The present study was registered in the research registry (www.chictr.org.cn; registration no. ChiCTR-OOC-16008095; 14 March 2016). The protocol (no. 2016-08; 1 March 2016) was approved by the review board of the Second Affiliated Hospital and Yuying Children's Hospital of Wenzhou Medical University (Wenzhou, China). Written informed consent had been obtained by the parents or legally authorized guardians.

A total of 36 pediatric patients [age, 4–6 years; American Society of Anesthesiologists (ASA) grade I or II], scheduled for elective tonsillectomy between May and September 2016 at the Second Affiliated Hospital and Yuying Children's Hospital of Wenzhou Medical University were enrolled in the present clinical trial.

Patients were excluded if they exhibited the following: i) No cooperation; ii) body mass index of <13.5 kg/m² or >31 kg/m²; iii) upper airway infection; iv) serious respiratory and/or cardiovascular disease, hepatic or renal insufficiency (the values of alanine aminotransferase, aspartate aminotransferase, blood urea nitrogen, creatinine >1.5 times the upper limit of the normal level); v) asthma or airway hyperresponsiveness, neuromuscular diseases or cachexia; vi) airway abnormalities and a previous history of an abnormal response to anesthesia; vii) an acid-base imbalance or severe electrolyte disorder; viii) participation in another clinical study within 30 days.

After arrival in the operating room, intravenous access was established into the peripheral vein in the forearm for induction of anaesthesia. Throughout the present study, all patients were continuously monitored, with their rcSO₂ (SenSmart™; Nonin Medical, Inc.) being assessed using a cerebral oximetry probe (reading rcSO₂ every 5 sec), which was placed on the middle of the forehead, and SpO₂ being assessed using an oximetry probe (M1133A; Philips Medical Systems, Inc.), which was placed on the right index finger. Non-invasive systolic blood pressure (SBP), mean arterial pressure (MAP) and diastolic blood pressure (DBP) were measured every 1 min on a different limb to the SpO₂ probe. Heart rate (HR), electrocardiogram and end-tidal carbon dioxide partial pressure (P_ETCO₂) were also continuously monitored. Induction of anaesthesia was performed using propofol 2–3 mg/kg, fentanyl 2–3 µg/kg and cisatracurium 0.1–0.2 mg/kg. Anaesthesia was maintained with a continuous target-controlled infusion of propofol and remifentanil. Pressure-controlled ventilation of 100% oxygen through a mask, with a flow rate of 6 l/min, was administered, and P_ETCO₂ was maintained between 30 and 35 mmHg. After a period of 6 min, mechanical ventilation was stopped and the tracheal tube was successfully introduced using a video laryngoscope. The tracheal tube was subsequently disconnected from the circuit and the proximal end was opened until the SpO₂ decreased to 90% or until the rcSO₂ decreased by >10% of the baseline level. The tracheal tube was then reconnected to the circuit and ventilation was recovered with a flow rate of 6 l/min of 100% oxygen.

The values of NIBP, HR, SpO₂ and rcSO₂ were recorded at the designated time-points: T₀ indicates the time-point prior to application of oxygen prior to oxygenation; T₁ indicates baseline, the time-point at which the mechanical ventilation was stopped; T₂ indicates the time-point at which SpO₂ began to drop from the baseline level; t₂ indicates the time-point at which rcSO₂ began to drop from the baseline level; T₃ indicates the time-point of SpO₂ decreasing to 90% or rcSO₂ decreasing by >10% of the baseline level and mechanical ventilation being recovered; T₄ indicates the time-point at which SpO₂ began to rise from the minimum value following ventilation; t₄ indicates the time-point at which rcSO₂ began to rise from the minimum value following ventilation; T₅ indicates the time-point at which SpO₂ returned to the baseline level, t₅ indicates the time-point at which rcSO₂ returned to the baseline level. S_T1-T4 indicates the value of SpO₂ at T₁ (baseline)-the value of SpO₂ at T₄ (the minimum value); R_T1-t4 indicates the value of rcSO₂ at the T₁ time-point (baseline)-the value of rcSO₂ at t₄ (the minimum value; Fig. 1).

All data were expressed as the mean ± standard deviation or as n (%), as appropriate. Statistical analysis was performed using SPSS 18.0 (SPSS Inc.). The calculation of the sample size, besides being based on the pilot study, mainly referred to that in previous studies (Koch et al (8), where the sample size was n=21, and the authors studied the perioperative use of cerebral and renal near-infrared spectroscopy in neonates; and Eichhorn et al (11), where the sample size was n=10, and a clinical trial was used to evaluate the use of near-infrared spectroscopy under apnea-dependent hypoxia in humans).

The normality of distribution of data was examined using the Shapiro-Wilk test. For the data that did not exhibit a normal distribution, a Wilcoxon signed-rank test and Spearman's rank correlation were used. Data exhibiting a normal distribution were analyzed using a repeated-measures one-way analysis of variance and Pearson's linear correlation. P<0.05 was considered to indicate statistical significance.

Among the 36 pediatric patients considered for the present study, 6 cases were excluded due to upper airway infection or body mass index >31 kg/m², which may have added complexity to the procedure. Finally, a total of 30 patients, including 21 males and 9 females (age, 4.9±0.8 years; body weight, 21.8±5.5 kg) were enrolled in the present study.

Compared with the values at T₀, the SBP, MAP and DBP were decreased at the time-points from T₁ to T₅/t₅, and the HR was decreased at the T₁ time-point (P<0.001). Compared with those at T₁, the MAP and DBP were increased at the T₂ time-point and the HR was increased from the T₂/t₂ to the T₅/t₅ time-point (P<0.001), as presented in Table I.

The values for rcSO₂ and SpO₂ are provided in Table II and the different time-intervals are stated in Table III. Compared with the SpO₂, the rcSO₂ exhibited an earlier decrease in response to hypoxia (t₂-T₁=80.2±23.6 sec vs. T₂-T₁=124.4±20.5 sec; P<0.001). However, the rcSO₂ decreased slower than the SpO₂ (T₃-t₂=104.8±27.3 sec vs. T₃-T₂=60.6±13.7 sec; P<0.001). Furthermore, the decrease of SpO₂ to 90% of the baseline occurred earlier than that of rcSO₂ decreasing by >10% of the baseline in all thirty cases. After the recovery of ventilation, rcSO₂ was increased earlier than SpO₂ (t₄-T3=13.4±6.2 sec vs. T₄-T3=18.9±6.5 sec; P<0.001) and the duration of t₅-t₄ was longer than that of T₅-T₄ (84.8±24.3 sec vs. 15.2±6.8 sec; P<0.001). In addition, the duration of t₅-T₃ was longer than that of T₅-T₃ (98.2±24.3 sec vs. 34.1±6.8 sec; P<0.001). From T₂/t₂ to T₃, the rcSO₂ and SpO₂ values exhibited a decrease and a significant correlation of the two parameters was determined (Pearson's correlation coefficient=0.317; P=0.027). From T₃ to T₄/t₄, the rcSO₂ and SpO₂ values decreased significantly and a significant correlation of the two parameters was obtained (Spearman's correlation coefficient=0.489; P=0.006), as shown in Figs. 2 and 3. Compared with S_T1-T4, R_T1-t4 was smaller (9.7±0.5 sec vs. 5.3±2.7%; P<0.001; Fig. 4).