Acute Respiratory Failure Clinical Trial
Official title:
New Setting of Neurally Adjusted Ventilatory Assist During Postextubation Prophylactic Noninvasive Ventilation Through a Mask: a Physiologic Study
Non invasive ventilation (NIV) is generally delivered by pneumatically triggered and
cycled-off Pressure Support (PSP) through a facial mask. Compared to PSP, Neurally Adjusted
Ventilatory Assist (NAVA), which is the only ventilatory mode using a non-pneumatic signal,
i.e., diaphragm electrical activity (EAdi), to trigger and drive ventilator assistance,
improves patient-ventilator interaction. A specific setting to generate neurally controlled
Pressure Support (PSN) was recently proposed for delivering NIV by helmet. The investigators
here compare PSN with PSP and NAVA during NIV by facial mask, with respect to arterial blood
gases (ABGs), patient comfort, and patient-ventilator interaction and synchrony.
Three 30-minute trials of NIV were randomly delivered to 14 patients immediately after
extubation to prevent post-extubation respiratory failure: 1) PSP, with an inspiratory
support ≥8 cmH2O; 2) NAVA, adjusting the NAVA level to achieve a comparable peak EAdi
(EAdipeak) as during PSP; 3) PSN, setting the NAVA level at 15 cmH2O/mcV with an upper
airway pressure (Paw) limit such to obtain the same overall Paw applied during PSP. We
assessed EAdipeak, ABGs, peak inspiratory flow (PIF), time to reach PIF (PIFtime),
pressure-time product of the first 300 (PTP300-index) and 500 (PTP500-index) milliseconds
after initiation of patient effort, patient comfort, inspiratory trigger delay
(DelayTR-insp), and the rate of asynchrony, as assessed by the Asynchrony Index (AI%).
Non Invasive Ventilation (NIV) is increasingly used for treatment of Acute Respiratory
Failure (ARF) and is commonly applied through an oral-nasal mask by means of pneumatically
triggered and cycled-off Pressure Support (PSP). Although better tolerated than invasive
mechanical ventilation, NIV is characterized by drawbacks such as poor patient-ventilator
interaction and discomfort, which are major determinants of NIV failure.
In particular, the pneumatic signals, i.e., flow, volume and airway pressure (Paw), are leak
sensitive and frequently cause patient-ventilator asynchrony. The only mode that does not
use pneumatic signals to trigger and drive the ventilator is Neurally Adjusted Ventilator
Assist (NAVA). In fact, with NAVA the ventilator assistance is under control of diaphragm
electrical activity (EAdi), as assessed through an esophageal catheter. As opposed to PSP,
NAVA has been repeatedly shown to improve patient-ventilator interaction and reduce
asynchronies, both during invasive ventilation and NIV. However, NAVA is characterized by a
lower rate of pressurization than PSP.
Very recently, a specific NIV setting to generate a neurally, i.e., EAdi, controlled
Pressure Support (PSN) has been proposed and applied during both invasive ventilation and
NIV delivered via helmet. PSN consists in increasing the user-controlled gain factor (NAVA
level) at maximum, while restraining inspiratory Paw by adjusting on the ventilator the
upper pressure limit.
During NIV delivered through helmets, PSN has been shown, compared to both PSP and NAVA, to
result in better pressurization and triggering performance, which improve patient's comfort
while reducing EAdi, without affecting respiratory rate and arterial blood gases (ABGs). Due
to the different characteristics of helmets and masks, it is unclear whether these
advantages could be extended to NIV delivered by mask. The investigators therefore designed
this physiological study aimed at comparing PSN with PSP and NAVA, with respect to breathing
pattern, respiratory drive, ABGs, pressurization and triggering performance, patient's
comfort and patient-ventilator synchrony.
After patient enrollment, a nasal-gastric feeding tube able to detect EAdi (EAdi catheter,
Maquet Critical Care, Solna, Sweden) was placed and the correct positioning ascertained. The
study was performed using a Servo-I ventilator (Maquet Critical Care, Solna, Sweden)
equipped with a NIV software for air-leaks. The oral-nasal mask was individually selected
for each patients based on the anthropometric characteristics and in order to minimize air
leaks and optimize patient tolerance, among three different models, FreeMotion RT041 Non
Vented Full Face Mask (Fisher and Paykel, Auckland, New Zealand), Ultra Mirage FFM-NV
(ResMed, San Diego, CA, USA) and PerforMax Face Mask (Philips Respironics, Murrysville, PA,
USA).
All patients underwent three 30-minute trials in random order: 1) PSP, setting the
inspiratory pressure support ≥8 cmH2O to obtain a tidal volume of 6-8 mL•kg-1 of body
weight, the fastest rate of pressurization (0.0 sec) and I/E cycling at 35% of peak
inspiratory flow (PIF); 2) NAVA, adjusting the NAVA level in order to achieve a comparable
peak EAdi (EAdipeak) as during PSP with a safety Paw upper limit of 30 cmH2O; 3) PSN,
setting the NAVA level at its maximum (i.e; 15 cmH2O/mcV), and an upper Paw limit such to
obtain the same overall Paw applied during PSP. During both NAVA and PSN the trigger
sensitivity was set at 0.5 mcV while, the default cycling-off is 70% EAdipeak, as fixed by
the manufacturer. PEEP was set by the attending physicians in a range between 5 and 10
cmH2O, and left unmodified throughout the whole study period. The inspiratory oxygen
fraction (FiO2) was regulated to obtain peripheral oxygen saturation (SpO2) between 94% and
96%, before starting the protocol, and kept unmodified throughout the study period.
The three modes of ventilation were applied according to a computer-generated random
sequence using sealed, opaque numbered envelops. The envelopes were kept in the head of
nurses' office in both institutions. The envelope was opened by the nurse in charge of the
patient, and the sequence of modes to be applied communicated to the investigators.
Predefined criteria for protocol interruption were: 1) need for emergency re-intubation; 2)
SpO2 <90%, 3) acute respiratory acidosis, as defined by PaCO2 >50 mmHg and pH <7.30; 3)
inability to expectorate secretions; 4) hemodynamic instability (i.e.; need for continuous
infusion of dopamine or dobutamine >5 µg∙kg-1∙min-1, norepinephrine >0.1 µg∙kg-1∙min-1 or
epinephrine or vasopressin at any dosage to maintain mean arterial blood pressure >60 mmHg);
5) life-threatening arrhythmias or electrocardiographic signs of ischemia; or 6) loss of 2
or more points of GCS.
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