e., thrombotic thrombocytopenic purpura).[12] We hypothesized that VWF also compensates for qualitative or quantitative platelet abnormalities in patients with ALI/ALF. To test this hypothesis, we analyzed qualitative and quantitative parameters
of VWF and ADAMTS13 in a group of 50 patients with ALI/ALF in samples taken on admission to a single tertiary referral center. In addition, we used plasma of these patients in a model of primary hemostasis to examine the ability of VWF to support platelet adhesion under physiological flow conditions. Finally, given that the liver is the major source of ADAMTS13 synthesis, we anticipated reduced ADAMTS13 plasma levels with a consequent substantial unbalance between ADAMTS13 and VWF in these patients. A VWF/ADAMTS13 unbalance is a potential high-risk state
for unintentional platelet (micro)thrombus formation.[13] GDC-0973 manufacturer Emerging evidence from epidemiological, clinical, and animal studies indicates that intrahepatic activation of hemostasis and formation of microthrombi contributes to liver failure progression,[3, 4, 14] and ADAMTS13 and VWF have even been proposed as new predictors for outcome in patients with liver failure.[15-17] Therefore, we also see more explored possible relationships between VWF, ADAMTS13, and the outcome of patients with ALI/ALF in the present study. Fifty consecutive patients were prospectively studied after admission for acute liver injury/acute liver failure (ALI/ALF) to Virginia Commonwealth University Medical Center between March 2009 and May 2011. Patients’ details have been provided.[7] Informed consent was obtained from either the patient or their next-of-kin, depending on the patient’s level of altered mental status HSP90 (hepatic encephalopathy), as part of entry into the US Acute Liver Failure Study Group Registry. Patients with acute liver injury were defined as those with (1) an international normalized ratio (INR) of ≥ 1.5; (2) absence of a history of liver disease; and (3) illness of ≤26 weeks duration. Patients with
ALF were defined as those with ALI and hepatic encephalopathy. Patients who received procoagulant treatment other than vitamin K prior to enrollment were excluded. The INR was assayed using the Innovin reagent (Siemens Healthcare Diagnostics, Marburg, Germany), which has an international sensitivity index of 0.9. We calculated Model for End-Stage Liver Disease (MELD) scores according to the equation: [0.957 × loge (creatinine) + 0.378 × loge (bilirubin) + 1.12 × loge (INR) + 0.643] × 10, and determined whether patients fulfilled the King’s College criteria for acute liver failure as described.[18] Plasma samples from 40 healthy volunteers were used to establish reference values for the various tests performed in this study. Blood sample retrieval and processing have been described.