Lanari-IDIM,

University of Buenos Aires–National Council of Scientific and Technological Research (CONICET), Buenos Aires, Argentina. “
“Patients with cirrhosis PARP inhibitors clinical trials are at risk of developing acute portal vein thrombosis (PVT). Anticoagulation for at least 3 months is generally recommended for recanalization to avoid intestinal infarction and worsening of portal hypertension.[1] Generally, unfractionated heparin or low molecular weight heparin is initiated with subsequent transition to oral anticoagulation with warfarin.[1] Unfortunately, warfarin is limited by a narrow therapeutic window and a highly variable dose-response requiring frequent dose adjustments and monitoring. Rivaroxaban is the first oral anticoagulant agent available within the class of factor Xa inhibitors and is approved for use in prevention or treatment of stroke, deep vein thrombosis, and pulmonary embolism.[2] The efficacy of rivaroxaban for treatment of PVT was recently evaluated in a single patient with complete resolution in 4 weeks.[3] We report a case of acute PVT extending Olaparib to the superior mesenteric vein (SMV) in a patient with cirrhosis that required 6 months of therapy with rivaroxaban for complete resolution. A 50-year-old white man with extreme

obesity, heart failure, hypertension, diabetes mellitus type 2 (Hgb A1C 6.4%), and obstructive sleep apnea presented with acute abdominal pain of 1 day duration. His physical exam showed normal vital signs; his weight and height were 187 kg and 203 cm, respectively (body mass index [BMI] 46.7 kg/m2); he had periumbilical tenderness with no this website rebound tenderness or ascites. His blood work was essentially normal (serum creatinine

0.6 mg/dL, international normalized ratio [INR] 1.1) with the exception of thrombocytopenia (platelet count of 66,000/mm3). A computed tomography (CT) of his abdomen showed cirrhotic liver, PVT, MVT, and thickened small bowel loops (Fig. 1A). An upper endoscopy revealed small esophageal varices. A diagnosis of nonalcoholic steatohepatitis related to Child-Pugh Class A cirrhosis (Model for Endstage Liver Disease [MELD] 12) complicated by acute PVT and MVT was made after workup for competing etiology. He was initiated on unfractionated heparin given intravenously with subsequent transition to oral rivaroxaban 20 mg per day. Genetic testing for JAK2 mutations for occult myeloproliferative syndromes was negative. Follow-up CT scan at 4 months (Fig. 1B) showed partial resolution of the clot and rivaroxaban was continued at the same dose. At the 6-month visit, a repeat CT scan showed complete resolution of the clot (Fig. 2A,B). During the follow-up visits, the patient did not report any adverse events including bleeding. Serum creatinine levels were obtained at the time of each imaging study and they were in the normal range.