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2. Functional and genetic epidemiological characterisation of theFFAR4(GPR120) p.R270H variant in the Danish population

Author

Vestmar, Marie A, primary, Andersson, Ehm A, additional, Christensen, Charlotte R, additional, Hauge, Maria, additional, Glümer, Charlotte, additional, Linneberg, Allan, additional, Witte, Daniel R, additional, Jørgensen, Marit E, additional, Christensen, Cramer, additional, Brandslund, Ivan, additional, Lauritzen, Torsten, additional, Pedersen, Oluf, additional, Holst, Birgitte, additional, Grarup, Niels, additional, Schwartz, Thue W, additional, and Hansen, Torben, additional

Published
2016
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3. Exome sequencing-driven discovery of coding polymorphisms associated with common metabolic phenotypes

Author

Albrechtsen, Anders, Grarup, Niels, Li, Y., Sparsø, Thomas Hempel, Tian, G., Cao, H., Jiang, T., Kim, S.Y., Korneliussen, Thorfinn Sand, Li, Q., Nie, C., Wu, R., Skotte, Line, Morris, A.P., Ladenvall, C., Cauchi, S., Stancáková, A., Andersen, G., Astrup, Arne, Banasik, Karina, Bennett, A.J., Bolund, Lars, Charpentier, G., Chen, Y., Dekker, J.M., Doney, A.S.F., Dorkhan, M., Forsen, T., Frayling, T.M., Groves, C.J., Gui, Y., Hallmans, G., Hattersley, A.T., He, K., Hitman, G.A., Holmkvist, J., Huang, S., Jiang, H., Jin, X., Justesen, Johanne Marie, Kristiansen, Karsten, Kuusisto, J., Lajer, M., Lantieri, O., Li, W., Liang, H., Liao, Q., Liu, X., Ma, T., Ma, X., Manijak, M.P., Marre, M., Mokrosinski, Jacek, Morris, A.D., Mu, B., Nielsen, A.A., Nijpels, G., Nilsson, P., Palmer, C.N.A., Rayner, N.W., Renström, F., Ribel-Madsen, Rasmus, Robertson, N., Rolandsson, O., Rossing, P., Schwartz, Thue W., Slagboom, P.E., Sterner, M., Tang, M., Tarnow, L., Tuomi, T., Van't Riet, E., van Leeuwen, N., Varga, T.V., Vestmar, Marie Aare, Walker, M., Wang, B., Wang, Y., Wu, H., Xi, F., Yengo, L., Yu, C., Zhang, X., Zhang, J., Zhang, Q., Zhang, W., Zheng, H., Zhou, Y., Altshuler, D., 't Hart, L.M., Franks, P.W., Balkau, B., Froguel, P., McCarthy, M.I., Laakso, M., Groop, L., Christensen, C., Brandslund, I., Lauritzen, T., Witte, D.R., Linneberg, A., Jørgensen, Torben, Hansen, Torben, Wang, Jun, Nielsen, Rasmus, Pedersen, Oluf, Albrechtsen, Anders, Grarup, Niels, Li, Y., Sparsø, Thomas Hempel, Tian, G., Cao, H., Jiang, T., Kim, S.Y., Korneliussen, Thorfinn Sand, Li, Q., Nie, C., Wu, R., Skotte, Line, Morris, A.P., Ladenvall, C., Cauchi, S., Stancáková, A., Andersen, G., Astrup, Arne, Banasik, Karina, Bennett, A.J., Bolund, Lars, Charpentier, G., Chen, Y., Dekker, J.M., Doney, A.S.F., Dorkhan, M., Forsen, T., Frayling, T.M., Groves, C.J., Gui, Y., Hallmans, G., Hattersley, A.T., He, K., Hitman, G.A., Holmkvist, J., Huang, S., Jiang, H., Jin, X., Justesen, Johanne Marie, Kristiansen, Karsten, Kuusisto, J., Lajer, M., Lantieri, O., Li, W., Liang, H., Liao, Q., Liu, X., Ma, T., Ma, X., Manijak, M.P., Marre, M., Mokrosinski, Jacek, Morris, A.D., Mu, B., Nielsen, A.A., Nijpels, G., Nilsson, P., Palmer, C.N.A., Rayner, N.W., Renström, F., Ribel-Madsen, Rasmus, Robertson, N., Rolandsson, O., Rossing, P., Schwartz, Thue W., Slagboom, P.E., Sterner, M., Tang, M., Tarnow, L., Tuomi, T., Van't Riet, E., van Leeuwen, N., Varga, T.V., Vestmar, Marie Aare, Walker, M., Wang, B., Wang, Y., Wu, H., Xi, F., Yengo, L., Yu, C., Zhang, X., Zhang, J., Zhang, Q., Zhang, W., Zheng, H., Zhou, Y., Altshuler, D., 't Hart, L.M., Franks, P.W., Balkau, B., Froguel, P., McCarthy, M.I., Laakso, M., Groop, L., Christensen, C., Brandslund, I., Lauritzen, T., Witte, D.R., Linneberg, A., Jørgensen, Torben, Hansen, Torben, Wang, Jun, Nielsen, Rasmus, and Pedersen, Oluf

Abstract

AIMS/HYPOTHESIS: Human complex metabolic traits are in part regulated by genetic determinants. Here we applied exome sequencing to identify novel associations of coding polymorphisms at minor allele frequencies (MAFs) >1% with common metabolic phenotypes. METHODS: The study comprised three stages. We performed medium-depth (8×) whole exome sequencing in 1,000 cases with type 2 diabetes, BMI >27.5 kg/m(2) and hypertension and in 1,000 controls (stage 1). We selected 16,192 polymorphisms nominally associated (p¿1%. In stage 2 we identified 51 potential associations with one or more of eight metabolic phenotypes covered by 45 unique polymorphisms. In meta-analyses of stage 2 and stage 3 results, we demonstrated robust associations for coding polymorphisms in CD300LG (fasting HDL-cholesterol: MAF 3.5%, p¿=¿8.5¿×¿10(-14)), COBLL1 (type 2 diabetes: MAF 12.5%, OR 0.88, p¿=¿1.2¿×¿10(-11)) and MACF1 (type 2 diabetes: MAF 23.4%, OR 1.10, p¿=¿8.2¿×¿10(-10)). CONCLUSIONS/INTERPRETATION: We applied exome sequencing as a basis for finding genetic determinants of metabolic traits and show the existence of low-frequency and common coding polymorphisms with impact on common metabolic traits. Based on our study, coding polymorphisms with MAF above 1% do not seem to have particularly high effect sizes on the measured metabolic traits.

Published
2013

4. Studies of metabolic phenotypic correlates of 15 obesity associated gene variants

Author

Sandholt, Camilla Helene, Vestmar, Marie Aare, Bille, Dorthe Sadowa, Borglykke, Anders, Almind, Katrine, Hansen, Lars, Sandbæk, Annelli, Lauritzen, Torsten, Witte, Daniel, Jørgensen, Torben, Pedersen, Oluf, Hansen, Torben, Sandholt, Camilla Helene, Vestmar, Marie Aare, Bille, Dorthe Sadowa, Borglykke, Anders, Almind, Katrine, Hansen, Lars, Sandbæk, Annelli, Lauritzen, Torsten, Witte, Daniel, Jørgensen, Torben, Pedersen, Oluf, and Hansen, Torben

Abstract

Aims: Genome-wide association studies have identified novel BMI/obesity associated susceptibility loci. The purpose of this study is to determine associations with overweight, obesity, morbid obesity and/or general adiposity in a Danish population. Moreover, we want to investigate if these loci associate with type 2 diabetes and to elucidate potential underlying metabolic mechanisms. Methods: 15 gene variants in 14 loci including TMEM18 (rs7561317), SH2B1 (rs7498665), KCTD15 (rs29941), NEGR1 (rs2568958), ETV5 (rs7647305), BDNF (rs4923461, rs925946), SEC16B (rs10913469), FAIM2 (rs7138803), GNPDA2 (rs10938397), MTCH2 (rs10838738), BAT2 (rs2260000), NPC1 (rs1805081), MAF (rs1424233), and PTER (rs10508503) were genotyped in 18,014 middle-aged Danes. Results: Five of the 15 gene variants associated with overweight, obesity and/or morbid obesity. Per allele ORs ranged from 1.15–1.20 for overweight, 1.10–1.25 for obesity, and 1.41–1.46 for morbid obesity. Five of the 15 variants moreover associated with increased measures of adiposity. BDNF rs4923461 displayed a borderline BMI-dependent protective effect on type 2 diabetes (0.87 (0.78–0.96, p = 0.008)), whereas SH2B1 rs7498665 associated with nominally BMI-independent increased risk of type 2 diabetes (1.16 (1.07–1.27, p = 7.861024)). Conclusions: Associations with overweight and/or obesity and measures of obesity were confirmed for seven out of the 15 gene variants. The obesity risk allele of BDNF rs4923461 protected against type 2 diabetes, which could suggest neuronal and peripheral distinctive ways of actions for the protein. SH2B1 rs7498665 associated with type 2 diabetes independently of BMI.

Published
2011

5. The Effect of PCSK1 Variants on Waist, Waist-Hip Ratio and Glucose Metabolism Is Modified by Sex and Glucose Tolerance Status

Author

Gjesing, Anette P, Vestmar, Marie A, Jørgensen, Torben, Heni, Martin, Holst, Jens J, Witte, Daniel R, Hansen, Torben, Pedersen, Oluf, Gjesing, Anette P, Vestmar, Marie A, Jørgensen, Torben, Heni, Martin, Holst, Jens J, Witte, Daniel R, Hansen, Torben, and Pedersen, Oluf

Abstract

Background: We aimed to evaluate the effects of the G-allele of rs6232 and the C-allele of rs6235 within PCSK1 on measures of body fat and glucose homeostasis in Danish individuals and to assess interactions of genotypes with age, sex and glucose tolerance status. Data were included in meta-analyses of additional Europeans. Methodology/Principal Findings: Rs6232 and rs6235 were genotyped in 6,164 Danes from the Inter99 study of middleaged people. Results from these analyses were combined with previously published studies in meta-analyses of a total of 27,786 individuals. The impact of the variants was also investigated in a subset of 62 glucose-tolerant men during a meal challenge including measures of serum incretins. In men we found an effect on body composition in sex-stratified analyses where the rs6235 C-allele conferred an increased waist circumference of 0.8 cm per allele (0.2–1.5, p = 0.008) and increased waist-to-hip ratio of 0.004 (0.0005–0.008, p = 0.027). In the meta-analyses where men and women were combined, the rs6232 G-allele associated with increased waist-to-hip ratio (p = 0.02) and the rs6235 C-allele associated with increased waist circumference (p = 0.01). Furthermore, the rs6235 C-allele was associated nominally with a 0.6% (0.1–1%, p = 0.01) reduction in fasting glucose, it interacted with glucose tolerance status for traits related to glucose metabolism and analysis among individuals having abnormal glucose tolerance revealed a 5% (20.7–9%, p = 0.02) elevated level of acute insulin response for this variant. Finally, we found that the rs6232 G-allele associated with higher levels of GLP-1, GLP-2 and glucagon and that the rs6235 C-allele associated with higher levels of GIP and glucagon during a meal-test. Conclusions/Significance: PCSK1 rs6232 G-allele and rs6235 C-allele have an effect on body composition which may be modified by sex, whereas the effe

Published
2011

6. Functional and genetic epidemiological characterisation of the FFAR4 (GPR120) p.R270H variant in the Danish population.

Author

Vestmar, Marie A., Andersson, Ehm A., Christensen, Charlotte R., Hauge, Maria, Glümer, Charlotte, Linneberg, Allan, Witte, Daniel R., Jørgensen, Marit E., Christensen, Cramer, Brandslund, Ivan, Lauritzen, Torsten, Pedersen, Oluf, Holst, Birgitte, Grarup, Niels, Schwartz, Thue W., and Hansen, Torben

Abstract

Background p.R270H (rs116454156) in the long chain fatty acid 7TM receptor FFAR4 (GPR120) which results in impaired Gαq (Gq) coupled signalling, has been associated with obesity. We aimed to extend the functional in vitro analyses of p.R270H and to investigate the association with obesity and glucose- related traits in the Danish population. Methods Surface expression, Gq and Gi coupled signalling as well as β-arrestin recruitment were examined in vitro. p.R270H was genotyped using the exome chip array in 11 479 Danish adult individuals. Of these 4391 were obese and 4415 were normal weight. Association with quantitative metabolic traits comprised 8720 non-diabetic individuals. Results p.R270H showed reduced surface expression of FFAR4. Ligand-independent activity was eliminated and strongly impaired through the Gq and Gi signalling pathways, respectively. The ligand-induced maximal signalling efficacy of p.R270H was reduced only through the Gq pathway. The p.R270H variant did not affect β-arrestin recruitment. p.R270H was not associated with increased risk of obesity nor increased fasting plasma glucose levels in the Danish study populations. Nor was it associated with these two traits in the European Network for Genetic and Genomic Epidemiology consortium data (N=34 901-71 175; p>0.70). It was also not associated with waist-hip ratio, glucose metabolism during an oral glucose tolerance test, lipid levels or with markers of adiposity (leptin, adiponectin), inflammation (high-sensitive C reactive protein; hs-CRP) and liver function (alanine aminotransferase) in the Danish population (p>0.05). Conclusions We demonstrate that p.R270H of FFAR4 impairs Gq and Gi signalling of FFAR4 in vitro; however, this impaired signalling for p.R270H does not translate into associations with human metabolic phenotypes in the investigated populations. [ABSTRACT FROM AUTHOR]

Published
2016
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8. Studies of Metabolic Phenotypic Correlates of 15 Obesity Associated Gene Variants

Author

Sandholt, Camilla Helene, primary, Vestmar, Marie Aare, additional, Bille, Dorthe Sadowa, additional, Borglykke, Anders, additional, Almind, Katrine, additional, Hansen, Lars, additional, Sandbæk, Annelli, additional, Lauritzen, Torsten, additional, Witte, Daniel, additional, Jørgensen, Torben, additional, Pedersen, Oluf, additional, and Hansen, Torben, additional

Published
2011
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9. GPR40 (FFAR1) - Combined Gs and Gq signaling in vitro is associated with robust incretin secretagogue action ex vivo and in vivo.

Author

Hauge M, Vestmar MA, Husted AS, Ekberg JP, Wright MJ, Di Salvo J, Weinglass AB, Engelstoft MS, Madsen AN, Lückmann M, Miller MW, Trujillo ME, Frimurer TM, Holst B, Howard AD, and Schwartz TW

Abstract

Objectives: GPR40 (FFAR1), a clinically proven anti-diabetes target, is a Gq-coupled receptor for long chain fatty acids (LCFA) stimulating insulin secretion directly and mediating a major part of the dietary triglyceride-induced secretion of the incretins GLP-1 and GIP. In phase-II studies the GPR40 agonist TAK-875 decreased blood glucose but surprisingly without stimulating incretins., Methods and Results: Here we find that GPR40 can signal through not only Gq and IP3 but also Gs and cAMP when stimulated with certain agonists such as AM-1638 and AM-5262 in contrast to the endogenous LCFA ligands and agonists such as TAK-875 and AM-837, which only signal through Gq. In competition binding against [3H]AM-1638 and [3H]L358 the Gq + Gs and the Gq-only agonists either competed for or showed positive cooperativity by increasing the binding of the two different radio-ligands, in opposite ways. Nevertheless, both the Gq-only and the Gq + Gs agonists all docked surprisingly well into the binding site for TAK-875 in the X-ray structure of GPR40. In murine intestinal primary cell-cultures the endogenous LCFAs and the Gq-only agonists stimulated GLP-1 secretion with rather poor efficacy as compared with the high efficacy Gq + Gs GPR40 agonists and a prototype GPR119 agonist. Similarly, in fasting both male and female mice the Gq + Gs agonists showed significantly higher efficacy than the Gq-only agonists in respect of increasing plasma GLP-1 and plasma GIP in a GPR40-dependent manner., Conclusions: It is concluded that stimulation of GPR40 by endogenous LCFAs or by Gq-only synthetic agonists result in a rather limited incretin response, whereas Gq + Gs GPR40 agonists stimulate incretin secretion robustly.

Published
2014
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