Effect of tarenflurbil on cognitive decline and activities of daily living in patients with mild Alzheimer disease: a randomized controlled trial

Robert C Green, Lon S Schneider, David A Amato, Andrew P Beelen, Gordon Wilcock, Edward A Swabb, Kenton H Zavitz, Tarenflurbil Phase 3 Study Group, Scott Aaronson, Lawrence Adler, Paul Aisen, Gustavo Alva, Piero Antuono, Jeffrey Apter, Fares Arguello, Stephen Aronson, Kelly Askins, William Au, Dennis Aumentado, Andrius Baskys, Zinoviy Benzar, Bruce Berwald, John Beyer, Victor Biton, Bradley Boeve, Brian Bortnick, Michael Bowman, Adam Boxer, Melinda Campopiano, Fen-Lei Chang, David Chen, David Coffey, Gregory Cooper, Kerry Cranmer, Mario Cuervo, Jose De la Gandara, Steven DeKosky, G Michael Dempsey, Rachelle Doody, William Ellison, John Ervin, Nasrollah Eslami, Robert Feldman, Gerald Ferencz, Stephen Flitman, Miguel Flores, Stuart Fox, Franklin Galef, Suzanne Gazda, David Geldmacher, Jeffrey Geohas, Gary Gerard, Jerome Goldstein, Neill Graff-Radford, Robert Green, George Grossberg, Sanjay Gupta, James Hampsey, David Hart, John Heath, Lawrence Honig, Richard Hubbard, Naveed Iqbal, Valentin Isacescu, Cletus Iwuagwu, Travis Jackson, Mark Johnston, Marvin Kalafer, Curtis Kauffmann, Justine Kent, Louis Kirby 2nd, Richard Kishner, Smita Kittur, Jack Klapper, Michael Levy, Jonathon Licht, Scott Losk, Veena Luthra, Abe Marcadis, David Margolin, Samuel Markind, Paul Mazzeo, James McCarthy, John Meyer, David Michie, Jacobo Mintzer, George Morgan, Ruth Mulnard, John Nardandrea, Marshal Nash, Barry Packman, Jorg Pahl, Meenakshi Patel, William Petrie, Eric Pfeiffer, Anton Porsteinsson, Neil Pugach, Joseph Quinn, Joachim Raese, Ashok Raj, Surinder Randhawa, Stephen Rappaport, Barry Reisberg, Victor Richenstein, Kenneth Rictor, Barry Rovner, Donald Royall, Marwan Sabbagh, Carl Sadowsky, Beth Safirstein, Stephen Salloway, Frederick Schaerf, Douglas Scharre, Stephen Scheinthal, Lon Schneider, Harvey Schwartz, Ben Seltzer, Ram Shrivastava, Richard Singer, Bart Sloan, Paul Solomon, Sidney Spector, Stuart Stark, Mary Stedman, Susan Steen, John Stoukides, Herman Sullivan, Alan Swann, Leslie Taylor, Stephen Thein, Jack Tomlinson, Kathleen Toups, Ashley Tunkle, Christopher Van Dyck, Navin Varma, Daniel Weintraub, Jeanette Wendt, Kerri Wilks, Mark Willner, Jaron Winston, Kyle Womack, Robert C Green, Lon S Schneider, David A Amato, Andrew P Beelen, Gordon Wilcock, Edward A Swabb, Kenton H Zavitz, Tarenflurbil Phase 3 Study Group, Scott Aaronson, Lawrence Adler, Paul Aisen, Gustavo Alva, Piero Antuono, Jeffrey Apter, Fares Arguello, Stephen Aronson, Kelly Askins, William Au, Dennis Aumentado, Andrius Baskys, Zinoviy Benzar, Bruce Berwald, John Beyer, Victor Biton, Bradley Boeve, Brian Bortnick, Michael Bowman, Adam Boxer, Melinda Campopiano, Fen-Lei Chang, David Chen, David Coffey, Gregory Cooper, Kerry Cranmer, Mario Cuervo, Jose De la Gandara, Steven DeKosky, G Michael Dempsey, Rachelle Doody, William Ellison, John Ervin, Nasrollah Eslami, Robert Feldman, Gerald Ferencz, Stephen Flitman, Miguel Flores, Stuart Fox, Franklin Galef, Suzanne Gazda, David Geldmacher, Jeffrey Geohas, Gary Gerard, Jerome Goldstein, Neill Graff-Radford, Robert Green, George Grossberg, Sanjay Gupta, James Hampsey, David Hart, John Heath, Lawrence Honig, Richard Hubbard, Naveed Iqbal, Valentin Isacescu, Cletus Iwuagwu, Travis Jackson, Mark Johnston, Marvin Kalafer, Curtis Kauffmann, Justine Kent, Louis Kirby 2nd, Richard Kishner, Smita Kittur, Jack Klapper, Michael Levy, Jonathon Licht, Scott Losk, Veena Luthra, Abe Marcadis, David Margolin, Samuel Markind, Paul Mazzeo, James McCarthy, John Meyer, David Michie, Jacobo Mintzer, George Morgan, Ruth Mulnard, John Nardandrea, Marshal Nash, Barry Packman, Jorg Pahl, Meenakshi Patel, William Petrie, Eric Pfeiffer, Anton Porsteinsson, Neil Pugach, Joseph Quinn, Joachim Raese, Ashok Raj, Surinder Randhawa, Stephen Rappaport, Barry Reisberg, Victor Richenstein, Kenneth Rictor, Barry Rovner, Donald Royall, Marwan Sabbagh, Carl Sadowsky, Beth Safirstein, Stephen Salloway, Frederick Schaerf, Douglas Scharre, Stephen Scheinthal, Lon Schneider, Harvey Schwartz, Ben Seltzer, Ram Shrivastava, Richard Singer, Bart Sloan, Paul Solomon, Sidney Spector, Stuart Stark, Mary Stedman, Susan Steen, John Stoukides, Herman Sullivan, Alan Swann, Leslie Taylor, Stephen Thein, Jack Tomlinson, Kathleen Toups, Ashley Tunkle, Christopher Van Dyck, Navin Varma, Daniel Weintraub, Jeanette Wendt, Kerri Wilks, Mark Willner, Jaron Winston, Kyle Womack

Abstract

Context: Amyloid-beta peptide (Abeta(42)) has been implicated in the pathogenesis of Alzheimer disease (AD). Tarenflurbil, a selective Abeta(42)-lowering agent, demonstrated encouraging results on cognitive and functional outcomes among mildly affected patients in an earlier phase 2 trial.

Objective: To determine the efficacy, safety, and tolerability of tarenflurbil.

Design, setting, and patients: A multicenter, randomized, double-blind, placebo-controlled trial enrolling patients with mild AD was conducted at 133 trial sites in the United States between February 21, 2005, and April 30, 2008. Concomitant treatment with cholinesterase inhibitors or memantine was permitted.

Intervention: Tarenflurbil, 800 mg, or placebo, administered twice a day.

Main outcome measures: Co-primary efficacy end points were the change from baseline to month 18 in total score on the subscale of the Alzheimer Disease Assessment Scale-Cognitive Subscale (ADAS-Cog, 80-point version) and Alzheimer Disease Cooperative Studies-activities of daily living (ADCS-ADL) scale. Additional prespecified slope analyses explored the possibility of disease modification.

Results: Of the 1684 participants randomized, 1649 were included in the analysis, and 1046 completed the trial. Tarenflurbil had no beneficial effect on the co-primary outcomes (difference in change from baseline to month 18 vs placebo, based on least squares means: 0.1 for ADAS-Cog; 95% CI, -0.9 to 1.1; P = .86 and -0.5 for ADCS-ADL; 95% CI, -1.9 to 0.9; P = .48) using an intent-to-treat analysis. No significant differences occurred in the secondary outcomes. The ADAS-Cog score decreased by 7.1 points over 18 months. The tarenflurbil group had a small increase in frequency of dizziness, anemia, and infections.

Conclusion: Tarenflurbil did not slow cognitive decline or the loss of activities of daily living in patients with mild AD.

Trial registration: clinicaltrials.gov Identifier: NCT00105547.

Figures

Figure 1
Figure 1
Participant Flow Chart aPatients originally assigned to receive twice daily 400 mg of tarenflurbil were incorporated into the twice daily 800-mg group. bExcluded from the main efficacy analyses using the intent-to-treat population but were included in the safety analyses. Rates of adverse events leading to study discontinuation are based on the intent-to-treat population. The numbers differ from those in the text, which are based on the safety population.
Figure 2
Figure 2
Alzheimer Disease Assessment Cognitive Subscale and Alzheimer Disease Cooperative Studies–Activities of Daily Living Scale Scores by Visit Values represent means using imputed last observation carried forward. Error bars represent 95% CIs.

Source: PubMed

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