The topic explored in this powerpoint presentation is Radiosurgery in Liver Tumors: Recent Updates.''

1. ------------------------ HCC ?
Radiosurgery in liver tumours: Recent updates

2. Worldwide Incidence of Hepatocellular Carcinoma
High (> 30:100,000)
Low or data unavailable (< 3:100,000)
Intermediate (3-30:100,000)
Worldwide Incidence of Hepatocellular Carcinoma
HCC Epidemiology
El-Serag HB,
Gastroenterology
2004

3. HCC: Facts
- 70% of pts present with advanced disease (Stage BCLC C)
- Majority have background hepatitis B/C with cirrhosis
- Nodal involvement common
- Majority have impaired liver function
Curative intent surgery/ transplant possible only 30% patients

4. Inoperable HCC: Sorafinib
Study Type N Result
Llovet JM*
(2008)
Multi-centric
Ph III
602 Median OS: 10.7 vs 7.9 mo (P<0.001).
Symptomatic progression : 4.1 vs. 4.9 mo, (P=0.77).
Radiologic progression: 5.5 vs 2.8 mo (P<0.001).
3 month survival benefit
Abou-Alfa GK^
(2006)
Ph II 137 Median TTP: 4.2 mo & OS: 9.2 mo.
Grade 3/4 toxicities: Fatigue (9.5%), diarrhea (8.0%), & hand-
foot skin reaction (5.1%).
Muszbek N#
(2008)
Ph III
Economic
analysis
- LYG was longer for sorafenib.
(1.52 vs. 1.03 LYG/pt for sorafenib & BSC).
Lifetime total costs: $47,51 for sorafenib & $10,376 for BSC
ICER: $75,821/LYG.
Cheng AL^^
(2009)
Multi-centric
Ph III
271 Median OS: 6.5 vs 4.2 mo(p=0.014).
Median TTP :2.8 vs1.4 mo (p=0.0005).
*N Engl J Med. 2008 ;359(4):378-90. ^J Clin Oncol. 2006 ;24(26):4293-300.
#Curr Med Res Opin. 2008 ;24(12):3559-69. ^^Lancet Oncol. 2009 Jan;10(1):25-34
Median survival 10.7 months: Grade 3/4 toxicity: 10%

5. Where is radiation ?
Bruix et al Lancet 2009

6. Llovet. J of Hepatology 2008
HCC treatment: Based on low level of evidence

7. Why RT is not the initial choice in HCC
- HCC considered ‘radio-resistant’
- Usually late presentation: large tumour- ONLY palliative care
- Liver is relative radiosensitive; low tolerance
- ‘Radiation induced liver disease (RILD)’: ‘anicteric hepatitis’
- Difficult to deliver high dose!!
- Liver moves with respiration: need 3-4 cm margin- difficult to spare liver
- Technology not available to deliver precise radiation therapy

8. Sonaki N et al, W J Gastro 2015
HCC Management
Role of Radiosurgery in HCC is established

9. Role of RT in HCC
- Radical radiation therapy / SBRT
- ‘Bridge to transplant’
- Palliative intent RT
- SBRT along with systemic therapy

10. 3-D Conformal RT

11. IMRT

12. Radiosurgery

13. Modern SBRT Systems

14. Modern SBRT Accuracy
• Mechanical Accuracy = 0.2 mm
• Total Clinical Accuracy
– Stationary lesions: 0.95 mm
– Moving lesions: 1.5 mm
Total
Clinical
Accuracy
CyberKnife
Total Clinical Accuracy
Chang et al.Neurosurgery, 2003
Murphy MJ et al. Int J Radiat Oncol Biol Phys. 2003

15. Synchrony
TM
Fiducial based tracking along
with respiratory motion tracking

16. Radical RT/ SBRT
• Early stage (0-A) disease
• Few occasions even in multifocal lesions (Stage B)
• Cirrhotic background- surgery is difficult
• Medically inoperable or comorbidities
• Technically ‘difficult to do surgery’ (subdiaphragamatic, porta)
• Patient not willing for surgery

17. Study Type n Dose Median
FU (Mo)
LC (%) OS Toxicity
Mendez (2006) Ph I/II 8 25Gy/%#
30Gy/3#
13 82 1-Yr: 75%
2-Yr: 40%
Gr-3/4: 1 pt
Choi (2006) Ph II 20 50Gy/5-10# 23 NR 1-Yr: 70% Gr-3: Nil
Tse (2008) Ph I 31 36Gy/6# 17.6 65 Median OS: 11.6 mo
1-Yr: 48%
Gr-3: 8 pt
Choi (2008) Ph II 31 30-36Gy/3# 10.5 72 At 11 mo: 72% Gr-3: Nil
Yang (2009) Ph II 40 50Gy/10# 35 65 1-Yr: 73% Gr-3: Nil
Cardenes (2010) Ph I 6 12-16 Gy/2-3# 24 100 1 Yr: 75%
2-Yr: 60%
Gr-3: 3 pt
Louis (2010) Ph II 25 45Gy/3# 12.7 95% 1-Yr OS: 79% Gr-3: 2 pt
Early studies: SBRT for HCC
All recurrent / resistant HCCs
Local control / survival function: impressive

18. HCC: Recent studies
Author Jour n Study criteria FU Outcome
Price TR Cancer
2012
26 Awaiting for liver
transplant
13 CR-4
PR-15
Resp rate 73%
CTCAE Gr-3: Nil
Ibarra RA Acta
Oncol
2012
21 Inoperable HCC 12.9 TTP=6.3 mo
1-Yr OS 87%
2-Yr OS 55%
Facciuto
ME
J Surg
Oncol
2012
39 Post TACE residual
Progressive
CR 30%
Stable 57%
Prog 7%
Excellent response rate with SBRT

19. HCC: Recent studies
Author Jour n Study criteria FU
(mo)
Outcome
Goyal HPB 2012 17 Recurrent
Dose 35Gy
8 Vol reduction: 44%
LC 82%
Seo YS J Surg
Oncol
2010
38 Inoperable HCC ,
10 cm / post-TACE
Dose 45Gy
High dose indepent prog factor
2-Yr OS 61.4%
Kwow JH BMC
2010
42 Post TACE residual
Progressive
Dose 39 Gy
1-Yr OS 92.9%
3-Yr OS 58.6%
High dose RT independent prognostic factor

20. Recurrent/ progressive HCC (n=174)
Recurrent progressive HCC
SBRT= 42
No SBRT= 138
Median FU= 20 months
Dose= 37Gy
Local control
1-Yr: 87.6%
2-Yr: 75.1%
Overall survival
2-Yr: 64%
Median Survival: 8 mo
Independent prognostic factor:
1.SBRT
2.T<4 cm
3.Stage I
4.Child Pugh A
2-Yr OS p-value
SBRT 72.6%
0.013NO SBRT 42.1%
Huang WY et al, IJROBP 2012

21. SBRT: Prognostic factors
Evaluated 153 HCC pts
HCC= 48 pts
Median FU= 15 mo
Dose= 45Gy/3#
T= 33 mm
Local Control-
1-Yr: 84%
2-Yr: 74.6%
Factors influencing outcome:
T<50 mm (p=0.019)
TD>45Gy (p=0.001)
D/Fr >15Gy (p=0.019)
Dewas S et al, Radiat Oncol 2012

22. TACE+ SBRT in unresectable HCC
Study n RT Dose Results
Yoshikawa (1990) 31 48 Gy 5-Yr: 35%
Guo (2003) 107 55 Gy 3-Yr: 28.4%
5-Yr: 15.8%
Wu (2004) - - 1-Yr: 93.6%
2-Yr: 53.8%
3-Yr: 25.9%
MS: 25 mo
Marelli (2006) Meta-analysis
7 RCT
- Improves survival with
TACE+SRT
Zhou 50 - 1-Yr: 60%
2-Yr: 38%
3-Yr: 28%
MS: 17 mo
TACE + SRT is a safe an effective palliation treatment in unresectable HCC

23. Liver tumour: CyberKnife: ASH protocol
Liver tumour prior to CK evaluated by hepatic surgeon
Inoperable or not willing for surgery counseled for CK
Assessed with triphasic 320 slice CT scan
Vacloc preparation
MRI scan of liver as per CK protocol
Fiducial placement under USG/CT scan guidance
Wait for 3-5 days for fiducial stabilization
CT scan with vacloc as per CK protocol
Treatment with fiducial tracking on Syncrony
21-45 Gy/3# treatment as per critical structure constraints

24. Planning & treatment execution
Contouring:
CT scan & MRI scan fusion
Occasionally PET scan fusion
Target (GTV) & critical structures contoured
(liver, duodenum, small intestine, kidney)
PTV margin ≅ 2 mm
Planning done: on Multiplan
Plan approved as per:
1.Target coverage
2.Critical structure dose
3.Nodes / beamlets / MU / time
Critical structure constraints as per protocol

25. CK planning: Normal tissue constraints
Organ/ Critical
structure
Dose Constraints
Liver V21<33%
Spinal cord Dmax 22 Gy
Kidney V15< 33%
Stomach V21< 5 cm3
Intestine V16<5 cm3; Dmax < 27 Gy
Duodenum D15 < 5cm3; Dmax < 24 Gy
Timmerman et al, Sem Oncol 2008
At least 800 cc of liver <10Gy

26. CK planning

27. Demographic profile (n=50)
Mean age: 57.5 yrs
Male: 82%
Child Pugh A & B: 64%
KPS>80: 24%
Hepatitis: 46%
Single lesion: 72%
Tumour vol <90cc: 66%
Prior Rx: 76%
Dutta et al ESTRO 2013 (Abstr)

28. All pt HCC Mets
PTV (Target)
Mean vol (cc)
Range (cc)
Max dose (Gy)
Mean dose (Gy)
Prescription isodose (%)
Target Coverage (%)
Mean CI
Mean nCI
Mean HI
192
(10-
710)
36.3
33.3
84
94
1.13
1.28
1.19
196
(10-
710)
39
35.7
84
94
1.06
1.26
1.18
200
(50.7-628)
36
33.5
84
92
1.21
1.31
1.19
Liver
Mean volume (cc)
Mean dose (Gy)
20Gy Vol (cc)
10Gy Vol (cc)
800cc liver dose (Gy)
1197
4.7
111
357
8.2
1143
4.3
92.9
313.7
7.5
1582
7
182.5
532
10.2
Small intestine
Mean dose (Gy)
2% volume dose (Gy)
3.4
10.6
2.8
8.9
3.2
9.9
Dosimetry
Mean target Vol: 192 cc
Pres Isodose: 84%
Target coverage: 94%
Mean dose: 33 Gy
Dose Range: 21-45Gy
Fractions: 3
Mean liver dose: 4.7 Gy
800 cc liver: < 8.2 Gy
2% Small Intestine: 10.6 Gy
Dutta et al ESTRO 2013 (Abstr)

29. All pt
(n=31)
HCC
(n=13)
Mets
(n=18)
Median OS (mo) 9 10.5 6.5
Mean OS (mo)
Range
12.4
1.9-44.6
18.4
2.1-44.6
8.2
1.9-24.6
Status at LFU
Local control
Progression
Metastasis*
Dead
Alive
9 (29)
15 (48)
6 (19)
19 (61)
12 (39)
2 (15)
7 (53)
3 (23)
10 (77)
3 (23)
7 (39)
8 (44)
3 (17)
9 (50)
9 (50)
Toxicity profile
GI Toxicity Gr- I-II
Gr-III-IV
Other^
5 (29)
0
1 (12)
1 (11)
0
1 (11)
2 (50)
0
0
Fiducial related toxicity
Pain 2 (24) 1 (11) 1 (25)
*One pt with HCC had brain metastasis at 2 yrs FU. One HCC pt had extensive mets at 7 mo post-CK.
^One pt had anicteric ascites, pedal oedema, high alk phos 3 mo post-CK, resolved with supportive care
Survival function
Dutta et al ESTRO 2013 (Abstr)

30. Survival function
p-value: NS
Median Survival:
HCC: 10.1 mo
Mets: 9.0 mo
1yr Survival:
HCC: 45%
Mets: 30%
Dutta et al ESTRO 2013 (Abstr)

38. Factors
Median OS
(mo)
p-value^
KPS
70-80 8.3
0.034
90-100 15.4
Child Pugh
A/B 13.3
0.039
C 4.9
Cirrhosis
No 13.3
0.005
Yes 9.4
Prior Rx
yes 8.3
0.006
No 16.6
Hepatitis
No 10.5
0.977
yes 9.5
Dose
<39Gy 9.5
0.02
>39Gy 15.4
Volume
<10cc 15.7
0.011
>90cc 7.2
Factors influence outcome
1) Higher KPS,
2) Favourable Child Pugh,
3) No corrhosis,
4) No prior Rx,
5) Dose>39Gy
6) Small volume disease patients
have significantly better survival
^Log Rank test
Dutta et al ESTRO 2013 (Abstr)

39. Our Survival function data: HCC
Study Type n Survival (mo) Toxicity (Gr-3/4)
Llovet JM* (2008)
Ph III 602 10.7
Abou-Alfa GK^ (2006) Ph II 137 9.2 Fatigue (5%),
diarrhea (8.0%),
hand-foot dis (5.1%)
Cheng AL (2009) Ph III 271 6.5
Our study (2015) Retro 50 10.4 1 pt with anecteric
hepatitis
Our pt cohort is heavily pre-treated (76%),
Progression on chemotherapy
and high viral load (Hep B/C)
Dutta et al ESTRO 2013 (Abstr)

40. Patient selection
NOT only the size, site of lesion also matters

41. Outcome depends not ONLY on planning
BUT also on execution

42. Liver movement (n=51 snaps)
Liver movement is more erratic than we think
Snap1 Snap2 Snap3
Lat shift 1.8 1.04 1.2
Ant Shift 1.2 1.28 1.91
Sup shift 2.9 3.3 2.84

43. Need internal fiducial based intra-fraction
tracking system
To treat liver tumour

44. Single vs multiple fiducial
No difference in survival function, BUT difference in T Time
Multiple fiducials Single fiducial
Survival: 15.6 vs 10.4 mo
No difference in survival function, BUT difference in T Time

45. Challenges: evaluation for local control
NO suitable imaging method to assess response after CK,
need to evaluate efficacy only with Survival Function

48. Survival Function in
Small Vol (<10cc), CP A, Single lesion, No prior Rx
p-value: 0.001
Median survival
Vol<10 cc, KPS>80, No Prior Rx:
19.2 months
Vol>90cc, KPS<80, Prior Rx:
6.4 months

49. ‘Palliative SBRT’
• Inoperable
• Progressive/ Recurrent disease
• Not responding to chemotherapy
• Not able to tolerate chemotherapy
• Poor GC: no systemic therapy
• Aim: symptom palliation

50. Phase II Trial: Palliative RT for HCC (n=42)
Purpose Evaluate feasibility & response of liver radiotherapy (RT) in improving symptoms QOL
Patients and Methods Pts unsuitable for or refractory to standard therapies, with an index symptom of pain,
abdominal discomfort, nausea, or fatigue. The Brief Pain Inventory (BPI), Functional Assessment of Cancer
Therapy–Hepatobiliary (FACT-Hep), and EORTC QLQ-C30 were completed by pts at baseline and each follow-
up.
Primary outcome: % of pts with a clinically significant change at 1 mo BPI subscale of symptom
Results
At 1 mo, 48% had an improvement in symptom on average in the past wk.
52% had improvement in symptom at its worst, 37% at its least, and 33% now.
Improvements FACT-G & hepatobiliary subscale in 23% and 29%.
Improvements in EORTC QLQ-C30 functional (range, 11% to 21%) and symptom (range, 11% to 50%) domains.
Conclusion Improvements in symptoms were observed at 1 month in a substantial proportion of patients.
Soliman H et al JCO 2013

51. ‘Bridge to transplant’
• Patient eligible for transplant but need to wait >3months
• Non-invasive option
• Evaluate response to radiation therapy

53. Bridge to transplant: literature
Median Follow up: 62 months
Patients: 10
Median SBRT dose: 51 Gy (33-54Gy)
All patients had orthotropic transplant
Pathological response: 27% CR
73% PR
No progression after SBRT (CK)
At 5 yr disease free survival: 100%
4 pts had acute toxicities (all grade I) (nausea, abdominal discomfort, fatigue)
O’Connor JK et al, Liver Transpl Mar 2012

54. CLOCC study
Presented By Theo Ruers at 2015 ASCO Annual Meeting ASC0 2015 Abstr

55. Overall Survival
Presented By Theo Ruers at 2015 ASCO Annual Meeting ASC0 2015 Abstr

59. Conclusions
- Robotic radiosurgery is an option in inoperable or medically not
suitable for surgery and in patient with progression / not tolerating
systemic therapy
- Initial results are impressive with low toxicity, good response rate
- Pts with small tumour, no prior treatment with good performance
treated with high dose have significantly better survival
- Dose >45 Gy; 15Gy/# and small vol tumour (<50cc) have better prognosis
- Need multi-centric prospective studies.

60. www.radiosurgery-india.com
duttadeb07@gmail.com
Oscar Lambart Centre. Nice, France
Dr Eric Latigo
Dr Mirabel
Lille CyberKnife Centre, France
Dr Bondiaue
Munich CyberKnife Centre, Germany
Dr Alex Muciavic
Dr Barnad Wowra
Apollo Hospitals team
Liver transplant team
Medical & Surgical gastroentrologist
Medical Oncologist
Radiologist
Medical Physicists
Acknowledgements