| Literature DB >> 27293899 |
M Sean Peach1, Daniel M Trifiletti1, Bruce Libby1.
Abstract
Prostate cancer is the most common malignancy found in North American and European men and the second most common cause of cancer related death. Since the practice of PSA screening has become common the disease is most often found early and can have a long indolent course. Current definitive therapy treats the whole gland but has considerable long-term side effects. Focal therapies may be able to target the cancer while decreasing dose to organs at risk. Our objective was to determine if focal prostate brachytherapy could meet target objectives while permitting a decrease in dose to organs at risk in a way that would allow future salvage treatments. Further, we wanted to determine if focal treatment results in less toxicity. Utilizing the Medline repository, dosimetric papers comparing whole gland to partial gland brachytherapy and clinical papers that reported toxicity of focal brachytherapy were selected. A total of 9 dosimetric and 6 clinical papers met these inclusion criteria. Together, these manuscripts suggest that focal brachytherapy may be employed to decrease dose to organs at risk with decreased toxicity. Of current technology, image-guided HDR brachytherapy using MRI registered to transrectal ultrasound offers the flexibility and efficiency to achieve such focal treatments.Entities:
Year: 2016 PMID: 27293899 PMCID: PMC4884850 DOI: 10.1155/2016/4754031
Source DB: PubMed Journal: Prostate Cancer ISSN: 2090-312X
Figure 1Literature selection process (PRISMA flow diagram).
Summary of dosimetric manuscripts.
| Author/year | Focal/focused | Tumor imaging | Treatment imaging | Patient number/technique | Dosing data summary | Sal |
|---|---|---|---|---|---|---|
| Todor et al. 2011 [ | Focused | MRI/MRS | MRI reg US |
| Mixed seeds allowed 20%–66% increase in dose to tumor PTV while decreasing urethra dose by 10% compared to standard single type seed plans | No |
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| Kamrava et al. 2013 [ | Focal | CT | CT |
| WG: D90 112%, V100 97.6%, V150 33.8%, D2ccRectum 64.1%, D2ccBladder 67.5%, D2ccUrethra 95.2% | Yes |
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| Mason et al. 2014 [ | Focused | MRI | MRI reg US |
| WG: median D90 17.6 Gy, V150 27.3%, D10ccUrethra 17.2 Gy, D2ccRectum 8 Gy | No |
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| Mason et al. 2014 [ | Focal | MRI | MRI reg US |
| WG: D90 20.4 Gy, V100 97.9%, D2ccRectal 20.3 Gy, D10Urethra 12.5 Gy | Yes |
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| Polders et al. 2015 [ | Focal | MRI | MRI reg US |
| WG: D90GTV 198 ± 44 Gy, V100GTV 94% (89–100), D2ccRectal 99 ± 19 Gy, D10Urethra 214 ± 21 Gy, | Yes |
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| Banerjee et al. 2015 [ | Focal | CT | CT |
| WG: D90 109.3% V100 98.7 D2ccBladder 64.8%, D2ccRectal 65.3%, D1ccUrethra 103.8% V75Urethra 75% | Yes |
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| Al-Qaisieh et al. 2015 [ | Focal | MRI/biopsy mapping | MRI reg US |
| WG: D90 181.3 Gy, V100 99.8%, D2ccRectal 107.5 Gy, D10Urethra 205.9 Gy | Yes |
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| Mason et al. 2015 [ | Focused | MRI | MRI reg US |
| Median values for PTVFocused in WG: | No |
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| Moman et al. 2010 [ | Focal | MRI/biopsy mapping | NR |
| WG: V100GTV 25–53%, D2ccRectal 5.0–7.2 Gy, D2ccBladder 6.5–12 Gy | NA |
MRS: magnetic resonance spectroscopy, reg: registered, Sal: salvageable, WG: whole gland, HG: hemigland, FG: focal gland plan, fG: focused gland plan, NR: not reported, and NA: not applicable.
Summary of clinical manuscripts.
| Author/ | Focal/ focused | Tumor/ | Technique (HDR/LDR) | Dosimetry | Symptoms/outcome | Salv. |
|---|---|---|---|---|---|---|
| DiBiase et al. 2002 [ | Focused | MRI, |
| V100 95% (89–98%) | FU duration not recorded, progression not reported | No |
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| Hsu et al. 2013 [ | Focal | MRI, MRS, biopsy mapping/MRI reg US |
| D90CTV 187.5 Gy (107.5–247.5) V100CTV 99.0% (91.7–100.0) V100Rectum 5.5% (0.1–18.7) | 5 y FU, recurrence (Phoenix criteria): 1 y 0%, 2 y 0%, and 3 y 62.7% | Yes |
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| Barret et al. 2013 [ | Focal | biopsy mapping/TRUS |
| NR | FU to one year, PSA change median 6.2 (5–7.9) baseline to 2.5 (0.9–4.4) at 1 year | NA |
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| Wallace et al. 2013 [ | Focal | MRI, biopsy mapping/NR |
| D90GTV 100%, | Median FU 1 month, PSA at one year 0.52 and decreasing | Yes |
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| Peters et al. 2014 [ | Focal | MRI/MRI reg US |
| D90GTV 198 Gy (150–330) | Median FU 36 months, recurrence (Phoenix criteria): 15% (3 of 6 no initial response) | No** |
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| Ennis et al. 2015 [ | Focused | TTI TRUS/TRUS |
| Standard whole gland plan: | Biological recurrence: 0% at 31.5 months | No |
FU: follow-up, GU: genitourinary, GI: gastrointestinal, Salv.: salvageable, LR: low risk, IR: intermediate risk, HR: high risk, reg: registered, ED: erectile dysfunction, NR: not reported, TTI: tissue-type imaging, IPSS: International Prostate Symptom Score, IIEF-5: 5-item version of the International Index of Erectile Function.
Would be salvageable given data if not salvage therapy.
Would not be salvageable given data if not salvage therapy.
Figure 2Organ/isodose contours, DVH for focal plan (a), salvage plan (b), composite of focal plan and salvage plan (c), and standard whole gland plan (d) of ideal focal HDR patient. Isodose lines are as follows: Black 450 cGy, Magenta 750 cGy, Green 1275 cGy, Cyan 1500 cGy, Orange 1875 cGy, Dark Pink 2250 cGy, and Yellow 3000 cGy. Target (e) and organ at risk doses (f).
Experimental dose to target and OAR between focal, salvage, and whole gland HDR brachytherapy.
| Parameter | Focal | Salvage | Composite | Standard |
|---|---|---|---|---|
| D2ccRectum (Gy) | 1.76 | 8.90 | 10.29 | 9.98 |
| D10Urethra (%) | 0.00 | 111.66 | 113.85 | 115.64 |
| D90PTV (%) | 149.30 | 94.15 | 193.9 | 104.54 |
| V100PTV (%) | 100.00 | 86.51 | 100.00 | 92.70 |
| V150PTV (%) | 89.70 | 37.89 | 100.00 | 43.72 |
Figure 3(a) Preprocedural MRI demonstrating GTV (yellow) and nondiseased prostate (red). Preprocedural MRI using two anchor points (green and yellow circles) (b) are able to be registered to intraprocedural TRUS with 2.5 mm grid spacing (c). (d) The resulting merge of the TRUS grid and preprocedural MRI with GTV (thick light blue), urethra (thick solid light green), rectum (thick blue line), and isodose lines (thin lines) for typical whole gland plan using 18 HDR catheters.