Carbon Dioxide (CO₂)

Although peripheral CO₂ receptors contribute to CO₂‐induced ventilatory responses, the primary CO₂‐/pH‐sensitive chemoreceptors are located in the CNS throughout the brainstem (i.e., retrotrapezoid nuclei, serotonergic raphe neurons, noradrenergic neurons in the locus coeruleus, nucleus of the solitary tract, pre‐Bötzinger complex, etc.) [7]. These chemoreceptors are extremely sensitive and even small deviations from a normal PaCO₂ level affect ventilation linearly and dramatically.

CO₂ diffuses rapidly from tissues into red blood cells where it forms bicarbonate according to the reaction: CO₂ + H₂O ↔ H₂CO₃ ↔ H⁺ + HCO₃⁻. The first reaction is slow in plasma, but rapid inside the red cell due to the presence of carbonic anhydrase. CO₂ is then transported mostly as bicarbonate (approximately 81%) with a small amount dissolved in plasma (approximately 8%) and combined with amino groups of blood proteins (approximately 11%) [4].

As previously mentioned, in the steady‐state, PaCO₂ is inversely proportional to V&c.dotab;_A based on the alveolar ventilation equation:

(2.2)

is the metabolic production of CO₂ and 0.863 is a constant that corrects for dissimilar units. CO₂ is approximately 20–24 times more diffusible than oxygen; as such, there is complete equilibration across the alveolar membrane under normal situations. Thus, the PaCO₂ is essentially the same as the PACO₂ (within a few mmHg, primarily due to a small amount of dead‐space ventilation) in healthy animals. However, these values may significantly diverge in the presence of pulmonary disease states such as profound ventilation–perfusion inequalities or pulmonary shunting.

Overall ventilation is a measure of the animal’s ability to regulate the level of CO₂ within the body; it is the only route for elimination. Adequate ventilation is present when CO₂ is maintained at an optimal partial pressure in arterial blood (Table 2.1) [11, 15, 17]. Accordingly, hyperventilation occurs when V&c.dotab;_A is increased and the resultant PaCO₂ falls below normal values, while hypoventilation is defined as a reduction in V&c.dotab;_A, increasing PaCO₂ values from normal. Although blood gas analysis is the definitive way to assess the adequacy of ventilation, noninvasive technology such as the use of end‐tidal CO₂ (ETCO₂) capnometers has become increasingly popular in small‐animal (as well as exotic‐animal) practice, since they closely approximate alveolar CO₂ levels under normal situations and can be easily used in most species (Figure 2.4). Since capnometry relies on adequate cardiac output to return CO₂ to the lungs, as well as pulmonary function to eliminate CO₂ from the body, it is an essential piece of equipment in any case where respiratory impairment or dysfunction is a concern and should become a routine monitor for any veterinary practice [18].

Oxygen

Once oxygen is carried from the conducting airways to the respiratory exchange tissues (respiratory bronchioles and alveoli), it quickly diffuses into the blood where it is carried both dissolved in solution and bound to hemoglobin (Hb). Approximately 1.36–1.39 ml of O₂ can combine with 1 g of hemoglobin compared to only a small amount that is dissolved in blood (0.003 ml per 100 ml blood per mmHg PO₂) [4, 19]. The total oxygen content of blood (CaO₂) is therefore calculated as: CaO₂ = (1.39 × Hb × SaO₂) + (0.003 × PaO₂), where SaO₂ is the oxygen saturation of Hb. Thus, the amount combined with Hb impacts CaO₂ to a greater extent than does the dissolved amount, and altered Hb levels (i.e., anemia) will have a profound effect on not just CaO₂ but oxygen delivery (DO₂) to the tissues, since DO₂ = CaO₂ × cardiac output. However, in an anemic animal, the dissolved portion plays an increasing important role; increasing PaO₂ (through enriching inspired O₂ levels, for example) will be advantageous to these patients.

As determined by the oxygen–Hb dissociation curve, the amount of O₂ carried by Hb increases rapidly until PO₂ reaches approximately 60–70 mmHg where the curve flattens off (Figure 2.5). Many factors affect the curve placement including temperature, PCO₂, pH, and 2,3‐diphosphoglycerate (2,3‐DPG) levels, an enzyme which competes with O₂ for its binding site on Hb (Figure 2.5). Hemoglobin is normally nearly 100% saturated in healthy patients breathing room air (approximately 21% O₂) and should always be above 90–95% [20]. In most normal anesthetized patients, the PaO₂ is very high due to 100% O₂ used as a carrier gas for the inhalant (frequently >500 mmHg; Table 2.1). As per the oxygen–Hb dissociation curve, a very high percentage of Hb will therefore be bound with O₂. Since arterial blood gas analysis may not be available to every practitioner, pulse oximetry is a standard, yet indirect measure of oxygenation in anesthetized dogs and cats which measures pulse rate and estimates the Hb oxygen saturation (termed SpO₂; Figures 2.4 and 2.6) [21]. However, one must be cautious, since significant pathology must exist in the anesthetized patient administered 100% oxygen for the PaO₂ to drop to a level where the pulse oximeter will alert the anesthetist; a PaO₂ of approximately 60 mmHg corresponds to an SpO₂ of approximately 90%, and a PaO₂ of approximately 80 mmHg corresponds to an SpO₂ of approximately 95%. In addition, pulse oximetry does not indicate if adequate ventilation is present to remove CO₂, since the pulse oximeter only estimates the percentage of Hb saturation with O₂. Although this monitor has become one of the most widely used anesthetic monitors for a variety of species in veterinary medicine (Figures 2.4, 2.6, and 2.7), it provides little information concerning the animal’s ventilatory status during anesthesia unless severe pathology is present and should be used with care.

Hypoxemia (low PaO₂) is commonly encountered in patients with respiratory impairment and is primarily due to one of the five reasons: low inspired O₂ fraction, hypoventilation, diffusion impairments, ventilation–perfusion mismatching, and right‐to‐left shunts (cardiac or pulmonary). Discerning between these causes is sometimes difficult. However, some information can be obtained from the alveolar gas equation which predicts that the arterial (a) or alveolar (A) O₂ tension will decrease with an increase in PCO₂: PAO₂ = PIO₂ − (PACO₂/R), where PIO₂ is the inspired O₂ level and R is the respiratory exchange ratio (approximately 0.8 in normal animals). The difference between alveolar and arterial oxygen levels is defined as the (A‐a) gradient. Substituting PaCO₂ for PACO₂, the (A‐a) oxygen gradient equation becomes: (A‐a) gradient = PAO₂ − PaO₂ = (PIO₂ − 1.25PaCO₂). Generally, values between 5 and 15 mmHg in animals breathing room air are considered normal [4].

Hypoxemia due to low inspired O₂ levels (i.e., low atmospheric pressure, use of nitrous oxide without appropriate O₂ flows) does not usually result in increased (A‐a) O₂ gradients, since frequently there is a subsequent increase in V&c.dotab;_A (thus, decreasing PaCO₂) secondary to hypoxemia. In addition, if hypoxemia is solely due to hypoventilation, the PAO₂ and PaO₂ decrease, while the PaCO₂ and PACO₂ must increase and the (A‐a) difference should not change. However, in the case of ventilation–perfusion abnormalities or right‐to‐left shunting (both very common during anesthesia), the (A‐a) gradients are significantly elevated. These two are differentiated from each other, as administration of 100% O₂ to patients with ventilation–perfusion abnormalities significantly increases the PaO₂, whereas PaO₂ levels fail to return to normal in patients with significant shunting, as blood traverses across the lungs or through the heart and does not pick up the oxygen [4].

Interactions Between CO₂ and O₂ Transport

Although management of CO₂ and O₂ within the body appears independent, they are not mutually exclusive of each other [9]. For example, acidity (lower pH) associated with carbonic acid produced from CO₂ in tissues promotes O₂ release from Hb with no change in dissolved oxygen levels, whereas CO₂ release from the lungs promotes oxygen uptake; this is known as the Bohr effect. In addition, the Haldane effect states that deoxygenation of Hb causes Hb to become a weaker acid, this increases its ability to carry hydrogen ions [9].

Ventilatory Cycle

Normally, there are three ventilatory cycle phases: inspiration, expiration, and an expiratory pause (which are important to understand in evaluating breathing or during adjustments of ventilatory support). Inspiratory pauses are not normally present in conscious dogs and cats. Expiration, in most cases, is a passive process related to the elastic recoil of the chest. One exception is the horse in which expiration normally has an active phase even at rest [22]. The respiratory cycle is primarily changed by adjustments of the “pause” phase of the cycle. Ventilatory rates are usually increased by decreasing the pause time between each inhalation and exhalation. For mechanical ventilation, adjustment of the inspiratory to expiratory ratio (I:E) is possible and is important when changing the respiratory rate (Figure 2.8). As a guideline, the inspiratory time should be less than or equal to the expiratory time. Thus, the I:E ratio will be at least 1:1, but may vary to a ratio as high as 1:5. For example, if inspiratory time is kept at 1–2 s in duration and the respiratory rate is 10 breaths min⁻¹, then the I:E ratio will be between 1:5 and 1:2. Typically, the I:E ratio is usually not less than 1:1, which allows adequate time for lung filling and emptying.

Ventilatory Support with Intermittent Positive Pressure Ventilation (IPPV)

Mechanical ventilation differs significantly from spontaneous ventilation. Normally, air enters the respiratory system because of contraction of inspiratory intercostal muscles and the diaphragm. During normal inspiration, the change in alveolar pressure is only about 1 cm of water pressure [23]. However, IPPV is not a “normal” situation for the animal, as positive pressure is “forced” into the lungs; too much pressure can result in detrimental effects such as reducing cardiac output, volutrauma, barotrauma, etc. (Figure 2.9) [24].

Ultimately, the concern with IPPV is that intermittent high thoracic pressures can lead to tissue perfusion failure. For example, although during the positive pressure breath, pressurization of chest can augment cardiac ejection, increased intrathoracic pressure often exceeds central venous pressure, resulting in a decrease in venous return to the heart. The resulting decrease in ventricular filling may reduce cardiac output on the subsequent heartbeat and often decrease systolic arterial pressure [24]. To minimize the negative effects of IPPV, the inspiratory time should be kept short and should not exceed 2–3 s. Additionally, the lowest peak inspiratory pressure (PIP) capable of inflating the lungs should be used. In many animals, a PIP of less than 15 cmH₂O will be sufficient to fully inflate the lungs. In mammals, the guideline is to keep the PIP below 20 cmH₂O; for reptiles and birds the guideline is a maximum of 15 cmH₂O [25]. In animals with normal thoracic compliance, if PIP is set to approximately 10 cmH₂O, respiratory rate is approximately 10 breaths min⁻¹, and V_T is approximately 10–15 ml kg⁻¹, the PaCO₂ frequently approaches normal levels; minor adjustments can then be made to achieve the precise, desired PaCO₂ for the patient.

Because of the aforementioned concerns, mechanical ventilation may not be warranted in every patient. If the patient is healthy, having a short procedure (<1h), does not display airway obstruction, is not apneic, and is oxygenated, mild‐to‐moderate hypercapnia is usually well tolerated. However, ventilatory support should be available to all animals during general anesthesia and can include assisted “hand ventilation” by an anesthetist or the use of mechanical ventilation. This is because multiple factors contribute to an inability to adequately ventilate including drug‐induced respiratory depression, age, body weight, and preexisting disease. Ventilation not only ensures that the patient is oxygenated and CO₂ is removed, but also ensures consistent delivery of anesthetic gases. Delivery, maintenance, and recovery from inhaled anesthetics uniquely depend on the movement of the agents through the lungs. Consistent and effective ventilation with controlled or assisted ventilation makes inhalant anesthesia both more precise and easier to perform. However, if the goal is to keep PaCO₂ or ETCO₂ at normal levels, consistent ventilation must occur, as CO₂ levels quickly rise when ventilation is stopped, even for a few minutes. Any patient can benefit from effective ventilatory support; however, in the patient with preexisting respiratory disease, it is essential.

Opioids

Many pure opioid analgesics depress minute ventilation via effects at mu‐opioid receptors near and pathways projecting to brainstem respiratory centers. These dose‐dependent effects can be seen as a reduction in respiratory frequency, tidal volume, or both [24], and are more pronounced with the pure mu‐opioid receptor agonists when compared to the mixed agonist–antagonists or partial agonists [33, 34]. Mixed agonist–antagonists such as butorphanol may be used to reverse, at least in part, the respiratory depression seen with pure mu‐opioid agonists [34, 35]. The ventilatory response to hypoxia is reduced and the CO₂ response is shifted to the right and the slope is decreased, resulting in a rightward shift of the apneic threshold (level of CO₂ where breathing no longer occurs and the animal becomes apneic; Figure 2.11) [24, 36]. Interestingly, ventilatory responsiveness may show maturational changes, as the newborn dog appears to have increased sensitivity to the respiratory‐depressant effects of some opioids (e.g., morphine) [36]. In addition, these effects may be reversed with opioid receptor antagonists such as naloxone or naltrexone [24]. In any small‐animal patient with significant respiratory disease, caution should be used when opioids are administered systemically; careful monitoring of ventilation (PaCO₂) and oxygenation (PaO₂) is highly recommended.

Other Sedatives and Tranquilizers

Similar to opioids, other tranquilizers and sedatives such as acepromazine [37] and alpha‐2‐adrenergic receptor agonists (e.g., medetomidine, dexmedetomidine) [38] may also have at least some respiratory‐depressant effects in dogs and cats, although they appear to be minimal when the sedative agents are used alone and at clinical doses. For example, in dogs administered medetomidine, (the racemic mixture of levomedetomidine and dexmedetomidine (20 and 60 μg kg⁻¹)), respiratory rate significantly decreased and PaCO₂ significantly increased, albeit with little effect on PaO₂ [33,39–42]. By contrast, cats administered dexmedetomidine alone did not show decreased respiratory rates and medetomidine alone did not significantly alter arterial blood gas values significantly [43, 44]. It is important to recognize that the respiratory‐depressant effects of the alpha‐2‐adrenergic receptor agonists are likely to be exaggerated when used in combination with other anesthetic/analgesic agents (i.e., propofol, opioids) [42].

Acepromazine has minimal effects on the respiratory control system in unanesthetized patients, at least at clinical doses. Studies in small animals show a reduction in respiratory rate following acepromazine administration with minimal changes in minute ventilation, PaO₂, PaCO₂, and arterial pH [34, 45, 46]. Similarly, benzodiazepines (diazepam, midazolam) are associated with minimal pulmonary effects in small animals [47]. However, as always, in animals with respiratory disease, care should be used when administration of the agents is required; proper respiratory monitoring should be performed.

Injectable and Inhalant Anesthetics

Similar to the pure mu‐opioid agonists, most induction and inhalational agents depress minute ventilation significantly. PaCO₂ increases because of decreased respiratory rates and volumes; these changes are frequently dose‐dependent. For example, propofol administered to small animals significantly reduces diaphragm contractility [48], arterial pH, and PaO₂ while significantly increasing PaCO₂; large doses can result in apnea [49]. Propofol also suppresses carotid body chemoreceptor activity involved in hypoxia‐induced respiratory responses [50]. Alfaxalone dose‐dependently decreases respiratory rate and minute volume similar to propofol in cats [51] and in dogs [52], although apnea appears to be more of an issue in dogs. By contrast, intravenous ketamine administration appears to have less respiratory‐depressant effects than other agents, especially at low doses. Indeed, ketamine infusions improve respiratory (and cardiovascular) depressant effects associated with inhalant anesthetics in small animals when used as part of a balanced anesthesia technique [53].

All inhalant agents shift the CO₂–ventilatory response curve to the right and reduce the slope in a dose‐dependent manner, and the CO₂ response curve is almost horizontal at high inhalant levels (2.0 × the minimum alveolar concentration) (Figure 2.11) [54, 55]. In addition, the ventilatory response to hypoxia is also diminished via significantly depressed carotid body chemoreflexes [56]. When inhalant anesthetics are used in animals with respiratory disease (as well as in normal patients), the anesthetist should be ready to assist or control ventilation, since the combination of anesthetic agents used (i.e., opioids along with sedatives and inhalants) is expected to result in significant respiratory depression in almost every anesthetized case.

Upper Airway Disorders or Dysfunction

Disturbances in the upper airway include, but are not limited to, laryngeal paralysis, brachycephalic airway syndrome, collapsing trachea, intraluminal or extraluminal masses or abscesses, etc. Patients may present for anesthetic procedures unrelated to the airway disturbance or for surgical intervention to correct the primary airway problem. If an airway crisis is reached, patients frequently present anxious, dyspneic, and hypoxemic.

Sedation and Analgesia

Sedatives should be chosen on an individual patient basis and doses adjusted toward individual pathologies. However, sedation with low doses of tranquilizers (i.e., acepromazine 0.01–0.05 mg kg⁻¹ IM, IV) or anxiolytics (i.e., dexmedetomidine at 0.001–0.010 mg kg⁻¹ IM, IV) and nonstressful handling are important during the preanesthetic period. Although some upper airway disorders (i.e., laryngeal paralysis, tracheal collapse, brachycephalic airway syndrome, etc.) are not believed to be painful conditions in and of themselves, opioid analgesics are frequently administered (i.e., butorphanol at 0.02–0.05 mg kg⁻¹ IM, IV; hydromorphone at 0.1–0.2 mg kg⁻¹ IM, IV, etc.). If respiratory depression is a concern, and any anticipated pain is considered mild‐to‐moderate, buprenorphine (0.02–0.05 mg kg⁻¹ IV, IM, TM in cats) can also be used. The synergism of sedatives with the opioid often reduces anxiety and stress and improves the animal’s comfort and breathing without significant respiratory depression; if inhalant anesthetics are subsequently used, levels may be reduced.

One caveat associated with sedation in patients with upper airway disease is the potential for vomiting and subsequent aspiration. Thus, if possible, antiemetics such as maropitant (1 mg kg⁻¹ IV, SC; 2–4 mg kg⁻¹ PO) should be administered at least 1–2 h prior to sedation (depending on route) and/or general anesthesia [63]. In addition, mu‐opioid agonists and alpha‐2‐adrenergic receptor agonists should be administered cautiously, especially when used in combination. The IV route should be considered over IM opioid administration, since IV use may somewhat reduce the chances for vomiting [64].

In any case, if the procedure is anticipated to be painful, opioid agonists should not be withheld; however, the analgesic plan should be tailored to the specific case. For example, a multimodal approach including the use of ketamine and nonsteroidal anti‐inflammatory drugs (NSAIDs) may be warranted. However, if steroid administration is likely to occur during the procedure to reduce airway inflammation, NSAIDs should be avoided. If appropriate, local anesthetic techniques including nerve blocks, fascial plane blocks, and epidurals should be used if appropriate. Depending on required duration of action, lidocaine, bupivacaine, mepivacaine, or ropivacaine can be chosen. In addition, the intraincisional use of liposomal bupivacaine (Nocita^®, Elanco Animal Health, Greenfield, IN) may be an excellent adjunct in the analgesic plan, as analgesia occurs locally with no systemic sedative effects. However, no studies exist concerning the use of liposomal bupivacaine in airway surgeries.

Ventilatory Support

Along with preoxygenation, securing an airway quickly is quite important in these patients. All equipment including orotracheal tubes, laryngoscopes, ties, and cuff inflators should be organized and accessible. Orotracheal intubation is the most common and efficient means to deliver 100% oxygen and inhalants. However, in an emergent situation, supraglottic airway devices (v‐gel®, Jorgensen Laboratories, Loveland, CO) may be used in cats (and rabbits) (Figure 2.13).

An important factor associated with respiratory fatigue is airway resistance. Resistance to laminar flow is governed by the Hagen–Poiseuille law, and is estimated by:

(2.3)

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