Sigh in Acute Hypoxemic Respiratory Failure — PROTECTION  

Acute Respiratory Distress Syndrome Clinical Trial

Official title: PRessure suppOrT vEntilation + Sigh in aCuTe hypoxemIc respiratOry Failure patieNts (PROTECTION): a Pilot Randomized Controlled Trial

Status Completed

Clinical Trial Summary

Mortality of intubated acute hypoxemic respiratory failure (AHRF) and acute respiratory distress syndrome (ARDS) patients remains considerably high (around 40%) (Bellani 2016). Early implementation of a specific mechanical ventilation mode that enhances lung protection in patients with mild to moderate AHRF and ARDS on spontaneous breathing may have a tremendous impact on clinical practice. Previous studies showed that the addition of cyclic short recruitment maneuvers (Sigh) to assisted mechanical ventilation: improves oxygenation without increasing ventilation pressures and FiO2; decreases the tidal volumes by decreasing the patient's inspiratory drive; increases the EELV by regional alveolar recruitment; decreases regional heterogeneity of lung parenchyma; decreases patients' inspiratory efforts limiting transpulmonary pressure; improves regional compliances. Thus, physiologic studies generated the hypothesis that addition of Sigh to pressure support ventilation (PSV, the most common assisted mechanical ventilation mode) might decrease ventilation pressures and FiO2, and limit regional lung strain and stress through various synergic mechanisms potentially yielding decreased risk of VILI, faster weaning and improved clinical outcomes. The investigators conceived a pilot RCT to verify clinical feasibility of the addition of Sigh to PSV in comparison to standard PSV. The investigators will enrol 258 intubated spontaneously breathing patients with mild to moderate AHRF and ARDS admitted to the ICU. Patients will be randomized through an online automatic centralized and computerized system to the following study groups (1:1 ratio): - PSV group: will be treated by protective PSV settings until day 28 or death or performance of spontaneous breathing trial (SBT); - PSV+Sigh group: will be treated by protective PSV settings with the addition of Sigh until day 28 or death or performance of spontaneous breathing trial (SBT). Indications on ventilation settings, weaning, spontaneous breathing trial and rescue treatment will be specified.

Clinical Trial Description

Steering committee: Tommaso Mauri, Laurent Brochard, Jean-Michel Constantin, Giuseppe Foti, Claude Guerin, Jordi Mancebo, Paolo Pelosi, Marco Ranieri, Antonio Pesenti Statistical support: Carla Fornari and Sara Conti Specific aims This pilot RCT will serve to test the hypothesis that application of PSV+Sigh in spontaneously breathing intubated patients with mild to moderate AHRF and ARDS is feasible and to collect preliminary data on the safety of such an approach. Methods Study design. The investigators will conduct a pilot RCT on intubated spontaneously breathing patients with mild to moderate AHRF and ARDS admitted to the ICU. Ethics approval. The investigators will seek approval from the institutional review boards of each participating center prior to start of enrollment and consent/information will be obtained from each patient or next of kin following local regulations. Prevalence of Sigh responders. After enrollment, FiO2 will be titrated to obtain SpO2 of 90-96% and then each patient will first undergo a clinical test of PSV vs. PSV+Sigh to assess the prevalence of Sigh responders vs. non-responders in respect to improved oxygenation. After 30 minutes of clinical PSV+Sigh, SpO2/FiO2 ratio will be collected again to quantify the number of patients in whom it increased (i.e., "Sigh responders"). Randomization. After this test, patients will be randomized through an online automatic centralized and computerized system to the following study groups (1:1 ratio): - PSV group: will be treated by protective PSV settings until day 28 or death or performance of spontaneous breathing trial (SBT); - PSV+Sigh group: will be treated by protective PSV settings with the addition of Sigh until day 28 or death or performance of spontaneous breathing trial (SBT). PSV group settings. Initially, clinicians will set PSV to meet the following targets: tidal volume (Vt) of 6-8 mL/Kg of predicted body weight (PBW), with respiratory rate (RR) 20-35 bpm. In presence of Vt >8 ml/kg PBW and/or RR <20 bpm, PSV zero (CPAP) will be selected. FiO2 will be left as selected before the pre-randomization Sigh test, while PEEP will be left as clinically set. PSV+Sigh group settings. Similarly, PSV in this group will be set with the same protective targets of the PSV group (see above) and cyclic pressure control phase at 30 cmH2O for 3 seconds delivered once per minute (i.e., Sigh) will be added. PSV+Sigh is an easy to implement ventilation mode and, for the present study, the investigators will use high performance ICU ventilators already available in each clinical unit. Briefly, ventilators will be switched to biphasic positive airway pressure mode (e.g., BiPAP on Drager ventilators, SIMV-PC on Maquet and GE, DuoPAP on Hamilton) with the lower pressure level set at clinical PEEP and the higher pressure level set at 30 cmH2O with a 3-second inspiratory time and then a 57-second expiratory time. This Sigh rate of one per minute can be obtained by virtually all the already available high performance ICU ventilators, thus, even though a lower Sigh rate might be regarded as more physiological, we choose the 1/min rate for feasibility and costs related to the future large RCT. FiO2 will be left as selected before the pre-randomization Sigh test. Adjusting ventilation settings. In both groups, PSV will be adjusted at least every 8 hours in the following way: - PSV support will be decreased by 2 cmH2O step if Vt >8 ml/kg PBW and/or RR <20; - PSV support will be increased by 2 cmH2O step if Vt <6 ml/kg PBW and/or RR >35 and or signs of respiratory distress (e.g., marked use of the accessory muscles). - PEEP and then FiO2 will be increased by 2 cmH2O and 0.1 steps if SpO2 is <90%; - FiO2 and then PEEP will be decreased by 0.1 and 2 cmH2O steps if SpO2 is >96%; Sigh settings instead will be left unchanged until day 28, death or SBT. Switch to controlled mechanical ventilation. In both groups, switch to protective controlled ventilation will be allowed if patient will develop at least one of the following conditions: - PSV support >20 cmH2O; - PEEP ≥15 cmH2O; - unstable hemodynamic status (SBP <90 mmHg with vasoactive drug); - active cardiac ischemia (dynamic ST changes on cardiac monitor or electrocardiogram); - unstable arrhythmias (heart rate >140 or <40); - uncontrolled hypertension (SBP>180 mmHg); - abrupt decrease in the level of consciousness (RASS <-3); - dangerous agitation (RASS >+2); - pH <7.30; - PaO2/FiO2 ratio ≤100 mmHg; - necessity to perform diagnostic test (e.g., CT scan or bronchoscopy). Controlled ventilation will be set on volume mode with Vt 6-8 ml/kg PBW, RR to control pH, unchanged PEEP and FiO2. Controlled ventilation will be thereafter adjusted according to clinical evolution. Patients switched to controlled ventilation will be reassessed at least every 8 hours and they will be switched back to PSV or PSV+Sigh (to maintain study group assignment) targeting the abovementioned settings and adjustments as soon as all the following conditions will be met: - Patient is able to trigger ventilator breaths; - PaO2/FiO2 >100 mmHg; - PEEP <15 cmH2O; - pH ≥7.3; - Stable hemodynamic status with stable or decreasing doses of vasopressors for ≥6 hours. Rescue therapy. In case of desaturation (SpO2 ≤90%) of a patient it will be crucial to exclude hemodynamic impairment as a possible cause. Also, airway obstruction and ventilator malfunction must be ruled out as possible causes. Provided those factors are excluded, a rescue step-up strategy is allowed as follows: institution of protective controlled mechanical ventilation (see above for settings) and performance of recruitment maneuvers at 40-50 cmH2O, PEEP ≥15 cmH2O, prone positioning, inhaled nitric oxide, extracorporeal membrane oxygenation. Patients undergoing rescue treatments will be reassessed at least every 8 hours and switched back to PSV or PSV+Sigh (to maintain study group assignment) with the abovementioned settings and adjustments as soon as all the above mentioned conditions will be met. Spontaneous breathing trial (SBT). Patients with SpO2 ≥90% on FiO2 ≤0.4 and PEEP ≤5 cmH2O, no agitation, hemodynamically stable with norepinephrine ≤0.1 ug/kg/min or equivalent and at a stable or decreasing dose ≥6 hours and without any of the abovementioned criteria for switch to controlled ventilation will undergo a SBT: - For patients in the PSV group, the attending physician will perform the SBT directly. - For patients in the PSV+Sigh group, the attending physician will first withdraw Sigh, wait 60 min and confirm criteria: if confirmed, SBT will be performed; if not, Sigh will be reintroduced and clinical criteria will be checked again to repeat the procedure after at least 8 hours. SBT will last at least 60 minutes with a combination of PEEP 0-5 cm H2O and PSV 0-5 cm H2O. At the end of the 60 minutes, patient will fail the SBT if any of the following will be present: - criteria to start the SBT will not be confirmed; - sustained (>5 min) respiratory rate >35 bpm; - HR >140 bpm; - SBP >180 or <80 mmHg; - marked complaint of dyspnea; - increased somnolence with elevated pCO2 and/or pH<7.3 - a cough will not be strong enough to clear secretions - active cardiac ischemia (dynamic ST changes on cardiac monitor or electrocardiogram) - abrupt decrease in the level of consciousness with RASS <-3. Patients who will fail the SBT will be switched back to PSV or PSV+Sigh (to maintain study group assignment) and clinical criteria will be checked again to repeat the procedure after at least 6 hours. Patients who will pass the SBT will be extubated or, in the presence of tracheostomy, mechanical ventilation will be discontinued. If a patient will be re-intubated or mechanically ventilated through a tracheostomy again within 48 hours, PSV or PSV+Sigh (to maintain study group assignment) will be restored. If a patient will remain extubated or separated from the ventilator for >48 hours data collection only will continue. Reasons for re-intubation. After extubation, re-intubation should be promptly performed if at least one of the following criteria is present: - cardiac arrest; - respiratory arrest (respiratory pauses with loss of consciousness or gasping for air); - respiratory failure with SpO2 <90% and/or RR >35 bpm despite NIV; - decreased level of consciousness impairing ability to protect airway; - hemoptysis or hematemesis impairing ability to protect airway; - abundant secretions that cannot be effectively cleared or are associated with lobar collapse, acidosis, hypoxemia, or change in mental status; - surgical/invasive procedure requiring sedation/anaesthesia +/- neuromuscular blockade such that patient will no longer be able to sustain unassisted breathing; - hemodynamic instability with SBP <80 mmHg despite vasoactive drugs. Data collection At enrolment. Before the Sigh test, the investigators will anonymously collect patients' demographic information (e.g., age, sex, height, weight), past (e.g., hypertension, chronic medications) and recent (e.g., etiology of the acute respiratory failure, days since intubation) medical history, severity of lung injury (e.g., ventilation setting, arterial blood gases, respiratory system compliance, diagnosis of ARDS) and of systemic diseases (e.g., presence of shock, number of organs failure), ventilation settings (e.g., PEEP, FiO2, PSV level). After the Sigh test. Then, the investigators will collect SatO2/FiO2 change in response to the pre-randomization Sigh test. First 24 hours from randomization. In both groups for the first 24 hours the investigators will assess every 4 hours the SpO2/FiO2 ratio, RR and tidal volume delivered both during protective PSV and during Sigh to further characterize physiologic response to Sigh over time. Daily. From day 1 (i.e., within 24 hours from enrollment) to day 28 or death or discharge from the ICU, the following data will be collected every day between 6:00 and 10:00 in the morning: switch from the allocated treatment to the other study arm for ≥24 hours, reason for switch from the allocated treatment, adverse events (i.e., hemodynamic instability with hypotension with SBP <90 mmHg despite vasoactive drugs; arrhythmias with heart rate <40 or >140 bpm; radiographic evidence of barotrauma with pneumothorax, pneumomediastinum, pneumatocoele, or subcutaneous emphysema), arterial SpO2, arterial and central venous blood gas analyses, numbers of quadrants involved on standard chest X-ray, ventilation settings and pattern (i.e., Sigh pressure level, Sigh tidal volume, PSV level, PSV tidal volume, respiratory rate, PEEP, FiO2, minute ventilation, P0.1, mean airway pressure), switch to controlled ventilation for ≥24 hours, reason for switch to controlled ventilation, use of rescue treatments (i.e., use of PEEP ≥15 cmH2O, prone positioning, inhaled nitric oxide, extracorporeal membrane oxygenation), dosage of sedative agents, RASS value, tracheostomy, patient's comfort through visual analog scale, heart rate, arterial blood pressure, central venous pressure, dosage of vaso-active drugs, cumulative fluid balance, SOFA score, SBT failure in the previous 24 hours, reason for SBT failure, time since extubation or separation from mechanical ventilation, time since re-intubation, reason for re-intubation. Day 28. At day 28, for all enrolled patients, mortality and ventilator-free days will be collected. Ventilator-free days will be calculated as 28 minus the number of days between intubation and successful extubation or separation from mechanical ventilation for tracheostomized patients (i.e., for ≥48 hours). ;

Related Conditions & MeSH terms

• Acute Lung Injury
• Acute Respiratory Distress Syndrome
• Respiratory Distress Syndrome, Adult
• Respiratory Distress Syndrome, Newborn
• Respiratory Failure
• Respiratory Insufficiency
• Ventilator Lung

• NCT number: NCT03201263
• Study type: Interventional
• Source: Fondazione IRCCS Ca' Granda, Ospedale Maggiore Policlinico
• Status: Completed
• Phase: N/A
• Start date: December 20, 2017
• Completion date: May 9, 2019