Variability of Normal Pressure Hydrocephalus Imaging Biomarkers with Respect to Section Plane Angulation: How Wrong a Radiologist Can Be?

Study Population

Eighty subjects were prospectively enrolled in the study: 35 subjects with clinically confirmed iNPH (25 men and 10 women; mean age, 74.0 [SD, 7.2] years) and 45 sex- and age-matched healthy controls (HCs: 32 men and 13 women; mean age, 72.6 [SD, 5.7] years).

Patient history, neurologic objective findings, and brain MR imaging were used for diagnosing iNPH in accordance with the international iNPH guidelines.¹⁸ Six subjects with iNPH (17%) showed signs of dementia (Mini-Mental State Examination scores, 20–24 points), and 15 subjects (43%) had mild cognitive impairment (Mini-Mental State Examination scores, 24–27 points). All patients except one were able to walk 10 m with or without an assistive device. In addition, all patients underwent a CSF dynamic investigation (including estimation of CSF outflow resistance) and a short-term tap test, which had positive findings in 19 patients (54%). Eighty-nine percent of patients (31/35) were categorized as having probable iNPH, and 11% (4/35), as having possible iNPH. Subjects with significant neurologic comorbidities or a known etiology of NPH (secondary NPH) were not included in the study.

The healthy control group comprised sex- and age-matched volunteers primarily recruited through an advertisement in a local newspaper who showed no signs of neurologic, psychiatric, or advanced atherosclerotic disease on a subsequent clinical examination performed by a neurologist. We applied the following exclusion criteria: medications influencing the central nervous system or blood coagulation; electrocardiogram evidence of arrhythmia, left ventricular hypertrophy, or myocardial infarction; a history and/or clinical or radiologic signs of neurologic disease (including ventriculomegaly, stroke, tremor, ataxia, walking/balance difficulties); significant cardiovascular disease; diabetes mellitus; ≥2 ancillary vascular risk factor (smoking, hypertension, hyperlipidemia); ongoing infectious disease; known serious disease that may reduce life expectancy; and contraindications to MR imaging. Cognition, balance, and gait were tested using the Mini-Mental State Examination (>27 points required) and the one-legged balancing test (30 seconds), tandem stand (10 seconds), Timed Up-and-Go test, and 300-m walk test. Of 59 screened subjects, 50 passed the clinical evaluation and underwent brain MR imaging. Five subjects were subsequently excluded from participating in the study due to MR imaging findings of cortical infarctions (n = 3), cerebellar tonsillar herniation (n = 1), and subdural hygroma (n = 1). Thus, the HC group consisted of 45 individuals.

The study was approved by the Umeå University institutional review board. Signed informed consent was obtained from all participants of the study.

MR Image Acquisition and Analysis

All subjects were examined on a 3T MR imaging system by means of a 3D T1-weighted spoiled gradient-echo imaging sequence with a voxel size of 0.49 mm³. Multiplanar reformats parallel and perpendicular to the bicallosal, bicommissural, Hy-Fa, and brain stem vertical line were obtained.

Anonymized MR imaging data were independently evaluated by 2 observers: a senior radiology resident with 5 years of radiology training and a neuroradiologist with 21 years of clinical experience. Both readers were blinded to clinical data.

Definition of Anatomic Planes on Midsagittal Sections

Inferior margins of the rostrum and splenium of the corpus callosum were used as anatomic landmarks for defining the bicallosal plane (Fig 1). The anterior and posterior commissure defined the bicommissural plane. The inferior pituitary gland margin and the apex of the fourth ventricle defined the hypophysis-fastigium (Hy-Fa) plane. The brain stem vertical line (ie, fourth ventricle floor plane) was parallel to the posterior brain stem margin (PBSM).

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FIG 1.

Definition of standard transverse imaging planes: bicallosal (yellow), bicommissural (blue), Hy-Fa (green), and perpendicular to the posterior brain stem margin (red), shown on midsagittal MR images of 2 different individuals. Note the differences in their mutual alignment between the 2 subjects.

iNPH Biomarker Definitions

Ten previously published radiologic measures as well as 4 calculated indexes^{5⇓-7,12,16⇓⇓⇓-21} were individually evaluated on transverse/coronal imaging sections of 4 different angulations (bicallosal, bicommissural, Hy-Fa, and PBSM) (Fig 2): The frontal horn diameter (FHD) was defined by the maximum distance between the lateral margins of the frontal ventricular horns on the respective transverse sections.^16,17 The inner skull diameter (ISD) was defined by the maximum lateral-to-lateral distance between the inner laminae of the parietal bones on the same transverse sections that were used for FHD measurements.^16,17 The frontal horn vertical diameter (FHVD) was defined by the maximum z-axis (vertical) diameter of the frontal horns measured at the level of the foramen of Monro, ie, the vertical distance between the ceiling of the lateral ventricle and the midpoint of the foramen of Monro on 4 coronal sections.⁷ The maximum supratentorial intracranial diameter (MSID) was measured bone-to-bone on the midsagittal section; the measurement line was drawn parallel to the coronal plane used for FHVD measurement.⁷

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FIG 2.

Graphic representation of biomarker measurements. A, Maximum frontal horn diameter (FHD) and inner skull diameter (ISD). B, Frontal horn vertical diameter (FHVD) measured to the midpoint of the foramen of Monro. C, Maximum supratentorial intracranial diameter (MSID) measured perpendicular to the bicommissural line (dotted line). D, Maximum vertical widths of the supraventricular brain (SVW), cella media (CMW), and temporal horn (THW), respectively; callosal angle (CA); and DESH (curved dashed lines, rated as severe, grade 2 in this case) measured on the coronal section passing through the posterior commissure. E, Simplified callosal angle (simpCA) measured at the corpus callosum midpoint on the coronal section paralleling the PBSM (F, dotted line). Note that for each biomarker, 4 measurement values have been obtained from 4 different sections (as defined in Fig 1). To keep the illustration simple, we show measurements on sections aligned parallel and perpendicular to the bicommissural line, except for the simpCA (E and F). For details, see the Materials and Methods section.

The maximum vertical width of the supraventricular brain (SVW; width of brain tissue superior to the ventricle), the cella media of the lateral ventricle (CMW), and the temporal horn (THW) were measured on 4 coronal sections passing through the posterior commissure (modified from Yamada et al¹²). Depending on the degree of ventricular dilation, the THW was measured either superior to the hippocampus only (if the hippocampus completely covered the floor of the temporal horn) or superior + lateral + inferior to the hippocampus (if the dilated temporal horn extended below the level of the hippocampus).

Disproportionately enlarged subarachnoid space hydrocephalus (DESH) referred to visual semiquantitative assessment of the disproportion between enlarged volumes of subarachnoid spaces at the Sylvian fissure and decreased volumes at the superior parasagittal convexity on the respective coronal sections passing through the posterior commissure.^19,20 DESH was rated as follows: no disproportion = 0, mild-to-moderate disproportion = 1, severe disproportion = 2 (Figs 2 and 3). A single enlarged sulcus in otherwise reduced subarachnoid spaces did not alter the rating because it was known to be a relatively common feature of iNPH.¹⁹ In rare cases when the Sylvian fissure was narrower than the parasagittal convexity sulci, findings were rated as −1 or −2, respectively.

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FIG 3.

Variability of the CA (middle row) and EI (lower row) as measured on bicallosal (yellow), bicommissural (blue), Hy-Fa (green), and PBSM (red) sections of a single subject with iNPH. The CA yields 73°, 69°, 70°, and 103° in the 4 respective planes (maximum percentage difference of 39.5%). The EI shows a less variable range of values: 0.364, 0.361, 0.359, and 0.380, respectively (maximum difference of 5.7%). Color lines on the sagittal sections (upper row) refer to the alignment of the respective coronal and transverse sections below. The disproportion between Sylvian and parasagittal convexity subarachnoid spaces (DESH) has been rated moderate in this case (grade 1).

The callosal angle (CA) was defined by 2 lines tangentially aligned with the superior-medial walls of the lateral ventricles on the coronal sections passing through the posterior commissure.⁵ The simplified callosal angle (simpCA) was assessed on the coronal sections passing through the corpus callosum midpoint, which was identified on the midsagittal section. The angle was drawn with the vertex placed in the inferior point of the corpus callosum and the sides tangential to the lateral ventricles.⁶

In addition, 4 calculated indexes (ratios) derived from the above-mentioned linear measurements were assessed on 4 differently angulated transverse/coronal sections: The Evans Index (EI) was defined as the FHD divided by the ISD obtained from the same section.^16,17 The z-Evans Index (ZEI) was defined as the FHVD divided by the MSID.⁷ The brain-to-ventricle ratio (BVR) was defined as the ratio between the SVW and the CMW.¹² The cella media-to-temporal horn ratio (CTR) was defined as the ratio between the CMW and THW. In cases of ventricular asymmetry, the hemisphere with a larger cella media was used for all measurements.

Note that the inner skull diameter and maximum supratentorial intracranial diameter were neither considered nor evaluated as iNPH biomarkers, yet they were prerequisites for calculating the EI or ZEI, respectively.

Data Analysis

Interrater agreement was studied by means of the intraclass correlation coefficient for a 2-way random effects model and absolute agreement. Correlation coefficient analysis of each biomarker was based on measurements from all 4 planes, giving a total of n = 320 (4 × 80) measurements per biomarker. Results of the reliability analysis were presented as intraclass correlation coefficients with 95% confidence intervals for 2 independent raters.

To assess whether individual biomarkers showed systematic differences when measured on sections with different angulations, we used 2-way repeated measures ANOVA (Huynh-Feldt correction) with angulation as a within-subjects factor and disease status (iNPH/HC) as a between-subjects factor, including the angulation by disease status interaction term (angulaton iNPH/HC). For biomarkers that showed statistically significant dependence on angulation in the repeated measures ANOVA, we analyzed the pair-wise comparison among angulation planes. Means ± standard errors of paired differences were calculated and presented (n = 80) for the paired tests that were significant. A Bonferroni correction was used for the pair-wise comparisons. The level of statistical significance was set to P < .05.