Motor Function Measure

COA At-a-Glance

Evidence of cognitive interviewing of draft instrument in target patient population

Evidence of internal consistency

Evidence of test-retest or inter-rater reliability

Evidence of concurrent validity

Evidence of known-groups validity

Evidence of ability to detect change over time

Evidence of responder thresholds

Inclusion of the COA in product labelling

Daily function
Gross motor function

Overview

Instrument Name: Motor Function Measure

Abbreviation: MFM-32

Points for Consideration:

Has been used in FDA labels

Description of Tool:

The Motor Function Measure (MFM)-32 is a ClinRO developed to monitor the severity and progression of motor function in most neuromuscular diseases in patients aged 6-60 years. It is composed of 32 items assessing standing position and transfers,
axial and proaxial motor function, and
distal motor function.

Other Related Tools (if applicable):

MFM-20 (Not included in Resource)

Minimum Qualification Required by COA Administrator: MA or BA

Comment:

Another version exists for pediatrics: MFM-20.
In order to familiarize examiners with the use of the MFM and its rigorous scoring principles, a training session is required. For routine clinical use, this training may be administered ideally by taking part in a training session with video support

Year: 2005

Objective of Development:

To monitor the severity and progression of motor function in most neuromuscular diseases

Population of Development: Age range (therapeutic indication):

6-60 years (Muscular Dystrophy, Duchenne;
Muscular Dystrophy, Facioscapulohumeral; Muscular Dystrophies, Limb-Girdle; Myotonic Dystrophy; Muscular Atrophy, Spinal; Myopathies, Structural, Congenital;
Muscular Dystrophies; Neuromuscular Diseases

Pediatric Population(s) in which COA has been used:

MFM: Nervous System Diseases; Musculoskeletal Diseases; Congenital, Hereditary, and Neonatal Diseases and Abnormalities; Nutritional and Metabolic Diseases; Immune System Diseases; Bacterial Infections; Pathological Conditions, Signs and Symptoms; Mental Disorders

COA type:

Number of Items 32

Mode of Administration:

Data Collection Mode:

Time for Completion: 36 minutes on average

Response Scales: 4-point verbal rating scale ranging from 0 "Does Not initiate movement or starting position canNot be maintained" to 3 "Completes the exercise with a standard pattern"

Summary of Scoring:

Available scores:
Global score ranging from 0 to 96
Scores by domains

Weighting: No

Score Interpretation: Higher score = Higher level of motor function


Content Validity

Evidence of Literature Review: None identified

Evidence of Instrument Review: Yes

Evidence of Clinical or Expert Input: Yes

Evidence of concept elicitation in target patient population: None identified

Evidence of a Saturation Grid: None identified

Evidence for Selection of Data Collection Method: None identified

Recall/Observation Period:

Evidence for Selection of Reponse Options: None identified

Evidence of cognitive interviewing of draft instrument in target patient population: Yes

Evidence of Preliminary Scoring of Items and Domains: Yes

Evidence related to respondent and administrator burden: None identified

Evidence of a Conceptual Framework: None identified

Evidence of an item-tracking matrix: None identified

Evidence related to item selection: Yes

Evidence of re-testing the final version: Yes


Reliability

Internal consistency (Cronbach's alpha): Yes

Evidence of internal consistency:

Test-retest Reliability (ICC):

Not applicable

Inter-rater/ inter-interviewer reliability (kappa):

Berard (2005)
Intra-rater reliability
- Intraclass Correlation Coefficient (ICC): 0.96
- Kappa Coefficient ranged from 0.81-0.94 for 25 items, and from 0.61-0.80 for 7 items
- Was a definition of stability applied to identify stable patients: Yes; No change was expected over a 15-30 day period
- Time frame or interval between the two administrations: 15-30 days
- Population/Disease: Patients with muscular disease (mean age 24.5 years+15.4 (6–62 years); n= 50

- Intraclass Correlation Coefficient (ICC): 0.99
- Kappa Coefficient ranged from 0.81-0.94 for 9 items, from 0.61-0.80 for 20 items, and 0.51-0.60 for 3 items
- Population/Disease: Patients with muscular disease (mean age 24.5 years+15.4 (6–62 years); n= 50

Trundell (2020)
Intra-rater reliability
1- Intraclass Correlation Coefficient (ICC): 0.97
- Was a definition of stability applied to identify stable patients: Yes; patients with No change in CGI-S (Clinical Global Impression of Severity) score
- Time frame or interval between the two administrations: mean of 305 days
- Population/Disease: Patients with SMA Type 2 and 3 (age range 2-25 years, mean age 11.76 years); n= 15

2- Intraclass Correlation Coefficient (ICC): 0.95/0.94
- Was a definition of stability applied to identify stable patients: Yes; patients with No change in VigNos grade/CGIS score
- Time frame or interval between the two administrations: mean of 348 days
- Population/Disease: Children with neuromuscular diseases (age range 2-5 years, mean age 4.87 years); n= 14

Evidence of test-retest or inter-rater reliability: Yes


Validity

Concurrent validity (convergent, divergent):

Berard (2005)
- Correlation coefficient used: Spearman rank correlation
- Measure: Functional Independence Measure (FIM)
- Results: p Not stated for all results
0.91 for total
0.87 for standing position and using transfers domain
0.84 for axial and proximal motor function
0.64 for distal motor function
- Population/Disease: Patients with muscular disease (mean age 24.5 years+15.4 (6–62 years); n= 303

Seferian AM (2015)
Correlation coefficient used: Spearman's correlation coefficient
- Measure: Brooke Scale
- Results: p<0.01 for all results Significant correlation was found between MFM-D2 and Brooke Scale: rho = -0.76 Significant correlation was found between MFM-D3 and Brooke Scale rho = -0.68 Significant correlation was found between MFM-Total and Brooke Scale rho = -0.78 - Population/Disease: Patients with DMD, n= 50 to 53, age: mean= 17.1 (4.8) and median= 16.5 (9-28.1) Bulut N (2019) - Correlation coefficient used: Not stated - Measure: Trunk control measurement scale (TCMS) - Results: Significant correlation was found between TCMS and MFM: r= 0.88; p<0.01 - Population/Disease: Patients with DMD; n= 20, mean age 9.4+/-3.3 years

Known-group validity:

Berard (2005)
1- KNown-groups validity:
- Measure/Groups of patients: 4 groups according to the Clinical Global Impression (CGI) results (completed by physicians)
- A priori hypotheses: Not stated
- Were hypotheses confirmed: Not applicable
- Results: Mean scores significantly decreased with degree of motor disability as evaluated by the CGI (ANOVA: F= 293.2, p< 0.0001 - all means significantly different in pairwise comparisons) 2-Measure/Groups of patients: VigNos Grade, Brooke Grade - A priori hypotheses: Not stated - Were hypotheses confirmed: Not applicable - Results: Spearman rank correlation; p Not stated for all results - High correlation between MFM-32 and VigNos Grade: 0.91; and the Brooke Grade: 0.85 - Highest correlation for Standing position and transfers domain with the VigNos Grade (0.93) - Highest correlation for Axial and proaxial motor function domain with the Brooke Grade (0.87) - Distal motor function domain showed a moderate correlation with any of the other scores (ranging from 0.56 to 0.70) 3-Measure/Groups of patients: Visual Analog Scale (VAS) completed by physicians and physiotherapists - A priori hypotheses: Not stated - Were hypotheses confirmed: Not applicable - Results: Spearman rank correlation; p Not stated for all results High correlation between the VAS completed by physicians (0.88) and physiotherapists (0.91) and the MFM-32 - Population/Disease: Patients with muscular disease (mean age 24.5 years+15.4 (6–62 years); n= 303 Jansen (2012) KNown-groups validity 1-Measure/Groups of patients: Ambulatory patients (n= 18) vs Wheelchair-dependent patients (n= 12) - Apriori hypotheses: Not stated - Were hypotheses confirmed: Not applicable - Results: Method Not stated. Ambulatory patients had significantly higher MFM (%) scores (75.0 + 9.3 (54.2–91.7) than wheelchair-dependent patients (52.8 + 8.5 (32.3–61.5)); p< 0.01 Clinical validity 2-Measure/Groups of patients: Assisted 6-Minute Cycling Test (A6MCT) - Apriori hypotheses: Not stated - Were hypotheses confirmed: Not applicable - Results: Spearman correlation - The number of revolutions achieved with the A6MCT for legs was positively correlated with the MFM in the total group of boys with DMD (rho= 0.65, p< 0.01), the ambulatory boys (rho= 0.72, p< 0.01), and the wheelchair-dependent boys (rho= 0.74, p= 0.01). This means that the number of revolutions achieved with the A6MCT for legs decreased with a decrease in motor function - A similar positive correlation between the A6MCT for arms and the MFM was found for wheelchair-dependent boys (rho= 0.84, p< 0.01) - Population/Disease: Boys with Duchenne muscular dystrophy (DMD) (mean age 10.5 + 2.6, age range 6.4–16.6); n= 30 Trundell (2020) Clinical validity 1-Measure/Groups of patients: CGI-S (Clinical Global Impression of Severity) score; VigNos Grade - Apriori hypotheses: Not stated - Were hypotheses confirmed: Not applicable - Results: Spearman rank correlation; p< 0.0001 for all results - There was a significant correlation between the MFM32 and the CGI-S (rho= -0.84) and the VigNos Grade (rho= -0.79) - Population/Disease: Children with neuromuscular diseases (age range 2-5 years, mean age 4.87 years); n= 37-47 2-Measure/Groups of patients: CGI-S (Clinical Global Impression of Severity) score - Apriori hypotheses: Not stated - Were hypotheses confirmed: Not applicable - Results: Spearman rank correlation - There was a significant correlation between the MFM32 and the CGI-S (rho= -0.49; p< 0.001) - Population/Disease: Patients with SMA Type 2 and 3 (age range 2-25 years, mean age 11.76 years); n= 51 KNown-groups validity 3-Measure/Groups of patients: Patients grouped according to disease severity as assessed by CGI-S score (Mild/Moderate vs Severe/Very severe) and VigNos Grade (Grade 1-5 vs Grade 6-10); n per groups Not stated - Apriori hypotheses: Not stated - Were hypotheses confirmed: Not applicable - Results: ANOVA; p< 0.0001 for all results - MFM-32 Least square (LS) means were significantly higher in the groups with less disease severity than in the groups with higher disease severity. LS mean differences for CGI-S were 34.51 (95% confidence interval [CI] 25.8–43.2) and for the VigNos Grade 39.24 (95% CI 29.9–48.6) - Population/Disease: Children with neuromuscular diseases (age range 2-5 years, mean age 4.87 years); n Not stated 4-Measure/Groups of patients: Patients grouped according to disease severity as assessed by CGI-S score (Mild/Moderate vs Severe/Very severe); n per group Not stated - Apriori hypotheses: Not stated - Were hypotheses confirmed: Not applicable - Results: ANOVA - MFM-32 Least square (LS) means were significantly higher in the groups with less disease severity than in the groups with higher disease severity. LS mean differences for CGI-S were 25.56 (95% CI 11.8–39.3); p< 0.001 - Population/Disease: Patients with SMA Type 2 and 3 (age range 2-25 years, mean age 11.76 years); n Not stated Okama LO (2017) . Measure/Groups of patients: North Star Ambulatory Assessment (NSAA) - A priori hypotheses: Correlation would be found - Were hypotheses confirmed: Yes - Results: Spearman's coefficient correlation Significant correlations were found between MFM and NSAA items (except item 10 and 12: "Gets to sitting" and "Lifts head"; r= 0.494 to 0.842; p<0.01 to 0.05 Significant correlation was food between MFM and NSAA total scores: r= 0.863; p<0.01 - Population/Disease: Infants and Children with (n= 35)or without DMD n= 73 age: 4-15 years for DMD sample and 5-13 control sample Servais L (2013) . Measure/Groups of patients: Handgrip and Key pinch assessed with the MyoPinch - A priori hypotheses: Not stated - Were hypotheses confirmed: Not applicable - Results: p<0.01 for all results Significant correlation was found between MFM and Handgrip: r= 0.874 Significant correlation was found between MFM D3 and Handgrip: r= 0.831 Significant correlation was found between MFM and Key pinch r= 0.854 Significant correlation was found between MFM D3 and Key pinch r= 0.806 - Population/Disease: Patients with genetically confirmed DMD (n=30) and age-matched healthy control subjects (n= 30), n= 60 in total, age of patients 16.8 +/- 4.4 (10-27.7) years and age of controls: 16.3 +/- 5.5 (8.2-8) years . Measure/Groups of patients: wrist flexion and wrist extension strength assessed with the MyoWrist - A priori hypotheses: Not stated - Were hypotheses confirmed: Not applicable - Results: Significant correlation was found between MFM and wrist flexion r= 0.769 Significant correlation was found between MFM D3 and wrist flexion r= 0.733 Significant correlation was found between MFM and wrist extension r= 0.795 Significant correlation was found between MFM D3 and wrist extension r= 0.591 - Population/Disease: Patients with genetically confirmed DMD (n=30) and age-matched healthy control subjects (n= 30), n= 60 in total, age of patients 16.8 +/- 4.4 (10-27.7) years and age of controls: 16.3 +/- 5.5 (8.2-8) years Seferian AM (2015) 1. Measure/Groups of patients: MyoGrip-Non Dominant, MyoGrip-Dominant - A priori hypotheses: Not stated - Were hypotheses confirmed: Not applicable - Results: Spearman's correlation coefficient; p<0.01 for all results Significant correlation was found between MFM-D2 and MyoGrip-Non Dominant, rho= 0.77 Significant correlation was found between MFM-D3 and MyoGrip-Non Dominant,rho= 0.86 Significant correlation was found between MFM-Total and MyoGrip-Non Dominant, rho= 0.82 Significant correlation was found between MFM-D2 and MyoGrip Dominant, rho= 0.78 Significant correlation was found between MFM-D3 and MyoGrip Dominant, rho= 0.87 Significant correlation was found between MFM-Total and MyoGrip Dominant, rho= 0.82 - Population/Disease: Patients with DMD, n= 50 to 53, age: mean= 17.1 (4.8) and median= 16.5 (9-28.1) 2.Measure/Groups of patients: MyoPïnch-Non Dominant, MyoPinch-Dominant - A priori hypotheses: Not stated - Were hypotheses confirmed: Not applicable - Results: Spearman's correlation coefficient; p<0.01 for all results Significant correlation was found between MFM-D2 and MyoPïnch-Non Dominant, rho= 0.77 Significant correlation was found between MFM-D3 and MyoPïnch-Non Dominant,rho= 0.82 Significant correlation was found between MFM-Total and MyoPïnch-Non Dominant, rho= 0.81 Significant correlation was found between MFM-D2 and MyoPinch-Dominant, rho= 0.81 Significant correlation was found between MFM-D3 and MyoPinch-Dominant, rho= 0.86 Significant correlation was found between MFM-Total and MyoPinch-Dominant, rho= 0.84 - Population/Disease: Patients with DMD, n= 50 to 53, age: mean= 17.1 (4.8) and median= 16.5 (9-28.1) 3.Measure/Groups of patients: Forced Vital Capacity - A priori hypotheses: Not stated - Were hypotheses confirmed: Not applicable - Results: Spearman's correlation coefficient; p<0.01 for all results Significant correlation was found between MFM-D2 and FVC: rho = 0.70 Significant correlation was found between MFM-D3 and FVC: rho = 0.62 Significant correlation was found between MFM-Total and FVC: rho = 0.72 - Population/Disease: Patients with DMD, n= 50 to 53, age: mean= 17.1 (4.8) and median= 16.5 (9-28.1)

Evidence of Translatability Assessment: None identified

Evidence related to missing data: None identified

Evidence for Selection of Recall Period: None identified

Evidence of Administration Instructions and Training Provided: None identified

Evidence of concurrent validity: Yes

Evidence of known-groups validity: Yes

Evidence of ability to detect change over time: Yes


Ability to Detect Change

Ability to detect change (Responsiveness):

Vuillerot (2010)
A threshold value for loss of ambulation (total score 63.6% (range 54.7–70.8%) and 25.0% (range 16.7–33.3%) for the Standing and transfers domain) and a predictive value 1 year before loss (total score 70% and 40% for the Standing and transfers domain) were estimated using linear interpolation
- Population/Disease: Patients with Duchenne
muscular dystrophy (DMD) (age range 7-12 years); n= 11


Responder Thresholds

Evidence of responder thresholds: None identified


Reference(s) of development / validation

Bérard C, Payan C, Hodgkinson I, Fermanian J; MFM Collaborative Study Group. A motor function measure for neuromuscular diseases. Construction and validation study. Neuromuscul Disord. 2005 Jul;15(7):463-70
PubMed Abstract: https://pubmed.ncbi.nlm.nih.gov/16106528/


Other references

Jansen M, De Jong M, Coes HM, Eggermont F, Van Alfen N, De Groot IJ. The assisted 6-minute cycling test to assess endurance in children with a neuromuscular disorder. Muscle Nerve. 2012 Oct;46(4):520-30
Abstract: https://pubmed.ncbi.nlm.nih.gov/22987692/

Vuillerot C, Girardot F, Payan C, Fermanian J, Iwaz J, De Lattre C, Berard C. Monitoring changes and predicting loss of ambulation in Duchenne muscular dystrophy with the Motor Function Measure. Dev Med Child Neurol. 2010 Jan;52(1):60-5
Full Text Article: https://onlinelibrary.wiley.com/doi/full/10.1111/j.1469-8749.2009.03316.x

Trundell D, Le Scouiller S, Gorni K, Seabrook T, Vuillerot C; SMA MFM Study Group. Validity and Reliability of the 32-Item Motor Function Measure in 2- to 5-Year-Olds with Neuromuscular Disorders and 2- to 25-Year-Olds with Spinal Muscular Atrophy. Neurol Ther. 2020 Dec;9(2):575-584
Full Text Article: https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7606363/

Servais L, Deconinck N, Moraux A, Benali M, Canal A, Van Parys F, Vereecke W, Wittevrongel S, Mayer M, Desguerre I, Maincent K, Themar-Noel C, QuijaNo-Roy S, Serari N, Voit T, Hogrel JY. InNovative methods to assess upper limb strength and function in Non-ambulant Duchenne patients. Neuromuscul Disord. 2013 Feb;23(2):139-48.
Full Text Article: https://pubmed.ncbi.nlm.nih.gov/23219352/

Okama LO, Zampieri LM, Ramos CL, Toledo FO, Alves CRJ, Mattiello-Sverzut AC, Mayhew A, Sobreira CFR. Reliability and validity analyses of the North Star Ambulatory Assessment in Brazilian Portuguese. Neuromuscul Disord. 2017 Aug;27(8):723-729.
PubMed Abstract: https://pubmed.ncbi.nlm.nih.gov/28648683/

Seferian AM, Moraux A, AnNoussamy M, Canal A, Decostre V, Diebate O, Le Moing AG, Gidaro T, Deconinck N, Van Parys F, Vereecke W, Wittevrongel S, Mayer M, Maincent K, Desguerre I, Thémar-Noël C, Cuisset JM, Tiffreau V, Denis S, Jousten V, QuijaNo-Roy S, Voit T, Hogrel JY, Servais L. Upper limb strength and function changes during a one-year follow-up in Non-ambulant patients with Duchenne Muscular Dystrophy: an observational multicenter trial. PLoS One. 2015 Feb 2;10(2):e0113999.
Full Text Article: https://pubmed.ncbi.nlm.nih.gov/25643053/

[Conference Abstract] Bulut N,Yardimci LokmaNoglu B, Aydin G, Kabakci F, Atci M, Gurbuz I, Topaloglu H, Karaduman A, Yilmaz O. EP.94Reliability and validity of trunk control measurement scale in Duchenne muscular dystrophy. Neuromuscular Disorders. Conference: 24the International Congress of the World Muscle Society. Tivoli Gardens, Copenhagen Denmark. 29 (Supplement 1) (pp S180), 2019. Date of Publication: October 2019.


Inclusion of the COA in product labelling

Yes


Existence of Scoring / Interpretation / User Manual


Original language and translations

Original: French and English

Translations:
Russian
Arabic
Chinese
Japanese
Czech
Polish
Italian
German
Dutch
Portuguese
Spanish
Turkish


References of translations

Chinese:
Huang M, Cao J, Sun J, Li W, Qin L, Li H, Zhai C, Huang W, Gui T, Zhang K, Wang J, Vuillerot C, Wang Y, Dai M. Cross-cultural Adaptation and Multi-centric Validation of the Motor Function Measure Chinese Version (MFM-32-CN) for Patients with Neuromuscular Diseases. Dev Neurorehabil. 2020 May;23(4):210-217 (PubMed abstract: https://pubmed.ncbi.nlm.nih.gov/31307263/)

Turkish:
İnal HS, Tarakçı E, Tarakçı D, Aksoy G, Mergen Kılıç S, Beşer H, Beşer Ç, Özdinçler AR, Durmuş Tekçe H, Parman FY, Deymeer F, Oflazer ZP. Turkish version of the Motor Function Measure Scale (MFM-32) for neuromuscular diseases: a cross-cultural adaptation, reliability, and validity study. Turk J Med Sci. 2017 Dec 19;47(6):1826-1833 (PubMed abstract: https://www.ncbi.nlm.nih.gov/pubmed/29306245)


Authors and contact information

Author:
Carole Vuillerot MD, PhD
Chef de service L’Escale
Hospital Femme Mère Enfant
Lyon
France
Phone: 04.72.12.94.50
E-mail: carole.vuillerot@chu-lyon.fr

Contact:
MFM Group
E-mail: contact@mfm-nmd.org

Contact form (https://mfm-nmd.org/contact/)


Website

MFM website (https://mfm-nmd.org/)


Review copy

List of items available in Bérard C et al, 2005