A 3-year randomized therapeutic trial of nitisinone in alkaptonuria

Introne, Wendy J.; Perry, Monique B.; Troendle, James; Tsilou, Ekaterini; Kayser, Michael A.; Suwannarat, Pim; O’Brien, Kevin; Bryant, Joy; Sachdev, Vandana; Reynolds, James C.; Moylan, Elizabeth; Bernardini, Isa; Gahl, William A.

doi:10.1016/j.ymgme.2011.04.016

Cited by 171 publications

(245 citation statements)

References 25 publications

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“…It converts homogentisic acid (HGA, 2,5-dihydroxyphenylacetic acid) to 4-maleylacetoacetic acid. Inability to metabolize HGA leads to urinary excretion of at least 90% of the compound, or 3-6 g per day, in patients with AKU (Garrod 1902;Lustberg et al 1969;Introne et al 2011). Despite this pronounced renal elimination, some HGA is oxidized to a melanin-like polymeric pigment via benzoquinone acetic acid.…”

Section: Introductionmentioning

confidence: 99%

“…In HT-1, nitisinone prevents the formation of the highly toxic metabolites maleylacetoacetate, fumarylacetoacetate, and succinylacetone (Lindstedt et al 1992), and in combination with a tyrosine-restricted diet, it serves as a successful therapeutic intervention. In AKU, nitisinone can effectively reduce HGA and prevent ochronosis in mice (Suzuki et al Preston et al 2013) and reduce HGA in patients (Introne et al 2011).…”

Section: Introductionmentioning

confidence: 99%

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Relationship Between Serum Concentrations of Nitisinone and Its Effect on Homogentisic Acid and Tyrosine in Patients with Alkaptonuria

et al. 2015

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Background: Alkaptonuria (AKU) is a serious genetic disease due to a defect in tyrosine metabolism, leading to increased serum levels of homogentisic acid (HGA). Nitisinone decreases HGA in AKU, but the concentration-response relationship has not been previously reported.Objectives: To determine the relationship between serum concentrations of nitisinone and the effect on both HGA and tyrosine; secondly to determine steady-state pharmacokinetics of nitisinone in AKU patients.Method: Thirty-two patients with AKU received either 1, 2, 4, or 8 mg nitisinone daily. Urine and serum HGA and serum tyrosine and nitisinone were measured during 24 h at baseline (before first dose) and after 4 weeks of treatment.Results: Nitisinone pharmacokinetics (area under the curve [AUC] and maximum concentrations [C max ]) were dose proportional. The median oral clearance determined in all patients, irrespective of dose, was 3.18 mL/hÁkg (range 1.6-6.7).Nitisinone decreased urinary excretion of HGA in a concentration-dependent manner, with a maximum effect seen at average nitisinone concentrations of 3 mmol/L. The association between nitisinone and tyrosine concentrations was less pronounced. Serum levels of HGA at Week 4 were below the limit of quantitation in 65% of samples, which prevented determination of the relationship with nitisinone concentrations.Conclusion: Nitisinone exhibits dose-proportional pharmacokinetics in the studied dosage interval. Urinary excretion of HGA decreases in a concentration-dependent manner, while the increase in tyrosine is less clearly related to nitisinone concentrations.

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Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Relationship Between Serum Concentrations of Nitisinone and Its Effect on Homogentisic Acid and Tyrosine in Patients with Alkaptonuria

et al. 2015

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“…This is based on the experience of using nitisinone in the National Institutes of Health, USA (Phornphutkul et al 2002;Suwannarat et al 2005;Introne et al 2011). However, one patient in the clinical trial of nitisinone in AKU developed corneal keratopathy that resolved fully with discontinuation of nitisinone (Introne et al 2011).…”

Section: Introductionmentioning

confidence: 99%

Reversible Keratopathy Due to Hypertyrosinaemia Following Intermittent Low-Dose Nitisinone in Alkaptonuria: A Case Report

et al. 2014

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We describe a patient with ultra-rare disease, alkaptonuria, who developed tyrosine keratopathy following nitisinone therapy of 2 mg on alternate days. His vision became impaired approximately 7 weeks following the commencement of nitisinone and ophthalmological examination at week nine showed characteristic dendritic keratopathy associated with tyrosinaemia. The corneal lesion as well as his visual symptoms normalized completely following discontinuation of nitisinone. This is the first documented report of keratopathy due to acquired tyrosinaemia due to very low-dose nitisinone.

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“…As expected, plasma tyrosine concentrations rose approximately from 70 to 760 AE 181 mM with no ill-effects attributable. At dose administered and as predicted, nitisinone was well tolerated; and although the trial failed its primary therapeutic endpoint, improvement of joint symptoms in some patients with established joint disease was identified (Introne et al 2011). …”

Section: First Clinical Trials In Alkaptonuriamentioning

confidence: 87%

“…Alkaptonuria, a neglected ultraorphan disease and the firstidentified inborn error of metabolism, represents an extreme case for therapeutic advance. While in retrospect, it is not surprising that nitisinone failed to increase hip mobility in alkaptonuric patients with established ochronotic arthropathy, given the definitive effects of nitisinone on the primary biochemical defect in alkaptonuria, it is difficult to ignore the potential for clinical utility (Phornphutkul et al 2002;Suwannarat et al 2005;Introne et al 2011). However, the problem of how best to investigate its putative therapeutic and more likely preventative action on disease-related events that are meaningful for patientsand obtain appropriate funding for long-term studies and regulatory approval -remains (Buckley 2008;Griggs et al 2009).…”

Section: Alkaptonuria and The Complexities Of Orphan Therapeuticsmentioning

confidence: 99%

Alkaptonuria: Leading to the Treasure in Exceptions

Cox

2011

JIMD Reports

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The brilliant geneticist, William Bateson, a formidable English experimentalist, was the first to recognize the nature of the "inborn" in Archibald Garrod's errors of metabolism. Bateson's advice to young scientists: "Treasure your exceptions!" summarizes much of the vigorous empiricism associated with the study of rare disorders.The first inborn error of metabolism to be so recognized was alkaptonuria, and it is only recently that a proper understanding of this condition as a disease, rather than a biochemical curiosity, has emerged. Abnormal excretion of the reactive tyrosine metabolite, homogentisic acid, not only provides a tangible biomarker of alkaptonuria, but also a focus for detailed mechanistic understanding.Currently, there is no proven treatment for alkaptonuria but emergence of orphan drug legislation internationally has promoted the licensing of nitisinone (Orfadin™) for an equally rare disorder of tyrosine metabolism -hereditary tyrosinaemia type 1. Nitisinone, a triketone competitive inhibitor of a proximal step leading to the formation of homogentisic acid, has potent therapeutic effects in hereditary tyrosinemia and rapidly ameliorates the primary biochemical abnormality in patients with alkaptonuria.Here, we discuss the context in which nitisinone should be further explored for the treatment of alkaptonuria. This exceptional disease is a paradigm case, which opens up unusual opportunities for basic and applied research. In modern times, it also shows how the conflation of orphan drug legislation and the emerging power and commitment of patient organizations can synergize effectively to advance basic research and therapeutic development in ultra-orphan diseases.

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A 3-year randomized therapeutic trial of nitisinone in alkaptonuria

Cited by 171 publications

References 25 publications

Relationship Between Serum Concentrations of Nitisinone and Its Effect on Homogentisic Acid and Tyrosine in Patients with Alkaptonuria

Relationship Between Serum Concentrations of Nitisinone and Its Effect on Homogentisic Acid and Tyrosine in Patients with Alkaptonuria

Reversible Keratopathy Due to Hypertyrosinaemia Following Intermittent Low-Dose Nitisinone in Alkaptonuria: A Case Report

Alkaptonuria: Leading to the Treasure in Exceptions

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