Your search keyword '"Vivian Y. Pao"' showing total 3 results

1. The protease inhibitor combination lopinavir/ritonavir does not decrease insulin secretion in healthy, HIV-seronegative volunteers

Author

Francesca T. Aweeka, Jean-Marc Schwarz, Morris Schambelan, Kathleen Mulligan, Steven A. Taylor, Vivian Y. Pao, Carl Grunfeld, and Grace A. Lee

Subjects

Adult, Blood Glucose, Male, medicine.medical_specialty, Lipoproteins, medicine.medical_treatment, Immunology, Lopinavir/ritonavir, Pyrimidinones, Lopinavir, chemistry.chemical_compound, Insulin resistance, HIV Seronegativity, Internal medicine, Insulin Secretion, medicine, Humans, Insulin, Immunology and Allergy, HIV Protease Inhibitor, Triglycerides, Ritonavir, biology, Triglyceride, virus diseases, HIV Protease Inhibitors, Middle Aged, Lipid Metabolism, medicine.disease, Drug Combinations, Cholesterol, Infectious Diseases, Endocrinology, chemistry, Enzyme inhibitor, Glucose Clamp Technique, biology.protein, medicine.drug

Abstract

BACKGROUND HIV protease inhibitors have been shown to worsen glucose and lipid metabolism. Recent studies have suggested that protease inhibitors can impair insulin secretion in HIV-infected patients. We studied the effects of the protease inhibitor combination lopinavir and ritonavir on insulin secretion, insulin sensitivity, and lipid metabolism in HIV-negative persons. METHODS A combination dose of lopinavir 400 mg and ritonavir 100 mg was given twice daily to eight HIV-seronegative men for 4 weeks. Fasting glucose, insulin, lipid, and lipoprotein profiles; oral glucose tolerance; insulin secretion and insulin-mediated glucose disposal by hyperglycemic clamp; and body composition by dual energy X-ray absorptiometry were determined before and after lopinavir/ritonavir administration. RESULTS There was no change in first-phase insulin secretion (2.82 +/- 0.30 versus 2.71 +/- 0.31 nmol/l; P = 0.60), as well as fasting insulin and glucose levels, oral glucose tolerance, or insulin-mediated glucose disposal after 4 weeks administration of lopinavir/ritonavir. However, there were significant increases in fasting triglycerides (1.02 +/- 0.13 versus 2.20 +/- 0.31 mmol/l; P = 0.001), total cholesterol (4.42 +/- 0.30 versus 5.70 +/- 0.60 mmol/l; P = 0.007), and apo B-100 levels (0.86 +/- 0.07 versus 1.07 +/- 0.11 g/l; P = 0.0009). High-density lipoprotein cholesterol decreased (0.99 +/- 0.11 versus 0.82 +/- 0.10 mmol/l; P = 0.005). There were no changes in body composition, weight, or body fat. CONCLUSION Although administration of lopinavir/ritonavir to healthy, HIV-seronegative volunteers for 4 weeks resulted in increased triglyceride and decreased high-density lipoprotein cholesterol levels, there was no change in first-phase insulin secretion during the hyperglycemic clamp. The reported effects of protease inhibitor on insulin secretion in HIV-infected individuals may be due to changes in HIV-related factors and not a direct drug effect.

Published

2010

2. Structural Requirements for Catalysis and Dimerization of Human Methionine Adenosyltransferase I/III

Author

Tsuneyuki Ubagai, Margaret E. Chamberlin, Vivian Y. Pao, Robert A. Pearlstein, and Janice Yang Chou

Subjects

Models, Molecular, Stereochemistry, Dimer, Molecular Sequence Data, Biophysics, In Vitro Techniques, Biochemistry, Phosphates, chemistry.chemical_compound, Species Specificity, Catalytic Domain, Escherichia coli, Humans, Amino Acid Sequence, Homology modeling, Codon, Protein Structure, Quaternary, Molecular Biology, Conserved Sequence, chemistry.chemical_classification, Base Sequence, Sequence Homology, Amino Acid, biology, Mutagenesis, Active site, Methionine Adenosyltransferase, Amino acid, Isoenzymes, Kinetics, Enzyme, Monomer, chemistry, Mutagenesis, Site-Directed, biology.protein, Dimerization

Abstract

We have used site-directed mutagenesis to probe the structural requirements for catalysis and dimerization of human hepatic methionine adenosyltransferase (hMAT). We built a homology model of the dimeric hMAT III inferred by the crystal structure of the highly homologous Escherichia coli MAT dimer. The active sites of both enzymes comprise the same amino acids and are located in the inter-subunit interface. All of the amino acids predicted to be in the hMAT III active site were mutated, as well as residues in a conserved ATP binding region. All of the mutations except one severely affected catalytic activity. On the other hand, dimerization was affected only by single mutations of three different residues, all on one monomer. The homology model suggested that the side chains of these residues stabilized the monomer and participated in a bridge between subunits consisting of a network of metal and phosphate ions. In agreement with this observation, we demonstrated that dimerization cannot occur in the absence of phosphate.

Published

2000

3. Methionine Adenosyltransferase I/III Deficiency: Novel Mutationsand Clinical Variations

Author

Tsuneyuki Ubagai, Vivian Y. Pao, Margaret E. Chamberlin, Thien Nguyen, Carol L. Greene, S. Harvey Mudd, Janice Yang Chou, Cynthia Freehauf, Harvey L. Levy, and Janet A. Thomas

Subjects

Methionine Adenosyltransferase Deficiency, Adult, Male, Homocysteine, Adolescent, Mutation, Missense, Genes, Recessive, Biology, Hypermethioninemia, Compound heterozygosity, medicine.disease_cause, MAT1A, chemistry.chemical_compound, Methionine, Genetics, medicine, Missense mutation, Humans, Genetics(clinical), RNA, Messenger, Child, Genetics (clinical), Alleles, Polymorphism, Single-Stranded Conformational, Genes, Dominant, Mutation, Infant, Newborn, Brain, Infant, Brain demyelination, Exons, Articles, medicine.disease, Introns, Pedigree, Alternative Splicing, Phenotype, chemistry, Methionine Adenosyltransferase, Child, Preschool, Methionine adenosyltransferase, Female, Metabolism, Inborn Errors

Abstract

Summary Methionine adenosyltransferase (MAT) I/III deficiency, caused by mutations in the MAT1A gene, is characterized by persistent hypermethioninemia without elevated homocysteine or tyrosine. Clinical manifestations are variable and poorly understood, although a number of individuals with homozygous null mutations in MAT1A have neurological problems, including brain demyelination. We analyzed MAT1A in seven hypermethioninemic individuals, to provide insight into the relationship between genotype and phenotype. We identified six novel mutations and demonstrated that mutations resulting in high plasma methionines may signal clinical difficulties. Two patients—a compound heterozygote for truncating and severely inactivating missense mutations and a homozygote for an aberrant splicing MAT1A mutation—have plasma methionine in the 1,226–1,870 μM range (normal 5–35 μM) and manifest abnormalities of the brain gray matter or signs of brain demyelination. Another compound heterozygote for truncating and inactivating missense mutations has 770–1,240 μM plasma methionine and mild cognitive impairment. Four individuals carrying either two inactivating missense mutations or the single-allelic R264H mutation have 105–467 μM plasma methionine and are clinically unaffected. Our data underscore the necessity of further studies to firmly establish the relationship between genotypes in MAT I/III deficiency and clinical phenotypes, to elucidate the molecular bases of variability in manifestations of MAT1A mutations.