Literature DB >> 25310201

Safety and pharmacokinetics of lisdexamfetamine dimesylate in adults with clinically stable schizophrenia: a randomized, double-blind, placebo-controlled trial of ascending multiple doses.

Patrick Martin1, Bryan Dirks, Lev Gertsik, David Walling, Annette Stevenson, Mary Corcoran, Aparna Raychaudhuri, James Ermer.   

Abstract

To assess the safety and pharmacokinetics of lisdexamfetamine dimesylate (LDX), a d-amphetamine prodrug, this double-blind study enrolled adults with clinically stable schizophrenia who were adherent (≥12 weeks) to antipsychotic pharmacotherapy. The participants received placebo or ascending LDX doses (50, 70, 100, 150, 200, and 250 mg) daily for 5 days at each dose (dose periods, 1-6; days, 1-5). Of the 31 enrolled participants, 27 completed the study (placebo, n = 6; LDX, n = 21). Treatment-emergent adverse events (AEs) were reported by 4 participants receiving placebo and by 23 participants receiving LDX (all doses) with no serious AEs while on active treatment. For all periods, the mean postdose change on day 5 (up to 12 hours postdose) in systolic and diastolic blood pressure and pulse, respectively, ranged from -4.62 to 8.05 mm Hg, -3.67 to 4.43 mm Hg, and -3.57 to 14.43 beats per minute for placebo and -3.83 to 11.25 mm Hg, -1.55 to 5.80 mm Hg, and -0.36 to 21.26 beats per minute for LDX. With ascending LDX dose, the mean (SD) maximum plasma concentration for LDX-derived d-amphetamine ranged from 51.68 (10.28) to 266.27 (56.55) ng/mL. The area under the plasma concentration-time curve for 24 hours ranged from 801.8 (170.2) to 4397.9 (1085.9) ng[BULLET OPERATOR]h/mL. The d-amphetamine maximum plasma concentration and area under the plasma concentration-time curve increased linearly with ascending LDX dose. Antipsychotic agents did not markedly affect d-amphetamine pharmacokinetics. Over a wide range of ascending doses, LDX safety profile in adults with schizophrenia was consistent with previous findings with no unexpected treatment-emergent AEs. Pulse tended to increase with LDX dose; overall, blood pressure did not increase with LDX dose. Consistent with previous studies, pharmacokinetic parameters increased linearly with increasing LDX dose.

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Year:  2014        PMID: 25310201     DOI: 10.1097/JCP.0000000000000205

Source DB:  PubMed          Journal:  J Clin Psychopharmacol        ISSN: 0271-0749            Impact factor:   3.153


  4 in total

1.  Single Dose Comparative Bioavailability Study of Lisdexamfetamine Dimesylate as Oral Solution Versus Reference Hard Capsules in Healthy Volunteers.

Authors:  Simona Rizea-Savu; Simona Nicoleta Duna; Dimitrios Panagiotopoulos; Roxana Colette Sandulovici
Journal:  Front Pharmacol       Date:  2022-04-05       Impact factor: 5.988

2.  Safety and tolerability of oral lisdexamfetamine in adults with methamphetamine dependence: a phase-2 dose-escalation study.

Authors:  Nadine Ezard; Brendan Clifford; Adrian Dunlop; Raimondo Bruno; Andrew Carr; Zhixin Liu; Krista J Siefried; Nicholas Lintzeris
Journal:  BMJ Open       Date:  2021-05-18       Impact factor: 2.692

3.  Trial protocol of an open label pilot study of lisdexamfetamine for the treatment of acute methamphetamine withdrawal.

Authors:  Liam S Acheson; Nadine Ezard; Nicholas Lintzeris; Adrian Dunlop; Jonathan Brett; Craig Rodgers; Anthony Gill; Michael Christmass; Rebecca McKetin; Michael Farrell; Steve Shoptaw; Krista J Siefried
Journal:  PLoS One       Date:  2022-10-03       Impact factor: 3.752

4.  LiMA: a study protocol for a randomised, double-blind, placebo controlled trial of lisdexamfetamine for the treatment of methamphetamine dependence.

Authors:  Nadine Ezard; Adrian Dunlop; Michelle Hall; Robert Ali; Rebecca McKetin; Raimondo Bruno; Nghi Phung; Andrew Carr; Jason White; Brendan Clifford; Zhixin Liu; Marian Shanahan; Kate Dolan; Amanda L Baker; Nicholas Lintzeris
Journal:  BMJ Open       Date:  2018-07-19       Impact factor: 2.692
  4 in total

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