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磁共振成像引导与缩小边缘计算机断层扫描引导的立体定向体部放射治疗用于局限性前列腺癌的剂量学比较:一项3期试验的事后分析

Dosimetric Comparison of Magnetic Resonance Imaging Guided Versus Reduced Margin Computed Tomography Guided Stereotactic Body Radiation Therapy for Localized Prostate Cancer: Post Hoc Analysis of a Phase 3 Trial.

作者信息

Courtney Patrick Travis, Dong Huiming, Lao Yi, Pham Jonathan, Lauria Michael, Chu Fang-I, Krupien Andrew J, Valle Luca F, Low Daniel A, Lamb James, Steinberg Michael L, Qi Xiarong Sharon, Cao Minsong, Kishan Amar U

机构信息

Department of Radiation Oncology, University of California, Los Angeles, California.

Department of Radiation Oncology, University of California, Los Angeles, California.

出版信息

Int J Radiat Oncol Biol Phys. 2025 Jun 5. doi: 10.1016/j.ijrobp.2025.05.066.

Abstract

PURPOSE

The MIRAGE (Magnetic resonance imaging-guided versus computed tomography-guided stereotactic body radiotherapy for prostate cancer) trial (NCT04384770) showed that aggressive planning target volume (PTV) margin reduction, achieved by leveraging the advanced image-guidance of magnetic resonance imaging guided radiation therapy, led to lower toxicity after stereotactic body radiation therapy (SBRT) to the prostate compared with computed tomography guided SBRT (CTgSBRT) with a standard PTV margin. It is unknown whether the dosimetric benefit of reducing PTV margins alone-independent of the other components of advanced image guided radiation therapy that allowed margin reduction-would be predicted to replicate this decrease in toxicity.

METHODS AND MATERIALS

We retrospectively replanned 16 CTgSBRT patients with 3- and 2-mm PTV margins from the 4 mm used in MIRAGE to compare with magnetic resonance imaging guided SBRT (MRgSBRT) patients' radiation therapy plans (n = 79), which used a 2-mm PTV margin. We compared target and organs-at-risk dosimetry and performed multivariable linear regression to control for potentially related covariates. We estimated normal tissue complication probability to assess the potential impact of PTV margin reduction on the risks of rectal and bladder toxicity.

RESULTS

Compared with MRgSBRT patients, replanned CTgSBRT patients had similar (3 mm) or statistically significantly improved (2 mm) rectal dosimetry and similar bladder dosimetry (2 mm). These trends persisted on multivariable linear regression. Normal tissue complication probability modeling demonstrated a statistically significant improvement in rectal toxicity whereby margin reduction from 4→3 mm and 4→2 mm resulted in relative reductions in toxicity probabilities of 56% and 78%, respectively. For bladder toxicity, reducing margins from 4 to 3 or 2 mm reduced the probability of bladder toxicity by 96%, although these relative differences were not statistically significantly.

CONCLUSIONS

Reducing PTV margins for CTgSBRT plans produced similar to improved organs-at-risk dosimetry compared with the clinical MRgSBRT plans, which in turn would be predicted to reduce toxicity when compared to larger margin CTgSBRT plans. This improvement in dosimetry could explain the reduction in modeled rectal toxicity, but the impact on bladder toxicity is unclear, with large, but nonsignificant relative differences underscoring our incomplete understanding of the drivers of post-SBRT urinary toxicity.

摘要

目的

MIRAGE(磁共振成像引导与计算机断层扫描引导的前列腺癌立体定向体部放射治疗)试验(NCT04384770)表明,与采用标准计划靶体积(PTV)边界的计算机断层扫描引导的立体定向体部放射治疗(CTgSBRT)相比,利用磁共振成像引导放射治疗的先进图像引导技术实现的激进PTV边界缩小,可降低前列腺立体定向体部放射治疗(SBRT)后的毒性。单独降低PTV边界(独立于允许边界缩小的先进图像引导放射治疗的其他组成部分)的剂量学益处是否会预测出毒性的这种降低尚不清楚。

方法和材料

我们回顾性地重新规划了16例CTgSBRT患者的放疗计划,将PTV边界从MIRAGE试验中使用的4毫米分别调整为3毫米和2毫米,以便与磁共振成像引导的SBRT(MRgSBRT)患者的放疗计划(n = 79)进行比较,后者使用2毫米的PTV边界。我们比较了靶区和危及器官的剂量学,并进行多变量线性回归以控制潜在的相关协变量。我们估计正常组织并发症概率,以评估PTV边界缩小对直肠和膀胱毒性风险的潜在影响。

结果

与MRgSBRT患者相比,重新规划的CTgSBRT患者的直肠剂量学相似(3毫米)或在统计学上有显著改善(2毫米),膀胱剂量学相似(2毫米)。这些趋势在多变量线性回归中持续存在。正常组织并发症概率模型显示直肠毒性有统计学上的显著改善,即边界从4毫米缩小到3毫米和4毫米缩小到2毫米分别导致毒性概率相对降低56%和78%。对于膀胱毒性,将边界从4毫米缩小到3毫米或2毫米可使膀胱毒性概率降低96%,尽管这些相对差异在统计学上不显著。

结论

与临床MRgSBRT计划相比,降低CTgSBRT计划的PTV边界可产生相似或更好的危及器官剂量学,与更大边界的CTgSBRT计划相比,这反过来预计会降低毒性。剂量学的这种改善可以解释模拟直肠毒性的降低,但对膀胱毒性的影响尚不清楚,较大但不显著的相对差异突出了我们对SBRT后泌尿毒性驱动因素的不完全理解。

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