PURPOSE: Study goals were to characterize gastrointestinal effects of proton therapy (PT) in a large cohort of patients treated for prostate cancer, identify factors associated with rectal bleeding (RB), and compare RB between patients receiving investigational protocols versus those in outcome-tracking protocols. METHODS AND MATERIALS: A total of 1285 consecutive patients were treated with PT between August 2006 and May 2010. Potential pre-existing clinical and treatment-related risk factors for rectal toxicity were recorded. Common Terminology Criteria for Adverse Events version 3.0 was used to score toxicity. RESULTS: Transient RB was the predominant grade 2 or higher (GR2+) toxicity after PT, accounting for 95% of gastrointestinal events. GR1 RB occurred in 217 patients (16.9%), GR2 RB in 187 patients (14.5%), and GR3 in 11 (0.9%) patients. There were no GR4 or GR5 events. Univariate analyses showed correlations between GR2+ RB and anticoagulation therapy (P=.008) and rectal and rectal wall dose-volume histogram (DVH) parameters (P<.001). On multivariate analysis, anticoagulation therapy (P=.0034), relative volume of rectum receiving 75 Gy (V75; P=.0102), and relative rectal wall V75 (P=.0017) were significant predictors for G2+ RB. Patients treated with investigational protocols had toxicity rates similar to those receiving outcome-tracking protocols. CONCLUSIONS: PT was associated with a low rate of GR2+ gastrointestinal toxicity, predominantly transient RB, which was highly correlated with anticoagulation and rectal DVH parameters. Techniques that limit rectal exposure should be used when possible.
PURPOSE: Study goals were to characterize gastrointestinal effects of proton therapy (PT) in a large cohort of patients treated for prostate cancer, identify factors associated with rectal bleeding (RB), and compare RB between patients receiving investigational protocols versus those in outcome-tracking protocols. METHODS AND MATERIALS: A total of 1285 consecutive patients were treated with PT between August 2006 and May 2010. Potential pre-existing clinical and treatment-related risk factors for rectal toxicity were recorded. Common Terminology Criteria for Adverse Events version 3.0 was used to score toxicity. RESULTS: Transient RB was the predominant grade 2 or higher (GR2+) toxicity after PT, accounting for 95% of gastrointestinal events. GR1 RB occurred in 217 patients (16.9%), GR2 RB in 187 patients (14.5%), and GR3 in 11 (0.9%) patients. There were no GR4 or GR5 events. Univariate analyses showed correlations between GR2+ RB and anticoagulation therapy (P=.008) and rectal and rectal wall dose-volume histogram (DVH) parameters (P<.001). On multivariate analysis, anticoagulation therapy (P=.0034), relative volume of rectum receiving 75 Gy (V75; P=.0102), and relative rectal wall V75 (P=.0017) were significant predictors for G2+ RB. Patients treated with investigational protocols had toxicity rates similar to those receiving outcome-tracking protocols. CONCLUSIONS: PT was associated with a low rate of GR2+gastrointestinal toxicity, predominantly transient RB, which was highly correlated with anticoagulation and rectal DVH parameters. Techniques that limit rectal exposure should be used when possible.
Authors: Ronik S Bhangoo; Molly M Petersen; Gabriella F Bulman; Carlos E Vargas; Cameron S Thorpe; Jason Shen; William W Wong; Jean-Claude M Rwigema; Thomas B Daniels; Sameer R Keole; Steven E Schild; Yi Rong; Todd A DeWees Journal: Int J Part Ther Date: 2021-09-08
Authors: Howard J Lee; Meghan W Macomber; Matthew B Spraker; Stephen R Bowen; Daniel Hippe; Angela Fung; Kenneth J Russell; George E Laramore; Ramesh Rengan; Jay Liao; Smith Apisarnthanarax; Jing Zeng Journal: Adv Radiat Oncol Date: 2018-08-13
Authors: Howard J Lee; Meghan W Macomber; Matthew B Spraker; Stephen R Bowen; Daniel S Hippe; Angela Fung; Kenneth J Russell; George E Laramore; Ramesh Rengan; Jay Liao; Smith Apisarnthanarax; Jing Zeng Journal: Radiat Oncol Date: 2018-09-17 Impact factor: 3.481