Intraparenchymal intracranial pressure monitoring for hydrocephalus and cerebrospinal fluid disorders

Factor 1 = 0.984 (PA (all)) + 0.956 (PA (day)) + 0.953 (PA (night)) + 0.134 (ICP (all)) + 0.137 (ICP (day)) + 0.172 (ICP (night)).

Factor 2 = 0.146 (PA (all)) + 0.133 (PA (day)) + 0.166 (PA (night)) + 0.980 (ICP (all)) + 0.949 (ICP (day)) + 0.939 (ICP (night)).

A scatter plot of the factors, separated by post hoc diagnostic groups suggested separation of the diagnostic groups, with the ‘conservatively managed’ group towards the middle of the normalized data (Fig. 3).

The PCA suggests that all six variables play a major role in separating the data into its principal components with the PA readings constituting factor 1 and the ICP readings constituting factor 2. To explore these relationships further, a descriptive analysis of the data was carried out, based on the post hoc diagnostic groupings.

Mean recordings of the median PAs (all, day, and night) and median ICPs (all, day, and night) for the patients in each diagnostic group are shown in Figs. 4 and 5, respectively. Independent-sample Kruskal–Wallis test showed significant differences between the different diagnostic groups in all six paradigms. Post hoc two-way heteroscedastic t tests were performed with a Bonferroni correction (p = 0.01 as five tests were performed for each paradigm, comparing each group with the ‘conservatively managed’ group; significant results are indicated on the figures (*). These indicate median PA values were significantly different between the ‘conservatively managed’ group and the Chiari/syrinx (all and day, but not night), IIH (all, day, and night) and NPH/LOVA (all, day, and night) groups. Median ICP values were significantly different between the ‘conservatively managed’ group and groups diagnosed with IIH (all, day, and night), high-pressure states (all, day, and night) and low-pressure states (all and day, but not night).

To explore the data further, correlations were explored between ICP and PA and age. Regression curves were constructed using locally weighted scatter plot smoothing (LOESS regression) with the smoothing parameter, α, set at 90%. This method was chosen as an exploratory analysis as the relationship between the variables was not known.

Assessment of the relationship between ICP and PA (Fig. 6), stratified by diagnostic subgroups, revealed a relatively flat relationship between ICP and PA for the conservatively managed and low-pressure cohorts, with a linear direct relationship for the IIH and high-pressure state cohorts. The relationship for the Chiari/syrinx and NPH/LOVA cohorts revealed an interesting trend with PA initially rising with ICP (until a median ICP of around 5 mmHg) and then decreasing, revealing perhaps a more complex physiology in these mainly compliance-associated pathologies.

Assessment of ICP and PA changes with age in the whole cohort (Fig. 7a and b respectively) revealed a slow decrease in ICP and increase in PA with increasing age, although interpretation of this is limited due to the confounds of different age distributions of the pathologies investigated (Fig. 2b).

The PCA extracted two factors with an eigenvalue >1, indicating two principal components to the data set. The first factor, incorporating all three median PA readings, accounts for almost two-thirds of the variance in the data and the second factor, incorporating all three median ICP readings, accounts for almost one-third of the variance in the data. This indicates that PA measurement might play a more important role in separating the data than ICP measurement, but that both contribute significantly to the overall spread in the data.

On exploratory descriptive analysis, significant differences were observed between the PA values in the conservatively managed group and the IIH, Chiari/syrinx and NPH/LOVA groups (Fig. 4). These findings fit with the findings of other studies that show Chiari malformations and NPH/LOVA to be primarily disorders of CSF pulsatility and compliance [8, 11‐15, 20, 21]. There was a trend towards significance in the PA for the high-pressure group; it may be hypothesized that this is due to the heterogeneous nature of this diagnostic group, encompassing a number of etiologies (including post-infectious, post-hemorrhagic, and congenital), some of which may be associated with relatively normal intracranial compliance. Interestingly, the PAs were not different between the conservatively managed group and low-pressure groups, as would be predicted by the intracranial volume–pressure curves.

Significant differences were observed in the median ICP values between the conservatively managed group and those with high-pressure states, low-pressure states, and IIH (Fig. 5). Interestingly, the median ICP was no different between the low-pressure state and conservatively managed groups at night, perhaps due to redistribution of CSF associated with the supine population. There was no difference in the median ICPs between the conservatively managed and the Chiari/syrinx and NPH/LOVA groups, as would be expected from the etiologies and pathogeneses of the respective conditions.

Assessment of correlations between ICP and PA revealed some interesting trends. The differences in the regression curves between the conservatively managed cohort and the IIH and high-pressure state cohorts were expected and can be explained by a decrease in compliance in these conditions, even at low ICP values, and advocates for the measurement of PA as a marker of compliance in addition to ICP. The regression curves generated for the Chiari/syrinx and NPH/LOVA cohorts are somewhat more complex, with decreasing compliance beyond a certain ICP threshold of about 5 mmHg. This is more difficult to explain from a mechanistic perspective and perhaps accounts for the complex pathophysiology of these conditions. It remains to be seen if this relationship is true for individual patients and, importantly, in predicting treatment success in these patients.

Analysis of the conservatively managed group also provides valuable insights into the physiology and dynamics of CSF in ‘normal’ individuals. Given the ethical issues surrounding monitoring ICP in normal individuals, few studies have attempted to establish the hydrodynamics of CSF in normal individuals. Previous studies have sought to establish these normal values by measuring ICP in patients following excision of small, well-demarcated brain tumors [1‐3]. Although these studies have provided insight into ICP in healthy states, this is the first study to provide such data for pulse amplitudes. Although there are clear limitations with considering this pre-selected cohort of patients as entirely normal given the fact that they were chosen to undergo ICP monitoring because of their symptoms and the post hoc nature of their diagnoses, some insights may be drawn from these data.

Firstly, median ICP in this population was 3.21 mmHg (95% CI 2.29–4.13), with this being lower during the day (0.36 mmHg, 95% CI -0.62 - 1.34) and higher at night (5.84 mmHg, 95% CI 4.90–6.78), as expected by the change in posture. These values differ greatly from the accepted ‘normal range’ during a supine lumbar puncture but agree broadly with the other studies in this field [1‐3]; Andresen and colleagues measure mean ICP (rather than median ICP) following removal of a small tumor and found pressures to be 0.5 ± 4.0 mmHg in the supine position and −3.7 ± 3.8 mmHg in the standing position [3]. The median pulse amplitudes also follow a similar trend, with median PA being 4.12 mmHg (95% CI 3.72–4.52) during the recordings, higher during the day (4.42 mmHg, 95% CI 4.00–4.84) and lower during the night (3.84 mmHg, 95% CI 3.43–4.25).

We also acknowledge that the recorded values are vastly different to the values and thresholds used in the sphere of traumatic brain injury (TBI) [6, 7, 16] but hypothesize that this can be explained by the chronicity of the rise in these disorders, compared to the acute rises seen in TBI.

The changes in ICP and PA with age elucidated in this study are also of interest. The trend suggests that ICP slowly decreases with age and PA slowly increases with age. These findings must be interpreted cautiously due to the selection bias of the patients in this study. The findings could be explained by age-associated atrophy, or the fact that the age distribution for patients being investigated for conditions like IIH and high-pressure states were younger than those being investigated for conditions like NPH.

This study has a number of limitations. It is retrospective and therefore subject to all the biases associated with retrospective studies. Perhaps the most important limitation, however, is the comparison group, designated as the conservatively managed group. These were patients chosen by a specialist multidisciplinary team to undergo ICP monitoring due to symptoms that could have been consistent with disorders of CSF dynamics; they were diagnosed as likely having a primary headache disorder post-monitoring by the same multidisciplinary team, and therefore used as a comparison group to provide insight into ‘normal’ CSF dynamics. There is clearly a circular nature to this diagnosis. However, given the ethical implications of undertaking invasive ICP monitoring in normal asymptomatic individuals, this may be the closest next-best alternative. In addition, the PCA conducted in this study was independent of the post hoc diagnostic groupings, suggesting that a composite of the median PA and ICP measures account for the variance in the data.

Another limitation is the fact that only median measures were used. This was due to the historical nature of the data and the lack of raw data for the older recordings. More in-depth analysis using minute-by-minute data for each patient is warranted. In addition, further analyses accounting for postural changes using an accelerometer and studying the within-patient correlations between ICP and PA over the monitoring period will prove invaluable in elucidating the pathophysiology of these complex disorders.

These findings are an important stepping stone to allow a more nuanced use of ICP monitoring for the diagnosis and management of hydrocephalus and CSF disorders. The next step would involve the development of thresholds for each diagnostic category and prospective validation of these thresholds based on the recording results, blinded to the clinical and radiological information.

Future work also needs to focus on a more detailed interrogation of the recordings, by analyzing the spread of minute-by-minute ICP and PA recordings and utilizing these detailed data to assess symptom-pressure correlations. In addition, future analyses need to build on the work of Andresen and colleagues to formulate a more detailed understanding of the relationship between posture and ICP [2]. Analyzing individual patient ICP-PA correlations may also aid the understanding of the differences between individuals, both in health and disease, with the aim of achieving optimum personalized ICP and PA targets for individuals where intracranial pressure and compliance are normalized.