Performance and Hemocompatibility of a Novel Polysulfone Dialyzer: A Randomized Controlled Trial

聚砜 医学 交叉研究 三醋酸纤维素 外科 生物医学工程 化学 安慰剂 纤维素 病理 生物化学 替代医学
作者
Götz Ehlerding,Ansgar Erlenkötter,Adelheid Gauly,Bettina Griesshaber,James Kennedy,Lena Rauber,W Ries,Hans Schmidt-Gürtler,Manuela Stauss‐Grabo,Stefan Wagner,Adam M. Zawada,Sebastian Zschätzsch,Manuela Kempkes-Koch
出处
期刊:Kidney360 [American Society of Nephrology (ASN)]
卷期号:2 (6): 937-947 被引量:18
标识
DOI:10.34067/kid.0000302021
摘要

Abstract Key Points We investigated the performance and hemocompatibility of a new polysulfone hemodialyzer with enhanced membrane properties. β2-Microglobulin removal rate was noninferior to both comparator dialyzers and superior to a cellulose-acetate–based dialyzer. The dialyzer showed a favorable hemocompatibility profile on the basis of markers for complement, cell and contact activation, and coagulation. Background High-flux dialyzers effectively remove uremic toxins, are hemocompatible to minimize intradialytic humoral and cellular stimulation, and have long-term effects on patient outcomes. A new dialyzer with a modified membrane surface has been tested for performance and hemocompatibility. Methods This multicenter, prospective, randomized, crossover study involved the application of the new polysulfone-based FX CorAL 600 (Fresenius Medical Care, Bad Homburg, Germany), the polyarylethersulfone-based Polyflux 170H (Baxter Healthcare Corporation, Deerfield, IL), and the cellulose triacetate–based SureFlux 17UX (Nipro Medical Europe, Mechelen, Belgium), for 1 week each, to assess the noninferiority of the FX CorAL 600’s removal rate of β 2-microglobulin. Performance was assessed by removal rate and clearance of small- and medium-sized molecules. Hemocompatibility was assessed through markers of complement, cell activation, contact activation, and coagulation. Results Of 70 patients, 58 composed the intention-to-treat population. The FX CorAL 600’s removal rate of β 2-microglobulin was noninferior to both comparators ( P <0.001 versus SureFlux 17UX; P =0.0006 versus Polyflux 170H), and superior to the SureFlux 17UX. The activation of C3a and C5a with FX CorAL 600 was significantly lower 15 minutes after treatment start than with SureFlux 17UX. The activation of sC5b-9 with FX CorAL 600 was significantly lower over the whole treatment than with SureFlux 17UX, and lower after 60 minutes than with the Polyflux 170H. The treatments with FX CorAL 600 were well tolerated. Conclusions FX CorAL 600 efficiently removed small- and medium-sized molecules, showed a favorable hemocompatibility profile, and was associated with a low frequency of adverse events in this study, with a limited patient number and follow-up time. Further studies, with longer observation times, are warranted to provide further evidence supporting the use of the new dialyzer in a wide range of therapeutic options, and for long-term treatment of patients on hemodialysis, to minimize the potential effects on inflammatory processes.
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