Immunology Clinical Trial
Official title:
ABO Blood Group Antibody Elimination by a Combination of Semiselective Immunoadsorption Therapy and Membrane Filtration
- Recipient desensitization protocols were shown to enable successful living donor kidney
transplantation across major ABO blood group barriers. For extracorporeal depletion of
circulating ABO antibodies plasmapheresis or ABO blood group specific immunoadsorption
(IA) are most commonly used.
- The efficiency of semiselective non-antigen specific IA in ABO-incompatible
transplantation is currently not well established. One potential drawback of
semiselective adsorbers could be an incomplete elimination of IgM.
- This randomized controlled crossover trial was designed to clarify whether membrane
filtration, as an adjunct to semiselective IA, can substantially enhance elimination of
IgM.
-Background and study aims
ABO-incompatible living donor kidney transplantation offers the possibility to expand the
donor pool by approximately 30%. A variety of different desensitization protocols were shown
to enable successful transplantation across major ABO barriers. In this context, apheresis
for antibody depletion represents the therapeutic mainstay. Two distinct technical
principles, plasmapheresis and ABO antigen-specific immunoadsorption, were shown to allow for
excellent short- and intermediate-term outcomes. A particular technical advantage of
immunoadsorption may be its high selectivity regarding antibody depletion, which precludes
major losses of essential plasma constituents, including coagulation factors and albumin,
even after treatment of large plasma volumes. Nevertheless, high treatment costs associated
with the use of ABO-specific columns (that are not approved for reuse) may limit their
widespread clinical application.
The efficiency of semi-selective immunoadsorption technologies regarding ABO antibody
depletion and recipient desensitization is less well established. Theoretically,
non-antigen-specific immunoglobulin depletion using protein A-, GAM peptide-, or anti-Ig
antibody-based adsorbers, could bring about several advantages, such as lower treatment costs
associated with the use of reusable twin columns, and the potential to simultaneously deplete
antibodies also against HLA antigens. A critical drawback, however, may be an evident
inefficiency regarding (ABO-specific) IgM depletion, and this could pose a considerable risk
of rejection.
One strategy to overcome the drawback of incomplete IgM depletion could be the use of
semiselective immunoadsorption combined with other antibody depletion technologies. In this
context, one attractive option could be an enhancement of antibody elimination by connecting
a membrane filter (cascade filter) to the immunoadsorption device. We propose to conduct an
open randomized crossover study that is designed to see if membrane filtration when applied
as an adjunct to semiselective immunoadsorption (GAM peptide adsorbers) is able to enhance
anti-ABO IgM elimination to an extent comparable to ABO antigen-specific immunoadsorption.
The results of this study, which will enrol 14 patients receiving IA treatment for clinical
indications outside the transplantation field, are expected to provide a valuable basis for
the use of combined apheresis approaches in the context of ABO-incompatible kidney
transplantation.
-Who can participate?
We are planning to recruit 14 adult patients (>18 years, both genders eligible, healthy
volunteers not accepted) that are subject to regular routine IA therapy at >1 weekly
intervals for clinical indications that are not related to ABO-incompatible transplantation
(antibody-mediated autoimmune disorders, such as systemic lupus erythematosus or myasthenia
gravis).
-What does the study involve?
For membrane filtration, we will use a membrane filter with documented capacity to eliminate
plasma IgM. The study will be conducted in a randomized crossover design (AB vs. BA design;
stratified randomization). Treatment consists in IA plus membrane filtration (A) or IA as the
sole treatment (B), respectively. The primary study endpoint is the percent reduction of ABO
blood group specific IgM. The study is powered to detect a 30% increase in IgM elimination.
-What are the possible benefits and risks of participating?
We do not expect any direct benefits for the study subjects. This pilot study, however, may
provide a valuable basis for a future trial evaluating the clinical impact of combined IA
plus membrane filtration in ABO incompatible transplantation. Potential risks include:
adverse reactions upon exposure to polysulfone (rash, pruritus, fever), reduction in
fibrinogen levels and eventually a transient increase in the risk of bleeding.
;
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