Gluteal Muscle Activity and Patellofemoral Pain Syndrome, A Systematic Review

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  • Gluteal muscle activity and patellofemoral painsyndrome: a systematic reviewChristian J Barton, Simon Lack, Peter Malliaras, Dylan Morrissey

    Centre for Sports and ExerciseMedicine, Queen MaryUniversity of London, London,UK

    Correspondence toDr Dylan Morrissey, Centre forSports and Exercise Medicine,Queen Mary University ofLondon Mile End Hospital,Bancroft road, London E14DG, UK;[email protected]

    Received 11 January 2012Revised 26 July 2012Accepted 2 August 2012Published Online First3 September 2012

    To cite: Barton CJ, Lack S,Malliaras P, et al. Br J SportsMed 2013;47:207214.

    ABSTRACTObjective There is growing evidence to support theassociation of gluteal muscle strength decits inindividuals with patellofemoral pain syndrome (PFPS)and the effectiveness of gluteal strengthening whentreating PFPS. In additiona, an impressive body of workevaluating gluteal electromyography (EMG) has recentlyemerged, further supporting the importance of glutealmuscle function in PFPS. This systematic reviewsynthesises these EMG ndings in order to betterunderstand the role of gluteal muscle activity in theaetiology, presentation and management of PFPS.Methods MEDLINE, EMBASE, CINAHL, Web ofKnowledge and Google Scholar databases were searchedin September 2011 for prospective and casecontrolstudies evaluating the association of gluteal EMG withPFPS. Two independent reviewers assessed each paperfor inclusion and quality. Means and SDs were extractedfrom each included study to allow effect size calculationsand comparison of results.Results Ten casecontrol, but no prospective studieswere identied. Moderate-to-strong evidence indicatesgluteus medius (GMed) activity is delayed and of shorterduration during stair negotiation in PFPS sufferers. Inaddition, limited evidence indicates GMed activity isdelayed and of shorter duration during running, andgluteus maximus (GMax) activity is increased during stairdescent.Conclusions Delayed and shorter duration of GMedEMG may indicate impaired ability to control frontal andtransverse plane hip motion. Further research evaluatingthe value of gluteal muscle activity screening inidentifying individuals most likely to develop PFPS, andthe effectiveness of interventions targeting changes togluteal muscle activation patterns is needed.

    INTRODUCTIONPatellofemoral pain syndrome (PFPS) is one of themost common presentations to sports medicinepractitioners. In a large study of 2519 presentationsto a sports medicine clinic, 5.4% were diagnosedwith PFPS, accounting for 25% of all knee injurypresentations.1 In additiona, incidence estimatesrange between 9% and 15% in active populationssuch as athletes and military recruits.210 Puttogether, these statistics highlight the importance ofunderstanding aetiology and developing effectivemanagement strategies for PFPS.Despite debate regarding the source of pain,11

    consensus that PFPS results due to altered or ele-vated lateral patellofemoral joint (PFJ) stress cur-rently exists.1114 Multiple factors are thought tolead to altered lateral PFJ stress, with variousextrinsic and intrinsic biomechanical characteristicsthought to be involved. One particular intrinsic

    biomechanical factor that has received increasingattention within previous literature is neuromuscu-lar control at the knee and the hip. Traditionally,research has focused on muscle function of thevastii, with imbalance between vastus medialisoblique (VMO) and vastus lateralis (VL) thought toelevate lateral PFJ stress.15 Providing tentative evi-dence to support this theory, a recent systematicreview and meta-analysis reported a delayed onsetof VMO relative to VL may exist in some indivi-duals with PFPS.16 In additional, previous researchindicates reversal of this delay through physiother-apy may be associated with better clinicaloutcomes.17

    With developing clarity about the role of musclesacting primarily at the knee, it is an ideal time toconsider neuromuscular control of the hip in moredetail. Recent research and theoretical analyses18

    have expanded the neuromuscular control focus toaddress this. It is theorised that impaired glutealmuscle function may result in increased hip jointadduction and internal rotation movement duringactivities such as running, squatting and stair nego-tiation. This excessive hip motion is proposed toincrease lateral PFJ stress, associated with PFPSdevelopment.18 Supporting this theory, glutealmuscle strengthening programmes have been asso-ciated with positive clinical outcomes.19 20 In add-itional, a recent systematic review21 found thatindividuals with PFPS exhibit reduced gluteusmedius (GMed) and gluteus maximus (GMax)muscle strength.Despite the growing evidence to support the ef-

    cacy of gluteal muscle strengthening19 20 and indi-cating individuals with PFPS possess impairedgluteal muscle strength,21 one recent prospectivestudy reported PFPS development may not be pre-dicted through gluteal muscle strength testing,22

    while another reported greater hip external rotationstrength may be predictive.2 This may indicategluteal muscle weakness develops due to the pres-ence of PFPS rather than being an aetiologicalfactor.22 Regardless of the true relationship, evalu-ating gluteal muscle strength in isolation does notprovide a complete picture of the inuence ofgluteal muscle function on PFPS. Indeed, isometricstrength tests may relate only loosely to functionalmuscle activity, kinematics or joint forces.Addressing this gap, an impressive body of workhas recently emerged, utilising electromyography(EMG) measurement of the gluteal muscles duringa range of functional tasks, often reporting differ-ences in onset times, amplitude levels and/or activ-ity durations between symptomatic and controlparticipants. A systematic literature review designedto synthesise recent EMG ndings in order to

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  • better understand the role of gluteal muscle activity in the aeti-ology, presentation and management of PFPS was thereforeundertaken. This review aims to provide clinicians with a betterunderstanding of the relationship between gluteal muscle activ-ity and PFPS with the ultimate objective of facilitating improvedpatient management, while also identifying priorities for futureresearch.

    METHODSInclusion and exclusion criteriaProspective and casecontrol studies evaluating gluteal EMGvariables were considered for inclusion. The inclusion criteriarequired participants to be described as having patellofemoralpain, anterior knee pain or chondromalacia patellae. Studiesincluding participants with other knee conditions such as patel-lar tendinopathy or osteoarthritis, where individuals with PFPScould not be separately analysed, were excluded.

    Search strategyMEDLINE, EMBASE, CINAHL, Web of Knowledge andGoogle Scholar databases were searched from inception untilSeptember 2011. A search strategy from the Cochrane system-atic review on exercise therapy for PFPS was used for diagnosissearch terms.23 This was then combined with the key termsEMG or muscle; and gluteal or hip or trunk or proximal.Reference lists and citing articles of included papers were alsoscreened and a cited reference search for each included paperwas completed in Google Scholar for additional publications ofinterest. Unpublished research was not sought. Although thismay potentially lead to publication bias,24 it was deemed

    impractical to identify all unpublished work on EMG activityassociated with PFPS from all authors and institutions aroundthe world interested in this research area.

    Review processTitles and abstracts identied in the search were downloadedinto Endnote V.X4 (Thomson, Reuters, Carlsbad, California,USA), cross referenced and any duplicates deleted. All potentialpublications were assessed by two independent reviewers (CBand SL) for inclusion, with full texts obtained if necessary. Anydiscrepancies were resolved during a consensus meeting, and athird reviewer was available if needed, but was not required.

    Study analysisTwo separate scales were used to evaluate methodologicalquality, including a modied version of the Downs and BlackQuality Index25 and the PFPS diagnosis checklist.26 Each scalewas applied by two reviewers (CB and DM), with discrepanciesresolved during a consensus meeting. A third reviewer was avail-able if needed, but was not required. The diagnosis checklist is aseven-item scale summarising the reporting of key inclusion andexclusion criteria for the diagnosis of PFPS, with higher scoresindicating a greater number of desired criteria had beenreported. The modied version of the Downs and Black QualityIndex25 is scored out of 16, with higher scores indicatinghigher-quality studies. Studies with scores of 10 or greater wereconsidered to be high quality (HQ) and studies with scoresbelow 10 were considered to be low quality (LQ).Sample sizes, participant demographics, population sources,

    activities, muscles and variables evaluated were also extracted.

    Figure 1 Flow diagram summarisingstudy selection for inclusion.

    Table 1 Study details including sample sizes, participant demographics and population sources

    Paper

    Sample size Gender (F:M) Age range (mean age) Height (m), weight (kg)

    PFPS CON PFPS CON PFPS CON PFPS CON

    Aminaka et al36 20 20 13 : 7 13 : 7 NR (214) NR (214) 1.700.10, 7115 1.720.09, 7010Brindle et al39 16 12 12 : 4 7 : 5 1835 (NR) 1835 NR, NR NR, NRBoling et al34 14 14 9 : 5 9 : 5 1842 (246) 1842 (232) 1.680.10, 7212 1.710.07, 7216Cowan et al32 10 27 7 : 3 15 : 12 1840 (2610) 1840 (256) 1.720.04, 638 1.900.09, 699Earl et al33 16 16 13 : 3 13 : 3 NR (224) NR (216) 1.650.10, 6213 1.660.12, 6514Nakagawa et al38 9 10 9 : 0 10 : 0 1835 (235) 1835 (232) 1.650.07, 6110 1.630.06, 564Ott et al40 20* 20 NR NR 1845 (21NR) 1845 (234) 1.710.07, 708 1.680.07, 777Saad et al37 15 15 NR NR NR (232) NR (232) 1.603, 594 1.603, 532Souza and Powers35 21 20 21 : 0 20 : 0 1845 (276) 1845 (265) 1.700.06, 6510 1.700.05, 637Willson et al31 20 20 20 : 0 20 : 0 1835 (213) 1835 (225) 1.680.06, 638 1.690.09, 629

    *Comprised of two groups; (1) low pain1.4 cm increase in pain visual analogue scale following aerobic exercise, n=9 and (2) high pain1.4 cm increase in pain visual analogue scalefollowing aerobic exercise, n=11.CON, control; F, female; M, male; NR, not reported; PFPS, patellofemoral pain syndrome.

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  • Means and SDs of each variable were extracted or sought fromoriginal authors to allow effect size (ES) calculations. Data werepooled where studies evaluated the same EMG variable andfunctional activity. Calculated individual or pooled ES werecategorised as small (0.59), medium (0.601.19) or large(1.20). The level of statistical heterogeneity for pooled datawas established using the 2 and I2 statistics (heterogeneitydened as p0.05)may be associated with a statis-tically signicant or non-signicant pooled result.Moderate evidence = statistically signicant pooled results

    derived from multiple studies, including at least one HQ study,which are statistically heterogeneous (p0.05).Limited evidence = results from multiple LQ studies which

    are statistically heterogeneous (p

  • the outcome assessor and only two studies31 32 reported the val-idity and reliability of their methodology. Additionally, in alllower-quality studies3740 there was a lack of, or inadequate con-sideration in relation to confounding factors (items 5 and 25),and inappropriate matching between cases and controls.3740

    Scores from the diagnosis checklist ranged from 1 to 7, indicat-ing large heterogeneity in reporting and/or denition of inclu-sion/exclusion criteria used.

    Onset time of muscle activationSeven studies3134 36 38 39 evaluated GMed onset timing duringfunctional tasks, and one study31 evaluated GMax (see gure 2).Strong evidence indicates individuals with PFPS exhibit delayedGMed onset during stair descent (two HQ34 36 and twoLQ38 39_studies; I2=51%, p=0.10), with a small pooled ES(0.53, 0.91 to 0.15). Moderate evidence indicates that indi-viduals with PFPS exhibit delayed GMed onset during stairascent (three HQ32 34 36 and one LQ39 study; I2=67%,p=0.02) with a small ES (0.52, 0.85 to 0.19). Limited evi-dence indicates individuals with PFPS exhibit delayed GMedonset during running (one HQ study31) with a medium ES(0.74, 1.38 to 0.10). Single HQ studies indicate limited evi-dence that GMed timing is not different during a lateral stepdown,33 and GMax timing is not different during running.31 Inaddition, one LQ study indicates very limited evidence thatGMed timing is not different during a single leg jumping task.38

    Duration of muscle activationFour studies31 34 36 39 evaluated duration of muscle activity forGMed during functional tasks, and one study31 evaluatedGMax (see gure 3). Strong evidence indicated individuals withPFPS demonstrate a shorter duration of GMed activity duringstair ascent (two HQ34 36 and one LQ39 study; I2=32%,p=0.23), with a small pooled ES (0.43, 0.84 to 0.02).Moderate evidence indicates individuals that with PFPS exhibita shorter duration of GMed activity during stair descent (twoHQ34 36 and one LQ39; I2=70%, p=0.04) with a medium ES(0.91, 1.34 to 0.47). Limited evidence indicates individualswith PFPS exhibit a shorter duration of GMed activity duringrunning (one HQ study31) with a medium ES (0.85, 1.50 to0.20). A single HQ study indicates limited evidence thatGMax timing is not different during running.31

    Muscle activation levelsFive studies31 35 37 38 40 evaluated muscle activation levels(peak or average/linear envelope) for GMed during functionaltasks, and two evaluated GMax (see gure 4). Only one variablewas found to signicantly differ, with limited evidence indicat-ing increased average GMax activity during stair descent (oneHQ study35), with a medium ES (0.80, 0.16 to 1.44). Moderateevidence indicates no differences in GMed average activityduring running (two HQ31 35 studies; I2=2%, p=0.31).Limited evidence from one HQ study31 indicates no differencein peak GMed or GMax during running and drop jumplanding. Very limited evidence indicates no difference in averageGMed activity during walking,38 stair ascent,37 a single leg verti-cal jump38 or single leg anterior reach task.40 Conicting evi-dence was found for average GMed activity during stair descent(one HQ and two LQ studies; I2=79%, p=0.009) and averageGMax activity during running (two HQ; I2=80%, p=0.02).

    DISCUSSIONThis systematic review was completed to synthesise ndingsfrom previous research evaluating the association of gluteal

    Table3

    Mod

    ified

    Downs

    andBlackscale2

    5

    Pape

    r

    Prospe

    ctive

    (P)or

    retrospe

    ctive

    (R)stud

    y

    (1)Clea

    raim/

    hypo

    thesis

    (2)

    Outcome

    mea

    sures

    clea

    rlyde

    scrib

    ed

    (3)Patie

    ntcharacteristic

    sclea

    rlyde

    scrib

    ed

    (5)

    Confou

    nding

    varia

    bles

    describ

    ed

    (6)Main

    finding

    sclea

    rlyde

    scrib

    ed

    (7)

    Mea

    sures

    ofrand

    omva

    riability

    prov

    ided

    (10)

    Actua

    lprob

    ability

    values

    repo

    rted

    (11)

    Participan

    tsaskedto

    participate

    represen

    tativ

    eof

    entire

    popu

    latio

    n

    (12)

    Participan

    tsprep

    ared

    topa

    rticipate

    represen

    tativ

    eof

    entire

    popu

    latio

    n

    (15)

    Blinding

    of outcom

    emea

    surer

    (16)

    Ana

    lysis

    completed

    was

    plan

    ned

    (18)

    App

    ropriate

    statistic

    s

    (20)

    Valid

    and

    relia

    ble

    outcom

    emea

    sures

    (21)

    App

    ropriate

    casecontrol

    matching

    (25)

    Adjustm

    ent

    mad

    efor

    confou

    nding

    varia

    bles

    Total

    Cowan

    etal32

    R1

    11

    21

    11

    UU

    11

    11

    11

    14

    Earl

    etal33

    R1

    11

    21

    10

    1U

    01

    1U

    11

    12

    Bolin

    get

    al34

    R1

    11

    21

    11

    0U

    01

    1U

    11

    12

    Aminaka

    etal36

    R1

    11

    11

    10

    1U

    01

    1U

    11

    11

    Souzaan

    dPo

    wers3

    5R

    11

    12

    11

    00

    U0

    11

    U1

    111

    Willson

    etal31

    R1

    11

    11

    11

    0U

    01

    11

    1U

    11

    Nakag

    awa

    etal38

    R1

    11

    11

    11

    0U

    01

    1U

    00

    9

    Brindle

    etal39

    R1

    11

    01

    11

    0U

    01

    1U

    0U

    8

    Ott

    etal40

    R1

    10

    10

    11

    UU

    00

    1U

    UU

    6

    Saad

    etal37

    R1

    00

    01

    10

    0U

    01

    1U

    00

    5

    (For

    items1

    3,6,

    7,1012

    ,15,

    16,1

    8,20

    ,21an

    d25

    )0,

    no;1

    ,yes;U

    ,una

    bleto

    determ

    ine.

    (For

    item

    5)

    0,no

    :1;p

    artia

    lly:2

    ,yes.

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  • muscle activity with PFPS. There is currently moderate tostrong evidence that GMed muscle activity is delayed and ofshorter duration during stair ascent and descent in indivi-duals with PFPS. In additiona, limited evidence indicatesthat GMed muscle activity is delayed and of shorter dur-ation during running. Limited evidence indicated thatGMax muscle activity was increased during stair descent.However, the remaining ndings related to activation levelsfor both GMed and GMax were generally inconsistent, pos-sibly owing to heterogeneity of the condition, varying meth-odological quality, the small number of studies in some

    areas and/or data reduction and processing procedures ofincluded studies.

    Onset time and duration of muscle activationPooled data indicated moderate-to-strong evidence for delayed,and shorter, duration of GMed during stair negotiation; andlimited evidence indicated delayed and shorter duration ofGMed during running in individuals with PFPS. However, theseactivation pattern differences were not consistent across allstudies and tasks (see gures 2 and 3). Importantly, ndingsfrom Boling et al34 indicated a trend towards earlier GMed

    Figure 2 Gluteal electromyography onset times during various functional tasks. (A) Gluteus medius and (B) Gluteus maximus. PFPS, patellofemoralpain syndrome; PGM, posterior gluteus medius (indwelling electrode). This gure is only reproduced in colour in the online version.

    Table 4 Patellofemoral pain syndrome diagnosis checklist26

    Inclusion items Exclusion items

    TotalscorePaper

    Cleardefinition oflocation

    Insidious onsetunrelated totrauma

    Symptomsconsistent withdiagnosis

    Previousknee surgery

    Internalderangement

    Ligamentousinstability

    Other sources ofanterior kneepain

    Souza and Powers35 1 1 1 1 1 1 1 7Cowan et al32 1 1 1 0 1 1 1 6Nakagawa et al38 1 1 1 0 1 1 1 6Ott et al40 1 1 0 1 1 1 1 6Aminaka et al36 1 1 1 1 0 0 1 5Willson et al31 1 1 1 0 1 1 0 5Boling et al34 1 1 1 1 0 0 0 4Brindle et al39 0 1 1 0 1 1 0 4Earl et al33 0 0 1 1 0 0 0 2Saad et al37 0 0 0 1 0 0 0 1

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  • muscle activity during stair ascent (see gure 2A). Whenattempting to identify methodological differences to explain thisdisparate nding, it appears the methods for identifying GMedonset time were similar in the study by Boling et al34 (>3 SDabove resting EMG activity) to other studies36 39 (>35 SDabove resting EMG activity) where onsets were signicantlylater during stair negotiation. In additiona, the age and genderbalances were also similar across the related studies32 34 36 39

    (see table 1) and no key consistent difference in inclusion/exclu-sion criteria including pain and function levels was apparent(see table 4). Therefore, this difference may reect the multifac-torial nature of PFPS.Altered patterns of GMed muscle activity (ie, delayed onset and

    shorter duration) identied in this review may be a primary factorassociated with PFPS in some individuals, although without pro-spective research it cannot be determined whether this relationshipis one of cause or effect. Regardless, delayed and shorter durationof GMed may provide an explanation for greater hip adductionand internal rotation reported in some previous PFPS casecontrolstudies evaluating lower-limb kinematics.41 If gluteal muscle acti-vation is delayed, frontal and transverse plane hip motion controlmay be impaired, leading to increased stress on the PFJ and subse-quent symptoms associated with PFPS. Supporting this theory,Willson et al31 recently reported a moderate correlation betweendelayed GMed onset time and greater magnitude of hip adductionexcursion during running. Further research is needed to determinethe relationship of GMed onset time and duration on kinematicsat the hip and ultimately PFJ loading.

    Muscle activation levelsFor the majority of comparisons, GMed and GMax muscleactivity levels did not differ between groups (see gure 4). Thismay indicate that the level of gluteal muscle activation is of lessimportance than activation pattern in relation to pathology inPFPS. However, prospective evaluation of gluteal muscle activityin those who develop PFPS is required to conrm this.

    Conicting ndings related to average GMed muscle activityduring stair descent and average GMax activity during runningmay be explained by methodological differences between identi-ed studies. During running, Souza et al35 established averageGMax activity over the stance period (ie, from foot strike untiltoe off ), with ndings indicating a signicant increase in activityfor the PFPS group. However, Willson et al31 established averageGMax from activity onset to offset, taking into account activa-tion prior to heel strike. Their ndings indicated no differencesbetween groups. Considering the methodological differences,these ndings may indicate that the gluteal musculature demon-strates reduced activity prior to foot strike, followed by increasedactivity in response to loading in individuals with PFPS. Furtherevaluation of these different approaches and periods of activityin the same cohorts is needed in future research.Conicting ndings were produced by three studies evaluating

    average GMed muscle activities during stair descent (see gure4A). Specically, one study38 indicated a signicant increase,one study35 indicated a non-signicant increase and one study37

    indicated a signicant decrease in activity in individuals withPFPS. One possible explanation for these conicting ndingsmay be the lack of control in relation to cadence by Saadet al,37 whose ndings indicated a signicant decrease inaverage GMed activity during stair descent. Decreased groundreaction force was also found in the study by Saad et al,37 pos-sibly indicating reduced cadence and an attempt to reduce loadon the PFJ. Such a reduction in ground reaction force mayultimately reduce the work required by the gluteal musculatureand subsequent EMG activity. Both Nakagawa et al38and Souzaand Powers35 controlled cadence that may have reduced theability to compensate, with their ndings indicating greaterGMed activity during stair descent. However, without evalu-ation of ground reaction force (GRF) in these studies, this possi-bility cannot be conrmed. Further research evaluating theinuence of cadence and GRF on gluteal muscle activity isneeded to provide clarity.

    Figure 3 Gluteal electromyography durations during various functional tasks. (A) Gluteus medius and (B) Gluteus maximus. PFPS, patellofemoralpain syndrome. This gure is only reproduced in colour in the online version.

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  • Clinical implicationsFindings from this systematic review indicate that delayed andshorter duration of gluteal muscle activity may exist in indivi-duals with PFPS. Considering this, specically targeting inter-ventions towards correcting these decits (eg, biofeedback orgait retraining) should also be considered in the management ofPFPS. Further research evaluating the effectiveness of such strat-egies compared to, or combined with effective hip-strengtheningprogrammes4245 is needed. This systematic review has identi-ed a large level of heterogeneity in the ndings related togluteal muscle activity characteristics associated with PFPS.Although this may reect varying methodological design, it mayalso be a function of the multifactorial nature of the condition,highlighting the importance of not considering hip muscle func-tion in isolation when treating PFPS.

    Methodological considerations and directions for futureresearchA number of methodological limitations were identied fol-lowing application of the modied Downs and Black QualityIndex,25 including the absence of outcome measurer blindingand reporting of validity/reliability of methodology; lack of,or inadequate consideration in relation to confoundingfactors such as control of gait velocity/cadence and inappro-priate matching on participant characteristics such as age,height, weight and gender between cases and controls. Theseareas should be addressed in future research. In additiona,many non-signicant ndings in this review may be the resultof low participant numbers and the absence of a sample sizecalculation, a weakness that should be addressed in futureresearch.

    Figure 4 Gluteal electromyography activation levels during various functional tasks. (A) Gluteus medius and (B) Gluteus maximus. PFPS,patellofemoral pain syndrome. This gure is only reproduced in colour in the online version.

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  • The SENIAM guidelines46 provide clear and valid guidanceregarding the preparation and application of electrodes duringthe collection of gluteal EMG. However, the same clear guid-ance is lacking for data collection procedures, reduction andanalysis. As a result, these methodological aspects varied acrossthe included studies (see table 2), possibly explaining some ofthe conicting ndings. Unfortunately, without direct evaluationcomparing outcomes due to varied approaches in the samecohorts, it is difcult to establish the exact nature or size oftheir inuence on results. Future studies evaluating gluteal EMGin individuals with PFPS should consider addressing this. In par-ticular, the inuence of cadence, method of identifying muscleonset time and method of establishing EMG activity levels onresults needs to be established.The ability to distinguish between cause and effect in relation

    to identied differences is impaired by the absence of prospect-ive research. Additional research is needed to determine ifscreening of gluteal muscle activity can successfully identifythose most likely to develop PFPS. Findings from casecontrolstudies were inconsistent for all variables evaluated. This may bea function of the large heterogeneity in methodological design,and in particular inconsistent inclusion/exclusion criteria fordiagnosis. It is recommended that future casecontrol studiesuse inclusion/exclusion criteria checklist26 to guide participantrecruitment which is based on high-quality randomised con-trolled trials evaluating conservative PFPS interventions.47 48

    CONCLUSIONCurrent research evaluating the association of gluteal muscleactivity with PFPS is limited by an absence of prospectiveresearch, low sample sizes and heterogeneity in methodologicaldesign including procedures, data reduction and analysis andparticipant inclusion and exclusion criteria. Conicting ndingsmay be a function of these methodological differences and/orthe multifactorial nature of PFPS. Moderate-to-strong evidenceindicates that GMed muscle activity is delayed and of shorterduration during stair ascent and descent in individuals withPFPS. Additionally, limited evidence indicates that GMedmuscle activity is delayed and of shorter duration duringrunning, and GMax muscle activity is increased during stairdescent. Further research evaluating the value of glutealmuscle activity screening in identifying individuals most likely todevelop PFPS is needed. Additionally, evaluating the effective-ness of interventions such as biofeedback and gait retraining tar-geting changes of gluteal muscle activation patterns is needed.

    Contributors All authors contributed signicantly to the article formulation. SL andCJB had the original idea and led on the writing. PM and DM assisted this process.DM also did the quality assessment.

    Competing interests None.

    Provenance and peer review Not commissioned; externally peer reviewed.

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  • doi: 10.1136/bjsports-2012-090953September 3, 2012

    2013 47: 207-214 originally published onlineBr J Sports Med

    Christian J Barton, Simon Lack, Peter Malliaras, et al.

    pain syndrome: a systematic reviewGluteal muscle activity and patellofemoral

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