The NorthStar Ambulatory Assessment in Duchenne muscular dystrophy: considerations for the design of clinical trials

V Ricotti; DA Ridout; Marika Pane; M Main; A Mayhew; Eugenio Maria Mercuri; AY Manzur; F Muntoni; S Robb; R Quinlivan; A Sarkozy; J Butler; K Bushby; V Straub; M Guglieri; M Eagle; H Roper; H McMurchie; A Childs; K Pysden; L Pallant; S Spinty; G Peachey; A Shillington; E Wraige; H Jungbluth; J Sheehan; R Spahr; I Hughes; E Bateman; C Cammiss; T Willis; L Groves; N Emery; P Baxter; M Senior; E Scott; L Hartley; B Parsons; A Majumdar; L Jenkins; B Toms; K Naismith; A Keddie; I Horrocks; M Di Marco; G Chow; A Miah; C de Goede; N Thomas; M Geary; J Palmer; C White; K Greenfield; I Wilson; S Messina; A Berardinelli; G Comi; A D'Amico; E Bertini; C Bruno; L Politano; R Battini; E Pegoraro; A Pini; T Mongini; L Morandi

doi:10.1136/jnnp-2014-309405

The NorthStar Ambulatory Assessment in Duchenne muscular dystrophy: considerations for the design of clinical trials

V Ricotti, DA Ridout, Marika Pane, M Main, A Mayhew, Eugenio Maria Mercuri, AY Manzur, F Muntoni^*, S Robb, R Quinlivan, A Sarkozy, J Butler, K Bushby, V Straub, M Guglieri, M Eagle, H Roper, H McMurchie, A Childs, K PysdenL Pallant, S Spinty, G Peachey, A Shillington, E Wraige, H Jungbluth, J Sheehan, R Spahr, I Hughes, E Bateman, C Cammiss, T Willis, L Groves, N Emery, P Baxter, M Senior, E Scott, L Hartley, B Parsons, A Majumdar, L Jenkins, B Toms, K Naismith, A Keddie, I Horrocks, M Di Marco, G Chow, A Miah, C de Goede, N Thomas, M Geary, J Palmer, C White, K Greenfield, I Wilson, S Messina, A Berardinelli, G Comi, A D'Amico, E Bertini, C Bruno, L Politano, R Battini, E Pegoraro, A Pini, T Mongini, L Morandi

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63 Citazioni (Scopus)

Abstract

Objective With the emergence of experimental therapies for Duchenne muscular dystrophy (DMD), it is fundamental to understand the natural history of this disorder to properly design clinical trials. The aims of this study were to assess the effects produced on motor function by different DMD genotypes and early initiation of glucocorticoids.Methods Through the NorthStar Network, standardised clinical data including the NorthStar Ambulatory Assessment score (NSAA) on 513 ambulant UK boys with DMD were analysed from 2004 to 2012. For the analysis of the genetic subpopulation, we also included data from 172 Italian boys with DMD. NSAA raw scores were converted into linear scores.Results On the linearised NSAA, we observed an average decline of 8 units/year (4 units on raw NSAA analysis) after age 7. The median age at loss of ambulation (LOA) was 13 years (95% CI 12.1 to 13.5); 2 years prior to LOA, the estimated mean linearised NSAA score was 42/100 (13/34 raw scale). Starting glucocorticoids between 3 and 5 years conferred an additional gain in motor function of 3 units/year (1.3 raw units) up to age 7. When analysing the effect of genotype in the UK and Italian cumulative cohorts, individuals with deletions amenable to exons 44 and 46 skipping declined at a slower rate over 2 years (9 units (4 raw units), p<0.001), while 53 and 51 skippable deletions showed a faster decline of 14 (4.5; p<0.001) and 5 linearised units (2.4 NSAA units; p=0.02), respectively.Conclusions Our study provides a novel insight on the current natural history of DMD, which will be instrumental for the design of future clinical trials.

Lingua originale	Inglese
pagine (da-a)	149-155
Numero di pagine	7
Rivista	Journal of Neurology, Neurosurgery and Psychiatry
Volume	87
Numero di pubblicazione	2
DOI	https://doi.org/10.1136/jnnp-2014-309405
Stato di pubblicazione	Pubblicato - 2016

All Science Journal Classification (ASJC) codes

Chirurgia
Neurologia (clinica)
Psichiatria e Salute Mentale

Keywords

N/A

Accesso al documento

10.1136/jnnp-2014-309405

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Ricotti, V., Ridout, DA., Pane, M., Main, M., Mayhew, A., Mercuri, E. M., Manzur, AY., Muntoni, F., Robb, S., Quinlivan, R., Sarkozy, A., Butler, J., Bushby, K., Straub, V., Guglieri, M., Eagle, M., Roper, H., McMurchie, H., Childs, A., ... Morandi, L. (2016). The NorthStar Ambulatory Assessment in Duchenne muscular dystrophy: considerations for the design of clinical trials. Journal of Neurology, Neurosurgery and Psychiatry, 87(2), 149-155. https://doi.org/10.1136/jnnp-2014-309405

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abstract = "Objective With the emergence of experimental therapies for Duchenne muscular dystrophy (DMD), it is fundamental to understand the natural history of this disorder to properly design clinical trials. The aims of this study were to assess the effects produced on motor function by different DMD genotypes and early initiation of glucocorticoids.Methods Through the NorthStar Network, standardised clinical data including the NorthStar Ambulatory Assessment score (NSAA) on 513 ambulant UK boys with DMD were analysed from 2004 to 2012. For the analysis of the genetic subpopulation, we also included data from 172 Italian boys with DMD. NSAA raw scores were converted into linear scores.Results On the linearised NSAA, we observed an average decline of 8 units/year (4 units on raw NSAA analysis) after age 7. The median age at loss of ambulation (LOA) was 13 years (95% CI 12.1 to 13.5); 2 years prior to LOA, the estimated mean linearised NSAA score was 42/100 (13/34 raw scale). Starting glucocorticoids between 3 and 5 years conferred an additional gain in motor function of 3 units/year (1.3 raw units) up to age 7. When analysing the effect of genotype in the UK and Italian cumulative cohorts, individuals with deletions amenable to exons 44 and 46 skipping declined at a slower rate over 2 years (9 units (4 raw units), p<0.001), while 53 and 51 skippable deletions showed a faster decline of 14 (4.5; p<0.001) and 5 linearised units (2.4 NSAA units; p=0.02), respectively.Conclusions Our study provides a novel insight on the current natural history of DMD, which will be instrumental for the design of future clinical trials.",

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author = "V Ricotti and DA Ridout and Marika Pane and M Main and A Mayhew and Mercuri, {Eugenio Maria} and AY Manzur and F Muntoni and S Robb and R Quinlivan and A Sarkozy and J Butler and K Bushby and V Straub and M Guglieri and M Eagle and H Roper and H McMurchie and A Childs and K Pysden and L Pallant and S Spinty and G Peachey and A Shillington and E Wraige and H Jungbluth and J Sheehan and R Spahr and I Hughes and E Bateman and C Cammiss and T Willis and L Groves and N Emery and P Baxter and M Senior and E Scott and L Hartley and B Parsons and A Majumdar and L Jenkins and B Toms and K Naismith and A Keddie and I Horrocks and {Di Marco}, M and G Chow and A Miah and {de Goede}, C and N Thomas and M Geary and J Palmer and C White and K Greenfield and I Wilson and S Messina and A Berardinelli and G Comi and A D'Amico and E Bertini and C Bruno and L Politano and R Battini and E Pegoraro and A Pini and T Mongini and L Morandi",

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doi = "10.1136/jnnp-2014-309405",

language = "English",

volume = "87",

pages = "149--155",

journal = "Journal of Neurology, Neurosurgery and Psychiatry",

issn = "0022-3050",

publisher = "BMJ / British Medical Journal Publishing Group:PO Box 299, London WC1H 9TD United Kingdom:011 44 20 73836270, EMAIL: [email protected], INTERNET: http://www.bmjpg.com/bmj, Fax: 011 44 20 73836402",

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Ricotti, V, Ridout, DA, Pane, M, Main, M, Mayhew, A, Mercuri, EM, Manzur, AY, Muntoni, F, Robb, S, Quinlivan, R, Sarkozy, A, Butler, J, Bushby, K, Straub, V, Guglieri, M, Eagle, M, Roper, H, McMurchie, H, Childs, A, Pysden, K, Pallant, L, Spinty, S, Peachey, G, Shillington, A, Wraige, E, Jungbluth, H, Sheehan, J, Spahr, R, Hughes, I, Bateman, E, Cammiss, C, Willis, T, Groves, L, Emery, N, Baxter, P, Senior, M, Scott, E, Hartley, L, Parsons, B, Majumdar, A, Jenkins, L, Toms, B, Naismith, K, Keddie, A, Horrocks, I, Di Marco, M, Chow, G, Miah, A, de Goede, C, Thomas, N, Geary, M, Palmer, J, White, C, Greenfield, K, Wilson, I, Messina, S, Berardinelli, A, Comi, G, D'Amico, A, Bertini, E, Bruno, C, Politano, L, Battini, R, Pegoraro, E, Pini, A, Mongini, T & Morandi, L 2016, 'The NorthStar Ambulatory Assessment in Duchenne muscular dystrophy: considerations for the design of clinical trials', Journal of Neurology, Neurosurgery and Psychiatry, vol. 87, n. 2, pagg. 149-155. https://doi.org/10.1136/jnnp-2014-309405

TY - JOUR

T1 - The NorthStar Ambulatory Assessment in Duchenne muscular dystrophy: considerations for the design of clinical trials

AU - Ricotti, V

AU - Ridout, DA

AU - Pane, Marika

AU - Main, M

AU - Mayhew, A

AU - Mercuri, Eugenio Maria

AU - Manzur, AY

AU - Muntoni, F

AU - Robb, S

AU - Quinlivan, R

AU - Sarkozy, A

AU - Butler, J

AU - Bushby, K

AU - Straub, V

AU - Guglieri, M

AU - Eagle, M

AU - Roper, H

AU - McMurchie, H

AU - Childs, A

AU - Pysden, K

AU - Pallant, L

AU - Spinty, S

AU - Peachey, G

AU - Shillington, A

AU - Wraige, E

AU - Jungbluth, H

AU - Sheehan, J

AU - Spahr, R

AU - Hughes, I

AU - Bateman, E

AU - Cammiss, C

AU - Willis, T

AU - Groves, L

AU - Emery, N

AU - Baxter, P

AU - Senior, M

AU - Scott, E

AU - Hartley, L

AU - Parsons, B

AU - Majumdar, A

AU - Jenkins, L

AU - Toms, B

AU - Naismith, K

AU - Keddie, A

AU - Horrocks, I

AU - Di Marco, M

AU - Chow, G

AU - Miah, A

AU - de Goede, C

AU - Thomas, N

AU - Geary, M

AU - Palmer, J

AU - White, C

AU - Greenfield, K

AU - Wilson, I

AU - Messina, S

AU - Berardinelli, A

AU - Comi, G

AU - D'Amico, A

AU - Bertini, E

AU - Bruno, C

AU - Politano, L

AU - Battini, R

AU - Pegoraro, E

AU - Pini, A

AU - Mongini, T

AU - Morandi, L

PY - 2016

Y1 - 2016

N2 - Objective With the emergence of experimental therapies for Duchenne muscular dystrophy (DMD), it is fundamental to understand the natural history of this disorder to properly design clinical trials. The aims of this study were to assess the effects produced on motor function by different DMD genotypes and early initiation of glucocorticoids.Methods Through the NorthStar Network, standardised clinical data including the NorthStar Ambulatory Assessment score (NSAA) on 513 ambulant UK boys with DMD were analysed from 2004 to 2012. For the analysis of the genetic subpopulation, we also included data from 172 Italian boys with DMD. NSAA raw scores were converted into linear scores.Results On the linearised NSAA, we observed an average decline of 8 units/year (4 units on raw NSAA analysis) after age 7. The median age at loss of ambulation (LOA) was 13 years (95% CI 12.1 to 13.5); 2 years prior to LOA, the estimated mean linearised NSAA score was 42/100 (13/34 raw scale). Starting glucocorticoids between 3 and 5 years conferred an additional gain in motor function of 3 units/year (1.3 raw units) up to age 7. When analysing the effect of genotype in the UK and Italian cumulative cohorts, individuals with deletions amenable to exons 44 and 46 skipping declined at a slower rate over 2 years (9 units (4 raw units), p<0.001), while 53 and 51 skippable deletions showed a faster decline of 14 (4.5; p<0.001) and 5 linearised units (2.4 NSAA units; p=0.02), respectively.Conclusions Our study provides a novel insight on the current natural history of DMD, which will be instrumental for the design of future clinical trials.

AB - Objective With the emergence of experimental therapies for Duchenne muscular dystrophy (DMD), it is fundamental to understand the natural history of this disorder to properly design clinical trials. The aims of this study were to assess the effects produced on motor function by different DMD genotypes and early initiation of glucocorticoids.Methods Through the NorthStar Network, standardised clinical data including the NorthStar Ambulatory Assessment score (NSAA) on 513 ambulant UK boys with DMD were analysed from 2004 to 2012. For the analysis of the genetic subpopulation, we also included data from 172 Italian boys with DMD. NSAA raw scores were converted into linear scores.Results On the linearised NSAA, we observed an average decline of 8 units/year (4 units on raw NSAA analysis) after age 7. The median age at loss of ambulation (LOA) was 13 years (95% CI 12.1 to 13.5); 2 years prior to LOA, the estimated mean linearised NSAA score was 42/100 (13/34 raw scale). Starting glucocorticoids between 3 and 5 years conferred an additional gain in motor function of 3 units/year (1.3 raw units) up to age 7. When analysing the effect of genotype in the UK and Italian cumulative cohorts, individuals with deletions amenable to exons 44 and 46 skipping declined at a slower rate over 2 years (9 units (4 raw units), p<0.001), while 53 and 51 skippable deletions showed a faster decline of 14 (4.5; p<0.001) and 5 linearised units (2.4 NSAA units; p=0.02), respectively.Conclusions Our study provides a novel insight on the current natural history of DMD, which will be instrumental for the design of future clinical trials.

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U2 - 10.1136/jnnp-2014-309405

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SN - 0022-3050

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The NorthStar Ambulatory Assessment in Duchenne muscular dystrophy: considerations for the design of clinical trials

Abstract

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