Coupling of CSF and sagittal sinus pressure in adult patients with pseudotumour cerebri

Access was gained via lumbar puncture using two 21-gauge Quincke needles at the intervertebral space L4-L5 using lidocaine local anaesthesia, with the patient lying on their side. A strict aseptic technique was used to keep all the pre-filled tubing and the transducer sterile. The skin was carefully prepared with antiseptic solution. Connection of a standard, disposable fluid-filled pressure transducer (Edwards Lifesciences^TM manometry lines, length 180 cm and inner diameter 1.2 mm), and pressure amplifier (Spiegelberg or Philips) to the LP needle allowed for pressure recording at a frequency of 30–100 Hz, with following processing by ICM+ (University of Cambridge Enterprise Ltd.) [4, 30].

Once a satisfactory CSFp pulse waveform had been achieved, baseline measurements were taken for 10 min, followed by infusion of Hartmann’s solution at 1.5 ml/min or 1.0 ml/min if the baseline CSF was ≥ 15 mmHg until the ICP had plateaued for 5–10 min. The protocol included a safety measure that required the infusion to stop if the mean ICP increased to 40 mmHg or above. This did not occur in any of these patients. The total duration of the infusion tests was 30 to 45 min. After the end of the infusion test, pressure-controlled withdrawal of CSF was carried out without removing the pressure transducer, via a tap connected to the pressure lines. This allowed us to assess CSFp while continuing to measure and record SSp during and after the end of CSF removal. Withdrawal was stopped when the pressure reached ~ 10 mmHg or if the patient started complaining of headaches and/or blurred vision.

The catheter inserted for pressure measurement with DRCV was longer and narrower than the manometry lines used for CSF pressure.

SSp was monitored and recorded with ICM+ in the same way as CSFp. The mean pressure level, slow vasogenic waves (period from 20 s to 2 min), and amplitude of pulse waveform (AMP_SSp) were extracted through computer data analysis and recorded alongside CSFp.

All tests were performed as part of routine clinical management. All patients consented to the use of their data recordings for research purposes. At the time of this study, such consent did not include permission for data sharing.

Using linear regression for each individual patient, SSp was expressed as a function of CSFp in the format SSp = a × CSFp + b (for example, Fig. 4).

In all patients who had undergone infusion and drainage, ‘a’ was calculated to be 0.70 ± 0.14 for 9 patients. ‘b’ was calculated as 6.3 ± 3.5 mmHg which represents the intercept of this correlation that physiologically should correspond to central venous pressure (CVP). In the one patient, CVP was measured and found to be 11 mmHg; the intercept of the correlation was 9.2 mmHg, which is within the limits of measurement error (e.g. zeroing of external transducers).

After the start of infusion, even though there is a direct coupling between changes in CSFp and SSp, the two pressures appeared to diverge compared with baseline (as shown in Fig. 1). This divergence between mean CSFp and SSp may reflect that, at the beginning of the CSF infusion, all the infused fluid is initially accommodated within the intracranial compliant space. As CSFp increases towards its plateau, the infused CSF is absorbed into the sagittal and transverse sinuses [2, 3, 6].

Davson’s equation refers to the steady state and assumes that SSp is independent of CSFp:where Rout is the resistance to CSF outflow and I_f is the CSF formation rate [6].

In hydrocephalus, when SSp is not coupled to CSFp, a constant-rate infusion study enables the calculation of Rout as:

One approach is to modify Davson’s equation by expressing SSp as a function of CSFp (Fig. 4: SSp = a × CSFp + b). Therefore, Davson’s equation may be rewritten for PTCS as:and subsequently,

The average product of Rout × I_f is 3 mmHg [8], 1.5 in IIH with the corrected Rout (see above); therefore, the average CSFp = (1.5 + 6.3)/0.3 = 26 mmHg.

Finally, as derived from the simplified Davson’s equation for IIH, CSFp is increased and is estimated to be around 26 mmHg. This estimation is almost identical to the mean baseline CSFp in our patients, which is calculated as 27 mmHg. The derived formula explains why in IIH with CSFp-SSp coupling, the baseline intracranial pressure is elevated. Moreover, correcting Rout as derived by Davson’s equation, gives a more realistic estimation of a Rout on average < 7 mmHg × min/ml. We have observed in most of our classic IIH patients, that CSFp at plateau is generally not much higher than baseline, resembling the normal CSF circulation, as opposed to hydrocephalus patients. In few exceptional cases, where a higher than expected CSF plateau is observed, knowledge of the SSp could provide valuable information about the differential diagnosis.

Malm and colleagues [23], using a constant pressure infusion technique, demonstrated that there may be two groups of PTCS patients—one group with genuinely reduced conductance (increased Rout) and a second group with increased SSp as the cause of their impaired CSF absorption. They also showed that changes in CSF conductance changed with time after onset of PTCS.

However, these interpretations do not take into account the spatially distributed nature of CSF absorption. In most situations, CSF absorption is probably mainly intracranial and there is only a small gradient of pressure between the sagittal sinus and jugular foramen so that it is reasonable to use one single value for SSp. In contrast, in PTCS, there may be two CSF absorption pressure gradients—above and below an area of sinus narrowing. In other words, one Davson’s equation is required to describe CSF absorption upstream of the stenosis and another Davson’s equation for downstream absorption. Davson’s equation assumes that all the infused CSF is drained through channel(s) that may be described by a single parameter. If CSF absorption is split between upstream and downstream channels, Davson’s equation cannot be used as the relative proportion of ‘I_f’ drained by the two systems is unknown. The transverse sinus pressure/JVP below the level of the stenosis is much lower than SSp above the stenosis. Lublinsky and colleagues have recently demonstrated the presence of arachnoid granulations in the transverse sinuses in both normal subjects and patients with IIH [21]. Interestingly, the total volume and interface contact area of intracranial arachnoid granulations is increased in IIH patients.

The situation may become even more complex if the stenosis is reversible with CSF removal and behaves as a Starling resistor [29]. If part of the transverse sinus is compressible, any rise in CSFp can decrease its lumen and increase the hydrodynamic resistance for sinus blood flow, increasing in the same way the SSp (if cerebral blood flow stays constant), which in turns increases CSFp. This mechanism works as a ‘vicious circle’ until CSFp and SSp reach an elevated state of equilibrium. This has been previously numerically simulated using an elegant mathematical model. The model forecasted that the system with collapsible transverse sinus (represented as a ‘Starling Resistor’) has two steady states: at low and at high CSFp.

An important question that merits systematic study is whether the phenomenon of direct coupling of CSFp to SSp is limited only to PTCS or may also play a role in some cases of acute intracranial hypertension seen during brain swelling (head injury, stroke, meningitis, etc.). A study in this direction from early work suggested that 60% of ICP should be attributed to vascular mechanisms, rather than CSF circulatory component [18‐20, 22, 32]. In one post-TBI patient, we anecdotally studied with double SSp and CSFp measurement during an infusion study; SSp appeared to stay constant when CSFp elevated.

Finally, our statistically strong and significant findings could have important implications for PTCS patients, both in the adult and paediatric populations, and it would be worth designing future randomised trials aiming at treating PTCS patients by stopping the reported pathophysiological coupling of the two pressures.