ble 1). The vast majority (89 ) of patients with active cancer received the suggested edoxaban dose according to prescribing data. At 1-year follow up, the annualized clinical occasion rate was 6.3 for recurrent VTE, eight.2 for ISTH MB (intracranial hemorrhage 0.6 , main gastrointestinal bleeding two.5 ). Malignancy-related deaths accounted for the majority of all-cause mortality (Table 2).Guy’s and St Thomas’ NHS Foundation Trust, King’s College London,London, United kingdom; 2Nakamura Health-related Clinic, Department of Internal Medicine, Pediatrics and Cardiology, Kuwana, Japan; 3Far Eastern Memorial Bax Inhibitor manufacturer Hospital, Cardiovascular Center, New Taipei City, Taiwan, Caspase 2 Activator custom synthesis Province of China; 4Yuan Ze University, Electrical Engineering, Taoyuan City, Taiwan, Province of China; 5Hanyang University Myongji Hospital, Division of Internal Medicine, Goyang-si, Korea, Republic of; Daiichi Sankyo Europe GmbH, Clinical Operations and Biostatistics and Information Operations, Munich, Germany; 7Daiichi Sankyo, Inc., Basking Ridge, United states; 8University of Perugia, Internal and Cardiovascular Medicine-Stroke Unit, Perugia, Italy Background: Active cancer is usually a significant threat factor for recurrent venous thromboembolism (VTE) and key bleeding (MB). The direct oral800 of|ABSTRACTTABLE 1 Baseline characteristics and medical historyAll Patients (N = 4,595) Age – yr, Mean (SD) Male gender, n ( ) Weight – kg, Imply (SD) Creatinine Clearance – mL/min, Mean (SD) VTE-BLEED score, imply (SD) HAS-BLED score, imply (SD) History of VTE History of bleeding History of big bleedingPatients with active cancer (n = 539) 66.9 (11.9) 233 (43.2) 61.8 (15.1) 82.0 (36.2) three.9 (1.three) 1.six (1.2) 40 (7.4) 47 (eight.7) 18 (three.3)Sufferers with no active cancer (n = 4,056) 64.six (15.9) 1,989 (49.0) 74.three (19.2) 88.eight (41.1) 1.six (1.three) 1.7 (1.two) 753 (18.6) 160 (3.9) 78 (1.9)64.9 (15.5) two,222 (48.4) 72.8 (19.2) 87.9 (40.six) 1.eight (1.5) 1.7 (1.two) 793 (17.3) 207 (4.five) 96 (2.1)Modified HAS-BLED score excluding labile INRTABLE 2 Annualized prices of clinical eventsData shown as /year, [95 CI] Recurrent VTE PE with or without having DVT DVT only Main bleeding (ISTH) Intracranial hemorrhage Big GI bleeding All-cause death Malignancy death Cardiovascular death All Sufferers (N = 4,595) three.09 [2.55; 3.70] 1.19 [0.87; 1.59] 1.99 [1.56; 2.49] two.44 [1.97; 2.99] 0.58 [0.36; 0.88] 0.66 [0.43; 0.97] 5.15 [4.45; five.92] 2.60 [2.11; three.17] 1.08 [0.77; 1.46] Patients with active cancer (n = 539) 6.33 [3.87; 9.77] two.81 [1.29; 5.34] four.39 [2.40; 7.36] 8.23 [5.37; 12.06] 0.62 [0.08; two.24] two.48 [1.07; 4.90] 31.89 [26.03; 38.67] 25.08 [19.92; 31.17] two.79 [1.27; 5.29] Sufferers with no active cancer (n = four,056) 2.79 [2.26; 3.41] 1.04 [0.73; 1.44] 1.76 [1.35; two.27] 1.91 [1.48; 2.43] 0.58 [0.35; 0.89] 0.49 [0.28; 0.78] two.67 [2.15; 3.27] 0.52 [0.31; 0.82] 0.92 [0.63; 1.30]Conclusions: Within the real-world international ETNA-VTE system, patients with active cancer had greater VTE and bleeding event rates than those without. Edoxaban demonstrated a security and effectiveness profile in sufferers with VTE and active cancer that may be constant together with the findings from prior randomized controlled trial.symptoms at IPE diagnosis (1). It stratifies individuals into low, intermediate and higher risk for adverse outcomes at 30, 90 and 180 days. Aims: To validate the HULL CPR inside a prospective cohort of ambulatory cancer sufferers with IPE derived in the similar clinical setting. Procedures: 284 consecutive patients managed below the IPE-acute oncology service in HUTH NHS trust from