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9 results on '"Pietilainen, K. H."'

2. Eating styles, overweight and obesity in young adult twins

Author

Keski-Rahkonen, A, Bulik, C M., Pietilainen, K H., Rose, R J., Kaprio, J, and Rissanen, A

Abstract

Author(s): A Keski-Rahkonen [1, 2, 3]; C M Bulik [4]; K H Pietiläinen [2, 3]; R J Rose [5]; J Kaprio [2, 6]; A Rissanen [3] Introduction Various theoretical approaches [...]

Published
2007
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3. Differences in genetic and environmental variation in adult BMI by sex, age, time period, and region : An individual-based pooled analysis of 40 twin cohorts

Author

Silventoinen, K., Jelenkovic, A., Sund, R., Yokoyama, Y., Hur, Y. -M, Cozen, W., Hwang, A. E., Mack, T. M., Honda, C., Inui, F., Iwatani, Y., Watanabe, M., Tomizawa, R., Pietilainen, K. H., Rissanen, A., Siribaddana, S. H., Hotopf, M., Sumathipala, A., Rijsdijk, F., Tan, Q., Zhang, D., Pang, Z., Piirtola, M., Aaltonen, S., Oncel, S. Y., Aliev, F., Rebato, E., Hjelmborg, J. B., Christensen, K., Skytthe, A., Kyvik, K. O., Silberg, J. L., Eaves, L. J., Cutler, T. L., Ordonana, J. R., Sanchez-Romera, J. F., Colodro-Conde, L., Song, Y. -M, Yang, S., Lee, K., Franz, C. E., Kremen, W. S., Lyons, M. J., Busjahn, A., Nelson, T. L., Whitfield, K. E., Kandler, C., Jang, K. L., Gatz, M., Butler, D. A., Stazi, M. A., Fagnani, C., D'Ippolito, C., Duncan, G. E., Buchwald, D., Martin, N. G., Medland, S. E., Montgomery, G. W., Jeong, H. -U, Swan, G. E., Krasnow, R., Magnusson, P. K. E., Pedersen, N. L., Dahl Aslan, Anna K., McAdams, T. A., Eley, T. C., Gregory, A. M., Tynelius, P., Baker, L. A., Tuvblad, C., Bayasgalan, G., Narandalai, D., Spector, T. D., Mangino, M., Lachance, G., Burt, S. A., Klump, K. L., Harris, J. R., Brandt, I., Nilsen, T. S., Krueger, R. F., McGue, M., Pahlen, S., Corley, R. P., Huibregtse, B. M., Bartels, M., Van Beijsterveldt, C. E. M., Willemsen, G., Goldberg, J. H., Rasmussen, F., Tarnoki, A. D., Tarnoki, D. L., Derom, C. A., Vlietinck, R. F., Loos, R. J. F., Hopper, J. L., Sung, J., Maes, H. H., Turkheimer, E., Boomsma, D. I., Sørensen, T. I. A., Kaprio, J., Silventoinen, K., Jelenkovic, A., Sund, R., Yokoyama, Y., Hur, Y. -M, Cozen, W., Hwang, A. E., Mack, T. M., Honda, C., Inui, F., Iwatani, Y., Watanabe, M., Tomizawa, R., Pietilainen, K. H., Rissanen, A., Siribaddana, S. H., Hotopf, M., Sumathipala, A., Rijsdijk, F., Tan, Q., Zhang, D., Pang, Z., Piirtola, M., Aaltonen, S., Oncel, S. Y., Aliev, F., Rebato, E., Hjelmborg, J. B., Christensen, K., Skytthe, A., Kyvik, K. O., Silberg, J. L., Eaves, L. J., Cutler, T. L., Ordonana, J. R., Sanchez-Romera, J. F., Colodro-Conde, L., Song, Y. -M, Yang, S., Lee, K., Franz, C. E., Kremen, W. S., Lyons, M. J., Busjahn, A., Nelson, T. L., Whitfield, K. E., Kandler, C., Jang, K. L., Gatz, M., Butler, D. A., Stazi, M. A., Fagnani, C., D'Ippolito, C., Duncan, G. E., Buchwald, D., Martin, N. G., Medland, S. E., Montgomery, G. W., Jeong, H. -U, Swan, G. E., Krasnow, R., Magnusson, P. K. E., Pedersen, N. L., Dahl Aslan, Anna K., McAdams, T. A., Eley, T. C., Gregory, A. M., Tynelius, P., Baker, L. A., Tuvblad, C., Bayasgalan, G., Narandalai, D., Spector, T. D., Mangino, M., Lachance, G., Burt, S. A., Klump, K. L., Harris, J. R., Brandt, I., Nilsen, T. S., Krueger, R. F., McGue, M., Pahlen, S., Corley, R. P., Huibregtse, B. M., Bartels, M., Van Beijsterveldt, C. E. M., Willemsen, G., Goldberg, J. H., Rasmussen, F., Tarnoki, A. D., Tarnoki, D. L., Derom, C. A., Vlietinck, R. F., Loos, R. J. F., Hopper, J. L., Sung, J., Maes, H. H., Turkheimer, E., Boomsma, D. I., Sørensen, T. I. A., and Kaprio, J.

Abstract

Background: Genes and the environment contribute to variation in adult body mass index [BMI (in kg/m2)], but factors modifying these variance components are poorly understood. Objective: We analyzed genetic and environmental variation in BMI between men and women from young adulthood to old age from the 1940s to the 2000s and between cultural-geographic regions representing high (North America and Australia), moderate (Europe), and low (East Asia) prevalence of obesity. Design: We used genetic structural equation modeling to analyze BMI in twins ≥20 y of age from 40 cohorts representing 20 countries (140,379 complete twin pairs). Results: The heritability of BMI decreased from 0.77 (95% CI: 0.77, 0.78) and 0.75 (95% CI: 0.74, 0.75) in men and women 20-29 y of age to 0.57 (95% CI: 0.54, 0.60) and 0.59 (95% CI: 0.53, 0.65) in men 70-79 y of age and women 80 y of age, respectively. The relative influence of unique environmental factors correspondingly increased. Differences in the sets of genes affecting BMI in men and women increased from 20-29 to 60-69 y of age. Mean BMI and variances in BMI increased from the 1940s to the 2000s and were greatest in North America and Australia, followed by Europe and East Asia. However, heritability estimates were largely similar over measurement years and between regions. There was no evidence of environmental factors shared by co-twins affecting BMI. Conclusions: The heritability of BMI decreased and differences in the sets of genes affecting BMI in men and women increased from young adulthood to old age. The heritability of BMI was largely similar between cultural-geographic regions and measurement years, despite large differences in mean BMI and variances in BMI. Our results show a strong influence of genetic factors on BMI, especially in early adulthood, regardless of the obesity level in the population.

Published
2017
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4. Acquired liver fat is a key determinant of serum lipid alterations in healthy monozygotic twins

Author

Kaye, S. M., Maranghi, Marianna, Bogl, L. H., Kaprio, J., Hakkarainen, A., Lundbom, J., Lundbom, N., Rissanen, A., Taskinen, M. R., and Pietilainen, K. H.

Subjects
Adult, Male, Cholesterol, HDL, Abdominal Fat, Subcutaneous Fat, Cholesterol, LDL, Twins, Monozygotic, Obesity: liver fat, Body Mass Index, lipids, Fatty Liver, Young Adult, Cholesterol, Liver, Multivariate Analysis, Humans, Female, Obesity, Exercise, Finland, Apolipoproteins B
Abstract

The effects of acquired obesity on lipid profile and lipoprotein composition in rare BMI-discordant monozygotic (MZ) twin pairs were studied.Abdominal fat distribution, liver fat (magnetic resonance imaging and spectroscopy), fasting serum lipid profile (ultracentrifugation, gradient gel-electrophoresis, and colorimetric enzymatic methods), and lifestyle factors (questionnaires and diaries) were assessed in 15 BMI-discordant (within-pair difference [Δ] in BMI3 kg/m2) and nin concordant (ΔBMI3 kg/m2) MZ twin pairs, identified from two nationwide cohorts of Finnish twins.Despite a strong similarity of MZ twins in lipid parameters (intra-class correlations 0.42-0.90, P0.05), concentrations of apolipoprotein B (ApoB), intermediate-density lipoprotein cholesterol, low-density lipoprotein cholesterol (LDL-C), high-density lipoprotein 3a% (HDL3a%), and HDL3c% were higher (P0.05) and those of HDL cholesterol, HDL2-C, and HDL2b% were lower (P0.01) in the heavier co-twins of BMI-discordant pairs. The composition of lipoprotein particles was similar in the co-twins. When BMI-discordant pairs were further divided into liver fat-discordant and concordant (based on median for Δliver fat, 2.6%), the adverse lipid profile was only seen in those heavy co-twins who also had high liver fat. Conversely, BMI-discordant pairs concordant for liver fat did not differ significantly in lipid parameters. In multivariate analyses controlling for Δsubcutaneous, Δintra-abdominal fat, sex, Δsmoking and Δphysical activity, Δliver fat was the only independent variable explaining the variation in ΔApoB, Δtotal cholesterol, and ΔLDL-C concentration.Several pro-atherogenic changes in the amounts of lipids but not in the composition of lipoprotein particles were observed in acquired obesity. In particular, accumulation of liver fat was associated with lipid disturbances, independent of genetic effects.

Published
2012

5. Telomere length in circulating leukocytes is associated with lung function and disease

Author

Albrecht, E., primary, Sillanpaa, E., additional, Karrasch, S., additional, Alves, A. C., additional, Codd, V., additional, Hovatta, I., additional, Buxton, J. L., additional, Nelson, C. P., additional, Broer, L., additional, Hagg, S., additional, Mangino, M., additional, Willemsen, G., additional, Surakka, I., additional, Ferreira, M. A. R., additional, Amin, N., additional, Oostra, B. A., additional, Backmand, H. M., additional, Peltonen, M., additional, Sarna, S., additional, Rantanen, T., additional, Sipila, S., additional, Korhonen, T., additional, Madden, P. A. F., additional, Gieger, C., additional, Jorres, R. A., additional, Heinrich, J., additional, Behr, J., additional, Huber, R. M., additional, Peters, A., additional, Strauch, K., additional, Wichmann, H. E., additional, Waldenberger, M., additional, Blakemore, A. I. F., additional, de Geus, E. J. C., additional, Nyholt, D. R., additional, Henders, A. K., additional, Piirila, P. L., additional, Rissanen, A., additional, Magnusson, P. K. E., additional, Vinuela, A., additional, Pietilainen, K. H., additional, Martin, N. G., additional, Pedersen, N. L., additional, Boomsma, D. I., additional, Spector, T. D., additional, van Duijn, C. M., additional, Kaprio, J., additional, Samani, N. J., additional, Jarvelin, M.-R., additional, and Schulz, H., additional

Published
2013
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9. The mitochondrial protein Opa1 promotes adipocyte browning that is dependent on urea cycle metabolites

Author

Camilla Bean, Matteo Audano, Tatiana Varanita, Francesca Favaretto, Marta Medaglia, Marco Gerdol, Lena Pernas, Fabio Stasi, Marta Giacomello, Stèphanie Herkenne, Maheswary Muniandy, Sini Heinonen, Emma Cazaly, Miina Ollikainen, Gabriella Milan, Alberto Pallavicini, Kirsi H. Pietiläinen, Roberto Vettor, Nico Mitro, Luca Scorrano, Bean, C., Audano, M., Varanita, T., Favaretto, F., Medaglia, M., Gerdol, M., Pernas, L., Stasi, F., Giacomello, M., Herkenne, S., Muniandy, M., Heinonen, S., Cazaly, E., Ollikainen, M., Milan, G., Pallavicini, A., Pietilainen, K. H., Vettor, R., Mitro, N., and Scorrano, L.

Subjects
Jumonji Domain-Containing Histone Demethylases, Endocrinology, Diabetes and Metabolism, Adipocytes, White, Mice, Transgenic, White, Diet, High-Fat, Transgenic, GTP Phosphohydrolases, GTP Phosphohydrolase, Mitochondrial Proteins, Mice, Physiology (medical), Internal Medicine, Adipocytes, Mitochondrial Protein, Animals, Humans, Urea, Adipocytes, Beige, Obesity, Cyclic AMP Response Element-Binding Protein, Uncoupling Protein 1, Adipocytes, Brown, Adipose Tissue, Gene Expression Regulation, Mitochondria, Thermogenesis, Metabolic Networks and Pathways, Animal, Beige, Thermogenesi, Jumonji Domain-Containing Histone Demethylase, Brown, Cell Biology, Diet, High-Fat, Human
Abstract

White to brown/beige adipocytes conversion is a possible therapeutic strategy to tackle the current obesity epidemics. While mitochondria are key for energy dissipation in brown fat, it is unknown if they can drive adipocyte browning. Here, we show that the mitochondrial cristae biogenesis protein optic atrophy 1 (Opa1) facilitates cell-autonomous adipocyte browning. In two cohorts of patients with obesity, including weight discordant monozygotic twin pairs, adipose tissue OPA1 levels are reduced. In the mouse, Opa1 overexpression favours white adipose tissue expandability as well as browning, ultimately improving glucose tolerance and insulin sensitivity. Transcriptomics and metabolomics analyses identify the Jumanji family chromatin remodelling protein Kdm3a and urea cycle metabolites, including fumarate, as effectors of Opa1-dependent browning. Mechanistically, the higher cyclic adenosine monophosphate (cAMP) levels in Opa1 pre-adipocytes activate cAMP-responsive element binding protein (CREB), which transcribes urea cycle enzymes. Flux analyses in pre-adipocytes indicate that Opa1-dependent fumarate accumulation depends on the urea cycle. Conversely, adipocyte-specific Opa1 deletion curtails urea cycle and beige differentiation of pre-adipocytes, and is rescued by fumarate supplementation. Thus, the urea cycle links the mitochondrial dynamics protein Opa1 to white adipocyte browning.

Published
2021

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