Dalle linee guida dell'epatocarcinoma alla pratica clinica - Gastrolearning®
1. Corso
“Gastrolearning”
Bologna, 20 Maggio 2013
Linee guida AISF
Franco Trevisani
Semeiotica Medica
Dipartimento di Scienze Mediche e Chirurgiche
Alma Mater Studiorum - Università di Bologna
5. Surveillance for HCC: the RCT
Zhang BH, et al. J Cancer Res Clin Oncol. 2004;130:417-22
18,816 patients with HBsAg+ chronic hepatitis
9,373
AFP + US (semi-annual)
9,443
No surveillance
86 67HCC
83/100,000 131/100,000HCC mortality
HCC mortality rate ratio:
0.63 (95% CI 0.41–0.98)
- Compliance 58%
- LT not available
AFP = alpha-fetoprotein;
RCT = randomized controlled trial; US = ultrasonography.
6. 205 cirrhotic patients (Child–Pugh A/B)
Decision aid
paper
Surveillance for HCC in cirrhosis: unfeasibility of
RCT when informed consent is given
Poustchi H, et al. Hepatology ,2010; 54: 1998–2004 [Epub ahead of print 2011 July 28]
181
chose
surveillance
21
continued their
usual care
2
were
undecided
6 mo. US + 3 mo. AFP
vs
no surveillance
204 pts. (99.5%)
declined randomization
This topic can be only
addressed with carefully
conducted cohort studies
7. Surveillance for HCC in cirrhosis:
survival in cohort studies
De Masi S, et al. Dig Liver Dis. 2005;37:260-8.
Cirrhosis 3-year survival rate
Kemp, 2005
Australia
HCV, HBV,
alcohol
Retrospective US 6–12 m 41 55 38% 19% 329 days
(median)
Toyoda, 2006
Japan
HCV, HBV Retrospective US + AFP +
DCP
1,050 591 36% 19%
Stravitz, 2008
USA
HCV, acohol Retrospective US (others)
12 m
172 107 40% 13% 916 days
(median)
Kuo, 2010
Taiwan
HBV, HCV Retrospective US ≤12 m 318 1118 59% 29%
Kemp W, et al., J Gastroenterol Hepatol. 2005;20:873-8. Toyoda H, et al., Clin Gastroenterol Hepatol. 2006;4:1170–6. Stravitz RT, et al., Am
J Med. 2008 Feb;121:119-26. Kuo Y-H, et al., Eur J Cancer 2010; 46:744-51
8. Surveillance for HCC in cirrhosis:
survival in cohort studies
De Masi S, et al. Dig Liver Dis. 2005;37:260-8.
Lead time
11. Subject to PATH Program Disclaimer
Effect of surveillance on survival
(adjusted for the “lead time”) in cirrhosis
Child–Pugh CChild–Pugh B
Trevisani F et al., for ITA.LI.CA. Am J Gastroenterol 2002;97:734-44
Trevisani F et al., for ITA.LI.CA. Am J Gastroenterol 2007;102:2448-57
Surveillance
No surveillance
Lead time
Child–Pugh A
13. Baseline HBV-DNA level and
risk of HCC in chronic hepatitis B
Chen et al., JAMA 2006
<10˙000 c/mL
1˙000˙000 c/mL
>1˙000˙000 c/mL
100˙000 c/mL
At entry:
- HBeAg neg.
- Normal ALT
- No cirrhosis
HBV-DNA (c/mL) Annual incidence of HCC (%)
<10,000 0.11
10,000-99,9999 0.29
100,0000-999,9999 0.96
≥1 Million 1.15
14. Yang HI, et al. Lancet Oncol. 2011;12:568-74.
Risk estimation for hepatocellular carcinoma in
chronic hepatitis B (REACH-B):
development and validation of a predictive score
12 months
6 months
19. Rischio HCC in pazienti divenuti non viremici
HBV
HCV
Aghemo et al., J Hepatol 2012;57:1326-35
20. Surveillance for HCC: how?
The popularity of US relies on the absence of risk, non-invasiveness,
easy accessibility, and relatively moderate cost
Bruix J, Sherman M. Hepatology. 2011;53:1020-2
Raccomadazioni AISF 2012; www.webaisf.org
EASL-EORTTC guidelines. J Hepatol 2012; 56; 908–943
Surveillance with US should be performed by an experienced
operator (evidence 5, strengh D).
21. Pooled sensitivity of ultrasoundultrasound for
early stageearly stage HCCHCC
Surveillance for HCC: how?
Singal A, et al. Aliment Pharmacol Ther 2009;30:37-47
22. Pooled sensitivity of ultrasoundultrasound for
early stage HCCearly stage HCC
Pooled sensitivity of ultrasound + AFPultrasound + AFP for
early stage HCCearly stage HCC
Sensitivity: + 6%
Surveillance for HCC: is US plus AFP better?
Singal A, et al. Aliment Pharmacol Ther 2009;30:37-47
23. Sensitiv. False + PPV
• US 84% 2.9% 6.6%
• US + AFP 92% 7.5% 3.0%
• AFP 69% 5.0% 3.3%
Semi-annual surveillance of 9,373 patients
with HBsAg+ or with chronic hepatitis
+ 8%
Zhang B, Yang B. J Med Screen 1999;6:108-10
PPV = positive predictive
value.
Alpha-fetoprotein as surveillance test
24. Cost for each small
HCC detected
(USA $)
• US 1,980
• US + AFP 3,640 (+84%)
• AFP 3,030 (+53%)
Alpha-fetoprotein as surveillance test
Semi-annual surveillance of 9,373 patients
with HBsAg+ or with chronic hepatitis
Zhang B, Yang B. J Med Screen 1999;6:108-10
25. Sensitivity of US-based surveillance
for early HCCearly HCC by interval (6 vs 12 months)
Meta-regression
Singal A, et al. Aliment Pharmacol Ther 2009;30:37-47
26. Distribution of HCC staging according to the
surveillance interval (6 vs 12 months)
Retrospective study on 634 patients with
Child–Pugh class A/B cirrhosis
HCC (number and ∅)
6 months
(497 patients)
12 months
(137 patients)
Single ≤ 2 cm (very early) 120 (24%) 7 (5%)
Single 2.1–3 cm (early) 94 (19%) 22 (16%)
Single 3.1–5 cm (early) 61 (13%) 30 (22%)
2–3 x ≤ 3 cm (early) 73 (15%) 20 (15%)
Milan out 149 (30.0%) 58 (42%)
p < 0.001
S
T
A
G
E
M
I
G
R
A
T
I
O
N
Santi V et al., for ITA.LI.CA, J Hepatol 2010;53:291-7
27. Survival according to the
surveillance interval (6 vs 12 months)
Corrected (for the lead time) survival
Sensitivity analysis: semi-annual is superior to annual program in patients with
a tumor volume doubling time ≤ 147 days
Observed survival
Santi V et al., for ITA.LI.CA, J Hepatol 2010;53:291-7
Retrospective study on 634 patients with
Child–Pugh class A/B cirrhosis
29. * OneOne imaging technique only in centers of excellence with high-end radiological equipmentin centers of excellence with high-end radiological equipment.
** HCC radiological hallmark: arterial hypervascularity and venous/late phase washout
Mass/nodule on US
< 1 cm 1-2 cm > 2 cm
4-phase CT or Dynamic
Contrast enhanced MRI
4-phase CT/Dynamic
Contrast enhanced MRI
Repeat US at 4 mo
Growing/Changing
Character
Stable
1 or 2 positive techniques*:
HCC radiological Hallmarks**
1 positive technique:
HCC radiological Hallmarks**
Yes No
HCC Biopsy
Investigate
according to size
Inconclusive
Yes No
HCC Biopsy
EASL–EORTC Clinical Practice Guidelines: Management of hepatocellular carcinoma. J Hepatol 2012; 56; 908–943
Diagnostic recall policy
?
30. Algoritmo diagnostico raccomandazioni AISF
Nuovo nodulo in cirrosi
Aumento (Ø > 1 cm)
NO Sì
Ecografia/3 mesi
Ø < 1 cm
Aumento (Ø > 1 cm)
Ecografia/3 mesi
(per 12 mesi)
NO
Ecografia/6 mesi
Sì
HCC
Non diagnostica
Ø > 1 cm
Aspetto atipico
Altra metodica
contrastografica
Aspetto tipico
(wash-in e wash-out)
NO Sì
Aspetto tipico
Biopsia
TC, RM, CEUS
Altra diagnosi
AISF position paper, Digest Liver Dis, 2013
31. Efficacy vs effectiveness of surveillance
Efficacy (mortality reduction) H R 3-year
- ITA.LI.CA (Am J Gastroenterol, 2002) 41% -
- Kemp et al. (J Gastroent Hepatol,2005) 76% 100%
- Bolondi et al. (Gut, 2001) - 42%
- Toyoda et al. (Clin Gastroenterol Heptol, 2008) - 89%
- Kuo et al. (Eur J Cancer, 2010) - 103%
Determinants of Effectiveness
- Doctor recommendation 80%
- Patient acceptance 90%
- Patient adherence 80%
- Proper recall policy 80%
- Timely available diagnostic and therapeutic options 80%
Effectiveness:
40% x 0.8 x 0.9 x 0.8 x 0.8 x 0.8 = 15%
80% x 0.8 x 0.9 x 0.8 x 0.8 x 0.8 = 29%
33. Portal pressure/
bilirubin
HCC
PEI/RFA Sorafenib
Stage 0
PST 0, Child–Pugh A
Very early stage (0)
1 HCC < 2 cm
Carcinoma in situ
Early stage (A)
1 HCC or 3 nodules
< 3 cm, PST 0
End stage (D)
Liver transplantation TACEResection
Curative treatments (30%)
5-year survival (40–70%)
Target: 20%
OS: 20 mo (45-14)
Associated diseases
YesNo
3 nodules ≤ 3 cm
Increased
Normal
1 HCC
Stage D
PST > 2, Child–Pugh C
Intermediate stage (B)
Multinodular,
PST 0
Advanced stage (C)
Portal invasion,
N1, M1, PST 1–2
Stage A–C
PST 0–2, Child–Pugh A–B
EASL–EORTC Clinical Practice Guidelines: Management of hepatocellular carcinoma. Journal of Hepatology 2012 vol. 56 j 908–943
Target: 40%
OS: 11 mo (6-14)
Best supportive
care
Target: 10%
OS: <3 mo
Updated BCLC staging system and
treatment strategy
PST 0-1
34. PERFORMANCE STATUS
(Eastern Cooperative Oncology Group)
Grade ECOG
0 Fully active, able to carry on all pre-disease performance without
restriction
1 Restricted in physically strenuous activity but ambulatory and able to
carry out work of a light or sedentary nature, e.g., light house work,
office work
2 Ambulatory and capable of all selfcare but unable to carry out any
work activities. Up and about more than 50% of waking hours
3 Capable of only limited selfcare, confined to bed or chair more than
50% of waking hours
4 Completely disabled. Cannot carry on any selfcare. Totally confined
to bed or chair
5 Dead
Oken, et al., Am J Clin Oncol 5:649-655, 1982
36. Portal pressure/
bilirubin
HCC
PEI/RFA Sorafenib
Stage 0
PST 0, Child–Pugh A
Very early stage (0)
1 HCC < 2 cm
Carcinoma in situ
Early stage (A)
1 HCC or 3 nodules
< 3 cm, PST 0
End stage (D)
Liver transplantation TACEResectionResection
Curative treatments (30%)
5-year survival (40–70%)
Target: 20%
OS: 20 mo (45-14)
Associated diseases
YesNo
3 nodules ≤ 3 cm
Increased
Normal
1 HCC
Stage D
PST > 2, Child–Pugh C
Intermediate stage (B)
Multinodular,
PST 0
Advanced stage (C)
Portal invasion,
N1, M1, PST 1–2
Stage A–C
PST 0–2, Child–Pugh A–B
EASL–EORTC Clinical Practice Guidelines: Management of hepatocellular carcinoma. Journal of Hepatology 2012 vol. 56 j 908–943
Target: 40%
OS: 11 mo (6-14)
Best supportive
care
Target: 10%
OS: <3 mo
Updated BCLC staging system and
treatment strategy
PST 0-1
37. Resection for HCC
Only single? Only without PHT
Ishizawa et al., Gastro 2008
CPA = Child Pugh Class A
CPB = Child Pugh Class B
PHT = Portal Hypertension
40. MELD score
9 - 10
Serum sodium level
Cirrhotic patient eligible for
liver resection
≥ 140 mEq/L < 140 mEq/L
Segmentectomy or
bisegmentectomy
Segmentectomy
or limited
resection
Major
hepatectomy (up
to 4 segments)
Risk of
IPLF>15% in
all types of
hepatectomy
>10<9
Algoritmo per candidare alla resezione
epatica il paziente con HCC
0 - 3.3% 0 – 2.5%0Mortalità
AISF position paper, Digest Liver Dis, 2013
41. Algoritmo per candidare alla resezione
epatica il paziente con HCC
Ascites, Bilirubin, Indocianine green retention rate at 15 min
Imamura H et al, J Hepatobiliary Pancreat Surg. 2005:16-22
A
B
I
43. RF results in Child-Pugh A patients
with a single HCC ≤2 cm
Livraghi et al., Hepatology 2008
Mortality 0
Major complications 1.8%
(1 seeding case)
Complete radiological necrosis
- 1st course 86%
- 2nd course 12%
- Total 98%
Sustained complete response 97%
(median follow-up 31 mo)
Treatment failure 3%
232 pts
218 pts
6 pts
(2.6%)
unfeasibility
44. Survival of patients with single HCC <2 cm
treated by ablation
Analysis by surgical candidacy (100 vs 118)
Livraghi et al., Hepatology 2008
45. Results of RF and resection in patients with
very early HCC (single <2 cm)
Propensity analysis (resection 52 vs RF 91→52)
Wang JH et al., J Hepatol 2011 [Epub haed of print]
One-to-one near-neighbor matching for:
sex, age, HBsAg, anti-HCV, platelet, Child-Pugh, AFP, ALT, BMI, hypertension, diabetes.
• Negligible mortality
• Lower liver mutilation
• Lower costs
• Shorter hospital stay
• Easy repeatibility
46. Cho YK et al., Hepatology 2010; 51: 1284-90
In compensated cirrhosis, first-line RF (followed by resection if failure)
is better than resection (followed by RF for recurrence)
if:
>
>
>
>
<
47. Cho YK et al., Hepatology 2010; 51:1284-90
Two-way sensitivity analysis:
HR mortality vs. local recurrence for overall mortality
HResection
RF (± HR)
2.5% increase in local recurrence = 1% increase in periop. Mortality
48. Tumor size and first-line treatment
≤ 2 cm
2.1- 3 cm
> 3 cm
RFA
Resection
AISF position paper, Digest Liver Dis, 2013
49. Portal pressure/
bilirubin
HCC
PEI/RFA Sorafenib
Stage 0
PST 0, Child–Pugh A
Very early stage (0)
1 HCC < 2 cm
Carcinoma in situ
Early stage (A)
1 HCC or 3 nodules
< 3 cm, PST 0
End stage (D)
Liver transplantation TACEResection
Curative treatments (30%)
5-year survival (40–70%)
Target: 20%
OS: 20 mo (45-14)
Associated diseases
YesNo
3 nodules ≤ 3 cm
Increased
Normal
1 HCC
Stage D
PST > 2, Child–Pugh C
Intermediate stage (B)
Multinodular,
PST 0
Advanced stage (C)
Portal invasion,
N1, M1, PST 1–2
Stage A–C
PST 0–2, Child–Pugh A–B
EASL–EORTC Clinical Practice Guidelines: Management of hepatocellular carcinoma. Journal of Hepatology 2012 vol. 56 j 908–943
Target: 40%
OS: 11 mo (6-14)
Best supportive
care
Target: 10%
OS: <3 mo
Updated BCLC staging system and
treatment strategy
PST 0-1
50. Mazzaferro et al., Lancet Oncol 2009
1556 pts. from 36 centres (1122 Milano-out at pathology examination)
5-year overall-survival
Linee guida: rapidi cambiamenti delle evidenze.
Chi trapiantare?
1 5 1510 8520 25 30 35 504540 55 60 65 7570 80
Size of the largest tumor (mm)
51. Linee guida: rapidi cambiamenti delle evidenze.
Criteri down-staging di Bologna
Down-staging:
- 5.1-6 cm
- 3.1-5 cm “Milano-in” dopo down-staging
- ≤4 cm ciascuno, somma Ø ≤12 cm
0
20
40
60
80
100
0 12 24 36
Actuarialsurvival(%)
Milano-in Down-staging
Post-Tx (88 vs. 32 pts)
0
20
40
60
80
100
0 12 24 36
Actuarialsurvival(%) Milano-in Down-staging
Intention-to-treat (129 vs. 48 pts)
Ravaioli et al., Am J Transplant 2008
52. Linee guida: rapidi cambiamenti delle evidenze.
Criteri down-staging UCSF
Down-staging:
- ≤ 8 cm
- ≤ 5 cm ciascuno, somma Ø ≤ 8 cm
- ≤ 3 cm ciascuno, somma Ø ≤12 cm
Yao et al., Hepatology 2008
Inizio down-staging
53. Multimodal treatment of HCC
OLT and neoadjuvant theraphy: the down-staging
Clavien et al., Lancet Oncol 2012; 13: 11-22
54. Multimodal treatment of HCC
OLT and neoadjuvant theraphy
AISF position paper, Digest Liver Dis, 2013
55. Portal pressure/
bilirubin
HCC
PEI/RFA Sorafenib
Stage 0
PST 0, Child–Pugh A
Very early stage (0)
1 HCC < 2 cm
Carcinoma in situ
Early stage (A)
1 HCC or 3 nodules
< 3 cm, PST 0
End stage (D)
Liver transplantation TACEResection
Curative treatments (30%)
5-year survival (40–70%)
Target: 20%
OS: 20 mo (45-14)
Associated diseases
YesNo
3 nodules ≤ 3 cm
Increased
Normal
1 HCC
Stage D
PST > 2, Child–Pugh C
Intermediate stage (B)
Multinodular,
PST 0
Advanced stage (C)
Portal invasion,
N1, M1, PST 1–2
Stage A–C
PST 0–2, Child–Pugh A–B
EASL–EORTC Clinical Practice Guidelines: Management of hepatocellular carcinoma. Journal of Hepatology 2012 vol. 56 j 908–943
Target: 40%
OS: 11 mo (6-14)
Best supportive
care
Target: 10%
OS: <3 mo
Updated BCLC staging system and
treatment strategy
PST 0-1
56. HCC in stadio intermedio
Paz. 58 aa, Child-Pugh A, MELD 9, PS 0, non invasione portale, N 0, M 0,
non comorbilità, varici F1.
6 cm
TACE (sempre?)
3.5
cm
57. Trattamento HCC in stadio BCLC intermedio
Lin et al., W J Surg 2010
Overall survivals adjusted for serum albumin (independent factor)
in Hepatic Resection (n. 93) and TACE (n. 73) pts.
Child-Pugh A
59. Trattamento HCC in stadio BCLC intermedio
Wang et al., Eur J Cancer 2008
Resection
TAE
60. Resection for HCC: an international study from referral centersResection for HCC: an international study from referral centers
(Asia, Europe, America)(Asia, Europe, America)
Trattamento HCC in stadio BCLC intermedio
Torzilli G et al., Ann Surg 2013 257; 929-37
61. Recommendation
Contraindications and
specifications
BCLC stage B pts not eligible for surgery or ablation (1a-A).
Best candidates are asymptomatic (PS 0) Child-Pugh class A pts (1b-A);
Child-Pugh score of B7 or PS 1 can be considered (5-D)
Jaundice, untreatable
ascites, portal or main
branch thrombosis,
hepatofugal portal flow, and
HCC >10 cm
TACE can be utilized in pts with early stage HCC if surgical or ablative
techniques are not applicable (technical reasons and/or comorbidities)
TACE should be performed with a selective or super-selective (segmental
or sub-segmental) technique to optimize risk/benefit ratio and increase
likelihood of complete response (2b-B)
For bi-lobar HCCs not
treatable with a super-
selective approach, treating
a single lobe per session
should be considered (5-D)
Peripheral, segmental or intra-tumoral thrombosis is not an absolute
contraindication to TACE, and should be used in association with a systemic
treatment (5-D)
Should be considered in
the frame of controlled
clinical studies
In absence of radiologic evidence of disease persistence (complete
response), TACE should not be repeated, due to its risks, costs and impact
on the pt’s quality of life. TACE should be repeated “on demand” (5-D)
2012 AISF recommendations for
TACE in HCC
AISF position paper, Digest Liver Dis, 2013
62. HCC in stadio intermedio
Paz. 58 aa, Child-Pugh A, MELD 9, PS 0, non invasione portale, N 0, M 0,
non comorbilità, varici F1.
TACE (sempre?)
64. Quale trattamento per HCC intermedio?
Sorafenib
Chemoembolizatio
n
PEI/RFA
Liver
transplantation
(CLT/LDLT)
Resectio
n
Curative treatments
HCC
Stage A–C
Okuda 1–2, PS 0–2, Child-Pugh A–B
Stage 0
PS 0, Child-Pugh A
Stage D
PS >2, Child-Pugh C
Very early stage
(0)
Single <2 cm
carcinoma in situ
Early stage
(A)
1–3 nodules <3 cm, PS
0
Intermediate stage
(B)
Multinodular,
PS 0
Advanced stage
(C)
Portal invasion,
N1, M1, PS 1–2
End stage
(D)
Single 3 nodules ≤3 cm
Portal pressure/bilirubin
Increased Associated diseases
Normal No Yes
Randomized controlled trials
Symptomatic
treatment
66. 1979 1992 2000 2001 2009 20102008
WHO
Handbook for
reporting results of
cancer treatment1
mWHO
Modified WHO
criteria2,3
RECIST
Response
Evaluation Criteria In
Solid Tumors4
EASL criteria
Conclusions from the
Barcelona 2000 EASL
conference5
RECIST 1.1
Revised RECIST
guidelines8
mRECIST for HCC
Proposed modifications to
RECIST 1.1 for assessing
response in HCC6,7
EASL, European Association for the Study of the Liver; HCC, hepatocellular carcinoma; RECIST, Response Evaluation Criteria In Solid Tumors;
WHO, World Health Organisation.
1. WHO 1979. Available at: http://whqlibdoc.who.int/offset/WHO_OFFSET_48.pdf; 2. Green S, et al. Invest New Drugs 1992;10:239-53; 3. P. Therasse
Ann Oncol (2002) 13(suppl 4): 127-129 ; 4. Therasse P, et al. J Natl Cancer Inst 2000;92:205-16; 5. Bruix J, et al. J Hepatol 2001;35:421-30; 6. Llovet JM, et al.
J Natl Cancer Inst 2008;100:698-791; 7. Lencioni R, et al. Semin Liver Dis 2010;30:52-60; 8. Eisenhauer EA, et al. Eur J Cancer 2009;45:228-47; 9. EASL-
EORTC Guidelines. J Hepatology 2012;56:908-43
Guidelines for evaluating response to treatment
in solid tumours have evolved
mRECIST
EASL-EORTC
HCC guideline9
2012
68. RECIST vs mRECIST criteria
Dr. Golfieri
(Bologna, Italy)
has proposed a
graphical
representation of
the change in
tumour dynamic
for RECIST vs
mRECIST
69. TACE: concordance between EASL
and mRECIST responses
Gillmore R, et al. J Hepatol 2011;55:1309–16;
Overall response (CR +PR), assessed at a median of 64 days
after TACE, was:
- almost identical using EASL and mRECIST
- much better than that calculated with RECIST
•EASL: 58%
•mRECIST: 57%
•RECIST 1.1: 7%
70. TACE: prognostic power of the response according to
the criteria utilized
EASL1
RECIST1
mRECIST1
Survival similar with EASL and mRECIST, and better in pts. with an overall response,
assessed at an early time point (median 64 days)1
:
Responder Non-responders P
•EASL: 22.0 months 12.7 months 0.019
•mRECIST: 20.7 months 13.3 months 0.009
•RECIST 1.1: 12.4 months 16.8 months n.s
1. Shim et al. Radiology 2012;262(2):708-18; 2. Llovet JM, Ducreux M, et al. J Hepatol. 2012;56:908-943
71. TACE: concordance between EASL and mRECIST
responses
Retrospective analysis: 332 patients in Korea treated with TACE1
– CP-A liver function and BCLC-B disease prior to treatment
•Excellent agreement between EASL and mRECIST
– κ value of 0.94 (95% CI: 0.91-0.97)
•Poor correlation between WHO and RECIST vs enhancement criteria
– κ value of <0.20 for both comparisons
EASLRECIST mRECIST
1. Shim et al. Radiology 2012;262(2):708-18; 2. Llovet JM, Ducreux M, et al. J Hepatol. 2012;56:908-943
WHO
OS according to:
EASL-EORTC and AISF guidelines recommend mRECIST
criteria for assessment of response in HCC2
73. RECIST vs. mRECIST with Sorafenib
Edeline J et al., Cancer 2011;118:147–56
Before After
rafenib
RECIST
mRECIST
74. Quando continuare e quando
fermarsi con la TACE?
Proposta di un algoritmo AISF
«razionale»
75. * percorso valido per ogni seduta di TACE; ** :i caso di cTACE è preferibile RM, in quanto alla TC l’accumulo di lipidol può “mascherare un’attività residua di malattia
*** risposta al trattamento definita secondo i criteri RECIST modificati [CR: risposta completa; PR: risposta parziale; SD: malattia stabile (si intende nessuna
modificazione favorevole della lesione trattata); DP: progressione di malattia.
HCC CANDIDATO A TACEHCC CANDIDATO A TACE
- No trombosi portale (ammessa trombosi di ramo segmentario)
- No malattia extraepatica
- Classe di Child Pugh A o B7
Deterioramento epatico,
complicazioni maggiori *
CR ***
RM o TC
trimestrale
Recidiva di malattia ***
PR ***
RisoluzioneNo
Palliazione
Sì
Progressione di malattia
(DP) o non risposta al
trattamento (SD) ***
Nuova
lesione
Crescita lesioni
trattate o SD***
Considera
SORAFENIB
Considera nuovo trattamento
(cTACE o DEB-TACE)
Trattamento cTACE o DEB-TACE
RM o TC **
(dopo 1 mese)
Trattamento cTACE o DEB-TACE
RM o TC **
(dopo 1 mese)
AISF position paper, Digest Liver Dis, 2013
77. Per-nodule response rate to the
1st
TACE: the role of tumour size
• Retrospective cohort study: 271 patients eligible to TACE with 635 treated nodules
• cTACE* performed ‘on demand’ upon demonstration of viable tumour (non-CR)
• Tumour assessment according to mRECIST (after 1 month and then every 3–4 months)
• Mean follow-up: 12 months (range 1-51)
CR, complete response; PR, partial response;; TACE, transarterial chemoembolization
*cTACE was 50 mg doxorubicin + Spongel; superselective technique where possible
Golfieri R et al., JVIR
2013
Tumor diameter ≤2 cm (N=386) 2.1-5 cm (N=211) >5 cm (N=36)
N. nodes % N. nodes % N. nodes %
Tumour response
CR 263 68 134 64 9 25
PR 123 32 77 36 27 75
Local Recurrence
Rate
52 20 36 27 6 57
Only 25% of large (>5 cm) nodules achieve CR and, in these nodules,
local relapse is very frequent.
79. Trattamenti locoregionali combinati
Wang W et al., Liver International 2010; 30: 741-749
Sopravvivenza a:
- 1 anno: 512 paz. → OR = 3.26 (95% CI = 1.23-8.69)
- 2 anni: 437 paz. → OR = 4.53 (95% CI = 2.62-7.82)
- 3 anni: 425 paz. → OR = 3.50 (95% CI = 1.75-7.02)
Confronto N. trials:
•TACE + PEI vs. TACE 4
•TACE + RF vs. RF 2
•TACE + PEI vs. PEI 1
•TACE + RF vs. TACE 1
•TACE + PEI vs. TACE o PEI 1
•TACE + RF vs. TACE o RF 1
Recurrence rate
80. Preliminary OS from start of sorafenib therapy in patients who did and did not
receive concomitant TACE
CI, confidence interval; OS, overall survival ASCO GI 2012
82. Sorafenib
Target: 40%
OS: 11 mo (6-14)
Portal pressure/
bilirubin
HCC
PEI/RFA
Stage 0
PST 0, Child–Pugh A
Very early stage (0)
1 HCC < 2 cm
Carcinoma in situ
Early stage (A)
1 HCC or 3 nodules
< 3 cm, PST 0
End stage (D)
Liver transplantation TACEResection
Curative treatments (30%)
5-year survival (40–70%)
Target: 20%
OS: 20 mo (45-14)
Associated diseases
YesNo
3 nodules ≤ 3 cm
Increased
Normal
1 HCC
Stage D
PST > 2, Child–Pugh C
Intermediate stage (B)
Multinodular,
PST 0
Advanced stage (C)
Portal invasion,
N1, M1, PST 1–2
Stage A–C
PST 0–2, Child–Pugh A–B
EASL–EORTC Clinical Practice Guidelines: Management of hepatocellular carcinoma. Journal of Hepatology 2012 vol. 56 j 908–943
Best supportive
care
Target: 10%
OS: <3 mo
Updated BCLC staging system and
treatment strategy
PST 0-1
83. Sorafenib increased overall survival in
different patient populations
1.00
0.75
0.50
0.25
0 4 6 8 10 12 14 162
0.00
18
Survivalprobability
Months
Sorafenib (n = 150)
Median OS: 6.5 months
(95% CI: 5.6–7.6)
Placebo (n = 76)
Median OS: 4.2 months
(95% CI: 3.7–5.5)
1.00
0.75
0.50
0.25
0 4 8 12 22
0.00
2 6 10 14 16 18 20
HR = 0.68
Asia–Pacific 2
1. Llovet JM, et al. N Engl J Med. 2008;359:378-90.
2. Cheng A-L, et al. Lancet Oncol. 2009;10:25-34.
Survivalprobability
Months
Sorafenib (n = 299)
Median OS: 10.7 months
(95% CI: 40.9–57.9)
HR = 0.69
SHARP 1
Placebo (n = 303)
Median OS: 7.9 months
(95% CI: 29.4–39.4)
Sorafenib prolongs OS by 44% Sorafenib prolongs OS by 47%
84. Sorafenib dose and overall survival in clinical practice
SOFIA study
GIDEON study
85. • Systemic chemotherapy with conventional agents, octreotide, interferon,
tamoxifen, and anti-androgenic drugs has no role in HCC treatment (1b-A).
****
• Full dose sorafenib is the recommended treatment for HCC patients with
preserved liver function who are not amenable to surgery and loco-
regional treatments or in whom TACE failed, according to the Italian
National Health Service rules (1b-A).
In patients intolerant to full dose sorafenib, the tolerance to a reduced dose
(400 mg/day) is to be pursued before definitively suspending the
treatment (2b-B).
****
• HCC patients who cannot receive any effective treatment for HCC must
receive symptomatic treatment for pain management, and nutritional and
psychological support (5-D).
Terapia sistemica dell’HCC:
raccomandazioni AISF
AISF position paper, Digest Liver Dis, 2013
86. Terapia antivirale:
raccomandazioni AISF
• All HBV-DNA positive patients should receive antiviral
therapy with nucleos(t)ide analogues at the time of and after
HCC treatment (2b-B).
• HCV-RNA positive patients with preserved liver function
(Child-Pugh class ≤8) whose HCC has been treated with
curative intent should be considered potential candidates to
antiviral therapy (2b-B).
• The AISF position on the usage of antiviral drugs is reported in greater
detailed elsewhere
AISF position paper, Digest Liver Dis, 2013
Sappiamo con certezza che, nelle aree non colpite da una iperendemia da HBV, almeno l’80%. Se poi consideriamo le cause più comune di CLD e HCC nel mondo occidentale (C ed alcool), raggiungiamo prevalenze prossime al 100%.
Alllora si può pensare di accoppiare, come viene accettato dalle attuali linee guida, di accoppiare i due test di sorveglianza. Vediamo vantaggi e svantaggi di questa strategia analizzando i risultati di uno studio prospettico su un grande campione di soggetti con infezione cronica da HBV: accoppiandoli si ottiene un aumento della sensibilità dell’8%, ma a prezzo di un raddoppiamento dei risultati falsi positivi ed un dimezzmento del PPP.
La ripercussione economica è pesantissima, aumentando il costo di ogni HCC diagnosticato dell’84% rispetto all’uso della sola US.
Rispetto alle AASLD Practice Guidelines 2010 (1), l’algoritmo proposto: 1) contempla anche la CEUS fra le tecniche di diagnosi per immagini utilizzabili ai fini diagnostici 2) predilige la sorveglianza trimestrale (invece che lasciare spazio a un programma semestrale o trimestrale, a scelta del clinico) per i primi 12 mesi, nel caso di nodulo < 1cm o nodulo atipico.
Lo schema di trattamento BCLC propone differenti opzioni terapeutiche in base allo stadio del tumore. I pazienti in stadio 0 (HCC molto precoce) sono candidati ideali alla resezione. I pazienti in stadio A presentano tumori in stadio precoce asintomatici e sono idonei a trattamenti radicali (resezione, trapianto, trattamenti percutanei, quali alcolizzazione o radiofrequenza). Lo stadio B (HCC intermedio) include pazienti con HCC multinodulare asintomatico che possono trarre beneficio dalla chemioembolizzazione. Nello stadio C (HCC avanzato) sono inclusi pazienti con tumori sintomatici e/o con invasione vascolare/disseminazione extraepatica. Questa categoria di pazienti è idonea al trattamento con sorafenib. I pazienti appartenenti allo stadio D presentano una prognosi molto sfavorevole, per loro si suggerisce un trattamento sintomatico. Llovet JM et al. J Gastroenterol 2005; 40: 225-235; Llovet JM et al. J Natl Cancer Inst 2008;100: 698 – 711
This slide presents preliminary OS by concomitant TACE use from the start of sorafenib therapy Preliminary median OS from the start of sorafenib therapy was longer for patients who received concomitant TACE Median OS was 13.1 months and 8.5 months, respectively, in patients who did and did not receive TACE concomitantly with sorafenib In this second interim analysis, outcomes data must be considered preliminary. Final analyses are planned in the future, in fully mature data