Design

This study was a cross-sectional analysis of explorative pre-operative data from a subsample of patients included in a randomized controlled trial. The trial is registered at ClinicalTrials.gov. No.:NCT01616667 and described in detail elsewhere [24].

Participants

Forty-seven patients were recruited from the outpatient clinic at the Department of Orthopaedic Surgery and Traumatology, Odense University Hospital and Svendborg Hospital (SvB), Denmark between May 2012 and May 2014. The inclusion criteria were patients aged 45–70 years with primary unilateral hip OA, scheduled for cementless THA. Patients were excluded if they had had prior THA or major lower limb surgery, BMI>35 (kg/m²) (due to difficulties with gait analysis marker placement), if they were unable to walk without walking aid of any kind, if they had any neurological or medical disease compromising their walking ability, inability to read and understand Danish, or if they declined to participate. All patients were clinically and radio-graphically evaluated and diagnosed with primary OA and scheduled for THA. A convenience sample of 20 able-bodied adults aged 45 to 70 years was recruited to provide a reference group on kinematic data.

The patients’ characteristics are summarized in Table 1. Forty-seven patients and 20 able-bodied participants completed the evaluation with 3DGA and hip muscle iMVC. The patient group included 34 males and 13 females. They had a mean age of 61.1 ± 6.7 years and a mean BMI of 27.3 ± 3.4 (kg/m2).

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Table 1. Characteristics of hip OA patients and able-bodied.

https://doi.org/10.1371/journal.pone.0153177.t001

The able-bodied participants (55% female) had a mean age of 59.6 ±7.1 years and mean BMI of 25.6 ±2.9 (kg/m2), Table 1. The able-bodied participants walked, as expected, significantly faster than the OA patients (p < 0.01).

The trial complied with the Declaration of Helsinki. It was approved by the Danish Data Protection Agency and The Danish Regional Committee on Biomedical Research Ethics (Southern Denmark), Project-ID S-20120009. A written and orally informed consent was collected prior to the inclusion of all participants.

Gait data collection

3DGA data were collected using a six-camera motion capture system (Vicon MX03, Oxford, UK) and further processed in Nexus 1.7–8 [25, 26]. Prior to the gait analysis the leg length, pelvic, knee and angle width were measured. These measurements were used to estimate joint rotation centres for each individual. A total of 16 markers were placed on anatomical landmarks on the pelvic, thigh, knee and foot according the standardized Plug-in-Gait marker set model [27]. All the participants walked barefooted at self-selected walking speed on a 10 meter long walking corridor. The patients and able-bodied participants completed an identical motion capture protocol. We captured five separate gait trials for each participant as recommended by Laroche et al. 2011 [28]. To avoid acceleration and deceleration only the stride in the centre of the capturing volume for each trial (five left and five right) were analysed.

Maximal hip muscle strength

The muscle strength of the hip abductor, hip flexor and hip extensor muscles was measured with three consecutive isometric maximal voluntary contractions (iMVC) for each muscle group. Maximal hip muscle strength was recorded in the upright standing position, according to the protocol described by Jensen et al. [29]. For each muscle group, one submaximal test contraction (for familiarization) and three maximal contractions were performed. The participants received both visual feedback on a pc-monitor (in the form of a graphical plot of the force over time) and verbal feedback during each test contraction. To avoid a systematic learning bias, two dice randomizations were used to determine first the starting leg and second the sequence of muscle groups to be tested. The two data collectors performed a visual inspection (face validity) together of the contraction curves to ensure no pretension using a custom-made MATLAB^® program (MathWorks, Natick, MA, US). The contraction with the highest peak moment (Nm) was selected and normalized according to body mass (Nm/kg). Only iMVC performed with the affected limb was used in the current study. iMVC in the standing position has shown acceptable validity [30] and high test-retest reliability has been reported in healthy adults and patients with THA [29, 30].

Pain assessment

Pain was measured immediately after completion of the 3DGA using an 11-point (0–10) Numeric Rating Scale (NRS); where 0 represents ‘no pain’ and 10 represents ‘the worst possible pain’. The patients were asked to assess their hip pain intensity for the affected limb immediately after walking. A second pain intensity assessment was performed immediately after the last iMVC contraction. The NRS scores for the affected limbs recorded after walking were used in the association analyses. The NRS has been shown to be both valid and reliable in geriatric patients [31].

Patient-reported outcome measures

We used the Hip disability and Osteoarthritis Outcome Score–Physical Function Short-form together with its subscales of Pain and Quality Of Life in HOOS 2.0 (HOOS-Pain and HOOS-QOL) to measure physical function, pain and quality of life, respectively. The total score for each of the three subscales ranges from 0 points (extreme symptoms) to 100 points (no symptoms). HOOS-Physical Function has shown good validity when compared with the HOOS subscale for Activity of Daily Living and high responsiveness in THA patients [32]. HOOS 2.0 has shown high validity, reliability and responsiveness in patients diagnosed with hip OA [33]. The patients completed the Danish version of the questionnaire that has been validated for trans-cultural adaptation [34].

Data processing

The GDI is calculated for each limb using nine kinematic variables collected during 3DGA- namely, all three planes from the pelvis and hip, the sagittal plane from the knee and ankle and the foot progression [14]. First, the GDI scores for the 20 able-bodied participants were calculated according to the instructions described by its authors using the electronic addendum (an Microsoft Excel file) provided with the original paper by Schwartz and Rozumalski 2008 [14]. We validated our reference group data based on the original reference data of typically developing children [14] and found that our reference group had a mean GDI (mGDI) of 94.4 ± 7.3 Next, we replaced the original reference data in the electronic addendum with our reference group data–which per se had an index value of 100. Finally, we calculated the GDI scores for the hip OA patients against our reference group data. mGDI scores based on five trials were calculated. We only used the mGDI of the affected limbs in the analyses. A GDI score of 100 or above represents no gait pathology. Each 10-point decrement from 100 indicates approximately one standard deviation from the normal gait pattern [14]. GDI has shown good validity in children with cerebral palsy [35] and excellent inter-trial and intra-rater reliability [16, 21].

Statistical Analysis

Data were checked for completeness and normality (Q-Q plot). A one-sample t-test was used to test the difference between the patients’ mGDI and the reference group’s GDI of 100 points.

We used Pearson’s correlation to investigate the associations between mGDI and continuous variables (iMVC in hip flexion, extension and abduction, HOOS-Physical Function, HOOS-Pain and HOOS-QOL). Spearman correlation was used to investigate the association between mGDI and pain measured by the NRS (ordinal data). Preliminary analyses were performed to ensure all correlation analysis assumptions were fulfilled and data were checked for linearity and outliers (Fig 1A and 1B. representative examples). Further, multiple linear regression was used to investigate the associations adjusting for walking speed. Walking speed has an influence on the kinematic in the lower limb [36, 37] and it has also been shown that the GDI may be affected by gait speed [38]. The correlation coefficients (r-value) and the determination coefficient (R²) were reported. The correlation coefficients were interpreted according to Dancey and Reidy [39]: an r-value of 0.1–0.3 was regarded as weak; 0.4–0.6 as moderate; 0.7–0.9 as strong and 1 as perfect correlation. The statistical analyses were performed using Stata 13.1 (Stata Corp LP, Brownsville, TX, US) and we used a 0.05 significance level.

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Fig 1.

A-B. Representative examples of the association between mGDI and clinical outcomes.

https://doi.org/10.1371/journal.pone.0153177.g001

Hip muscle strength and gait ‘quality’

The results confirmed our hypotheses that hip OA patients who experience low hip muscle strength also walk with reduced gait ‘quality’, but to a lesser degree than anticipated. The current weak to moderate associations emphasize that reduced iMVC does not reflect the entire functional limitation of gait suggesting that factors not identified in the current study are also of importance for gait ‘quality’. However, our results are consistent with previous findings of weak to moderate associations between hip abductor muscle strength and discrete kinematic variables of gait in hip OA patients and healthy older adults [12, 40]. The GDI was measured during horizontal walking at a self-selected walking speed. This task may not be challenging enough to ensure high demand on the hip muscles in hip OA patients, which is reflected in the weak to moderate association. This may also be the reason why we did not find any association between mGDI and hip extensor muscle strength. Little strength requirements in this muscle group is needed during horizontal walking [41]. The hip muscle strength was measured isometrically in a standing position with the limb in an anatomically neutral position. However, this position only represents the position of the joint at one time point in the gait cycle. Analysis of measures of isokinetic hip muscle strength in a dynamic setup mimicking the range of motion and force-velocity during gait may supply the analysis and represent a more functional model. Our finding of a positive association between hip abductor muscle strength and mGDI is however in line with several previous studies that found hip abductor muscle strength to be important for gait function and emphasized the need for increased muscle strengthening regimens [5, 42–45]. The hip abductors are important to stabilize the pelvis in the frontal plane during the stance phase and hip abductor weakness may cause the pelvis to drop towards the swing limb [46] and thus influence the kinematic of the pelvis included in the GDI. Our results suggest that an effective rehabilitation intervention with special focus on the hip abductor muscles will, to some extent, improve the gait ‘quality’ for patients with hip OA although it only accounted for 16% of the variation in gait. Thus, this study contributed to identify adjustable physical parameters that influence the gait ‘quality’. It is essential to identify these parameters and know the strength of associations to gait when developing rehabilitation programs that intend to improve the overall gait in patients with hip OA.

Pain and gait ‘quality’

We found a moderately negative association between gait ‘quality’ and pain measured directly after walking that explained 20% of the variation in GDI but we found no association between gait ‘quality’ and pain measured over the past week (HOOS-pain). The discrepancy in our results could be explained by the way the two pain score are collected. The NRS score is directly connected to the pain level experienced by the patient at the time of walking, whereas the items in the HOOS-pain subscale cover several situations over the past week, not only related to the activity of walking. In accordance with our result, both Behery and Foucher 2014 and Zeni et al. 2014 [10, 12] investigated the association between pain measured as the average over the last week and discrete 3DGA parameters and they found no association in patients with hip OA. Thus, our finding suggests that high pain level experienced directly in relation to gait is negatively associated with the objective measured gait ‘quality’ and that it matters at which time-point pain is measured. Our results imply that interventions aimed at improving pain management may improve gait ‘quality’ to a moderate degree in patients with severe hip OA.

Patient-reported outcomes and gait ‘quality’

The moderate association between mGDI and self-reported physical function and quality of life is also in agreement with previous findings [10]. Associations between the Harris Hip Score (HHS) (which is a commonly used surgeon-reported outcome measure) and several specific gait variables (hip range of motion and joint moments in all three planes of the hip) before and after THA surgery have been identified [10]. An association between the HHS subscale of physical function and kinematic gait parameters, in particular, has been observed [10]. The variance not accounted for between mGDI and PROs in this study may be because self-reported physical function and actual physical performance are two different constructs, but hypothesized to have some similarities. Therefore, strong associations cannot be expected. However, our results underline that both types of measurement are important to obtain a more complete evaluation of hip OA patients [47, 48]. Further this study has shown an association between patient-reported outcome and gait ‘quality’. These findings indicate that gait ‘quality’ may be important for the well-being of patients with hip OA as it has been shown for patients with THA [11].

Interactions of outcomes between domains

As recommended by ‘Outcome Measures in Rheumatology Clinical Trials’ [49], evaluation of both objective and patient-reported measures was performed in the current study. However, in this study, we did not investigate the associations between hip muscle strength and PROs directly, but it has previously been shown that improving the hip abductors significantly improves both pain and patient-reported physical function in people with knee OA [50] and hip OA [47, 51]. Thus, improvement of hip abductor strength would possibly improve both physical function and gait ‘quality’ in hip OA patients.

We have also investigated the interaction between different domains in accordance with WHO International Classification of Functioning, Disability and Health (ICF) classification [52]. The ICF classification specifies three domains (‘body function’, ‘activity’ and ‘participation’) that influence a person’s functioning, disability and health status and the model implies that the domains are interacting. This study covered two of the domains, namely, ‘body function’ with the measure of gait ‘quality’ and hip muscle strength and the ‘participation’ domain reflected in the PROs. We observed weak to moderate associations both within the domain of ‘body function’ (gait ‘quality’ and hip muscle strength) and between the domains (gait ‘quality’ and PROs) supporting the interaction between the domains.

Strengths and limitations

We conducted an explorative study on a well-defined patient group with unilateral hip OA, which supports the internal validity of the study. The use of the GDI as a measure of gait ‘quality’ has advantages over more common ways of reporting the results from 3DGA. Firstly, by reporting a single composite score rather than several discrete gait variables extracted at specific time points in the gait cycle, the GDI can be used as an overall score of gait pathology. Secondly, the GDI has shown previously to be a potentially useful classification and evaluation tool in different patients [15, 18, 19, 21, 22, 53]. Furthermore, we based the GDI calculation upon 3DGA data collected on an adult abled-bodied reference group in our own laboratory instead of using the reference data from the literature based upon typically developing children [14]. Walking speed is known to influence the kinematic parameters [36, 37, 54]; however, all significant results remained significant after adjusting for walking speed, which shows robustness in our findings.

Finally, the evaluation included the valid and reliable HOOS-questionnaire, pain measured directly related to the gait analysis session and measurement of hip muscle strength. Thus, our results may be one step towards providing ‘validity’ to the use of the GDI in hip OA patients.

However, limitations of the current study should be mentioned. Firstly, limitations with regard to 3DGA methodology made strict inclusion criteria necessary [24]. This can affect the external validity of the study. Secondly, the GDI score does not provide any information of the underlying cause of the deviations from normal gait and does not include tempo-spatial parameters or kinetic data. Thirdly, pain during testing may limit the measurements of iMVC, because pain potentially reduces the patient’s effort in reaching maximal strength [55]. As twenty-four (51%) patients in our study had NRS pain scores of five or above after the iMVC test, (Table 2), this may have affected the association between the GDI and hip muscle strength. Finally, it must be emphasized that this is an explorative cross-sectional study where clear causal relationships cannot be established. A prospective intervention study investigating if improving the maximal hip muscle strength improves the gait ‘quality’, as this cross-sectional study implies, is therefore warranted.