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. Author manuscript; available in PMC: 2019 Apr 23.
Published in final edited form as: Eur Spine J. 2017 Jul 21;27(1):163–170. doi: 10.1007/s00586-017-5217-1

Non-Specific Chronic Low Back Pain: Differences in Spinal Kinematics in Subgroups During Functional Tasks

Rebecca Hemming 1, Liba Sheeran 1, Robert van Deursen 1, Valerie Sparkes 1
PMCID: PMC6478114  EMSID: EMS82579  PMID: 28733722

Abstract

Purpose

A multidimensional classification approach suggests motor control impairment subgroups exist in non-specific chronic low back pain (NSCLBP). Differences in sitting lumbar posture have been identified between two such subgroups (Flexion Pattern (FP) and Active Extension Pattern (AEP)) and healthy individuals, however functional spinal movement has not been explored. This study will evaluate whether NSCLBP subgroups exhibit regional spinal kinematic differences, compared to healthy individuals, during functional tasks.

Methods

Observational, cross-sectional study design. Spinal kinematics of 50 NSCLBP subjects (27 FP, 23 AEP) and 28 healthy individuals were investigated using 3D motion analysis (Vicon™) during functional tasks (reaching upwards, step-down, step-up, lifting and replacing a box, stand-to-sit, sit-to-stand, bending to retrieve (and returning from retrieving) a pen from the floor). Mean sagittal angle for the total thoracic, total lumbar, upper thoracic, lower thoracic, upper lumbar and lower lumbar regions between groups were compared.

Results

Significant differences were observed in lower thoracic and upper lumbar regions between NSCLBP subgroups during most tasks. Significant differences were observed between the FP and healthy group in the lower thoracic region during stand-to-sit-to-stand tasks and bending (and returning from) to retrieve a pen from the floor. All significant results demonstrated the FP group to operate in comparatively greater flexion.

Conclusions

The thoraco-lumbar spine discriminated between FP and AEP, and FP and healthy groups during functional tasks. FP individuals demonstrated more kyphotic thoraco-lumbar postures, which may be pain provocative. No significant differences were observed between AEP and healthy groups suggesting alternative mechanisms may occur in AEP.

Keywords: non-specific chronic low back pain, functional movement, kinematics, Lumbar, thoracic

Introduction

Non-specific chronic low back pain (NSCLBP) is a complex heterogeneous biopsychosocial disorder with multiple manifestations[1]. Despite considerable NSCLBP research there is little reported change in long-term prognosis[2] with intervention outcomes reported to be short-term and moderate at best[3]. Difficulties in establishing effective interventions are likely to be due to an inability to define clear homogeneous NSCLBP subgroups therefore identifying specific NSCLBP subgroups using validated subclassification approaches is paramount[4].

For some NSCLBP individuals, the main driver for pain may be movement and posture behaviour indicating a mechanical basis for the disorder. A multidimensional classification system (MDCS) which considers such mechanisms, for example maladaptive motor control impairment (MCI) (characterised by pain provocative behaviours) has been proposed[5].

This MDCS[5] outlines five NSCLBP MCI subgroups where individuals are proposed to display full range of movement (ROM) in the direction of pain provocation and are clinically observed to habitually adopt end range postures. These MCI subgroups are based upon subjective reporting of direction-specific aggravating and easing factors (described elsewhere[6]). MCI patients have been shown to display high levels of fear avoidance to adopt maladaptive end-range postures and movement strategies that may promote increased pain[7,8,6]. Treatment for these individuals focuses on reducing fear avoidance and optimising spinal control during functional activity to avoid end range repetitive strain, reduce spinal loading and subsequently reduce peripheral nociceptor sensitivity[5]. Previous work has established distinct physical characteristics between two proposed MCI subgroups (Active Extension Pattern and Flexion Pattern) and healthy individuals in adolescent and adult populations, with alterations in spinal position sense, spinal kinematics and trunk muscle activity observed during static postures[710].

Interventions focussed on targeted intervention for these MCI subgroups, such as Classification-based cognitive functional therapy (CB-CFT), have also been proposed to be effective when compared with usual care[11]. Despite CB-CFT incorporating functional re-education approaches, to date no published work has evaluated how NSCLBP MCI subgroups operate during dynamic functional activities.

The purpose of this study is to better understand differences in spinal kinematics between NSCLBP subgroups and healthy individuals during functional tasks. This knowledge may assist in informing specific movement re-education in CB-CFT and aid development of novel sensor and biofeedback technologies to promote back pain self-management.

The hypothesis for this observational, cross-sectional study is that a difference in regional sagittal spinal curvatures between NSCLBP subgroups and healthy controls will be observed during a series of functional tasks.

Materials and Methods

NSCLBP patients were recruited from routine physiotherapy waiting lists in Cardiff and Vale University Health Board (Cardiff, UK). Fifty NSCLBP and 28 healthy individuals volunteered. Ethical approval was obtained from The Research Ethics Committee 3 Wales (10/MRE09/28) within the Arthritis Research UK Biomechanics and Bioengineering Centre, Cardiff University. Informed consent was obtained from all participants. Sample size was based on lower lumbar sagittal spinal angle, which has been shown to discriminate between AEP and FP subgroups in sitting[7]. Power set at priori at 0.7, alpha level of 0.05, a sample of 24 subjects per group was calculated.

Inclusion and exclusion criteria are outlined in table 1. NSCLBP subjects were classified independently by two physiotherapists (RH, LS) based on MDCS criteria[5]. Only subjects classified as FP or AEP (where both clinicians were in agreement) were included. To establish NSCLBP classification a comprehensive subjective assessment including a full history of the individuals back pain, pain behaviour (including aggravating and easing postures and movements) and objective assessment was conducted. Full details of this procedure are published elsewhere[5,12]. Gender, age, anthropometric data (weight, height and body mass index (BMI)) and duration of pain were collected. Patient reported measures for pain (Visual Analogue Scale (VAS))[13], disability (Oswestry Disability Questionnaire (ODQ))[14], distress (Distress and Risk Assessment Method (DRAM))[15] and fear of movement (Tampa Scale of Kinesiophobia (TSK))[16] were completed to evaluate group baseline characteristics. Data collection was conducted at the Research Centre for Clinical Kinesiology, Cardiff University, Wales, United Kingdom.

Table 1. Inclusion and exclusion criteria for the non-specific chronic low back pain (NSCLBP) group.

Inclusion criteria for the NSCLBP group Exclusion criteria for the NSCLBP group
  • Aged 18-65 years

  • History of chronic LBP (>12 weeks)

  • Pain in the lumbar and / or buttock region (defined as pain reported below the level of T12 and no lower than the buttock line)

  • Clear mechanical basis of the disorder aligned with specific aggravating and easing postures and movements, with distinct symptom relief observed during movement conducted in the opposing direction of reported pain provocation (assessed subjectively and objectively)

  • Clinical diagnosis of specific MCI - either FP or AEP

  • Signs of serious spinal pathology (Red flags) including significant trauma, unexplained weight loss and widespread neurologic changes

  • Any vestibular, visual or neurological dysfunction affecting balance

  • Current radiating symptoms (and / or neurological deficit) below the level of the buttock crease

  • Current pregnancy or breastfeeding

  • History of spinal surgery, fracture or malignancy

  • Inability to perform any of the functional tasks unaided

  • Inability to read written English language documents and follow verbal instructions in English

  • Not fulfilling the inclusion criteria

Data Collection

Data were captured using an eight-camera Vicon® motion analysis system (Vicon 512 Motion Systems Ltd, Oxford, UK) at a sampling rate of 100 samples per second. Spherical retro-reflective markers (10mm) (Vicon Motion Systems Ltd, Oxford, UK) were attached using double-sided tape over the following anatomical positions: spinous processes of the 7th cervical, 2nd, 4th, 6th, 8th, 10th and 12th thoracic and 2nd and 4th lumbar vertebrae, manubrium sterni (superior border) and bilaterally on the anterior superior iliac spine (ASIS), posterior superior iliac spine (PSIS), iliac crest (mid-crest, vertically aligned with the greater trochanter) acromioclavicular joint, ulna styloid process, 10cm lateral of the 12th thoracic spinous process, lateral knee joint line and the lateral malleoli creating a full body model (Figure 1). The marker set used was custom-designed (Cardiff University, UK). To minimise error cameras were calibrated prior to data collection and a chartered physiotherapist (RH) performed all marker placement[17].

Fig. 1.

Fig. 1

Custom-designed marker set a) anterior view, b) posterior view

Nine standardised functional tasks (reach up, sitting-to-standing, standing-to-sitting, step up, step down, box lift, box replace, bending to retrieve (and returning from retrieving) a pen from the floor) were evaluated. Tasks were chosen to reflect a range of usual functional activities and elicit a variation of flexion-related and extension-related tasks. Each task was repeated and recorded three times. Following each trial data was visualised in Vicon Nexus (Nexus 1.8.2 Vicon Motion Systems, Oxford, UK) to ensure markers were consistently present (Figure 2).

Fig. 2.

Fig. 2

Labelled marker set as visualised in Vicon®

Data Processing and Analysis

Data processing was conducted in Vicon Nexus. The sacral marker S1 was calculated as the average point between PSIS markers. Processed trials were converted to a c3d file and run through a custom developed analysis programme in MATLAB (version R2013a, The Mathworks Inc., Natick, MA). Prior to the calculation of spine curvatures, the coordinates of the motion capture markers on the spine were transformed from the global (lab) coordinate system to the local (pelvis) coordinate system. The spine was modeled as a curve in the sagittal plane defined by the marker placement over the spinous processes. The change in orientation between the lines interconnecting the adjacent markers was used to define each spinal region curvature in degrees. This was calculated by summing all angular changes within each region: lower lumbar (S1 to L3); upper lumbar (L3 to T12); lower thoracic (T12 to T6); upper thoracic (T6 to C7) (Figure 4). The midpoint spinal curvature of the subjects’ total range of movement was determined for each task. This was calculated as follows: (Maximum flexion sagittal spinal angle + Maximum extension sagittal spinal angle)/2.

Fig. 4.

Fig. 4

Sub-division of spinal curvature

Statistical Analysis

Statistical tests were performed based on the normal distribution and homogeneity of variance[18]. Differences in baseline characteristics between groups were determined using: one-way ANOVA with post-hoc comparisons (Bonferroni) for age and height; independent samples Kruskal-Wallis for mass and BMI, Chi2 for gender; independent t-tests for ODQ, VAS and TSK; and Mann-Whitney U for DRAM. Following a Repeated Measures ANOVA for overall group effect, one-way ANOVAs with post-hoc Bonferroni testing determined between group kinematic differences. All statistical testing was performed in SPSS (version 20.0, IBM Corp, Armonk, NY). The alpha level was set at 0.05[18,19].

Results

Fifty NSCLBP subjects (23 AEP, 27 FP) and 28 healthy individuals were included in the final kinematic analysis. One FP participant failed to complete the patient reported measures therefore 26 FP patient reported measures data sets were included. Table 2 presents the subject characteristics and patient reported measures. There were no significant differences between groups for age or BMI. Significant differences were observed between groups for gender, mass (AEP vs FP) and height (AEP vs FP, FP vs healthy). The location of back pain was similarly reported between groups with the majority of subjects in both groups reporting central symptoms.

Table 2. Subject baseline characteristics across groups.

(Note: Values are mean (SD) unless otherwise stated)

Variable AEP FP Healthy Significance
(n=23) (n=27) (n=28)
Subject Demographics
Gender Males 4 (17.4%) 21 (77.8%) 12 (42.9%) p<0.001*
Females 19 (82.6%) 6 (22.2%) 16 (57.1%)
Age (years) 43.7 (11.2) 41.0 (10.0) 38.5 (11.2) p=0.238
Mass (kg) 68.9 (18.0) 82.5 (14.6) 72.9 (15.2) p=0.005*
(AEP vs. FP)
Height (cm) 164.9
(10.2)
175.9 (8.7) 169.4 (7.3) p<0.001*
(AEP vs. FP / FP vs. H)
BMI (kg/m2) 20.8 (4.9) 23.4 (3.5) 21.5 (4.1) p=0.127
Pain
Site of Back Pain N(%) Right 8 (34.8%) 5 (18.5%) - -
Left 2 (8.7%) 3 (11.1%)
Central 13 (56.4%) 19 (70.4%)
Time Since Pain Onset N(%) 3-6 months 2 (8.7%) 8 (29.6%) - -
6 -12 months 7 (30.4%) 2 (7.4%) - -
1 - 2 years 1 (4.3%) 3 (11.1%) - -
2 - 3 years 0 (0%) 1 (3.7%) - -
3 - 4 years 2 (8.7%) 2 (7.4%) - -
4 - 5 years 3 (13%) 3 (11.1%) - -
5 - 10 years 3 (13%) 4 (14.8%) - -
10+ years 5 (21.7%) 4 (14.8%) - -
Patient Reported Measures
AEP FP
(n=23) (n=26)
ODQ 22.5 (11.6) 21.6 (10.0) - p=0.773
DRAM 29.8 (12.5) 22.7 (10.9) - p=0.027*
VAS 4.6 (1.4) 4.5 (1.4) - p=0.986
TSK 37.5 (6.8) 37.6 (5.3) - p=0.993

Key: FP = Flexion pattern motor control impairment, AEP = Active extension pattern motor control impairment, H = Healthy, BMI = Body Mass Index (mass (kg)/height (m)2), kg = kilogrammes, cm = centimetres, *significant difference (p<0.05), ODQ = Oswestry Disability Questionnaire, DRAM = Distress and Risk assessment method, VAS = Visual Analogue Scale, TSK = Tampa Scale of Kinesiophobia

Reliability

Test re-test reliability was established in a sub-sample of 10 healthy volunteers (5 male, 5 female) across 4 consecutive trials of each functional task. Intraclass correlation coefficients (ICC) were calculated using a two-way mixed model (single measures) with consistency and demonstrated substantial to excellent reliability (ICC 0.746-0.977) across all spinal regions and tasks[20].

Patient Reported Measures

Independent t-tests for ODQ, VAS, and TSK revealed no significant between differences between the AEP and FP groups indicating comparable baseline levels of disability, pain and fear of movement between groups. A Mann Whitney-U test revealed the AEP group to display a significantly more distressed profile compared to the FP group (p=0.027).

Spinal Kinematics in the FP, AEP and Healthy Groups

The Repeated Measures ANOVA for overall group effect was significant (p=0.014) which led to the further exploration of differences within the spinal regions (Tables 3 and 4).

Table 3. Descriptive and inferential results (one-way ANOVA and post-hoc Bonferroni) for the mid-point sagittal thoracic spinal curvatures for each functional task between the active extension pattern, flexion pattern and healthy groups.

Classification Group Descriptives (°)
Task Mean (SD) One-way ANOVA
(p<0.05)
Post-hoc Bonferroni
(p<0.05)
AEP FP Healthy F p
n=23 n=27 n=28
Upper Thoracic

Reach Up 27.2 (8.2) 25.3 (7.8) 27.1 (7.6) 0.485 0.618 -
Step Down 34.5 (8.2) 33.8 (7.9) 35.2 (6.9) 0.206 0.815 -
Step Up 33.1 (7.5) 32.1 (7.4) 34.1 (6.9) 0.521 0.596 -
Box Replace 26.8 (8.5) 25.4 (7.2) 26.6 (7.7) 0.238 0.789 -
Box Lift 23.3 (9.9) 23.9 (7.1) 24.0 (8.5) 0.049 0.952 -
Stand-to-Sit 22.1 (8.8) 20.5 (6.7) 22.5 (7.8) 0.48 0.621 -
Sit-to-Stand 20.4 (8.7) 18.8 (6.2) 20.6 (7.4) 0.454 0.637 -
Pick up Pen (Bend Down) 17.2 (10.5) 19.2 (9.0) 18.8 (8.2) 0.296 0.745 -
Pick Up Pen (Return) 14.3 (11.5) 15.1 (8.5) 15.6 (9.1) 0.099 0.905 -

Lower Thoracic

Reach Up 4.4 (13.1) 11.1 (9.2) 6.4 (11.4) 2.344 0.103 -
Step Down 9.5 (13.2) 18.4 (9.1) 12.6 (10.3) 4.353 0.016* AEP vs. FP
Step Up 10.0 (12.5) 18.0 (9.2) 11.8 (10.3) 3.967 0.023* AEP vs. FP
Box Replace 13.0 (10.0) 21.7 (8.2) 15.5 (11.0) 5.231 0.007* AEP vs. FP
Box Lift 14.1 (9.8) 22.4 (7.9) 16.7 (10.2) 5.144 0.008* AEP vs. FP
Stand-to-Sit 8.8 (11.2) 18.1 (8.5) 10.7 (10.9) 5.997 0.004* AEP vs. FP / FP vs. H
Sit-to-Stand 7.8 (11.0) 17.6 (8.1) 9.9 (11.2) 6.638 0.002* AEP vs. FP / FP vs. H
Pick up Pen (Bend Down) 20.4 (9.9) 26.4 (6.6) 20.4 (7.4) 5.027 0.009* AEP vs. FP / FP vs. H
Pick Up Pen (Return) 19.0 (8.7) 25.0 (6.1) 19.3 (7.6) 5.478 0.006* AEP vs. FP / FP vs. H

Key: FP = Flexion pattern motor control impairment, AEP = Active extension pattern motor control impairment, H = Healthy, SD = Standard deviation, ° = degrees, * = significant difference (p<0.05)

NB: Positive values refer to relative spinal flexion, whilst negative values refer to relative spinal extension.

Table 4. Descriptive and inferential results (one-way ANOVA and post-hoc Bonferroni) for the mid-point sagittal lumbar spinal curvatures for each functional task between the active extension pattern, flexion pattern and healthy groups.

Classification Group Descriptives (º)
Task Mean (SD) One-way ANOVA
(p<0.05)
Post-hoc Bonferroni
(p<0.05)
AEP FP Healthy F P
n=23 n=27 n=28
Upper Lumbar

Reach Up -19.2 (12.0) -11.0 (10.0) -17.4 (8.0) 4.824 0.011* AEP vs. FP
Step Down -18.0 (11.8) -8.1 (9.5) -15.1 (8.4) 6.902 0.002* AEP vs. FP / FP vs. H
Step Up -17.0 (11.2) -7.3 (8.9) -14.1 (7.8) 7.432 0.001* AEP vs. FP / FP vs. H
Box Replace -13.8 (10.9) -3.8 (8.6) -10.1 (7.4) 7.844 0.001* AEP vs. FP / FP vs. H
Box Lift -11.6 (9.4) -2.4 (9.4) -7.5 (7.5) 6.849 0.002* AEP vs. FP
Stand-to-Sit -11.9 (9.7) -0.8 (8.5) -6.3 (7.3) 10.53 <0.001* AEP vs. FP
Sit-to-Stand -10.6 (8.7) -0.6 (8.3) -5.4 (7.6) 9.05 <0.001* AEP vs. FP
Pick up Pen (Bend Down) -1.6 (7.0) 4.3 (6.3) 0.1 (5.3) 5.83 0.005* AEP vs. FP / FP vs. H
Pick Up Pen (Return) -1.9 (7.3) 3.9 (6.2) 1.1 (5.4) 4.978 0.009* AEP vs. FP

Lower Lumbar

Reach Up -23.3 (19.8) -29.9 (18.5) -22.6 (13.9) 1.426 0.247 -
Step Down -21.1 (20.8) -23.7 (16.1) -20.2 (9.9) 0.341 0.712 -
Step Up -19.0 (19.6) -22.8 (15.7) -17.4 (9.9) 0.922 0.402 -
Box Replace -20.5 (17.3) -24.7 (13.5) -18.9 (10.1) 1.258 0.29 -
Box Lift -14.8 (16.7) -20.4 (13.7) -15.0 (9.7) 1.426 0.247 -
Stand-to-Sit -11.6 (15.0) -12.0 (11.6) -9.7 (9.4) 0.292 0.748 -
Sit-to-Stand -11.0 (15.8) -11.3 (12.0) -9.0 (8.9) 0.283 0.755 -
Pick up Pen (Bend Down) -5.2 (16.3) -5.4 (11.9) -2.2 (10.3) 0.506 0.605 -
Pick Up Pen (Return) -5.3 (15.2) -4.8 (13.1) -2.5 (10.0) 0.36 0.699 -

Key: FP = Flexion pattern motor control impairment, AEP = Active extension pattern motor control impairment, H = Healthy, SD = Standard deviation, º = degrees * = significant difference (p<0.05)

NB: Positive values refer to relative spinal flexion, whilst negative values refer to relative spinal extension.

Analyses identified differences primarily in the lower thoracic and upper lumbar spinal regions between the FP and AEP group, and the FP and healthy group. In both instances the FP group consistently operated in greater thoraco-lumbar spinal flexion. This was evident between the AEP and FP groups in the upper lumbar and lower thoracic region during all tasks, with the exception of the lower thoracic region during the reach up task (p=0.103). Significant differences were observed between the FP and healthy group in the lower thoracic region during the stand-to-sit and sit-to-stand tasks and during bending (and returning from) retrieving a pen from the floor. No significant differences were observed between the AEP and healthy groups in any spinal region. No between group significant differences were observed in the upper thoracic or lower lumbar regions during any task.

Discussion

This is the first study to identify distinct subgroup differences in lower thoracic spinal kinematics during functional activity which can aid in informing personalised rehabilitation strategies for CB-CFT interventions[11].

In-line with recent observations of lumbar movement in LBP subgroups[21], consistent patterns of different spinal movement in the thoraco-lumbar spine were noted between the NSCLBP subgroups throughout the functional tasks. Additionally, this region is able to discriminate between the FP and healthy groups, highlighting distinct increases in thoraco-lumbar flexion in the FP group. These findings support those of Dankaerts et al[7] where differences were observed in usual sitting upper lumbar posture between AEP and FP groups. However, in contrast to the results reported here, Dankaerts et al[7] observed differences between AEP and healthy individuals in the upper lumbar region, whilst no differences were observed between FP and healthy individuals. However, similarities are noted between the current study and adolescent cohort data, both identifying significant differences in usual sitting in the upper but not lower lumbar spine [9]. Both Dankaerts et al[7] and Astfack et al[9] demonstrate significant differences between all 3 groups (FP, AEP, healthy) in upper lumbar posture which were not replicated in this study. Differences in instrumentation (electromagnetic 3Space Fastrak®), subject numbers and mean age (41.1 compared to 36.0[7] and 15.6[9] years) may account for some variation in results as well as observation of static postures rather than functional activities.

Overall, AEP individuals operated in significantly greater extension compared to FP during almost all functional tasks in upper lumbar and lower thoracic regions (p<0.05). This may reflect the more extended nature of the task where ROM in this region appears to be similar across all groups. The between group differences observed in the lower thoracic region are novel findings in this study. A non-significant trend (following adjustment for gender differences) for a reduction in overall trunk curvature in AEP compared to FP individuals has been observed previously in adolescent cohorts[22], suggesting the AEP group may adopt a less kyphotic trunk posture compared to the FP group. However the methods utilised to calculate gross trunk angle do not allow for regional analysis.

Interestingly, no significant between group differences were identified between the AEP and healthy groups, contradicting previous work evaluating static postures[7,10] and intimates that AEP and healthy individuals may utilise similar spinal movement patterns during functional tasks. There are multiple hypotheses for this observation. AEP individuals subjectively report extension-related activities as pain provocative due to a reduced capacity to control extension movement[5]. Therefore, the functional tasks may not have challenged the spine into substantial extension to elicit pain and maladaptive movement control. Patients often report prolonged exposure to static postures such as sitting and standing as provoking pain therefore extension may be more apparent in static postures compared to dynamic functional activity. There are also reported difficulties in accurately classifying AEP individuals, with approximately only 50-62% of AEP subjects correctly classified by experienced clinicians[23]. Since, the AEP group displayed an overall higher risk of distress compared to the FP group other factors, such as maladaptive trunk muscle activity, or psychosocial factors[24], may be greater contributory mechanisms to pain than spinal movement.

Limitations and Future Work

The limitations include optoelectronic spinal measurement which allows only for evaluation of general spinal curvature, as opposed to underlying vertebral movement. Radiographic techniques (e.g. video fluoroscopy) are advancing in NSCLBP research [25] and are warranted to understand true vertebral movement during functional activity. Analysis of other NSCLBP MCI subgroups, trunk muscle activity and psychosocial factors is required to better understand underlying pain mechanisms[24] as spinal movement alone appears insufficient to comprehensively explain subjectively reported pain presentations. Further, explorations of how NSCLBP subgroups operate over prolonged time periods (using continuous postural measurement devices) will aid in understanding habitual spinal movement behaviours, carry-over between therapeutic sessions and longer-term movement behaviour change. An important consideration is gender as a confounding factor (FP: 77.8% male, AEP: 82.6% female). Although this is reflective of previous MCI sub-grouped cohorts[9,7], within-group gender distribution should be considered in future work evaluating the MDCS.

Clinical implications

The results support the MDCS as a clinical framework for subgrouping NSCLBP, and can inform the refinement of CB-CFT interventions by identifying key regions of differentiated spinal movement. There is strong evidence that individuals with NSCLBP MCI adopt thoraco-lumbar spinal movement behaviours which are consistent with the direction of subjectively reported patterns of pain provocation. Therefore, it is recommended that physical examination incorporates assessment of functional thoraco-lumbar spine movement, with treatment strategies incorporating targeted functional thoraco-lumbar movement re-education for FP individuals.

Conclusions

Regional spinal curvatures appear to distinctly differ in MCI subgroups, with the thoraco-lumbar region discriminating between FP and AEP, and FP and healthy groups during functional tasks. The FP group demonstrated more kyphotic postures in these spinal regions whereas no significant differences between the AEP and healthy groups were observed, suggesting these groups adopt more similar functional movement strategies. Alternatively postures or activities may have needed to be more involved or sustained in order to elicit a response in these groups. The differences observed in the thoracic spine also highlight the importance of incorporating thoracic spine evaluation into NSCLBP assessment. Gender should also be considered as a confounding factor in future studies.

Supplementary Material

Supplementary material

Fig. 3.

Fig. 3

Example calculation of regional spinal curvature (Upper Thoracic)

Acknowledgments

Support for the study is acknowledged from Health and Care Research Wales (formerly National Institute of Social, Health and Care (NISCHR) Wales) who provided research officers to support data collection.

Conflicts of Interest and Source of Funding

Dr Rebecca Hemming received funding from Arthritis Research UK as part of the Arthritis Research UK Biomechanics and Bioengineering Centre, Cardiff University. Dr Rebecca Hemming also received funding via a Presidents Scholarship Award, Cardiff University. For the remaining authors none were declared.

Footnotes

Ethical approval: All procedures performed were in accordance with the ethical standards of the institutional research committee and with the 1964 Helsinki declaration and its later amendments or comparable ethical standards.

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