<b><i>TAT</i></b> gene mutation analysis in three Palestinian kindreds with oculocutaneous tyrosinaemia type II; characterization of a silent exonic transversion that causes complete missplicing by exon 11 skipping

Maydan, Gal; Andresen, Brage S.; Madsen, Pia Pinholt; Zeigler, Marsha; Raas‐Rothschild, Annick; Zlotogorski, A.; Gutman, Alisa; Korman, Stanley H.

doi:10.1007/s10545-006-0407-8

Cited by 23 publications

(11 citation statements)

References 27 publications

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“…Indeed, we report a case (patient 141), diagnosed at age 54, with both skin and neurological symptoms but no ocular phenotype. Seasonal variation in ocular and cutaneous symptoms, as in our patient 136, have already been noted by Hanhart and related to changes in temperature, but could also be related to diet, making it more difficult to reach solid diagnostic conclusions from specific symptoms observed at a given time point during the course of disease. Furthermore, even tyrosine plasma levels appear inconclusive in the prediction of specific phenotypes, as asymptomatic individuals presenting with high tyrosinemia do exist.…”

Section: Discussionmentioning

confidence: 55%

“…Regarding plasma tyrosine levels, patient 85 showed the highest value with 2836 µmol/L, while patient 97, asymptomatic at age 21, exhibited the lowest serum levels at 515 µmol/L (Table ).…”

Section: Resultsmentioning

confidence: 99%

“…Skin symptoms are mostly represented by painful hyperkeratotic plaques of soles and palms, which usually develop after the first year of life, although they may appear earlier. Intellectual disability is a relatively common feature but may be mild or absent …”

Section: Introductionmentioning

confidence: 99%

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Tyrosinemia type II: Mutation update, 11 novel mutations and description of 5 independent subjects with a novel founder mutation

et al. 2017

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Section: Discussionmentioning

confidence: 55%

Section: Resultsmentioning

confidence: 99%

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Tyrosinemia type II: Mutation update, 11 novel mutations and description of 5 independent subjects with a novel founder mutation

et al. 2017

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“…In tyrosinemia type II, tyrosine accumulates in blood, eventually causing lesions in the patients (al-Hemidan and al-Hazzaa, 1995). In humans, more than 15 mutations have been identified in the patients of tyrosinemia type II in Italy, France, USA and the UK (Natt et al, 1992; Endo, 1998; Charfeddine et al, 2006; Maydan et al, 2006; Minami-Hori et al, 2006; Meissner et al, 2008; Pasternack et al, 2009). Tyrosinemia type II is often associated with consanguinity.…”

Section: Introductionmentioning

confidence: 99%

Tyrosine aminotransferase: biochemical and structural properties and molecular dynamics simulations

et al. 2010

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Tyrosine aminotransferase (TAT) catalyzes the transamination of tyrosine and other aromatic amino acids. The enzyme is thought to play a role in tyrosinemia type II, hepatitis and hepatic carcinoma recovery. The objective of this study is to investigate its biochemical and structural characteristics and substrate specificity in order to provide insight regarding its involvement in these diseases. Mouse TAT (mTAT) was cloned from a mouse cDNA library, and its recombinant protein was produced using Escherichia coli cells and purified using various chromatographic techniques. The recombinant mTAT is able to catalyze the transamination of tyrosine using α-ketoglutaric acid as an amino group acceptor at neutral pH. The enzyme also can use glutamate and phenylalanine as amino group donors and p-hydroxy-phenylpyruvate, phenylpyruvate and alpha-ketocaproic acid as amino group acceptors. Through macromolecular crystallography we have determined the mTAT crystal structure at 2.9 Å resolution. The crystal structure revealed the interaction between the pyridoxal-5′-phosphate cofactor and the enzyme, as well as the formation of a disulphide bond. The detection of disulphide bond provides some rational explanation regarding previously observed TAT inactivation under oxidative conditions and reactivation of the inactive TAT in the presence of a reducing agent. Molecular dynamics simulations using the crystal structures of Trypanosoma cruzi TAT and human TAT provided further insight regarding the substrate-enzyme interactions and substrate specificity. The biochemical and structural properties of TAT and the binding of its cofactor and the substrate may help in elucidation of the mechanism of TAT inhibition and activation.

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“…Deficiency of TAT, which is caused by genetic mutations in the Tat gene, in humans leads to tyrosinemia type II syndrome characterized by elevated blood tyrosine levels, mental retardation, etc [8]. To date, more than 15 distinct mutations [8], [9], [10], [11], [12], [13], [14], [15] have been identified in humans that cause tyrosinemia type II.…”

Section: Introductionmentioning

confidence: 99%

Relaxed Evolution in the Tyrosine Aminotransferase Gene Tat in Old World Fruit Bats (Chiroptera: Pteropodidae)

et al. 2014

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Frugivorous and nectarivorous bats fuel their metabolism mostly by using carbohydrates and allocate the restricted amounts of ingested proteins mainly for anabolic protein syntheses rather than for catabolic energy production. Thus, it is possible that genes involved in protein (amino acid) catabolism may have undergone relaxed evolution in these fruit- and nectar-eating bats. The tyrosine aminotransferase (TAT, encoded by the Tat gene) is the rate-limiting enzyme in the tyrosine catabolic pathway. To test whether the Tat gene has undergone relaxed evolution in the fruit- and nectar-eating bats, we obtained the Tat coding region from 20 bat species including four Old World fruit bats (Pteropodidae) and two New World fruit bats (Phyllostomidae). Phylogenetic reconstructions revealed a gene tree in which all echolocating bats (including the New World fruit bats) formed a monophyletic group. The phylogenetic conflict appears to stem from accelerated TAT protein sequence evolution in the Old World fruit bats. Our molecular evolutionary analyses confirmed a change in the selection pressure acting on Tat, which was likely caused by a relaxation of the evolutionary constraints on the Tat gene in the Old World fruit bats. Hepatic TAT activity assays showed that TAT activities in species of the Old World fruit bats are significantly lower than those of insectivorous bats and omnivorous mice, which was not caused by a change in TAT protein levels in the liver. Our study provides unambiguous evidence that the Tat gene has undergone relaxed evolution in the Old World fruit bats in response to changes in their metabolism due to the evolution of their special diet.

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TAT gene mutation analysis in three Palestinian kindreds with oculocutaneous tyrosinaemia type II; characterization of a silent exonic transversion that causes complete missplicing by exon 11 skipping

Cited by 23 publications

References 27 publications

Tyrosinemia type II: Mutation update, 11 novel mutations and description of 5 independent subjects with a novel founder mutation

Tyrosinemia type II: Mutation update, 11 novel mutations and description of 5 independent subjects with a novel founder mutation

Tyrosine aminotransferase: biochemical and structural properties and molecular dynamics simulations

Relaxed Evolution in the Tyrosine Aminotransferase Gene Tat in Old World Fruit Bats (Chiroptera: Pteropodidae)

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