IMRT

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ESTRO Course Book IMRT and Other Conformal Techniques in Practice

4 - 8 October, 2015 Brussels, Belgium

NOTE TO THE PARTICIPANTS

The present slides are provided to you as a basis for taking notes during the course. In as many instances as practically possible, we have tried to indicate from which author these slides have been borrowed to illustrate this course. It should be realised that the present texts can only be considered as notes for a teaching course and should not in any way be copied or circulated. They are only for personal use. Please be very strict in this, as it is the only condition under which such services can be provided to the participants of the course.

Faculty

Marco Schwarz and Frank Lohr

Disclaimer

The faculty of the teachers for this event has disclosed any potential conflict of interest that the teachers may have.

Programme

Sunday 04 October 8.30 – 8.45 Introduction to the course - Marco Schwarz 8.45 - Group B : Going to UZ Brussel 9.30 – 10.00 Demo 1: Tomo patient QA - Katrien Leysen – Red Team 10.00 – 10.30 Demo 2: Tomo absolute calibration - Dirk Verellen – Orange Team 10.30 – 11.00 Coffee break 11.00-11.30 Demo 3: Real-time Tumour tracking - Jennifer Dhont – Green Team 11.30 – 12.00 Demo 4: Planning - Marlies Boussaert; Paul Bijderke - White Team Group A : Lectures at the Hotel Chair: Frank Lohr 9.00 – 9.30 Opening and welcome - Koen Tournel 9.30 – 10.00 Treatment of Rectal cancer using IMRT/IGRT at the UZ Brussel - Benedikt Engels 10.00 – 10.30 Coffee break 10.30 – 11.00 Treatment of lung and liver tumors using dynamic tracking - Thierry Gevaert

11.00 - 11.40 Treatment of oligometastases using an SBRT/IMRT/IGRT approach Robbe Van Den Begin 11.40 – 12.10 Radiosurgery at the UZ Brussel - Thierry Gevaert 12.30 - 13.30 Lunch 13.30 - Group A going to UZ Brussel 14.00 – 14.30 Demo 1: Tomo patient QA - Katrien Leysen – Red Team 14.30 – 15.00 Demo 2: Tomo absolute calibration - Dirk Verellen – Orange Team 15.30 – 16.00 Coffee break 16.00-16.30 Demo 3: Real-time Tumour tracking - Jennifer Dhont – Green Team 16.30 – 17.00 Demo 4: Planning - Marlies Boussaert; Paul Bijderke - White Team Group B - Lectures at the hotel: Chair: Matthias Söhn 14.00 – 14.30 Opening and welcome - Koen Tournel 14.30 – 15.00 Treatment of Rectal cancer using IMRT/IGRT at the UZ Brussel - Benedikt Engels

14.00 - 14.45 Image-guidance & Adaptive: concept and approaches – Matthias Söhn 14.45 - 15.30 Image-guidance & Adaptive: Clinical applications – Frank Lohr 15.30 - 16.00 Coffee break 16.00 - 16.45 IMRT in breast and risk of secondary cancer after IMRT – Frank Lohr 16.45 – 17.30 IMRT in Hodgkin's Lymphoma and secondary cancer risks– Andrea Filippi 17.30 – 22.30 Social Event @ Atomium Tuesday 6 Oct Chair: Matthias Söhn 9.00 - 9.45 ‘Patient specific’ QA – Marco Schwarz 9.45 – 10.30 Modeling adverse effects after 3DCRT and IMRT– Giovanna Gagliardi 10.30 - 11.00 Coffee break 11.00 -11.45 Review of Dose-volume relationships I: H&N - Giovanna Gagliardi 11.45 - 12.30 IMRT in Head and neck – Frank Lohr 12.30 - 14.00 Lunch

15.00 – 15.30 Coffee break 15.30 – 16.00 Treatment of lung and liver tumors using dynamic tracking - Thierry Gevaert 16.00 - 16.30 Treatment of oligometastases using an SBRT/IMRT/IGRT approach Robbe Van Den Begin 16.30 – 17.00 Radiosurgery at the UZ Brussel - Thierry Gevaert Monday 05 October Chair: Giovanna Gagliardi 9.00 - 9.30 Rational of IMRT. A clinician’s point of view - Frank Lohr 9.30 - 10.15 IMRT delivery techniques – Marco Schwarz 10.15 - 10.45 Coffee Break 10.45 - 11.30 Dosimetry issues in IMRT – Koen Tournel 11.30 - 12.00 TPS commissioning – M. Schwarz 12.00 – 12.45 IMRT optimization: algorithms and cost functions – Matthias Söhn

12.45 - 14.00 Lunch Chair: Koen Tournel

Clinical session 3 : local MD , Matthias Söhn – Prostate - LILLEHAMMER Room Group B: free

14.00 - 15.30 Group A: Clinical case discussion 1 (14.00-14.45) Clinical session 1 : Andrea Filippi , Koen Tournel Lymphoma - HARALD Room Clinical session 2 : local MD , Matthias Söhn – Prostate – STAVANGER Room Clinical session 3 : Frank Lohr , Giovanna Gagliardi– H&N - LILLEHAMMER Room Clinical case discussion 2 (14.50-15.30) Clinical session 1 : local MD , Matthias Söhn – Prostate - HARALD Room Clinical session 2 : Frank Lohr , Giovanna Gagliardi – H&N - STAVANGER Room Clinical session 3 : Andrea Filippi , Koen Tournel Lymphoma - LILLEHAMMER Room Group B: Vendor session Chair of the session: Marco Schwarz 15.30 - 16.00 Coffee break 16.00 – 16.45 Group A: Clinical case discussion 3 Clinical session 1 : Lymphoma Frank Lohr , Giovanna Gagliardi – H&N - HARALD Room Clinical session 2 : Andrea Filippi , Koen Tournel Lymphoma - STAVANGER Room

Wednesday 7 Oct Chair: Frank Lohr 9.00 - 09.45 Practical IMRT planning and ‘biological optimization’ – Marco Schwarz 9.45 - 10.30 Impact of geometrical uncertainties on IMRT dose distributions – Koen Tournel 10.30 - 11.00 Coffee break 11.00 - 11.45 Review of Dose-volume relationships II: Pelvis – Giovanna Gagliardi 11.45 – 12.30 IMRT of prostate cancer – F. Lohr 12.30-14.00 Lunch 14.00-15.30 Group B: Clinical case discussion 1 (14.00-14.45) Clinical session 1 : Andrea Filippi , Koen Tournel Lymphoma - HARALD Room Clinical session 2 : local MD , Matthias Söhn – Prostate – STAVANGER Room Clinical session 3 : Frank Lohr , Giovanna Gagliardi– H&N - LILLEHAMMER Room

Thursday 8 October Chair: Andrea Filippi 9.00 - 9.45 Dose calculations in static and rotational IMRT - Matthias Söhn 9.45 - 10.30 Potential and limitations of rotational IMRT – Koen Tournel 10.30-11.00 Coffee break 11.00 - 11.45 Highly conformal techniques in early stage lung cancer: indications, techniques, normal tissue constraints, results – Andrea Filippi 11.45 - 12.30 Highly conformal techniques in advanced stage lung cancer: indications, techniques, normal tissue constraints, results – Andrea Filippi 12.30 -13.00 Final discussion and closing of the course

Clinical case discussion 2 (14.50-15.30) Clinical session 1 : local MD , Matthias Söhn – Prostate - HARALD Room Clinical session 2 : Frank Lohr , Giovanna Gagliardi – H&N - STAVANGER Room Clinical session 3 : Andrea Filippi , Koen Tournel Lymphoma - LILLEHAMMER Room Group A: Vendor session / Chair of the session: Marco Schwarz 15.30-16.00 Coffee break 16.00 – 16.45 Group B: Clinical case discussion 3 Clinical session 1 : Lymphoma Frank Lohr , Giovanna Gagliardi – H&N - HARALD Room Clinical session 2 : Andrea Filippi , Koen Tournel Lymphoma - STAVANGER Room Clinical session 3 : local MD , Matthias Söhn – Prostate - LILLEHAMMER Room Group A: free

Faculty

Marco Schwarz

Protontherapy Centre Trento, Italy marco.schwarz@apss.tn.it University Medical Centre Mannheim, Germany f.lohr@gmx.de

Frank Lohr

Andrea Riccardo Filippi AOU Città della Salute e della Scienza Turin, Italy afilippi@unito.it

Giovanna Gagliardi

Karolinska University Hospital Stockholm, Sweden giovanna.gagliardi@karolinska.se

Matthias Söhn

LMU University Hospital Munich, Germany Matthias.Soehn@med.uni- muenchen.de UZ Brussel (VUB) Brussels, Belgium koen.tournel@uzbrussel.be

Koen Tournel

Welcome to Brussels Brussel/Bruxelles

NOT dr.Prof Mark De Ridder, head of department Koen Tournel, Medical Physicist

A rich history….

Bruocsella

est. 10 century AC

“Village by the swamp”

A rich history….

Pieter Brueghel the elder

Capital of Belgium

• 11.000.000 inhabitants • Official languages : Dutch (60%), French (39,3%), German (0,7%) (English widely spoken and understood) • Cities : Brussels, Antwerp, Liege, Gent, Namur, Brugge… Brussels: • 1.200.000 inhabitants • French (38%), Dutch (5%), Dutch and French ( 17%), French and others (23%), others (17%)

Language map of Belgium

Comm. of Flanders

Comm. of Flanders

Capital of Europe

Capital of surrealism

Rene Magritte 1898-1967

Belgium : country of surrealism

• Federal monarchy • 9 parliaments • 8 governments • 48 ministers + 10 secretaries of state • 10 provinces, 11 governors • 1 king, 2 queens

• world record holder in number of days without government : 541 • European and world champion in tax pressure on labor : 56% • Traffic jam capital of Europe

Belgium : country of surrealism

Sights and Sounds

The Atomium (expo 1958)

BCC Ferro crystal

Manneken Pis

Grote Markt / Grand Place

Mont des arts / kunstberg

Architecture

Galerie des Reines

Art nouveau

Home of Belgian beers….

“gueuze” or “kriek”

Home of Belgian chocolates

Home of gastronomy

UZ Brussel

• Academic Hospital of the Vrije Universiteit Brussel • connected to the medical faculty and the Erasmus school for life sciences • Only native Dutch-speaking hospital in Brussels (in practice multilingual) • 3500 employees

Oncology Center

Radiotherapy

Oncology

Onc. Surgery

1600 patients/year

7 Linacs – 2 locations

Aalst

Jette (Brussels)

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© M. De Ridder

April 2014

• 12 Radiation oncologists (3 in training) • 7 physicists/2 dosimetrists • 5 engineers for linac maintenance • 25 nurses/therapists • 1 logistics

Multi-vendor environment

• 2 Elekta • 1 Varian • 2 tomotherapy • 1 Mitsubishi/brainlab • Brainscan/iPlan/Xio/Monaco/Tomo/ Eclipse/Raysearch

• Vero RV/Aria/Mosaiq • SN/IBA/PTW/Ashland • MIM

Milestones

• 1994 : Stereotactic frame • 1998 : IMRT using the mimic • 2000 : 1st European Novalis • 2003 : Stereoscopic Xray positioning for prostate • 2005 : 2nd European Tomotherapy device • 2013 : Dynamic tracking

Research interests • Rectal cancer : RectumSIB trial -B.Engels • SBRT T1,2 Lung (tracking, ITV) • NSCLC T3,4 : C.Collen • SBRT of metastatic disease (R.Van Den Begin) • SRS Brain : AVM, frameless : T.Gevaert • Markerless tracking : J.Dhondt

Preoperative RT of rectal cancer using IMRT/IGRT at the UZ Brussel

Benedikt Engels, MD PhD Department of Radiotherapy UZ Brussel, Vrije Universiteit Brussel

ESTRO course on IMRT and other conformal techniques 2015 Oct 4-8, Brussels, Belgium

Introduction

 823 patients with stage II/III rectal cancer  Randomly assigned  Preoperative 28 x 1.8 Gy + 5FU  Postoperative 31 x 1.8 Gy + 5FU ( 5 FU: 120 h CI, 1000 mg/m 2/day , week 1 & 5) Sauer et al, N Eng J Med 2004

2

Local recurrence rate (update)

Sauer et al, J Clin Oncol 2012

3

Preoperative chemoRT or RT alone?

 EORTC 22921 (1) and FFCD 9203 (2) : preoperative 5-FU chemoRT superior over RT alone with respect to pCR and LC, but no difference in:  Overall survival

 Rate of sphincter sparing surgery  Occurrence of distant metastases

(1) Bosset et al., N Engl J Med 2006 (2) Gérard et al., J Clin Oncol 2006

Bosset et al, Lancet Oncol 2014

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Adverse effects of long-course chemoRT

 Radiation enteritis = primary acute/late side effect  German trial: preop chemoRT less toxic than postop (1)

 Acute grade ≥ 3 toxicity rate up to 5 times higher with the addition of 5-FU to preoperative RT as compared to preoperative RT alone (2)  Intensified chemotherapy + RT:

(1)Sauer et al., N Engl J Med 2004 (2)Gérard et al., J Clin Oncol 2006

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Efforts to improve outcome

 Preoperatively:  Induction chemotherapy prior to 5-FU chemoRT  Concurrent multi-agent 5-FU based chemoRT:

 Biologic agents (cetuximab/bevacizumab)

 Oxaliplatin: phase III evidence

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3D-Conformal RT: 3-field technique

postero-anterior beam (40% of the dose)

2 opposing latero-lateral beams (60% of the dose)

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3D-conformal RT vs IMRT

Wolff et al, R&O 2012

PTV Organ at risk

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+ Image-guided RT (IG-IMRT)

Planning CT CT prior to treatment co-registration => the dose distribution is delivered at the exact location within the patient by image guidance

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UZ Brussel approach

 Alternative strategy UZ Brussel: IG-IMRT + simultaneous integrated boost (SIB) by helical tomotherapy

 To decrease the toxicity  by reducing the irradiated volumes of small bowel and bladder by IG-IMRT  by omitting concomitant 5-FU chemotherapy  To maintain the oncological safety  by delivery of a simultaneous integrated boost to bad T3 (CRM ≤ 2mm) and T4 tumors

 Phase II Study: primary endpoint 2-year local control

 ≤ 3/100 patients with local failure

De Ridder and Engels et al, Int J Radiat Oncol Biol Phys and Radiother Oncol 2008 - 2014

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Phase II study 2005 – 2010

 108 patients with cT3-4 rectal cancer treated preoperatively

 Radiotherapy (RT): 23 x 2 Gy with IG-IMRT by helical tomotherapy with daily MVCT scan positioning and without concurrent chemotherapy

 SIB of 0.4 Gy/day on the primary tumor up to a total dose of 55.2 Gy for patients with a narrow CRM on MRI ( ≤ 2 mm) to maintain oncological safety

Radiotherapy

follow-up

Late toxicity Outcome

adjuvant chemotherapy

5-6 weeks

5 weeks

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Dose-volume constraints for IMRT: small bowel  Baglan et al. (n=40, 3D-CRT)  V15 < 150cc: no grade 3+ acute GI toxicity  V15 > 150cc: 50% grade 3+ acute GI toxicity  Gunnlaugsson et al. (n=28, 3D-CRT)  V15 ≤ 150cc: 11% diarrhea  V15 > 150cc: 52% diarrhea  Tho et al. (n=41, 3D-CRT)  V5-V30 correlated with severity of diarrhea  Yang et al. (n=177, IMRT/3D-CRT)  V45 < 3%: no grade 2+ diarrhea  V45 ≥ 27%: 20% grade 2+ diarrhea  Reis et al. (n=45, 3D-CRT)  V5 < 292cc: 29% grade 2-3 diarrhea  V5 > 292cc: 82% grade 2-3 diarrhea  QUANTEC (Marks LB et al.): V15 < 120cc (< 10% risk of severe acute GI toxicity)

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Dose-volume constraints for IMRT: bladder

 Less radiosensitive as compared to small bowel 

e.g. primary RT gynaecological/urological malignancies (often doses > 70Gy)

 Sauer et al: only 2% grade 3+ late GU toxicity  Appelt et al. (n=345, preoperative long-course chemoRT):  first report on dose-volume relationship for acute urinary toxicity in rectal cancer

 No clinically significant benefit is to be expected from IMRT with regard to GU toxicity

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Dose-volume constraints for IMRT: pelvic bone + plexus

 Baxter et al: 

Increased risk of pelvic fractures in elderly women  Holm et al (follow-up data Stockholm trials):   No reports on dose-response relationship:  max 45-50 Gy

5.3% femoral neck/pelvic fractures + hospitalization (vs 2.4% no RT)

 Sacral insufficiency fractures:  Rare but significant morbidity  Incidence: 3-7% 

Independent risk factors: osteoporosis, female gender, age > 60 years  No data on dose-response relationship  Lumbosacral plexus:  Tunio et al (cervical cancer) 8% grade 2 or more plexopathy  Prospective studies in rectal cancer are warranted

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Dose-volume constraints for IMRT: bone marrow  40% of total body bone marrow reserves located in pelvis:  up to 8% hematological toxicity with preop chemoRT  Mell et al (chemoRT anal cancer):  V10-20 significantly correlated with hematological toxicty  = low-dose treshold > myelosuppressive chemotherapy  Dosimetric benefit of IMRT (Mell et al, cervical cancer):  Reduction of lumbosacral BM irradiation all dose levels  Reduction of pelvic BM irradiation to high doses  Yang et al (rectal cancer):  Sacral BM: V45 < 51%  Coxal BM: V45 < 13%  Higher dose treshold (vs anal cancer)

15

Proposed dose-volume constraints IMRT rectal cancer

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IG-IMRT by helical tomotherapy with a simultaneous integrated boost

SIB

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Acute toxicity

Only 1% grade ≥ 3 acute toxicity

According to the NCI CTC AE v 3.0 scale

De Ridder and Engels et al, Int J Radiat Oncol Biol Phys and Radiother Oncol 2008 - 2014

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Surgical characteristics and downstaging

8% pCR rate 40% of cT3-4 was downstaged to ypT0-2

De Ridder and Engels et al, Int J Radiat Oncol Biol Phys and Radiother Oncol 2008 - 2014

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Late toxicity

According to the NCI CTC AE v 3.0 scale

9% grade ≥ 3 late gastrointestinal toxicity 4% grade ≥ 3 late urinary toxicity 13% any grade ≥ 3 late toxicity

De Ridder and Engels et al, Int J Radiat Oncol Biol Phys and Radiother Oncol 2008 - 2014

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Follow-up (median 54 months; range: 27-79 months)

3 locoregional relapses

MVA: R1 resection (p=0.03) ypN2 disease (p=0.04) UVA: adjuvant chemotherapy (p=0.04)

5-year: 97% LC 57% PFS 68% OS

MVA: R1 resection (p=0.03) ypN2 disease (p=0.04) UVA: adjuvant chemotherapy (p=0.04) ypT3-4 tumor (p=0.01) Dworak grade 0-2 (p=0.03)

De Ridder and Engels et al, Int J Radiat Oncol Biol Phys and Radiother Oncol 2008 - 2014

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2010: Multicentric randomized trial (NCT 01224392)

 Preoperative IG-IMRT with a simultaneous integrated boost (SIB) compared to chemoradiotherapy for T3-4 rectal cancer

Collaborating Centres  National Cancer Institute Aviano, Italy  IRCC Candiolo, Italy  IRCCS San Martino-IST Genoa, Italy  Institute of Oncology Vilnius University, Lithuania  UZ Brussel, Belgium (PI)  University of Torino, Italy  Nantes, France (2014)

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Study design

cT3-4 rectal cancer

Arm 2: RT-boost

Arm 1: chemoRT

IG-IMRT 23 x 2 Gy + capecitabine (825mg/m 2 )

IG-IMRT 23 x 2 Gy + SIB 0.4 Gy/day ( Σ 55.2 Gy)

TME surgery 6 weeks post RT + adjuvant capecitabine (x 6)

 Primary endpoint: reduction in metabolic tumor activity  SUV max on sequential 18FDG-PET imaging  Non-inferiority: difference in metabolic response ≤ 10%  Sample size: 78 in both arms ( α : 0.05, power: 80%)

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Patient population (n = 169)

25

Acute toxicity

26

Surgical parameters

75%

68%

27

Pathology

49%

45%

51%

60%

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Primary endpoint

 Mean decrease in SUV max on 18FDG-PET 5 weeks after completion of preoperative RT as compared to baseline:

 Difference: -2.9% (95% CI, -10.1% to 4.3%)

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Outcome (median follow-up 14 months)

2-y 86% vs 82%

2-y 75% vs 82%

2-y 93% vs 98%

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compared to chemoRT for T3-4 rectal cancer: a multicentric randomized trial

Conclusions:

 The use of image-guided and intensity-modulated radiotherapy (IG-IMRT) results in very low rates of acute grade 3 toxicity in both arms (6% vs 4%)

 IMRT improves significantly the tolerance of preoperative RT for rectal cancer, especially radiation enteritis

 Higher pCR rates are observed in the chemo-RT arm (24% vs 14% in the RT-SIB arm), no differences in major tumoral downstaging

 Difference in SUVmax reduction -2.9% in favor of chemoRT (95% CI, -10.1% to 4.3%, p = 0.06) => RT-SIB marginally failed to prove non-inferiority to chemoRT

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Acknowledgements

Antonino De Paoli (Aviano), Gabriella Cattari (Candiolo), Fernando Munoz (Torino), Stefano Vagge (Genova), Darius Norkus (Lithuania), Gianna Tabaro (Aviano), Harijati Versmessen (Brussels), Mark De Ridder (Brussels), …

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SBRT in UZ Brussel

Thierry Gevaert, PhD Radiotherapy, UZ Brussel

The VERO System

Gimbaled linac tilt/pan ampl.: ± 4.4 cm (at iso)

Dual O-ring Gantry rotation Horizontal axis ± 185°

Vertical axis: : ± 60°

2

Nicely flattened 6MV beam

MLC leaves : 60 x 5 mm single focus 50 mm/s leaf speed Max. field size : 15 x 15 cm

Transversal profiles @ 10cm depth

Diagonal profiles @ 10cm depth

The VERO positioning system

è Dual orthogonal kV X-ray system:

ExacTrac IR marker pre-positioning device

Stereoscopic X-rays (Imaging size : 15.89 x 21.18 cm) kV cone-beam CT imaging in 200°, FOV ∅ 20 x 15 cm

l

l

MV

kV 1

kV 2

EPID MV portal imaging (0.2 mm pixel size) FPD 1 FPD 2

Fluoroscopy imaging for tracking (15 fr/sec)

Novalis Body 6DOF postioning

FPD 2

FPD 1

4

Image guidance accuracy

“ Hidden-target test on anthropomorphic phantom, pelvic region ”

kV planar, kV CBCT imaging

iso 2mm BB in isocenter

Plan 30x30mm open fields

Treatment plan delivery

Phantom positionning

EPID Image analysis

-EPID images (0.2mm pixels) -Automatic detection of field outline (Hough transform) and BB (Kernel based) -Detection estimated accuracy 0.1 mm

Image guidance accuracy

“ Hidden-target test on anthropomorphic phantom, pelvic region ”

kV 0°-90° bony

kV 45°-135° bony

kV CBCT CW bony kV 0°-90° marker

X (LAT) 0.23 (0.10) mm 0.08 (0.18) mm -0.63 (0.04) mm 0.17 (0.06) mm -0.18 (0.09) mm -0.20 (0.05) mm -0.08 (0.11) mm -0.18 (0.03) mm -0.13 (0.04) mm -0.58 (0.16) mm 0.32 (0.27) mm -0.71 (0.03) mm 3D VECTOR modulus 0.62 mm 0.67 mm 0.71 mm 0.75 mm Y (LONG) Z (VERT)

O-ring stability

BrainLab/MHI Vero

Elekta Infinity

BrainLab/Varian Novalis

Elekta Compact

Varian Truebeam

Tomotherapy Hi Art

Brussel, Aalst, BE

Munich, GE

Zurich, CH

Milano, IT Como, IT

Dallas, TX

USA

Europe

Phys. Med. Biol. 57 (2012) 2997–3011)

O-ring stability

è “ visual ” inspection of star shot film è Quality indicated by multi-axial symmetry of the star pattern l Radiosensitive film placed in plane of rotations l Sequence of narrow fields at different angles l Intersection of these fields forms a star-shaped pattern

Central “ Star ” pattern

Depuydt et al. 2012 (Phys. Med. Biol. 57 (2012) 2997–3011)

8

O-ring stability

Quality indicated by radius of smallest intersecting circle

1 Digitization of film 2 Detection of beam axis 3 Representation of beam axis as linear equations 4 Calculate smallest intersecting circle radius

R

Depuydt et al. 2012 (Phys. Med. Biol. 57 (2012) 2997–3011)

O-ring stability

Collimator rotation

Gantry rotation

Vero

Tomotherapy

Truebeam

Infinity

Couch rotation

O-ring rotation

Gantry Wobble

Truebeam

Vero

Vero

Novalis

All fields collimated with MLC

Phys. Med. Biol. 57 (2012) 2997–3011)

O-ring stability

- Best O-ring and best C-arm system show comparable results ...

Depuydt et al. 2012 (Phys. Med. Biol. 57 (2012) 2997–3011)

iPlan treatment techniques

TECHNIQUES IN DEVELOPMENT??

Multiple Modality Treatment Delivery

CONFORMAL BEAM

INVERS ARC

DYNAMIC CONFORMAL ARC

IMRT

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Accomodation moving tumors l 4D CT: respiratory correlation, motion measurement

ITV GTV

13

Reliability 4D CT

è Repeated 4D CT before treatment planning: l Four 4D CT in ten minutes interval (Guckenberger IJROBP ‘07)

Ø No systematic changes of motion pattern Ø Increased variability for lower lobe tumors

l Two successive 4D CT (van der Geld radiat oncol ‘06) Ø Volume of the PTV not systematically different Ø Motion range variability < 2mm in 81 % Ø Coverage not compromised

No benefit of repeated 4D CT in one session

Reliability 4D CT

è Repeated 4D CT during treatment course: l Second 4D CT after > 2 fractions (Haasbeck IJROBP ‘07) Ø No systematic changes of motion pattern and PTV Ø Target coverage compromised in one patient (atelectasis) l Repeated 4D CBCT scans during RT (Sonke IJROBP ‘08) Ø Stable trajectory with variability (1SD) less than 1mm Ø Significant base-line shifts l Tumor tracking in EPID images (Richter IJROBP ’10) Ø Stable tumor trajectory, both intra- and inter fractional No benefit of replanning because of motion variability

Accomodation moving tumors

l Movement < 7mm : ITV concept

ITV GTV

l GTV contoured on 10 phase CT (propagation) = ITV

PTV = ITV + 5 mm

l

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Reliable day to day treatments: ITV

Planning CT

Vero CBCT

Cone beam CT positioning with ITV approach

PTV ITV

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Online Epid imaging

EPID%

ITV%

MLC%

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Accomodation moving tumors

l Movement > 7mm : tracking concept

ITV GTV

l Placement of internal marker + dynamic tumor tracking

Visicoil TM

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è Effectiveness of Tracking relies on a stable relationship between the marker and tumor l Changes in tumor geometry (long-course RT) l Migration between CT and radiation delivery (bronchofiberscopy)

è Ideal location Visicoil:

in the center of the lesion

l

l not in the same axial-CT image plane (e.g. 45 degree angle)

è Time interval between marker placement and CT for ‘scarring in’

è Lung and liver: percutaneous insertion under CT- fluoroscopic guidance

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Surrogate value: COM Single Visicoil marker vs. COM GTV Fiducial marker surrogate value for GTV position

“ Max deviation ”

Ex. 1

LAT

AP

CC

1.2 mm in CC

(CT slice 2 mm)

(x,y,z) COM , Visicoil =(x,y,z) COM,GTV +Cte

Ex. 2

LAT

AP

CC

+ Regular verification of marker surrogate value on CT imaging

Acitve versus passive approach

Active approach: Tracking approach Passive approach: ITV approach

Example ITV vs. Tracking approach

PTV definition: Tracking: CTV=GTV, PTV TR =CTV + 5mm isotropically ITV backup plan: ITV= sum CTV all phases + 5 mm isotropically (for CBCT guidance) PTV ITV =ITV+5mm isotropically PTV TR = 18.3 ccm , PTV ITV =30.2 ccm (39% PTV volume reduction)

Patient History: Male, 74 years old: 7/2009: primary disease: cT4N3M0, treated induction chemo , consolidation RT 8/2010: metastatic disease: Tarceva 5/2012: progression of solitary metastasis lower left lobe , RT 2x20 Gy Delineation: On 60% phase in stable exhale ( volume 4.30 ccm ) Size: AP: 2.6 cm, CC: 2.2 cm, LR: 2.2 cm Motion: Visicoil marker 0.75 mm diameter, 10 mm length Amplitude CC of 14mm p2p in 4D CT

Goal of dynamic tracking as compared to the ITV approach

1) Reduction of volume receiving high-doses (PTV 100cc vs PTV 50cc)

=> potential advantage in terms of NTCP still needs to be determined!

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Goal of dynamic tracking as compared to the ITV approach

DRIFT

2) Real-time adaptation of periodic breathing motion and systematic drifts in patients with a variable and unpredictable magnitude of motion ( lower lobe tumors and patients with poor pulmonary function*)

*Guckenberger et al, IJROBP 2007

3) Increased efficiency of respiratory correlated treatments (as compared to gating)

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Translation tracking versus BEV tracking

Accuracy CyberKnife

BrainLab/MHI Vero

XYZ Translation Tracking

Pan/Tilt Rotation Beams-eye-view Tracking

Behavior symmetry of Pan/Tilt, tracking/MLC decoupling

Gimbals Tracking

DMLC Tracking

Motion

MLC

Moving No tracking

Not Moving No tracking

Moving Tracking

EPID images (3fps)

Courtesy Andreas Krauß, DKFZ

Dynamic tracking concept

29

Tumor with implanted visicoil marker

Moving infrared marker on skin (surrogate)

“Mathema#cal model to predict mo#on of the on the basis of the moving infrared on skin”

Pa#ent

X-­‐ray images

Internal moving tumor

Workflow dynamic tracking

1. X-ray guided setup based on bony landmarks CBCT s ft tissue matching

Patient Positioning

Acquiring breathing signal

20-40 sec kV fluoro sequence + infra- red marker motion

Visicoil detection + building correlation model

VERO BREATH-HOLD CONE BEAM CT

kV imaging monitoring

kV imaging monitoring

Beam on

31

Treatment time aspects

patient setup

modelling Treatment delivery

modelling

Treatment delivery

...

modelling

Treatment delivery

Average breathing amplitude [mm]

Netto treatment time

Time in room MIN

Time in room AVERAGE

Time in room MAX

Building of Cor. Model

Usage of Cor. Model

Site

2m 59s 5m 59s 20m 58s 34m 31s 34m 38s 34m 44s 3m 3s 5m 28s 14m 29s 19m 9s 22m 41s 37m 44s 2m 23s 8m 48s 20m 0s 32m 12s 33m 49s 36m 15s

Patient 1 lung (17Gy/ fr)

10.8

lung (5Gy/fr)

Patient 2

6.8

Patient 7 lung (12Gy/ fr)

23.7

2m 50s 6m 24s 18m 49s

31m 26s

Average

15.3

Dynamic tracking new version

Analyze of deviation between predictive and real time position marker Based on these information, update of correlation model

33

Updating correlation model

è Investigation of potential benefit of updating the Vero correlation model using X-ray verification images during real-time tumor tracking: è Gain in time!! l 30% reduction in overall treatment time l 5.5 min. ± 4 min. è Occurred in 80% of fractions

Poels et al.

34

EBT3 film Sinusoidal tumor motion : Tracking for different bpm

25 bpm

15 bpm

static

“ The 20%-80% isodose distance was not significant increased for the 15 bpm, and only 0.2 mm for the 25 bpm signal. ”

Tracking for tumor motion from patients

CTV-PTV margin calculation

Prediction error tolerance level of 3 mm

σ = 1.5 mm (dose blurring) Σ= 1.5 mm (shift)

3 mm

3 mm

1.5 mm

R=3 mm

rebuild CM

Mechanical tracking errors

Penumbra: σ p =4.05mm β=0.73 (for 80% isodose)

marker-TV surrogate uncertainty

Gimbals systematic error

+

Correlation model Fit errors ( σ = 1 mm)

σ = 0.5 mm

Σ=CT-slice/2=1 mm

Σ= 0.4 mm

M=2.5*√(( 1mm ) 2 +( 1.5mm ) 2 +( 0.4mm ) 2 )+0.73*√(( 1.5mm ) 2 +( 0.5mm ) 2 +( 1mm ) 2 +(4.05mm) 2 )-0.73*4.05mm

-surrogate vs TV relative rotation in “ relative ITV ”

Based on Van Herk et al. 2000

CTV-PTV margin calculation

Prediction error tolerance level of 3 mm

σ = 1.5 mm (dose blurring) Σ= 1.5 mm (shift)

3 mm

3 mm

1.5 mm

R=3 mm

rebuild CM

Mechanical tracking errors

Penumbra: σ p =4.05mm β=0.73 (for 80% isodose)

marker-TV surrogate uncertainty

Gimbals systematic error

+

Correlation model Fit errors ( σ = 1 mm)

σ = 0.5 mm

Σ=CT-slice/2=1 mm

Σ= 0.4 mm

M=2.5*√(( 1mm ) 2 +( 1.5mm ) 2 +( 0.4mm ) 2 )+0.73*√(( 1.5mm ) 2 +( 0.5mm ) 2 +( 1mm ) 2 +(4.05mm) 2 )-0.73*4.05mm =4.9 mm => 5 mm

Based on Van Herk et al. 2000

Patient specific intra/post-fraction QA

Gimbals position logging

“Redundant sources of tracking performance information”

Per fraction QA through combination of different information sources

Vero Tracking

kV Monitoring Imaging

EPID MV Imaging

Poels et al.

Patient specific intra/post-fraction QA

Poels et al.

40

Patient specific intra/post-fraction QA Beams-Eye-View Tracking error

Prob. [%] BEV Tracking error< 5mm

Average breathing amplitude [mm]

Site

99%

Patient 1

lung (3x18Gy/fr) lung (10x5Gy/fr) liver(10x5Gy/fr) liver (10x5Gy/fr) liver (10x5Gy/fr) lung (10x5Gy/fr)

10.8

100%

Patient 2

6.8

97%

Patient 3

11.5

100% 100%

Patient 4

6.3

Patient 5

14.1

93%

Patient 6

19.7

100%

Patient 7

lung (4x12Gy/fr)

23.7

93% 98%

Patient 8

lung (4x12Gy/fr)

17.9

Average

13.9

Poels et al, Radiother Oncol 2013

Impact of motion management

VERO SBRT Tracking

Korreman et al, Int J Radiat Oncol Biol Phys 2012

42

Conclusion

è Depending on tumor location, we have to correct for tumor motion è Different treatment strategies l Passive ITV or mid ventilation approach o All cases l Gating / Tracking o Fewer amount of patients will benefit of this approach o Depending on philosophy of department, tumor location

43

Conclusion

è Designer machines: Gadget or useful tool? l Latest machine incorporate the knowledge of the past l More robust way of treating patients

o Online verification on board o Patient specific treatment

44

Treatment strategy UZB

4D-CT

< 7 mm => PTV = ITV + 5 mm* ITV approach ≥ 7 mm => internal marker if no contra-indication PTV = GTV + 5mm Dynamic tracking •lesions < 1cm: 8mm PTV margin •lesions < 1cm: no Tracking

Courtesy of B. Engels, MD PhD

45

Acknowledgments

46

Motion compensation techniques

Classic

Motion encompassing (passive)

Active compensation

Coventional free-breathing

ITV

Mid-position

Gated at exhale

Tracking

Max. exhale

Time-weighted average position

Max. inhale

Courtesy of Wolfhaus et al IJROBP 2008

47

Motion compensation techniques

Prescription isodose

ITV

4D

è The radiation beam does not necessarily need encompass the complete breathing amplitude l Broad beam penumbra in the lung tissue

Time spend at edges of “ITV” is short

l

l Dose loss at edges can be compensated for by higher doses at the centre

Radiother Oncol. 2011 Mar;98(3):317-22

A moving treatment beam

Medical linac full beam line

“ What parts of the beam line should move to create a moving beam? ” Dynamics of breathing/tracking: -Frequencies up to 30 Hz -Amplitudes of a few centimeters -Sub-milimeter accuracy Too heavy !!! (>>1000kg)

Electron Gun

RF Power

Accelerator

Target Primary collimator

Flattening filter

Jaws (X,Y)

“ Loose some of that weight ” -by compact design? -by omitting some heavy components?

MLC

A moving treatment beam… Robot

Medical linac “ reduced ” beam line

Accuray CyberKnife -Light and compact linac -Mounted on an robot ” -Both rotation and translations

Electron Gun

RF Power

Accelerator

Target Primary collimator

Cones or Circular Diaphragm

A moving treatment beam

Medical linac full beam line

“ What parts of the beam line should move to create a moving beam? ” Dynamics of breathing/tracking: -Frequencies up to 30 Hz -Amplitudes of a few centimeters -Sub-milimeter accuracy Too heavy !!! (>>1000kg)

Electron Gun

RF Power

Accelerator

Target Primary collimator

Flattening filter

Jaws (X,Y)

“ Loose some of that weight ” -by compact design? -by omitting some heavy components?

MLC

A moving treatment beam … Gimbaled Linac

Keeping the MLC/FF = Still very heavy (700kg)

Vero “ reduced ” beam line

Electron Gun

RF Power

Astronaut training: “ the gimbals chair ”

Accelerator

Target Primary collimator

Flattening filter

-Allows rotation of the linac/MLC assembly around the “ Center of mass ” -Only 2 DOF dynamic ( Pan/Tilt rotation ) -MLC and flattening filter remain

MLC

Conclusion

Linac

“ Safety margins incorporating motion ”

“ Gating ”

Linac

“ Exposure of large volumes of healthy tissue ”

-static beam -static couch -small beam -20-30% duty cycle “ Very long treatment ti es (duty cycle 20-30%) ”

-static beam -static couch -wide beam -100% duty cycle

Linac

Linac

“ Dynamic couch compensation ”

“ Tracking/Pusuit ”

-static beam “ Some parts of the achine have to move actively, responding real-time to tumor motion for counteracting or pursuit ” -dynamic couch -small beam ->90% duty cycle -dynamic beam -static couch -small beam ->90% duty cycle

Patient case: bilateral kidney

l 10x5 Gy to PTV with boost 6.25Gy l Right kidney: Tracking approach l Left kidney: ITV approach l Active part kidney: V15

54

Patient case: bilateral kidney

l Right kidney: 8 non-coplanar beams l Left kidney: 7 non-coplanar beams

Patient case: bilateral kidney

l Right kidney: 8 non-coplanar beams l Left kidney: 7 non-coplanar beams

Patient case: bilateral kidney

IMRT beam

Conformal beam

57

Patient case: bilateral kidney

Conformal beam: dashed line IMRT beam: solid line

58

Patient case: bilateral kidney

IMRT beam

Conformal beam

Tracking or ITV approach

59

Treatment of oligometastases using SBRT/IMRT/IGRT

Dr. Robbe Van den Begin

Department of Radiotherapy UZ Brussel, Vrije Universiteit Brussel (VUB), Brussels, Belgium

1. SBRT and oligometastatic disease

Stereotactic Body Radiation Therapy

 External beam radiation therapy  very precise  high dose of radiation  extracranial target  using either a single dose or a small number of fractions  AAPM: conformation of high doses to the target and rapid fall-off doses away from the target is critical. ’

ASTRO & ACR Practice Guidelines, Int J Radiat Oncol Biol Phys, 76 (2010) SBRT: the report of AAPM Task Group 101, Med Phys, 37 (8) (2010)

27-1-2016

Oligometastatic disease

 ‘ Oligometastases ’ state = disease state between locoregionally confined and widely spread metastatic cancer  de novo → metachronic  induced? → synchronic  Long-term survival after metastasectomy  Non-surgical local “ ablative ” therapy:  radiofrequency ablation (RFA)  SBRT  Selection of patients

Hellman and Weichselbaum. JCO 1995

4

27-1-2016

Oligometastases: A distinct disease entity at the clinical level

Lussier and Weichselbaum et al, Plos One 2012

10

27-1-2016

Stereotactic radiotherapy for oligometastases: a prognostic model for survival

 Aim: to identify subsets of patients that benefit in terms of overall survival  2005 – 2011: 309 patients ≤ 5 mets  SBRT (n = 209) or SRS (n = 107)  Median delivered BED = 60 Gy (range: 26 – 112 Gy)

 Median follow-up = 12 months (range: 1 – 84 months)

De Vin et al, Ann Oncol 2014

11

27-1-2016

Overall Survival

De Vin et al, Ann Oncol 2014

12

27-1-2016

Patient-inherent risk factors associated with impaired OS

De Vin et al, Ann Oncol 2014

14

27-1-2016

Risk factor analysis

- Non-adenocarcinoma - Intracranial - Synchronous - Male

Good prognosis  ≤ 2 risk factors

 Median survival time of 23-40 months

Bad prognosis

 3 and 4 risk factors  Median survival time of 4-9 months

De Vin et al, Ann Oncol 2014

15

27-1-2016

Patient non-inherent risk factors associated with impaired OS

 BED < 75 Gy vs ≥ 75 Gy

De Vin et al, Ann Oncol 2014

16

27-1-2016

Impact of SBRT on overall survival as compared to standard of care?

SABR-COMET, Palma et al, BMC Cancer 2012

17

27-1-2016

2. Helical Tomotherapy IMRT for oligometastatic disease: analysis of recurrences

Helical tomotherapy for oligometastatic cancer: UZ Brussel experience

 Inoperable CRC patients with ≤ 5 metastases

 Radiotherapy (RT): • 40 to 50 Gy (homogeneous) in 10 fractions • Tomotherapy Hi-Art System with daily MV-CT positioning

 Primary endpoint: metabolic complete response rate by comparing baseline FDG-PET with FDG-PET 3 months after start of RT

Engels et al., Ann Oncol 2010, Radiat Oncol 2012

19

27-1-2016

Helical tomotherapy for oligometastatic CRC: UZ Brussel experience

 40-50 Gy in 2 weeks =>

median survival > 2 years after RT.

 Grade 3 toxicity < 5%  1-year local control of only 54%:  Geographical miss (no respiratory motion

n = 105

management, only free- breathing planning CT)

 BED < 100 Gy

Engels et al., Ann Oncol 2010, Radiat Oncol 2012

20

Cause of local failure after SBRT

 Modeling local recurrences:  within GTV: ‘ in-field ’ => insufficient dose  near GTV border: ‘ marginal ’

=> positioning error

Van den Begin et al, Radiother Oncol 2014

21

Patterns of local failure

In Field

Marginal

Lymph nodes (2/22)

0

2

Liver and lung (25/64) Other (3/19)

13

12

2

1

lymph nodes

liver/lung

(MVA p = 0.01)

Individual motion management + Dose escalation

Van den Begin et al, Radiother Oncol 2014

22

Tomotherapy for moving targets?

 Theoretical possibility of “ interplay effect ” when using IMRT for treatments with few fractions = Interplay between tumor motion and leaf opening  Scanning motion of Tomotherapy  Sterpin et al: very small effect on dose (coached patients)  Good resulting dose distribution when patients breathe regularly  Safe to keep in to account:  Large field width (2,5-5cm)  Low pitch  Low modulation factor

23

3. Phase II study of SBRT for oligometastatic cancer

Phase II study of Vero SBRT for oligometastatic cancer

1. Dose escalation:  10 x 5 Gy to 80% isodose line (on PTV)  Partial tumor boost: 100% isodose (62.5 Gy, BED 101.6 Gy) to at least 60% of the GTV (or ITV)  Monte Carlo dose calculation (convolution/superposition on Tomotherapy)

Virtual volume reduction

Boost volume

Modeled effect of boosting a fraction of the GTV (Deasy JO and Fowler JF)

25

2. Motion management

Classic

Motion encompassing

Active compensation

(passive)

UZ Brussel

UZ Brussel

Coventional free-breathing

Gated at exhale

Mid-position

Max. exhale

Time-weighted average position

Max. inhale

Real-time Tumor Tracking

Internal Target Volume (ITV)

26

27-1-2016

Treatment algorithm

• < 7 mm

• ≤ 3 metastases: ITV (Vero: PTV 5 mm)* • > 3 metastases: ITV

(Tomotherapy: PTV 8 mm)

• ≥ 7 mm: internal marker in met(s) with largest peak-to-peak: Dynamic Tracking Vero: PTV 5mm • 2-3 mets: other mets ITV Vero: PTV 5 mm)* • > 3 mets: other mets ITV (Tomotherapy: PTV 8 mm)

* lesions < 1cm: 8mm PTV margin

27

A. ITV-approach: 4D-CT

27-1-2016 Figures: M. Guckenberger

A. ITV-approach: contouring

27-1-2016

Case 1: 54 year old patient with lungmetastasis

2007: Primary sigmoid cancer 2010: lung + livermetastasis => chemotherapy 2011: resection liver + lungmetastasis 2011: RT 42 Gy (15x 2.8 Gy) thoracic wall 2012: lungmetastasis in right inferior lobe, referred for SBRT 10 x 5 Gy Motion: Amplitude CC of 4 mm in 4D CT

30

Daily cone beam CT positioning with ITV approach

PTV ITV

31

B. Dynamic Tumor tracking: Vero

Dual O-ring Gantry rotation horizontal axis

Gimbaled linac

vertical axis

Gimbaled linac for real time tracking

Rotational therapy

O-ring: geometric stability for non coplanar treatments

32

27-1-2016

The Vero positioning system

ExacTrack (IR marker tracking)

ExacTrac IR marker based positioning device Dual orthogonal kV X-ray system:

MV

kV 1

kV 2

=> X-rays and fluoroscopy => kV cone-beam CT imaging 

FPD 1

FPD 2

EPID MV

Novalis Body system 6D set-up correction

EPID: MV portal imaging

33

27-1-2016

Implantation of fiducial

27-1-2016

B. Dynamic Tumor tracking

35

Potential benefits of Dynamic Tracking

1. Reduction of volume receiving high-doses (35%)

Graphics: K. Poels

36

Potential benefits of Dynamic Tracking

DRIFT

2. Real-time adaptation of periodic breathing motion and systematic drifts in patients with a variable and unpredictable magnitude of motion: lower lobe tumors and patients with poor pulmonary function*

3. IGRT for liver tumors that are difficult to visualize on cone beam CT

4. Increased efficiency of respiratory correlated treatments compared to gating

Graphics: K. Poels

38

*Guckenberger et al, IJROBP 2007

Case 2: multiple-met tracking

67-year female: pT3N2cM1 coloncancer

chemotherapy

39

Case 2: 2 livermetastases

GTV PTV

colon

visicoil 1

visicoil 2

4D-CT

4D-CT

40

Volumetric imaging + Dynamic Tracking

Planning CT

colon

small bowel

VERO BREATH-HOLD CONEBEAM CT

43

Inter-fractional organ-at-risk motion

VERO BREATH-HOLD CONE BEAM CT

44

Patient population

Accrual: n = 87 metastases (in 44 patients) Age 64y ± 11y, KPS 60-100%  mostly colorectal cancer (n = 29 patients)  lung mets (n = 62), liver (n = 17), lymph nodes (n = 4), soft tissue (n = 4)  Median follow-up = 12 months

Treatment:

 60 mets with ITV concept (5 patients treated with Tomotherapy)  27 mets with a peak-to-peak motion > 7 mm: Vero dynamic tracking

Van den Begin et al, manuscript in preparation

45

Toxicity

Highest Grade 1

2

3

4

5

Acute

33% 9%

2%

-

-

Late

20% 7%

2%

-

2%

grade 3 acute nausea (n=1) grade 3 late pneumonitis (n=1) grade 5 late cholangitis (n=1)

NCI CTC AE v 4.0

Van den Begin et al, manuscript in preparation

46

Local control (median follow-up 12 months)

1-y LC 89%

2-y LC 78%

n = 87 mets

Van den Begin et al, manuscript in preparation

47

Local control ITV vs Tracking

1-y LC 90% 1-y LC 88%

Van den Begin et al, manuscript in preparation

48

Local control according to location

1-y LC 90% 1-y LC 88%

Van den Begin et al, manuscript in preparation

49

PFS and OS (n=44 patients)

1-y OS 97%

1-y PFS 21%

Van den Begin et al, manuscript in preparation

50

Conclusions: SBRT for oligometastases

 Excellent local control with 10-fraction SBRT using motion management

 Feasibility of

ITV-approach and Dynamic Tracking on the Vero machine

 Acceptable toxicity  Excellent overall survival  Future: analysis of PFS, treatment-free interval?

27-1-2016

Acknowledgements

Dr Benedikt Engels Prof. Mark De Ridder Prof. Dirk Verellen Prof. Tom Depuydt Kenneth Poels Thierry Gevaert Dr Christine Collen Dr Tessa de Vin

UZ Brussel Radiotherapy Team

53

Frameless radiosurgery

T. Gevaert, PhD Radiotherapy, UZ Brussel

Stereotaxy: principle

l Stereotactic:

g Stereos: rigid, fixed

g Taxis: ordering

g Rigid relation between an external system of 3D coordinates and the internal anatomy of the brain Invasive fixation of the stereotactic frame to the bone skull was considered to ensure sub-millimeter accuracy of surgery / radiotherapy

Horsley, Clarke and Mussen

2

Stereotactic radiosurgery: definition l Radiosurgery: g Single high ablative dose g Tightly conforming the target g Sparing the surrounding healthy tissues

3

Stereotactic radiosurgery: definition l Frame-based vs. frameless g When a stereotactic system of coordinates is used

for localization and positioning l External coordinates vs. anatomy

l Invasive vs. non-invasive g When patient is rigidly fixed to the stereotactic system using: l Invasive fixation vs. thermoplastic masks

4

Stereotactic radiosurgery: requirements l A dedicated system for treatment planning and delivery of radiation to the lesion

l Accurate targeting to reproduce the dose planning

l Immobilization technique to maintain accuracy

5

Invasive frame-based: targeting

l Originally defined by invasive head frame g Golden standard l Origin coordinates = center of head frame l Accurate determination of stereotactic coordinates of a target point g Usually center of the target volume

Figure 1: The invasive head frame fixation (frame-based) (left) and the mask immobilization (frameless approach) (right)

6

Finally, even with the technological advancements that enable a good dosimetrical

Made with