A novel, efficient, randomized selection trial comparing combinations of drug therapy for ALS

Paul H. Gordon; Ying Kuen Cheung; Bruce Levin; Howard Andrews; Carolyn Doorish; Robert B. MacArthur; Jacqueline Montes; Kate Bednarz; Julaine Florence; Julie Rowin; Kevin Boylan; Tahseen Mozaffar; Rup Tandan; Hiroshi Mitsumoto; Elizabeth A. Kelvin; John Chapin; Richard Bedlack; Michael Rivner; Leo F. McCluskey; Alan Pestronk; Michael Graves; Eric J. Sorenson; Richard Barohn; Jerry M. Belsh; Jau Shin Lou; Todd Levine; David Saperstein; Robert G. Miller; Stephen N. Scelsa

doi:10.1080/17482960802195632

A novel, efficient, randomized selection trial comparing combinations of drug therapy for ALS

Paul H. Gordon, Ying Kuen Cheung, Bruce Levin, Howard Andrews, Carolyn Doorish, Robert B. MacArthur, Jacqueline Montes, Kate Bednarz, Julaine Florence, Julie Rowin, Kevin Boylan, Tahseen Mozaffar, Rup Tandan, Hiroshi Mitsumoto, Elizabeth A. Kelvin, John Chapin, Richard Bedlack, Michael Rivner, Leo F. McCluskey, Alan PestronkMichael Graves, Eric J. Sorenson, Richard Barohn, Jerry M. Belsh, Jau Shin Lou, Todd Levine, David Saperstein, Robert G. Miller, Stephen N. Scelsa

Neurology

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

70 Scopus citations

Abstract

Combining agents with different mechanisms of action may be necessary for meaningful results in treating ALS. The combinations of minocycline-creatine and celecoxib-creatine have additive effects in the murine model. New trial designs are needed to efficiently screen the growing number of potential neuroprotective agents. Our objective was to assess two drug combinations in ALS using a novel phase II trial design. We conducted a randomized, double-blind selection trial in sequential pools of 60 patients. Participants received minocycline (100 mg)-creatine (10 g) twice daily or celecoxib (400 mg)-creatine (10 g) twice daily for six months. The primary objective was treatment selection based on which combination best slowed deterioration in the ALS Functional Rating Scale-Revised (ALSFRS-R); the trial could be stopped after one pool if the difference between the two arms was adequately large. At trial conclusion, each arm was compared to a historical control group in a futility analysis. Safety measures were also examined. After the first patient pool, the mean six-month decline in ALSFRS-R was 5.27 (SD=5.54) in the celecoxib-creatine group and 6.47 (SD=9.14) in the minocycline-creatine group. The corresponding decline was 5.82 (SD=6.77) in the historical controls. The difference between the two sample means exceeded the stopping criterion. The null hypothesis of superiority was not rejected in the futility analysis. Skin rash occurred more frequently in the celecoxib-creatine group. In conclusion, the celecoxib-creatine combination was selected as preferable to the minocycline-creatine combination for further evaluation. This phase II design was efficient, leading to treatment selection after just 60 patients, and can be used in other phase II trials to assess different agents.

Original language	English (US)
Pages (from-to)	212-222
Number of pages	11
Journal	Amyotrophic Lateral Sclerosis
Volume	9
Issue number	4
DOIs	https://doi.org/10.1080/17482960802195632
State	Published - 2008

Keywords

ALS
Amyotrophic lateral sclerosis
Celecoxib
Clinical trial
Combination therapy
Creatine
Minocycline
Neuroprotection
Selection trial

ASJC Scopus subject areas

Neurology
Clinical Neurology

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10.1080/17482960802195632

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Gordon, P. H., Cheung, Y. K., Levin, B., Andrews, H., Doorish, C., MacArthur, R. B., Montes, J., Bednarz, K., Florence, J., Rowin, J., Boylan, K., Mozaffar, T., Tandan, R., Mitsumoto, H., Kelvin, E. A., Chapin, J., Bedlack, R., Rivner, M., McCluskey, L. F., ... Scelsa, S. N. (2008). A novel, efficient, randomized selection trial comparing combinations of drug therapy for ALS. Amyotrophic Lateral Sclerosis, 9(4), 212-222. https://doi.org/10.1080/17482960802195632

Gordon, PH, Cheung, YK, Levin, B, Andrews, H, Doorish, C, MacArthur, RB, Montes, J, Bednarz, K, Florence, J, Rowin, J, Boylan, K, Mozaffar, T, Tandan, R, Mitsumoto, H, Kelvin, EA, Chapin, J, Bedlack, R, Rivner, M, McCluskey, LF, Pestronk, A, Graves, M, Sorenson, EJ, Barohn, R, Belsh, JM, Lou, JS, Levine, T, Saperstein, D, Miller, RG & Scelsa, SN 2008, 'A novel, efficient, randomized selection trial comparing combinations of drug therapy for ALS', Amyotrophic Lateral Sclerosis, vol. 9, no. 4, pp. 212-222. https://doi.org/10.1080/17482960802195632

@article{a74cfafc1c0a461ea590fe1315ba4e64,

title = "A novel, efficient, randomized selection trial comparing combinations of drug therapy for ALS",

abstract = "Combining agents with different mechanisms of action may be necessary for meaningful results in treating ALS. The combinations of minocycline-creatine and celecoxib-creatine have additive effects in the murine model. New trial designs are needed to efficiently screen the growing number of potential neuroprotective agents. Our objective was to assess two drug combinations in ALS using a novel phase II trial design. We conducted a randomized, double-blind selection trial in sequential pools of 60 patients. Participants received minocycline (100 mg)-creatine (10 g) twice daily or celecoxib (400 mg)-creatine (10 g) twice daily for six months. The primary objective was treatment selection based on which combination best slowed deterioration in the ALS Functional Rating Scale-Revised (ALSFRS-R); the trial could be stopped after one pool if the difference between the two arms was adequately large. At trial conclusion, each arm was compared to a historical control group in a futility analysis. Safety measures were also examined. After the first patient pool, the mean six-month decline in ALSFRS-R was 5.27 (SD=5.54) in the celecoxib-creatine group and 6.47 (SD=9.14) in the minocycline-creatine group. The corresponding decline was 5.82 (SD=6.77) in the historical controls. The difference between the two sample means exceeded the stopping criterion. The null hypothesis of superiority was not rejected in the futility analysis. Skin rash occurred more frequently in the celecoxib-creatine group. In conclusion, the celecoxib-creatine combination was selected as preferable to the minocycline-creatine combination for further evaluation. This phase II design was efficient, leading to treatment selection after just 60 patients, and can be used in other phase II trials to assess different agents.",

keywords = "ALS, Amyotrophic lateral sclerosis, Celecoxib, Clinical trial, Combination therapy, Creatine, Minocycline, Neuroprotection, Selection trial",

author = "Gordon, {Paul H.} and Cheung, {Ying Kuen} and Bruce Levin and Howard Andrews and Carolyn Doorish and MacArthur, {Robert B.} and Jacqueline Montes and Kate Bednarz and Julaine Florence and Julie Rowin and Kevin Boylan and Tahseen Mozaffar and Rup Tandan and Hiroshi Mitsumoto and Kelvin, {Elizabeth A.} and John Chapin and Richard Bedlack and Michael Rivner and McCluskey, {Leo F.} and Alan Pestronk and Michael Graves and Sorenson, {Eric J.} and Richard Barohn and Belsh, {Jerry M.} and Lou, {Jau Shin} and Todd Levine and David Saperstein and Miller, {Robert G.} and Scelsa, {Stephen N.}",

note = "Funding Information: The trial was supported by an ALSA TREAT ALS grant, MDA Wings Over Wall Street, Avicena Corporation, Carol and Bill Spina and Ross Bowen Funds, and Ride for Life. Dr. Gordon received $30,000 from Avicena Group, Inc to support the trial. Funding Information: The trial was also supported in part by the following GCRC grants: NIH MO1 RR023940 supporting the University of Kansas Medical Center; NIH UL1RR024992 supporting the Center for Applied Research Sciences at the Washington University School of Medicine; NIH 5M01RR 00827-29 supporting the University of California Irvine; and NIH RR-00109 supporting the University of Vermont.",

year = "2008",

doi = "10.1080/17482960802195632",

language = "English (US)",

volume = "9",

pages = "212--222",

journal = "Amyotrophic Lateral Sclerosis",

issn = "1748-2968",

publisher = "Informa Healthcare",

number = "4",

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TY - JOUR

T1 - A novel, efficient, randomized selection trial comparing combinations of drug therapy for ALS

AU - Gordon, Paul H.

AU - Cheung, Ying Kuen

AU - Levin, Bruce

AU - Andrews, Howard

AU - Doorish, Carolyn

AU - MacArthur, Robert B.

AU - Montes, Jacqueline

AU - Bednarz, Kate

AU - Florence, Julaine

AU - Rowin, Julie

AU - Boylan, Kevin

AU - Mozaffar, Tahseen

AU - Tandan, Rup

AU - Mitsumoto, Hiroshi

AU - Kelvin, Elizabeth A.

AU - Chapin, John

AU - Bedlack, Richard

AU - Rivner, Michael

AU - McCluskey, Leo F.

AU - Pestronk, Alan

AU - Graves, Michael

AU - Sorenson, Eric J.

AU - Barohn, Richard

AU - Belsh, Jerry M.

AU - Lou, Jau Shin

AU - Levine, Todd

AU - Saperstein, David

AU - Miller, Robert G.

AU - Scelsa, Stephen N.

N1 - Funding Information: The trial was supported by an ALSA TREAT ALS grant, MDA Wings Over Wall Street, Avicena Corporation, Carol and Bill Spina and Ross Bowen Funds, and Ride for Life. Dr. Gordon received $30,000 from Avicena Group, Inc to support the trial. Funding Information: The trial was also supported in part by the following GCRC grants: NIH MO1 RR023940 supporting the University of Kansas Medical Center; NIH UL1RR024992 supporting the Center for Applied Research Sciences at the Washington University School of Medicine; NIH 5M01RR 00827-29 supporting the University of California Irvine; and NIH RR-00109 supporting the University of Vermont.

PY - 2008

Y1 - 2008

N2 - Combining agents with different mechanisms of action may be necessary for meaningful results in treating ALS. The combinations of minocycline-creatine and celecoxib-creatine have additive effects in the murine model. New trial designs are needed to efficiently screen the growing number of potential neuroprotective agents. Our objective was to assess two drug combinations in ALS using a novel phase II trial design. We conducted a randomized, double-blind selection trial in sequential pools of 60 patients. Participants received minocycline (100 mg)-creatine (10 g) twice daily or celecoxib (400 mg)-creatine (10 g) twice daily for six months. The primary objective was treatment selection based on which combination best slowed deterioration in the ALS Functional Rating Scale-Revised (ALSFRS-R); the trial could be stopped after one pool if the difference between the two arms was adequately large. At trial conclusion, each arm was compared to a historical control group in a futility analysis. Safety measures were also examined. After the first patient pool, the mean six-month decline in ALSFRS-R was 5.27 (SD=5.54) in the celecoxib-creatine group and 6.47 (SD=9.14) in the minocycline-creatine group. The corresponding decline was 5.82 (SD=6.77) in the historical controls. The difference between the two sample means exceeded the stopping criterion. The null hypothesis of superiority was not rejected in the futility analysis. Skin rash occurred more frequently in the celecoxib-creatine group. In conclusion, the celecoxib-creatine combination was selected as preferable to the minocycline-creatine combination for further evaluation. This phase II design was efficient, leading to treatment selection after just 60 patients, and can be used in other phase II trials to assess different agents.

AB - Combining agents with different mechanisms of action may be necessary for meaningful results in treating ALS. The combinations of minocycline-creatine and celecoxib-creatine have additive effects in the murine model. New trial designs are needed to efficiently screen the growing number of potential neuroprotective agents. Our objective was to assess two drug combinations in ALS using a novel phase II trial design. We conducted a randomized, double-blind selection trial in sequential pools of 60 patients. Participants received minocycline (100 mg)-creatine (10 g) twice daily or celecoxib (400 mg)-creatine (10 g) twice daily for six months. The primary objective was treatment selection based on which combination best slowed deterioration in the ALS Functional Rating Scale-Revised (ALSFRS-R); the trial could be stopped after one pool if the difference between the two arms was adequately large. At trial conclusion, each arm was compared to a historical control group in a futility analysis. Safety measures were also examined. After the first patient pool, the mean six-month decline in ALSFRS-R was 5.27 (SD=5.54) in the celecoxib-creatine group and 6.47 (SD=9.14) in the minocycline-creatine group. The corresponding decline was 5.82 (SD=6.77) in the historical controls. The difference between the two sample means exceeded the stopping criterion. The null hypothesis of superiority was not rejected in the futility analysis. Skin rash occurred more frequently in the celecoxib-creatine group. In conclusion, the celecoxib-creatine combination was selected as preferable to the minocycline-creatine combination for further evaluation. This phase II design was efficient, leading to treatment selection after just 60 patients, and can be used in other phase II trials to assess different agents.

KW - ALS

KW - Amyotrophic lateral sclerosis

KW - Celecoxib

KW - Clinical trial

KW - Combination therapy

KW - Creatine

KW - Minocycline

KW - Neuroprotection

KW - Selection trial

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ER -

A novel, efficient, randomized selection trial comparing combinations of drug therapy for ALS

Abstract

Keywords

ASJC Scopus subject areas

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