable metastases


 Induction chemotherapy in patients with
isolated but initially unresectable CRC liver
metastases
Selecting patients for neoadjuvant
                    therapy
   Resection was always preferred, if possible, over local ablation
    strategies (cryosurgery, radiofrequency ablation [RFA], laser
    techniques).

   Immediate resection appropriate if adequate margins could be
    radiographically defined, there was no portal lymph node
    involvement, and four or fewer lesions. Resection could be
    considered for more than four lesions if they were localized to
    a single lobe.

   For patients with more than four metastases or bilobar
    involvement, resection considered appropriate only after
    tumor shrinkage using neoadjuvant chemotherapy.
TIMING OF HEPATECTOMY IN PATIENTS
      PRESENTING WITH SYNCHRONOUS
               METASTASES

   Staged – Allows biological behavior of the metastatic
    disease become evident, improving the selection of
    patients

   Simultaneous resection of the primary and metastatic
    disease - preferable from the patient's perspective


    No proof of inferior survival or greater morbidity for a one-stage
    procedure as compared to delayed (staged) hepatic resection
SURVEILLANCE AFTER
           METASTASECTOMY
Surveillance strategy for patients with stage IV disease who
  are rendered surgically NED (no evidence of disease)
 CEA every three months for two years, then every six
  months for three to five years
 CT of the chest/abdomen and pelvis every three to six
  months for two years, then every 6 to 12 months up to a
  total of five years
 Colonoscopy in one year; if no advanced adenoma repeat
  in three years, then every five years; if advanced adenoma
  is found, repeat in one year
ABLATION
Indications
 Patients who do not meet the criteria for
  resectability

   Presence of liver-only disease.

   A complete margin-negative ablation can be
    achieved
ABLATION
1. Cryotherapy
     Destruction of tumor cells by freeze thaw
      cycle.
     Probe positioned inside tumor
     Liquid nitrogen is circulated through tip of
      probe
     Temp lowered to -100° C
     1-3 cycles of freezing for 15 mins with
      spontaneous periods of thaw
     Lethal temp -20° C
     Intracellular or extra cellular ice forms
     Ice ball of ~3-6cm
     Complications - biliary, abscess,
      myoglobinuria, haemorrhage, coagulopathy,
      cryoshock
ABLATION
2. Radiofrequency ablation
       Radiofrequency waves (high frequency
        alternating current - 460khz) are
        converted into thermal energy
       Friction from rapidly moving ions
        results in heat
       Temp of ~60°C
       Coagulative necrosis
       Open/laparoscopic or percutaneous
        technique
       Effective with tumors upto 5 cm
   Complications – bilioma, biliary
    fistula, stricture, abscess
ABLATION
  3. Laser interstitial thermal
     therapy (LITT)
        Placement of laser fiber or
         fibers directly into the tissue to
         be treated.
        Infrared laser producing lethal
         thermal injury to tumor cells
        LITT utilizes diode laser or
         more frequently Nd-YAG laser
        Coagulative necrosis
        Procedure is usually performed
         under MRI guidance
ABLATION
4. Microwave coagulation therapy
   Uses microwave of frequency 2450 Mhz
   Produces heat by stimulation of water
    molecule
   Produces rapid frictional heating and
    coagulative necrosis
5. Intratumoral alcohol injection
   Causes denaturation of protein leading to
    cell death
   Can be used for tumors <3cm
RADIOTHERAPY
Stereo tactic body radiation
   Tolerance of liver to radiation is poor.
   Conformational radiation therapy using
    multiple field & beam angles is used to
    deliver large doses to a target sparing
    surrounding normal tissues.
Selective Interstitial Radiation Therapy
   Injecting micro spheres containing
    yttrium 90 via hepatic artery
   Percutaneous cannulation of hepatic
    artery
   Spheres selectively lodge into tumor cells
   200-300 Gy to tumor ,15-50 Gy to liver
   Emits Beta radiation with a penetrance
    of 2-3 mm
   Half life of 64 hours.
Chemotherapy for Metastatic Colorectal
                  Cancer
Conventional chemotherapy
   Thymidylate synthase inhibitors
        Fluoropyrimidines: 5-FU (intravenous), capecitabine (oral)
        Raltitrexed
   Topoisomerase I inhibitors
        Irinotecan
   Alkylating agents
        Oxaliplatin

     Traditional 5-FU–based chemotherapy associated with modestly
    improved survival
        Newer agents (ie, irinotecan, oxaliplatin) lengthen survival outcomes
Chemotherapy for Metastatic Colorectal
              Cancer


Targeted therapies

   Bevacizumab ( Avastin)—binds the vascular
    endothelial growth factor ( VEGF).

   Cetuximab ( Erbitux)– targets the epidermal growth
    factor receptor ( EGFR).

   Pantumumab ( Vectibix)– targets the EGFR, in a
    different way than Cetuximab.
First- line chemotherapy
   FOLFOX( Oxaliplatin plus 5-FU and leucovorin Q2W)
    FOLFIRI( Irinotecan plus 5-FU and leucovorin Q2W)
       Patients should have a central line and a portable IV pump.
       In the U.S.A, most patients are offered first- line FOLFOX, and
        FOLFIRI is reserved for second- line therapy.
    CAPOX        (capecitabine plus oxaliplatin)
   Benefit of adding Bevacizumab
        A significant higher response, it prolongs survival.
   Patients who can’t tolerate Irinotecan or
    Oxaliplatin
       Less toxic alternative: 5-FU+ leucovorin( +Bevacizumab)
Multiple Active Agents Associated With
              Increased Survival
   Combinations of multiple active agents associated with better
    outcome
      5-FU, irinotecan, oxaliplatin

   Compared with 5-FU/LV, use of all 3 active therapies associated
    with improved survival
      Median survival with triple-drug regimens: ~ 20 months

   First-line doublet chemotherapy
      Associated with increased exposure to all 3 active agents
        during therapeutic course
Metastatic CRC: Which Chemotherapy
               First?

   FOLFOX = FOLFIRI
   CapeOx = FOLFOX
   Sequencing = combinations

                  FOLFOX             FOLFIRI     FOLFIRI            FOLFOX
                  (1st line          2nd line)   (1st line          2nd line)
    N pts (229)     111                69          109                81

    RR             54%                 4%         56%                15%
    Liver
                   21%                             9%
    resection
    PFS (mos)       8.1                2.5         8.5                4.2
    OS (mos)                  20.6                           21.5

    GERCOR study
Second- line chemotherapy
   If FOLFOX( or Capecitabine+ Oxaliplatin) plus
    Bevacizumab was the first line regimen, the patient is
    usually switched to FOLFIRI with or without
    Bevacizumab.
   FOLFIRI+ Bevacizumab → FOLFOX( or
    Capecitabine+ Oxaliplatin) with or without
    Bevacizumab.
   Adding Cetuximab to Irinotecan can shrink tumors in
    patients who stop responding FOLFIRI regimen.
        Cetuximab plus Irinotecan is used for third- line therapy
        after failure of both FOLFOX and FOLFIRI.
       It is also used as second– line therapy if there is progression
        on FOLFIRI plus Cetuximab.
New paradigm: continuum of care


   Exposure to all active agents and modalities


   Maximal Overall Survival and Quality Of Life by
    minimizing toxicity and unnecessary treatment


        No more distinct “lines of therapy”
Achievements in the first-line treatment of mCRC


           BSC (1980s)
        5-FU/FA (1990s)
     FOLFOX, FOLFIRI
CT combination + MAbs

      CT combination +
  Tailored MAb therapy

                          0   6     12     18     24   30
                                  Time (months)
CRC: Adenoma-Carcinoma Sequence



  Normal           Hyperproliferative
                                                    Adenoma                 Carcinoma
  Colon               Epithelium


    APC          Methylation       APC          KRAS        18q        p53         Further
   hMSH2        abnormalities     hMSH2        mutation   deletion   deletion   accumulation
   hMLH1                          hMLH1                                          of genetic
abnormalities                   inactivation                                    abnormalities
 (hereditary)

                                                 32% to 57%
                                                 KRAS mutant
Toward Personalized Therapy of CRC
                                                                  Ligand:
                                                                  AREG/EREG
                                                                Target for EGFR-ERBITUX


Target for EGFT-TK inhibitor                                    EGFR-TK
                                                         pY   GRB2
                                  pY                                      SOS
                      P13K         pY                                                RAS   RAF
                                STAT                                                   MEK
                        AKT
    PTEN
                                                                                       MAPK
                                Gene transcription
                        P       Cell-cycle progression
                  P
                               MYC                                  Cyclin D1
                         JUN   FOS
                                               MYC                  Cyclin D1
Proliferation/
 maturation
                     Chemotherapy/                                                         Survival
                                                                      Invasion and
                 radiotherapy resistance       Angiogenesis                            (anti-apoptosis)
                                                                       metastasis
Toward Personalized Therapy of CRC
   EGFR antibodies
       KRAS and BRAF mutations correlate
        with lack of response to treatment with
        monoclonal antibodies targeting EGFR
   VEGF antibodies
       Patients who do not have a
        contraindication may benefit from
        bevacizumab, although no predictive
        marker has been identified
   Combining EGFR and VEGF
    antibodies
       Data do not demonstrate benefit
NCCN: KRAS Mutation Testing
     Recommended to guide treatment plan

   KRAS codons 12 and 13
   Testing considerations
       Qualified laboratories
       Formalin-fixed paraffin-embedded tissue
       Primary tumor and/or the metastasis
NCCN: BRAF Mutation Testing
        Not yet recommended, but noted in the guidelines



   Testing considerations
     Formalin-fixed paraffin-embedded tissues
     Typically PCR and direct DNA sequence analysis

     Qualified laboratories
Chemotherapy side effects

       Drug                       Side effects
5-FU and Leucovorin    Diarrhea, mucositis, temporary low
                                  blood counts

      Xeloda                 Hand- foot syndrome
                             diarrhea and mucositis

    Irinotecan        Diarrhea, low blood counts, fatigue,
                                   hair loss
Chemotherapy side effects

  Drug                         Side effects
Oxaliplatin   Sensory neuropathy, acute paresthesias and
              dysesthesias of the hands, feet and perioral
                      region, jaw tightness, and
                         pseudolaryngospasm
 Avastin        Increase BP, impair wound healing, bleeding,
              bowel perforation(1.4~2%) and fistula formation,
                 proteinuria, thromboembolic events(4.5%):
                              stroke, heart attack
 Erbitux         Allergic reactions, skin rash, headache,
                     nausea, low blood magnesium
Duration of therapy
   Traditional practice – continue till
     Unacceptable toxicity
     Clinical deterioration or

     Disease progression



   Newer approach – discontinuation of treatment
    after fixed time period
Treatment-Free Intervals
   Rationale
      Decrease intensity of therapy

      Reduce toxicity

      Prevent discontinuation of therapy

      Increase QOL



   Types of treatment breaks
       Treatment break with maintenance regimen
       Complete Chemotherapy-free intervals (CFI)
Metastatic CRC: Progress in OS
                               BSC        4–6 months

                            5-FU/AF               11–14.7 months

                    IFL or FOLFIRI                     15–17.4 months

  5-FU/AF + bevacizumab                                  18.3 months

         FOLFOX4 or CapeOx                                   16.2–20 months

           IFL + bevacizumab                                  20.3 months

         FOLFOX6  FOLFIRI                                    20.6 months
  Bevacizumab+ FOLFOX/CAPOX
                                                                21.3 months

         FOLFIRI  FOLFOX6                                         21.5 months

         Cetuximab + Std CT*0                                        23.5 months
* KRAS wild type patients             6   OS (months) 18
                                              12                24
Assessment during therapy
   CT scan, PET ( every 2~3 cycles)
   CEA ( every 1~3months)
       Persistently rising CEA levels should prompt restaging, but
        suggest disease progression and the need for an alternative
        treatment strategy.
       Caution should be used when interpreting a rising CEA level
        during the first 4 to 6 weeks of a new therapy, since spurious
        early elevation in serum CEA may occur, especially after
        Oxaliplatin.
Management of metastatic colorectal
               cancer
General Principles
 Patients with mCRC, particularly those with liver or lung only metastases,
  should be carefully evaluated upfront to determine the feasibility of curative
  resection
 The current approach to the treatment of mCRC is to use various agents (5-
  fluorouracil/leucovorin [5-FU/LV], capecitabine, irinotecan, oxaliplatin,
  bevacizumab, cetuximab, and patitumumab) in combination or as single
  agents
 FOLFIRI (infusional 5-FU, leucovorin, plus irinotecan) and FOLFOX
  (infusional 5-FU, leucovorin, plus oxaliplatin) exhibit similar efficacy in
  mCRC.
  5-FU/LV in patients who cannot tolerate intensive therapy , either may be
  combined with bevacizumab
Unusual colorectal
     tumors
Carcinoid tumors
   Neuroendocrine tumors
   More common in appendix and rectum
   Half are functional – MC produce seratonin
   Appendicial carcinoids
       < 1 cm – no risk of metastasis and managed with
        appendectomy
       Tumors 1 – 2 cm – controversial
       > 2 cm – managed with formal right hemicolectomy
   Rectal carcinoids – typically not functional
       < 1 cm never metastasize – managed with local excision
        or fulguration
       1 – 2 cm controversial
       > 2cm – more radical surgery
High grade neuroendocrine carcinoma
        Extrapulmonary small cell
    carcinoma
   Chest imaging always performed to
    rule out mets from lung
   Nonspecific presentation and clinical
    features similar to adenocarcinoma
   Distant spread common
   Recommendations extrapolated
    from small cell lung cancer
   Combined modality treatment with
    chemo and surgery
Lymphoma
   Majority non Hodgkins type
   Maybe low, intermediate or high grade
    histology
   B cell diffuse large cell histology most
    common
   Majority affect cecum or rectum
   Usually present with non specific
    abdominal pain, rectal bleeding,
    obstruction or a mass
   Diagnosis made n histology
   Work up – bone marrow biopsy, full body
    scanning
   Treatment – combined modality with
    chemotherapy and surgery
   Role of radiation therapy unclear
Conclusion
   Patients with mCRC, particularly those with
    liver or lung only metastases, should be carefully
    evaluated upfront to determine the feasibility of
    curative resection
   The availability of multiple therapies and the
    judicious use of surgery have improved
    outcomes for metastatic CRC
   Use of these agents may soon be individualized
    as data about predictive factors evolves
 management of metastatic colorectal cancer

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management of metastatic colorectal cancer

  • 1. Management of Metastatic Colorectal Cancer Dr Sujay Susikar Post Graduate Student Department of Surgical Oncology Government Royapettah Hospital
  • 2. The challenges of metastatic CRC • A significant number of patients present with ~40% metastatic disease ~50% • Many newly diagnosed patients eventually develop metastatic disease 5-year survival rate — 2% (if unresectable) to 50% (if resectable)
  • 3. Management of synchronous metastasis Non Systemic Synchronous obstructing therapy addominal/ peritoneal Colon resection/ mets Obstructing or diverting Systemic imminent colostomy/ therapy obstruction bypass/ stenting Synchronous Metastatic colorectal carcinoma Colectomy with synchronous or staged resection OR neoadjuvant Resectable chemo OR colectolmy Adjuvant therapy F/B chemo and staged resection Synchronous liver and /or lung only mets Converted to resectable – synchronous or staged resection Unresectable Systemic therapy Remains unresectable – continuum of care
  • 5. Management of potentially resectable colorectal cancer liver metastases Regional treatments for hepatic metastases from CRC  Surgical resection  Local tumor ablation  Percutaneous injection  Cryotherapy,  Radiofrequency ablation  Regional hepatic intraarterial chemotherapy  Chemoembolization,  Radiation therapy (RT). Only surgery is associated with a survival advantage
  • 6. Management of potentially resectable colorectal cancer liver metastases  Resection offers the greatest likelihood of cure for patients with liver-isolated CRC.  Five -year survival rates after resection range from 24 to 58 percent, averaging 40 percent  Surgical mortality rates are generally <5 %
  • 7. Patient selection for resection Criteria for absolute unresectability  Nontreatable extrahepatic disease,  Unfit for surgery  Involvement of more than 70 percent of the liver or six segments  Radiographic evidence of involvement of the hepatic artery, major bile ducts, main portal vein, or celiac/paraaortic lymph nodes Modern multidisciplinary consensus defines resectable CRC liver metastases simply as tumors that can be resected completely, leaving an adequate liver remnant
  • 8. CRITERIA FOR RESECTABILITY  General criteria for fitness 1. Good performance status 2. Absence of extra hepatic disease  Specific Criteria that decides the outcome 1. Risk of recurrence- Clinical Risk Score for CRC  Anatomical criteria for resectability 1. Number of metastases 2. Precise location 3. Relationship with the portal pedicle and the hepatic veins
  • 9. Clinical Risk Score 5 clinical criteria each assigned 1 point: 1) Node-positive primary 2)<12 month disease-free interval 3) >1 liver tumors 4) Largest tumor >5 cm 5) CEA >200 ng/mL.
  • 10. Principles of Resection in Colorectal Liver Metastases  An R0 resection of both the intra- and extrahepatic disease sites must be feasible.  At least two adjacent liver segments need to be spared.  Vascular inflow and outflow, as well as biliary drainage to the remaining segments, must be preserved.  The volume of the liver remaining after resection (i.e., the future liver remnant) must be adequate
  • 11. Preoperative Patient Evaluation  Colonoscopy  Chest / abdominal/ pelvic CT  CBC, Platelets, Chemistry  CEA  Determination of tumor K- RAS status  Needle biopsy – if clinically indicated  PET – CT only if potentially surgically curable M1 disease
  • 12. Conversion therapy for initially unresectable metastases Induction chemotherapy in patients with isolated but initially unresectable CRC liver metastases
  • 13. Selecting patients for neoadjuvant therapy  Resection was always preferred, if possible, over local ablation strategies (cryosurgery, radiofrequency ablation [RFA], laser techniques).  Immediate resection appropriate if adequate margins could be radiographically defined, there was no portal lymph node involvement, and four or fewer lesions. Resection could be considered for more than four lesions if they were localized to a single lobe.  For patients with more than four metastases or bilobar involvement, resection considered appropriate only after tumor shrinkage using neoadjuvant chemotherapy.
  • 14. TIMING OF HEPATECTOMY IN PATIENTS PRESENTING WITH SYNCHRONOUS METASTASES  Staged – Allows biological behavior of the metastatic disease become evident, improving the selection of patients  Simultaneous resection of the primary and metastatic disease - preferable from the patient's perspective No proof of inferior survival or greater morbidity for a one-stage procedure as compared to delayed (staged) hepatic resection
  • 15. SURVEILLANCE AFTER METASTASECTOMY Surveillance strategy for patients with stage IV disease who are rendered surgically NED (no evidence of disease)  CEA every three months for two years, then every six months for three to five years  CT of the chest/abdomen and pelvis every three to six months for two years, then every 6 to 12 months up to a total of five years  Colonoscopy in one year; if no advanced adenoma repeat in three years, then every five years; if advanced adenoma is found, repeat in one year
  • 16. ABLATION Indications  Patients who do not meet the criteria for resectability  Presence of liver-only disease.  A complete margin-negative ablation can be achieved
  • 17. ABLATION 1. Cryotherapy  Destruction of tumor cells by freeze thaw cycle.  Probe positioned inside tumor  Liquid nitrogen is circulated through tip of probe  Temp lowered to -100° C  1-3 cycles of freezing for 15 mins with spontaneous periods of thaw  Lethal temp -20° C  Intracellular or extra cellular ice forms  Ice ball of ~3-6cm  Complications - biliary, abscess, myoglobinuria, haemorrhage, coagulopathy, cryoshock
  • 18. ABLATION 2. Radiofrequency ablation  Radiofrequency waves (high frequency alternating current - 460khz) are converted into thermal energy  Friction from rapidly moving ions results in heat  Temp of ~60°C  Coagulative necrosis  Open/laparoscopic or percutaneous technique  Effective with tumors upto 5 cm  Complications – bilioma, biliary fistula, stricture, abscess
  • 19. ABLATION 3. Laser interstitial thermal therapy (LITT)  Placement of laser fiber or fibers directly into the tissue to be treated.  Infrared laser producing lethal thermal injury to tumor cells  LITT utilizes diode laser or more frequently Nd-YAG laser  Coagulative necrosis  Procedure is usually performed under MRI guidance
  • 20. ABLATION 4. Microwave coagulation therapy  Uses microwave of frequency 2450 Mhz  Produces heat by stimulation of water molecule  Produces rapid frictional heating and coagulative necrosis 5. Intratumoral alcohol injection  Causes denaturation of protein leading to cell death  Can be used for tumors <3cm
  • 21. RADIOTHERAPY Stereo tactic body radiation  Tolerance of liver to radiation is poor.  Conformational radiation therapy using multiple field & beam angles is used to deliver large doses to a target sparing surrounding normal tissues.
  • 22. Selective Interstitial Radiation Therapy  Injecting micro spheres containing yttrium 90 via hepatic artery  Percutaneous cannulation of hepatic artery  Spheres selectively lodge into tumor cells  200-300 Gy to tumor ,15-50 Gy to liver  Emits Beta radiation with a penetrance of 2-3 mm  Half life of 64 hours.
  • 23. Chemotherapy for Metastatic Colorectal Cancer Conventional chemotherapy  Thymidylate synthase inhibitors  Fluoropyrimidines: 5-FU (intravenous), capecitabine (oral)  Raltitrexed  Topoisomerase I inhibitors  Irinotecan  Alkylating agents  Oxaliplatin Traditional 5-FU–based chemotherapy associated with modestly improved survival  Newer agents (ie, irinotecan, oxaliplatin) lengthen survival outcomes
  • 24. Chemotherapy for Metastatic Colorectal Cancer Targeted therapies  Bevacizumab ( Avastin)—binds the vascular endothelial growth factor ( VEGF).  Cetuximab ( Erbitux)– targets the epidermal growth factor receptor ( EGFR).  Pantumumab ( Vectibix)– targets the EGFR, in a different way than Cetuximab.
  • 25. First- line chemotherapy  FOLFOX( Oxaliplatin plus 5-FU and leucovorin Q2W) FOLFIRI( Irinotecan plus 5-FU and leucovorin Q2W)  Patients should have a central line and a portable IV pump.  In the U.S.A, most patients are offered first- line FOLFOX, and FOLFIRI is reserved for second- line therapy. CAPOX (capecitabine plus oxaliplatin)  Benefit of adding Bevacizumab A significant higher response, it prolongs survival.  Patients who can’t tolerate Irinotecan or Oxaliplatin  Less toxic alternative: 5-FU+ leucovorin( +Bevacizumab)
  • 26. Multiple Active Agents Associated With Increased Survival  Combinations of multiple active agents associated with better outcome  5-FU, irinotecan, oxaliplatin  Compared with 5-FU/LV, use of all 3 active therapies associated with improved survival  Median survival with triple-drug regimens: ~ 20 months  First-line doublet chemotherapy  Associated with increased exposure to all 3 active agents during therapeutic course
  • 27. Metastatic CRC: Which Chemotherapy First?  FOLFOX = FOLFIRI  CapeOx = FOLFOX  Sequencing = combinations FOLFOX FOLFIRI FOLFIRI FOLFOX (1st line 2nd line) (1st line 2nd line) N pts (229) 111 69 109 81 RR 54% 4% 56% 15% Liver 21% 9% resection PFS (mos) 8.1 2.5 8.5 4.2 OS (mos) 20.6 21.5 GERCOR study
  • 28. Second- line chemotherapy  If FOLFOX( or Capecitabine+ Oxaliplatin) plus Bevacizumab was the first line regimen, the patient is usually switched to FOLFIRI with or without Bevacizumab.  FOLFIRI+ Bevacizumab → FOLFOX( or Capecitabine+ Oxaliplatin) with or without Bevacizumab.  Adding Cetuximab to Irinotecan can shrink tumors in patients who stop responding FOLFIRI regimen.  Cetuximab plus Irinotecan is used for third- line therapy after failure of both FOLFOX and FOLFIRI.  It is also used as second– line therapy if there is progression on FOLFIRI plus Cetuximab.
  • 29. New paradigm: continuum of care  Exposure to all active agents and modalities  Maximal Overall Survival and Quality Of Life by minimizing toxicity and unnecessary treatment No more distinct “lines of therapy”
  • 30. Achievements in the first-line treatment of mCRC BSC (1980s) 5-FU/FA (1990s) FOLFOX, FOLFIRI CT combination + MAbs CT combination + Tailored MAb therapy 0 6 12 18 24 30 Time (months)
  • 31. CRC: Adenoma-Carcinoma Sequence Normal Hyperproliferative Adenoma Carcinoma Colon Epithelium APC Methylation APC KRAS 18q p53 Further hMSH2 abnormalities hMSH2 mutation deletion deletion accumulation hMLH1 hMLH1 of genetic abnormalities inactivation abnormalities (hereditary) 32% to 57% KRAS mutant
  • 32. Toward Personalized Therapy of CRC Ligand: AREG/EREG Target for EGFR-ERBITUX Target for EGFT-TK inhibitor EGFR-TK pY GRB2 pY SOS P13K pY RAS RAF STAT MEK AKT PTEN MAPK Gene transcription P Cell-cycle progression P MYC Cyclin D1 JUN FOS MYC Cyclin D1 Proliferation/ maturation Chemotherapy/ Survival Invasion and radiotherapy resistance Angiogenesis (anti-apoptosis) metastasis
  • 33. Toward Personalized Therapy of CRC  EGFR antibodies  KRAS and BRAF mutations correlate with lack of response to treatment with monoclonal antibodies targeting EGFR  VEGF antibodies  Patients who do not have a contraindication may benefit from bevacizumab, although no predictive marker has been identified  Combining EGFR and VEGF antibodies  Data do not demonstrate benefit
  • 34. NCCN: KRAS Mutation Testing Recommended to guide treatment plan  KRAS codons 12 and 13  Testing considerations  Qualified laboratories  Formalin-fixed paraffin-embedded tissue  Primary tumor and/or the metastasis
  • 35. NCCN: BRAF Mutation Testing Not yet recommended, but noted in the guidelines  Testing considerations  Formalin-fixed paraffin-embedded tissues  Typically PCR and direct DNA sequence analysis  Qualified laboratories
  • 36. Chemotherapy side effects Drug Side effects 5-FU and Leucovorin Diarrhea, mucositis, temporary low blood counts Xeloda Hand- foot syndrome diarrhea and mucositis Irinotecan Diarrhea, low blood counts, fatigue, hair loss
  • 37. Chemotherapy side effects Drug Side effects Oxaliplatin Sensory neuropathy, acute paresthesias and dysesthesias of the hands, feet and perioral region, jaw tightness, and pseudolaryngospasm Avastin Increase BP, impair wound healing, bleeding, bowel perforation(1.4~2%) and fistula formation, proteinuria, thromboembolic events(4.5%): stroke, heart attack Erbitux Allergic reactions, skin rash, headache, nausea, low blood magnesium
  • 38. Duration of therapy  Traditional practice – continue till  Unacceptable toxicity  Clinical deterioration or  Disease progression  Newer approach – discontinuation of treatment after fixed time period
  • 39. Treatment-Free Intervals  Rationale  Decrease intensity of therapy  Reduce toxicity  Prevent discontinuation of therapy  Increase QOL  Types of treatment breaks  Treatment break with maintenance regimen  Complete Chemotherapy-free intervals (CFI)
  • 40. Metastatic CRC: Progress in OS BSC 4–6 months 5-FU/AF 11–14.7 months IFL or FOLFIRI 15–17.4 months 5-FU/AF + bevacizumab 18.3 months FOLFOX4 or CapeOx 16.2–20 months IFL + bevacizumab 20.3 months FOLFOX6  FOLFIRI 20.6 months Bevacizumab+ FOLFOX/CAPOX 21.3 months FOLFIRI  FOLFOX6 21.5 months Cetuximab + Std CT*0 23.5 months * KRAS wild type patients 6 OS (months) 18 12 24
  • 41. Assessment during therapy  CT scan, PET ( every 2~3 cycles)  CEA ( every 1~3months)  Persistently rising CEA levels should prompt restaging, but suggest disease progression and the need for an alternative treatment strategy.  Caution should be used when interpreting a rising CEA level during the first 4 to 6 weeks of a new therapy, since spurious early elevation in serum CEA may occur, especially after Oxaliplatin.
  • 42. Management of metastatic colorectal cancer General Principles  Patients with mCRC, particularly those with liver or lung only metastases, should be carefully evaluated upfront to determine the feasibility of curative resection  The current approach to the treatment of mCRC is to use various agents (5- fluorouracil/leucovorin [5-FU/LV], capecitabine, irinotecan, oxaliplatin, bevacizumab, cetuximab, and patitumumab) in combination or as single agents  FOLFIRI (infusional 5-FU, leucovorin, plus irinotecan) and FOLFOX (infusional 5-FU, leucovorin, plus oxaliplatin) exhibit similar efficacy in mCRC.  5-FU/LV in patients who cannot tolerate intensive therapy , either may be combined with bevacizumab
  • 44. Carcinoid tumors  Neuroendocrine tumors  More common in appendix and rectum  Half are functional – MC produce seratonin  Appendicial carcinoids  < 1 cm – no risk of metastasis and managed with appendectomy  Tumors 1 – 2 cm – controversial  > 2 cm – managed with formal right hemicolectomy  Rectal carcinoids – typically not functional  < 1 cm never metastasize – managed with local excision or fulguration  1 – 2 cm controversial  > 2cm – more radical surgery
  • 45. High grade neuroendocrine carcinoma Extrapulmonary small cell carcinoma  Chest imaging always performed to rule out mets from lung  Nonspecific presentation and clinical features similar to adenocarcinoma  Distant spread common  Recommendations extrapolated from small cell lung cancer  Combined modality treatment with chemo and surgery
  • 46. Lymphoma  Majority non Hodgkins type  Maybe low, intermediate or high grade histology  B cell diffuse large cell histology most common  Majority affect cecum or rectum  Usually present with non specific abdominal pain, rectal bleeding, obstruction or a mass  Diagnosis made n histology  Work up – bone marrow biopsy, full body scanning  Treatment – combined modality with chemotherapy and surgery  Role of radiation therapy unclear
  • 47. Conclusion  Patients with mCRC, particularly those with liver or lung only metastases, should be carefully evaluated upfront to determine the feasibility of curative resection  The availability of multiple therapies and the judicious use of surgery have improved outcomes for metastatic CRC  Use of these agents may soon be individualized as data about predictive factors evolves