Quantitative 3D analysis of bone in hip osteoarthritis using clinical computed tomography

Participants for this observational study were taken from a cohort of 204 female control volunteers involved in existing Cambridge trials investigating hip fracture risk (57 from FEMCO: LREC 07-H0305-61; 38 from MRC-Hip fx and 100 from MRC-Ageing: LREC 06/Q0108/180; 9 from MRC-Stroke: LREC 01/245). The local research ethics committee approved each of these studies, with each participant giving informed consent for the analysis of their CT data for the investigation of hip disease. All participants were free of hip fracture, osteomyelitis, bone malignancy, unilateral metabolic bone disease, terminal illness and prior treatment with teriparatide or strontium ranelate. All examinations were reported by a consultant radiologist as part of the routine clinical care of patients. One of the 204 examinations was unavailable for analysis on account of data corruption and so imaging was used from 203 individuals. The mean [± standard deviation (SD)] age of this final group was 65 ± 18 years; mean weight was 70.1 ± 14.4 kg; mean height was 1.62 ± 0.07 m; mean body mass index (BMI) was 26.9 ± 5.4 kg/m². No height data was available for one individual and so she was given the sample mean value.

Imaging of the hips was acquired helically in the supine position on five different clinical whole-body multi-detector CT machines (Siemens SOMATOM Sensation 16, Sensation 64, Definition Flash, Definition AS+, and a GE Medical Systems Discovery 690). The acquisition protocol involved imaging inclusively from the superior margin of the acetabuli to the lesser trochanters. All acquisitions were processed with a standard smooth-edge body kernel and reconstructed with axial slice separation ranging from 0.75 to 1.5 mm, equivalent to slice thickness in all cases. In-plane pixel spacing varied from 0.59 to 0.78 mm, with field of view consistently 512 by 512 pixels. Peak kV was routinely 120 kV. When available from the fully anonymised metadata, recorded exposure ranged from 67-274 mAs, varying due to routine use of dose limiting.

Since there were no clinical measures of disease available in this cohort, we used radiological scores to grade disease severity. Digitally reconstructed radiographs (DRRs) were created using an anatomically standardised coronal mean intensity projection with a window level of 200 Hounsfield units (HU) and a width of 700 HU. DRRs were reviewed by a consultant radiologist (AF) for K&L grading (0 to 4) [4] and minimum JSW, recorded to the nearest 0.1 mm with electronic callipers. Multi-planar reformats were reviewed by another consultant radiologist (TT) for osteophyte load, a reviewer-generated cumulative score of osteophytes graded from 0 to 3 in 42 separate sectors from around the proximal femur [10]. The maximum score in this cohort was 47, and so this was the upper limit used in our analysis. Full details of DRR and scoring methodologies (including reliability) have been previously published [8, 10].

We investigated the effect of these radiological measures on cortical thickness in the proximal femur, with the assumption of a linear relationship with disease for each. Frequency histograms were created for each radiological score using MATLAB 2013a (© 1984-2013, The MathsWork, Inc.) to demonstrate the spread of disease severity (Fig. 1). The assumption of linearity was validated by scatter plots and calculation of Kendall’s tau correlation coefficient using StatPlus®:mac 2009 (AnalystSoft, StatPlus:mac - statistical analysis program for Mac OS. Version 2009; http://​www.​analystsoft.​com/​en/​). Each covariate showed a linear relationship and significant correlation with the other (Electronic Supplementary Material 1). When both femurs were available, the side with the worse disease score was selected for analysis in order to minimise the risk of including only those with no or minimal disease. If disease scores were equal, then a side was chosen randomly for inclusion. Repeating analyses with different randomisation did not affect the pattern or significance of our results.

Cortical thickness measurement was performed using CBM, implemented by a freely available in-house program called Stradwin (http://​mi.​eng.​cam.​ac.​uk/​~rwp/​stradwin/​). The main strength of this technique is its ability to accurately estimate cortical bone thickness below the pixel spacing of the imaging system, irrespective of partial volume effect. It has been validated for clinical CT against high resolution quantitative CT data acquired at 82 microns per pixel, and applied in clinical CT data sets up to a slice separation of 3 mm [14, 17, 18]. Following semi-automatic segmentation and proximal femur mesh generation, cortical thickness was measured at each of ~6,000-mesh vertices at a normal to the underlying cortical surface. Creation of a single 3D thickness map takes, on average, 15 minutes; the majority of this time is spent on semi-automatic segmentation, which varies according to noise in the data, while automatic thickness analysis usually takes under 1 minute on a standard desktop computer. Measurement error (± SD) at any given point has been previously reported as 0.12 ± 0.39 mm, well below the pixel spacing size in this study and otherwise in daily clinical practice [18]. Precision has also been assessed in repeat analysis of 19 individuals re-imaged with CT and re-analysed after an average of 61 days (SD 22 days, range 34 to 107 days) giving a measurement precision of 5 % of the mean at individual points, dropping to 1 % of the mean when measurements were averaged over a defined region of interest (ROI) [19].

In order to account for differences in hip morphology, each proximal femur was spatially re-aligned with a canonical right femur using B-spline free-form deformation as calculated by an iterative closest-point registration algorithm [20]. This was performed using freely available in-house software called WxRegSurf (http://​mi.​eng.​cam.​ac.​uk/​~ahg/​wxRegSurf/​). Spatially normalised cortical thickness maps were then smoothed with a 10-mm full width at half maximum (FWHM) filter, required for statistical parametric mapping (SPM). After registration of each bone to the canonical femur, SPM was performed to determine regions of significantly different cortical thickness for changes in radiological disease score.

SPM was initially developed for applications in neuroimaging to allow regionally located statistical inferences to be made from the comparison of data at multiple points in space. It uses a general linear model to account for variability in measurement data (here, cortical thickness) in terms of experimental and confounding effects. Effects in our general linear model were radiological disease score (experimental), age and weight (confounding, as revealed by preliminary analysis). Standard two-tail F testing across the cohort gave p-values at each measurement location that were uncorrected for multiple comparisons. As required for SPM, random field theory delivered p-values corrected for these multiple comparisons to control for false positive results (type I errors) [21]. SPM was performed using the SurfStat package [22] in MATLAB 2013a (© 1984-2013, The MathsWork, Inc.). A mean thickness map was also produced for the whole cohort (Fig. 2), allowing change in cortical thickness to be represented as a percentage of the mean. Therefore, three sets of results were calculated for each disease score:

Significant regions of cortical bone thickness difference are “clusters” that meet statistical significance when tested after random field theory correction. For the purposes of visualising results effectively, all non-significant regions were indicated by washed out colour over the relative thickness maps (Figs. 3, 4, and 5). Absolute cortical thickness maps are included in the Electronic Supplementary Material (2 to 4) for reference against these relative thickness maps. An overview of the CBM pathway from data acquisition to results is presented as a flowchart in Fig. 6.