Literature DB >> 21612962

Ammonia control in children with urea cycle disorders (UCDs); phase 2 comparison of sodium phenylbutyrate and glycerol phenylbutyrate.

Uta Lichter-Konecki1, G A Diaz, J L Merritt, A Feigenbaum, C Jomphe, J F Marier, M Beliveau, J Mauney, K Dickinson, A Martinez, M Mokhtarani, B Scharschmidt, W Rhead.   

Abstract

UNLABELLED: Twenty four hour ammonia profiles and correlates of drug effect were examined in a phase 2 comparison of sodium phenylbutyrate (NaPBA) and glycerol phenylbutyrate (GPB or HPN-100), an investigational drug being developed for urea cycle disorders (UCDs). STUDY
DESIGN: Protocol HPN-100-005 involved open label fixed-sequence switch-over from the prescribed NaPBA dose to a PBA-equimolar GPB dose with controlled diet. After 7 days on NaPBA or GPB, subjects underwent 24-hour blood sampling for ammonia and drug metabolite levels as well as measurement of 24-hour urinary phenyacetylglutamine (PAGN). Adverse events (AEs), safety labs and triplicate ECGs were monitored.
RESULTS: Eleven subjects (9 OTC, 1 ASS, 1 ASL) enrolled and completed the switch-over from NaPBA (mean dose=12.4 g/d or 322 mg/kg/d; range=198-476 mg/kg/d) to GPB (mean dose=10.8 mL or 0.284 mL/kg/d or 313 mg/kg/d; range=192-449 mg/kg/d). Possibly-related AEs were reported in 2 subjects on NaPBA and 4 subjects on GPB. All were mild, except for one moderate AE of vomiting on GPB related to an intercurrent illness. No clinically significant laboratory or ECG changes were observed. Ammonia was lowest after overnight fast, peaked postprandially in the afternoon to early evening and varied widely over 24h with occasional values >100 μmol/L without symptoms. Ammonia values were ~25% lower on GPB vs. NaPBA (p≥0.1 for ITT and p<0.05 for per protocol population). The upper 95% confidence interval for the difference between ammonia on GPB vs. NaPBA in the ITT population (95% CI 0.575, 1.061; p=0.102) was less than the predefined non-inferiority margin of 1.25 and less than 1.0 in the pre-defined per-protocol population (95% CI 0.516, 0.958; p<0.05). No statistically significant differences were observed in plasma phenylacetic acid and PAGN exposure during dosing with GPB vs. NaPBA, and the percentage of orally administered PBA excreted as PAGN (66% for GPB vs. 69% for NaPBA) was very similar. GPB and NaPBA dose correlated best with urinary-PAGN.
CONCLUSIONS: These findings suggest that GPB is at least equivalent to NaPBA in terms of ammonia control, has potential utility in pediatric UCD patients and that U-PAGN is a clinically useful biomarker for dose selection and monitoring.
Copyright © 2011 Elsevier Inc. All rights reserved.

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Year:  2011        PMID: 21612962      PMCID: PMC4880058          DOI: 10.1016/j.ymgme.2011.04.013

Source DB:  PubMed          Journal:  Mol Genet Metab        ISSN: 1096-7192            Impact factor:   4.797


  11 in total

Review 1.  Urea cycle disorders: diagnosis, pathophysiology, and therapy.

Authors:  S W Brusilow; N E Maestri
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2.  Phase 2 comparison of a novel ammonia scavenging agent with sodium phenylbutyrate in patients with urea cycle disorders: safety, pharmacokinetics and ammonia control.

Authors:  Brendan Lee; William Rhead; George A Diaz; Bruce F Scharschmidt; Asad Mian; Oleg Shchelochkov; J F Marier; Martin Beliveau; Joseph Mauney; Klara Dickinson; Antonia Martinez; Sharron Gargosky; Masoud Mokhtarani; Susan A Berry
Journal:  Mol Genet Metab       Date:  2010-03-23       Impact factor: 4.797

3.  Phenylacetylglutamine may replace urea as a vehicle for waste nitrogen excretion.

Authors:  S W Brusilow
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4.  Pharmacology and safety of glycerol phenylbutyrate in healthy adults and adults with cirrhosis.

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Journal:  Hepatology       Date:  2010-06       Impact factor: 17.425

5.  Cross-sectional multicenter study of patients with urea cycle disorders in the United States.

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Journal:  Mol Genet Metab       Date:  2008-06-17       Impact factor: 4.797

6.  Restoration of nitrogen homeostasis in a man with ornithine transcarbamylase deficiency.

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8.  Diagnosis, symptoms, frequency and mortality of 260 patients with urea cycle disorders from a 21-year, multicentre study of acute hyperammonaemic episodes.

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9.  A phase I and pharmacokinetic study of intravenous phenylacetate in patients with cancer.

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10.  Phase I study of phenylacetate administered twice daily to patients with cancer.

Authors:  A Thibault; D Samid; M R Cooper; W D Figg; A C Tompkins; N Patronas; D J Headlee; D R Kohler; D J Venzon; C E Myers
Journal:  Cancer       Date:  1995-06-15       Impact factor: 6.860

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4.  Ammonia control in children ages 2 months through 5 years with urea cycle disorders: comparison of sodium phenylbutyrate and glycerol phenylbutyrate.

Authors:  Wendy Smith; George A Diaz; Uta Lichter-Konecki; Susan A Berry; Cary O Harding; Shawn E McCandless; Cindy LeMons; Joe Mauney; Klara Dickinson; Dion F Coakley; Tristen Moors; Masoud Mokhtarani; Bruce F Scharschmidt; Brendan Lee
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5.  Ammonia control and neurocognitive outcome among urea cycle disorder patients treated with glycerol phenylbutyrate.

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6.  Elevated phenylacetic acid levels do not correlate with adverse events in patients with urea cycle disorders or hepatic encephalopathy and can be predicted based on the plasma PAA to PAGN ratio.

Authors:  M Mokhtarani; G A Diaz; W Rhead; S A Berry; U Lichter-Konecki; A Feigenbaum; A Schulze; N Longo; J Bartley; W Berquist; R Gallagher; W Smith; S E McCandless; C Harding; D C Rockey; J M Vierling; P Mantry; M Ghabril; R S Brown; K Dickinson; T Moors; C Norris; D Coakley; D A Milikien; S C Nagamani; C Lemons; B Lee; B F Scharschmidt
Journal:  Mol Genet Metab       Date:  2013-10-08       Impact factor: 4.797

7.  Switch from Sodium Phenylbutyrate to Glycerol Phenylbutyrate Improved Metabolic Stability in an Adolescent with Ornithine Transcarbamylase Deficiency.

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8.  Urinary phenylacetylglutamine as dosing biomarker for patients with urea cycle disorders.

Authors:  M Mokhtarani; G A Diaz; W Rhead; U Lichter-Konecki; J Bartley; A Feigenbaum; N Longo; W Berquist; S A Berry; R Gallagher; D Bartholomew; C O Harding; M S Korson; S E McCandless; W Smith; J Vockley; S Bart; D Kronn; R Zori; S Cederbaum; N Dorrani; J L Merritt; Sandesh Sreenath-Nagamani; M Summar; C Lemons; K Dickinson; D F Coakley; T L Moors; B Lee; B F Scharschmidt
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Journal:  Mol Genet Metab       Date:  2015-08-05       Impact factor: 4.797

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