Panigrahi / Bhattacharjee / Muthukumar Neurosurgery Updates, Vol. 3

2
Mechanical Ventilation and Weaning in the Brain-Injured Patient
Ann Campos and Harsh Khandelia
Introduction Weaning Off Mechanical Ventilation Conclusion 2 Mechanical Ventilation and Weaning in the Brain-Injured Patient Ann Campos and Harsh Khandelia Introduction Clinical guidelines for mechanical ventilation and subsequent weaning in patients with injury to the brain are debatable and not clearly understood, as brain-injured patients have always been excluded from trials on mechanical ventilation and acute respiratory distress syndrome (ARDS). However, in 2020, the European Society of Intensive Care Medicine1 suggested preliminary clinical practice recommendations based on the findings of an international consensus panel. Etiology for acute brain injury (ABI) is multifactorial. ABI could be due to varied causes such as intracranial hemorrhage (ICH), subarachnoid hemorrhage (SAH), large strokes, and trauma. Irrespective of the cause of injury (Flowchart 2.1), there is usually a catecholamine surge and release of inflammatory mediators from the injured brain tissue, which makes the lungs susceptible to injury, due to altered alveolar capillary permeability and decreased macrophage activity. This can lead to hypoxia and hypercarbia as well as release of neuroinflammatory mediators from the injured lung, which in turn can result in secondary brain injury.2 Therefore, early identification of lung injury and use of mechanical ventilation forms an important aspect of breaking this chain of events. Flowchart 2.1 Brain–lung crosstalk. SIRS, systemic inflammatory response syndrome. The main indications for mechanical ventilation in ABI are the following: •Respiratory insufficiency secondary to seizures, lung injury due to trauma, ARDS, neurogenic pulmonary edema or cardiovascular insufficiency, and depressed brainstem reflexes. •Loss of protective airway reflexes which may lead to aspiration. •As an adjunct to reduce raised intracranial pressure (ICP).3 Although mechanical ventilation helps in oxygenation and controls CO2 levels, it can have some unwanted effects on the brain. Since cerebral perfusion is the difference between mean arterial pressure (MAP) and ICP, that is, cerebral perfusion pressure (CPP) = MAP – ICP, factors that alter MAP or ICP can alter cerebral perfusion. During mechanical ventilation, positive pressure applied to the lungs in inspiration increases intrathoracic pressure with resultant reduction in venous return to the heart. This leads to a drop in cardiac output and subsequent fall in MAP with a consequent reduction in CPP. Obstruction of venous return from the brain via the jugular veins results in an increase in ICP, which also causes reduced CPP. A 30-degree head-up position, therefore, can aid jugular venous drainage by gravity4 (Flowchart 2.2). Additionally, use of large tidal volumes and high airway pressures while ventilating these patients has been shown to cause ventilator-induced lung injury (in the form of volutrauma, atelectotrauma, and biotrauma) and worsen outcomes. Hence, there is a need to use lung protective ventilation strategies like low tidal volumes and some positive end-expiratory pressure (PEEP).5 Flowchart 2.2 Mechanical ventilation–brain interaction. CPP, cerebral perfusion pressure; ICP, intracranial pressure; MAP, mean arterial pressure; VR, venous return. In ARDS, use of lung protective ventilation with low tidal volumes and high PEEP often results in increased CO2 levels, which is termed permissive hypercapnia and is acceptable as long as the pH of blood is maintained above 7.2. The hypercapnia that is permitted in lung protective ventilation, however, is likely to cause cerebral vasodilation and an increase in ICP. Use of high PEEP can also adversely impact cerebral perfusion due to a reduction in venous return to the heart. This can be quite detrimental in the brain-injured patient.1 The ventilatory strategy in ABI should be aimed at achieving normal oxygen and carbon dioxide levels while maintaining cerebral perfusion and minimizing lung injury.6 When the patient is first connected to the ventilator, the FiO2 or oxygen level should be set at 100% and reduced to below 60% as soon as feasible. The minimum oxygen concentration needed to maintain a PaO2 of 80 to 120 or SpO2 between 94 and 98% should be aimed for. Prolonged hyperoxemia (>200 mm Hg) not only has harmful effects on all organs but is also associated with increased mortality, so it must be avoided. CO2 levels can be controlled by changing minute ventilation (minute ventilation = tidal volume × respirator rate). It is recommended to use low to intermediate tidal volumes (6–8 mL/kg ideal body weight [IBW]) and adjust the respiratory rate (12–15/min) to achieve a PaCO2 between 35 and 45 mm Hg. A target PaCO2 between 30 and 35 mm Hg may be used temporarily, only as a rescue measure when ICP is very high.1 Prolonged hypocapnia causes cerebral ischemia and reduces chances of recovery. End tidal CO2 may be used to monitor CO2 levels noninvasively due to its good correlation with arterial CO2 if the patient does not have severe lung disease and is not in shock or hypovolemic. PEEP has been shown to have a beneficial effect on brain oxygenation and also prevents excessive overdistension of alveoli.5 PEEP is considered safe under the following conditions: •The hemodynamic status and euvolemia are maintained in order to minimize the effects of PEEP on cerebral perfusion pressure (via a decrease in MAP). •Value of PEEP is lower than ICP, to avoid a decrease in venous outflow. PEEP can decrease cerebral perfusion only if there is hypovolemia. Physiological PEEP of 3 to 5 cm prevents atelectasis. Optimal PEEP is targeted based on lung mechanics and the PaO2/FiO2 ratio. Zero end-expiratory pressure, which was the earlier norm, is no longer recommended.1 Usual levels of PEEP can be used in ABI with or without ARDS, if ICP is not elevated or where ICP is PEEP insensitive (usually when lung compliance is low). When ICP is elevated, PEEP will need to be carefully titrated according to lung mechanics and with close monitoring of ICP. It is important to keep plateau pressures <30 in order to avoid barotrauma. Due to loss of cerebral autoregulation in the injured brain, adequate hydration and use of inotropes may be needed to keep the MAP between 80 and 85 mm Hg in order to maintain CPP above 60 mm Hg in the presence of raised ICP. There is no clear consensus on the use of recruitment maneuvers in ABI as they can increase ICP. They may be of benefit in refractory hypoxemia in patients having both lung and brain damage. However, they must be done under strict multimodal neuromonitoring. Thus, the PaO2, PCO2, MAP, and ICP of the brain-injured patient should be closely monitored during mechanical ventilation.1 Although COVID-19 has generated a renewed interest in proning patients with ARDS, a systematic literature review indicates that there are changes in physiology. These changes are limited, and prone ventilation is not contraindicated in the presence of moderate to severe ARDS, where benefits of hypoxia correction outweigh the risks involved. Spinal instability and open chest are absolute contraindications for proning. Although the prone position in ABI can be challenging and associated with an increase in ICP, it remains an option when we consider the negative effects of hypoxemia on the brain.7 With limited neurological examination, special monitoring like continuous electroencephalogram (EEG), ICP, brain tissue oximetry, and transcranial Doppler (TCD) can be used.8 Weaning Off Mechanical Ventilation Weaning is the gradual process of liberating the patient from the ventilator. Weaning is started once the patient is hemodynamically stable, has spontaneous respiration, and is on minimal or no sedation. During weaning, the patient should first be put on an assisted or support mode of ventilation. The FiO2, respiratory rate, and pressure support should be slowly reduced over time, ensuring that O2 and CO2 levels are maintained without signs of respiratory distress.9,10 Once the patient is comfortable with minimal ventilator supports, a spontaneous breathing trial (SBT) for 30 minutes can be instituted. If the patient fails the trial, the ventilator support can be increased. A low Glasgow Coma Scale (GCS) score is not a contraindication to weaning. The next step after a successful SBT is extubation. This can present a dilemma in these patients, as they may be unable to protect their airway or their neurological status may be impaired. Since it may be difficult to apply all the usual extubation criteria in this group of patients, other scores have been developed. In an analysis by Asehnoune et al,11 a total of 3 out of 4 on the VISAGE (visual pursuit, swallowing, age, Glasgow for extubation) score (Box 2.1) based on age < 40 years, GCS > 10, visual pursuit, and swallowing resulted in a successful extubation in 90% of patients. The airway care score (ACS; Table 2.1), which focuses on the presence of cough and gag reflex as well as the amount and quality of tracheal secretions, predicted successful extubation in those who scored less than 7.9 Box 2.1 VISAGE score11 •Age <40...