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12 results on '"TMS, trimethylsilyl"'

3. An incidental finding in newborn screening leading to the diagnosis of a patient with ECHS1 mutations

Author

Sonia Pajares, J. Garcia-Villoria, Laura Gort, Ana Argudo-Ramírez, Olatz Ugarteburu, J.M. González De Aledo-Castillo, Antonia Ribes, J. A. Arranz, Frederic Tort, R.M. López, M.D. Casellas, Raúl Debesa Fernández, José Luis Marín, and M. del Toro

Subjects
Newborn screening, Pediatrics, medicine.medical_specialty, C3DC, malonylcarnitine, Tiglylcarnitine, Genetic counseling, 2-methyl-2,3-dihydroxybutyric acid, Case Report, ECHS1 deficiency, Disease, Congenital lactic acidosis, TMS, trimethylsilyl, ECHS1, short-chain enoyl-CoA hydratase, 3MGA, 3-methylglutaconic acid, Endocrinology, Mutations in ECHS1, Genetics, medicine, HIBCH, 3-hydroxy-isobutyryl-CoA hydrolase, Molecular Biology, Exome, lcsh:QH301-705.5, C4OH, 3-hydroxy-butyrylcarnitine\3-hydoxy-isobutyrylcarnitine, DBS, dried blood spot, Dystonia, lcsh:R5-920, business.industry, medicine.disease, PDH, pyruvate dehydrogenase, C5:1, tiglylcarnitine, NBS, Newborn Screening, lcsh:Biology (General), MS, mass spectrometry, 3-hydroxy-butyrylcarnitine\3-hydoxy-isobutyrylcarnitine, Hypertonia, medicine.symptom, DUS, dried urine spot, business, lcsh:Medicine (General), GC, gas chromatography, MRI, magnetic resonance imaging, Cutis laxa
Abstract

Short-chain enoyl-CoA hydratase (ECHS1) is a mitochondrial beta-oxidation enzyme involved in the metabolism of acyl-CoA fatty acid esters, as well as in valine metabolism. ECHS1 deficiency has multiple manifestations, including Leigh syndrome early at birth or in childhood with poor prognosis, to cutis laxa, exercise-induced dystonia and congenital lactic acidosis.Here we describe the case of a newborn with mutations in ECHS1 that caught our attention after the incidental finding of 3-hydroxy-butyryl/3-hydroxy-isobutyryl/malonylcarnitine (C4OH/C3DC) and tiglylcarnitine (C5:1) on blood spot in the newborn screening (NBS) program. Diagnosis was suspected based on the analysis of organic acids on dried urine spot. A moderate increase of 2-methyl-2,3-dihydroxybutyric acid, was detected, which is a known marker of this disease. Exome analysis showed c.404A>G (p.Asn135Ser) mutation in homozygosis in the ECHS1 gene. The child was therefore admitted to the hospital. Initial examination showed little response to auditory stimuli and mild hypertonia of the extremities. Clinical deterioration was evident at 4 months of age, including neurological and cardiac involvement, and the patient died at 5 months of age. This case illustrates how an incidental detection in the NBS Program can lead to the diagnosis ECHS1 deficiency. Although it is a severe disease, with no treatment available, early detection would allow adequate genetic counseling avoiding the odyssey that suffered most of these families. Keywords: ECHS1 deficiency, Mutations in ECHS1, Newborn screening, 2-methyl-2,3-dihydroxybutyric acid, 3-hydroxy-butyrylcarnitine/3-hydoxy-isobutyrylcarnitine, Tiglylcarnitine

Published
2020

5. Structural Basis for Antibody Catalysis of a Cationic Cyclization Reaction

Author

Zhu, Xueyong, Heine, Andreas, Monnat, Frédéric, Houk, K.N., Janda, Kim D., and Wilson, Ian A.

Subjects
*IMMUNOGLOBULINS, *RING formation (Chemistry)
Abstract

Antibody 4C6 efficiently catalyzes a cationic cyclization reaction. Crystal structures of the antibody 4C6 Fab in complex with benzoic acid and in complex with its eliciting hapten were determined to 1.30 A˚ and 2.45 A˚ resolution, respectively. These crystal structures, together with computational analysis, have elucidated a possible mechanism for the monocyclization reaction. The hapten complex revealed a combining site pocket with high shape complementarity to the hapten. This active site cleft is dominated by aromatic residues that shield the highly reactive carbocation intermediates from solvent and stabilize the carbocation intermediates through cation–π interactions. Modeling of an acyclic olefinic sulfonate ester substrate and the transition state (TS) structures shows that the chair-like transition state is favored, and trapping by water directly produces trans-2-(dimethylphenylsilyl)-cyclohexanol, whereas the less favored boat-like transition state leads to cyclohexene. The only significant change observed upon hapten binding is a side-chain rotation of TrpL89, which reorients to form the base of the combining site. Intriguingly, a benzoic acid molecule was sequestered in the combining site of the unliganded antibody. The 4C6 active site was compared to that observed in a previously reported tandem cyclization antibody 19A4 hapten complex. These cationic cyclization antibodies exhibit convergent structural features with terpenoid cyclases that appear to be important for catalysis. [Copyright &y& Elsevier]

Published
2003
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7. Role of structure and pH in cyclization of allene oxide fatty acids: Implications for the reaction mechanism

Author

Grechkin, Alexander N., Chechetkin, Ivan R., Mukhtarova, Lucia S., and Hamberg, Mats

Subjects
*FATTY acids, *HYDROGEN-ion concentration, *LIPOXYGENASES
Abstract

Incubations of allene oxide synthases of flax or maize with the E,E-isomers of the 13- and 9-hydroperoxides of linoleic acid (E,E-13- and E,E-9-HPOD, respectively) at pH 7.5 afforded substantial yields of trans-disubstituted cyclopentenones. Under the conditions used, (Z,E)-HPODs were converted mainly into α-ketols and afforded only trace amount of cyclopentenones. These findings indicated that changing the double bond geometry from Z to E dramatically increased the rate of formation of the pericyclic pentadienyl cation intermediate necessary for electrocyclization of 18:2-allene oxides and thus the yield of cyclopentenones. The well-known cyclization of the homoallylic allene oxide (12,13-EOT) derived from α-linolenic acid 13-hydroperoxide (E,Z-13-HPOT) into cis-12-oxo-10,15-phytodienoic acid was suppressed at pH below neutral and was not observable at pH 4.5. In contrast, cyclization of the allene oxide ((9E)-12,13-EOD) derived from (E,E)-13-HPOD was slightly favoured at low pH. The finding that the cyclizations of 12,13-EOT and (9E)-12,13-EOD were differently affected by changes in pH suggested that the mechanisms of cyclization of these allene oxides are distinct. [Copyright &y& Elsevier]

Published
2002
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9. In vivo biodistribution studies and ex vivo lymph node imaging using heavy metal-free quantum dots

Author

Elnaz, Yaghini, Helen D, Turner, Alix M, Le Marois, Klaus, Suhling, Imad, Naasani, and Alexander J, MacRobert

Subjects
Heavy metal-free quantum dots, MA, myristic acid, HF, hydrofluoric acid, ICG, indocyanine green, NIR, near-infra red, Metal Nanoparticles, QD, quantum dot, ALN, axillary lymph node, Indium, Sensitivity and Specificity, Article, TMS, trimethylsilyl, Breast cancer, SLN, sentinel lymph node, Metals, Heavy, Quantum Dots, Animals, Nanotechnology, Tissue Distribution, LNs, lymph nodes, SLNB, sentinel lymph node biopsy, TEM, transmission electron microscopy, Photoluminescence, PL, photoluminescence, LED, light-emitting diode, NPs, nanoparticles, PEG, polyethylene glycol, DLS, dynamic light scattering, FLIM, fluorescence lifetime imaging, Reproducibility of Results, ALND, Axillary lymph node dissection, LALN, left axillary lymph node, LTLN, left thoracic lymph node, Rats, ICP-MS, inductively coupled plasma-mass spectroscopy, TLN, thoracic lymph node, CCD, charge-coupled device, Luminescent Measurements, Nanoparticles, Female, QY, quantum yield, Sentinel Lymph Node, RES, reticuloendothelial system
Abstract

Quantum dots (QDs) are attractive photoluminescence probes for biomedical imaging due to their unique photophysical properties. However, the potential toxicity of QDs has remained a major obstacle to their clinical use because they commonly incorporate the toxic heavy metal cadmium within the core of the QDs. In this work, we have evaluated a novel type of heavy metal-free/cadmium-free and biocompatible QD nanoparticles (bio CFQD(®) nanoparticles) with a good photoluminescence quantum yield. Sentinel lymph node mapping is an increasingly important treatment option in the management of breast cancer. We have demonstrated their potential for lymph node mapping by ex vivo imaging of regional lymph nodes after subcutaneous injection in the paw of rats. Using photoluminescence imaging and chemical extraction measurements based on elemental analysis by inductively coupled plasma mass spectroscopy, the quantum dots are shown to accumulate quickly and selectively in the axillary and thoracic regional lymph nodes. In addition, lifetime imaging microscopy of the QD photoluminescence indicates minimal perturbation to their photoluminescence properties in biological systems.

Published
2016

10. An incidental finding in newborn screening leading to the diagnosis of a patient with ECHS1 mutations.

Author

Pajares S, López RM, Gort L, Argudo-Ramírez A, Marín JL, González de Aledo-Castillo JM, García-Villoria J, Arranz JA, Del Toro M, Tort F, Ugarteburu O, Casellas MD, Fernández R, and Ribes A

Abstract

Short-chain enoyl-CoA hydratase (ECHS1) is a mitochondrial beta-oxidation enzyme involved in the metabolism of acyl-CoA fatty acid esters, as well as in valine metabolism. ECHS1 deficiency has multiple manifestations, including Leigh syndrome early at birth or in childhood with poor prognosis, to cutis laxa, exercise-induced dystonia and congenital lactic acidosis. Here we describe the case of a newborn with mutations in ECHS1 that caught our attention after the incidental finding of 3-hydroxy-butyryl\3-hydroxy-isobutyryl\malonylcarnitine (C4OH\C3DC) and tiglylcarnitine (C5:1) on blood spot in the newborn screening (NBS) program. Diagnosis was suspected based on the analysis of organic acids on dried urine spot. A moderate increase of 2-methyl-2,3-dihydroxybutyric acid, was detected, which is a known marker of this disease. Exome analysis showed c.404A>G (p.Asn135Ser) mutation in homozygosis in the ECHS1 gene. The child was therefore admitted to the hospital. Initial examination showed little response to auditory stimuli and mild hypertonia of the extremities. Clinical deterioration was evident at 4 months of age, including neurological and cardiac involvement, and the patient died at 5 months of age. This case illustrates how an incidental detection in the NBS Program can lead to the diagnosis ECHS1 deficiency. Although it is a severe disease, with no treatment available, early detection would allow adequate genetic counseling avoiding the odyssey that suffered most of these families., Competing Interests: The authors have no conflicts of interest to disclose., (© 2019 Published by Elsevier Inc.)

Published
2020
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11. Metabolic and transcriptional response to a high-fat diet in Drosophila melanogaster

Author

William J. Joiner, John T. Ngo, Christian M. Metallo, Rolf Bodmer, Hui Zhang, Soda Balla Diop, Gabriel G. Haddad, Erilynn T. Heinrichsen, and James E. Robinson

Subjects
EASE, Expression Analysis Systematic Explorer (DAVID analysis), Physiology, polymerase chain reaction, capillary feeder, BCAA, branch chain amino acid, w1118, AcCoA, acetyl-coenzyme A, da-GAL4, Triglyceride, TMS, trimethylsilyl, Argininosuccinate lyase, chemistry.chemical_compound, PCR, polymerase chain reaction, VDRC, Vienna Drosophila RNAi Center, acetyl-coenzyme A, CAFE, branch chain amino acid, BCAA, high-fat Diet, chemistry.chemical_classification, Gene knockdown, TG, triglyceride, biology, Lifespan, TBDMS, tert-butyldimethylsilyl, GC/MS, fatty acid methyl ester, TCA, ASL, argininosuccinate lyase, GC/MS, gas chromatography/mass spectrometry, Cell biology, Expression Analysis Systematic Explorer, Vienna Drosophila RNAi Center, white-1118, PCR, HFD, high-fat Diet, Biochemistry, arm-GAL4, armadillo-GAL4, Original Article, TG, arm-GAL4, Drosophila melanogaster, CAFE, capillary feeder, EASE, TCA, tricarboxylic acid, RT-PCR, tert-butyldimethylsilyl, Carbohydrate metabolism, Fdr, gas chromatography/mass spectrometry, Metabolomics, VDRC, ASL, armadillo-GAL4, Obesity, Molecular Biology, Metabolic and endocrine, methanol, Nutrition, w1118, white-1118, Prevention, FAME, fatty acid methyl ester, Fatty acid, trimethylsilyl, Cell Biology, Metabolism, reverse-transcriptase PCR, biology.organism_classification, MeOH, FAME, chemistry, daughterless-Gal4, da-GAL4, daughterless-Gal4, RT-PCR, reverse-transcriptase PCR, TMS, Fdr, false discovery rate, HFD, AcCoA, false discovery rate, Biochemistry and Cell Biology, MeOH, methanol, TBDMS, tricarboxylic acid
Abstract

Obesity has dramatically increased in prevalence, making it essential to understand its accompanying metabolic changes. Modeling diet-induced obesity in Drosophila melanogaster (fruit flies), we elucidated transcriptional and metabolic changes in w1118 flies on a high-fat diet (HFD). Mass spectrometry-based metabolomics revealed altered fatty acid, amino acid, and carbohydrate metabolism with HFD. Microarray analysis uncovered transcriptional changes in nitrogen metabolism, including CG9510, homolog of human argininosuccinate lyase (ASL). CG9510 knockdown in flies phenocopied traits observed with HFD, namely increased triglyceride levels and decreased cold tolerance. Restoration of CG9510 expression ameliorated observed negative consequences of HFD. Metabolomic analysis of CG9510 knockdown flies confirmed functional similarity to ASL, regulating the balance of carbon and nitrogen metabolism. In summary, we found that HFD suppresses CG9510 expression, a gene required for proper triglyceride storage and stress tolerance. These results draw an important link between regulation of amino acid metabolism and the response to diet-induced obesity. © 2013 The Authors.

Published
2014
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12. Metabolic and transcriptional response to a high-fat diet in Drosophila melanogaster.

Author

Heinrichsen ET, Zhang H, Robinson JE, Ngo J, Diop S, Bodmer R, Joiner WJ, Metallo CM, and Haddad GG

Abstract

Obesity has dramatically increased in prevalence, making it essential to understand its accompanying metabolic changes. Modeling diet-induced obesity in Drosophila melanogaster (fruit flies), we elucidated transcriptional and metabolic changes in w (1118) flies on a high-fat diet (HFD). Mass spectrometry-based metabolomics revealed altered fatty acid, amino acid, and carbohydrate metabolism with HFD. Microarray analysis uncovered transcriptional changes in nitrogen metabolism, including CG9510, homolog of human argininosuccinate lyase (ASL). CG9510 knockdown in flies phenocopied traits observed with HFD, namely increased triglyceride levels and decreased cold tolerance. Restoration of CG9510 expression ameliorated observed negative consequences of HFD. Metabolomic analysis of CG9510 knockdown flies confirmed functional similarity to ASL, regulating the balance of carbon and nitrogen metabolism. In summary, we found that HFD suppresses CG9510 expression, a gene required for proper triglyceride storage and stress tolerance. These results draw an important link between regulation of amino acid metabolism and the response to diet-induced obesity.

Published
2013
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