Plan quality ‐ RayStation

Transcription

2013‐11‐28
A deliverability comparison of equivalent dual‐
arc VMAT plans generated in two different TPSs
KRISTOFFER PETERSSON, MEDICINSK STRÅLNINGSFYSIK, LUND Plan quality ‐ RayStation
• Pareto fronts
1
2013‐11‐28
Pareto front evaluation‐ Method
Better
Objective OAR
TPS 1
TPS 2
Worse
Better
Objective Target
Worse
Dmean OAR
Area under the plan (AUP)
VPTV, <95%
2
2013‐11‐28
Dmean OAR
Δiy
• AUPi =∆ ∙ ∆
Δix
VPTV, <95%
Δiy
Dmean OAR
• AUPi =∆ ∙ ∆
Δix
VPTV, <95%
3
2013‐11‐28
Area under the plans (AUPs)
∆
∙∆
∆
∙∆
.. ∆
∙∆
Δny
Δ2y
Δ1y
Dmean OAR
• AUPs = ∑ AUPi = ∑
Δ1x
Δ2x
VPTV, <95%
Δnx
35
Eclipse
RayStation
25
15
0.0
25
Eclipse
RayStation
20
15
10
70
1.0
2.0
VPTV, D<95% (%)
3.0
4.0
60
Eclipse
55
RayStation
50
45
40
0.0
1.0
2.0
VPTV, D<95% (%)
3.0
4.0
35
25
0.0
1.0
2.0
VPTV, D<95% (%)
Eclipse
RayStation Wilcoxon
Eclipse
RayStation
Wilcoxon
Eclipse
H&N 1
76.1
89.2
p=0.36
144
110
p=0.04
RayStation
H&N 2
69.0
128
p<0.01
199
191
p=0.84
H&N 3
169
177
p=0.88
226
213
p=0.88
15
3.0
H&N 2 in RayStation
30
25
Eclipse
20
RayStation
15
10
0.0
70
H&N 3 in Eclipse
65
AUPs
H&N 1 in RayStation
45
35
H&N 2 in Eclipse
30
0.0
Dmean Parotis dx (Gy)
3.0
35
1.0
2.0
VPTV, D<95% (%)
H&N 1 in Eclipse
45
Pareto fronts
1.0
2.0
VPTV, D<95% (%)
3.0
4.0
H&N 3 in RayStation
65
60
55
Eclipse
50
RayStation
45
40
0.0
1.0
2.0
VPTV, D<95% (%)
3.0
4.0
4
2013‐11‐28
Pareto fronts
Eclipse
RayStation
25
15
0.0
30
25
Eclipse
RayStation
20
15
10
70
1.0
2.0
VPTV, D<95% (%)
3.0
4.0
60
Eclipse
55
RayStation
50
45
40
0.0
1.0
2.0
VPTV, D<95% (%)
3.0
35
Eclipse
RayStation
Gold
25
15
0.0
1.0
2.0
VPTV, D<95% (%)
3.0
H&N 2 in RayStation
30
25
Eclipse
20
RayStation
Gold
15
10
0.0
70
H&N 3 in Eclipse
65
H&N 1 in RayStation
45
35
H&N 2 in Eclipse
0.0
3.0
35
1.0
2.0
VPTV, D<95% (%)
35
H&N 1 in Eclipse
45
1.0
2.0
VPTV, D<95% (%)
3.0
4.0
H&N 3 in RayStation
65
60
Eclipse
55
RayStation
50
Gold
45
40
0.0
4.0
1.0
2.0
VPTV, D<95% (%)
3.0
4.0
Pareto fronts
Eclipse
10
RayStation
5
0
1.0
2.0
3.0
VPTV, D<95% (%)
4.0
5.0
Dmean Ren sin (Gy)
15
Eclipse
30
RayStation
25
20
0.0
2.0
4.0
VPTV, D<95% (%)
35
30
Eclipse
RayStation
25
20
15
0.0
2.0
4.0
VPTV, D<95% (%)
RayStation
5
0
Eclipse
6.0
1.0
2.0
3.0
VPTV, D<95% (%)
4.0
RayStation Wilcoxon
Abdomen 1
77.1
45.6
Abdomen 2
46.0
80.9
Abdomen 3
256
261
Eclipse
RayStation
Wilcoxon
p=0.44
118
71.8
p<0.01
p=0.05
83.7
87.4
p=0.84
p=0.38
254
260
p=0.21
5.0
Abdomen 2 in RayStation
35
Eclipse
30
RayStation
25
20
0.0
6.0
Abdomen 3 in Eclipse
40
Eclipse
10
40
Dmean Ren sin (Gy)
35
15
0.0
40
Dmean Ren sin (Gy)
20
0.0
Dmean Ren sin (Gy)
25
20
2.0
4.0
VPTV, D<95% (%)
6.0
40
Dmean Ren sin (Gy)
Dmean Ren sin (Gy)
25
AUPs
35
30
Eclipse
RayStation
25
20
15
0.0
2.0
4.0
VPTV, D<95% (%)
6.0
5
2013‐11‐28
Pareto fronts
Eclipse
10
RayStation
5
0
1.0
2.0
3.0
VPTV, D<95% (%)
4.0
5.0
Dmean Ren sin (Gy)
15
Eclipse
30
RayStation
25
20
0.0
2.0
4.0
VPTV, D<95% (%)
35
30
Eclipse
RayStation
25
20
15
0.0
5
0
2.0
4.0
VPTV, D<95% (%)
1.0
2.0
3.0
VPTV, D<95% (%)
4.0
5.0
35
Eclipse
RayStation
Gold
30
25
20
0.0
6.0
40
Eclipse
RayStation
Gold
10
0.0
Dmean Ren sin (Gy)
35
15
40
40
Dmean Ren sin (Gy)
20
0.0
Dmean Ren sin (Gy)
25
20
2.0
4.0
VPTV, D<95% (%)
6.0
40
Dmean Ren sin (Gy)
Dmean Ren sin (Gy)
25
35
Eclipse
RayStation
Gold
30
25
20
15
6.0
0.0
2.0
4.0
VPTV, D<95% (%)
6.0
Pareto fronts
25
Intracranial 1 in Eclipse
20
Eclipse
RayStation
15
10
0.0
0.5
1.0
1.5
Dmean Hemisphere dx(Gy)
25
Intracranial 1 in RayStation
20
RayStation
10
0.0
0.5
5
0
Dmean Hippocampus sin(Gy)
1.0
2.0
VPTV, D<95% (%)
3.0
DmeanCochlea dx (Gy)
Eclipse
RayStation
10
25
Eclipse
RayStation
20
15
10
1.0
2.0
VPTV, D<95% (%)
RayStation
p=0.21
25.3
18.8
p=0.26
p<0.01
164
114
p<0.01
123
142
p=0.71
10.7
14.3
Intracranial 2
16.4
104
Intracranial 3
15.0
78.1
p<0.01
Wilcoxon
1.5
3.0
4.0
15
Eclipse
10
RayStation
5
0
0.0
30
0.0
Eclipse
20
Dmean Cochlea dx (Gy)
30
1.0
RayStation Wilcoxon
VPTV, D<95% (%)
15
0.0
Eclipse
Intracranial 1
Eclipse
15
VPTV, D<95% (%)
20
AUPs
1.0
2.0
VPTV, D<95% (%)
3.0
25
Eclipse
20
RayStation
15
10
0.0
1.0
2.0
VPTV, D<95% (%)
3.0
4.0
6
2013‐11‐28
Pareto fronts
25
20
Eclipse
RayStation
15
10
0.0
0.5
1.0
1.5
25
20
Eclipse
RayStation
Gold
15
10
0.0
0.5
1.0
VPTV, D<95% (%)
VPTV, D<95% (%)
Eclipse
RayStation
10
5
0
0.0
30
1.0
2.0
VPTV, D<95% (%)
3.0
25
Eclipse
RayStation
20
15
10
0.0
1.0
2.0
VPTV, D<95% (%)
3.0
4.0
15
Eclipse
RayStation
Gold
10
5
0
0.0
30
1.5
20
DmeanCochlea dx (Gy)
15
Dmean Cochlea dx (Gy)
20
1.0
2.0
VPTV, D<95% (%)
3.0
25
Eclipse
RayStation
Gold
20
15
10
0.0
1.0
2.0
VPTV, D<95% (%)
3.0
4.0
Pareto fronts
Eclipse
RayStation
34
32
0.0
Dmean Small Intestine(Gy)
1.0
2.0
VPTV, D<95% (%)
3.0
4.0
43
42
Eclipse
RayStation
41
40
39
0.0
42
1.0
2.0
VPTV, D<95% (%)
3.0
4.0
Pelvis 3 in Eclipse
40
38
Eclipse
RayStation
36
34
32
0.0
1.0
2.0
VPTV, D<95% (%)
3.0
Pelvis 1 in RayStation
4.0
Eclipse
RayStation Wilcoxon
Eclipse
RayStation
Wilcoxon
67.8
63.2
p=0.47
38
Eclipse
36
RayStation
Pelvis 1
78.3
Pelvis 2
21.3
37.9
p=0.02
26.6
35.2
p=0.04
Pelvis 3
37.0
68.2
p=0.03
85.4
65.2
P<0.01
34
32
0.0
44
Pelvis 2 in Eclipse
36
38
44
40
Pelvis 1 in Eclipse
1.0
2.0
VPTV, D<95% (%)
3.0
4.0
70.8
p=0.41
43
42
Eclipse
RayStation
41
40
39
0.0
42
40
AUPs
1.0
2.0
VPTV, D<95% (%)
3.0
4.0
40
38
Eclipse
RayStation
36
34
32
0.0
1.0
2.0
VPTV, D<95% (%)
3.0
4.0
7
2013‐11‐28
Pareto fronts
RayStation
34
32
1.0
2.0
VPTV, D<95% (%)
3.0
4.0
Pelvis 2 in Eclipse
43
42
Eclipse
RayStation
41
40
39
0.0
42
1.0
2.0
VPTV, D<95% (%)
3.0
4.0
Eclipse
RayStation
34
32
0.0
1.0
2.0
VPTV, D<95% (%)
3.0
32
30
0.0
1.0 2.0 3.0 4.0
VPTV, D<95% (%)
4.0
5.0
6.0
43
42
Eclipse
RayStation
Gold
41
40
39
0.0
Pelvis 3 in Eclipse
36
Eclipse
RayStation
Gold
34
1.0
2.0
VPTV, D<95% (%)
42
40
38
36
44
0.0
38
Eclipse
36
44
40
Pelvis 1 in Eclipse
38
40
3.0
4.0
40
38
Eclipse
RayStation
Gold
36
34
32
30
0.0
1.0
2.0
VPTV, D<95% (%)
3.0
4.0
Plan quality ‐ RayStation
• Conclusions: Significant difference in plan quality
• In Eclipse
• RayStation fronts superior for:
• 1 Intracranial
• Eclipse fronts superior for:
•
•
•
•
1 H&N, 1 Abdomen, 1 Intracranial, 2 Pelvis
• In RayStation
• RayStation fronts superior for:
•
•
•
•
1 H&N 1 Abdomen, 1 Intracranial, 1 Pelvis
• Eclipse fronts superior for:
• 1 Pelvis
8
2013‐11‐28
Inledning ‐ Bakgrund
RaySearch Laboratories
• SharePlanTM
• Automatisk konvertering av tomoterapi‐dosplaner 
step‐and‐shoot IMRT planer (levereras på vanlig linac).
• Välfungerande men begränsat användningsområde.
Inledning ‐ Bakgrund
RaySearch Laboratories
• RayStation
Modul för “Fallback planning” • Vidareutveckling av SharePlan funktionen
• Automatisk konvertering av alla typer av dosplaner 
alla modaliteter som finns tillgängliga på en vanlig linac.
•
•
•
•
3D conformal radiation therapy (CRT) Step‐and‐shoot IMRT Sliding window IMRT VMAT
9
2013‐11‐28
Syfte
Kontrollera levererbarheten
• automatiskt genererade backup‐
planer skapade i RayStation.
• Kontrollera # MU i planerna
• Jämfört med motsvarande planer som skapats i Eclipse.
• Dual‐arc VMAT planer
• Kontrollera mot levererbarhet
• Jämfört med motsvarande planer som skapats i Eclipse.
• Korrelation?
10
2013‐11‐28
Metodik
152 st planer skapas i Eclipse
Automatiskt genererade backup‐planer skapas i RayStation
• 6MV
• Baseras på Eclipseplaner
• Dual‐arc VMAT
• 3 backup planer per Eclipseplan
• Pareto‐optimala
•
1 Pareto‐front per patientfall
• 12 Patient fall
•
•
•
•
3 H&N
3 hjärntumörer
3 buktumörer
3 tumörer i bäckenet
• Olika Target vs. OAR viktfaktorer
• 1000:1, 100:1, 10:1
• Samma inställningar/restriktioner
• Ex: •
•
•
•
Kollimatorvinkel: 30°
gantry kontrollpunktseparation: 2°
Beräkningsgrid: 2.5 x 2.5 x 2.5 mm3
Etc.
• 1 backup‐plan per Eclipseplan sparas
• Bäst plankvalité
Metodik
• 304 planer (152 Eclipse +152 RayStation)
• Levererade med en TrueBeam linac (Varian)
• Mätta med Delta4 system (ScandiDos AB)
11
2013‐11‐28
ΔDm
δ
y
Γ(rm,rc)
Dc,rc
δ(rm,rc)
rc
Δdm
rc-rm
Dm,rm
x
Metodik
Gamma analys
Krav:
• Dosdifferens 3%
• DTA 2 mm
Tröskelvärde 15%
Kliniskt acceptabel plan:
≥ 95 % godkända mätpunkter
Statistisk metod:
Wilcoxon signed‐rank test
12
2013‐11‐28
Resultat
Gamma‐analys
Andel godkända mätpunkter • Signifikant högre för RayStation planer jmf. Eclipse
• Wilcoxon, (p<0.001)
• 93.0%≤ Eclipse ≤ 100%, 98.6%≤ RayStation ≤ 100%
• 66/152 RayStation > Eclipse
7/152 RayStation < Eclipse
• Enbart 3 planer < 95%, ej kliniskt acceptabla.
# MU i planerna
• Signifikant fler MU i Eclipse planer jmf. motsvarande RayStation plan
• Wilcoxon, (p<0.001)
• I medel: 29%
# MU korrelerar med grad av levererbarhet (andel godkända mätpunkter)
Pearson product‐moment correlation method r = ‐0.77
p<0.001
Korrelation mellan # MU och grad av levererbarhet
Eclipse
Andel godkända mätpunkter[%]
100
RayStation
99
98
97
Pearson korrelation
r = ‐0.77
p < 0.001
96
95
94
93
92
0
500
1000
MU
1500
2000
13
2013‐11‐28
Två patientfall med lägre värden
Andel godkända mätpunkter[%]
99
98
97
96
95
94
93
r = ‐0.79
p < 0.001
92
Eclipse H&N 2
100
Andel godkända mätpunkter [%]
Eclipse
Abdomen 2
RayStation
Abdomen 2
100
RayStation H&N 2
99
98
97
96
95
94
r = ‐0.89
p < 0.001
93
92
500
600
700
800
MU
Eclipse Arc 1 av 2
900
1000
0
500
1000
MU
1500
2000
RayStation Arc 1 av 2
14
2013‐11‐28
Eclipse Arc 1 av 2
RayStation Arc 1 av 2
Diskussion – Plankvalité
Plankvalité har kontrollerats
• Pareto‐front utvärdering
• Jämförbar mellan systemen
• Signifikant skillnad för 5/12 fall
• RayStation‐front bättre för:
•
•
•
•
1 H&N 1 Buktumör 1 hjärntumör 1 tumör i bäckenet
• Eclipse‐front bättre för :
• 1 tumör i bäckenet
15
2013‐11‐28
Slutsats
• Signifikant högre levererbarhet för RayStation planer vs. Eclipse planer.
• Antal MU signifikant högre för Eclipse planer vs. RayStation planer (29% i medel).
• OBS! • Antalet MU i en plan korrelerade signifikant med dess grad av levererbarhet.
•
Enbart 3/304 planer var ej kliniskt acceptabla(< 95%) RayStation Manus
• Differences in plan quality for available treatment techniques:
• VMAT, • IMRT (SW and SS), • 3DCRT (non‐coplanar)
• Evaluation methods
• Objective value, • CGA
• Approach
• “Gold standard” plans created in TomoTherapy planning system the 12 cases
• Plans with the highest plan quality clinically available:
• Field width: 1.05 cm
• Pitch: 0.172
• Modulation factor: 5 • Backup plans created and evaluated in RayStation
16
2013‐11‐28
Objective values
After Backup generation
Optimized # iterations
1.00E+01
1.00E+01
1.00E+00
1.00E+00
1.00E‐01
1.00E‐01
1.00E‐02
1.00E‐02
1.00E‐03
1.00E‐03
1.00E‐04
1.00E‐04
1
2
3
4
3DCRT
5
SS‐IMRT
6
7
SW‐IMRT
8
9
10
11
1
12
2
3
4
3DCRT
Dual‐Arc
5
6
SS‐IMRT
7
8
SW‐IMRT
9
10
11
12
Dual‐Arc
After Backup generation
1.00E+01
1.00E+01
1.00E+00
1.00E+00
1.00E‐01
1.00E‐01
1.00E‐02
1.00E‐02
1.00E‐03
1.00E‐03
1.00E‐04
1.00E‐04
1
2
3
3DCRT
4
5
SS‐IMRT
6
7
SW‐IMRT
8
9
10
11
1
12
2
3
4
3DCRT
Dual‐Arc
5
6
SS‐IMRT
7
8
SW‐IMRT
9
10
11
12
Dual‐Arc
• After optimization (approximate
dose):
• No significant difference
between techniques
directly after Backup gen.
• If # iterations is optimized:
• VMAT quality
improves significantly
• VMAT significantly
superior to other
techniques
• SS‐IMRT significantly
superior to 3DCRT
• After final dose:
superior to SW‐IMRT
• If # iterations is optimized:
• VMAT quality
improves significantly
• VMAT significantly
superior to other
techniques
Objective values
• After optimization (approximate
dose):
• If ”Reduce OAR” is used:
• Plan quality improves
significantly for all available techniques
superior to VMAT
Direkt efter Backup‐skapandet
1.00E+01
1.00E+00
1.00E+00
1.00E‐01
1.00E‐01
1.00E‐02
1.00E‐02
1.00E‐03
1.00E‐03
1.00E‐04
1.00E‐04
1
2
3
3DCRT
• After final dose:
• If ”Reduce OAR” is used:
• No significant
improvement
• No significant
difference between
techniques
Reduce OAR
1.00E+01
4
5
SS‐IMRT
6
7
8
SW‐IMRT
9
10
11
12
1
2
Dual‐Arc
3
Direkt efter Backup‐skapandet
1.00E+01
1.00E+00
1.00E+00
1.00E‐01
1.00E‐01
1.00E‐02
1.00E‐02
1.00E‐03
1.00E‐03
1.00E‐04
1.00E‐04
2
3
3DCRT
4
5
SS‐IMRT
6
7
SW‐IMRT
8
9
5
6
7
SS‐IMRT
8
9
10
11
12
9
10
11
12
Dual‐Arc
Reduce OAR
1.00E+01
1
4
3DCRT
10
Dual‐Arc
11
12
1
2
3
4
3DCRT
5
6
SS‐IMRT
7
8
Dual‐Arc
17
2013‐11‐28
CGA‐ Method
• Inspired by VGA‐ Visual Grading Analysis
• Determine image quality (Radiology)
• Dual‐arc VMAT plans, 7‐beam SS‐IMRT, 7‐beam 3DCRT (non‐coplanar) plans
• Demonstrated for ROs (individually)
• Plans side‐by‐side
• Mimic ordinary clinical rounds
• Dose distributions
• DVHs
• ROI data
• Clinical assessment
• Identify clinical relevant differences between plans
CGA‐ Method
• ROs grade plans and motivate their opinion
•A
SS‐IMRT/3DCRT plan considerably better than the VMAT plan
•B
SS‐IMRT/3DCRT plan somewhat better than the VMAT plan
•C
SS‐IMRT/3DCRT plan as good as the VMAT plan
•D
VMAT plan somewhat better than the SS‐IMRT/3DCRT plan
•E
VMAT plan considerably better than the SS‐IMRT/3DCRT plan
18
2013‐11‐28
CGA‐ Results (so far!)
1.00E+01
1.00E+00
1.00E‐01
1.00E‐02
1.00E‐03
1.00E‐04
1
2
3
4
5
3DCRT
6
SS‐IMRT
7
8
9
10
11
12
Dual‐Arc
CGA‐ Results (so far!)
• Hot‐spots are not penalized enough in the optimization
• Problem for complex cases
• Problem for IMRT techniques 19
2013‐11‐28
20

Plan quality ‐ RayStation

Transcription

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