Multicentre, randomised, blinded, control trial of drug-eluting balloon vs Sham in recurrent native dialysis fistula stenoses

Jan Swinnen; Kerry Hitos; Lukas Kairaitis; Simon M. Gruenewald; George Larcos; David Farlow; David Huber; Gabriel Cassorla; Christopher Cheang Han Leo; Laurencia Villalba; Richard D. Allen; Farshid Niknam; David Burgess

doi:10.1177/1129729818801556

Multicentre, randomised, blinded, control trial of drug-eluting balloon vs Sham in recurrent native dialysis fistula stenoses

Jan Swinnen(The University of Sydney), Kerry Hitos(The University of Sydney), Lukas Kairaitis(Camden and Campbelltown Hospitals), Simon M. Gruenewald(Westmead Hospital), George Larcos(Westmead Hospital), David Farlow(Westmead Hospital), David Huber(University of Wollongong), Gabriel Cassorla(Pontificia Universidad Católica de Chile), Christopher Cheang Han Leo(National University Hospital), Laurencia Villalba(University of Wollongong), Richard D. Allen(The University of Sydney), Farshid Niknam(University of Wollongong), David Burgess(Blacktown & Mount Druitt Hospital)

The Journal of Vascular Access

September 18, 2018

10.1177/1129729818801556

Cited by 61

Abstract

BACKGROUND: Endovascular treatment of autogenous arteriovenous haemodialysis fistula stenosis has high reintervention rates. We investigate the effect of drug-eluting balloons in the treatment of recurrent haemodialysis fistula stenosis. METHODS: This is a randomised, controlled, investigator-initiated and run, prospective, blinded, multicentre trial. Patients with recurrent autogenous arteriovenous haemodialysis fistula stenosis received standard endovascular treatment plus drug-eluting balloon or standard endovascular treatment plus uncoated balloon (Sham). Primary endpoint was late lumen loss in trial area on ultrasound at 6 weeks, 3, 6 and 12 months. Secondary endpoints were freedom from reintervention to the Index Trial Area and decline in fistula flow (Qa). Interim analysis was performed at 6 months (unblinded due to timeliness). RESULTS: Patients with 132 recurrent stenoses (48% in bare Nitinol stents) were randomised with 70 receiving drug-eluting balloon and 62 Sham. At 6 months, decline in late lumen loss was 0.23 ± 0.03 mm/month for Sham and 0.045 ± 0.03 mm/month for drug-eluting balloon arm, a significant difference (0.18 mm, p = 0.0002). At 12 months, this difference persisted at 0.12 mm (p = 0.0003). At 6 months, significant difference in late lumen loss for instent restenoses (p = 0.0004) was observed, with non-significant difference for unstented restenoses (p = 0.065). Mean time for freedom from reintervention was 10.14 months for Sham versus 42.39 months for drug-eluting balloon (p = 0.001). The same was shown for instent (p = 0.014) and unstented (p = 0.029) restenoses. Qa decline rate at 6 months was 36.89 mL/min/month (Sham) and 0.41 mL/min (drug-eluting balloon). The difference was significant (36.48 mL/min; p = 0.02) and persisted to 12 months (p = 0.44). CONCLUSION: Paclitaxel drug-eluting balloon significantly delays restenosis after angioplasty for recurrent autogenous arteriovenous haemodialysis fistula stenosis, persisting to 12 months. Drug-eluting balloon significantly increases freedom from reintervention at 12 months with these effects true in stented and unstented fistulas.

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