Glatiramer acetate in primary progressive multiple sclerosis: Results of a multinational, multicenter, double-blind, placebo-controlled trial

Jerry S. Wolinsky; Ponnada A. Narayana; Paul O'Connor; Patricia K. Coyle; Corey Ford; Kenneth Johnson; Aaron Miller; Lillian Pardo; Shaul Kadosh; David Ladkani; Lorne Kastrukoff; Pierre Duquette; Mark Freedman; Marc Debouverie; Catherine Lubetski; Gilles Edan; Etienne Roullet; Christian Confavreux; Alan Thompson; Lance Blumhardt; Stanley Hawkins; Thomas Scott; Daniel Wynn; Joanna Cooper; Stephen Thurston; Stanton Elias; Clyde Markowitz; David Mattson; John Noseworthy; Elizabeth Shuster; Jonathan Carter; Fred Lublin; William Stuart; Michael Kaufman; Gary Birnbaum; Kottil Rammohan; Ruth Whitham; Cornelia Mihai; Steven Greenberg; Craig Smith; Mark Agius; Stan Van Den Noort; Lawrence Myers; James Nelson; Douglas Goodin; Barry Arnason; Khurram Bashir; Sharon Lynch; Patricia Coyle; Stephen Kamin; William Sheremata; Galen Mitchell; Andrew Goodman; Norman Kachuck; Peter Dunne; J. William Lindsey; Elliot Frohman; James Bowen; Benjamin Brooks; John Rose; Harold Moses; Douglas Jeffrey; Ann Cross; Robert Lisak; Tim Vollmer; Jack Antel; Gary Cutter; Luanne Metz; Henry McFarland; Steven Reingold; Fred D. Lublin; Irina Vainrub; Lucie Lambert; Fengwei Zhong; Jeff Rasmituth; Saria Momin; Rivka Kreitman; Galia Shifroni; Irit Pinchasi; Yafit Stark

doi:10.1002/ana.21079

Glatiramer acetate in primary progressive multiple sclerosis: Results of a multinational, multicenter, double-blind, placebo-controlled trial

Jerry S. Wolinsky, Ponnada A. Narayana, Paul O'Connor, Patricia K. Coyle, Corey Ford, Kenneth Johnson, Aaron Miller, Lillian Pardo, Shaul Kadosh, David Ladkani, Lorne Kastrukoff, Pierre Duquette, Mark Freedman, Marc Debouverie, Catherine Lubetski, Gilles Edan, Etienne Roullet, Christian Confavreux, Alan Thompson, Lance BlumhardtStanley Hawkins, Thomas Scott, Daniel Wynn, Joanna Cooper, Stephen Thurston, Stanton Elias, Clyde Markowitz, David Mattson, John Noseworthy, Elizabeth Shuster, Jonathan Carter, Fred Lublin, William Stuart, Michael Kaufman, Gary Birnbaum, Kottil Rammohan, Ruth Whitham, Cornelia Mihai, Steven Greenberg, Craig Smith, Mark Agius, Stan Van Den Noort, Lawrence Myers, James Nelson, Douglas Goodin, Barry Arnason, Khurram Bashir, Sharon Lynch, Patricia Coyle, Stephen Kamin, William Sheremata, Galen Mitchell, Andrew Goodman, Norman Kachuck, Peter Dunne, J. William Lindsey, Elliot Frohman, James Bowen, Benjamin Brooks, John Rose, Harold Moses, Douglas Jeffrey, Ann Cross, Robert Lisak, Tim Vollmer, Jack Antel, Gary Cutter, Luanne Metz, Henry McFarland, Steven Reingold, Fred D. Lublin, Irina Vainrub, Lucie Lambert, Fengwei Zhong, Jeff Rasmituth, Saria Momin, Rivka Kreitman, Galia Shifroni, Irit Pinchasi, Yafit Stark

Research output: Contribution to journal › Article › peer-review

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Abstract

Objective: To determine whether glatiramer acetate (GA) slows accumulation of disability in primary progressive multiple sclerosis. Methods: A total of 943 patients with primary progressive multiple sclerosis were randomized to GA or placebo (PBO) in this 3-year, double-blind trial. The primary end point was an intention-to-treat analysis of time to 1- (entry expanded disability status scale, 3.0-5.0) or 0.5-point expanded disability status scale change (entry expanded disability status scale, 5.5-6.5) sustained for 3 months. The trial was stopped after an interim analysis by an independent data safety monitoring board indicated no discernible treatment effect on the primary outcome. Intention-to-treat analyses of disability and magnetic resonance imaging end points were performed. Results: There was a nonsignificant delay in time to sustained accumulated disability in GA- versus PBO-treated patients (hazard ratio, 0.87 [95% confidence interval, 0.71-1.07]; p = 0.1753), with significant decreases in enhancing lesions in year 1 and smaller increases in T2 lesion volumes in years 2 and 3 versus PBO. Post hoc analysis showed that survival curves for GA-treated male patients diverged early from PBO-treated male subjects (hazard ratio, 0.71 [95% confidence interval, 0.53-0.95]; p = 0.0193). Interpretation: The trial failed to demonstrate a treatment effect of GA on primary progressive multiple sclerosis. Both the unanticipated low event rate and premature discontinuation of study medication decreased the power to detect a treatment effect. Post hoc analysis suggests GA may have slowed clinical progression in male patients who showed more rapid progression when untreated.

Original language	English (US)
Pages (from-to)	14-24
Number of pages	11
Journal	Annals of Neurology
Volume	61
Issue number	1
DOIs	https://doi.org/10.1002/ana.21079
State	Published - Jan 1 2007

ASJC Scopus subject areas

Neurology
Clinical Neurology

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Wolinsky, J. S., Narayana, P. A., O'Connor, P., Coyle, P. K., Ford, C., Johnson, K., Miller, A., Pardo, L., Kadosh, S., Ladkani, D., Kastrukoff, L., Duquette, P., Freedman, M., Debouverie, M., Lubetski, C., Edan, G., Roullet, E., Confavreux, C., Thompson, A., ... Stark, Y. (2007). Glatiramer acetate in primary progressive multiple sclerosis: Results of a multinational, multicenter, double-blind, placebo-controlled trial. Annals of Neurology, 61(1), 14-24. https://doi.org/10.1002/ana.21079

Wolinsky, JS, Narayana, PA, O'Connor, P, Coyle, PK, Ford, C, Johnson, K, Miller, A, Pardo, L, Kadosh, S, Ladkani, D, Kastrukoff, L, Duquette, P, Freedman, M, Debouverie, M, Lubetski, C, Edan, G, Roullet, E, Confavreux, C, Thompson, A, Blumhardt, L, Hawkins, S, Scott, T, Wynn, D, Cooper, J, Thurston, S, Elias, S, Markowitz, C, Mattson, D, Noseworthy, J, Shuster, E, Carter, J, Lublin, F, Stuart, W, Kaufman, M, Birnbaum, G, Rammohan, K, Whitham, R, Mihai, C, Greenberg, S, Smith, C, Agius, M, Van Den Noort, S, Myers, L, Nelson, J, Goodin, D, Arnason, B, Bashir, K, Lynch, S, Coyle, P, Kamin, S, Sheremata, W, Mitchell, G, Goodman, A, Kachuck, N, Dunne, P, Lindsey, JW, Frohman, E, Bowen, J, Brooks, B, Rose, J, Moses, H, Jeffrey, D, Cross, A, Lisak, R, Vollmer, T, Antel, J, Cutter, G, Metz, L, McFarland, H, Reingold, S, Lublin, FD, Vainrub, I, Lambert, L, Zhong, F, Rasmituth, J, Momin, S, Kreitman, R, Shifroni, G, Pinchasi, I & Stark, Y 2007, 'Glatiramer acetate in primary progressive multiple sclerosis: Results of a multinational, multicenter, double-blind, placebo-controlled trial', Annals of Neurology, vol. 61, no. 1, pp. 14-24. https://doi.org/10.1002/ana.21079

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title = "Glatiramer acetate in primary progressive multiple sclerosis: Results of a multinational, multicenter, double-blind, placebo-controlled trial",

abstract = "Objective: To determine whether glatiramer acetate (GA) slows accumulation of disability in primary progressive multiple sclerosis. Methods: A total of 943 patients with primary progressive multiple sclerosis were randomized to GA or placebo (PBO) in this 3-year, double-blind trial. The primary end point was an intention-to-treat analysis of time to 1- (entry expanded disability status scale, 3.0-5.0) or 0.5-point expanded disability status scale change (entry expanded disability status scale, 5.5-6.5) sustained for 3 months. The trial was stopped after an interim analysis by an independent data safety monitoring board indicated no discernible treatment effect on the primary outcome. Intention-to-treat analyses of disability and magnetic resonance imaging end points were performed. Results: There was a nonsignificant delay in time to sustained accumulated disability in GA- versus PBO-treated patients (hazard ratio, 0.87 [95% confidence interval, 0.71-1.07]; p = 0.1753), with significant decreases in enhancing lesions in year 1 and smaller increases in T2 lesion volumes in years 2 and 3 versus PBO. Post hoc analysis showed that survival curves for GA-treated male patients diverged early from PBO-treated male subjects (hazard ratio, 0.71 [95% confidence interval, 0.53-0.95]; p = 0.0193). Interpretation: The trial failed to demonstrate a treatment effect of GA on primary progressive multiple sclerosis. Both the unanticipated low event rate and premature discontinuation of study medication decreased the power to detect a treatment effect. Post hoc analysis suggests GA may have slowed clinical progression in male patients who showed more rapid progression when untreated.",

author = "Wolinsky, {Jerry S.} and Narayana, {Ponnada A.} and Paul O'Connor and Coyle, {Patricia K.} and Corey Ford and Kenneth Johnson and Aaron Miller and Lillian Pardo and Shaul Kadosh and David Ladkani and Lorne Kastrukoff and Pierre Duquette and Mark Freedman and Marc Debouverie and Catherine Lubetski and Gilles Edan and Etienne Roullet and Christian Confavreux and Alan Thompson and Lance Blumhardt and Stanley Hawkins and Thomas Scott and Daniel Wynn and Joanna Cooper and Stephen Thurston and Stanton Elias and Clyde Markowitz and David Mattson and John Noseworthy and Elizabeth Shuster and Jonathan Carter and Fred Lublin and William Stuart and Michael Kaufman and Gary Birnbaum and Kottil Rammohan and Ruth Whitham and Cornelia Mihai and Steven Greenberg and Craig Smith and Mark Agius and {Van Den Noort}, Stan and Lawrence Myers and James Nelson and Douglas Goodin and Barry Arnason and Khurram Bashir and Sharon Lynch and Patricia Coyle and Stephen Kamin and William Sheremata and Galen Mitchell and Andrew Goodman and Norman Kachuck and Peter Dunne and Lindsey, {J. William} and Elliot Frohman and James Bowen and Benjamin Brooks and John Rose and Harold Moses and Douglas Jeffrey and Ann Cross and Robert Lisak and Tim Vollmer and Jack Antel and Gary Cutter and Luanne Metz and Henry McFarland and Steven Reingold and Lublin, {Fred D.} and Irina Vainrub and Lucie Lambert and Fengwei Zhong and Jeff Rasmituth and Saria Momin and Rivka Kreitman and Galia Shifroni and Irit Pinchasi and Yafit Stark",

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day = "1",

doi = "10.1002/ana.21079",

language = "English (US)",

volume = "61",

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journal = "Annals of Neurology",

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T1 - Glatiramer acetate in primary progressive multiple sclerosis

T2 - Results of a multinational, multicenter, double-blind, placebo-controlled trial

AU - Wolinsky, Jerry S.

AU - Narayana, Ponnada A.

AU - O'Connor, Paul

AU - Coyle, Patricia K.

AU - Ford, Corey

AU - Johnson, Kenneth

AU - Miller, Aaron

AU - Pardo, Lillian

AU - Kadosh, Shaul

AU - Ladkani, David

AU - Kastrukoff, Lorne

AU - Duquette, Pierre

AU - Freedman, Mark

AU - Debouverie, Marc

AU - Lubetski, Catherine

AU - Edan, Gilles

AU - Roullet, Etienne

AU - Confavreux, Christian

AU - Thompson, Alan

AU - Blumhardt, Lance

AU - Hawkins, Stanley

AU - Scott, Thomas

AU - Wynn, Daniel

AU - Cooper, Joanna

AU - Thurston, Stephen

AU - Elias, Stanton

AU - Markowitz, Clyde

AU - Mattson, David

AU - Noseworthy, John

AU - Shuster, Elizabeth

AU - Carter, Jonathan

AU - Lublin, Fred

AU - Stuart, William

AU - Kaufman, Michael

AU - Birnbaum, Gary

AU - Rammohan, Kottil

AU - Whitham, Ruth

AU - Mihai, Cornelia

AU - Greenberg, Steven

AU - Smith, Craig

AU - Agius, Mark

AU - Van Den Noort, Stan

AU - Myers, Lawrence

AU - Nelson, James

AU - Goodin, Douglas

AU - Arnason, Barry

AU - Bashir, Khurram

AU - Lynch, Sharon

AU - Coyle, Patricia

AU - Kamin, Stephen

AU - Sheremata, William

AU - Mitchell, Galen

AU - Goodman, Andrew

AU - Kachuck, Norman

AU - Dunne, Peter

AU - Lindsey, J. William

AU - Frohman, Elliot

AU - Bowen, James

AU - Brooks, Benjamin

AU - Rose, John

AU - Moses, Harold

AU - Jeffrey, Douglas

AU - Cross, Ann

AU - Lisak, Robert

AU - Vollmer, Tim

AU - Antel, Jack

AU - Cutter, Gary

AU - Metz, Luanne

AU - McFarland, Henry

AU - Reingold, Steven

AU - Lublin, Fred D.

AU - Vainrub, Irina

AU - Lambert, Lucie

AU - Zhong, Fengwei

AU - Rasmituth, Jeff

AU - Momin, Saria

AU - Kreitman, Rivka

AU - Shifroni, Galia

AU - Pinchasi, Irit

AU - Stark, Yafit

PY - 2007/1/1

Y1 - 2007/1/1

N2 - Objective: To determine whether glatiramer acetate (GA) slows accumulation of disability in primary progressive multiple sclerosis. Methods: A total of 943 patients with primary progressive multiple sclerosis were randomized to GA or placebo (PBO) in this 3-year, double-blind trial. The primary end point was an intention-to-treat analysis of time to 1- (entry expanded disability status scale, 3.0-5.0) or 0.5-point expanded disability status scale change (entry expanded disability status scale, 5.5-6.5) sustained for 3 months. The trial was stopped after an interim analysis by an independent data safety monitoring board indicated no discernible treatment effect on the primary outcome. Intention-to-treat analyses of disability and magnetic resonance imaging end points were performed. Results: There was a nonsignificant delay in time to sustained accumulated disability in GA- versus PBO-treated patients (hazard ratio, 0.87 [95% confidence interval, 0.71-1.07]; p = 0.1753), with significant decreases in enhancing lesions in year 1 and smaller increases in T2 lesion volumes in years 2 and 3 versus PBO. Post hoc analysis showed that survival curves for GA-treated male patients diverged early from PBO-treated male subjects (hazard ratio, 0.71 [95% confidence interval, 0.53-0.95]; p = 0.0193). Interpretation: The trial failed to demonstrate a treatment effect of GA on primary progressive multiple sclerosis. Both the unanticipated low event rate and premature discontinuation of study medication decreased the power to detect a treatment effect. Post hoc analysis suggests GA may have slowed clinical progression in male patients who showed more rapid progression when untreated.

AB - Objective: To determine whether glatiramer acetate (GA) slows accumulation of disability in primary progressive multiple sclerosis. Methods: A total of 943 patients with primary progressive multiple sclerosis were randomized to GA or placebo (PBO) in this 3-year, double-blind trial. The primary end point was an intention-to-treat analysis of time to 1- (entry expanded disability status scale, 3.0-5.0) or 0.5-point expanded disability status scale change (entry expanded disability status scale, 5.5-6.5) sustained for 3 months. The trial was stopped after an interim analysis by an independent data safety monitoring board indicated no discernible treatment effect on the primary outcome. Intention-to-treat analyses of disability and magnetic resonance imaging end points were performed. Results: There was a nonsignificant delay in time to sustained accumulated disability in GA- versus PBO-treated patients (hazard ratio, 0.87 [95% confidence interval, 0.71-1.07]; p = 0.1753), with significant decreases in enhancing lesions in year 1 and smaller increases in T2 lesion volumes in years 2 and 3 versus PBO. Post hoc analysis showed that survival curves for GA-treated male patients diverged early from PBO-treated male subjects (hazard ratio, 0.71 [95% confidence interval, 0.53-0.95]; p = 0.0193). Interpretation: The trial failed to demonstrate a treatment effect of GA on primary progressive multiple sclerosis. Both the unanticipated low event rate and premature discontinuation of study medication decreased the power to detect a treatment effect. Post hoc analysis suggests GA may have slowed clinical progression in male patients who showed more rapid progression when untreated.

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Glatiramer acetate in primary progressive multiple sclerosis: Results of a multinational, multicenter, double-blind, placebo-controlled trial

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