Late GU Grade 1 and 2 toxicities were observed in 38% and 48%, respectively, and one patient developed Grade 3 urinary incontinence. Three patients developed urethral stricture (Grade 3), which were corrected with urethral dilatation. The median time to develop Grade 3 complications was
9 months (range, 9–12 months), and the median time for resolution of Grade 3 symptoms was 7 months (range, 23–21 months). No Grade 4 urinary toxicities were observed. Baseline urinary status was found to be significantly associated with post-treatment late urinary toxicity for the development of Common Toxicity Criteria for Adverse Events Grade 2 (p = 0.008) but not for Grade 3 or higher toxicity. Figure 3 illustrates the rates of Grade 2 GU toxicity based on baseline scores. Seventy-eight percent of patients were without significant urinary symptoms (GU Grade 0–1) before the administration of salvage treatment, and 52% of these
remained Rapamycin supplier free of additional urinary toxicity at the time of last followup. Thus, the majority of urinary toxicity PI3K Inhibitor Library order resolved to baseline. Of the three patients who developed Grade 3 urinary toxicity, two were characterized at baseline as having Grade 2 symptoms, and one patient was classified as having Grade 1 symptoms at baseline. The median IPSS at baseline was 6 (range, 1–17), and the median IPSS at last followup was 12 (range, 1–30). Resolution of an elevated IPSS was seen in 41% of patients (returned within 2 points of baseline) within a median time of 4.5 months. IPSS
did not return to baseline values at the time of last followup in 24 patients, with a reported median IPSS value of 14.5 at the time of last followup (range, Venetoclax 5–30). Late Grade 1 and 2 gastrointestinal (GI) toxicities were noted in 43% and 14% of patients, respectively, and 83% of patients were free of Grade 2 or higher GI complications (Fig. 3). GI complications consisted almost entirely of transient rectal bleeding. No Grade 3 or higher GI complications were encountered. The majority of patients were not sexually active at baseline. The median International Index of Erectile Function score before and after treatment was 2 and 1.5, respectively. No dosimetric values such as V100 (volume of the prostate receiving PD) or D90 (dose to 90% of the prostate exposed to PD) were significantly associated with the risk of disease progression or any complications. In this prospective study of salvage HDR monotherapy, 76% of patients were able to achieve biochemical control in a patient population that is by definition radioresistant. Our data suggest that reirradiation with high-dose hypofractionation may be a rational salvage approach to eradicate tumor cells that have survived conventionally fractionated radiotherapy. We also noted an excellent tolerance profile to patients who received salvage HDR despite the high initial doses that patients had received as part of their definitive EBRT.