Peringatan Keamanan

In animal reproduction studies, oral administration of lumacaftor to pregnant rats and rabbits during organogenesis demonstrated no teratogenicity or adverse effects on fetal development at doses that produced maternal exposures up to approximately 8 (rats) and 5 (rabbits) times the exposure at the maximum recommended human dose (MRHD). No adverse developmental effects were observed after oral administration of lumacaftor to pregnant rats from organogenesis through lactation at doses that produced maternal exposures approximately 8 and 5 times the exposures at the MRHD, respectively. There are no animal reproduction studies with concomitant administration of lumacaftor and ivacaftor.L43060

There have been no reports of overdose with ORKAMBI. The highest repeated dose was lumacaftor 1000 mg once daily/ivacaftor 450 mg q12h administered to 49 healthy subjects for 7 days in a trial evaluating the effect of ORKAMBI on electrocardiograms (ECGs). Adverse events reported at an increased incidence of ?5% compared to the lumacaftor 600 mg/ivacaftor 250 mg dosing period and placebo included: headache (29%), transaminase increase (18%), and generalized rash (10%). No specific antidote is available for overdose with ORKAMBI. Treatment of overdose consists of general supportive measures including monitoring of vital signs and
observation of the clinical status of the patient.L43060

A two-year study in Sprague-Dawley rats and a 26-week study in transgenic Tg.rasH2 mice were conducted to assess the carcinogenic potential of lumacaftor. No evidence of tumorigenicity was observed in rats at lumacaftor oral doses up to 1000 mg/kg/day (approximately 5 and 13 times the MRHD on a lumacaftor AUC basis in males and females, respectively). No evidence of tumorigenicity was observed in Tg.rasH2 mice at lumacaftor oral doses up to 1500 and 2000 mg/kg/day in female and male mice, respectively. Lumacaftor was negative for genotoxicity in the following assays: Ames test for bacterial gene mutation, in vitro chromosomal aberration assay in Chinese hamster ovary cells, and in vivo mouse micronucleus test.L43060

Lumacaftor had no effects on fertility and reproductive performance indices in male and female rats at an oral dose of 1000 mg/kg/day (approximately 3 and 8 times, respectively, the MRHD on a lumacaftor AUC basis).L43060

Lumacaftor

DB09280

small molecule approved

Deskripsi

Lumacaftor is a drug used in combination with DB08820 as the fixed dose combination product Orkambi for the management of Cystic Fibrosis (CF) in patients aged 6 years and older. Cystic Fibrosis is an autosomal recessive disorder caused by one of several different mutations in the gene for the Cystic Fibrosis Transmembrane Conductance Regulator (CFTR) protein, a transmembrane ion channel involved in the transport of chloride and sodium ions across cell membranes of the lungs, pancreas, and other organs. Mutations in the CFTR gene result in altered production, misfolding, or function of the CFTR protein and consequently abnormal fluid and ion transport across cell membranes.A20298, A20299 As a result, CF patients produce thick, sticky mucus that clogs the ducts of organs where it is produced making patients more susceptible to infections, lung damage, pancreatic insufficiency, and malnutrition.A20302 Lumacaftor improves CF symptoms and underlying disease pathology by aiding the conformational stability of F508del-mutated CFTR proteins, preventing misfolding and resulting in increased processing and trafficking of mature protein to the cell surface.

Results from clinical trials indicated that treatment with Orkambi (lumacaftor/ivacaftor) results in improved lung function, reduced chance of experiencing a pulmonary exacerbation, increased weight gain, and improvements in CF symptoms.FDA Label This data has been heavily scrutinized, however, with clinical trials showing only modest improvements despite a hefty yearly cost of $259,000 for Orkambi.A20343 Improvements in lung function (ppFEV1) were found to be statistically significant, but minimal, with only a 2.6-3.0% change from baseline with more than 70% of patients failing to achieve an absolute improvement of at least 5%.A20343, L936

A wide variety of CFTR mutations correlate to the Cystic Fibrosis phenotype and are associated with differing levels of disease severity. The most common mutation, affecting approximately 70% of patients with CF worldwide, is known as F508del-CFTR, or delta-F508 (?F508), in which a deletion in the amino acid phenylalanine at position 508 results in impaired production of the CFTR protein, thereby causing a significant reduction in the amount of ion transporter present on cell membranes.A20301 When used in combination with DB08820 as the fixed dose combination product Orkambi, lumacaftor is specific for the management of CF in patients with delta-F508 mutations as it acts as a protein-folding chaperone, aiding the conformational stability of the mutated CFTR protein. Consequently, lumacaftor increases successful production of CFTR ion channels and the total number of receptors available for use at the cell membrane for fluid and ion transport.A18395 The next most common mutation, G551D, affecting 4-5% of CF patients worldwide, is characterized as a missense mutation, whereby there is sufficient amount of protein at the cell surface, but opening and closing mechanisms of the channel are altered.A17564 Treatment of patients with G551D and other rarer missense mutations is usually managed with DB08820 (Kalydeco), as it aids with altered gating mechanisms by potentiating channel opening probability of CFTR protein.

Prior to the development of lumacaftor and DB08820 (Kalydeco), management of CF primarily involved therapies for the control of infections, nutritional support, clearance of mucus, and management of symptoms rather than improvements in the underlying disease process. Approved for use by the Food and Drug Administration in July 2015 and by Health Canada in January 2016, Orkambi was the first combination product approved for the management of Cystic Fibrosis with delta-F508 mutations.

Ivacaftor is manufactured and distributed by Vertex Pharmaceuticals.

Struktur Molekul 2D

Berat 452.414
Wujud solid

Peta Jejaring Molekuler
Legenda: ObatTargetGenEnzim(Panah → menunjukkan arah efek / relasi)TransporterCarrier

Profil Farmakokinetik

Waktu Paruh (Half-Life) The half-life of lumacaftor is approximately 26 hours in patients with cystic fibrosis.[L43060]
Volume Distribusi Following oral administration of 200 mg of lumacaftor every 24 hours to cystic fibrosis patients in a fed state for 28 days, the mean (+/-SD) for apparent volumes of distribution was 86.0 (69.8) L.[L43060]
Klirens (Clearance) The typical apparent clearance, CL/F (CV), of lumacaftor was estimated to be 2.38 L/hr.[L43060]

Absorpsi

When a single dose of lumacaftor/ivacaftor was administered with fat-containing foods, lumacaftor exposure was approximately 2 times higher than when taken in a fasting state.L43060 Following multiple oral dose administrations of lumacaftor in combination with ivacaftor, the exposure of lumacaftor generally increased proportionally to doses over the range of 200 mg every 24 hours to 400 mg every 12 hours. The median (range) tmax of lumacaftor is approximately 4.0 hours (2.0; 9.0) in the fed state.L43060

Metabolisme

Lumacaftor is mostly excreted unchanged in the feces and is not extensively metabolized. When metabolism does occur, oxidation and glucuronidation are the main processes involved.L43060

Rute Eliminasi

Following oral administration of lumacaftor, the majority of lumacaftor (51%) is excreted unchanged in the feces. There was minimal elimination of lumacaftor and its metabolites in urine (only 8.6% of total radioactivity was recovered in the urine with 0.18% as the unchanged parent drug).L43060

Interaksi Makanan

1 Data
  • 1. Take with a high fat meal. A fat-containing meal or snack should be consumed just before or just after dosing for all formulations.

Interaksi Obat

949 Data
Afatinib The serum concentration of Afatinib can be increased when it is combined with Lumacaftor.
Bosutinib The serum concentration of Bosutinib can be increased when it is combined with Lumacaftor.
Brentuximab vedotin The serum concentration of Brentuximab vedotin can be decreased when it is combined with Lumacaftor.
Colchicine The serum concentration of Colchicine can be increased when it is combined with Lumacaftor.
Edoxaban The serum concentration of Edoxaban can be increased when it is combined with Lumacaftor.
Naloxegol The serum concentration of Naloxegol can be increased when it is combined with Lumacaftor.
Pazopanib The serum concentration of Pazopanib can be increased when it is combined with Lumacaftor.
Prucalopride The serum concentration of Prucalopride can be increased when it is combined with Lumacaftor.
Silodosin The excretion of Silodosin can be decreased when combined with Lumacaftor.
Topotecan The serum concentration of Topotecan can be increased when it is combined with Lumacaftor.
Aripiprazole The metabolism of Aripiprazole can be increased when combined with Lumacaftor.
Rifaximin The serum concentration of Rifaximin can be increased when it is combined with Lumacaftor.
Dabigatran etexilate The serum concentration of Dabigatran etexilate can be decreased when it is combined with Lumacaftor.
Sofosbuvir The serum concentration of Sofosbuvir can be decreased when it is combined with Lumacaftor.
Ifosfamide The metabolism of Ifosfamide can be increased when combined with Lumacaftor.
Ledipasvir The serum concentration of Ledipasvir can be decreased when it is combined with Lumacaftor.
Perampanel The metabolism of Perampanel can be increased when combined with Lumacaftor.
R,S-Warfarin alcohol The metabolism of R,S-Warfarin alcohol can be increased when combined with Lumacaftor.
S,R-Warfarin alcohol The metabolism of S,R-Warfarin alcohol can be increased when combined with Lumacaftor.
Warfarin The serum concentration of Warfarin can be decreased when it is combined with Lumacaftor.
Pantoprazole The serum concentration of Pantoprazole can be decreased when it is combined with Lumacaftor.
Citalopram The serum concentration of Citalopram can be decreased when it is combined with Lumacaftor.
Phenytoin The serum concentration of Phenytoin can be decreased when it is combined with Lumacaftor.
Pentobarbital The serum concentration of Pentobarbital can be decreased when it is combined with Lumacaftor.
Amitriptyline The serum concentration of Amitriptyline can be decreased when it is combined with Lumacaftor.
Methadone The serum concentration of Methadone can be decreased when it is combined with Lumacaftor.
Omeprazole The serum concentration of Omeprazole can be decreased when it is combined with Lumacaftor.
Trimethadione The serum concentration of Trimethadione can be decreased when it is combined with Lumacaftor.
Clobazam The serum concentration of Clobazam can be decreased when it is combined with Lumacaftor.
Timolol The serum concentration of Timolol can be decreased when it is combined with Lumacaftor.
Carisoprodol The serum concentration of Carisoprodol can be decreased when it is combined with Lumacaftor.
Progesterone The serum concentration of Progesterone can be decreased when it is combined with Lumacaftor.
Zolpidem The serum concentration of Zolpidem can be decreased when it is combined with Lumacaftor.
Lansoprazole The serum concentration of Lansoprazole can be decreased when it is combined with Lumacaftor.
Imipramine The serum concentration of Imipramine can be decreased when it is combined with Lumacaftor.
Quinine The serum concentration of Quinine can be decreased when it is combined with Lumacaftor.
Fluoxetine The serum concentration of Fluoxetine can be decreased when it is combined with Lumacaftor.
Albendazole The serum concentration of Albendazole can be decreased when it is combined with Lumacaftor.
Cyclophosphamide The serum concentration of Cyclophosphamide can be decreased when it is combined with Lumacaftor.
Voriconazole The serum concentration of Voriconazole can be decreased when it is combined with Lumacaftor.
Doxazosin The serum concentration of Doxazosin can be decreased when it is combined with Lumacaftor.
Thiopental The serum concentration of Thiopental can be decreased when it is combined with Lumacaftor.
Tamoxifen The serum concentration of Tamoxifen can be decreased when it is combined with Lumacaftor.
Thioridazine The serum concentration of Thioridazine can be decreased when it is combined with Lumacaftor.
Esomeprazole The serum concentration of Esomeprazole can be decreased when it is combined with Lumacaftor.
Clopidogrel The serum concentration of Clopidogrel can be decreased when it is combined with Lumacaftor.
Primidone The serum concentration of Primidone can be decreased when it is combined with Lumacaftor.
Diazepam The serum concentration of Diazepam can be decreased when it is combined with Lumacaftor.
Methylphenobarbital The serum concentration of Methylphenobarbital can be decreased when it is combined with Lumacaftor.
Zonisamide The serum concentration of Zonisamide can be decreased when it is combined with Lumacaftor.
Ramelteon The serum concentration of Ramelteon can be decreased when it is combined with Lumacaftor.
Rabeprazole The serum concentration of Rabeprazole can be decreased when it is combined with Lumacaftor.
Proguanil The serum concentration of Proguanil can be decreased when it is combined with Lumacaftor.
Doxepin The serum concentration of Doxepin can be decreased when it is combined with Lumacaftor.
Phenobarbital The serum concentration of Phenobarbital can be decreased when it is combined with Lumacaftor.
Escitalopram The serum concentration of Escitalopram can be decreased when it is combined with Lumacaftor.
Clomipramine The serum concentration of Clomipramine can be decreased when it is combined with Lumacaftor.
Fosphenytoin The serum concentration of Fosphenytoin can be decreased when it is combined with Lumacaftor.
St. John's Wort The serum concentration of St. John's Wort can be decreased when it is combined with Lumacaftor.
Hexobarbital The serum concentration of Hexobarbital can be decreased when it is combined with Lumacaftor.
Acenocoumarol The serum concentration of Acenocoumarol can be decreased when it is combined with Lumacaftor.
Barbital The serum concentration of Barbital can be decreased when it is combined with Lumacaftor.
Methsuximide The serum concentration of Methsuximide can be decreased when it is combined with Lumacaftor.
Dexlansoprazole The metabolism of Dexlansoprazole can be increased when combined with Lumacaftor.
Lacosamide The serum concentration of Lacosamide can be decreased when it is combined with Lumacaftor.
Etravirine The serum concentration of Etravirine can be decreased when it is combined with Lumacaftor.
Apixaban The serum concentration of Apixaban can be decreased when it is combined with Lumacaftor.
Axitinib The serum concentration of Axitinib can be decreased when it is combined with Lumacaftor.
Artemether The serum concentration of Artemether can be decreased when it is combined with Lumacaftor.
Seratrodast The serum concentration of Seratrodast can be decreased when it is combined with Lumacaftor.
(R)-warfarin The serum concentration of (R)-warfarin can be decreased when it is combined with Lumacaftor.
Etizolam The serum concentration of Etizolam can be decreased when it is combined with Lumacaftor.
Esketamine The serum concentration of Esketamine can be decreased when it is combined with Lumacaftor.
Triclabendazole The serum concentration of Triclabendazole can be decreased when it is combined with Lumacaftor.
Lynestrenol The serum concentration of Lynestrenol can be decreased when it is combined with Lumacaftor.
Dexrabeprazole The serum concentration of Dexrabeprazole can be decreased when it is combined with Lumacaftor.
(S)-Warfarin The serum concentration of (S)-Warfarin can be decreased when it is combined with Lumacaftor.
Propranolol The serum concentration of Propranolol can be decreased when it is combined with Lumacaftor.
Verapamil The serum concentration of Verapamil can be decreased when it is combined with Lumacaftor.
Estradiol The serum concentration of Estradiol can be decreased when it is combined with Lumacaftor.
Paroxetine The serum concentration of Paroxetine can be decreased when it is combined with Lumacaftor.
Fedratinib The serum concentration of Fedratinib can be decreased when it is combined with Lumacaftor.
Formoterol The serum concentration of Formoterol can be decreased when it is combined with Lumacaftor.
Gliclazide The serum concentration of Gliclazide can be decreased when it is combined with Lumacaftor.
Enasidenib The serum concentration of Enasidenib can be decreased when it is combined with Lumacaftor.
Testosterone The serum concentration of Testosterone can be decreased when it is combined with Lumacaftor.
Glyburide The serum concentration of Glyburide can be decreased when it is combined with Lumacaftor.
Sertraline The serum concentration of Sertraline can be decreased when it is combined with Lumacaftor.
Voxelotor The serum concentration of Voxelotor can be decreased when it is combined with Lumacaftor.
Cenobamate The serum concentration of Cenobamate can be decreased when it is combined with Lumacaftor.
Labetalol The serum concentration of Labetalol can be decreased when it is combined with Lumacaftor.
Nebivolol The serum concentration of Nebivolol can be decreased when it is combined with Lumacaftor.
Methylene blue The serum concentration of Methylene blue can be decreased when it is combined with Lumacaftor.
Teniposide The serum concentration of Teniposide can be decreased when it is combined with Lumacaftor.
Valproic acid The serum concentration of Valproic acid can be decreased when it is combined with Lumacaftor.
Nilutamide The serum concentration of Nilutamide can be decreased when it is combined with Lumacaftor.
Pentamidine The serum concentration of Pentamidine can be decreased when it is combined with Lumacaftor.
Moclobemide The serum concentration of Moclobemide can be decreased when it is combined with Lumacaftor.
Ticlopidine The serum concentration of Ticlopidine can be decreased when it is combined with Lumacaftor.
Benzocaine The serum concentration of Benzocaine can be decreased when it is combined with Lumacaftor.

Target Protein

Cystic fibrosis transmembrane conductance regulator CFTR

Referensi & Sumber

Artikel (PubMed)
  • PMID: 24973281
    Boyle MP, Bell SC, Konstan MW, McColley SA, Rowe SM, Rietschel E, Huang X, Waltz D, Patel NR, Rodman D: A CFTR corrector (lumacaftor) and a CFTR potentiator (ivacaftor) for treatment of patients with cystic fibrosis who have a phe508del CFTR mutation: a phase 2 randomised controlled trial. Lancet Respir Med. 2014 Jul;2(7):527-38. doi: 10.1016/S2213-2600(14)70132-8. Epub 2014 Jun 24.
  • PMID: 26416827
    Kuk K, Taylor-Cousar JL: Lumacaftor and ivacaftor in the management of patients with cystic fibrosis: current evidence and future prospects. Ther Adv Respir Dis. 2015 Dec;9(6):313-26. doi: 10.1177/1753465815601934. Epub 2015 Sep 28.
  • PMID: 27714410
    Saint-Criq V, Gray MA: Role of CFTR in epithelial physiology. Cell Mol Life Sci. 2017 Jan;74(1):93-115. doi: 10.1007/s00018-016-2391-y. Epub 2016 Oct 6.
  • PMID: 14719996
    Kunzelmann K, Mall M: Pharmacotherapy of the ion transport defect in cystic fibrosis: role of purinergic receptor agonists and other potential therapeutics. Am J Respir Med. 2003;2(4):299-309.
  • PMID: 28031875
    Fraser-Pitt D, O'Neil D: Cystic fibrosis - a multiorgan protein misfolding disease. Future Sci OA. 2015 Sep 1;1(2):FSO57. doi: 10.4155/fso.15.57. eCollection 2015 Sep.
  • PMID: 17291132
    MacDonald KD, McKenzie KR, Zeitlin PL: Cystic fibrosis transmembrane regulator protein mutations: 'class' opportunity for novel drug innovation. Paediatr Drugs. 2007;9(1):1-10.
  • PMID: 22293084
    Yu H, Burton B, Huang CJ, Worley J, Cao D, Johnson JP Jr, Urrutia A, Joubran J, Seepersaud S, Sussky K, Hoffman BJ, Van Goor F: Ivacaftor potentiation of multiple CFTR channels with gating mutations. J Cyst Fibros. 2012 May;11(3):237-45. doi: 10.1016/j.jcf.2011.12.005. Epub 2012 Jan 30.
  • PMID: 26718821
    Mayer M: Lumacaftor-ivacaftor (Orkambi) for cystic fibrosis: behind the 'breakthrough'. Evid Based Med. 2016 Jun;21(3):83-6. doi: 10.1136/ebmed-2015-110325. Epub 2015 Dec 30.

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