Your search keyword '"Andrew T. Hughes"' showing total 38 results

1. Method development and validation for analysis of phenylalanine, 4‐hydroxyphenyllactic acid and 4‐hydroxyphenylpyruvic acid in serum and urine

Author

Andrew T. Hughes, Anna M. Milan, Ella Shweihdi, James Gallagher, and Lakshminarayan Ranganath

Subjects

alkaptonuria, mass spectrometry, metabolites, nitisinone, tyrosine, Diseases of the endocrine glands. Clinical endocrinology, RC648-665, Genetics, QH426-470

Abstract

Abstract Alkaptonuria (AKU) is a rare debilitating autosomal recessive disorder of tyrosine (TYR) metabolism which results in a deficiency of the enzyme homogentisate 1,2‐dioxygenase activity. Several studies have reported the metabolic changes in homogentisic acid (HGA) concentrations and subsequent deposition of an ochronotic pigment in connective tissues, especially cartilage. Treatment with nitisinone (NTBC) reduces urinary and circulating HGA, but its mode of action results in hypertyrosinaemia. The effect of NTBC on other metabolites in the TYR pathway has not been reported. Modification of the current reverse phase liquid chromatography tandem mass spectrometry methods for serum and urine to include phenylalanine (PHE), hydroxyphenyllactate (HPLA) and hydroxyphenylpyruvate (HPPA) has been validated. HPPA and HPLA (negative ionisation) eluted at 2.8 and 2.9 min respectively on an Atlantis C18 column with PHE (positive ionisation) eluting earlier at 2.4 min. Intra‐ and inter‐assay accuracy was between 96.3% and 100.3% for PHE; 96.6% and 110.5% for HPLA and 95.0% and 107.8% for HPPA in both urine and serum. Precision, both inter‐ and intra‐assay, was

Published

2022

2. Metabolomic studies in the inborn error of metabolism alkaptonuria reveal new biotransformations in tyrosine metabolism

Author

Brendan P. Norman, Andrew S. Davison, Juliette H. Hughes, Hazel Sutherland, Peter JM. Wilson, Neil G. Berry, Andrew T. Hughes, Anna M. Milan, Jonathan C. Jarvis, Norman B. Roberts, Lakshminarayan R. Ranganath, George Bou-Gharios, and James A. Gallagher

Subjects

Alkaptonuria, Biotransformation, Metabolism, Metabolomics, Mice, Medicine (General), R5-920, Genetics, QH426-470

Abstract

Alkaptonuria (AKU) is an inherited disorder of tyrosine metabolism caused by lack of active enzyme homogentisate 1,2-dioxygenase (HGD). The primary consequence of HGD deficiency is increased circulating homogentisic acid (HGA), the main agent in the pathology of AKU disease. Here we report the first metabolomic analysis of AKU homozygous Hgd knockout (Hgd−/−) mice to model the wider metabolic effects of Hgd deletion and the implication for AKU in humans. Untargeted metabolic profiling was performed on urine from Hgd−/− AKU (n = 15) and Hgd+/− non-AKU control (n = 14) mice by liquid chromatography high-resolution time-of-flight mass spectrometry (Experiment 1). The metabolites showing alteration in Hgd−/− were further investigated in AKU mice (n = 18) and patients from the UK National AKU Centre (n = 25) at baseline and after treatment with the HGA-lowering agent nitisinone (Experiment 2). A metabolic flux experiment was carried out after administration of 13C-labelled HGA to Hgd−/−(n = 4) and Hgd+/−(n = 4) mice (Experiment 3) to confirm direct association with HGA. Hgd−/− mice showed the expected increase in HGA, together with unexpected alterations in tyrosine, purine and TCA-cycle pathways. Metabolites with the greatest abundance increases in Hgd−/− were HGA and previously unreported sulfate and glucuronide HGA conjugates, these were decreased in mice and patients on nitisinone and shown to be products from HGA by the 13C-labelled HGA tracer. Our findings reveal that increased HGA in AKU undergoes further metabolism by mainly phase II biotransformations. The data advance our understanding of overall tyrosine metabolism, demonstrating how specific metabolic conditions can elucidate hitherto undiscovered pathways in biochemistry and metabolism.

Published

2022

3. Comparing nitisinone 2 mg and 10 mg in the treatment of alkaptonuria—An approach using statistical modelling

Author

Lakshminarayan R. Ranganath, Anna M. Milan, Andrew T. Hughes, Milad Khedr, Brendan P. Norman, Mohammed Alsbou, Richard Imrich, Matthew Gornall, Nicolas Sireau, James A. Gallagher, and Richard Jackson

Subjects

AKUSSI, alkaptonuria, disease progression, homogentisic acid, nitisinone, safety, Diseases of the endocrine glands. Clinical endocrinology, RC648-665, Genetics, QH426-470

Abstract

Abstract Background Outcomes from studies employing nitisinone 10 mg and 2 mg in alkaptonuria were compared. Patients and methods Sixty‐nine patients in each of the nitisinone (10 mg daily) and controls of suitability of nitisinone in alkaptonuria 2 (SONIA 2), as well as 37 and 23 in nitisinone (2 mg daily) and control cohorts at the National Alkaptonuria Centre (NAC), respectively, were followed up for 4 years. Severity of alkaptonuria (AKU) was assessed by the AKU Severity Score Index (AKUSSI). 24‐h urine homogentisic acid (uHGA24), serum HGA (sHGA), serum tyrosine (sTYR) and serum nitisinone (sNIT) were also analysed at each time point. Dietetic support was used in the NAC, but not in SONIA 2. Safety outcomes were also compared. All statistical analyses were post hoc. Results The slope of the AKUSSI was 0.55, 0.19, 0.30, and 0.06 per month in the control NAC, nitisinone NAC, control SONIA 2, and nitisinone SONIA 2 cohorts, respectively. The intersection of the slopes on the x‐axis was −132, −411, −295, and − 1460 months, respectively. The control and nitisinone slope comparisons were statistically significant both in the NAC (p

Published

2022

4. Reversal of ochronotic pigmentation in alkaptonuria following nitisinone therapy: Analysis of data from the United Kingdom National Alkaptonuria Centre

Author

Lakshminarayan R. Ranganath, Anna M. Milan, Andrew T. Hughes, Milad Khedr, Andrew S. Davison, Peter J. Wilson, Jane P. Dillon, Elizabeth West, and James A. Gallagher

Subjects

alkaptonuria, nitisinone, homogentisic acid, eye ochronosis, ear ochronosis, ear cartilage biopsy, Diseases of the endocrine glands. Clinical endocrinology, RC648-665, Genetics, QH426-470

Abstract

Abstract Background Increased homogentisic acid (HGA) causes ochronosis. Nitisinone decreases HGA. The aim was to study the effect of nitisinone on the ochronosis progression. Methods Photographs of the eyes and ears were acquired from patients attending the National Alkaptonuria Centre (NAC) at V‐1 (pre‐baseline visit), V0 (baseline visit when 2 mg nitisinone was commenced), and yearly at V1, V2, and V3 visits. Photographs were inspected for evolution of ochronotic pigment and also scored categorically to derive eye, ear, and combined ochronosis scores. An ear cartilage biopsy was also carried out at V0 and one year after V3 (V4) and ochronotic pigment was assessed and quantitated. Visits were compared for changes in pigment. Fasting blood and 24‐hour urine samples were collected for measurement of HGA. Results There were 80 AKU patients at V0, and 52, 47, and 40 at V1, V2, and V3 in the group with variable numbers (VAR Group) respectively; 23 patients attended once before V0, in the V‐1 visit. Photographs of patients show increase in eye pigment between V‐1 and V0, followed by decrease post‐nitisinone at V1, V2, and V3. Ear and combined ochronosis semiquantitative scoring showed an increase between V‐1 and V0 (P

Published

2020

5. The nutritional status of people with alkaptonuria: An exploratory analysis suggests a protein/energy dilemma

Author

Shirley Judd, Milad Khedr, Anna M. Milan, Andrew S. Davison, Andrew T. Hughes, Alexander Needham, Eftychia E. Psarelli, Alan Shenkin, and Lakshiminaryan R. Ranganath

Subjects

alkaptonuria, global nutritional assessment, protein energy deficit, Diseases of the endocrine glands. Clinical endocrinology, RC648-665, Genetics, QH426-470

Abstract

Abstract Background Alkaptonuria (AKU) is a disorder of tyrosine/protein metabolism leading to accumulation of homogentisic acid. Clinical management historically recommended reducing dietary protein intake, especially in childhood, which has since been discredited in the literature. For the first time, analysis of baseline cross‐sectional nutritional surveillance data from a large cohort of AKU patients is presented, which has clinical implications in all aspects of treatment planning. Method Seventy‐four patients (mean 55 years) admitted to the National Alkaptonuria Centre (NAC), underwent a global nutritional assessment, which included objective anthropometry, bioimpedance measures, habitual nutritional intake using a 7‐day food diary and key nutritional biomarkers, including 24 hours urinary nitrogen, serum albumin, total protein and total 25‐hydroxy vitamin D. All data was compared with cohort norms or recommended nutrient intakes for health (RNI). The potential beneficial impact of protein and anti‐inflammatory nutrients such as vitamin C, selenium, and zinc were statistically interrogated against the AKU severity score index (AKUSSI)—a validated measure of disease progression stratified by age. Results Fifty percent of AKU patients reported some level of protein restriction at some point in their lives. In comparison with national data sets, AKU patients present with significantly lower than predicted mid‐upper arm circumference, grip strength, BMI, total energy and protein intake, and higher than predicted percentage body fat. They therefore meet the ESPEN criteria as “clinically undernourished.” Severity fluctuates over the life course. No statistical association is identified between protein intake, expressed as %RNI or g/kg, or anti‐inflammatory nutrients, including vitamin C as a high dose supplement on the severity of the disease, when correlated against the validated AKUSSI score. Conclusion AKU patients are at risk of protein depletion associated with a “perfect storm” of risk factors: historical, poorly evidenced recommendations to reduce total protein intake; limited mobility as the condition progresses, compromising muscle integrity; frequent hospital admissions for major surgery associated with multiple joint replacements, creating pinch points of high metabolic demand and the potential impact of the disease itself. As this is the first time this risk has been identified, the authors consider the dietetic implications of nitisinone treatment, which requires dietary protein control to manage the acquired tyrosinaemia. The lack of statistically significant evidence to support dietary manipulation of any kind to impede disease progression in AKU is demonstrated.

Published

2020

6. Evaluation of the serum metabolome of patients with alkaptonuria before and after two years of treatment with nitisinone using LC‐QTOF‐MS

Author

Andrew S. Davison, Brendan P. Norman, Gordon A. Ross, Andrew T. Hughes, Milad Khedr, Anna M. Milan, James A. Gallagher, and Lakshminarayan R. Ranganath

Subjects

alkaptonuria, metabolomics, nitisinone, tyrosine, Diseases of the endocrine glands. Clinical endocrinology, RC648-665, Genetics, QH426-470

Abstract

Abstract Background The homogentisic acid‐lowering therapy nitisinone is being evaluated for the treatment of alkaptonuria (AKU) at the National Centre for AKU. Beyond hypertyrosinemia, the wider metabolic consequences of its use are largely unknown. The aim of this work was to evaluate the impact of nitisinone on the serum metabolome of patients with AKU after 12 and 24 months of treatment. Methods Deproteinized serum from 25 patients with AKU (mean age[±SD] 51.1 ± 14.9 years, 12 male) was analyzed using the 1290 Infinity II liquid chromatography system coupled to a 6550 quadrupole time‐of‐flight mass spectrometry (Agilent, UK). Raw data were processed using a batch targeted feature extraction algorithm and an accurate mass retention time database containing 469 intermediary metabolites (MW 72‐785). Matched entities (±10 ppm theoretical accurate mass and ±0.3 minutes retention time window) were filtered based on their frequency and variability (

Published

2019

7. Revisiting Quantification of Phenylalanine/Tyrosine Flux in the Ochronotic Pathway during Long-Term Nitisinone Treatment of Alkaptonuria

Author

Lakshminarayan R. Ranganath, Andrew T. Hughes, Andrew S. Davison, Milad Khedr, Richard Imrich, Mattias Rudebeck, Birgitta Olsson, Brendan P. Norman, George Bou-Gharios, James A. Gallagher, and Anna M. Milan

Subjects

alkaptonuria, pigment, biliary excretion, ochronosis, nitisinone, homogentisic acid, Microbiology, QR1-502

Abstract

Changes in the phenylalanine (PHE)/tyrosine (TYR) pathway metabolites before and during homogentisic acid (HGA)-lowering by nitisinone in the Suitability of Nitisinone in Alkaptonuria (AKU) 2 (SONIA 2) study enabled the magnitude of the flux in the pathway to be examined. SONIA 2 was a 48-month randomised, open-label, evaluator-blinded, parallel-group study performed in the UK, France and Slovakia recruiting patients with confirmed AKU to receive either 10 mg nitisinone or no treatment. Site visits were performed at 3 months and yearly thereafter. Results from history, photographs of eyes/ears, whole body scintigraphy, echocardiography and abdomen/pelvis ultrasonography were combined to produce the Alkaptonuria Severity Score Index (cAKUSSI). PHE, TYR, hydroxyphenylpyruvate (HPPA), hydroxyphenyllactate (HPLA) and HGA metabolites were analysed by liquid chromatography/tandem mass spectrometry in 24 h urine and serum samples collected before and during nitisinone. Serum metabolites were corrected for total body water (TBW), and the sum of 24 h urine plus total body water metabolites of PHE, TYR, HPPA, HPLA and HGA were determined. The sum of urine metabolites (PHE, TYR, HPPA, HPLA and HGA) were similar pre- and peri-nitisinone. The sum of TBW metabolites and sum TBW + URINE metabolites were significantly higher peri-nitisinone (p < 0.001 for both) compared with pre-nitisinone baseline. Significantly higher concentrations of metabolites from the tyrosine metabolic pathway were observed during treatment with nitisinone. Arguments for unmasking of the ochronotic pathway and biliary elimination of HGA are put forward.

Published

2022

8. Comprehensive Biotransformation Analysis of Phenylalanine-Tyrosine Metabolism Reveals Alternative Routes of Metabolite Clearance in Nitisinone-Treated Alkaptonuria

Author

Brendan P. Norman, Andrew S. Davison, Bryony Hickton, Gordon A. Ross, Anna M. Milan, Andrew T. Hughes, Peter J. M. Wilson, Hazel Sutherland, Juliette H. Hughes, Norman B. Roberts, George Bou-Gharios, James A. Gallagher, and Lakshminarayan R. Ranganath

Subjects

alkaptonuria, hypertyrosinaemia, biotransformations, detoxification, metabolomics, Microbiology, QR1-502

Abstract

Metabolomic analyses in alkaptonuria (AKU) have recently revealed alternative pathways in phenylalanine-tyrosine (phe-tyr) metabolism from biotransformation of homogentisic acid (HGA), the active molecule in this disease. The aim of this research was to study the phe-tyr metabolic pathway and whether the metabolites upstream of HGA, increased in nitisinone-treated patients, also undergo phase 1 and 2 biotransformation reactions. Metabolomic analyses were performed on serum and urine from patients partaking in the SONIA 2 phase 3 international randomised-controlled trial of nitisinone in AKU (EudraCT no. 2013-001633-41). Serum and urine samples were taken from the same patients at baseline (pre-nitisinone) then at 24 and 48 months on nitisinone treatment (patients N = 47 serum; 53 urine) or no treatment (patients N = 45 serum; 50 urine). Targeted feature extraction was performed to specifically mine data for the entire complement of theoretically predicted phase 1 and 2 biotransformation products derived from phenylalanine, tyrosine, 4-hydroxyphenylpyruvic acid and 4-hydroxyphenyllactic acid, in addition to phenylalanine-derived metabolites with known increases in phenylketonuria. In total, we observed 13 phase 1 and 2 biotransformation products from phenylalanine through to HGA. Each of these products were observed in urine and two were detected in serum. The derivatives of the metabolites upstream of HGA were markedly increased in urine of nitisinone-treated patients (fold change 1.2–16.2) and increases in 12 of these compounds were directly proportional to the degree of nitisinone-induced hypertyrosinaemia (correlation coefficient with serum tyrosine = 0.2–0.7). Increases in the urinary phenylalanine metabolites were also observed across consecutive visits in the treated group. Nitisinone treatment results in marked increases in a wider network of phe-tyr metabolites than shown before. This network comprises alternative biotransformation products from the major metabolites of this pathway, produced by reactions including hydration (phase 1) and bioconjugation (phase 2) of acetyl, methyl, acetylcysteine, glucuronide, glycine and sulfate groups. We propose that these alternative routes of phe-tyr metabolism, predominantly in urine, minimise tyrosinaemia as well as phenylalanaemia.

Published

2022

9. Comparing the Phenylalanine/Tyrosine Pathway and Related Factors between Keratopathy and No-Keratopathy Groups as Well as between Genders in Alkaptonuria during Nitisinone Treatment

Author

Lakshminarayan R. Ranganath, Anna M. Milan, Andrew T. Hughes, Andrew S. Davison, Milad Khedr, Richard Imrich, Mattias Rudebeck, Birgitta Olsson, Brendan P. Norman, George Bou-Gharios, and James A. Gallagher

Subjects

sex, keratopathy, alkaptonuria, homogentisic acid, hydroxyphenylpyruvate, hydroxyphenyllactate, Microbiology, QR1-502

Abstract

Nitisinone (NIT) causes tyrosinaemia and corneal keratopathy (KP), especially in men. However, the adaptation within the phenylalanine (PHE)/tyrosine (TYR) catabolic pathway during KP is not understood. The objective of this study is to assess potential differences in the PHE/TYR pathway during KP and the influence of gender in NIT-induced tyrosinaemia in alkaptonuria (AKU). Samples of serum and 24 h urine collected from patients treated with NIT during a 4-year randomized study in NIT vs. no-treatment controls (SONIA 2; Suitability Of Nitisinone In Alkaptonuria 2; EudraCT no. 2013-001633-41) at months 3 (V2), 12 (V3), 24 (V4), 36 (V5) and 48 (V6) were included in these analyses. Homogentisic acid (HGA), TYR, PHE, hydroxyphenylpyruvate (HPPA), hydroxyphenyllactate (HPLA) and sNIT were analysed at all time-points in serum and urine in the NIT-group. All statistical analyses were post hoc. Keratopathy occurred in 10 out of 69 AKU patients, eight of them male. Thirty-five sampling points (serum and 24 h urine) were analysed in patients experiencing KP and 272 in those with no-KP (NKP) during NIT therapy. The KP group had a lower HPLA/TYR ratio and a higher TYR/PHE ratio compared with the NKP group (p < 0.05 for both). There were 24, 45, 100 and 207 sampling points (serum and 24 h urine) in the NIT group which were pre-NIT female, pre-NIT male, NIT female and NIT male, respectively. The PHE/TYR ratio and the HPLA/TYR ratio were lower in males (p < 0.001 and p < 0.01, respectively). In the KP group and in the male group during NIT therapy, adaptive responses to minimise TYR formation were impaired compared to NKP group and females, respectively.

Published

2022

10. Temporal Adaptations in the Phenylalanine/Tyrosine Pathway and Related Factors During Nitisinone-Induced Tyrosinaemia in Alkaptonuria

Author

Lakshminarayan Ranganath, Andrew T. Hughes, Andrew S. Davison, Milad Khedr, Birgitta Olsson, Mattias Rudebeck, Richard Imrich, Brendan P. Norman, George Bou-Gharios, James A. Gallagher, and Anna M. Milan

Published

2022

11. Nitisinone causes acquired tyrosinosis in alkaptonuria

Author

Eftychia-Eirini Psarelli, Andrew T. Hughes, Andrew S. Davison, Milad Khedr, Anna M. Milan, Hazel Sutherland, Parisa Ghane, James A. Gallagher, Maggie S. Cooper, Brendan P. Norman, Lakshminarayan R. Ranganath, Jonathan C. Jarvis, Richard Fitzgerald, Nicolaas E. P. Deutz, and Louise Markinson

Subjects

Adult, Male, RM, medicine.medical_specialty, Nitisinone, Phenylalanine, Tyrosinosis, Context (language use), Alkaptonuria, Mice, Young Adult, chemistry.chemical_compound, Internal medicine, Genetics, medicine, Animals, Humans, Homogentisic acid, Tyrosine, Amino Acid Metabolism, Inborn Errors, Genetics (clinical), Aged, Mice, Inbred BALB C, Cyclohexanones, business.industry, Middle Aged, medicine.disease, Endocrinology, chemistry, Nitrobenzoates, Female, Hypertyrosinaemia, business, medicine.drug

Abstract

For over two decades, nitisinone (NTBC) has been successfully used to manipulate the tyrosine degradation pathway and save the lives of many children with hereditary tyrosinaemia type 1. More recently, NTBC has been used to halt homogentisic acid accumulation in alkaptonuria (AKU) with evidence suggesting its efficacy as a disease modifying agent. NTBC-induced hypertyrosinaemia has been associated with cognitive impairment and potentially sight-threatening keratopathy. In the context of a non-lethal condition (ie, AKU), these serious risks call for an evaluation of the wider impact of NTBC on the tyrosine pathway. We hypothesised that NTBC increases the tyrosine pool size and concentrations in tissues. In AKU mice tyrosine concentrations of tissue homogenates were measured before and after treatment with NTBC. In humans, pulse injection with l-[13 C9 ]tyrosine and l-[d8 ]phenylalanine was used along with compartmental modelling to estimate the size of tyrosine pools before and after treatment with NTBC. We found that NTBC increased tyrosine concentrations in murine tissues by five to nine folds. It also significantly increased the tyrosine pool size in humans (P

Published

2020

12. Dietary restriction of tyrosine and phenylalanine lowers tyrosinemia associated with nitisinone therapy of alkaptonuria

Author

Juliette H. Hughes, James A. Gallagher, Jonathan C. Jarvis, S Judd, Anna M. Milan, Andrew T. Hughes, Peter Wilson, George Bou-Gharios, Lakshminarayan R. Ranganath, and Hazel Sutherland

Subjects

Male, medicine.medical_specialty, Nitisinone, phenylalanine, Phenylalanine, nitisinone, Alkaptonuria, Tyrosinemia, Mice, QH301, 03 medical and health sciences, chemistry.chemical_compound, RA0421, Internal medicine, Diet, Protein-Restricted, Genetics, Animals, Humans, Medicine, Homogentisic acid, Tyrosine, QH426, Genetics (clinical), 030304 developmental biology, Homogentisate 1,2-dioxygenase, chemistry.chemical_classification, alkaptonuria, 0303 health sciences, Cyclohexanones, Tyrosinemias, business.industry, 030305 genetics & heredity, Original Articles, medicine.disease, tyrosinemia, QP, Amino acid, Endocrinology, chemistry, Nitrobenzoates, Female, Original Article, protein, business, medicine.drug

Abstract

BACKGROUND: Alkaptonuria (AKU) is caused by homogentisate 1,2-dioxygenase deficiency that leads to homogentisic acid (HGA) accumulation, ochronosis and severe osteoarthropathy. Recently, nitisinone treatment, which blocks HGA formation, has been effective in AKU patients. However, a consequence of nitisinone is elevated tyrosine that can cause keratopathy. The effect of tyrosine and phenylalanine dietary restriction was investigated in nitisinone-treated AKU mice, and in an observational study of dietary intervention in AKU patients. METHODS: Nitisinone-treated AKU mice were fed tyrosine/phenylalanine-free and phenylalanine-free diets with phenylalanine supplementation in drinking water. Tyrosine metabolites were measured pre-nitisinone, post-nitisinone, and after dietary restriction. Subsequently an observational study was undertaken in 10 patients attending the National Alkaptonuria Centre (NAC), with tyrosine >700μmol/L who had been advised to restrict dietary protein intake and where necessary, to use tyrosine/phenylalanine-free amino acid supplements. RESULTS: Elevated tyrosine (813μmol/L) was significantly reduced in nitisinone-treated AKU mice fed a tyrosine/phenylalanine-free diet in a dose responsive manner. At 3 days of restriction, tyrosine was 389.3μmol/L, 274.8μmol/L and 144.3μmol/L with decreasing phenylalanine doses. In contrast, tyrosine was not effectively reduced in mice by a phenylalanine-free diet; at 3 days tyrosine was 757.3μmol/L, 530.2μmol/L and 656.2μmol/L, with no dose response to phenylalanine supplementation. In NAC patients, tyrosine was significantly reduced (p=0.002) when restricting dietary protein alone, and when combined with tyrosine/phenylalanine-free amino acid supplementation; 4 out of 10 patients achieved tyrosine

Published

2020

13. A Comprehensive LC-QTOF-MS Metabolic Phenotyping Strategy: Application to Alkaptonuria

Author

Andrew S. Davison, Andrew T. Hughes, James A. Gallagher, Gordon A. Ross, Norman B. Roberts, Brendan P. Norman, Jonathan C. Jarvis, Anna M. Milan, Hazel Sutherland, and Lakshminarayan R. Ranganath

Subjects

Male, 0301 basic medicine, Nitisinone, Metabolite, Clinical Biochemistry, Urine, Computational biology, Alkaptonuria, 01 natural sciences, Mass Spectrometry, Lc qtof ms, Mice, 03 medical and health sciences, chemistry.chemical_compound, Metabolomics, Metabolome, medicine, Animals, Humans, Aged, Homogentisate 1,2-Dioxygenase, Cyclohexanones, business.industry, 010401 analytical chemistry, Biochemistry (medical), Middle Aged, medicine.disease, 0104 chemical sciences, Phenotype, 030104 developmental biology, chemistry, Gene Knockdown Techniques, Nitrobenzoates, Female, business, Retention time, Databases, Chemical, Chromatography, Liquid, medicine.drug

Abstract

BACKGROUND Identification of unknown chemical entities is a major challenge in metabolomics. To address this challenge, we developed a comprehensive targeted profiling strategy, combining 3 complementary liquid chromatography quadrupole time-of-flight mass spectrometry (LC-QTOF-MS) techniques and in-house accurate mass retention time (AMRT) databases established from commercial standards. This strategy was used to evaluate the effect of nitisinone on the urinary metabolome of patients and mice with alkaptonuria (AKU). Because hypertyrosinemia is a known consequence of nitisinone therapy, we investigated the wider metabolic consequences beyond hypertyrosinemia. METHODS A total of 619 standards (molecular weight, 45–1354 Da) covering a range of primary metabolic pathways were analyzed using 3 liquid chromatography methods—2 reversed phase and 1 normal phase—coupled to QTOF-MS. Separate AMRT databases were generated for the 3 methods, comprising chemical name, formula, theoretical accurate mass, and measured retention time. Databases were used to identify chemical entities acquired from nontargeted analysis of AKU urine: match window theoretical accurate mass ±10 ppm and retention time ±0.3 min. RESULTS Application of the AMRT databases to data acquired from analysis of urine from 25 patients with AKU (pretreatment and after 3, 12, and 24 months on nitisinone) and 18 HGD−/− mice (pretreatment and after 1 week on nitisinone) revealed 31 previously unreported statistically significant changes in metabolite patterns and abundance, indicating alterations to tyrosine, tryptophan, and purine metabolism after nitisinone administration. CONCLUSIONS The comprehensive targeted profiling strategy described here has the potential of enabling discovery of novel pathways associated with pathogenesis and management of AKU.

Published

2019

14. Reversal of ochronotic pigmentation in alkaptonuria following nitisinone therapy: Analysis of data from the United Kingdom National Alkaptonuria Centre

Author

Andrew T. Hughes, Andrew S. Davison, J.P. Dillon, Milad Khedr, Peter Wilson, Anna M. Milan, Lakshminarayan R. Ranganath, James A. Gallagher, and Elizabeth West

Subjects

Research Report, medicine.medical_specialty, lcsh:QH426-470, Nitisinone, Endocrinology, Diabetes and Metabolism, Urine, eye ochronosis, ear cartilage biopsy, lcsh:Diseases of the endocrine glands. Clinical endocrinology, Biochemistry, Genetics and Molecular Biology (miscellaneous), Ochronotic pigmentation, nitisinone, Alkaptonuria, chemistry.chemical_compound, Biopsy, Internal Medicine, medicine, Increased homogentisic acid, Homogentisic acid, Ochronosis, alkaptonuria, lcsh:RC648-665, medicine.diagnostic_test, business.industry, Research Reports, homogentisic acid, medicine.disease, Dermatology, lcsh:Genetics, chemistry, natural history, reversal, sense organs, ear ochronosis, business, medicine.drug

Abstract

BackgroundIncreased homogentisic acid (HGA) causes ochronosis. Nitisinone decreases HGA. The aim was to study the effect of nitisinone on the ochronosis progression.MethodsPhotographs of the eyes and ears were acquired from patients attending the National Alkaptonuria Centre (NAC) at V-1 (pre-baseline visit), V0 (baseline visit when 2 mg nitisinone was commenced), and yearly at V1, V2, and V3 visits. Photographs were inspected for evolution of ochronotic pigment and also scored categorically to derive eye, ear, and combined ochronosis scores. An ear cartilage biopsy was also carried out at V0 and one year after V3 (V4) and ochronotic pigment was assessed and quantitated. Visits were compared for changes in pigment. Fasting blood and 24-hour urine samples were collected for measurement of HGA.ResultsThere were 80 AKU patients at V0, and 52, 47, and 40 at V1, V2, and V3 in the group with variable numbers (VAR Group) respectively; 23 patients attended once before V0, in the V-1 visit. Photographs of patients show increase in eye pigment between V-1 and V0, followed by decrease post-nitisinone at V1, V2, and V3. Ear and combined ochronosis semiquantitative scoring showed an increase between V-1 and V0 (P P P ConclusionsNitisinone decreases HGA and partially reverses ochronosis.

Published

2020

15. Evaluation of the Mitra microsampling device for use with key urinary metabolites in patients with Alkaptonuria

Author

Andrew T. Hughes, James Rudge, Lakshminarayan R. Ranganath, Andrew S. Davison, Anna M. Milan, and Joseph M Taylor

Subjects

medicine.medical_specialty, Time Factors, Urinary system, Clinical Biochemistry, Clinical Chemistry Tests, Urine, Alkaptonuria, 01 natural sciences, Analytical Chemistry, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Internal medicine, Lc ms ms, medicine, Humans, In patient, Homogentisic acid, General Pharmacology, Toxicology and Pharmaceutics, Tyrosine Metabolism, chemistry.chemical_classification, Molecular Structure, business.industry, 010401 analytical chemistry, General Medicine, medicine.disease, 0104 chemical sciences, Amino acid, Medical Laboratory Technology, Endocrinology, chemistry, 030220 oncology & carcinogenesis, business

Abstract

Aim: Alkaptonuria is a disorder of tyrosine metabolism where elevated circulating homogentisic acid causes progressive dysfunction of collagenous tissues. Logistical, financial and patient experience concerns with collection and transport of specimens to central laboratories makes evaluation of microsampling attractive. Methodology: Volumetric absorptive microsampling devices were evaluated for accuracy, precision and drying time. Elution methods were evaluated for several urinary metabolites of interest and stability assessed under multiple conditions. Comparison was performed between dried and liquid specimens via LC–MS/MS. Conclusion: Volumetric absorptive microsampling was found to be highly accurate and precise. Elution methods showed good recovery and reproducibility. Dried and liquid samples compared favorably. Analyte stability was variable, presenting barriers to implementation into routine use in this context.

Published

2018

16. Data on items of AKUSSI in Alkaptonuria collected over three years from the United Kingdom National Alkaptonuria Centre and the impact of nitisinone

Author

Andrew S. Davison, Sobhan Vinjamuri, S Judd, Anna M. Milan, Elizabeth West, Andrew T. Hughes, G. Hughes, J.P. Dillon, R Griffin, JM Devine, Nicolas Sireau, Jonathan C. Jarvis, N Loftus, A Jones, M McCormick, Lakshminarayan R. Ranganath, Anna Daroszewska, Sophie Taylor, Milad Khedr, James A. Gallagher, JL Usher, Michael Fisher, Joanne A. Harrold, M. C. Briggs, Trevor Cox, Eftychia E. Psarelli, and Gabor Barton

Subjects

Pediatrics, medicine.medical_specialty, Ochronosis, Multidisciplinary, Nitisinone, business.industry, 030209 endocrinology & metabolism, medicine.disease, lcsh:Computer applications to medicine. Medical informatics, R1, Alkaptonuria, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, chemistry, Metabolic effects, medicine, lcsh:R858-859.7, Homogentisic acid, business, lcsh:Science (General), 030217 neurology & neurosurgery, medicine.drug, lcsh:Q1-390

Abstract

Alkaptonuria is a rare genetic disorder characterized by a high level of circulating (and urine) homogentisic acid (HGA), which contributes to ochronosis when it is deposited in connective tissue as a pigmented polymer. In an observational study carried out by National AKU Centre (NAC) in Liverpool, a total of thirty-nine AKU patients attended yearly visits in varying numbers. At each visit a mixture of clinical, joint and spinal assessments were carried out and the results calculated to yield an AKUSSI (Alkaptonuria Severity Score Index), see "Nitisinone arrests ochronosis and decreases rate of progression of Alkaptonuria: evaluation of the effect of nitisinone in the United Kingdom National Alkaptonuria Centre" (Ranganath at el., 2018). The aim of this data article is to produce visual representation of the change in the components of AKUSSI over 3 years, through radar charts. The metabolic effect of nitisinone is shown through box plots.

Published

2018

17. Clinical and biochemical assessment of depressive symptoms in patients with Alkaptonuria before and after two years of treatment with nitisinone

Author

Halford J.C.G., J. Usher, James A. Gallagher, G. Hughes, Milad Khedr, Joanne A. Harrold, JM Devine, Brendan P. Norman, Anna M. Milan, Andrew S. Davison, Lakshminarayan R. Ranganath, and Andrew T. Hughes

Subjects

Adult, Male, 0301 basic medicine, medicine.medical_specialty, Adolescent, Nitisinone, Dopamine, Endocrinology, Diabetes and Metabolism, Urinary system, Alkaptonuria, Biochemistry, Gastroenterology, Young Adult, 03 medical and health sciences, Endocrinology, Internal medicine, Genetics, medicine, Humans, In patient, Tyrosine, Molecular Biology, Depression (differential diagnoses), Aged, Cyclohexanones, Depression, business.industry, Hydroxyindoleacetic Acid, Middle Aged, medicine.disease, 030104 developmental biology, Monoamine neurotransmitter, Mood, Nitrobenzoates, Female, business, medicine.drug

Abstract

Objective Concerns exist over hypertyrosinaemia that is observed following treatment with nitisinone. It has been suggested that tyrosine may compete with tryptophan for uptake into the central nervous system, and or inhibit tryptophan hydroxylase activity reducing serotonin production. At the National Alkaptonuria (AKU) Centre nitisinone is being used off-licence to treat AKU, and there is uncertainty over whether hypertyrosinaemia may alter mood. Herein results from clinical and biochemical assessments of depression in patients with AKU before and after treatment with nitisinone are presented. Patients and methods 63 patients were included pre-nitisinone treatment, of these 39 and 32 patients were followed up 12 and 24 months after treatment. All patients had Becks Depression Inventory-II (BDI-II) assessments (scores can range from 0 to 63, the higher the score the more severe the category of depression), and where possible urinary monoamine neurotransmitter metabolites and serum aromatic amino acids were measured as biochemical markers of depression. Results Mean (±standard deviation) BDI-II scores pre-nitisinone, and after 12 and 24 months were 10.1(9.6); 9.8(10.0) and 10.5(9.9) (p ≥ 0.05, all visits). Paired scores (n = 32), showed a significant increase at 24 months compared to baseline 10.5(9.9) vs. 8.6 (7.8) (p = 0.03). Serum tyrosine increased at least 6-fold following nitisinone (p ≤ 0.0001, all visits), and urinary 3-methoxytyramine (3-MT) increased at 12 and 24 months (p ≤ 0.0001), and 5-hydroxyindole acetic acid (5-HIAA) decreased at 12 months (p = 0.03). Conclusions BDI-II scores were significantly higher following 24 months of nitisinone therapy in patients that were followed up, however the majority of these patients remained in the minimal category of depression. Serum tyrosine and urinary 3-MT increased significantly following treatment with nitisinone. In contrast urinary 5-HIAA did not decrease consistently over the same period studied. Together these findings suggest nitisinone does not cause depression despite some observed effects on monoamine neurotransmitter metabolism.

Published

2018

18. Efficacy and safety of once-daily nitisinone for patients with alkaptonuria (SONIA 2): an international, multicentre, open-label, randomised controlled trial

Author

James A. Gallagher, Michael E. Briggs, Elizabeth Záňová, Birgitta Olsson, Ciarán Scott, Mattias Rudebeck, Sophie Taylor, Nadia Loftus, Nicolas Sireau, Brendan P. Norman, Roman Stančík, Jozef Rovenský, Alpesh Mistry, Andrew S. Davison, Elizabeth West, Richard Imrich, Nick Rhodes, Michael Fisher, Kim Hanh Le Quan Sang, Christa van Kan, Juliette H. Hughes, Emily Luangrath, J.P. Dillon, Jonathan C. Jarvis, Ol'ga Lukáčová, Eftychia E. Psarelli, Dinny Laan, Anthony K Hall, Trevor Cox, Andrea Zatkova, Anna M. Milan, Eva Vrtíková, Richard Fitzgerald, Jean Baptiste Arnoux, Helena Glasova, Jana Sedláková, Johan Szamosi, Lakshminarayan R. Ranganath, Daniela Braconi, Federica Genovese, Chris Webb, Milad Khedr, Anders Bröijersén, Vanda Mlynáriková, Helen Bygott, Annalisa Santucci, Sobhan Vinjamuri, Ella Shweihdi, and Andrew T. Hughes

Subjects

Adult, Male, medicine.medical_specialty, Internationality, Nitisinone, Endocrinology, Diabetes and Metabolism, Urinary system, Urine, Alkaptonuria, Drug Administration Schedule, law.invention, Excretion, Endocrinology, Randomized controlled trial, law, Internal medicine, Internal Medicine, Clinical endpoint, medicine, Humans, Single-Blind Method, Longitudinal Studies, Enzyme Inhibitors, Homogentisic Acid, Aged, Ochronosis, business.industry, Cyclohexanones, Female, Middle Aged, Nitrobenzoates, Treatment Outcome, medicine.disease, business, medicine.drug

Abstract

Background Alkaptonuria is a rare, genetic, multisystem disease characterised by the accumulation of homogentisic acid (HGA). No HGA-lowering therapy has been approved to date. The aim of SONIA 2 was to investigate the efficacy and safety of once-daily nitisinone for reducing HGA excretion in patients with alkaptonuria and to evaluate whether nitisinone has a clinical benefit. Methods SONIA 2 was a 4-year, open-label, evaluator-blind, randomised, no treatment controlled, parallel-group study done at three sites in the UK, France, and Slovakia. Patients aged 25 years or older with confirmed alkaptonuria and any clinical disease manifestations were randomly assigned (1:1) to receive either oral nitisinone 10 mg daily or no treatment. Patients could not be masked to treatment due to colour changes in the urine, but the study was evaluator-blinded as far as possible. The primary endpoint was daily urinary HGA excretion (u-HGA24) after 12 months. Clinical evaluation Alkaptonuria Severity Score Index (cAKUSSI) score was assessed at 12, 24, 36, and 48 months. Efficacy variables were analysed in all randomly assigned patients with a valid u-HGA24 measurement at baseline. Safety variables were analysed in all randomly assigned patients. The study was registered at ClinicalTrials.gov (NCT01916382). Findings Between May 7, 2014, and Feb 16, 2015, 139 patients were screened, of whom 138 were included in the study, with 69 patients randomly assigned to each group. 55 patients in the nitisinone group and 53 in the control group completed the study. u-HGA24 at 12 months was significantly decreased by 99·7% in the nitisinone group compared with the control group (adjusted geometric mean ratio of nitisinone/control 0·003 [95% CI 0·003 to 0·004], p

Published

2020

19. Conditional targeting in mice reveals that hepatic homogentisate 1,2-dioxygenase activity is essential in reducing circulating homogentisic acid and for effective therapy in the genetic disease alkaptonuria

Author

Peter Wilson, Andrew T. Hughes, Brendan P. Norman, Antonius Plagge, Hazel Sutherland, James A. Gallagher, Lakshminarayan R. Ranganath, George Bou-Gharios, Ke Liu, Juliette H. Hughes, Anna M. Milan, Takao Sakai, and Craig M. Keenan

Subjects

0301 basic medicine, Male, Genetic enhancement, Transgene, education, Mice, Transgenic, Biology, Alkaptonuria, 03 medical and health sciences, chemistry.chemical_compound, Exon, Gene Knockout Techniques, Mice, 0302 clinical medicine, Genetics, medicine, Animals, Homogentisic acid, Promoter Regions, Genetic, Molecular Biology, Homogentisic Acid, Genetics (clinical), Homogentisate 1,2-dioxygenase, Ochronosis, Kidney, Homogentisate 1,2-Dioxygenase, General Medicine, medicine.disease, Molecular biology, digestive system diseases, Disease Models, Animal, 030104 developmental biology, medicine.anatomical_structure, surgical procedures, operative, chemistry, Liver, 030220 oncology & carcinogenesis, General Article

Abstract

Alkaptonuria is an inherited disease caused by homogentisate 1,2-dioxygenase (HGD) deficiency. Circulating homogentisic acid (HGA) is elevated and deposits in connective tissues as ochronotic pigment. In this study, we aimed to define developmental and adult HGD tissue expression and determine the location and amount of gene activity required to lower circulating HGA and rescue the alkaptonuria phenotype.We generated an alkaptonuria mouse model using a knockout-first design for the disruption of the HGD gene. Hgd tm1a −/− mice showed elevated HGA and ochronosis in adulthood. LacZ staining driven by the endogenous HGD promoter was localised to only liver parenchymal cells and kidney proximal tubules in adulthood, commencing at E12.5 and E15.5 respectively. Following removal of the gene trap cassette to obtain a normal mouse with a floxed 6th HGD exon, a double transgenic was then created with Mx1-Cre which conditionally deleted HGD in liver in a dose dependent manner. 20% of HGD mRNA remaining in liver did not rescue the disease, suggesting that we need more than 20% of liver HGD to correct the disease in gene therapy.Kidney HGD activity which remained intact reduced urinary HGA, most likely by increased absorption, but did not reduce plasma HGA nor did it prevent ochronosis. In addition, downstream metabolites of exogenous 13C6-HGA, were detected in heterozygous plasma, revealing that hepatocytes take up and metabolise HGA.This novel alkaptonuria mouse model demonstrated the importance of targeting liver for therapeutic intervention, supported by our observation that hepatocytes take up and metabolise HGA.

Published

2019

20. Subclinical ochronosis features in alkaptonuria: A cross-sectional study

Author

Nicolas Sireau, H. Shepherd, Milad Khedr, Mark A. Robinson, Lakshminarayan R. Ranganath, Leah Frances Taylor, Andrew T. Hughes, Daniela Braconi, Federica Genovese, Trevor Cox, Anna M. Milan, Annalisa Santucci, Daniela Giustarini, Nick Rhodes, James A. Gallagher, Alpesh Mistry, J.P. Dillon, Elizabeth West, Sophie Taylor, Ranieri Rossi, Gabor Barton, and Eftychia E. Psarelli

Subjects

0301 basic medicine, medicine.medical_specialty, Nitisinone, Cross-sectional study, ear cartilage biopsy, Alkaptonuria, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Biopsy, medicine, Homogentisic acid, Subclinical infection, 030203 arthritis & rheumatology, Ochronosis, alkaptonuria, medicine.diagnostic_test, ochronosis, business.industry, General Medicine, medicine.disease, AKUSSI, Dermatology, Rash, R1, natural history, 030104 developmental biology, chemistry, medicine.symptom, business, medicine.drug

Abstract

BackgroundAlkaptonuria (AKU) is present from birth, yet clinical effects are considered to appear later in life. Morbidity of AKU, considered irreversible, is secondary to ochronosis. Age of ochronosis onset is not clearly known. Nitisinone profoundly lowers homogentisic acid (HGA), the metabolic defect in AKU. Nitisinone also arrests ochronosis and slows progression of AKU. However, tyrosinaemia post-nitisinone has been associated with corneal keratopathy, rash and cognitive impairment in HT 1. The optimal time to start nitisinone in AKU is unknown.MethodsIn an open, cross-sectional, single-site study, 32 patients with AKU were to be recruited. The primary outcome was presence of ochronosis in an ear biopsy. Secondary outcomes included analysis of photographs of eyes/ears, serum/urine HGA, markers of tissue damage/inflammation/oxidation, MRI imaging, gait, quality of life and Alkaptonuria Severity Score Index (qAKUSSI).ResultsThirty patients, with mean age (SD) 38 (14) years, were recruited. Percentage pigmentation within ear biopsies increased with age. Ear pigmentation was detected in a 20-year-old woman implying ochronosis can start in patients before the age of 20. Gait and qAKUSSI were outside the normal range in all the patients with AKU.ConclusionsOchronosis can be present before age 20 years.

Published

2019

21. Alkaptonuria - Many questions answered, further challenges beckon

Author

Andrew T. Hughes, Lakshminarayan R. Ranganath, Anna M. Milan, Nicolas Sireau, James A. Gallagher, and Andrew S. Davison

Subjects

0301 basic medicine, Nitisinone, Clinical Biochemistry, 030105 genetics & heredity, Bioinformatics, Alkaptonuria, 03 medical and health sciences, chemistry.chemical_compound, Mice, medicine, Animals, Humans, Homogentisic acid, Tyrosine, Enzyme Inhibitors, Homogentisic Acid, business.industry, Cyclohexanones, General Medicine, medicine.disease, Metabolic pathway, Disease Models, Animal, 030104 developmental biology, chemistry, Inborn error of metabolism, Nitrobenzoates, business, medicine.drug

Abstract

Alkaptonuria is an iconic rare inherited inborn error of metabolism affecting the tyrosine metabolic pathway, resulting in the accumulation of homogentisic acid in the circulation, and significant excretion in urine. Dating as far back as 1500 BC in the Egyptian mummy Harwa, homogentisic acid was shown to be central to the pathophysiology of alkaptonuria through its deposition in collagenous tissues in a process termed ochronosis. Clinical manifestations occurring as a consequence of this are typically observed from the third decade of life, are lifelong and significantly affect the quality of life. In large supportive and palliative treatment measures are available to patients, including analgesia, physiotherapy and joint replacement. Studying the natural history of alkaptonuria, in a murine model and human subjects, has provided key insights into the biochemical and molecular mechanisms underlying the pathophysiology associated with the disease, and has enabled a better understanding of the common disease osteoarthritis. In the last decade, a major focus has been on an unlicensed disease-modifying therapy called nitisinone. This has been shown to be highly efficacious in reducing homogentisic acid, and it is hoped this will halt ochronosis, thus limiting the clinical complications associated with the disease. A well-documented metabolic consequence of nitisinone therapy is hypertyrosinaemia, the clinical implications of which are uncertain. Recent metabolomic studies have helped understand the wider metabolic consequences of nitisinone therapy.

Published

2019

22. Homogentisic acid is not only eliminated by glomerular filtration and tubular secretion but also produced in the kidney in alkaptonuria

Author

Andrea Zatkova, Helen Bygott, Richard Fitzgerald, Daniela Braconi, Andrew T. Hughes, Nick Rhodes, Richard Imrich, Federica Genovese, Milad Khedr, Anna M. Milan, Roman Stančík, Helena Glasova, James A. Gallagher, Louise Mankowitz, Lakshminarayan R. Ranganath, Andrew S. Davison, Annalisa Santucci, Ella Shweihdi, Birgitta Olsson, Emily Luangrath, Christa van Kan, Jonathan C. Jarvis, Jean Baptiste Arnoux, Brendan P. Norman, Juliette H. Hughes, Dinny Laan, Mattias Rudebeck, Nicolas Sireau, Eftychia E. Psarelli, and Kim Hanh Le Quan Sang

Subjects

Adult, Male, medicine.medical_specialty, Phenylalanine, Renal function, alkaptonuria, GFR, homogentisic acid, renal clearance, tubular absorption, tubular secretion, Alkaptonuria, Kidney, Excretion, RC1200, 03 medical and health sciences, chemistry.chemical_compound, Sex Factors, Internal medicine, Genetics, medicine, Humans, Homogentisic acid, Homogentisic Acid, Genetics (clinical), 030304 developmental biology, 0303 health sciences, Creatinine, business.industry, 030305 genetics & heredity, Middle Aged, medicine.disease, 3. Good health, Endocrinology, medicine.anatomical_structure, Renal Elimination, chemistry, Renal blood flow, Case-Control Studies, Linear Models, Tyrosine, Female, business, Ochronosis, Glomerular Filtration Rate

Abstract

The clinical effects of alkaptonuria (AKU) are delayed and ageing influences disease progression. Morbidity of AKU is secondary to high circulating homogentisic acid (HGA) and ochronosis. It is not known whether HGA is produced by or processed in the kidney in AKU. Data from AKU patients from four studies were merged to form a single AKU group. A control group of non-AKU subjects was generated by merging data from two non-AKU studies. Data were used to derive renal clearance and fractional excretion (FE) ratios for creatinine, HGA, phenylalanine (PHE) and tyrosine (TYR) using standard calculations, for comparison between the AKU and the control groups. There were 225 AKU patients in the AKU group and 52 in the non-AKU control group. Circulating HGA increased with age (P

Published

2019

23. Quantification of the flux of tyrosine pathway metabolites during nitisinone treatment of Alkaptonuria

Author

James A. Gallagher, Trevor Cox, Andrew S. Davison, Andrew T. Hughes, Anna M. Milan, Nick Rhodes, Milad Khedr, Jozef Rovensky, Lakshminarayan R. Ranganath, and Eftychia E. Psarelli

Subjects

Adult, Male, 0301 basic medicine, medicine.medical_specialty, Nitisinone, Phenylalanine, Metabolite, Body water, lcsh:Medicine, Urine, Alkaptonuria, Article, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Tandem Mass Spectrometry, Internal medicine, Osteoarthritis, medicine, Humans, Homogentisic acid, Tyrosine, lcsh:Science, Bone, Homogentisic Acid, Multidisciplinary, Cyclohexanones, lcsh:R, Diagnostic markers, Pigments, Biological, Middle Aged, medicine.disease, 3. Good health, 030104 developmental biology, Endocrinology, chemistry, Nitrobenzoates, lcsh:Q, Female, 030217 neurology & neurosurgery, medicine.drug

Abstract

Nitisinone decreases homogentisic acid (HGA) in Alkaptonuria (AKU) by inhibiting the tyrosine metabolic pathway in humans. The effect of different daily doses of nitisinone on circulating and 24 h urinary excretion of phenylalanine (PA), tyrosine (TYR), hydroxyphenylpyruvate (HPPA), hydroxyphenyllactate (HPLA) and HGA in patients with AKU was studied over a four week period. Forty AKU patients, randomised into five groups of eight patients, received doses of 1, 2, 4 or 8 mg of nitisinone daily, or no drug (control). Metabolites were analysed by tandem mass spectrometry in 24 h urine and serum samples collected before and after nitisinone. Serum metabolites were corrected for total body water and the sum of 24 hr urine plus total body water metabolites of PA, TYR, HPPA, HPLA and HGA were determined. Body weight and urine urea were used to check on stability of diet and metabolism over the 4 weeks of study. The sum of quantities of urine metabolites (PA, TYR, HPPA, HPLA and HGA) were similar pre- and post-nitisinone. The sum of total body water metabolites were significantly higher post-nitisinone (p

Published

2019

24. Correction to: Assessing the effect of nitisinone induced hypertyrosinaemia on monoamine neurotransmitters in brain tissue from a murine model of alkaptonuria using mass spectrometry imaging

Author

James A. Gallagher, Andrew T. Hughes, Lakshminarayan R. Ranganath, Andrew S. Davison, Juliette H. Hughes, Hazel Sutherland, Nicole Strittmatter, Anna M. Milan, George Bou-Gharios, and Richard J. A. Goodwin

Subjects

0303 health sciences, Nitisinone, business.industry, Endocrinology, Diabetes and Metabolism, 010401 analytical chemistry, Clinical Biochemistry, Brain tissue, Bioinformatics, medicine.disease, 01 natural sciences, Biochemistry, Alkaptonuria, Mass spectrometry imaging, 0104 chemical sciences, 03 medical and health sciences, chemistry.chemical_compound, Monoamine neurotransmitter, chemistry, Murine model, medicine, Hypertyrosinaemia, Neurotransmitter, business, 030304 developmental biology, medicine.drug

Abstract

The original publication of this article contained an incorrect version that did not include some final reviewers' suggestions, was inadvertently received for production and published. The original article has been corrected.

Published

2019

25. The effect of nitisinone on homogentisic acid and tyrosine: a two-year survey of patients attending the National Alkaptonuria Centre, Liverpool

Author

Andrew T. Hughes, Milad Khedr, J. Usher, James A. Gallagher, Jean Devine, Sarah Curtis, Anna M. Milan, Andrew S. Davison, and Lakshminarayan R. Ranganath

Subjects

Adult, Male, 0301 basic medicine, medicine.medical_specialty, Nitisinone, Clinical Biochemistry, Alkaptonuria, Drug Administration Schedule, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Tandem Mass Spectrometry, Internal medicine, medicine, Humans, Longitudinal Studies, Homogentisic acid, Increased homogentisic acid, Enzyme Inhibitors, Tyrosine, Homogentisic Acid, Tyrosine Metabolism, Aged, Monitoring, Physiologic, Homogentisate 1,2-dioxygenase, Homogentisate 1,2-Dioxygenase, Cyclohexanones, business.industry, General Medicine, Middle Aged, medicine.disease, United Kingdom, Surgery, 030104 developmental biology, Endocrinology, chemistry, Nitrobenzoates, Female, business, 030217 neurology & neurosurgery, Chromatography, Liquid, medicine.drug

Abstract

Background Alkaptonuria is a rare, debilitating autosomal recessive disorder affecting tyrosine metabolism. Deficiency of homogentisate 1,2-dioxygenase leads to increased homogentisic acid which is deposited as ochronotic pigment. Clinical sequelae include severe early onset osteoarthritis, increased renal and prostate stone formation and cardiac complications. Treatment has been largely based on analgaesia and arthroplasty. The National Alkaptonuria Centre in Liverpool has been using 2 mg nitisinone (NTBC) off-license for all patients in the United Kingdom with alkaptonuria and monitoring the tyrosine metabolite profiles. Methods Patients with confirmed alkaptonuria are commenced on 2 mg dose (alternative days) of NTBC for three months with daily dose thereafter. Metabolite measurement by LC-MS/MS is performed at baseline, day 4, three-months, six-months and one-year post-commencing NTBC. Thereafter, monitoring and clinical assessments are performed annually. Results Urine homogentisic acid concentration decreased from a mean baseline 20,557 µmol/24 h (95th percentile confidence interval 18,446–22,669 µmol/24 h) by on average 95.4% by six months, 94.8% at one year and 94.1% at two year monitoring. A concurrent reduction in serum homogentisic acid concentration of 83.2% compared to baseline was also measured. Serum tyrosine increased from normal adult reference interval to a mean ± SD of 594 ± 184 µmol /L at year-two monitoring with an increased urinary excretion from 103 ± 81 µmol /24 h at baseline to 1071 ± 726 µmol /24 h two years from therapy. Conclusions The data presented represent the first longitudinal survey of NTBC use in an NHS service setting and demonstrate the sustained effect of NTBC on the tyrosine metabolite profile.

Published

2017

26. GENERATION AND PHENOTYPING OF A TARGETED MOUSE MODEL OF ALKAPTONURIA

Author

Juliette H. Hughes, James A. Gallagher, Ke Liu, Andrew T. Hughes, George Bou-Gharios, Peter Wilson, Lakshminarayan R. Ranganath, Anna M. Milan, and Hazel Sutherland

Subjects

Rheumatology, Biomedical Engineering, medicine, Orthopedics and Sports Medicine, Computational biology, Biology, medicine.disease, Alkaptonuria

Published

2018

27. Nitisinone arrests ochronosis and decreases rate of progression of Alkaptonuria: Evaluation of the effect of nitisinone in the United Kingdom National Alkaptonuria Centre

Author

G. Hughes, JM Devine, S Judd, Anna M. Milan, Nicolas Sireau, N Loftus, James A. Gallagher, Milad Khedr, Trevor Cox, Lakshminarayan R. Ranganath, Joanne A. Harrold, Elizabeth West, Andrew S. Davison, JL Usher, J.P. Dillon, Jonathan C. Jarvis, A Jones, R Griffin, M. C. Briggs, Michael J. Fisher, Eftychia E. Psarelli, Gabor Barton, Sobhan Vinjamuri, Andrew T. Hughes, M McCormick, Anna Daroszewska, and Sophie Taylor

Subjects

0301 basic medicine, Male, medicine.medical_specialty, Nitisinone, Endocrinology, Diabetes and Metabolism, Alkaptonuria, Biochemistry, 4-Hydroxyphenylpyruvate Dioxygenase, 03 medical and health sciences, chemistry.chemical_compound, Endocrinology, Internal medicine, Genetics, medicine, Humans, Homogentisic acid, Molecular Biology, Homogentisic Acid, Ochronosis, business.industry, Cyclohexanones, Disease progression, Treatment phases, Middle Aged, medicine.disease, R1, United Kingdom, 030104 developmental biology, chemistry, Nitrobenzoates, Disease Progression, Female, Ocular ochronosis, business, Clinical progression, medicine.drug

Abstract

QUESTION: Does Nitisinone prevent the clinical progression of the Alkaptonuria? FINDINGS: In this observational study on 39 patients, 2 mg of daily nitisinone inhibited ochronosis and significantly slowed the progression of AKU over a three-year period. MEANING: Nitisinone is a beneficial therapy in Alkaptonuria. BACKGROUND: Nitisinone decreases homogentisic acid (HGA), but has not been shown to modify progression of Alkaptonuria (AKU). METHODS: Thirty-nine AKU patients attended the National AKU Centre (NAC) in Liverpool for assessments and treatment. Nitisinone was commenced at V1 or baseline. Thirty nine, 34 and 22 AKU patients completed 1, 2 and 3 years of monitoring respectively (V2, V3 and V4) in the VAR group. Seventeen patients also attended a pre-baseline visit (V0) in the VAR group. Within the 39 patients, a subgroup of the same ten patients attended V0, V1, V2, V3 and V4 visits constituting the SAME Group. Severity of AKU was assessed by calculation of the AKU Severity Score Index (AKUSSI) allowing comparison between the pre-nitisinone and the nitisinone treatment phases. RESULTS: The ALL (sum of clinical, joint and spine AKUSSI features) AKUSSI rate of change of scores/patient/month, in the SAME group, was significantly lower at two (0.32 ± 0.19) and three (0.15 ± 0.13) years post-nitisinone when compared to pre-nitisinone (0.65 ± 0.15) (p

Published

2018

28. Serum Amino Acid Profiling in Patients with Alkaptonuria Before and After Treatment with Nitisinone

Author

Andrew T. Hughes, Lakshminarayan R. Ranganath, Milad Khedr, Brendan P. Norman, J. Usher, JM Devine, E. A. Smith, Anna M. Milan, James A. Gallagher, and Andrew S. Davison

Subjects

0301 basic medicine, chemistry.chemical_classification, Nitisinone, business.industry, Pharmacology, medicine.disease, Article, Alkaptonuria, Amino acid, 03 medical and health sciences, Metabolic pathway, 030104 developmental biology, 0302 clinical medicine, chemistry, medicine, In patient, Tyrosine, Hypertyrosinaemia, business, 030217 neurology & neurosurgery, After treatment, medicine.drug

Abstract

Alkaptonuria (AKU) is a rare inherited disorder of the tyrosine metabolic pathway. Our group is evaluating the use of the homogentisic acid-lowering agent nitisinone in patients with AKU. A major biochemical consequence of this treatment is hypertyrosinaemia. Herein we report the concentration of 20 serum amino acids over a 36-month period pre- and post-treatment with nitisinone.Fasting serum samples were collected at baseline (pre-nitisinone), 3 (2 mg nitisinone every other day), 6, 12, 24 and 36 (2 mg nitisinone daily) months. Amino acids were measured using the Biochrom 30 high-performance liquid chromatography cation exchange system with ninhydrin detection.Fifty patients [21 female, mean age (±standard deviation) 54.1 (15.6) years (range 25-75); 29 male, mean age 49.3 (11.6) years (range 22-70 years)] were included. Following treatment mean tyrosine concentrations increased seven- to eight-fold (baseline, 69.8 μmol/L; 3 months, 670.7 μmol/L; 6 months, 666.4 μmol/L; 12 months, 692.9 μmol/L; 24 months, 649.4 μmol/L; 36 months, 724.8 μmol/L, p = 0.001 for all visits compared to baseline).At baseline mean phenylalanine, aspartic acid and arginine were outside the normal reference range. Following treatment the ratios of phenylalanine/tyrosine, phenylalanine/large neutral amino acids, arginine/branched chain amino acids and branched chain/aromatic amino acids decreased (p = 0.05), and the tyrosine/large neutral amino acid ratio increased (p = 0.0001).Marked hypertyrosinaemia was observed following treatment with nitisinone. Noteworthy changes were also observed in the ratio of several amino acids following treatment with nitisinone suggesting that the availability of amino acids for neurotransmitter biosynthesis and liver function may be altered following treatment with nitisinone.

Published

2018

29. Asymptomatic Corneal Keratopathy Secondary to Hypertyrosinaemia Following Low Dose Nitisinone and a Literature Review of Tyrosine Keratopathy in Alkaptonuria

Author

Andrew T. Hughes, Lakshminarayan R. Ranganath, E. A. Lock, Rosalind M K Stewart, Milad Khedr, S Judd, Anna M. Milan, M. C. Briggs, and James A. Gallagher

Subjects

030203 arthritis & rheumatology, medicine.medical_specialty, Nitisinone, genetic structures, business.industry, Disease progression, Low dose, medicine.disease, Asymptomatic, Alkaptonuria, eye diseases, Article, Surgery, 03 medical and health sciences, 0302 clinical medicine, Ophthalmology, 030221 ophthalmology & optometry, medicine, sense organs, Red eye, medicine.symptom, Hypertyrosinaemia, business, Ocular pain, medicine.drug

Abstract

Nitisinone, although unapproved for use in alkaptonuria (AKU), is currently the only homogentisic acid lowering therapy with a potential to modify disease progression in AKU. Therefore, safe use of nitisinone off-label requires identifying and managing tyrosine keratopathy. A 22-year-old male with AKU commenced 2 mg daily nitisinone after full assessment. He was issued an alert card explaining potential ocular symptoms such as red eye, tearing, ocular pain and visual impairment and how to manage them. On his first and second annual follow-up visits to the National Alkaptonuria Centre (NAC), there was no corneal keratopathy on slit lamp examination. On his third follow-up annual visit to the NAC, he was found to have typical dendritiform corneal keratopathy in both eyes which was asymptomatic. Nitisinone was suspended until a repeat slit lamp examination, 2 weeks later, confirmed that the keratopathy had resolved. He recommenced nitisinone 2 mg daily with a stricter low protein diet. On his fourth annual follow-up visit to the NAC, a routine slit lamp examination showed mild corneal keratopathy in the left eye. This is despite him reporting no ocular symptoms. This case highlights the fact that corneal keratopathy can occur without symptoms and any monitoring plan with off-label use of nitisinone in AKU will need to take this possibility into account. This is also the first time that typical corneal keratopathy has been described with the use of low dose nitisinone in AKU without symptoms.

Published

2017

30. Assessment of the Effect of Once Daily Nitisinone Therapy on 24-h Urinary Metadrenalines and 5-Hydroxyindole Acetic Acid Excretion in Patients with Alkaptonuria After 4 Weeks of Treatment

Author

Andrew T. Hughes, James A. Gallagher, Anna M. Milan, Milad Khedr, Brendan P. Norman, Lakshminarayan R. Ranganath, Andrew S. Davison, and Jozef Rovensky

Subjects

0301 basic medicine, medicine.medical_specialty, Nitisinone, business.industry, Urinary system, Metabolite, Metabolism, medicine.disease, Article, Alkaptonuria, Excretion, 03 medical and health sciences, chemistry.chemical_compound, 030104 developmental biology, 0302 clinical medicine, Endocrinology, chemistry, Internal medicine, Catecholamine, Medicine, Tyrosine, business, 030217 neurology & neurosurgery, medicine.drug

Abstract

One of the major metabolic consequences of using nitisinone to treat patients with alkaptonuria is that circulating tyrosine concentrations increase. As tyrosine is required for the biosynthesis of catecholamine neurotransmitters, it is possible that their metabolism is altered as a consequence. Herein we report the 24-h urinary excretion of normetadrenaline (NMA), metadrenaline (MA), 3-methoxytyramine (3-MT) (catecholamine metabolites) and 5-hydroxyindole acetic acid (5-HIAA, metabolite of serotonin) in a cohort of AKU patients before and after a 4-week treatment trial with nitisinone.24 h urinary excretions of NMA, MA, 3-MT and 5-HIAA were determined by liquid chromatography tandem mass spectrometry. Interassay coefficient of variation was10% for all analytes measured, at all concentrations tested.Urine samples were assayed at baseline (pre-nitisinone, n = 36) and 4 weeks later; 7 received no nitisinone (4 male, mean age (±SD) 46.3 (16.4) years), and 29 received a daily dose of nitisinone [1 mg (n = 7, 6 male, mean age 45.9 (10.9) years), 2 mg (n = 8, 5 male, mean age 43.9 (13.7) years), 4 mg (n = 8, 5 male, mean age 47.3 (10.7) years) and 8 mg (n = 6, 4 male, mean age 53.8 (8.3) years)]. 3-MT concentrations increase significantly (p 0.01, at all doses) following nitisinone therapy but not in a dose-dependent manner. NMA concentrations decreased (p 0.05, at all doses) following nitisinone therapy at all doses. 5-HIAA concentrations decreased following nitisinone therapy and were significantly lower at a daily dose of 8 mg only (p 0.05).This study shows that catecholamine and serotonin metabolism is altered by treatment with nitisinone.

Published

2017

31. Serum markers in alkaptonuria: simultaneous analysis of homogentisic acid, tyrosine and nitisinone by liquid chromatography tandem mass spectrometry

Author

Andrew T. Hughes, Lakshminarayan R. Ranganath, Anna M. Milan, Gordon A. Ross, John Dutton, James A. Gallagher, Andrew S. Davison, and Peter Christensen

Subjects

Nitisinone, Clinical Biochemistry, Tandem mass spectrometry, Alkaptonuria, chemistry.chemical_compound, Liquid chromatography–mass spectrometry, Tandem Mass Spectrometry, medicine, Humans, Homogentisic acid, Tyrosine, Homogentisic Acid, Homogentisate 1,2-dioxygenase, Chromatography, Cyclohexanones, General Medicine, Reversed-phase chromatography, medicine.disease, chemistry, Biochemistry, Nitrobenzoates, Biomarkers, medicine.drug, Chromatography, Liquid

Abstract

Background Alkaptonuria is a rare debilitating autosomal recessive disorder of tyrosine metabolism, where deficiency of homogentisate 1,2-dioxygenase results in increased homogentisic acid. Homogentisic acid is deposited as an ochronotic pigment in connective tissues, especially cartilage, leading to a severe early onset form of osteoarthritis, increased renal and prostatic stone formation and hardening of heart vessels. Treatment with the orphan drug, nitisinone, an inhibitor of 4-hydroxyphenylpyruvate dioxygenase has been shown to reduce urinary excretion of homogentisic acid. Method A reverse phase liquid chromatography tandem mass spectrometry method has been developed to simultaneously analyse serum homogentisic acid, tyrosine and nitisinone. Using matrix-matched calibration standards, two product ion transitions were identified for each compound (homogentisic acid, tyrosine, nitisinone) and their respective isotopically labelled internal standards (13C6-homogentisic acid, d2-tyrosine, 13C6-nitisinone). Results Intrabatch accuracy was 94–108% for homogentisic acid, 95–109% for tyrosine and 89–106% for nitisinone; interbatch accuracy (n = 20) was 88–108% for homogentisic acid, 91–104% for tyrosine and 88–103% for nitisinone. Precision, both intra- and interbatch were Conclusions The method developed and validated shows good precision, accuracy and linearity appropriate for the monitoring of alkaptonuria patients, pre- and post-nitisinone therapy.

Published

2015

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

Author

Andrew T. Hughes, Eftychia E. Psarelli, Lakshminarayan R. Ranganath, Anna M. Milan, Anthony K Hall, Trevor Cox, Jozef Rovensky, Johan Szamosi, and Birgitta Olsson

Subjects

medicine.medical_specialty, Nitisinone, business.industry, Serum concentration, medicine.disease, Alkaptonuria, Article, Hereditary tyrosinemia, chemistry.chemical_compound, Endocrinology, chemistry, Internal medicine, medicine, In patient, Homogentisic acid, Tyrosine, business, Tyrosine Metabolism, medicine.drug

Abstract

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.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.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.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/h·kg (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 μmol/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.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.

Published

2014

33. Suitability Of Nitisinone In Alkaptonuria 1 (SONIA 1): an international, multicentre, randomised, open-label, no-treatment controlled, parallel-group, dose-response study to investigate the effect of once daily nitisinone on 24-h urinary homogentisic acid excretion in patients with alkaptonuria after 4 weeks of treatment

Author

Hana Ayoob, Judith McCaffrey, Andrea Zatkova, Christa van Kan, Carin Junestrand, Jonathan C. Jarvis, Andrew T. Hughes, Kim-Hanh Le Quan Sang, Helen Bygott, Gordon A. Ross, Lakshminarayan R. Ranganath, Richard Imrich, Anthony K Hall, Dinny Laan, Trevor Cox, Peter Christensen, Mattias Rudebeck, James A. Gallagher, Nicolas Sireau, Torbjörn Kullenberg, Lennart Svensson, Eftychia E. Psarelli, Birgitta Olsson, Daniela Braconi, Federica Genovese, Richard Fitzgerald, Oliver Timmis, Jozef Rovensky, Martina Nemethova, Anna M. Milan, Arvid Cronlund, Annalisa Santucci, Johan Szamosi, John Dutton, and M. C. Briggs

Subjects

0301 basic medicine, Adult, Male, medicine.medical_specialty, Nitisinone, Urinary system, Immunology, Urology, Osteoarthritis, Alkaptonuria, General Biochemistry, Genetics and Molecular Biology, Drug Administration Schedule, Arthritis, Spondyloarthritis, RC1200, Excretion, 03 medical and health sciences, chemistry.chemical_compound, Rheumatology, medicine, Immunology and Allergy, Humans, In patient, Homogentisic acid, Enzyme Inhibitors, Adverse effect, Homogentisic Acid, Dose-Response Relationship, Drug, business.industry, Cyclohexanones, Middle Aged, medicine.disease, 3. Good health, Surgery, 030104 developmental biology, chemistry, Research Design, Nitrobenzoates, Tyrosine, Female, business, medicine.drug

Abstract

Background Alkaptonuria (AKU) is a serious genetic disease characterised by premature spondyloarthropathy. Homogentisate-lowering therapy is being investigated for AKU. Nitisinone decreases homogentisic acid (HGA) in AKU but the dose-response relationship has not been previously studied. Methods Suitability Of Nitisinone In Alkaptonuria 1 (SONIA 1) was an international, multicentre, randomised, open-label, no-treatment controlled, parallel-group, dose-response study. The primary objective was to investigate the effect of different doses of nitisinone once daily on 24-h urinary HGA excretion (u-HGA 24 ) in patients with AKU after 4 weeks of treatment. Forty patients were randomised into five groups of eight patients each, with groups receiving no treatment or 1 mg, 2 mg, 4 mg and 8 mg of nitisinone. Findings A clear dose-response relationship was observed between nitisinone and the urinary excretion of HGA. At 4 weeks, the adjusted geometric mean u-HGA 24 was 31.53 mmol, 3.26 mmol, 1.44 mmol, 0.57 mmol and 0.15 mmol for the no treatment or 1 mg, 2 mg, 4 mg and 8 mg doses, respectively. For the most efficacious dose, 8 mg daily, this corresponds to a mean reduction of u-HGA 24 of 98.8% compared with baseline. An increase in tyrosine levels was seen at all doses but the dose-response relationship was less clear than the effect on HGA. Despite tyrosinaemia, there were no safety concerns and no serious adverse events were reported over the 4 weeks of nitisinone therapy. Conclusions In this study in patients with AKU, nitisinone therapy decreased urinary HGA excretion to low levels in a dose-dependent manner and was well tolerated within the studied dose range. Trial registration number EudraCT number: 2012-005340-24. Registered at ClinicalTrials.gov: NCTO1828463.

Published

2014

34. Antenatal glucocorticoid therapy suppresses angiotensin-converting enzyme activity in rats with nitrofen-induced congenital diaphragmatic hernia

Author

Paul D. Losty, Michael J. Fisher, David A. Lloyd, B O Okoye, and Andrew T. Hughes

Subjects

medicine.medical_specialty, Peptidyl-Dipeptidase A, Pulmonary compliance, Persistent Fetal Circulation Syndrome, Antenatal steroid, Dexamethasone, Rats, Sprague-Dawley, chemistry.chemical_compound, Pulmonary hypoplasia, Pregnancy, Internal medicine, Animals, Humans, Medicine, Glucocorticoids, Lung, Hernia, Diaphragmatic, biology, business.industry, Phenyl Ethers, Infant, Newborn, Congenital diaphragmatic hernia, Angiotensin-converting enzyme, General Medicine, Nitrofen, medicine.disease, Pulmonary hypertension, Rats, Fetal Diseases, Endocrinology, chemistry, Pediatrics, Perinatology and Child Health, biology.protein, Female, Surgery, Hernias, Diaphragmatic, Congenital, business, medicine.drug

Abstract

Neonates with congenital diaphragmatic hernia (CDH) have a high morbidity and mortality rate caused by pulmonary hypoplasia associated with pulmonary hypertension (PH). In experimental CDH, antenatal glucocorticoid therapy improves surfactant biochemical immaturity, enhances lung compliance, and induces morphological maturation in CDH rats. The effects of steroid therapy on preventing or treating PH in this condition have not been studied. Angiotensin converting enzyme (ACE), which is produced by the vascular endothelium, is implicated in the pathogenesis of pulmonary hypertension. The aim of this study was to evaluate the effect of antenatal glucocorticoid therapy on ACE activity and expression in CDH rat lungs.CDH was induced in fetal rats by the maternal administration of 100 mg nitrofen on day 9.5 of gestation (term, day 22). Dexamethasone (Dex) (0.25 mg/kg) was given by intraperitoneal injection on days 18.5 and 19.5 before delivery of the fetuses by cesarean section on day 21.5. Control animals received olive oil (OO) by gavage and normal saline (NS) as vehicle injection. ACE activity was measured spectrophotometrically in the lungs of rats from four treatment groups: CDH-NS, non-CDH-NS, CDH-Dex, and OO-NS controls. Total lung ACE activity (mU per lung) was significantly lower in CDH-NS (P = .002) and CDH-Dex (P = .004) rats compared with non-CDH-NS and OO-NS controls (9.1 +/- 1.0 and 10.7 +/- 1.3 v 16.2 +/- 1.6 and 15.4 +/- 1.7). When specific ACE activity (mU/mg protein) was derived by expressing ACE activity per milligram of lung protein, CDH-NS animals showed elevated specific ACE activity (P = .05) compared with OO-NS controls (6.31 +/- 1.1 v 4.4 +/- 0.4). CDH-Dex animals had a significantly lower specific ACE activity (P = .01) compared with CDH-NS and Non-CDH-NS rats (4.0 +/- 0.4 v 6.31 +/- 1.1 and 5.83 +/- 0.54). The specific ACE activity levels of CDH-Dex rats were equivalent to those seen in the lungs of OO-NS controls (P = .24).Antenatal steroid therapy, by suppressing pulmonary ACE activity, may reduce the risk of pulmonary hypertension developing in human newborns with antenatally diagnosed CDH.

Published

1998

35. Urine homogentisic acid and tyrosine: simultaneous analysis by liquid chromatography tandem mass spectrometry

Author

John Dutton, Lakshminarayan R. Ranganath, Gordon A. Ross, Anna M. Milan, James A. Gallagher, Andrew S. Davison, Peter Christensen, and Andrew T. Hughes

Subjects

Nitisinone, Clinical Biochemistry, Urine, Alkaptonuria, Biochemistry, Analytical Chemistry, chemistry.chemical_compound, Liquid chromatography–mass spectrometry, Limit of Detection, Tandem Mass Spectrometry, medicine, Humans, Homogentisic acid, Tyrosine, Homogentisic Acid, Homogentisate 1,2-dioxygenase, Ochronosis, Chromatography, Cell Biology, General Medicine, medicine.disease, chemistry, medicine.drug, Chromatography, Liquid

Abstract

Alkaptonuria (AKU) is a rare debilitating autosomal recessive disorder of tyrosine metabolism. Deficiency of homogentisate 1,2-dioxygenase results in increased homogentisic acid (HGA) which although excreted in gram quantities in the urine, is deposited as an ochronotic pigment in connective tissues, especially cartilage. Ochronosis leads to a severe, early-onset form of osteoarthritis, increased renal and prostatic stone formation and hardening of heart vessels. Treatment with the orphan drug, Nitisinone, an inhibitor of the enzyme 4-hydroxyphenylpyruvate dioxygenase has been shown to reduce urinary excretion of HGA, resulting in accumulation of the upstream pre-cursor, tyrosine. Using reverse phase LC-MS/MS, a method has been developed to simultaneously quantify urinary HGA and tyrosine. Using matrix-matched calibration standards, two product ion transitions were identified for each compound and their appropriate isotopically labelled internal standards. Validation was performed across the AKU and post-treatment concentrations expected. Intrabatch accuracy for acidified urine was 96-109% for tyrosine and 94-107% for HGA; interbatch accuracy (n=20 across ten assays) was 95-110% for tyrosine and 91-109% for HGA. Precision, both intra- and interbatch was

Published

2014

36. The incorporation of lamotrigine into the routine automated sequential trace enrichment of dialysates assay of anticonvulsants

Author

Andrew T. Hughes, John Dutton, G Higgins, and Norman B. Roberts

Subjects

Phenytoin, 030213 general clinical medicine, medicine.medical_treatment, Clinical Biochemistry, 030209 endocrinology & metabolism, Lamotrigine, High-performance liquid chromatography, 03 medical and health sciences, 0302 clinical medicine, Therapeutic index, medicine, Humans, Adverse effect, Chromatography, High Pressure Liquid, Chromatography, Chemistry, Triazines, General Medicine, Carbamazepine, Anticonvulsant, Phenobarbital, Anticonvulsants, Quantitative analysis (chemistry), medicine.drug

Abstract

We have extended automated sequential trace enrichment of dialysates and high performance liquid chromatography to include the simultaneous assay of lamotrigine with other anticonvulsant drugs: Phenobarbitone, carbamazepine and phenytoin. The procedure is reliable and precise (between-batch coefficients of variation < 2.8%) with no interference from other commonly prescribed drugs. Patients on lamotrigine presented with serum concentrations up to 67 μmol/L with no adverse effects, suggesting that the therapeutic range may need re-appraisal.

Published

1998

37. Studies in alkaptonuria reveal new roles beyond drug clearance for phase I and II biotransformations in tyrosine metabolism

Author

Lakshminarayan R. Ranganath, Andrew T. Hughes, Anna M. Milan, Brendan P. Norman, Jonathan C. Jarvis, Neil G. Berry, James A. Gallagher, Norman B. Roberts, Juliette H. Hughes, Hazel Sutherland, Peter Wilson, Andrew S. Davison, and George Bou-Gharios

Subjects

Purine, Nitisinone, business.industry, Pharmacology, medicine.disease, Alkaptonuria, chemistry.chemical_compound, Metabolic pathway, chemistry, Medicine, Homogentisic acid, Tyrosine, business, Drug metabolism, medicine.drug, Homogentisate 1,2-dioxygenase

Abstract

Background and Purposealkaptonuria (AKU) is an inherited disorder of tyrosine metabolism caused by lack of the enzyme homogentisate 1,2-dioxygenase (HGD). The primary biochemical consequence of HGD-deficiency is increased circulating homogentisic acid (HGA), which is central to AKU disease pathology. The aim of this study was to investigate the wider metabolic consequences of targeted Hgd disruption.Experimental Approachthe first metabolomic analysis of the Hgd−/− AKU mouse model was performed. Urinary metabolites altered in Hgd−/− were further validated by showing that the HGA-lowering drug nitisinone reversed their direction of alteration in AKUKey Resultscomparison of Hgd−/− (AKU) versus Hgd+/− (heterozygous control) urine revealed increases in HGA and a group of 8 previously unreported HGA-derived transformation products from phase I and II metabolism. HGA biotransformation products HGA-sulfate, HGA-glucuronide, HGA-hydrate and hydroxymethyl-HGA were also decreased in urine from both mice and patients with AKU on the HGA-lowering agent nitisinone. Hgd knockout also revealed a host of previously unrecognised associations between tyrosine, purine and TCA cycle metabolic pathways.Conclusion and ImplicationsAKU is rare, but our findings further what is currently understood about tyrosine metabolism more generally, and show for the first time that phase I and II detoxification is recruited to prevent accumulation of endogenously-produced metabolites in inborn errors of metabolism. The data highlight the misconception that phase I and II metabolic biotransformations are reserved solely for drug clearance; these are ancient mechanisms, which represent new potential treatment targets in inherited metabolic diseases.Abstract FigureBullet point summaryWhat is already known Increased circulating homogentisic acid is central to disease pathology in the inherited metabolic disease alkaptonuriaThe Hgd knockout mouse, created in our laboratory, accurately models human alkaptonuriaWhat this study adds Phase I and II biotransformations are recruited in alkaptonuria for detoxification of homogentisic acidThese data challenge misconceptions that phase I and II metabolism is solely for drug clearanceClinical significance Phase I and II metabolic processes represent new treatment targets in inherited metabolic diseasesThe molecular pathology of AKU extends much further than the known alteration to tyrosine metabolism

38. Metabolomic studies in the inborn error of metabolism alkaptonuria reveal new biotransformations in tyrosine metabolism

Author

James A. Gallagher, Andrew T. Hughes, Lakshminarayan R. Ranganath, Jonathan C. Jarvis, Brendan P. Norman, Norman B. Roberts, Hazel Sutherland, Anna M. Milan, Neil G. Berry, Juliette H. Hughes, George Bou-Gharios, Peter Wilson, and Andrew S. Davison

Subjects

0301 basic medicine, Purine, Nitisinone, education, Biochemistry, Alkaptonuria, RC1200, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, medicine, Homogentisic acid, Tyrosine, Molecular Biology, Genetics (clinical), Homogentisate 1,2-dioxygenase, Cell Biology, Metabolism, medicine.disease, Molecular biology, digestive system diseases, surgical procedures, operative, 030104 developmental biology, chemistry, Inborn error of metabolism, 030217 neurology & neurosurgery, medicine.drug

Abstract

Alkaptonuria (AKU) is an inherited disorder of tyrosine metabolism caused by lack of active enzyme homogentisate 1,2-dioxygenase (HGD). The primary consequence of HGD deficiency is increased circulating homogentisic acid (HGA), the main agent in the pathology of AKU disease. Here we report the first metabolomic analysis of AKU homozygous Hgd knockout (Hgd−/−) mice to model the wider metabolic effects of Hgd deletion and the implication for AKU in humans. Untargeted metabolic profiling was performed on urine from Hgd−/− AKU (n = 15) and Hgd+/− non-AKU control (n = 14) mice by liquid chromatography high-resolution time-of-flight mass spectrometry (Experiment 1). The metabolites showing alteration in Hgd−/− were further investigated in AKU mice (n = 18) and patients from the UK National AKU Centre (n = 25) at baseline and after treatment with the HGA-lowering agent nitisinone (Experiment 2). A metabolic flux experiment was carried out after administration of 13C-labelled HGA to Hgd−/−(n = 4) and Hgd+/−(n = 4) mice (Experiment 3) to confirm direct association with HGA. Hgd−/− mice showed the expected increase in HGA, together with unexpected alterations in tyrosine, purine and TCA-cycle pathways. Metabolites with the greatest abundance increases in Hgd−/− were HGA and previously unreported sulfate and glucuronide HGA conjugates, these were decreased in mice and patients on nitisinone and shown to be products from HGA by the 13C-labelled HGA tracer. Our findings reveal that increased HGA in AKU undergoes further metabolism by mainly phase II biotransformations. The data advance our understanding of overall tyrosine metabolism, demonstrating how specific metabolic conditions can elucidate hitherto undiscovered pathways in biochemistry and metabolism.