A novel application of Transnasal Humidified Rapid Insufflation Ventilatory Exchange via the oral route in morbidly obese patient during monitored anesthesia care - A case report -

Article information

Anesth Pain Med. 2020;15(4):505-509
Publication date (electronic) : 2020 October 30
doi : https://doi.org/10.17085/apm.20043
Department of Anesthesiology and Pain Medicine, Soonchunhyang University Bucheon Hospital, Soonchunhyang University College of Medicine, Bucheon, Korea
Corresponding Author: Won Seok Chae, M.D., Ph.D. Department of Anesthesiology and Pain Medicine, Soonchunhyang University Bucheon Hospital, Soonchunhyang University College of Medicine, 170 Jomaru-ro, Wonmi-gu, Bucheon 14584, Korea Tel: 82-32-621-5398, Fax: 82-32-621-5322, E-mail : ch1s@schmc.ac.kr
Received 2020 May 27; Revised 2020 July 4; Accepted 2020 July 23.

Abstract

Background

Transnasal Humidified Rapid Insufflation Ventilatory Exchange (THRIVE) is used to improve oxygenation, with the added benefit of a smaller increase in CO2 if self-respiration is maintained with THRIVE. Despite these advantages, the use of THRIVE through a nasal cannula is limited in situations such as epistaxis or a basal skull fracture.

Case

We successful used THRIVE, through the oral route under general anesthesia with spontaneous breathing in a morbidly obese patient (weight, 148 kg; height, 183 cm; body mass index, 44.2 kg/m2) who received transnasal steroid injections due to subglottic stenosis.

Conclusions

THRIVE through the oral route may be an effective novel option, although further studies are needed.

Morbidly obese patients tend to desaturate faster than non-obese patients due to decreased functional residual capacity, increased O2 consumption, and increased shunt flow [1]. Airway management is more challenging in morbidly obese patients because of the likelihood of a difficult airway [2].

Transnasal Humidified Rapid Insufflation Ventilatory Exchange (THRIVE) has been widely used outside of the operating room, but its use in the operating room is now also increasing [3]. Optiflow® (Fisher & Paykel Healthcare, New Zealand), a new commercial THRIVE device, supplies warmed, humidified, high flow O2 (~70 L/min) through a nasal cannula. It can be applied over the entire range of anesthesia, from preoxygenation [4,5] to post-extubation [6]. Optiflow® can also be safely applied in morbidly obese patients [7] to improve oxygenation and respiratory mechanics.

Despite the benefits of THRIVE, the use thereof through a nasal cannula is limited in situations such as nasal obstruction, epistaxis, and recent nasal trauma or surgery [8]. And in the case of steroid injection into the region of subglottic stenosis as adjunctive treatment after dilatation [9], the transoral approach with rigid laryngoscope is limited due to severe gag reflex. Therefore, the transnasal approach is commonly performed with a laryngoscope with a flexible working channel. The transnasal approach may limit O2 supply through a nasal cannula. In such cases, O2 can be supplied through the oral route. We experienced a morbidly obese patient who received serial transnasal steroid injections due to subglottic stenosis using a standard facial mask and THRIVE through the oral route under general anesthesia with spontaneous breathing. We report our experience and introduce the use of THRIVE through the oral route as an alternative for supplying O2.

CASE REPORT

The patient was a 37-year-old man (148 kg, 183 cm, body mass index [BMI] 44.2 kg/m2) with a history of tracheostomy due to hypertensive intracranial hemorrhage that occurred 4 years ago. He was diagnosed with grade I tracheal stenosis above the tracheostomy site 2 years ago. Despite conservative treatment, dyspnea developed and the patient underwent endoscopic tracheal dilatation under general anesthesia. Baseline peripheral capillary O2 saturation (SpO2) was 94% and Cormack-Lehane grade was 3 at the time of intubation. Surgery was performed using the intermittent apnea technique with extubation, and a total of six apnea events occurred, with a mean duration of apnea was 147 s. The lowest SpO2 was 64%, and SpO2 recovered to 96–98% after manual ventilation via endotracheal tube. The patient had been treated conservatively after balloon dilatation with portable O2 at home. Dyspnea worsened again 1 year ago, despite O2 therapy, and serial fiberoptic steroid injections to the subglottic stenosis site were planned. In our hospital, fiberoptic steroid injections are usually performed according to the following steps. Topical anesthesia at nostrils is followed by sedation, applied by surgeon. The fiberscope is inserted through the nostril, and the glottis and lesion are sprayed with additional local anesthetics. Then, the lesion is injected with steroid. The otolaryngologist consulted us for safe sedation and monitoring due to the possibility of emergency caused by airway edema or airway obstruction. Considering the patient’s general condition, symptoms, and experience of previous surgery, we decided to perform the operation under general anesthesia with spontaneous breathing in preparation for airway manipulation, because general anesthesia using the intermittent apnea technique could limit the view of surgical field and damage the larynx and subglottic lesions.

On entering the operating room, the patient was placed in a 30° sitting position for the first steroid injection. Standard American Society of Anesthesiologists monitoring (non-invasive blood pressure [NIBP], electrocardiogram, and SpO2) and bispectral index (BIS) monitoring were applied. The baseline vital signs were as follows: BP, 105/52 mmHg; heart rate (HR), 66 beats per minute (beats/min); SpO2, 95%. Oxygenation was applied at 6 L/min O2 through a standard facial mask. End-tidal CO2 (EtCO2) was monitored continuously by capnography to confirm self-respiration. Dexmedetomidine was used for sedation. After delivering a loading dose of 1 μg/kg over 10 min, continuous infusion of 0.6 μg/kg/h was maintained. During infusion of the loading dose, the EtCO2 level decreased gradually until apnea was induced. An oral airway was inserted and the jaw-thrust maneuver was applied to maintain airway patency and support self-respiration. After confirming that the patient was unresponsive to verbal commands and tactile stimulus, the surgery was started while self-respiration was maintained. The surgeon requested lowering of the facial mask so that it would not interfere with the procedure and applied topical anesthesia by packing gauze soaked with Bosmin® (0.1% epinephrine) and Beracaine® (10% lidocaine) into both nostrils. The fiberscope was passed through the nostril to access the glottic and subglottic lesions, and additional 2% lidocaine was sprayed around glottis and lesions, and 3 ml of tamcetone® (Triamcinolone 40 mg/ml) was then injected. The procedure was interrupted by bag-valve-mask ventilation because SpO2 fell to 86%. After ventilator assistance for 117 s, SpO2 recovered to 96%. During surgery, HR remained within 20% of the baseline, but BP increased by more than 20% of the baseline. However, systolic BP remained below 160 mmHg, so no additional drug administration was necessary. The value of BIS was maintained between 55 and 80. The total surgery time was 20 min and the total anesthesia time was 40 min. The patient was discharged after 1 day of monitoring in the Intensive Care Unit (ICU), without dyspnea or complications.

Dyspnea improved noticeably, but on physical examination, grade II subglottic stenosis and stridor remained, thus necessitating a second steroid injection 1 month later. Based on our previous experience, we considered that there was a need to improve oxygenation during the procedure, so we decided to apply Optiflow®. In the same manner as in the first operation, the patient was placed in the 30° sitting position, and standard American Society of Anesthesiologists and BIS monitoring were applied. Baseline vital signs were as follows: BP, 102/58 mmHg; HR, 70 beats/min; and SpO2, 94%. O2 (100% warmed, humidified) was supplied through a nasal cannula at a rate of 30 L/min for preoxygenation. The patient tolerated this well, without any complaints. Dexmedetomidine was used for sedation at the same dose as before. Once the patient was unconscious, the O2 flow rate was raised to 70 L/min. EtCO2 was monitored by placing the EtCO2 sampling line at the nostril next to the Optiflow® nasal cannula; however, a low value was obtained, so we could only confirm self-respiration by monitoring the shape of the waveform (Fig. 1A). Topical anesthesia was applied by packing gauze into both nostrils. This disturbed the O2 supply through the Optiflow® nasal cannula; therefore, we inserted an oral airway to maintain airway patency, and the Optiflow® nasal cannula was transferred to the opening of the oral airway. The EtCO2 line was also transferred to the opening of the oral airway, but it still showed a low value; thus, only the shape of waveform was monitored (Fig. 1B). SpO2 was maintained at 98–100%, and no intervention, such as mask ventilation or jet ventilation, was required during surgery. Despite self-respiration, there was a drop in SpO2 to 86% (Fig. 1C) due to O2 leakage; the Optiflow® nasal cannula dislocated from the airway opening. After fixing the nasal cannula to the airway with plaster (Fig. 2), SpO2 immediately recovered to 99% and no additional desaturation events occurred. The vital signs were stable within 20% of baseline. Additional bolus of midazolam was injected to prevent the event of awareness because the value of BIS was maintained between 70 and 79 when the procedure was performed; 1mg for oral airway insertion, 2 mg for gauze packing into both nostrils. During the operation, the value of BIS was well maintained between 35 and 50, and spontaneous breathing was generally maintained well. The patient endured the surgical stimuli without coughing and movement throughout entire operation. The total operation time was 15 min and total anesthesia time was 40 min. The surgeon had prepared jet ventilation because of the experience during the previous surgery, but ultimately did not use it; thus, the surgeon was highly satisfied with THRIVE. After the surgery, the patient was transferred to the ICU. Arterial Blood Gas Analysis (aBGA) was performed after arrival in the ICU; partial pressure of O2, 94 mmHg; partial pressure of CO2 (PaCO2), 49 mmHg; pH, 7.30; bicarbonate, 21.3 mEq/L. The patient was discharged after 1 day of monitoring without complications.

Fig. 1.

(A) End-tidal CO2 (EtCO2) at nostril. (B) EtCO2 at oral airway. (C) Desaturation event.

Fig. 2.

(A) Oral airway, (B) Optiflow nasal cannula, (C) EtCO2 sample line. EtCO2: end-tidal CO2.

This study was approved by the Institutional Review Board of Soonchunhyang University Bucheon Hospital (IRB No. 2020-02-026-001). And written informed consent, included the consent to publish images, was obtained from the patient in this study.

Discussion

We confirmed the effectiveness of THRIVE through the oral route in a morbidly obese patient receiving steroid injections due to subglottic stenosis. Some patients may be contraindicated for THRIVE through the nasal route, and a nasal cannula can prevent manipulation of the fiberscope during trannasal approach. In our case, it was impossible to supply O2 through a nasal route due to nasal packing, so we used the oral approach using an oral airway. Heard et al. [10] reported that oxygenation through a Ring-Adair-Elwyn (RAE) tube placed in buccal region results in significantly less desaturation in patients with a BMI of 30–40 kg/m2. Achar et al. [11] reported that oxygenation through a nasopharyngeal catheter is better than through nasal prongs. These results were based on the distance from the O2 supply outlet to the laryngeal inlet being reduced, such that O2 was effectively delivered to the inlet [11]. In our case, high O2 flow might be delivered well by reducing the distance to the laryngeal inlet through the oral airway as mentioned above. Also there was a desaturation event occurred due to dislocation of the THRIVE nasal cannula from the airway opening. Toner et al. [12] reported desaturation due to obstruction of an RAE tube. Therefore, it is important to note that patency of airway and the O2 supply device must be maintained.

EtCo2 monitoring is necessary to confirm self-respiration and CO2 accumulation. However, because EtCO2 monitoring is limited when using THRIVE, alternative option for CO2 monitoring is essential. The rate of increase in EtCO2 is lower in the case of THRIVE with spontaneous breathing [13] than THRIVE with apneic oxygenation [14]. In our case, postoperative aBGA showed that PaCO2 was 49 mmHg, which was not a significantly increase. Several studies have reported a difference between EtCO2 and PaCO2 over time when using THRIVE, but a good correlation between PaCO2 and transcutaneous CO2 (tcCO2) has also been reported [14,15]. Therefore, it is reasonable to consider tcCO2 monitoring when using THRIVE. The lack of CO2 monitoring through tcCO2 may be limitation in our case.

Our first attempt using a facial mask led to frequent desaturation events. However, our second attempt, using the THRIVE through the oral route, resulted in stable O2 saturation. The effectiveness of our technique cannot be confirmed based on only one case. Thus, further investigations are needed to determine whether supplying O2 through the oral route using THRIVE is comparable to supplying O2 through a nasal cannula. However, our experience demonstrates the possibility of applying THRIVE through the oral route.

In conclusion, THRIVE may be beneficial in morbidly obese patients undergoing upper airway surgery under general anesthesia with spontaneous breathing. As in our case, in cases where applying THRIVE through a nasal cannula is difficult, effective oxygenation can be achieved by application through the oral route.

Notes

CONFLICTS OF INTEREST

No potential conflict of interest relevant to this article was reported.

AUTHOR CONTRIBUTIONS

Conceptualization: Jaewoong Jung, Won Seok Chae. Data curation: Jaewoong Jung. Methodology: Yang-Hoon Chung. Writing - original draft: Jaewoong Jung. Writing - review & editing: Yang-Hoon Chung. Investigation: Jaewoong Jung. Supervision: Won Seok Chae.

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Fig. 1.

(A) End-tidal CO2 (EtCO2) at nostril. (B) EtCO2 at oral airway. (C) Desaturation event.

Fig. 2.

(A) Oral airway, (B) Optiflow nasal cannula, (C) EtCO2 sample line. EtCO2: end-tidal CO2.