Brachytherapy for Prostate Cancer 2017
Slides of the course held in Brussels, Belgium - 29 June-1 July 2017
WELCOME TO ESTRO PROSTATE BRACHYTHERAPY IN BRUSSELS
ESTRO, Brussels Elena Giusti
Your teachers ……………..
• Peter Hoskin:
Mount Vernon, UK
• Bashar AlQaisieh:
Leeds
• Stefan Machtens:
Bergisch Gladbach,DE
• Carl Salembier:
Brussels, BE
• Frank Andre Siebert:
Kiel, DE
Our exhibitors
• Eckert and Ziegler • Nucletron • Varian
Age specific incidence rates UK 2009/11
Age-Standardised Incidence Rates, , UK, 1993-2011
Cancer incidence and mortality, males, Europe: 2010
IARC
http://www.cancerresearchuk.org/cancer-info/cancerstats/world/incidence/#By
Age standardised incidence and mortality rates Europe 1975-2011
Incidence
Mortality
Worldwide Age standardised incidence and mortality rates 2010
IAR
182,123 men in SEER database
• Peer review evidence based trees estimate:
RP: 24% (15-30) EBRT: 58% (54-64%) BT: 9.6% (6-17.9%)
• Actual utilisations rates:
RP: 13-44% EBRT: 43-56% BT: 1.8-10.9%
Lo w
Intermediate
High
Prostate Brachytherapy: Anatomy
S. Machtens
Director of the
Department of Urology and Paediatric Urology
Academic Teaching Hospital
Marien-Hospital Bergisch Gladbach
With Courtesy from Geert Villeirs UZ Gent
ESTRO Teaching Course on Brachytherapy for Prostate Cancer Brussels, June 29th-July 1st 2017
The Prostate
The prostate surrounds the urethra and is situated below the bladder.
The prostate produces fluid that is needed by sperms to move.
Ultrasound Normal Anatomy
CG
PZ
PZ
Isoechoic PZ Hypo/hyperechoic CG
Corpora Amylacea
Ultrasound Normal Anatomy
Urethra
Urethra Sagittal
Ultrasound Normal Anatomy
Seminal Vesicles Convoluted Hypoechoic Cystic Structures
Ultrasound Sagittal: urethral measurements
ULTRASOUND – Dorsal vein plexus
Zonal Anatomy Central Gland
Periurethral Glands (paracoronal view)
Periurethral Glands
Zonal Anatomy Central Gland
Transition Zone (transverse view)
Transition Zone
Zonal Anatomy Central Gland
Central Zone (paracoronal view)
Central Zone
Zonal Anatomy Overview
Peripheral Zone (paracoronal view)
Peripheral Zone
Zonal Anatomy Overview
Anterior Fibromuscular Stroma
AFS (paracoronal view)
Zonal anatomy in MRI and Ultrasound
Anatomy Prostate
CG
CG
PZ PZ
PZ
PZ
PZ
PZ
Prostatic Apex Midprostate Prostatic Base
Imaging of Prostate Cancer Body coil versus Endorectal coil
Normal Prostate with Body Coil
Normal Prostate with Endorectal Coil
1.5 Tesla MRI
MRI: • Resolution: good • Contrast: good, especially soft tissue contrast
Zentrale Zone
Periphere Zone
Tumor
1.5 T
T2-weigthed
T1-weighted
3.0 Tesla MRI
T1 weighted
T2 -weighted
3.0 Tesla MRI + Endorectal coil
Anatomy Hyperplasia
CG
CG
CG
PZ
PZ
Benign Prostatic Hyperplasia
Variation of bladder neck according to BPH
Anatomy Urethra
External Sphincter
Urethra
Sagittal
Coronal
Transverse
Platinum Slide Series
Transversal section of the prostatic apex. A considerable part of the urethral sphincter is located intraprostatically between the prostatic apex and the colliculus seminalis.SMS = smooth muscle sphincter; SS = striated sphincter (rhabdosphincter); CS = colliculus seminalis; PA = prostatic apex.
Thorsten Schlomm et al. Eur Urol 2011;2:320-329
1/11
Platinum Slide Series
Anatomic variability of the prostatic apex. Depending on the individual apex shape, between 10% and 40% of the functional urethra is covered by parenchymal apex tissue. Otherwise, the prostatic apex is covered by some muscular tissue on the ventral and rectal aspects as rudiments of embryonic and adolescent prostatic development.
Thorsten Schlomm et al. Eur Urol 2011;2:320-329
10/11
Platinum Slide Series
Surgical anatomy of the urethral sphincter complex. (A) Fixation of the urethral sphincter (modified from Luschka [16]). (B) Lateral aspect of the urethral sphincter after nerve sparing.PPL = puboprostatic ligament; PVL = pubovesicalis ligament; PP = puboperinealis muscle; DA = detrusor apron; B = bladder; FSS = fascia of the striated sphincter; ML = Mueller's ligaments (ischioprostatic ligaments); NVB = neurovascular bundle; R = rectum; MDR = medial dorsal raphe; RU = rectourethralis muscle; OI = Os ischiadicum; SS = striated sphincter (rhabdosphincter); PB = pubis bone.
Thorsten Schlomm et al. Eur Urol 2011;2:320-329
8/11
Anatomy Seminal Vesicles
Transverse
Coronal
Anatomy Periprostatic Structures
S
IO
IO
P
L
L
P
IO
IO
ugd
i
i
c c B
i
i
R
L
L
Transverse
Coronal
Variation in Genitourinary diaphragm
Apex: Anatomische Variabilität
31 Akademie Expertenkurs
Walz et al, Eur Urol, 2010
Parasympathic nerves
Course of neurovascular bundle
Abb.: 5
Stolzenburg et al, Eur Urol, 2007
34 Akademie Expertenkurs
Standardtechnik
intrafasziale Technik
Abb.: 6
Stolzenburg et al, Eur Urol, 2007
35 Akademie Expertenkurs 35
Walz et al, Eur Urol, 2010
36 Akademie Expertenkurs
Prostate Brachytherapy Course
“Selection of patients for prostate cancer permanent implant brachytherapy”
C. Salembier
Department of Radiotherapy-Oncology Europe Hospitals – Brussels - Belgium
Patient selection: • do we have recommendations ? • if yes, what do they learn us ?
ABS 1999
ESTRO 2000
Actually only minor differences with the ABS paper ...
a lot of literature
but
no new recommendations
until …. 2012
199 9
200 0
201
Patient selection for prostate LDR brachytherapy …. Do we have all the answers reading these recommendations ?
… no … after reading the literature some questions remain …
High dose rate brachytherapy for prostate cancer: PATIENT SELECTION
Peter Hoskin Mount Vernon Cancer Centre Northwood UK
HDR prostate brachytherapy
• Practical ➢ Existing source, afterloading
• Physical ➢ Greater implant volume ➢ including seminal vesicles
• Biological ➢ Low / tumour; greater biological dose with high dose per fraction
Advantages of temporary HDR prostate brachytherapy
Radioprotection
– no free live sources – no risk of source loss – no radioprotection issues after discharge
Cheap: utilises existing HDR source and equipment
Day case procedure
Disadvantages of temporary HDR prostate brachytherapy
High dose rate radiation requires fractionation – no longer!?
– logistics:
• Quality assurance
Selection for HDR prostate brachytherapy
• Boost with external beam
• Monotherapy
Pre treatment investigations
• General medical assessment • Prostate biopsy
• PSA • IPSS • IEFS • Flow rate • Pelvic MRI • Staging investigations ➢ PSA ➢ Bone scan ➢ (Whole body MRI) ➢ (Choline PET) ➢ (PSMA PET)
Indications for HDR prostate brachytherapy BOOST
Where there is a significant predictive risk of extracapsular or seminal vesical involvement:
External beam
Brachytherapy
Indications for HDR prostate brachytherapy BOOST
Where there is a significant predictive risk of extracapsular or seminal vesical involvement:
T3a T3b ?T2c
Gleason 8 – 10 ?Gleason 4+3
Probability of organ confined disease
[Partin 2001]
PSA 6.1-10.0
Gleason T1c
T2a
T2b
T2c
3+4
54% (49-59)
35% (30-40)
26% (22-31)
24% (17-32)
4+3
43% (35-51)
25% (19-32)
19% (14-25)
16% (10-24 )
8-10
37% (28-48)
21% (15-28)
15% (10-21)
13% (8-20 )
Probability of organ confined disease
[Partin 2001]
PSA >10.0
Gleason T1c
T2a
T2b
T2c
3+4
37% (32-42)
20% (17-24)
14% (11-17)
11% (7-17)
4+3
27% (21-34)
14% (10-18)
9% (8-13)
7% (4-12 )
8-10
22% (16-30)
11% (7-15)
7% (4-10)
6% (3-10 )
Ext beam/HDR boost for prostate
?The low risk patient – PSA<10ng/ml
……….what is the risk of ECE or seminal vesicle invasion??...............
– Gleason 6 or below (?3+4) – T2a or less
Probability of organ confined disease
[Partin 2001]
PSA 4.1-6.0
Gleason T1c
T2a
T2b
T2c
2-4
90% (78-98)
81% (63-95)
75% (55-93)
73% (52-93 )
5-6
80% (78-83)
66% (62-70)
57% (52-63)
55% (44-64 )
3+4
63% (58-68)
44% (39-50)
35% (29-40)
31% (23-41)
54 patients Gland size median 57ml; range 50-97.3ml
All dosimetric goals achieved
164 patients HDR monotherapy; median CTV volume 60mls (range 14-2
Toxicity
bRFS
Pubic arch interference
• Patient position: ➢
Hyperextended vs standard Plane of prostate vs pubic arch
➢
➢
Table / stand positions
• Needle insertion ➢
Bend the needle?
➢
Enter via adjacent co-ordinate
HDR PROSTATE BRACHYTHERAPY INDICATIONS
• Boost with external beam therapy ➢ Intermediate/high risk disease ➢ ?Low risk disease
• Monotherapy
➢ Phase II studies….. ➢ Low/Intermediate/high risk disease
HDR monotherapy for prostate
? low risk patient
Intermediate risk patient
High risk patient
HDR monotherapy; published series and risk groups
LOW INT HIGH
Yoshioka et al MSKCC
X X
X
Hoskin et al MVCC
X X
Rogers et al
X
Mark et al Texas
X X
X
Prada et al Spain
X X
Martinez et al Michigan
X X
Demanes et al CET
X X
Zamboglu et al Offenbach X X
X
HDR monotherapy: what the guidelines say…………
GEC ESTRO
ABS
HDR for salvage? GEC ESTRO guidelines 2013
HDR for salvage? ABS guidelines 2013
Selection for HDR prostate brachytherapy
Boost with external beam
Monotherapy
Salvage
Selection for HDR prostate brachytherapy …………whole gland or focal…….
Indications for consideration of focal HDR BT
– HDR BT indicated – Focal lesion identified by:
• mpMRI ‘dominant’ lesion • Template biopsy mapping
Prostate Brachytherapy: Imaging for prostate brachytherapy
S. Machtens
Director of the
Department of Urology and Paediatric Urology
Academic Teaching Hospital
Marien-Hospital Bergisch Gladbach
Teaching Course Brussels 2017
Ultrasound Prostate Carcinoma
Hypoechoic nodule compared to normal PZ Low specificity (atrophy, prostatitis, ...)
Ultrasound Diagnostic Performance
• Performance in tumour localization
➢ Sensitivity : 32-85% : false negatives! ➢ Specificity : 41-79% : false positives!
• Inappropriate for screening of general population
Ultrasound Staging Performance
• Performance in tumour staging
➢
Extracapsular extension ▪ sensitivity : 50-90% ▪ specificity : 50-90% Seminal vesicle invasion ▪ sensitivity : 20-60% ▪ specificity : 50-90%
➢
• Inappropriate for staging
Ultrasound Value
• Initial evaluation of patients with elevated PSA and/or abnormal digital rectal examination
• Biopsy guidance
• Determination of prostate seize
• Guidance in brachytherapy
Elastography
Elastography
Sensitivität: 69-80% Spezifität: 78-90%
Elastography plus conventional TRUS-Bx Salomon et al., BJUInt. 2014; 113(4):548-53
1024 men (10+4 cores) Detektionsrates: 10fach TRUS 39,1%, RTE 29%, Combination 46,2%
Prostate HistoScanning™
Tissue Differentiation and Visualization
▪ Computer-based information of 3D data. ▪ Visualization based on different acustic signals. ▪ HistoScanning™ signals appear as red pixels.
Imaging of Prostate Cancer Body Coil Imaging
Imaging of Prostate Cancer Tumour Detection (Body Coil)
Decreased signal intensity relative to normal peripheral zone tissue (70% in peripheral zone)
Imaging of Prostate Cancer Diagnostic Accuracy (Body Coil) (Sensitivity)
Carter 48% Tempany Radiology 1994;192:47 54% Hricak Radiology 1994;193:703 68% Rifkin N Engl J Med 1990;323:621 69% Jager Radiology 1997;203:645 72% Huch Boni Clin Radiol 1995;50:593 76% Kier AJR 1993;161:601 87% Radiology 1991;178:523
Imaging of Prostate Cancer Endorectal Coil Imaging
Endorectal Coil
60 cc
Imaging of Prostate Cancer Body coil versus Endorectal coil
Normal Prostate with Body Coil
Normal Prostate with Endorectal Coil
Imaging of Prostate Cancer Tumour Presence (Endorectal Coil)
Peripheral Zone Tumour with Body Coil
Peripheral Zone Tumour with Endorectal Coil
Imaging of Prostate Cancer Diagnostic Accuracy (Endorectal Coil) (Sensitivity
Tempany Radiology 1994;192:47 61% Presti AJR 1996;166:103 63% Beyersdorff Radiology 2002;224:701 68% Perrotti J Urol 1999;162:1314 70% Vilanova Eur Radiol 2001;11:229 71% Ogura Urology 2001;57:721 72% Ikonen Acta Radiol 2001;42:348 74% Cornud Br J Urol 1996;77:843 74% Bates Clin Radiol 1996;51:550 77% Bartolozzi Eur Radiol 1996;6:339 82% Huch Boni JCAT 1995;19:232 82% Huch Boni Clin Radiol 1995;50:593 88%
Imaging of Prostate Cancer Tumour detection @ 3 Tesla
Courtesy: Fütterer JJ, Nijmegen
Kim, J Comput Assist Tomogr 2006;30:7-11 (70%) Heijmink, Radiology 2007;244:184 (ERC > BC)
1.5 Tesla MRI
MRI: • Resolution: good • Contrast: good, especially soft tissue contrast
Zentrale Zone
Periphere Zone
Tumor
1.5 T
T2-weigthed
T1-weighted
3.0 Tesla MRI
T1 weighted
T2 -weighted
3.0 Tesla MRI + Endorectal coil
MRT-Ultrasound-Fusion
Hradaschik, J Urol 2012
MR-guided Biopsy
Transrectal approach: roboter-guided biopsy
Transgluteal approach in open MR
Functional Imaging
Functional Imaging
• Magnetic Resonance Spectroscopy
• Dynamic Contrast-Enhanced MRI
• Diffusion Weighted Imaging
• Cholin PET
Magnetic Resonance Spectroscopy
MR-Spectroscopy
• acquisition of spectra from small volumes (voxels) throughout the prostate gland
• detection of cellular metabolites
➢
citrate in normal tissue and BPH
➢
choline in tumour lesions
MR-Spectroscopy Normal Prostate
1 H-spectra: dominant citrate peak no elevated choline
Normal prostate volume
MR-Spectroscopy Prostate Cancer
1 H-spectra: reduced citrate elevated choline
Prostate Cancer
MR-Spectroscopy Spectral Maps
MR-Spectroscopy Choline/Citrate Ratio Images
Choline
Citrate
Spectrum
Index
MR-Spectroscopy Choline/Citrate Ratio Images
MR-Spectroscopy Diagnostic accuracy (Sensitivity)
Dynamic Contrast-Enhanced MRI
Dynamic Contrast-Enhanced MRI Assessment of Angiogenesis
Enhancement
Lesion Morphology
Angiogenic Factors
Increased in- en efflux Expanded extracellular space Increased extravasation
Growth of existing vessels De novo angiogenesis
Abnormal configuration: AV-shunts and defective endothelium
Earlier onset of enhancement Increased slope
Dynamic Contrast-Enhanced MRI Assessment of Angiogenesis
Early
Fast
*G. Jager, J. Barentsz, Nijmegen Group
Dynamic Contrast-Enhanced MRI Assessment of Angiogenesis
Late
Slow
*G. Jager, J. Barentsz, Nijmegen Group
Dynamic Contrast-Enhanced MRI Assessment of Angiogenesis
63-year old man Suspicious lesion in left peripheral zone
Imaging of Prostate Cancer Diagnostic accuracy (dCE MRI)(Sensitivity)
Diffusion Weighted Imaging
Diffusion Weighted Imaging
• visualize the amount of random (‘Brownian’) movements of water molecules (diffusion)
• surrogate for “cellular density”
Diffusion Weighted Imaging
T2W
b1000
ADC
T2W
b1000
ADC
Dickinson L et al.; Eur Urol 59(2011):477-494
Dickinson L et al.; Eur Urol 59(2011):477-494
T2w: PI-RADS
Röthke M, Fortschr Röntgenstr 2013; 185: 253–261
DWI MRI: PI-RADS
Röthke M, Fortschr Röntgenstr 2013; 185: 253–261
DCE MRI: PI-RADS
Röthke M, Fortschr Röntgenstr 2013; 185: 253–261
Can clinically significant prostate cancer be detected with multipara- metric magnetic resonance imaging? A systematic review of the literature. Fütterer JJ et al., Eur Urol 2015; Epub ahead of print been shown that multiparametric magnetic resonance imaging (mpMRI) facilitates tion of PCa and can help in targeting prostate biopsy. Objective: To systematically review the literature to determine the diagnostic accuracy
localisa-
of
mpMRI
in
the detection
of
clinically
significant
PCa.
Evidenceacquisition:
ThePubmed,Embase,andCochraneCentral Register of ControlledTrials
(CENTRAL) databases were searched the search criteria‘‘prostateORPcaORPSAORprostaticORprostatecancer’’ AND‘‘MRORNMROR NMRI ORMRI ORmagnetic resonance ORADCORDWI ORDCEORdiffusion weighted OR dynamiccontrast ORmultiparametricORMRSI ORMRspectroscopy’’. Two reviewersindepen- dently assessed 1729 records. Two independent reviewersassessed themethodologic quality using theQuality Assessment of Diagnostic Accuracy Studies (QUADAS-2) 2 tool. Evidence synthesis: Twelve articles were eventually selected. Patients had a median age of 62–65 yr (range 39–83 yr), amedian prostate-specific antigen (PSA) level of 5.1–13.4 ng/ml (range1.2–228 ng/ml), and Gleason scoreof 6–10. Variousdefini tions of clinical significance were used, mainly based on maximum cancer core length and grade at biopsy, number of positive cores, and PSA. Detection of clinically significant PCausingmpMRI ranged from 44% to 87%in biopsy-naı¨vemales and men with prior negative biopsies using prostate biopsy or definitive pathology of a radical prostatectomy specimen as the reference standard. The negative predictive value for exclusion of significant disease ranged from 63%to 98%. Conclusions: mpMRI isabletodetect significant PCain biopsy-naı¨vemalesandmenwith prior negativebiopsies. Thenegativepredictivevalueof mpMRI is important to theclinician because mpMRI couldbeused toruleout significant disease.Thismay result in fewer or nosystematicor targeted biopsies in patientswith PSAsuspicious for prostate cancer. Patient summary: We reviewed the diagnostic accuracy of multiparametric magnetic reso- from January 1, 2000 to September 30, 2014, using
ith
atic
illeirs c ,
earch IRCCS of Urology, University artment of Radiology, r, New York, NY, USA; rology, LilleUniversity Institute,
jor
challenge.
It
has
)
facilitates
localisa-
gnostic accuracy
of
r of Controlled Trials 30, 2014, using the ND‘‘MRORNMROR fusion weighted OR reviewersindepen- ethodologic quality ) 2 tool. ad a median age of el of 5.1–13.4 ng/ml clinical significance t biopsy, number of RI ranged from 44% g prostate biopsy or
Hospital admissions after transrectal ultrasound- guided biopsy of the prostate in men diagnmosed with prostate cancer: a database analysis from England. Anastasiadis E et al., Int J Urol 2015; 22: 181 - 186
• n = 198.361 men between 2000 – 2008
• 30-days complicationrate: 3.7% • 1.1% Urinary infection / Sepsis • 1.4% Hematuria • 1.3% Urinary retention
• Increase 1998 => 2008 • HR = 1.20, 95% confidence interval 1.08-1.34 • HR = 1.72, 95% confidence interval 1.41-2.10 for infectin/sepsis
Seite 60
Biopsy: transrectal vs transperineal
Transrectal 1
Transperineal 2
Complication
43,6%
0%
Pain
17,5%
0%
Urinary infection
4.5%
0.4%
Prostatitis
0.7%
0%
Urosepsis
65,8%
41,8%
Hematuria
92,6%
N/A
Hematospermia
36,8%
0%
Hematochezie
n.k.
13,4%
Urinray retention
1 DJ. Rosario et al.BMJ 2012;344 2 Porres D et al., DGU 2014
Seite 61
Biopsy PCA-Detectionrates – Comparison Literature
PCA-Detectionrates
Transrectal Saturation (TRUS) 1
30% – 43%
Transperineal (TRUS) 2
62.5%
MRT-supported (biopsynaiv) 3
66%
1 EAU Guidelines on PCA 2 Porres D et al., DGU 2014 3 CM. Moore et al. Eur Urol 63 (2013), 125-140
Neue Tracer und ihre Anknüpfungspunkte beim PET
11 C Cholin PET
Simultaneous 68 Ga-PSMA HBED-CC PET/MRI improves the Localization of Primary Prostate Cancer Eiber et al; Eur Urol (16), 2016
ith
atic
N=66 Patienten
illeirs c ,
12/30 mit Lymphknotenmetastasen
earch IRCCS of Urology, University artment of Radiology, r, New York, NY, USA; rology, LilleUniversity Institute,
Sensitivität PET: 66% Sensitivität mpMRI: 92% Sensitivität PET/MRI: 98%
jor
challenge.
It
has
)
facilitates
localisa-
gnostic accuracy
of
Schlußfolgerung: Höchste diagnostische Genauigkeit bei PET/MRI im Vergleich zu PET und mpMRI
r of Controlled Trials 30, 2014, using the ND‘‘MRORNMROR fusion weighted OR reviewersindepen- ethodologic quality ) 2 tool. ad a median age of el of 5.1–13.4 ng/ml clinical significance t biopsy, number of RI ranged from 44% g prostate biopsy or
Initial Experience of 68Ga-PSMA PET/CT imaging in High-risk Prostate Cancer Patients prior to Radical Prostatectomy. Budäus et al; Eur Urol (15), 2015
ith
atic
N=30 Patienten
illeirs c ,
12/30 mit Lymphknotenmetastasen
earch IRCCS of Urology, University artment of Radiology, r, New York, NY, USA; rology, LilleUniversity Institute,
4 Patienten (33%) richtig positiv 8 Patienten (66,7%) als falsch negativ
jor
challenge.
It
has
)
facilitates
localisa-
Sensitivität: 33% Spezifität: 100%
gnostic accuracy
of
r of Controlled Trials 30, 2014, using the ND‘‘MRORNMROR fusion weighted OR reviewersindepen- ethodologic quality ) 2 tool. ad a median age of el of 5.1–13.4 ng/ml clinical significance t biopsy, number of RI ranged from 44% g prostate biopsy or
Positiv prädiktiver Wert: 100% Negativ prädiktiver Wert: 69,2%
Conclusions
• Ultrasound
➢ initial assessment of patients with increased PSA and/or abnormal DRE, but low diagnostic yield
➢
excellent for biopsy guidance
➢
no screening
➢
no staging
Conclusions
• CT
➢
no value for local tumor detection
➢
lymph node staging
➢
targeted imaging after bone scan
➢
(detection of visceral metastases)
Conclusions
• MRI
➢
optimally depicts prostatic anatomy
➢ primarily detects peripheral zone carcinoma
Conclusions
• Tumour detection
➢
T2-weighted imaging ▪
baseline examination!
➢
MR-spectroscopy ▪ primarily detects higher grade tumours
➢
dynamic contrast enhanced MRI ▪ imaging of tumor neovascularisation
➢
diffusion weighted imaging Minimal requirement in MRI imaging
Conclusions
• MRI
➢ Still not recommended before primary biopsy
➢ Recommendation before secondary biopsy
➢ Rising importance in follow-up under active surveillance
Conclusions
• PET
➢ Indication in primary tumour detection unclear.
➢
Unclear indication during staging.
➢ No indication in case of recurrence with PSA<1ng/ml
➢ Unclear indication and evidence in case of recurrence with PSA>1ng/ml
Bashar Al-Qaisieh
Planning modality
Description
Creation of a plan on the OR just before the implant procedure, with immediate execution of the plan
Intra-operative planning
Stepwise refinement of the treatment plan using computerised dose calculations derived from image-based needle position feedback Constant updating of calculations of dose distribution, using continuous deposited seed position feedback
Interactive planning
Dynamic dose distribution
From Polo et al. Review of intraoperative imaging and planning techniques in permanent seed prostate brachytherapy. RO 94(2010) 12-23.
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