Your search keyword '"Steven, Holleran"' showing total 5 results

1. Weight‐loss response to naltrexone/bupropion is modulated by the <scp>Taq1A</scp> genetic variant near <scp> DRD2 </scp> ( <scp>rs1800497</scp> ): A pilot study

Author

Jamie A. Mullally, Rajasekhar Ramakrishnan, Steven Holleran, Tirissa J. Reid, Charles A. LeDuc, Gerardo Febres, Wendy K. Chung, and Judith Korner

Subjects

Bupropion, Dopamine binding, ANKK1, medicine.medical_specialty, business.industry, Endocrinology, Diabetes and Metabolism, media_common.quotation_subject, Appetite, Naltrexone, Endocrinology, Weight loss, Internal medicine, Genotype, Internal Medicine, medicine, medicine.symptom, business, Pharmacogenetics, medicine.drug, media_common

Abstract

Naltrexone/bupropion (NB) is a US Food and Drug Administration-approved antiobesity medication. Clinical trials have shown variable weight loss, with responders and non-responders. NB is believed to act on central dopaminergic pathways to suppress appetite. The Taq1A polymorphism near DRD2 (rs1800497) is associated with the density of striatal dopamine D2 receptors, with individuals carrying the A allele (AA or AG; termed A1+) having 30%-40% fewer dopamine binding sites than those who do not carry the A allele (GG; termed A1-). We performed a pilot study to assess the association of the rs1800497 ANKK1 c.2137G > A (p.Glu713Lys) variant with weight loss with NB treatment in 33 subjects. Mean (SD) weight loss was 5.9% (3.2%) for the A1+ genotype group (n = 15) and 4.2% (4.2%) for the A1- genotype group (n = 18). The mean weight loss for the A1+ genotype group was significantly greater than the predefined clinically significant 4% weight-loss target (one-sample t-test, P = .035), whereas the mean weight loss for the A1- genotype group was not (P = .85). Individuals with the A1+ genotype appear to respond better to NB than A1- individuals.

Published

2021

2. A common Hpa I RFLP of apolipoprotein C-I increases gene transcription and exhibits an ethnically distinct pattern of linkage disequilibrium with the alleles of apolipoprotein E

Author

Yan Xu, Lars Berglund, Rajasekhar Ramakrishnan, Richard Mayeux, Colleen Ngai, Steven Holleran, Benjamin Tycko, Todd Leff, and Neil S. Shachter

Subjects

apolipoproteins C, apolipoproteins E, apolipoproteins B, biochemical genetics, genotype, VLDL, Biochemistry, QD415-436

Abstract

Apolipoprotein (apo) C-I is a constituent of triglyceride-rich lipoproteins (TGRL) that interferes with their hepatic clearance. Functional polymorphism in the apoC-I gene has not been established. We determined that an Hpa I site variably present at −317 relative to the apoC-I gene is produced by a 4-bp CGTT insertion. The apoC-I Hpa I alleles showed an ethnically distinct pattern of linkage disequilibrium with the alleles of the adjacent apoE gene. The frequency of apoC-I Hpa I-positive (H2) with apoE ε2 was 0.98, without significant ethnic difference. In contrast, the frequency of H2 with apoE ε4 was 0.85 in European-Americans but only 0.55 in African-Americans (P < 0.001). The frequency of H2 with apoE ε3 was 0.02 in European-Americans and 0.08 in African-Americans (P < 0.001). African-American apoE ε3/ε3 carriers of apoC-I H2 had 19% lower fasting triglyceride levels than H1 homozygotes (P = 0.03) along with 18% higher HDL-cholesterol levels (P = 0.02). ApoB levels were 21% lower (P = 0.002). H2-allelic reporter-gene constructions showed 50% higher expression in transient transfection studies. We localized the source of this difference in expression to the CGTT insertion itself. Deletion studies of the H1 allele showed a negative transcriptional effect of the polymorphic region. An H1 oligodeoxynucleotide showed specific binding of a hepatomacell nuclear protein not evident with an H2 oligodeoxynucleotide. The H2 sequence may decrease the binding of a negatively acting transcription factor, leading to overexpression of apoC-I. This may produce a functional effect on lipoprotein levels but confirmation is needed in other populations.—Xu, Y., L. Berglund, R. Ramakrishnan, R. Mayeux, C. Ngai, S. Holleran, B. Tycko, T. Leff, and N. S. Shachter. A common Hpa I RFLP of apolipoprotein C-I increases gene transcription and exhibits an ethnically distinct pattern of linkage disequilibrium with the alleles of apolipoprotein E. J. Lipid Res. 1999. 40: 50–58.

Published

1999

3. Weight-loss response to naltrexone/bupropion is modulated by the Taq1A genetic variant near DRD2 (rs1800497): A pilot study

Author

Jamie A, Mullally, Wendy K, Chung, Charles A, LeDuc, Tirissa J, Reid, Gerardo, Febres, Steven, Holleran, Rajasekhar, Ramakrishnan, and Judith, Korner

Subjects

Genotype, Receptors, Dopamine D2, Weight Loss, Humans, Pilot Projects, Protein Serine-Threonine Kinases, Bupropion, Polymorphism, Single Nucleotide, Naltrexone, Article

Abstract

Naltrexone/bupropion (NB) is a US Food and Drug Administration-approved antiobesity medication. Clinical trials have shown variable weight loss, with responders and non-responders. NB is believed to act on central dopaminergic pathways to suppress appetite. The Taq1A polymorphism near DRD2 (rs1800497) is associated with the density of striatal dopamine D2 receptors, with individuals carrying the A allele (AA or AG; termed A1+) having 30%−40% fewer dopamine binding sites than those who do not carry the A allele (GG; termed A1−). We performed a pilot study to assess the association of the rs1800497 ANKK1 c.2137G > A (p.Glu713Lys) variant with weight loss with NB treatment in 33 subjects. Mean (SD) weight loss was 5.9% (3.2%) for the A1+ genotype group (n = 15) and 4.2% (4.2%) for the A1− genotype group (n = 18). The mean weight loss for the A1+ genotype group was significantly greater than the predefined clinically significant 4% weight-loss target (one-sample t-test, P = .035), whereas the mean weight loss for the A1− genotype group was not (P = .85). Individuals with the A1+ genotype appear to respond better to NB than A1- individuals.

Published

2020

4. Catch‐up growth in males affected by the Union Carbide disaster of 1984 in Bhopal, India

Author

Daya R. Varma, Steven Holleran, Ritesh Pal, Tasneem Zaidi, Shree Mulay, Rajashekhar Ramakrishnan, Satinath Sarangi, and Diana Katgara

Subjects

Geography, Environmental health, digestive, oral, and skin physiology, Genetics, Toxic gas, Molecular Biology, Biochemistry, Union carbide, Biotechnology

Abstract

Our 2001 study found that exposure of toddlers and parents in Bhopal to toxic gases in 1984 caused stunting of boys but not of girls (JAMA, 290:1856, 2003); here we report on a follow-up study of a...

Published

2008

5. A common Hpa I RFLP of apolipoprotein C-I increases gene transcription and exhibits an ethnically distinct pattern of linkage disequilibrium with the alleles of apolipoprotein E

Author

Lars Berglund, Steven Holleran, Richard Mayeux, Neil S. Shachter, Yan Xu, Benjamin Tycko, Rajasekhar Ramakrishnan, Todd Leff, and Colleen Ngai

Subjects

Apolipoprotein E, Male, Linkage disequilibrium, Very low-density lipoprotein, Apolipoprotein B, Transcription, Genetic, genotype, Lipoproteins, Black People, QD415-436, Biology, Transfection, Biochemistry, Linkage Disequilibrium, White People, Cell Line, Endocrinology, Apolipoproteins E, Genotype, Humans, Allele, Apolipoproteins C, Deoxyribonucleases, Type II Site-Specific, Promoter Regions, Genetic, Alleles, DNA Primers, Genetics, Apolipoprotein C-I, Base Sequence, Nuclear Proteins, Cell Biology, DNA, Molecular biology, apolipoproteins B, biology.protein, biochemical genetics, lipids (amino acids, peptides, and proteins), Female, Restriction fragment length polymorphism, VLDL, Polymorphism, Restriction Fragment Length

Abstract

Apolipoprotein (apo) C-I is a constituent of triglyceride-rich lipoproteins (TGRL) that interferes with their hepatic clearance. Functional polymorphism in the apoC-I gene has not been established. We determined that an Hpa I site variably present at −317 relative to the apoC-I gene is produced by a 4-bp CGTT insertion. The apoC-I Hpa I alleles showed an ethnically distinct pattern of linkage disequilibrium with the alleles of the adjacent apoE gene. The frequency of apoC-I Hpa I-positive (H2) with apoE ε2 was 0.98, without significant ethnic difference. In contrast, the frequency of H2 with apoE ε4 was 0.85 in European-Americans but only 0.55 in African-Americans (P < 0.001). The frequency of H2 with apoE ε3 was 0.02 in European-Americans and 0.08 in African-Americans (P < 0.001). African-American apoE ε3/ε3 carriers of apoC-I H2 had 19% lower fasting triglyceride levels than H1 homozygotes (P = 0.03) along with 18% higher HDL-cholesterol levels (P = 0.02). ApoB levels were 21% lower (P = 0.002). H2-allelic reporter-gene constructions showed 50% higher expression in transient transfection studies. We localized the source of this difference in expression to the CGTT insertion itself. Deletion studies of the H1 allele showed a negative transcriptional effect of the polymorphic region. An H1 oligodeoxynucleotide showed specific binding of a hepatomacell nuclear protein not evident with an H2 oligodeoxynucleotide. The H2 sequence may decrease the binding of a negatively acting transcription factor, leading to overexpression of apoC-I. This may produce a functional effect on lipoprotein levels but confirmation is needed in other populations.—Xu, Y., L. Berglund, R. Ramakrishnan, R. Mayeux, C. Ngai, S. Holleran, B. Tycko, T. Leff, and N. S. Shachter. A common Hpa I RFLP of apolipoprotein C-I increases gene transcription and exhibits an ethnically distinct pattern of linkage disequilibrium with the alleles of apolipoprotein E. J. Lipid Res. 1999. 40: 50–58.

Published

1998