ASpirin for Patients With SEPsis and SeptIc Shock (ASP-SEPSIS)

Impact of Aspirin Use on the Severity of Organ Dysfunctions in Patients With Sepsis and Septic Shock: a Randomized, Double-blind, Placebo-controlled Trial - ASP-SEPSIS.

Terminated: The study was stopped prematurely and will not be resumed due to the higher number of bleeding cases in the intervention group, as recomended by the Data Safety Monitoring Board on February 7, 2023.

This Randomized, pragmatic, multicentric with blinding of patients and health professionals, intention-to-treat analysis has by primary endpoint to evaluate whether the aspirin use reduces the intensity of organic dysfunction measured by the variation of the SOFA score starting from the day of admission to the seventh day. Secundary endpoint: To evaluate if the aspirin use reduces the time of mechanical ventilation, length of stay in the ICU and in the hospital. In addition, to evaluate the safety of its administration regarding the occurrence of bleeding. The data will be collected directly from the chart of the patients admitted to the ICU. Data quality assurance will be made through periodic verification, aiming for complete and consistent data. The centers will receive periodic reports for adequacy of potentially inconsistent or incomplete data. The baseline SOFA of patients with sepsis is 8.8 with a standard deviation of 3. The expected reduction in the control group in the SOFA at day 7 is 2 points. Considering a power of 80% and a level of significance of 0.05, it is estimated that 109 patients will be needed in each group. A total of 218 patients will compose the sample. All analyzes will follow the intention-to-treat principle. We will evaluate the effect of aspirin compared to placebo on primary and binary outcomes by means of relative risks, 95% confidence intervals and chi-square tests. For continuous outcomes with normal distribution, we will present the mean difference, 95% confidence interval and P value calculated by t test. For continuous outcomes with asymmetric distribution, we will perform Wilcoxon test.

Design Randomized, pragmatic, multicentric with blinding of patients and health professionals. Bias control Allocation secrecy with web randomization. Blinding of patients and health professionals. Intention-to-treat analysis. Primary endpoint To evaluate whether the aspirin use reduces the intensity of organic dysfunction measured by the variation of the SOFA score starting from the day of admission to the seventh day. Secondary endpoint To evaluate if the aspirin use reduces the time of mechanical ventilation, time with vasopressors, time in renal replacement therapy, length of stay in the ICU and in the hospital. In addition, to evaluate the safety of its administration regarding the occurrence of bleeding. Eligibility Inclusion criteria: The three criteria below must be present: Signature of informed consent Patients must be older than 18 years old Diagnosis of sepsis and/or septic shock for less than 48 hours with at least one of the following organ dysfunctions: Lactate above 4mmol/L (36mg/dL) Thrombocytopenia < 100,000/mm3 or reduction > 50% in the count in the last 3 days PaO2/FiO2 < 200 without signs of apparent volume overload Hypotension MAP < 65mmHg refractory to volume replacement with the need to use vasopressor Exclusion Criteria: Pregnancy Impossibility to use the intestinal tract Death perspective in less than 24 hours Patients in the end of their lives or in exclusive palliative care Patients with active bleeding Prior study participation Known allergy to aspirin Active peptic ulcer Previous use of antiplatelet agents in the last 7 days Previous use of AINEs in the last 7 days, except for dipyrone. Hemorrhagic stroke in the last 7 days or central nervous system surgery in the last 72 hours. Platelets <30,000 cells/mm3. Large surgery in the last 24 hours if the attending surgeon judges that the risk of bleeding is high enough that aspirin cannot be used. Ophthalmologic surgery postoperative and transurethral resection of the prostate at the discretion of the attending physician. Hepatic cirrhosis or previous liver disease with altered prothrombin activity, manifested by INR above 2.0 or other previous coagulopathies. Severe head injury in the last 7 days. Use or indication of anticoagulation. Study intervention The treatments to be compared in the study are a dose of 200 mg of aspirin daily for 7 days and placebo. Both look identical. Study outcomes Primary outcomes: • Variation of the SOFA score between D7 and D1 Secondary outcomes: Death in the ICU Days free of mechanical ventilation within 28 days Days free of vasopressor within 28 days Length of ICU stay Length of hospital stay Renal injury KDIGO >= 2 within 7 days Renal replacement therapy use Major bleeding occurency Count of unitis of red blood cells received in 14 days Data management The data will be collected directly from the chart of the patients admitted to the ICU. Data quality assurance will be made through periodic verification, aiming for complete and consistent data. The centers will receive periodic reports for adequacy of potentially inconsistent or incomplete data. Statistics The baseline SOFA of patients with sepsis is 8.8 with a standard deviation of 3. The expected reduction in the control group in the SOFA at day 7 is 2 points. Considering a power of 80% and a level of significance of 0.05, it is estimated that 109 patients will be needed in each group. A total of 218 patients will compose the sample.

Difference between the Sequential Organ Failure Assessment (SOFA) Score on the seventh day of ICU stay and baseline (DeltaSOFA D7-D1).

To evaluate whether the aspirin use reduces the intensity of organic dysfunction. measured by the variation of the SOFA score starting from the day of admission to the seventh day. The Sequential Organ Failure Assessment (SOFA) Score ranges between 0 and 24.

To evaluate if the aspirin use reduces the time of mechanical ventilation, that ranges between 0 and 28 days.

To evaluate if the aspirin use reduces the days using vasoressors, that ranges between 0 and 28 days.

Eligibility - patients: Inclusion criteria: The three criteria below must be present: Signature of informed consent Patients must be older than 18 years old Diagnosis of sepsis and/or septic shock for less than 48 hours with at least one of the following organ dysfunctions: Lactate above 4mmol/L (36mg/dL) Thrombocytopenia < 100,000/mm3 or reduction > 50% in the count in the last 3 days PaO2/FiO2 < 200 without signs of apparent volume overload Hypotension MAP < 65mmHg refractory to volume replacement with the need to use vasopressor Acute renal injury increased by 2.0 to 2.9 times from baseline or diuresis rate less than 0.5ml/kg/h for more than 12 hours Exclusion Criteria: Pregnancy Impossibility to use the intestinal tract Death perspective in less than 24 hours Patients in the end of their lives or in exclusive palliative care Patients with active bleeding Prior study participation Known allergy to aspirin Active peptic ulcer Previous use of antiplatelet agents in the last 7 days Previous use of AINEs in the last 7 days, except for dipyrone. Hemorrhagic stroke in the last 7 days or central nervous system surgery in the last 72 hours. Platelets <30,000 cells/mm3. Large surgery in the last 24 hours if the attending surgeon judges that the risk of bleeding is high enough that aspirin cannot be used. Ophthalmologic surgery postoperative and transurethral resection of the prostate at the discretion of the attending physician. Hepatic cirrhosis or previous liver disease with altered prothrombin activity, manifested by INR above 2.0 or other previous coagulopathies. Severe head injury in the last 7 days. Use or indication of anticoagulation