Effect of extracorporeal liver support by MARS and Prometheus on serum cytokines in acute-on-chronic liver failure

Seven consecutive patients with ACLF as defined above and one patient with primary dysfunction of a liver graft after transplantation for decompensated liver cirrhosis were enrolled. In four of the eight patients, alcoholic hepatitis was the precipitating event causing acute decompensation of preexisting alcoholic liver cirrhosis (Table 1). To assess severity of liver disease, Child-Pugh score and model for end-stage liver disease (MELD) score were calculated at baseline [27, 28]. The acute physiology and chronic health evaluation II (APACHE II) and sepsis-related organ failure assessment (SOFA) scores were used to estimate multi-organ dysfunction [29, 30]. Besides, the presence or absence of a systemic inflammatory response syndrome (SIRS) was documented [31].

Patients were allocated to MARS or Prometheus treatments in a randomized cross-over design. By means of sealed envelopes, patients were randomly assigned to start with either MARS or Prometheus and underwent alternating MARS and Prometheus treatments on two to eight consecutive days. The number of treatments applied was dependent on the clinical course. The study protocol was approved by the Ethics Committee of the Medical University of Graz, and informed consent was obtained in accordance with the Declaration of Helsinki.

MARS and Prometheus treatments were performed for six hours at identical blood and dialyzate flows in all patients (200 and 300 ml/minute, respectively), and the same dialysis machine (4008 H; Fresenius Medical Care AG & Co. KGaA) was used during the entire study. The flows in the secondary circuit were set to 200 ml/minute in MARS and 300 ml/minute in Prometheus as recommended by the manufacturers. The dialyzate contained glucose (1 g/l) and magnesium (0.75 mmol/l), and sodium, potassium, and bicarbonate were adjusted to fit each patient's needs. Heparin, epoprostenol (Flolan^®; GlaxoSmithKline, Vienna, Austria) (4 ng/kg per minute), or both were used for anticoagulation, and activated partial thromboplastin time was aimed to remain less than 100 seconds. All patients were treated via a central venous catheter. Infusions of albumin or packed red cells were not allowed during treatments.

In four of the eight patients, a transjugular liver biopsy was performed prior to extracorporeal liver support. Liver biopsy specimens were routinely stained with hematoxylin and eosin and chromotrope aniline blue and were assessed for the presence of steatohepatitis by one of us (CL).

Blood samples were drawn at baseline, at the end of, and one hour after the end of each treatment. In addition, paired samples were obtained from the afferent and efferent branches of the central venous line at one hour. Serum samples from 28 voluntary blood donors were used as controls. Samples were centrifuged after 30 minutes, and serum aliquots were stored frozen at -70°C for later assay of cytokines. Interleukin (IL)-6 was analyzed by a chemiluminescent assay (Immulite 2000; DPC Biermann GmbH, Bad Nauheim, Germany). Enzyme-linked immunosorbent assay (ELISA) was used to measure the levels of IL-8, IL-10, tumor necrosis factor-alpha (TNF-α) (Quantikine^®; R&D Systems Inc., Minneapolis, MN, USA), and soluble TNF-α receptor 1 (sTNF-αR1) (BMS203CE; Bender MedSystems GmbH, Vienna, Austria). The methods were applied according to the manufacturers' recommendations. In brief, for IL-6, a solid-phase, enzyme-labeled, chemiluminescent sequential immunometric assay was performed. A 100-μl serum sample was added to the test tube containing an assay-specific coated bead and incubated at 37°C for 30 minutes. Unbound material was washed from the bead, and chemiluminescent substrate was added. Light emission was read with a high-sensitivity photon counter. For cytokine ELISA (IL-8, IL-10, TNF-α, and sTNF-αR1), analyte-specific antibodies (capture antibodies) were pre-coated onto a microplate. A 100-μl serum sample was added, and any analyte present was bound by the immobilized antibody. An enzyme-linked analyte-specific detection antibody then was bound to a second epitope on the analyte, forming the analyte-antibody complex. Substrate was added and optical density was read on a microplate reader.

Because cytokines are cleared from the plasma fraction of whole blood, plasma clearance (PlCl) rather than blood clearance was chosen. PlCl was calculated at one hour of treatment from paired afferent (a) and efferent (e) samples and from plasma flow. In treatments in which excess body water has to be removed by ultrafiltration, the concentration in the venous sample may be increased due to the effects of hemoconcentration on albumin and albumin-bound solutes. Failure to account for this will lead to an underestimation of PlCl. PlCl corrected for the effect of hemoconcentration was determined as follows: PlCl = [(1 - e/a) × Qp] + [UF × (e/a)], where Qp is plasma flow (Qp = blood flow × [1 - hematocrit], in milliliters per minute) and UF is ultrafiltration rate (in milliliters per minute).

Results are expressed as median (Q1; Q3) unless indicated otherwise. To analyze the relationship between variables, linear regression analysis was performed. Groups were compared by the Mann-Whitney test and, in the case of paired samples, by the Wilcoxon test. When more than two groups were compared, one-way analysis of variance with Dunnett T3 post hoc analysis was used. A p value less than 0.05 was considered statistically significant.