Propofol attenuates the increase of sonographic optic nerve sheath diameter during robot-assisted laparoscopic prostatectomy: a randomized clinical trial

Since robot-assisted laparoscopic prostatectomy (RALP) was first reported by Binder and Kramer in 2001, it has become the dominant surgical approach for prostate cancer treatment [1]. RALP has many benefits related to oncological outcomes and perioperative complications when compared to open surgery. These benefits include more precise manipulation of vessels and nerves; decreased blood loss; reduced surgical time, length of hospital stay, and postoperative pain; and improved quality of life [2, 3]. However, RALP requires carbon dioxide pneumoperitoneum and a steep Trendelenburg position to optimize surgical exposure. These conditions increase intracranial pressure (ICP) [4, 5]. Increased ICP and the resulting decreased cerebral perfusion pressure are associated with postoperative neurological complications such as cerebral ischemia and cerebrovascular disorders [6]. Therefore, it is necessary to minimize intraoperative ICP changes in robotic prostatectomy patients in whom ICP may increase beyond the normal range.

Anesthetic agents can influence ICP during surgery. In propofol anesthesia, a dose-related decrease in cerebral blood flow, cerebral metabolic rate, and ICP have been reported [7, 8]. Sevoflurane is a cerebral vasodilator with the potential to increase cerebral blood flow, cerebral blood volume, and ICP in a dose-dependent manner [9, 10]. However, the effects of anesthetics on ICP during carbon dioxide pneumoperitoneum and a steep Trendelenburg position during RALP have not been studied.

The purpose of this study was to compare the effects of propofol and sevoflurane on ICP in prostate cancer patients who underwent RALP. We evaluated the sonographic optic nerve sheath diameter (ONSD) as a surrogate for ICP [11].

This randomized clinical trial included 36 patients who underwent RALP at Asan Medical Center during September 2017. Ethical approval for this study was provided by the Institutional Review Board at Asan Medical Center, Seoul, Republic of Korea (approval no. 2017–1011) on August 24, 2017. This study was registered with ClinicalTrials.​gov (NCT03271502). Written informed consent was obtained from all patients.

During the study period, 45 patients were screened. Three patients were excluded due to a history of cerebrovascular disease and six patients refused to participate. A total of 36 patients were included and were randomly allocated to either the propofol group or the sevoflurane group (Fig. 1). Demographic and intraoperative data were not significantly different between the two groups (Table 1).

The ONSDs of the two groups are shown in Table 2. The ONSDs were not significantly different between the two groups 10 min after anesthetic induction in the supine position (T1) or 5 min after establishing carbon dioxide pneumoperitoneum and steep Trendelenburg position (T2). However, 30 min after carbon dioxide pneumoperitoneum and steep Trendelenburg position (T3), the ONSD tended to differ between the groups (5.22 ± 0.34 mm vs. 5.42 ± 0.36 mm, P = 0.096). Sixty minutes after carbon dioxide pneumoperitoneum and a steep Trendelenburg position (T4), the ONSD was significantly different between the two groups (5.27 ± 0.35 mm vs. 5.57 ± 0.28 mm, P = 0.007) (Fig. 2). There were significant increases in the ONSDs in both groups at T2, T3, and T4 compared to T1 (propofol group: all P < 0.001; sevoflurane group: all P < 0.001). During pneumoperitoneum and the Trendelenburg position at T2, T3, and T4, sonographic ONSDs tended to increase continuously (Table 2).

There were no significant differences in PaCO₂, PaO₂, peak airway pressure, plateau airway pressure, systolic blood pressure, pulse pressure variation, and body temperature between the groups (Fig. 3). However, heart rate was higher at T3, T4, and T5 in the sevoflurane group than in the propofol group (T3, P = 0.018; T4, P = 0.006; T5, P = 0.005). In addition, there were no significant differences in regional cerebral oxygen saturation between the propofol group and the sevoflurane group at all predetermined time points under general anesthesia (66.3% vs. 67.7%, P = 0.539 at T1; 65.1% vs. 66.1%, P = 0.614 at T2; 64.4% vs. 65.3%, P = 0.698 at T3; 64.3% vs. 65.9%, P = 0.470 at T4; 65.1% vs. 68.4%, P = 0.152 at T5).

The sonographic ONSD of propofol anesthesia was significantly lower than that of sevoflurane anesthesia 60 min after establishing carbon dioxide pneumoperitoneum and a steep Trendelenburg position in prostate cancer patients who underwent RALP. In addition, the sonographic ONSDs increase continuously after establishing carbon dioxide pneumoperitoneum and a steep Trendelenburg position in both groups.

Anesthetics suppress the activity of electroencephalogram and reduce the cerebral metabolic rate. However, changes in cerebral metabolic rate and cerebral blood flow are inconstant and depends on how the anesthetic affects the cerebral vascular smooth muscle [16]. Sevoflurane has a dose-dependent effect on the vascular smooth muscle relaxation and intrinsic cerebral vasodilatory activity through the direct inhibition of several pathways. Therefore, cerebral blood flow increases significantly during sevoflurane anesthesia, and ICP can increase as a result [10, 17, 18]. However, propofol slows the activity of electroencephalogram, decreases the rate of consumption of adenosine, and reduces the cerebral metabolic rate [8, 19, 20]. Decreased cerebral metabolic rate reduces cerebral blood perfusion, which is known to reduce cerebral blood flow and ICP [21]. In addition, previous human and animal studies determined that propofol led to a progressive decrease in ICP [22‐24]. In particular, ICP tended to decrease over time during the continuous administration of propofol. Farling et al. continuously administered propofol to head injury patients in intensive care and measured the ICP at multiple time points. They reported that ICP significantly decreased after 2 h of continuous administration [23]. Therefore, it could be expected that the difference in ICP between the two groups would gradually increase over time. In the present study, the difference in the ONSD between the two groups was not statistically significant at T2, but tended to differ between groups at T3. The ONSD at T4 was significantly different between the two groups. We consider that the continuous administration of propofol had a beneficial effect on ICP during RALP.

Many studies have determined that carbon dioxide pneumoperitoneum and a steep Trendelenburg position could increase ONSD as a surrogate for ICP [15, 25‐27]. The pneumoperitoneum and Trendelenburg position may disturb cerebral venous drainage due to increased intrathoracic pressure, and may lead to a subsequent increase in ICP [28‐30]. Moreover, carbon dioxide can increase intracranial vascular perfusion and elevate ICP [31‐33]. In the present study, ONSD increased steadily from the induction of carbon dioxide pneumoperitoneum and steep Trendelenburg position in both groups. A previous study reported that ONSD increased immediately after establishing pneumoperitoneum and a steep Trendelenburg position, but then remained unchanged [25]. The ongoing increase in ONSD in our study is thought to be due at least in part to an age-related difference. Based on a previous study regarding ONSD change in patients during RALP [34], the ONSD tended to increase continuously over time in patients greater than 63 years of age after establishing pneumoperitoneum and a steep Trendelenburg position. However, in patients less than 63 years of age, ONSD decreased over the course of pneumoperitoneum and a steep Trendelenburg position [34]. The authors explained that younger patients had better autoregulation of ONSD or ICP during pneumoperitoneum and the Trendelenburg position. In the present study, the average age of the propofol group was 66.1 ± 7.2 years, and that of the sevoflurane group was 63.6 ± 7.9 years. Therefore, it seems likely that the ability to compensate for ICP changes might be reduced, and so ONSD increased continuously over time during surgery.

ONSD measurement using ultrasonography is a simple, non-invasive technique for ICP assessment. Previous studies have reported that sonographic measurement of ONSD strongly correlates with measurement performed by inserting an invasive catheter into one of the lateral ventricles or the brain parenchyma in various clinical situations, including RALP [11, 15, 35, 36]. Intracranial hypertension is defined as ICP greater than 20 mmHg [37], and the cut off value of the ONSD for intracranial hypertension is known to be 4.8–5.2 mm [38‐41]. In the present study, ONSD was measured as 5.27 ± 0.35 mm in the propofol group and 5.57 ± 0.28 mm in the sevoflurane group at 60 min after establishing pneumoperitoneum and the Trendelenburg position. Because this is a situation in which intracranial hypertension might be suspected, it is important to minimize the increase in ONSD during RALP.

The present study has the following limitations. We could not measure ICP because the difficulty and invasiveness of the procedure made it impossible to be carried out in non-neurosurgical patients. However, sonographic measurement of ONSD is a non-invasive technique and has been shown to accurately reflect increases in ICP [42, 43]. Also, we did ONSD was not measured immediately after establishing carbon dioxide pneumoperitoneum and a steep Trendelenburg position. Instead, ONSD was measured at 5 min after establishing pneumoperitoneum and the Trendelenburg position, a time point that can adequately reflect the immediate change of ONSD during RALP.

We found that ONSD was significantly lower during propofol anesthesia than during sevoflurane anesthesia 60 min after carbon dioxide pneumoperitoneum and a steep Trendelenburg position in robotic prostatectomy patients. Our results suggest that propofol anesthesia might be used effectively to minimize intraoperative ICP changes in prostate cancer patients who are undergoing RALP using pneumoperitoneum and the Trendelenburg position.