Abstract
PurposeThese studies were undertaken to determine if fexapotide triflutate 2.5 mg transrectal injectable (FT) has significant long-term (LT) safety and efficacy for the treatment of benign prostatic hyperplasia (BPH).MethodsTwo placebo controlled double-blind randomized parallel group trials with 995 BPH patients at 72 sites treated 3:2 FT:placebo, with open-label FT crossover (CO) re-injection in 2 trials n = 344 and long-term follow-up (LF) 2–6.75 years (mean 3.58 years, median 3.67 years; FT re-injection CO mean 4.27 years, median 4.42 years) were evaluated. 12 months post-treatment patients elected no further treatment, approved oral medications, FT, or interventional treatment. Primary endpoint variable was change in Symptom Score (IPSS) at 12 months and at LF. CO primary co-endpoints were 3-year incidence of (1) surgery for BPH in FT treated CO patients versus patients crossed over to oral BPH medications and (2) surgery or acute urinary retention in FT-treated CO placebo patients versus placebo patients crossed over to oral BPH medications. 28 CO secondary endpoints assessed surgical and symptomatic outcomes in FT reinjected patients versus conventional BPH medication CO and control subgroups at 2 and 3 years.ResultsFT injection had no significant safety differences from placebo. LF IPSS change from baseline was higher in FT treated patients compared to placebo (median FT group improvement − 5.2 versus placebo − 3.0, p < 0.0001). LF incidence of AUR (1.08% p = 0.0058) and prostate cancer (PCa) (1.1% p = 0.0116) were both reduced in FT treated patients. LF incidence of intervention for BPH was reduced in the FT group versus oral BPH medications (8.08% versus 27.85% at 3 years, p < 0.0001). LF incidence of intervention or AUR in placebo CO group with FT versus placebo CO group with oral medications was reduced (6.07% versus 33.3% at 3 years, p < 0.0001). 28/28 secondary efficacy endpoints were reached in LF CO re-injection studies.ConclusionsFT 2.5 mg is a safe and effective transrectal injectable for LT treatment of BPH. FT treated patients also had reduced need for BPH intervention, and reduced incidence of PCa and AUR.
Highlights
Benign prostatic hyperplasia begins in middle age and affects the majority of men by age 70–80 [1,2,3,4,5,6,7]
long-term follow-up (LF) IPSS change from baseline was higher in FT treated patients compared to placebo
Patients were enrolled based on benign prostatic hyperplasia (BPH) Symptom Score (IPSS), transrectal ultrasound (TRUS) prostate volume (PV), urinary peak flow rate (Qmax) (Online Table 1)
Summary
Benign prostatic hyperplasia begins in middle age and affects the majority of men by age 70–80 [1,2,3,4,5,6,7]. Management includes diagnostic evaluation to exclude prostate cancer or benign conditions that are not attributable to prostate hyperplasia, treatment options with medications (alpha blockers; 5-alpha reductase inhibitors), and interventional therapies when necessary, such as transurethral minimally invasive. FT selectively causes loss of cell membrane integrity, mitochondrial metabolic arrest, depletion of RNA, DNA lysis and aggregation, and cell fragmentation and cell loss (Online Figures 2, 3) with subsequent decompression of the urethral lumen. On the basis of evidence from detailed toxicology studies in dogs given injections of FT directly into adjacent structures (bladder, urethra, rectum, periprostatic tissue) the adjacent tissues are unaffected. This report presents the safety and efficacy data from 2 long-term follow-up (LF) prospective double-blind randomized placebo controlled studies and 2 crossover (CO) studies of FT for BPH involving 995 patients at 72 U.S sites conducted from 2009 to 2017
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