Complement activation by dialysis membranes and its association with secondary membrane formation and surface charge

Pascal Melchior; Ansgar Erlenkötter; Adam M Zawada; Dirk Delinski; Christian Schall; Manuela Stauss-Grabo; James P Kennedy

doi:10.1111/aor.13887

Complement activation by dialysis membranes and its association with secondary membrane formation and surface charge

Artif Organs. 2021 Jul;45(7):770-778. doi: 10.1111/aor.13887. Epub 2021 Feb 13.

Authors

Pascal Melchior¹, Ansgar Erlenkötter², Adam M Zawada¹, Dirk Delinski¹, Christian Schall³, Manuela Stauss-Grabo⁴, James P Kennedy¹

Affiliations

¹ Global Research and Development, Product Engineering Center Dialyzers & Membranes, Product Development, Fresenius Medical Care Deutschland GmbH, Sankt Wendel, Germany.
² Global Research and Development, Product Engineering Center Dialyzers & Membranes, Biosciences - Biotechnology, Fresenius Medical Care Deutschland GmbH, Sankt Wendel, Germany.
³ Process Technology, Filter Production, Fresenius Medical Care Deutschland GmbH, Sankt Wendel, Germany.
⁴ Global Medical Office, Clinical and Epidemiological Research, Fresenius Medical Care Deutschland GmbH, Bad Homburg, Germany.

PMID: 33326619
DOI: 10.1111/aor.13887

Abstract

Activation of the complement system may occur during blood-membrane interactions in hemodialysis and contribute to chronic inflammation of patients with end-stage renal disease. Hydrophilic modification with polyvinylpyrrolidone (PVP) has been suggested to increase the biocompatibility profile of dialysis membranes. In the present study we compared the complement activation of synthetic and cellulose-based membranes, including the polysulfone membrane with α-tocopherol-stabilized PVP-enriched inner surface of the novel FX CorAL dialyzer, and linked the results to their physical characteristics. Eight synthetic and cellulose-based dialyzers (FX CorAL, FX CorDiax [Fresenius Medical Care]; Polyflux, THERANOVA [Baxter]; ELISIO, SUREFLUX [Nipro]; xevonta [B. Braun]; FDX [Nikkisio Medical]) were investigated in the present study. Complement activation (C3a, C5a, and sC5b-9) was evaluated in a 3 hours ex vivo recirculation model with human blood. Albumin sieving coefficients were determined over a 4 hours ex vivo recirculation model with human plasma as a surrogate of secondary membrane formation. Zeta potential was measured as an indicator for the surface charge of the membranes. The FX CorAL dialyzer induced the lowest activation of the three complement factors (C3a: -39.4%; C5a: -57.5%; and sC5b-9: -58.9% compared to the reference). Highest complement activation was found for the cellulose-based SUREFLUX (C3a: +154.0%) and the FDX (C5a: +335.0% and sC5b-9: +287.9%) dialyzers. Moreover, the FX CorAL dialyzer had the nearest-to-neutral zeta potential (-2.38 mV) and the lowest albumin sieving coefficient decrease over time. Albumin sieving coefficient decrease was associated with complement activation by the investigated dialyzers. Our present results indicate that the surface modification implemented in the FX CorAL dialyzer reduces the secondary membrane formation and improves the biocompatibility profile. Further clinical studies are needed to investigate whether these observations will result in a lower inflammatory burden of hemodialysis patients.

Keywords: biocompatibility; complement activation; hemocompatibility; hemodialysis membranes; membrane potential; protein fouling.

MeSH terms

Complement Activation*
Humans
Kidneys, Artificial*
Membranes, Artificial*

Substances

Membranes, Artificial