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Natural History and Staging System for HCC

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Page 1: Natural History and Staging System for HCC. Child–Pugh scoring system Points 123 Encephalopathy (grade)None1–23–4 AscitesNoneSlightModerate Albumin (g/dL)>3.52.8–3.5

Natural History andStaging System for HCC

Page 2: Natural History and Staging System for HCC. Child–Pugh scoring system Points 123 Encephalopathy (grade)None1–23–4 AscitesNoneSlightModerate Albumin (g/dL)>3.52.8–3.5

Child–Pugh scoring system

Points

1 2 3

Encephalopathy (grade) None 1–2 3–4

Ascites None Slight Moderate

Albumin (g/dL) >3.5 2.8–3.5 <2.8

Prothrombin time prolonged (sec) or INR

<4<1.7

4–61.7-2.3

>6>2.3

Bilirubin (mg/dL) <2 2–3 >3

for primary biliary cirrhosis <4 4–10 >10

Pugh RN, et al. Br J Surg. 1973 ;60: 646-649; Riley TR et al. Am Fam Physician 2001; 64: 1555-60

Class A: 5–6 points

Class B: 7–9 points

Class C: 10–15 points

Page 3: Natural History and Staging System for HCC. Child–Pugh scoring system Points 123 Encephalopathy (grade)None1–23–4 AscitesNoneSlightModerate Albumin (g/dL)>3.52.8–3.5

Median survival

Compensated cirrhosis: > 12 years

Decompensated cirrhosis: ~ 2 years

Natural history and prognostic indicators for survival in Cirrhotic Patients

Markedly longer survival in patients with compensated cirrhosis vs those with decompensated cirrhosis

1 year risk

D’Amico G, et al. J Hepatology. 2006;44:217-231

Page 4: Natural History and Staging System for HCC. Child–Pugh scoring system Points 123 Encephalopathy (grade)None1–23–4 AscitesNoneSlightModerate Albumin (g/dL)>3.52.8–3.5

Compensated cirrhosis: absence of jaundice, ascites, portal-systemic encephalopathy or variceal bleeding

Natural history and prognostic indicators for survival in Cirrhotic Patients

Pro

bab

ilit

y o

f su

rviv

al (

%)

Months

Compensated cirrhosisn=806

Decompensated cirrhosisn=843

100

75

50

25

00 12 24 36 48 60 72 84 96 108 120

100

80

60

40

20

0

100

80

60

40

20

Child–Pugh A

1 yr 2 yr 1 yr 2 yr 1 yr 2 yr

Child–Pugh B Child–Pugh C

Compensated

1 yr 2 yr

Decompensated

1 yr 2 yr

Su

rviv

al

(%)

Su

rviv

al

(%)

D’Amico G, et al. J Hepatology. 2006;44:217-231

Page 5: Natural History and Staging System for HCC. Child–Pugh scoring system Points 123 Encephalopathy (grade)None1–23–4 AscitesNoneSlightModerate Albumin (g/dL)>3.52.8–3.5

5

Liver cirrhosis: Prognosis by stage

1. de Franchis R [Editor]. Portal Hypertension V: Proceedings of the Fifth Baveno International Consensus Workshop, 5th Ed. 2010

Classification system proposed at the Baveno V workshop1

Compensated Decompensated

No varices

STAGE 1

DEATH

STAGE 2 STAGE 3 STAGE 4 STAGE 5

STAGE 6 ?

Varices Bleeding AscitesAscites

Bleeding

SepsisRenal failure

4–6%

8–12%

10–20%

5–8%

3–5%1%

10–15%

7–10%

~30%

26%

6–15%

N%= expected 1-year outcome rates

No varices

STAGE 1

DEATH

STAGE 2 STAGE 3 STAGE 4 STAGE 5

Varices Bleeding AscitesAscites

Bleeding

SepsisRenal failure

Page 6: Natural History and Staging System for HCC. Child–Pugh scoring system Points 123 Encephalopathy (grade)None1–23–4 AscitesNoneSlightModerate Albumin (g/dL)>3.52.8–3.5

6

Survival rates among untreated patients with unresectable HCC

Meta-analysis of patients included in the placebo or no-treatment arms of 30 randomized controlled trials (n=1927)

1. Cabibbo G et al. Hepatology 2010:51:1274-1283; 2. Cabibbo G et al. Hep Med Evidence Res2010:2;163-73.

Survival rates highly heterogeneous

Shorter survival for:– Impaired PS– CP-B or -C– Presence of PVT

Page 7: Natural History and Staging System for HCC. Child–Pugh scoring system Points 123 Encephalopathy (grade)None1–23–4 AscitesNoneSlightModerate Albumin (g/dL)>3.52.8–3.5

The TNM staging system

Stage Tumor Node Metastases

I T1 N0 M0

II T2 N0 M0

IIIA T3 N0 M0

IIIB T4 N0 M0

IIIC Any T N1 M0

IV Any T Any N M1M = metastases; N = node; T = tumor.

1.Bruix J, Sherman M. Hepatology. 2011;53:1020-2. 2. Pons F, et al. HPB (Oxford). 2005;7:35-41. 3. Kee K, et al. Int J Cancer. 2007;120:2650-

2655.

Advantage of TMN in HCC

• The TNM system and the simplified TNM system are used in many cancers, and therefore there is familiarity with the system1

• Commonly used in the USA in HCC patients1

• Widely tested in the surgical HCC population2

Page 8: Natural History and Staging System for HCC. Child–Pugh scoring system Points 123 Encephalopathy (grade)None1–23–4 AscitesNoneSlightModerate Albumin (g/dL)>3.52.8–3.5

Disadvantages of the TNM in HCC

• There is lack of homogeneity in outcomes for patients within certain current TNM categories1

• Poor stratification of survival at intermediate stages2

• Requires evidence of microvascular invasion, something that is not available except from surgical specimens3

• Use is limited as it is based on pathological findings and does not consider liver function or tumors < 5 cm4

• Changes to the TNM system have been proposed by several authors, but it still lacks adequate prognostic accuracy1,2,4

The TNM staging system

1. Wildi S, et al. Br J Surg. 2004;91:400-8. 2. Marrero JA, et al. Hepatology. 2005;41:707-16.

3. Bruix J, Sherman M. Hepatology. 2011;53:1020-2.4. Pons F, et al. HPB (Oxford). 2005;7:35-41.

Page 9: Natural History and Staging System for HCC. Child–Pugh scoring system Points 123 Encephalopathy (grade)None1–23–4 AscitesNoneSlightModerate Albumin (g/dL)>3.52.8–3.5

CLIP staging system for HCC

Median survivalCombined score 0: 35.7 months

Combined score 2: 8.5 months

Combined score 4-6: 3.2 months

Modified from The CLIP investigators. Hepatology 2000; 31: 840-845

Variable 0 1 2

Child-Pugh score A B C

Tumor morphologyUninodular and extension ≤ 50%

Multinodular and extension ≤ 50%

Massive or extension > 50%

AFP (ng/dL) < 400 ≥ 400

Portal vein thrombosis No Yes

Page 10: Natural History and Staging System for HCC. Child–Pugh scoring system Points 123 Encephalopathy (grade)None1–23–4 AscitesNoneSlightModerate Albumin (g/dL)>3.52.8–3.5

0 2 4 6 8 10

Survival period (year)

Su

rviv

al r

ate

(%)

(n = 722)

6

5

4 3

21

0

CLIP 0 (n = 229)

CLIP 1 (n = 241)

CLIP 2 (n = 136)

CLIP 3 (n = 70)

CLIP 4 (n = 31)

CLIP 5 (n = 8)

CLIP 6 (n = 7)

p < 0.0001

p < 0.01

p < 0.0001

NS

NS

NS

Survival according to the CLIP scoring system

Kudo M, et al. J Gastroenterol. 2003;38:207-15.

• Survival at 3, 5, and 10 years, respectively, for each CLIP group was

− 86%, 72%, and 23% for CLIP 0

− 70%, 47%, and 19% for CLIP 1

− 53%, 37%, and 8% for CLIP 2

− 20%, 7%, and 0% for CLIP 3

− 15%, 15%, and 15% for CLIP 4

− 0%, 0%, and 0% for CLIP 5/6

Page 11: Natural History and Staging System for HCC. Child–Pugh scoring system Points 123 Encephalopathy (grade)None1–23–4 AscitesNoneSlightModerate Albumin (g/dL)>3.52.8–3.5

The Barcelona Clinic Liver Cancer (BCLC) staging classification for HCC

Llovet JM et al. J Gastroenterol 2005; 40: 225-235

BCLC stagePerformance

statusTumor volume,

number and invasiveness Child-Pugh

0 Very early 0Single < 2 cm

Carcinoma in situA

A Early 0 Single or 3 nodules < 3 cm A – B

B Intermediate 0 Multinodular A – B

C Advanced 1 – 2 Portal invasion N1M1 A – B

D Terminal > 2 Any of above C

Page 12: Natural History and Staging System for HCC. Child–Pugh scoring system Points 123 Encephalopathy (grade)None1–23–4 AscitesNoneSlightModerate Albumin (g/dL)>3.52.8–3.5

Months

%

Survival

A

B

C

D

Log-rank PA vs B P=0.0002B vs C P<0.0001C vs D P=0.057

Prognosis of newly diagnosed HCC patients (1999 2005) by BCLC class

Cammà et al. Aliment Pharmacol Ther 2008; 28: 62-75

Page 13: Natural History and Staging System for HCC. Child–Pugh scoring system Points 123 Encephalopathy (grade)None1–23–4 AscitesNoneSlightModerate Albumin (g/dL)>3.52.8–3.5

Staging systems for HCC

Marrero JA et al. Hepatology 2005; 41: 707-716

Staging SystemHepatic function AFP PS Tumor staging

BCLC CTP No YesTumor size, No. of nodules

and PVT

OkudaAscitesAlbuminBilirubin

No NoTumor greater or less

than 50% of cross-sectional area of liver

TNM No No NoNo. of nodules, tumor size,

presence of PVT and metastasis

CLIP CTP< 400 or

≥ 400 ng/mLNo

No. of nodules, tumor greater or less than 50%

area of liver, PVT

CUPIAscites

Bilirubin, AP< 500 or

≥ 500 ng/mLSymptoms TNM

JIS CTP No No TNM

GRETCHBilirubin

AP< 35 or

≥ 35 μg/mLYes PVT

AFP: alpha fetoprotein; AP: alcaline phosphatase; CTP: Child-Turcotte-Pugh; PS: performance status; PVT: portal vein thrombosis

Page 14: Natural History and Staging System for HCC. Child–Pugh scoring system Points 123 Encephalopathy (grade)None1–23–4 AscitesNoneSlightModerate Albumin (g/dL)>3.52.8–3.5

Staging of HCC: Several different systems are available

AFP, alpha-fetoprotein; AP, alkaline phosphatase; BCLC, Barcelona Clinic Liver Cancer; CLIP, Cancer of the Lliver Italian Program; CUPI, Chinese University Prognostic Index; GRETCH, Groupe d'Etude et de Traitement du Carcinome Hépatocellulaire; HCC, hepatocellular carcinoma; Histol., histological; JIS, Japan Integrated Stage; TNM, tumor nodes metastases.1. American Cancer Society. Available at: http://www.cancer.org/docroot/CRI/content/CRI_2_4_3X_How_is_liver_cancer_staged_25.asp; 2. Schafer DF, et al. Lancet 1999;353:1253-7; 3. Makuuchi M, et al. World J Gastroenterol 2006;12:828-9; 4. CLIP. Hepatology 1998;28:751-5; 5. Chevret S, et al. J Hepatol 1999;31:133-41; 6. Llovet JM, et al. Semin Liver Dis 1999;19:329-38; 7. Leung T, et al. Cancer 2002;94:1760-9.

System

Tumour Spread Liver Symptoms

Tumour features

Histol. grade

AFP Vascular invasion

Metastases Child-Pugh

Bilirubin AP Ascites Cancer symptoms

TNM1 Okuda2 JIS3 CLIP4 GRETCH5 BCLC6 CUPI7

Page 15: Natural History and Staging System for HCC. Child–Pugh scoring system Points 123 Encephalopathy (grade)None1–23–4 AscitesNoneSlightModerate Albumin (g/dL)>3.52.8–3.5

HCC staging is complex and multifaceted

Staging is used for prognosisand to guide treatment1

Staging HCC1

• Most patients have underlyingliver disease

• Key prognostic indicatorsare not clearly defined

• Prognostic indicators vary during the course of disease

Factors affecting staging2,3

• Tumour stage

• Liver function

• Health status

• Impact of treatment

BCLC, Barcelona Clinic Liver Cancer; CLIP, cancer of the liver Italian program; CUPI, Chinese University Prognostic Index; ECOG PS, Eastern Cooperative Oncology Group performance status; GRETCH, Groupe d'Etude et de Traitement du Carcinome Hépatocellulaire; HCC, hepatocellular carcinoma; JIS, Japan Integrated Stage; TNM, tumor nodes metastases.

1. Llovet JM, et al. Lancet 2003;362:1907–17; 2. Marrero JA, et al. Clin Liver Dis 2006;10:339–51; 3. Marrero JA, et al. Hepatology 2005;41:707–16; 4. Llovet JM, et al. Semin Liver Dis 1999;19:329–38; 5. Leung T, et al. Cancer 2002;94:1760–1769; 6. Chevret S, et al. J Hepatol 1999;31:133–41; 7. Schafer DF, et al. Lancet 1999;353:1253–7; 8. CLIP. Hepatology 1998;28:751–5; 9. Makuuchi M, et al. World J Gastroenterol 2006;12:828–9.

Patient

TumourLiver

ECOGPS

Child-Pugh

TNM

BCLC4

Okuda7

CLIP8

JIS9

CUPI5

GRETCH6

Page 16: Natural History and Staging System for HCC. Child–Pugh scoring system Points 123 Encephalopathy (grade)None1–23–4 AscitesNoneSlightModerate Albumin (g/dL)>3.52.8–3.5

Cillo U, et al. J Hepatol. 2006;44:723-31.

Prospective validation of the BCLC staging system

The BCLC staging system gives a more precise prognostic stratification in a study group treated mainly with radical therapies

Univariate model(All patients n = 195)

Linear trend2 test

LHR 2 test(p value)

AIC

Okuda 3.98 8.87 (0.0118) 933.06

CLIP 4.17 7.83 (0.0979) 938.10

UNOS-TNM 20.03 28.31 (0.0000) 915.62

JIS 12.45 15.77 (0.0013) 928.16

BCLC 43.01 57.94 (0.0000) 885.98

Multivariate modelAll patients (n = 195)

Log-likelihoodLHR 2 test

(p value)AIC

Full model 434.80 – 899.60

Removing Okuda 436.29 2.97 (0.2258) 898.58

Removing CLIP 436.36 3.11 (0.5385) 894.72

Removing UNOS-TNM 437.47 5.32 (0.1494) 898.94

Removing JIS 435.43 1.26 (0.7386) 896.86

Removing BCLC 449.92 48.90 (0.0000) 923.84

Assessment of BCLC discrimination in the 195 HCC patients

Page 17: Natural History and Staging System for HCC. Child–Pugh scoring system Points 123 Encephalopathy (grade)None1–23–4 AscitesNoneSlightModerate Albumin (g/dL)>3.52.8–3.5

RFA Sorafenib

Stage 0PST 0, Child–Pugh A

Very early stage (0)

single <2cmCarcinoma in situ

Early stage (A)1 HCC or 3 nodules

<3cm, PST 0

Advanced stage (C)

Portal invasion, N1, M1, PST 1–2

End stage (D)

Liver transplantation TACEResection Symptomatictreatment Curative treatments Palliative treatments

Associated diseases

YesNo

3 nodules ≤3cm

Increased

Normal

1 HCC

Portal pressure/bilirubin

Stage DPST >2, Child–Pugh C

HCC

Intermediate stage (B)Multinodular,

PST 0

Stage A–CPST 0–2, Child–Pugh A–B

AASLD PRACTICE GUIDELINES 2011: Staging and treatment of HCC

Llovet JM, et al. J Natl Cancer Inst. 2008; 100: 698–711

Page 18: Natural History and Staging System for HCC. Child–Pugh scoring system Points 123 Encephalopathy (grade)None1–23–4 AscitesNoneSlightModerate Albumin (g/dL)>3.52.8–3.5

HCC presentation and survival by BCLC stage in untreated patients from randomized trials

HCC

Stage A–COkuda 1–2, PS 0–2, Child-Pugh A–B

Stage 0PS 0, Child-Pugh A

Stage DPS >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)

1. Lencioni R et al. Radiol 2005; 234:961–967; 2. Llovet JM, et al. J Natl Cancer Inst 2008;100:698–7; 3. Bruix B, Llovet J. Hepatology 2002;35:51924; 4. Cottone M et al. Gastroenterology 1989; 96:1566-71; 5. Cabibbo G et al. Hepatology 2010:51:1274-1283.

BCLC stage 0-A BCLC stage B BCLC stage C BCLC stage D

30% of pts at presentation3 50% of pts at presentation3 20% of pts3

Asymptomatic HCC: 96% 1-year survival4

50% 1-year survival5

25% 1-year survival5

11% 1-year survival5

Page 19: Natural History and Staging System for HCC. Child–Pugh scoring system Points 123 Encephalopathy (grade)None1–23–4 AscitesNoneSlightModerate Albumin (g/dL)>3.52.8–3.5

Tumour doubling in untreated nodules

59 small HCCs in 39 patients:

• No correlation to initial tumour size

• No significant relation to cirrhosis severity (trend to faster DT if more severe)

• Serial tumour volume measurements over time identified different growth patterns

Almost constant growth rate (n=8)

Declining growth rate over time (n=9)

Months

Ch

an

ge

in

tu

mo

ur

vo

lum

e

No or very slow initial growth (DT > 200 days); subsequent increasing growth rate (n=10)

Barbare L et al. Hepatology 1992;16:132-7.

Page 20: Natural History and Staging System for HCC. Child–Pugh scoring system Points 123 Encephalopathy (grade)None1–23–4 AscitesNoneSlightModerate Albumin (g/dL)>3.52.8–3.5

•T1: Resection

Ablation

•T2: Transplant

• 5-yr survival rates 50 – 70%

• HCCs detected in T1 & T2 stages show much better survival• Sensitive imaging modalities to detect HCCs in its early stages

El-Serag HB, et al. Gastroenterology 2008; 134:1752-1763.

Clinical Importance of Early Detection & Precise staging of HCC

Page 21: Natural History and Staging System for HCC. Child–Pugh scoring system Points 123 Encephalopathy (grade)None1–23–4 AscitesNoneSlightModerate Albumin (g/dL)>3.52.8–3.5

Common worldwide, although disease aetiology varies Often occurs in conjunction with liver cirrhosis Liver function of prognostic importance in cirrhotic patients

• CP-A survival > CP-B survival > CP-C survival Multitude of staging systems exist

• Tumour characteristics alone are unlikely to adequately predict prognosis

• Integrated staging systems are mandatory BCLC staging system links integrated staging and treatment strategy The natural history of intermediate/advanced stage HCC is dismal and prognosis

for patients still remains very poor

• In fact, surgical or locoregional treatments of large tumour burden may further worsen liver function, which might be compromised already

There is a pressing need for improved management strategies to improve survival

The natural history of HCC – a summary

HCC, hepatocellular carcinoma; CP, Child-Pugh.