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Pimasertib, a selective oral MEK1/2 inhibitor: absolute bioavailability, mass balance, elimination route, and metabolite profile in cancer patients.
von Richter, Oliver; Massimini, Giorgio; Scheible, Holger; Udvaros, Istvan; Johne, Andreas.
Afiliação
  • von Richter O; Merck KGaA, Clinical Pharmacology, 64293, Darmstadt, Germany.
  • Massimini G; Merck KGaA, Early Clinical Oncology, 64293, Darmstadt, Germany.
  • Scheible H; Merck KGaA, DMPK, 85567, Grafing, Germany.
  • Udvaros I; PRA International, EDS Patient Pharmacology, 1076, Budapest, Hungary.
  • Johne A; Merck KGaA, Clinical Pharmacology, 64293, Darmstadt, Germany.
Br J Clin Pharmacol ; 82(6): 1498-1508, 2016 12.
Article em En | MEDLINE | ID: mdl-27483391
AIM: This trial (NCT: 01713036) investigated the absolute bioavailability, mass balance and metabolite profile of pimasertib in a new design combining these investigations in a single group of patients. METHODS: Six male patients with pathologically confirmed, locally advanced or metastatic solid tumours were enrolled. Exclusion criteria included Eastern Cooperative Oncology Group performance status >1. In Part A of the trial, patients received a 60 mg oral dose of unlabelled pimasertib followed by an intravenous (i.v.) tracer dose of [14 C]pimasertib 2 µg (equalling 9 kBq) as a bolus injection, one hour after the oral dose, on Day 1. On Day 8, all patients received 60 mg pimasertib capsules spiked with 2.6 MBq of [14 C]pimasertib. Patients received 60 mg oral unlabelled pimasertib twice daily from Day 3 to Day 21 of Part A and in subsequent 21-day cycles in Part B. RESULTS: Following i.v. administration, [14 C]pimasertib exhibited a geometric mean total body clearance of 45.7 l h-1 (geometric coefficient of variation [geometric CV]: 47.2%) and a volume of distribution of 229 l (geometric CV: 42.0%). Absolute bioavailability was 73%. The majority of the oral [14 C] dose (85.1%) was recovered in excreta. Total radioactivity was mainly excreted into urine (52.8%) and faeces (30.7%) with 78.9% of the [14 C] dose recovered as metabolites. Two major circulating metabolites were identified in plasma: a carboxylic acid (M445) and a phosphoethanolamine conjugate (M554). The safety profile was in line with the published pimasertib trials. CONCLUSION: Pimasertib showed a favourable pharmacokinetic profile with high absolute bioavailability and a unique metabolic pathway (conjugation with phosphoethanolamine).
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Texto completo: 1 Base de dados: MEDLINE Assunto principal: Niacinamida / MAP Quinase Quinase 1 / MAP Quinase Quinase 2 / Neoplasias / Antineoplásicos Idioma: En Ano de publicação: 2016 Tipo de documento: Article

Texto completo: 1 Base de dados: MEDLINE Assunto principal: Niacinamida / MAP Quinase Quinase 1 / MAP Quinase Quinase 2 / Neoplasias / Antineoplásicos Idioma: En Ano de publicação: 2016 Tipo de documento: Article