Temperature variability in the day–night cycle is associated with further intracranial pressure during therapeutic hypothermia

We performed retrospective analysis from subarachnoid hemorrhage patients enrolled in the ongoing project named “ICU Cockpit”, which has been approved from local institutional review boards. Regarding the patients analyzed in this study, ICP and brain temperature (Neurovent-P, Raumedic AG, Helmbrechts, Germany) were used for brain monitoring. Body temperature was monitored by intra-arterial thermistors (PiCCO system, Pulsion Medical Systems SE, Munich, Germany). Hypothermia (target core body temperature 33.0–33.9 °C) was induced and maintained using endovascular cooling (Quattro™, Zoll Medical, Chelmsford, USA) according to a standardized protocol if intracranial hypertension and/or delayed cerebral ischemia refractory to conventional treatment occurred [1]. Glasgow outcome scale (GOS) was assessed after 1 year.

Neuromonitoring and systemic data obtained with Infinity^® Delta Monitor (Dräger AG, Lübeck, Germany) were conveyed to and synchronized in Component Neuromonitoring System (CNS) monitor (Moberg Research, Inc., Ambler, Pennsylvania, USA). Continuous parameters were stored at 1–10 Hz. Next, files obtained from CNS monitors were converted into Matlab files (Matlab R2014a, Natick, Massachusetts, USA) for statistical analysis. We selected the cases with ICP monitoring registered during more than 5 days. Because we suspected that the circadian rhythms could be a primary factor that correlates with brain injury, we built a spreadsheet in Excel (Excel 2010, Microsoft Corporation, Redmond, Washington, USA) containing the mean and standard deviation of all parameters in diurnal (6:00–18:00) and nocturnal (18:00–6:00) periods, encompassing all days of monitoring. We used this time to define diurnal and nocturnal periods based on the pattern of intrinsic circadian rhythms, which are related to endogenous oscillation of suprachiasmatic nucleus activity and observed through parameters such as serum level of melatonin and core body temperature [6]. To exclude values that corresponded to artifact, we set upper and lower limits based on clinical knowledge and visual analysis of the graphs plotted from data of each parameter. Days with more than 15% of values out of range were excluded of the analysis. Particularly regarding the assessment of the autonomic nervous system, we obtained as parameter the RR (or NN) interval in milliseconds to calculate the heart rate variability. Regarding temperature, we included for statistical analysis days with mean daily temperature <34.9 °C. This temperature limit includes from the first day of hypothermia (target temperature equals 33–33.9 °C) until the day when slow rewarming began. In this manner, this last day of monitoring comprehended initially a period during which the target temperature for hypothermia was maintained and next a period that corresponded to the beginning of rewarming. Importantly, this rewarming was slow in such a way that the mean temperature of that day was less than 34.9 °C. Statistical analysis to find a parameter that could correlate with ICP was carried out using Excel and Minitab 17 (Minitab Inc., State College, Pennsylvania, USA). Excel was used to perform descriptive statistics, ANOVA, and regression analysis. Minitab was used to obtain the graph of regression analysis including regression line and curves of confidence and prediction intervals (80%).

The ratio between the coefficient of variation (standard deviation/mean) of temperature during the nocturnal period (18:00–6:00) and the preceding diurnal period (6:00–18:00) (TV) ranged from 0.274 to 1.97 (Table 2). Mean ICP across the following day (ICP₂₄) ranged from 11.5 ± 3.1 to 24.2 ± 6.2 mmHg (Table 2). The principal result was that TV correlated inversely with ICP₂₄ (Pearson correlation = −0.861, adjusted coefficient of determination R² = 0.725, p < 0.001) (Fig. 1). This correlation can be visualized, for example, in the upper right-hand graph of Fig. 1, which shows that the inverse of TV parallels ICP₂₄ (i.e., the mean ICP that occurs in the following 24 h).

From regression analysis, we obtained the formula ICP₂₄ = 23.9–6.22 TV mmHg. A simplified manner to write this formula and facilitate its memorization is ICP₂₄ = 6 (4–TV) mmHg. This formula determines the regression line. Complementary, to calculate the range of expected ICP₂₄ with 80% of certainty for a certain day, one might use TV (for example, right after 6 a.m., when a 24 h-TV monitoring is completed) in the formula \({\text{ICP}}_{24} = 23.9 - 6.22\,\times\, {\text{TV }} \pm1.73\,\times\sqrt {1.06 + (({\text{TV}} - 1.1)^{2} /4.49)}\) mmHg. In other words, this is the formula for 80% prediction interval. For 80% confidence interval, the formula is expressed as \({\text{ICP}}_{24} = 23.9 - 6.22\,\times\,{\text{TV }} \pm 1.73\,\times\sqrt {0.06 + (({\text{TV}} - 1.1)^{2} /4.49)}\) mmHg. This confidence interval determines the slope in which the regression line fits with 80% of certainty. The graph at the upper left-hand side in Fig. 1 allows the visualization of the regression line, confidence interval (inner dashed lines), and prediction interval (outer dashed lines).