Lesch-Nyhan disease: from mechanism to model and back again

Jinnah, Hyder A.

doi:10.1242/dmm.002543

Cited by 64 publications

(58 citation statements)

References 33 publications

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“…However, this hypothesis does not explain why LNS variant phenotypes (>1% enzymatic activity) that have only slightly active HPRT do not exhibit the self-injurious behavior [Bakay et al, 1979;Sege-Peterson et al, 1992]. Furthermore, patients who are prenatally diagnosed with LNS and are administered allopurinol upon birth and never have significantly elevated levels of uric acid in their blood still develop the classic LNS neurobehavioral phenotype [Jinnah, 2009], suggesting a limited role of uric acid in the neurological features of LNS. Today, uric acid overproduction is still treated using allopurinol, and while this effectively manages several aspects of the disease, including gout and liver failure, it is not thought to influence the development of the neurobehavioral symptoms of LNS [Nyhan, 2005].…”

Section: Uric Acidmentioning

confidence: 98%

“…The earliest models used to study LNS were based on non-neural cells that could be easily acquired from patients, mostly from blood (erythrocytes and lymphocytes) or skin (fibroblasts) [Jinnah, 2009]. These models were easy to establish and had direct relevance to the patients they were derived from.…”

Section: Tissue Culture Models Of Lnsmentioning

confidence: 99%

“…Further studies administering adenine did so in tandem with allopurinol to control 2,8-dioxyadenine concentration and did not observe any improvement in behavior [Watts et al, 1974]. As uric acid levels can usually be managed well using allopurinol alone [Jinnah, 2009], adenine therapy is no longer used in the treatment of LNS.…”

Section: Adeninementioning

confidence: 99%

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Lesch-Nyhan Syndrome: Models, Theories, and Therapies

et al. 2016

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Lesch-Nyhan syndrome (LNS) is a rare X-linked disorder caused by mutations in HPRT1, an important enzyme in the purine salvage pathway. Symptoms of LNS include dystonia, gout, intellectual disability, and self-mutilation. Despite having been characterized over 50 years ago, it remains unclear precisely how deficits in hypoxanthine and guanine recycling can lead to such a profound neurological phenotype. Several studies have proposed different hypotheses regarding the etiology of this disease, and several treatments have been tried in patients, though none have led to a satisfactory explanation of the disease. New technologies such as next-generation sequencing, optogenetics, genome editing, and induced pluripotent stem cells provide a unique opportunity to map the precise sequential pathways leading from genotype to phenotype.

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Section: Uric Acidmentioning

confidence: 98%

Section: Tissue Culture Models Of Lnsmentioning

confidence: 99%

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Lesch-Nyhan Syndrome: Models, Theories, and Therapies

et al. 2016

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“…Despite substantial research efforts, the link between HPRT deficiency and self-injurious behavior in LND is still unknown (Jinnah 2009;Harris 2010;Duley et al 2011).…”

mentioning

confidence: 99%

Impairment of adenylyl cyclase 2 function and expression in hypoxanthine phosphoribosyltransferase-deficient rat B103 neuroblastoma cells as model for Lesch–Nyhan disease: BODIPY–forskolin as pharmacological tool

Kinast

Ohe

Burhenne

et al. 2012

Naunyn-Schmiedeberg's Arch Pharmacol

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Hypoxanthine phosphoribosyl transferase (HPRT) deficiency results in Lesch-Nyhan disease (LND). The link between the HPRT defect and the self-injurious behavior in LND is still unknown. HPRT-deficient rat B103 neuroblastoma cells serve as a model system for LND. In B103 cell membranes, HPRT deficiency is associated with a decrease of basal and guanosine triphosphate-stimulated adenylyl cyclase (AC) activity (Pinto and Seifert, J Neurochem 96:454-459, 2006). Since recombinant AC2 possesses a high basal activity, we tested the hypothesis that AC2 function and expression is impaired in HPRT deficiency. We examined AC regulation in B103 cell membranes, cAMP accumulation in intact B103 cells, AC isoform expression, and performed morphological studies. As most important pharmacological tool, we used 4,4-difluoro-4-bora-3a,4a-diaza-s-indacene forskolin (BODIPY-FS) that inhibits recombinant AC2 but activates ACs 1 and 5 (Erdorf et al., Biochem Pharmacol 82:1673-1681, 2011). In B103 control membranes, BODIPY-FS reduced catalysis, but in HPRT(-) membranes, BODIPY-FS was rather stimulatory. 2'(3')-O-(N-methylanthraniloyl) (MANT)-nucleoside 5'-[γ-thio]triphosphates inhibit recombinant ACs 1 and 5 more potently than AC2. In B103 control membranes, MANT-guanosine 5'-[γ-thio]triphosphate inhibited catalysis in control membranes less potently than in HPRT(-) membranes. Quantitative real-time PCR revealed that in HPRT deficiency, AC2 was virtually absent. In contrast, AC5 was up-regulated. Forskolin (FS) and BODIPY-FS induced cell clustering and rounding and neurite extension in B103 cells. The effects of FS and BODIPY-FS were much more prominent in control than in HPRT(-) cells, indicative for a differentiation defect in HPRT deficiency. Neither FS nor BODIPY-FS significantly changed cAMP concentrations in intact B103 cells. Collectively, our data show that HPRT deficiency in B103 cells is associated with impaired AC2 function and expression and reduced sensitivity to differentiation induced by FS and BODIPY-FS. We discuss the pathophysiological implications of our data for LND.

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“…At 20 months, the patient was unable to control his head or speak; he also showed swallowing and severe dystonic-dyskinetic movement disorder of the upper limbs with generalized hypertonia crisis towards opistotonus. LND is a rare X-linked recessive disorder [2] characterized by the progressive development of mental retardation, spasticity, choreo-athetosis, self-mutilation, and hyperuricemia [3,4], due to complete deficiency of the activity of HGPRT (OMIM 308000) [2]. However, partially HGPRTdeficient patients (OMIM 300323) present these symptoms with different degrees of intensity [5].…”

Section: Sirsmentioning

confidence: 99%

Orange-colored diapers as first sign of Lesch-Nyhan disease in an asymptomatic infant

Gasperini

Stagi²,

Gasperini

et al. 2010

Pediatr Nephrol

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Sirs, We read with great interest the letter of Demirdas and Schröder [1] about the differential diagnosis in changed color of urine in infants.We have followed a 3-month-old male who was hospitalized for the presence of orange-colored diapers. He was born from unrelated parents after an uneventful pregnancy. High levels of uric acid were found in the plasma (11.7 mg/dl; normal values 1.7-5.8). Kidney ultrasound examination showed mild and diffuse increase of signal in cortical area with nephrolithiasis. Fundus oculi, electroencephalogram (EEG), and brain ultrasound were normal. Successively, the infant presented dystonic movements, mild axial hypotonia, and hypertonia of the legs with increased tendon reflexes and scissoring. The study of purine and pyrimidine metabolism by electrospray ionization tandem mass spectrometry (MS-MS) showed high levels of hypoxanthine (20.3 mmol/mol of creatinine; normal values 0.43-11.31). Enzymatic assay in red cells showed an absence of hypoxanthine-guanine phosphoribosyltransferase activity (HGPRT). Molecular analysis confirmed the diagnosis of Lesch-Nyhan disease (LND; OMIM 300322) in the patient and his mother as a carrier: a duplication of 8 nucleotides 89-96 (89_96dupAGGATTTG) in exon 2 of HPRT1 gene was found in chromosome X.Brain magnetic resonance imaging showed white matter atrophy of bilateral symmetric temporal-insular regions with respective enlargement of subarachnoid spaces with mild decreased concentration of NAA and Cho at spectroscopy. At 20 months, the patient was unable to control his head or speak; he also showed swallowing and severe dystonic-dyskinetic movement disorder of the upper limbs with generalized hypertonia crisis towards opistotonus.

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Lesch-Nyhan disease: from mechanism to model and back again

Cited by 64 publications

References 33 publications

Lesch-Nyhan Syndrome: Models, Theories, and Therapies

Lesch-Nyhan Syndrome: Models, Theories, and Therapies

Impairment of adenylyl cyclase 2 function and expression in hypoxanthine phosphoribosyltransferase-deficient rat B103 neuroblastoma cells as model for Lesch–Nyhan disease: BODIPY–forskolin as pharmacological tool

Orange-colored diapers as first sign of Lesch-Nyhan disease in an asymptomatic infant

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