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Regional Therapy for Tumors

              By:
        Emil Cohen, MD
       Center Radiology
     cohenemil@gmail.com
Objectives
• Familiarize the audience with various
  options available for loco-regional
  treatment of tumors
• Gain input about needs and gaps in
  treatment of the oncology patients
Objectives
• Familiarize the audience with various
  options available for loco-regional
  treatment of tumors
     •Embolization
       •Bland
       •Chemo
       •Radio
     •Ablation
       •Radiofrequency
       •Cryo
Options for Liver Disease
What Cancers to Consider
•   Colorectal
•   Hepatocellular carcinoma
•   Intrahepatic cholangiocarcinoma
•   Neuroendocrine metastases
When to Consider
• Colorectal
  – After failure of first line
  – Chemo-Holiday
• Hepatocellular Carcinoma
  – List for transplant or resection
  – Give regional therapy
  – Ablation if possible/necessary
• Intrahepatic Cholangiocarcinoma – First Line
• Neuroendocrine tumors – failure of sandostatin;
  preferably before 50% of liver replaced
Background
• Liver metastases from colon and neuroendocrine tumors
  is common; overall liver is the most common site for
  metastatic disease
• In colon cancer, liver only metastatic disease is seen in
  approximately 30% of the patients
          Sasson AR, Sigurdson ER Surgical treatment of liver metastases. Semin
            Oncol. 2002 Apr;29(2):107-18
• Primary liver cancer (HCC or Cholangiocarcinoma) is
  one of the most common tumors worldwide(5th
  worldwide)
          Parkin DM, Bray F, Ferlay J, Pisani P. Estimating the world cancer
            burden:GLOBOCAN 2000. Int J Cancer 2001;94:153-156
   – This is predominantly due to endemic Hep B in southeast asia
   – Growing numbers of Hep C in the Europe and remainder of the
     world
Cholangiocarcinoma
• Increase in the rate of intrahepatic
  cholangiocarcinoma (more than doubled)
Shaib YH, Davila JA, McGlynn K, El-Serag HB. Rising incidence of intrahepatic
   cholangiocarcinoma in the United States: a true increase?
   J Hepatol. 2004 Mar;40(3):472-7.

• Decrease in the rate of extrahepatic
  cholangiocarcinoma
    – More cholecystectomies
Background
• Trans-arterial chemo-embolization (TACE)
  is primarily a palliative therapy
• Proven therapy in primary and liver
  dominant metastatic disease
Background
• Survival rates for untreated liver metastases is
  poor being approximately about a year
• Systemic chemotherapy is an option for most
  tumors except for HCC.
• Review of literature demonstrated a significant
  benefit of chemoembolization with doxirubicin or
  cisplatin
        Llovet et al Systematic review of randomized trials for
          unresectable hepatocellular carcinoma: Chemoembolization
          improves survival. Hepatology. 2003 Feb;37(2):429-42
Relative Contraindications
• Total bilirubin > 4
• Albumin < 2
• Creatinine > 1.7
• Encephalopathy
• Biliary colonization with gut flora (risk of abscess
  formation as high as 40%)
• PV thrombosis**, Hopkins study demonstrated
  no additional risk, other similar studies have
  followed
         Georgiades CS et al. Safety and efficacy of transarterial
          chemoembolization in patients with unresectable hepatocellular
          carcinoma and portal vein thrombosis. J Vasc Interv Radiol.
          2005 Dec;16(12):1653-9.
Complications
•   Hemorrhage
•   Liver Failure
•   Liver Abscess
•   Renal Failure
•   Allergic Reaction to contrast
•   Non-target embolization
Pre-procedure imaging
      evaluation
Pre-procedure planning


Baseline CT and/or MRI to be within 30
           days of treatment
What to look for
• Hyperenhancing lesion + washout is
  diagnostic for HCC and no biopsy is
  necessary
• Size and location of mets – most of the
  disease must be within the liver
HCC reading a good path book
HCC reading a good path book
Imaging and Treatment Options
• Resection
• Radiofrequency Ablation
  – location, location, location, size
• Chemo-Embolization
• Transplant
  – one lesion under 5 cm
  – 3 lesions each no more than 3 cm
• Vascular invasion
Pre procedure labs
• Metabolic panel
• Liver Function test
• Coagulation profile
Why it works?
• Dual Blood Supply of the normal liver
  parenchyma:
  – 70-80% from portal circulation
  – 10-20%Hepatic Artery
• Tumor blood supply:
  – Tumors >3 mm derive >90% of blood supply from
    artery
  – Micro analysis of tumor vessels reveals tumor arterial
    vascularity to be at least 5x normal liver parenchyma
Anatomical consideration
• On Pre-procedure imaging assess hepatic
  arterial supply (20% variant anatomy)
• Risk of non-target embolization; no
  deaths (as of 2003) recorded from non-
  target chemo-embolization
• Radio-embolization non-target
  embolization is potentially fatal (less than
  2%)
Procedure
• Administer chemotherapy (50-75 mg
  Doxorubicin, 10 mg Cisplatin, 50 mg
  Mitomycin)
• Lipiodol 1-5 ml vs 10-30 ml; concentrates
  chemotherapy but washes out over the
  course of a few weeks
• +/- lidocaine
• Achieve a pruned tree appearance not a
  complete stasis
Day of Treatment

Day of Treatment
Pre vs. Post Treatment
Neuroendocrine Metastases
Neuroendocrine Mets
• Treat only after failure of sandostatin
• Category 2B recommendation from NCCN
Hepatocellular Carcinoma
        (HCC)
Do not recommend following
   NCCN guidelines for
 screening or biopsy, use
       UNOS instead
Problems with NCCN guidelines
          for HCC
• Recommend US screening (sensitivity is
  60-80% at best)
• Over-biopsy with risk of underdiagnosis
  since false negatives are common with
  biopsies
• Requires two tests, may delay care
UNOS imaging criteria
HCC
•   Screen with CT or MRI once cirrhotic
•   US sensitivity 60-80%
•   Milan Criteria
•   Childs A/B Treat
•   Childs C – Meaningful treatment or
    palliation
Treatment for HCC
• Transplantation
• Resection
• Radiofrequency Ablation
• Chemoembolization (conventional or drug
  eluting beads)
• Radioembolization
    – Portal or hepatic vein invasion
• External beam radiation (SBRT) combined
  with TACE
Treatment for HCC
• RFA 80-95% cure rates for tumors up to 3
  cm
• 60-77% response rate for TACE (CR, PR,
  SD). CR less than 2% of patients.
• SBRT 60% infield response rate in non-
  operable patients
DEB for Unresectable HCC
 • 173 HCC patients not suitable for curable treatments
   were prospectively enrolled (mean age 70.4 ± 7.4 years)
 • Diameter was 7.6 ± 2.1 cm.
 • Included single and multifocal disease
 • Overall survival at 1, 2, 3, 4, and 5 years was 93.6, 83.8,
   62, 41.04, and 22.5 %,
 • Higher rates achieved in Child class A compared with
   Child class B patients (95, 88.2, 61.7, 45, and 29.4 % vs.
   91.5, 75, 50.7, 35.2, and 12.8 %).
 • Mean overall survival was 43.8 months (range 1.2–64.8)
Malagari, K. et al. Chemoembolization With Doxorubicin-Eluting Beads for Unresectable
Hepatocellular Carcinoma: Five-Year Survival Analysis. CardioVascular and
Interventional Radiology 35, 1119–1128 (2012).
Cholangiocarcinoma
Treatment
• Surgery is the only curative option
     – 10-15% Present early enough
     – 46% Recurrence rate
     – 3 month survival after non-curative resection
• No evidence for systemic adjuvant therapy
• Hepatic arterial port (case series)
     – Cisplatin
Yang, J. & Yan, L.-N. Current status of intrahepatic cholangiocarcinoma. World J
Gastroenterol 14, 6289–6297 (2008).
Treatment Options for Non-
         Resectable Tumors
•   Systemic Chemotherapy
•   Intra-arterial chemo
•   Radiation Therapy
•   Regional Therapy
    – TACE
    – Radioembolization
• Combination of Above
Systemic
 • Median survival: 11.7 months in cisplatin–
   gemcitabine group
 • Randomized study of 410 patients to
   gemcitabine vs cisplatin-gemcitabine
 • 81% SD+PR



Valle, J. et al. Cisplatin plus Gemcitabine versus Gemcitabine for Biliary Tract Cancer. New
England Journal of Medicine 362, 1273–1281 (2010).
TACE
  •   Median Survival 20 months
  •   62 Patients treated
  •   76% SD+PR
  •   No 30 day mortality




Kiefer, M. V. et al. Chemoembolization of intrahepatic cholangiocarcinoma with
cisplatinum, doxorubicin, mitomycin C, ethiodol, and polyvinyl alcohol: a 2-center study.
Cancer (2010).doi:10.1002/cncr.25625
TACE
   • Hopkins study with smaller patient set (24)
   • Traditional TACE
   • Median Survival 23 Months




Burger, I. et al. Transcatheter arterial chemoembolization in unresectable
cholangiocarcinoma: initial experience in a single institution. J Vasc Interv Radiol 16, 353–361
(2005).
Radioembolization
     • 25 patients
     • 9.3 months median survival




Saxena, A., Bester, L., Chua, T. C., Chu, F. C. & Morris, D. L. Yttrium-90 radiotherapy for
unresectable intrahepatic cholangiocarcinoma: a preliminary assessment of this novel
treatment option. Ann. Surg. Oncol. 17, 484–491 (2010).
Radioembolization
    • 24 patients
    • 48 treatments
    • 14.9 months median survival




Ibrahim, S. M. et al. Treatment of unresectable cholangiocarcinoma using yttrium-90
microspheres: results from a pilot study. Cancer 113, 2119–2128 (2008).
DEB TACE
    • 24 patients half of whom had failed
      resection and/or RFA
    • 17.5 month median survival




Schiffman, S. C. et al. Precision Hepatic Arterial Irinotecan Therapy in the Treatment of
Unresectable Intrahepatic Cholangiocellular Carcinoma: Optimal Tolerance and Prolonged
Overall Survival. Annals of Surgical Oncology 18, 431–438 (2010).
Note on Perihilar
                       Cholangiocarcinoma
    • Analysis of patients who underwent
      transplant after external radiation (99%),
      brachytherapy (75%), radio-sensitizing
      therapy (98%), and/or maintenance
      chemotherapy (65%)
    • 65% rate of recurrence-free survival after
      5 years

Murad, S. D. et al. Efficacy of Neoadjuvant Chemoradiation, followed by Liver Transplantation,
for Perihilar Cholangiocarcinoma at 12 US Centers. Gastroenterology
(2012).doi:10.1053/j.gastro.2012.04.008
Colorectal Metastases
Treatment options
•   Resection
•   Resection
•   Resection
•   RFA
•   Systemic Chemo FOLFOX
•   What then?
    – FOLFIRI
    – Cetuximab
Let’s compare
  • EPIC trial
  • Second line therapy: cetuximab (400 mg/m(2) day 1
    followed by 250 mg/m(2) weekly) plus irinotecan (350
    mg/m(2) every 3 weeks)
  • Median survival 10-10.7 months
  • Progression free survival (PFS): 4.0 months
  • PFS: 4.0 (cetuximab + irinotecan) vs. 5.5 months
    (radioembolization)
  • Median survival: 10.7 vs. 11 months with conventional
    TACE (salvage , usually sicker, patients)

Sobrero, A. F. et al. EPIC: Phase III Trial of Cetuximab Plus Irinotecan After Fluoropyrimidine and
Oxaliplatin Failure in Patients With Metastatic Colorectal Cancer. JCO 26, 2311–2319 (2008).
Irinotecan DEB (DEBIRI)
 • April 2012 Phase III research
 • 74 patients randomly assigned to FOLFIRI
   or DEBIRI
 • Endpoints : Survival (Primary)
 • Median survival 22 vs 15 months
 • Progression free survival 7 vs 4 months
 • Quality improvement of life 8 vs 3 months
Fiorentini, G. et al. Intra-Arterial Infusion of Irinotecan-Loaded Drug-Eluting Beads (DEBIRI) Versus
Intravenous Therapy (FOLFIRI) for Hepatic Metastases from Colorectal Cancer: Final Results of a Phase III
Study. Anticancer Res 32, 1387–1395 (2012).
Salvage Patients for
                       Radioembolization
 • Compared with BSC alone,
   radioembolization prolonged survival
   (median, 8.3 vs. 3.5 months; P < 0.001)
   with a hazard ratio of 0.3 (95% confidence
   interval, 0.16-0.55; P < 0.001) in a
   multivariate Cox proportional hazard
   model.


Seidensticker, R. et al. Matched-Pair Comparison of Radioembolization Plus Best Supportive
Care Versus Best Supportive Care Alone for Chemotherapy Refractory Liver-Dominant Colorectal
Metastases. CardioVascular and Interventional Radiology 35, 1066–1073 (2011).
Conventional Chemoembolization
  •   Many case series, no randomized studies
  •   121 patients (lipiodol, CAM)
  •   Median survival was 33 months from diagnosis of the primary colon
      cancer, 27 months from development of liver metastases, and 9
      months from chemoembolization.
  •   Survival was significantly better when chemoembolization was
      performed after first- or second-line systemic therapy (11-12
      months) than after third- to fifth-line therapies (6 months) (P = .03).
  •   Presence of extrahepatic metastases did not adversely affect
      survival (P = .48).
  •   Chemoembolization provided local disease control of hepatic
      metastases after 43% of treatment cycles. Median survival was 27
      months overall, and 11 months when initiated for salvage after
      failure of second-line systemic therapy.


Albert, M. et al. Chemoembolization of colorectal liver metastases with cisplatin, doxorubicin,
mitomycin C, ethiodol, and polyvinyl alcohol. Cancer (2010).
Renal Cell Carcinoma
Renal Ablation
 • Cryo is preffered
 • Embolize tumors more than 3 cm in
   diameter
 • Recent meta analysis of cryo-ablation and
   RFA of 457 patients 89-90% efficacy for
   tumors less than 4 cm in size
 • No significant difference between
   complication rates (salt, grain of)
El Dib, R., Touma, N. J. & Kapoor, A. Cryoablation vs radiofrequency ablation for the treatment of renal
cell carcinoma: a meta-analysis of case series studies. BJU Int. 110, 510–516 (2012).
Bony Metastases
Metastatic Disease to Bones
  • Several small case series until 2011
  • 309 embolization in 243 patients
  • 50% reduction in pain score for an average of 8
    months
  • Adverse events (87 patients):
        –   Postembolization syndrome
        –   ischemic pain at the site of embolization
        –   paresthesias
        –   skin breakdown
        –   subcutaneous necrosis
Rossi, G. et al. Selective Embolization with N-butyl Cyanoacrylate for Metastatic Bone Disease. Journal of
Vascular and Interventional Radiology 22, 462–470 (2011).
Summary
• Please consider regional therapy for:
  – Intrahepatic cholangiocarcinoma
  – HCC
  – Painful bone metastases (radiation first)
• Think about it for
  – Second line or at least salvage for
     • Colorectal cancer
  – Renal cell carcinoma

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Regional therapy for tumors 2

  • 1. Regional Therapy for Tumors By: Emil Cohen, MD Center Radiology cohenemil@gmail.com
  • 2. Objectives • Familiarize the audience with various options available for loco-regional treatment of tumors • Gain input about needs and gaps in treatment of the oncology patients
  • 3. Objectives • Familiarize the audience with various options available for loco-regional treatment of tumors •Embolization •Bland •Chemo •Radio •Ablation •Radiofrequency •Cryo
  • 5. What Cancers to Consider • Colorectal • Hepatocellular carcinoma • Intrahepatic cholangiocarcinoma • Neuroendocrine metastases
  • 6. When to Consider • Colorectal – After failure of first line – Chemo-Holiday • Hepatocellular Carcinoma – List for transplant or resection – Give regional therapy – Ablation if possible/necessary • Intrahepatic Cholangiocarcinoma – First Line • Neuroendocrine tumors – failure of sandostatin; preferably before 50% of liver replaced
  • 7. Background • Liver metastases from colon and neuroendocrine tumors is common; overall liver is the most common site for metastatic disease • In colon cancer, liver only metastatic disease is seen in approximately 30% of the patients Sasson AR, Sigurdson ER Surgical treatment of liver metastases. Semin Oncol. 2002 Apr;29(2):107-18 • Primary liver cancer (HCC or Cholangiocarcinoma) is one of the most common tumors worldwide(5th worldwide) Parkin DM, Bray F, Ferlay J, Pisani P. Estimating the world cancer burden:GLOBOCAN 2000. Int J Cancer 2001;94:153-156 – This is predominantly due to endemic Hep B in southeast asia – Growing numbers of Hep C in the Europe and remainder of the world
  • 8. Cholangiocarcinoma • Increase in the rate of intrahepatic cholangiocarcinoma (more than doubled) Shaib YH, Davila JA, McGlynn K, El-Serag HB. Rising incidence of intrahepatic cholangiocarcinoma in the United States: a true increase? J Hepatol. 2004 Mar;40(3):472-7. • Decrease in the rate of extrahepatic cholangiocarcinoma – More cholecystectomies
  • 9. Background • Trans-arterial chemo-embolization (TACE) is primarily a palliative therapy • Proven therapy in primary and liver dominant metastatic disease
  • 10. Background • Survival rates for untreated liver metastases is poor being approximately about a year • Systemic chemotherapy is an option for most tumors except for HCC. • Review of literature demonstrated a significant benefit of chemoembolization with doxirubicin or cisplatin Llovet et al Systematic review of randomized trials for unresectable hepatocellular carcinoma: Chemoembolization improves survival. Hepatology. 2003 Feb;37(2):429-42
  • 11. Relative Contraindications • Total bilirubin > 4 • Albumin < 2 • Creatinine > 1.7 • Encephalopathy • Biliary colonization with gut flora (risk of abscess formation as high as 40%) • PV thrombosis**, Hopkins study demonstrated no additional risk, other similar studies have followed Georgiades CS et al. Safety and efficacy of transarterial chemoembolization in patients with unresectable hepatocellular carcinoma and portal vein thrombosis. J Vasc Interv Radiol. 2005 Dec;16(12):1653-9.
  • 12. Complications • Hemorrhage • Liver Failure • Liver Abscess • Renal Failure • Allergic Reaction to contrast • Non-target embolization
  • 13. Pre-procedure imaging evaluation
  • 14. Pre-procedure planning Baseline CT and/or MRI to be within 30 days of treatment
  • 15. What to look for • Hyperenhancing lesion + washout is diagnostic for HCC and no biopsy is necessary • Size and location of mets – most of the disease must be within the liver
  • 16. HCC reading a good path book
  • 17. HCC reading a good path book
  • 18. Imaging and Treatment Options • Resection • Radiofrequency Ablation – location, location, location, size • Chemo-Embolization • Transplant – one lesion under 5 cm – 3 lesions each no more than 3 cm • Vascular invasion
  • 19. Pre procedure labs • Metabolic panel • Liver Function test • Coagulation profile
  • 20. Why it works? • Dual Blood Supply of the normal liver parenchyma: – 70-80% from portal circulation – 10-20%Hepatic Artery • Tumor blood supply: – Tumors >3 mm derive >90% of blood supply from artery – Micro analysis of tumor vessels reveals tumor arterial vascularity to be at least 5x normal liver parenchyma
  • 21. Anatomical consideration • On Pre-procedure imaging assess hepatic arterial supply (20% variant anatomy) • Risk of non-target embolization; no deaths (as of 2003) recorded from non- target chemo-embolization • Radio-embolization non-target embolization is potentially fatal (less than 2%)
  • 22. Procedure • Administer chemotherapy (50-75 mg Doxorubicin, 10 mg Cisplatin, 50 mg Mitomycin) • Lipiodol 1-5 ml vs 10-30 ml; concentrates chemotherapy but washes out over the course of a few weeks • +/- lidocaine • Achieve a pruned tree appearance not a complete stasis
  • 23.
  • 24. Day of Treatment Day of Treatment
  • 25. Pre vs. Post Treatment
  • 27. Neuroendocrine Mets • Treat only after failure of sandostatin • Category 2B recommendation from NCCN
  • 29. Do not recommend following NCCN guidelines for screening or biopsy, use UNOS instead
  • 30. Problems with NCCN guidelines for HCC • Recommend US screening (sensitivity is 60-80% at best) • Over-biopsy with risk of underdiagnosis since false negatives are common with biopsies • Requires two tests, may delay care
  • 32. HCC • Screen with CT or MRI once cirrhotic • US sensitivity 60-80% • Milan Criteria • Childs A/B Treat • Childs C – Meaningful treatment or palliation
  • 33. Treatment for HCC • Transplantation • Resection • Radiofrequency Ablation • Chemoembolization (conventional or drug eluting beads) • Radioembolization – Portal or hepatic vein invasion • External beam radiation (SBRT) combined with TACE
  • 34. Treatment for HCC • RFA 80-95% cure rates for tumors up to 3 cm • 60-77% response rate for TACE (CR, PR, SD). CR less than 2% of patients. • SBRT 60% infield response rate in non- operable patients
  • 35. DEB for Unresectable HCC • 173 HCC patients not suitable for curable treatments were prospectively enrolled (mean age 70.4 ± 7.4 years) • Diameter was 7.6 ± 2.1 cm. • Included single and multifocal disease • Overall survival at 1, 2, 3, 4, and 5 years was 93.6, 83.8, 62, 41.04, and 22.5 %, • Higher rates achieved in Child class A compared with Child class B patients (95, 88.2, 61.7, 45, and 29.4 % vs. 91.5, 75, 50.7, 35.2, and 12.8 %). • Mean overall survival was 43.8 months (range 1.2–64.8) Malagari, K. et al. Chemoembolization With Doxorubicin-Eluting Beads for Unresectable Hepatocellular Carcinoma: Five-Year Survival Analysis. CardioVascular and Interventional Radiology 35, 1119–1128 (2012).
  • 37. Treatment • Surgery is the only curative option – 10-15% Present early enough – 46% Recurrence rate – 3 month survival after non-curative resection • No evidence for systemic adjuvant therapy • Hepatic arterial port (case series) – Cisplatin Yang, J. & Yan, L.-N. Current status of intrahepatic cholangiocarcinoma. World J Gastroenterol 14, 6289–6297 (2008).
  • 38. Treatment Options for Non- Resectable Tumors • Systemic Chemotherapy • Intra-arterial chemo • Radiation Therapy • Regional Therapy – TACE – Radioembolization • Combination of Above
  • 39. Systemic • Median survival: 11.7 months in cisplatin– gemcitabine group • Randomized study of 410 patients to gemcitabine vs cisplatin-gemcitabine • 81% SD+PR Valle, J. et al. Cisplatin plus Gemcitabine versus Gemcitabine for Biliary Tract Cancer. New England Journal of Medicine 362, 1273–1281 (2010).
  • 40. TACE • Median Survival 20 months • 62 Patients treated • 76% SD+PR • No 30 day mortality Kiefer, M. V. et al. Chemoembolization of intrahepatic cholangiocarcinoma with cisplatinum, doxorubicin, mitomycin C, ethiodol, and polyvinyl alcohol: a 2-center study. Cancer (2010).doi:10.1002/cncr.25625
  • 41. TACE • Hopkins study with smaller patient set (24) • Traditional TACE • Median Survival 23 Months Burger, I. et al. Transcatheter arterial chemoembolization in unresectable cholangiocarcinoma: initial experience in a single institution. J Vasc Interv Radiol 16, 353–361 (2005).
  • 42. Radioembolization • 25 patients • 9.3 months median survival Saxena, A., Bester, L., Chua, T. C., Chu, F. C. & Morris, D. L. Yttrium-90 radiotherapy for unresectable intrahepatic cholangiocarcinoma: a preliminary assessment of this novel treatment option. Ann. Surg. Oncol. 17, 484–491 (2010).
  • 43. Radioembolization • 24 patients • 48 treatments • 14.9 months median survival Ibrahim, S. M. et al. Treatment of unresectable cholangiocarcinoma using yttrium-90 microspheres: results from a pilot study. Cancer 113, 2119–2128 (2008).
  • 44. DEB TACE • 24 patients half of whom had failed resection and/or RFA • 17.5 month median survival Schiffman, S. C. et al. Precision Hepatic Arterial Irinotecan Therapy in the Treatment of Unresectable Intrahepatic Cholangiocellular Carcinoma: Optimal Tolerance and Prolonged Overall Survival. Annals of Surgical Oncology 18, 431–438 (2010).
  • 45. Note on Perihilar Cholangiocarcinoma • Analysis of patients who underwent transplant after external radiation (99%), brachytherapy (75%), radio-sensitizing therapy (98%), and/or maintenance chemotherapy (65%) • 65% rate of recurrence-free survival after 5 years Murad, S. D. et al. Efficacy of Neoadjuvant Chemoradiation, followed by Liver Transplantation, for Perihilar Cholangiocarcinoma at 12 US Centers. Gastroenterology (2012).doi:10.1053/j.gastro.2012.04.008
  • 47. Treatment options • Resection • Resection • Resection • RFA • Systemic Chemo FOLFOX • What then? – FOLFIRI – Cetuximab
  • 48. Let’s compare • EPIC trial • Second line therapy: cetuximab (400 mg/m(2) day 1 followed by 250 mg/m(2) weekly) plus irinotecan (350 mg/m(2) every 3 weeks) • Median survival 10-10.7 months • Progression free survival (PFS): 4.0 months • PFS: 4.0 (cetuximab + irinotecan) vs. 5.5 months (radioembolization) • Median survival: 10.7 vs. 11 months with conventional TACE (salvage , usually sicker, patients) Sobrero, A. F. et al. EPIC: Phase III Trial of Cetuximab Plus Irinotecan After Fluoropyrimidine and Oxaliplatin Failure in Patients With Metastatic Colorectal Cancer. JCO 26, 2311–2319 (2008).
  • 49. Irinotecan DEB (DEBIRI) • April 2012 Phase III research • 74 patients randomly assigned to FOLFIRI or DEBIRI • Endpoints : Survival (Primary) • Median survival 22 vs 15 months • Progression free survival 7 vs 4 months • Quality improvement of life 8 vs 3 months Fiorentini, G. et al. Intra-Arterial Infusion of Irinotecan-Loaded Drug-Eluting Beads (DEBIRI) Versus Intravenous Therapy (FOLFIRI) for Hepatic Metastases from Colorectal Cancer: Final Results of a Phase III Study. Anticancer Res 32, 1387–1395 (2012).
  • 50. Salvage Patients for Radioembolization • Compared with BSC alone, radioembolization prolonged survival (median, 8.3 vs. 3.5 months; P < 0.001) with a hazard ratio of 0.3 (95% confidence interval, 0.16-0.55; P < 0.001) in a multivariate Cox proportional hazard model. Seidensticker, R. et al. Matched-Pair Comparison of Radioembolization Plus Best Supportive Care Versus Best Supportive Care Alone for Chemotherapy Refractory Liver-Dominant Colorectal Metastases. CardioVascular and Interventional Radiology 35, 1066–1073 (2011).
  • 51. Conventional Chemoembolization • Many case series, no randomized studies • 121 patients (lipiodol, CAM) • Median survival was 33 months from diagnosis of the primary colon cancer, 27 months from development of liver metastases, and 9 months from chemoembolization. • Survival was significantly better when chemoembolization was performed after first- or second-line systemic therapy (11-12 months) than after third- to fifth-line therapies (6 months) (P = .03). • Presence of extrahepatic metastases did not adversely affect survival (P = .48). • Chemoembolization provided local disease control of hepatic metastases after 43% of treatment cycles. Median survival was 27 months overall, and 11 months when initiated for salvage after failure of second-line systemic therapy. Albert, M. et al. Chemoembolization of colorectal liver metastases with cisplatin, doxorubicin, mitomycin C, ethiodol, and polyvinyl alcohol. Cancer (2010).
  • 53. Renal Ablation • Cryo is preffered • Embolize tumors more than 3 cm in diameter • Recent meta analysis of cryo-ablation and RFA of 457 patients 89-90% efficacy for tumors less than 4 cm in size • No significant difference between complication rates (salt, grain of) El Dib, R., Touma, N. J. & Kapoor, A. Cryoablation vs radiofrequency ablation for the treatment of renal cell carcinoma: a meta-analysis of case series studies. BJU Int. 110, 510–516 (2012).
  • 55. Metastatic Disease to Bones • Several small case series until 2011 • 309 embolization in 243 patients • 50% reduction in pain score for an average of 8 months • Adverse events (87 patients): – Postembolization syndrome – ischemic pain at the site of embolization – paresthesias – skin breakdown – subcutaneous necrosis Rossi, G. et al. Selective Embolization with N-butyl Cyanoacrylate for Metastatic Bone Disease. Journal of Vascular and Interventional Radiology 22, 462–470 (2011).
  • 56. Summary • Please consider regional therapy for: – Intrahepatic cholangiocarcinoma – HCC – Painful bone metastases (radiation first) • Think about it for – Second line or at least salvage for • Colorectal cancer – Renal cell carcinoma

Notas del editor

  1. Central Cholangio has actually decreased
  2. Patients in french study had a very high rate of liver failure and too many TACE’s which were too strong; no subselective catherization; the devil is in the detail
  3. May treat with subselective; treat with hydration +/- mucormyst; gut prep and anti
  4. Liver Abscess is difficult to get rid of even with perc drainage (thick) and antibiotics
  5. Two reasons for not achieving complete stasis is need for re-access and potential selection of anoxiphilic aggressive tumors