Recent data suggest

Recent data suggest Fluorouracil that adverse events (AEs) may be more common in real world practice than was observed in the registration studies, particularly in patients with cirrhosis1. The Australian experience in the use of these triple therapy regimens has not been previously

reported. In this study we present the combined experience of adverse events (AEs) associated with PI therapy at two large treatment centres in Melbourne. Methods: Treatment experience with TVR or BOC-based regimens at St Vincent’s Hospital Melbourne and Monash Medical Centre was collected in comprehensive HCV databases, including baseline patient characteristics, on-treatment virological responses and adverse events (AEs). Advanced liver fibrosis was defined as a composite of histology (METAVIR F3–4) and transient elastography (>9.5 kPa). We considered the following AEs: on-treatment anemia (endpoints – haemoglobin (Hb) reduction of >3 g/dL from baseline, Hb < 10 g/dL, RBV dose reduction, blood transfusion), clinically significant

rash (indicated by need for topical steroid treatment), treatment discontinuation, need for hospitalization, and death. Results: 150 patients have started DAA treatment (BOC, n = 80 and TVR, n = 70). Patients were older (mean 51 yrs), male (69%), and advanced fibrosis was common (50%). 34% had previously failed pIFN plus RBV therapy. No patient had Child-Pugh B or C cirrhosis. Baseline characteristics were similar for BOC and TVR-treated patients. At the time of submission, 64% remained on treatment. Adverse events were common. Comparison MAPK Inhibitor high throughput screening of the rates of anemia, anemia complications and rash are presented in Table 1.   BOC n = 80 TVR n = 70 Anemia Hb < 10 g/dL 35 (44%) 23 (33%) Hb reduction > 3 g/dL 62 (78%) 41 (59%) RBV dose reduction 26 (33%) 25 (36%) Transfusion 13 (16%) 10 (14%)

Rash Topical steroid 16 (20%) 40 (57%) Grade 4 0 2 (3%) Among BOC-treated patients, 10 (13%) patients stopped treatment due to AEs: severe depression (n = 2), refractory insomnia (n = 1), and profound lethargy (n = 7, only 1 of which CHIR-99021 concentration was associated with anemia), 3 patients were hospitalized for anaemia, infection in the setting of pancytopenia, and nausea and vomiting, respectively. Among TVR-treated patients, 7 (10%) discontinued due to AEs: 1 patient with severe anaemia (nadir Hb 79, 6 blood transfusions required in total) in the setting of cryoglobulinaemic myeloproliferative glomerulonephritis; 1 patient with grade 4 rash (DRESS syndrome); 1 cirrhotic patient developed a first hepatic decompensation event (spontaneous bacterial peritonitis requiring ICU admission); and 3 patients were hospitalised for symptomatic anaemia (fatigue and chest pain). 1 patient died from mucormycosis. 1 patient developed skin necrosis at a pIFN injection site 12 weeks after cessation of TVR and required a prolonged hospitalization . Conclusion: Treatment with PI-based triple therapy is challenging. Overall the rates of AEs were similar to those observed in the registration studies.

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