Your search keyword '"Lehtimäki, T"' showing total 187 results

1. Evolution of genetic networks for human creativity

Author

Zwir, I., Del-Val, C., Hintsanen, M., Cloninger, K. M., Romero-Zaliz, R., Mesa, A., Arnedo, J., Salas, R., Poblete, G. F., Raitoharju, E., Raitakari, O., Keltikangas-Järvinen, L., de Erausquin, G. A., Tattersall, I., Lehtimäki, T., and Cloninger, C. R.

Published

2022

2. Regulation of NC886 RNAs is associated with cardiometabolic risk factors, death and stroke

Author

Rajić, S., primary, Marttila, S., additional, Hutri-Kähönen, N., additional, Kähönen, M., additional, Lehtimäki, T., additional, Lyytikäinen, L.-P., additional, Mishra, P., additional, Mononen, N., additional, Raitakari, O., additional, Waldenberger, M., additional, Delerue, T., additional, März, W., additional, Kleber, M., additional, Harville, E., additional, Zhang, R., additional, and Raitoharju, E., additional

Published

2023

3. Identification of blood modular genome-wide gene expression biomarkers of cardiovascular health and depression in the young finns study

Author

Mishra, B., primary, Raitoharju, E., additional, Mononen, N., additional, Viikari, J., additional, Juonala, M., additional, Hutri-Kähönen, N., additional, Kähönen, M., additional, Raitakari, O., additional, Lehtimäki, T., additional, and Mishra, P., additional

Published

2023

4. Differentially methylated DNA loci between Eastern and Western Finns associate with CHD risk factors

Author

Ciantar, J., primary, Marttila, S., additional, Rajić, S., additional, Mishra, P., additional, Lehtimäki, T., additional, Raitakari, O., additional, and Raitoharju, E., additional

Published

2023

5. Genetic risk score for human serum lipidome and its association with angiographic coronary artery disease

Author

Mishra, P., primary, Mishra, B., additional, Kleber, M., additional, Delgado, G., additional, März, W., additional, and Lehtimäki, T., additional

Published

2023

6. Genetic insights into resting heart rate and its role in cardiovascular disease.

Author

Vegte, Y.J. van de, Eppinga, R.N., Ende, M.Y. van der, Hagemeijer, Y.P., Mahendran, Y., Salfati, E., Smith, A.V., Tan, V.Y., Arking, D.E., Ntalla, I., Appel, E.V., Schurmann, C., Brody, J.A., Rueedi, R., Polasek, O., Sveinbjornsson, G., Lecoeur, C., Ladenvall, C., Zhao, J.H., Isaacs, A., Wang, L., Luan, Jian'an, Hwang, S.J., Mononen, N., Auro, K., Jackson, A.U., Bielak, L.F., Zeng, L., Shah, N., Nethander, M., Campbell, A., Rankinen, T., Pechlivanis, S., Qi, L., Zhao, Wei, Rizzi, F., Tanaka, T., Robino, A., Cocca, M., Lange, L., Müller-Nurasyid, M., Roselli, C., Zhang, W, Kleber, M.E., Guo, X., Lin, H.J., Pavani, F., Galesloot, T.E., Noordam, R., Milaneschi, Y., Schraut, K.E., Hoed, M. den, Degenhardt, F., Trompet, S., Berg, M.E. van den, Pistis, G., Tham, Y.C., Weiss, S., Sim, X.S., Li, H.L., Most, P.J. van der, Nolte, I.M., Lyytikäinen, L.P., Said, M.A., Witte, D.R., Iribarren, C., Launer, L., Ring, S.M., Vries, P.S. de, Sever, P., Linneberg, A., Bottinger, E.P., Padmanabhan, S., Psaty, B.M., Sotoodehnia, N., Kolcic, I., Arnar, D.O., Gudbjartsson, D.F., Holm, H., Balkau, B., Silva, C.T., Newton-Cheh, C.H., Nikus, K., Salo, P., Mohlke, K.L., Peyser, P.A., Schunkert, H., Lorentzon, M., Lahti, J., Rao, D.C., Cornelis, M.C., Faul, J.D., Smith, J.A., Stolarz-Skrzypek, K., Bandinelli, S., Concas, M.P., Sinagra, G., Meitinger, T., Waldenberger, M., Sinner, M.F., Strauch, K., Delgado, G.E., Taylor, K.D., Yao, J., Foco, L., Melander, O., Graaf, J. de, Mutsert, R. de, Geus, E.J.C. de, Johansson, Å., Joshi, P.K., Lind, L., Franke, A., Macfarlane, P.W., Tarasov, K.V., Tan, N., Felix, S.B., Tai, E.S., Quek, D.Q., Snieder, H., Ormel, J., Ingelsson, M., Lindgren, C., Morris, A.P., Raitakari, O.T., Hansen, T., Assimes, T., Gudnason, V., Timpson, N.J., Morrison, A.C., Munroe, P.B., Strachan, D.P., Grarup, N., Loos, R.J.F., Heckbert, S.R., Vollenweider, P., Hayward, C., Stefansson, K., Froguel, P., Groop, L., Wareham, N.J., Duijn, C.M. van, Feitosa, M.F., O'Donnell, C.J., Kähönen, M., Perola, M., Boehnke, M., Kardia, S.L.R., Erdmann, J., Palmer, C.N.A., Ohlsson, C., Porteous, D.J., Eriksson, J.G., Bouchard, C., Moebus, S., Kraft, P., Weir, D.R., Cusi, D., Ferrucci, L., Ulivi, S., Girotto, G., Correa, A., Kääb, S., Peters, A., Chambers, J.C., Kooner, J.S., März, W., Rotter, J.I., Hicks, A.A., Smith, J.G., Kiemeney, L.A.L.M., Mook-Kanamori, D.O., Penninx, B.W.J.H., Gyllensten, U., Wilson, J.F., Burgess, S., Sundström, J., Lieb, W., Jukema, J.W., Eijgelsheim, M., Lakatta, E.L.M., Cheng, C.Y., Dörr, M., Wong, T.Y., Sabanayagam, C., Oldehinkel, A.J., Riese, H., Lehtimäki, T., Verweij, N., Harst, P. van der, Vegte, Y.J. van de, Eppinga, R.N., Ende, M.Y. van der, Hagemeijer, Y.P., Mahendran, Y., Salfati, E., Smith, A.V., Tan, V.Y., Arking, D.E., Ntalla, I., Appel, E.V., Schurmann, C., Brody, J.A., Rueedi, R., Polasek, O., Sveinbjornsson, G., Lecoeur, C., Ladenvall, C., Zhao, J.H., Isaacs, A., Wang, L., Luan, Jian'an, Hwang, S.J., Mononen, N., Auro, K., Jackson, A.U., Bielak, L.F., Zeng, L., Shah, N., Nethander, M., Campbell, A., Rankinen, T., Pechlivanis, S., Qi, L., Zhao, Wei, Rizzi, F., Tanaka, T., Robino, A., Cocca, M., Lange, L., Müller-Nurasyid, M., Roselli, C., Zhang, W, Kleber, M.E., Guo, X., Lin, H.J., Pavani, F., Galesloot, T.E., Noordam, R., Milaneschi, Y., Schraut, K.E., Hoed, M. den, Degenhardt, F., Trompet, S., Berg, M.E. van den, Pistis, G., Tham, Y.C., Weiss, S., Sim, X.S., Li, H.L., Most, P.J. van der, Nolte, I.M., Lyytikäinen, L.P., Said, M.A., Witte, D.R., Iribarren, C., Launer, L., Ring, S.M., Vries, P.S. de, Sever, P., Linneberg, A., Bottinger, E.P., Padmanabhan, S., Psaty, B.M., Sotoodehnia, N., Kolcic, I., Arnar, D.O., Gudbjartsson, D.F., Holm, H., Balkau, B., Silva, C.T., Newton-Cheh, C.H., Nikus, K., Salo, P., Mohlke, K.L., Peyser, P.A., Schunkert, H., Lorentzon, M., Lahti, J., Rao, D.C., Cornelis, M.C., Faul, J.D., Smith, J.A., Stolarz-Skrzypek, K., Bandinelli, S., Concas, M.P., Sinagra, G., Meitinger, T., Waldenberger, M., Sinner, M.F., Strauch, K., Delgado, G.E., Taylor, K.D., Yao, J., Foco, L., Melander, O., Graaf, J. de, Mutsert, R. de, Geus, E.J.C. de, Johansson, Å., Joshi, P.K., Lind, L., Franke, A., Macfarlane, P.W., Tarasov, K.V., Tan, N., Felix, S.B., Tai, E.S., Quek, D.Q., Snieder, H., Ormel, J., Ingelsson, M., Lindgren, C., Morris, A.P., Raitakari, O.T., Hansen, T., Assimes, T., Gudnason, V., Timpson, N.J., Morrison, A.C., Munroe, P.B., Strachan, D.P., Grarup, N., Loos, R.J.F., Heckbert, S.R., Vollenweider, P., Hayward, C., Stefansson, K., Froguel, P., Groop, L., Wareham, N.J., Duijn, C.M. van, Feitosa, M.F., O'Donnell, C.J., Kähönen, M., Perola, M., Boehnke, M., Kardia, S.L.R., Erdmann, J., Palmer, C.N.A., Ohlsson, C., Porteous, D.J., Eriksson, J.G., Bouchard, C., Moebus, S., Kraft, P., Weir, D.R., Cusi, D., Ferrucci, L., Ulivi, S., Girotto, G., Correa, A., Kääb, S., Peters, A., Chambers, J.C., Kooner, J.S., März, W., Rotter, J.I., Hicks, A.A., Smith, J.G., Kiemeney, L.A.L.M., Mook-Kanamori, D.O., Penninx, B.W.J.H., Gyllensten, U., Wilson, J.F., Burgess, S., Sundström, J., Lieb, W., Jukema, J.W., Eijgelsheim, M., Lakatta, E.L.M., Cheng, C.Y., Dörr, M., Wong, T.Y., Sabanayagam, C., Oldehinkel, A.J., Riese, H., Lehtimäki, T., Verweij, N., and Harst, P. van der

Abstract

Contains fulltext : 296013.pdf (Publisher’s version ) (Open Access), Resting heart rate is associated with cardiovascular diseases and mortality in observational and Mendelian randomization studies. The aims of this study are to extend the number of resting heart rate associated genetic variants and to obtain further insights in resting heart rate biology and its clinical consequences. A genome-wide meta-analysis of 100 studies in up to 835,465 individuals reveals 493 independent genetic variants in 352 loci, including 68 genetic variants outside previously identified resting heart rate associated loci. We prioritize 670 genes and in silico annotations point to their enrichment in cardiomyocytes and provide insights in their ECG signature. Two-sample Mendelian randomization analyses indicate that higher genetically predicted resting heart rate increases risk of dilated cardiomyopathy, but decreases risk of developing atrial fibrillation, ischemic stroke, and cardio-embolic stroke. We do not find evidence for a linear or non-linear genetic association between resting heart rate and all-cause mortality in contrast to our previous Mendelian randomization study. Systematic alteration of key differences between the current and previous Mendelian randomization study indicates that the most likely cause of the discrepancy between these studies arises from false positive findings in previous one-sample MR analyses caused by weak-instrument bias at lower P-value thresholds. The results extend our understanding of resting heart rate biology and give additional insights in its role in cardiovascular disease development.

Published

2023

7. Changing the market for a sustainable innovation

Author

Keränen, O. (Outi), Lehtimäki, T. (Tuula), Komulainen, H. (Hanna), Ulkuniemi, P. (Pauliina), Keränen, O. (Outi), Lehtimäki, T. (Tuula), Komulainen, H. (Hanna), and Ulkuniemi, P. (Pauliina)

Abstract

The development and diffusion of sustainable innovations are of interest to various public and private sector actors. The diffusion of sustainable innovations into value networks facilitates and is facilitated by the change of markets towards sustainability; however, this interaction needs further investigation. We examine how combinations of value network actors’ intentions and activities affect market change for a sustainable innovation We empirically explore market change related to introducing bioplastics into plastic food packaging value networks. We increase the understanding of market change for a sustainable innovation by showing how not only the actors with direct intentions to support the innovation but actors and activities indirectly related to the sustainable innovation contribute to market change. Such indirectly supportive activities focus on broader sustainability aims and can, for example, change market representations, practices, and norms in favor of the sustainable innovation. We propose sustainability layers to understand the diverse sustainability focuses of actors and their relation to the market change in question. Specifically, we contribute to market change literature by broadening the examination scope beyond the most active actors driving market change for an innovation.

Published

2023

8. The interplay between inflammatory cytokines and cardiometabolic disease: bi-directional mendelian randomisation study

Author

Karhunen, V. (Ville), Gill, D. (Dipender), Huang, J. (Jian), Bouras, E. (Emmanouil), Malik, R. (Rainer), Ponsford, M. J. (Mark J.), Ahola-Olli, A. (Ari), Papadopoulou, A. (Areti), Palaniswamy, S. (Saranya), Sebert, S. (Sylvain), Wielscher, M. (Matthias), Auvinen, J. (Juha), Veijola, J. (Juha), Herzig, K.-H. (Karl-Heinz), Timonen, M. (Markku), Keinänen-Kiukaanniemi, S. (Sirkka), Dichgans, M. (Martin), Salmi, M. (Marko), Jalkanen, S. (Sirpa), Lehtimäki, T. (Terho), Salomaa, V. (Veikko), Raitakari, O. (Olli), Jones, S. A. (Simon A.), Hovingh, G. K. (G. Kees), Tsilidis, K. K. (Konstantinos K.), Järvelin, M.-R. (Marjo-Riitta), Dehghan, A. (Abbas), Karhunen, V. (Ville), Gill, D. (Dipender), Huang, J. (Jian), Bouras, E. (Emmanouil), Malik, R. (Rainer), Ponsford, M. J. (Mark J.), Ahola-Olli, A. (Ari), Papadopoulou, A. (Areti), Palaniswamy, S. (Saranya), Sebert, S. (Sylvain), Wielscher, M. (Matthias), Auvinen, J. (Juha), Veijola, J. (Juha), Herzig, K.-H. (Karl-Heinz), Timonen, M. (Markku), Keinänen-Kiukaanniemi, S. (Sirkka), Dichgans, M. (Martin), Salmi, M. (Marko), Jalkanen, S. (Sirpa), Lehtimäki, T. (Terho), Salomaa, V. (Veikko), Raitakari, O. (Olli), Jones, S. A. (Simon A.), Hovingh, G. K. (G. Kees), Tsilidis, K. K. (Konstantinos K.), Järvelin, M.-R. (Marjo-Riitta), and Dehghan, A. (Abbas)

Abstract

Objective: To leverage large scale genetic association data to investigate the interplay between circulating cytokines and cardiometabolic traits, and thus identifying potential therapeutic targets. Design: Bi-directional Mendelian randomisation study. Setting: Genome-wide association studies from three Finnish cohorts (Northern Finland Birth Cohort 1966, Young Finns Study, or FINRISK study), and genetic association summary statistics pooled from observational studies for expression quantitative trait loci and cardiometabolic traits. Participants: Data for 47 circulating cytokines in 13 365 individuals from genome-wide association studies, summary statistic data for up to 21 735 individuals on circulating cytokines, summary statistic gene expression data across 49 tissues in 838 individuals, and summary statistic data for up to 1 320 016 individuals on cardiometabolic traits. Interventions: Relations between circulating cytokines and cardiovascular, anthropometric, lipid, or glycaemic traits (coronary artery disease, stroke, type 2 diabetes mellitus, body mass index, waist circumference, waist to hip ratio, systolic blood pressure, glycated haemoglobin, high density lipoprotein cholesterol, low density lipoprotein cholesterol, total cholesterol, triglycerides, C reactive protein, glucose, fasting insulin, and lifetime smoking). Main outcome methods: Genetic instrumental variables that are biologically plausible for the circulating cytokines were generated. The effects of cardiometabolic risk factors on concentrations of circulating cytokines, circulating cytokines on other circulating cytokines, and circulating cytokines on cardiometabolic outcomes were investigated. Results: Genetic evidence (mendelian randomisation P<0.0011) suggests that higher body mass index, waist circumference, smoking, higher concentrations of lipids, and systolic blood pressure increase circulating concentrations of several inflammatory cytokines and C reactive protein. Evidence

Published

2023

9. The relationship of trait-like compassion with epigenetic aging:the population-based prospective Young Finns Study

Author

Dobewall, H. (Henrik), Keltikangas-Järvinen, L. (Liisa), Marttila, S. (Saara), Mishra, P. P. (Pashupati P.), Saarinen, A. (Aino), Cloninger, C. R. (C. Robert), Zwir, I. (Igor), Kähönen, M. (Mika), Hurme, M. (Mikko), Raitakari, O. (Olli), Lehtimäki, T. (Terho), Hintsanen, M. (Mirka), Dobewall, H. (Henrik), Keltikangas-Järvinen, L. (Liisa), Marttila, S. (Saara), Mishra, P. P. (Pashupati P.), Saarinen, A. (Aino), Cloninger, C. R. (C. Robert), Zwir, I. (Igor), Kähönen, M. (Mika), Hurme, M. (Mikko), Raitakari, O. (Olli), Lehtimäki, T. (Terho), and Hintsanen, M. (Mirka)

Abstract

Introduction: Helping others within and beyond the family has been related to living a healthy and long life. Compassion is a prosocial personality trait characterized by concern for another person who is suffering and the motivation to help. The current study examines whether epigenetic aging is a potential biological mechanism that explains the link between prosociality and longevity. Methods: We used data from the Young Finns Study that follows six birth-cohorts from age 3–18 to 19–49. Trait-like compassion for others was measured with the Temperament and Character Inventory in the years 1997 and 2001. Epigenetic age acceleration and telomere length were measured with five DNA methylation (DNAm) indicators (DNAmAgeHorvath, IEAA_Hannum, EEAA_Hannum, DNAmPhenoAge, and DNAmTL) based on blood drawn in 2011. We controlled for sex, socioeconomic status in childhood and adulthood, and body-mass index. Results and discussion: An association between higher compassion in 1997 and a less accelerated DNAmPhenoAge, which builds on previous work on phenotypic aging, approached statistical significance in a sex-adjusted model (n = 1,030; b = −0.34; p = 0.050). Compassion in 1997 predicted less accelerated epigenetic aging over and above the control variables (n = 843; b = −0.47; p = 0.016). There was no relationship between compassion in 2001 (n = 1108/910) and any of the other four studied epigenetic aging indicators. High compassion for others might indeed influence whether an individual’s biological age is lower than their chronological age. The conducted robustness checks partially support this conclusion, yet cannot rule out that there might be a broader prosocial trait behind the findings. The observed associations are interesting but should be interpreted as weak requiring replication.

Published

2023

10. Longitudinal metabolomics of increasing body-mass index and waist-hip ratio reveals two dynamic patterns of obesity pandemic

Author

Mäkinen, V.-P. (Ville-Petteri), Kettunen, J. (Johannes), Lehtimäki, T. (Terho), Kähönen, M. (Mika), Viikari, J. (Jorma), Perola, M. (Markus), Salomaa, V. (Veikko), Järvelin, M.-R. (Marjo-Riitta), Raitakari, O. T. (Olli T.), Ala-Korpela, M. (Mika), Mäkinen, V.-P. (Ville-Petteri), Kettunen, J. (Johannes), Lehtimäki, T. (Terho), Kähönen, M. (Mika), Viikari, J. (Jorma), Perola, M. (Markus), Salomaa, V. (Veikko), Järvelin, M.-R. (Marjo-Riitta), Raitakari, O. T. (Olli T.), and Ala-Korpela, M. (Mika)

Abstract

Background/Objectives: This observational study dissects the complex temporal associations between body-mass index (BMI), waist-hip ratio (WHR) and circulating metabolomics using a combination of longitudinal and cross-sectional population-based datasets and new systems epidemiology tools. Subjects/Methods: Firstly, a data-driven subgrouping algorithm was employed to simplify high-dimensional metabolic profiling data into a single categorical variable: a self-organizing map (SOM) was created from 174 metabolic measures from cross-sectional surveys (FINRISK, n = 9708, ages 25–74) and a birth cohort (NFBC1966, n = 3117, age 31 at baseline, age 46 at follow-up) and an expert committee defined four subgroups of individuals based on visual inspection of the SOM. Secondly, the subgroups were compared regarding BMI and WHR trajectories in an independent longitudinal dataset: participants of the Young Finns Study (YFS, n = 1286, ages 24–39 at baseline, 10 years follow-up, three visits) were categorized into the four subgroups and subgroup-specific age-dependent trajectories of BMI, WHR and metabolic measures were modelled by linear regression. Results: The four subgroups were characterised at age 39 by high BMI, WHR and dyslipidemia (designated TG-rich); low BMI, WHR and favourable lipids (TG-poor); low lipids in general (Low lipid) and high low-density-lipoprotein cholesterol (High LDL-C). Trajectory modelling of the YFS dataset revealed a dynamic BMI divergence pattern: despite overlapping starting points at age 24, the subgroups diverged in BMI, fasting insulin (three-fold difference at age 49 between TG-rich and TG-poor) and insulin-associated measures such as triglyceride-cholesterol ratio. Trajectories also revealed a WHR progression pattern: despite different starting points at the age of 24 in WHR, LDL-C and cholesterol-associated measures, all subgroups exhibited similar rates of change in these measures, i.e. WHR progression was uniform regardless of the

Published

2023

11. Circulating cell-free DNA in health and disease:the relationship to health behaviours, ageing phenotypes and metabolomics

Author

Kananen, L. (Laura), Hurme, M. (Mikko), Buerkle, A. (Alexander), Moreno-Villanueva, M. (Maria), Bernhardt, J. (Jurgen), Debacq-Chainiaux, F. (Florence), Grubeck-Loebenstein, B. (Beatrix), Malavolta, M. (Marco), Basso, A. (Andrea), Piacenza, F. (Francesco), Collino, S. (Sebastiano), Gonos, E. S. (Efstathios S.), Sikora, E. (Ewa), Gradinaru, D. (Daniela), Jansen, E. H. (Eugene H. J. M.), Dolle, M. E. (Martijn E. T.), Salmon, M. (Michel), Stuetz, W. (Wolfgang), Weber, D. (Daniela), Grune, T. (Tilman), Breusing, N. (Nicolle), Simm, A. (Andreas), Capri, M. (Miriam), Franceschi, C. (Claudio), Slagboom, E. (Eline), Talbot, D. (Duncan), Libert, C. (Claude), Raitanen, J. (Jani), Koskinen, S. (Seppo), Härkänen, T. (Tommi), Stenholm, S. (Sari), Ala-Korpela, M. (Mika), Lehtimäki, T. (Terho), Raitakari, O. T. (Olli T.), Ukkola, O. (Olavi), Kähönen, M. (Mika), Jylhä, M. (Marja), Jylhävä, J. (Juulia), Kananen, L. (Laura), Hurme, M. (Mikko), Buerkle, A. (Alexander), Moreno-Villanueva, M. (Maria), Bernhardt, J. (Jurgen), Debacq-Chainiaux, F. (Florence), Grubeck-Loebenstein, B. (Beatrix), Malavolta, M. (Marco), Basso, A. (Andrea), Piacenza, F. (Francesco), Collino, S. (Sebastiano), Gonos, E. S. (Efstathios S.), Sikora, E. (Ewa), Gradinaru, D. (Daniela), Jansen, E. H. (Eugene H. J. M.), Dolle, M. E. (Martijn E. T.), Salmon, M. (Michel), Stuetz, W. (Wolfgang), Weber, D. (Daniela), Grune, T. (Tilman), Breusing, N. (Nicolle), Simm, A. (Andreas), Capri, M. (Miriam), Franceschi, C. (Claudio), Slagboom, E. (Eline), Talbot, D. (Duncan), Libert, C. (Claude), Raitanen, J. (Jani), Koskinen, S. (Seppo), Härkänen, T. (Tommi), Stenholm, S. (Sari), Ala-Korpela, M. (Mika), Lehtimäki, T. (Terho), Raitakari, O. T. (Olli T.), Ukkola, O. (Olavi), Kähönen, M. (Mika), Jylhä, M. (Marja), and Jylhävä, J. (Juulia)

Abstract

Circulating cell-free DNA (cf-DNA) has emerged as a promising biomarker of ageing, tissue damage and cellular stress. However, less is known about health behaviours, ageing phenotypes and metabolic processes that lead to elevated cf-DNA levels. We sought to analyse the relationship of circulating cf-DNA level to age, sex, smoking, physical activity, vegetable consumption, ageing phenotypes (physical functioning, the number of diseases, frailty) and an extensive panel of biomarkers including blood and urine metabolites and inflammatory markers in three human cohorts (N = 5385; 17‐82 years). The relationships were assessed using correlation statistics, and linear and penalised regressions (the Lasso), also stratified by sex. cf-DNA levels were significantly higher in men than in women, and especially in middle-aged men and women who smoke, and in older more frail individuals. Correlation statistics of biomarker data showed that cf-DNA level was higher with elevated inflammation (C-reactive protein, interleukin-6), and higher levels of homocysteine, and proportion of red blood cells and lower levels of ascorbic acid. Inflammation (C-reactive protein, glycoprotein acetylation), amino acids (isoleucine, leucine, tyrosine), and ketogenesis (3-hydroxybutyrate) were included in the cf-DNA level-related biomarker profiles in at least two of the cohorts. In conclusion, circulating cf-DNA level is different by sex, and related to health behaviour, health decline and metabolic processes common in health and disease. These results can inform future studies where epidemiological and biological pathways of cf-DNA are to be analysed in details, and for studies evaluating cf-DNA as a potential clinical marker.

Published

2023

12. Childhood dyslipidemia and carotid atherosclerotic plaque in adulthood:the Cardiovascular Risk in Young Finns Study

Author

Koskinen, J. S. (Juhani S.), Kytö, V. (Ville), Juonala, M. (Markus), Viikari, J. S. (Jorma S. A.), Nevalainen, J. (Jaakko), Kähönen, M. (Mika), Lehtimäki, T. (Terho), Hutri-Kähönen, N. (Nina), Laitinen, T. P. (Tomi P.), Tossavainen, P. (Päivi), Jokinen, E. (Eero), Magnussen, C. G. (Costan G.), Raitakari, O. T. (Olli T.), Koskinen, J. S. (Juhani S.), Kytö, V. (Ville), Juonala, M. (Markus), Viikari, J. S. (Jorma S. A.), Nevalainen, J. (Jaakko), Kähönen, M. (Mika), Lehtimäki, T. (Terho), Hutri-Kähönen, N. (Nina), Laitinen, T. P. (Tomi P.), Tossavainen, P. (Päivi), Jokinen, E. (Eero), Magnussen, C. G. (Costan G.), and Raitakari, O. T. (Olli T.)

Abstract

Background: Childhood exposure to dyslipidemia is associated with adult atherosclerosis, but it is unclear whether the long‐term risk associated with dyslipidemia is attenuated on its resolution by adulthood. We aimed to address this question by examining the links between childhood and adult dyslipidemia on carotid atherosclerotic plaques in adulthood. Methods and Results: The Cardiovascular Risk in Young Finns Study is a prospective follow‐up of children that began in 1980. Since then, follow‐up studies have been conducted regularly. In 2001 and 2007, carotid ultrasounds were performed on 2643 participants at the mean age of 36 years to identify carotid plaques and plaque areas. For childhood lipids, we exploited several risk factor measurements to determine the individual cumulative burden for each lipid during childhood. Participants were categorized into the following 4 groups based on their childhood and adult dyslipidemia status: no dyslipidemia (reference), incident, resolved, and persistent. Among individuals with carotid plaque, linear regression models were used to study the association of serum lipids with plaque area. The prevalence of plaque was 3.3% (N=88). In models adjusted for age, sex, and nonlipid cardiovascular risk factors, the relative risk for carotid plaque was 2.34 (95% CI, 0.91–6.00) for incident adult dyslipidemia, 3.00 (95% CI, 1.42–6.34) for dyslipidemia resolved by adulthood, and 5.23 (95% CI, 2.57–10.66) for persistent dyslipidemia. Carotid plaque area correlated with childhood total, low‐density lipoprotein, and non–high‐density lipoprotein cholesterol levels. Conclusions: Childhood dyslipidemia, even if resolved by adulthood, is a risk factor for adult carotid plaque. Furthermore, among individuals with carotid plaque, childhood lipids associate with plaque size. These findings highlight the importance of primordial prevention of dyslipidemia in childhood to reduce atherosclerosis development.

Published

2023

13. Cross-sectionally calculated metabolic aging does not relate to longitudinal metabolic changes:support for stratified aging models

Author

Ala-Korpela, M. (Mika), Lehtimäki, T. (Tero), Kähönen, M. (Mika), Viikari, J. (Jorma), Perola, M. (Markus), Salomaa, V. (Veikko), Kettunen, J. (Johannes), Raitakari, O. T. (Olli T.), Mäkinen, V.-P. (Ville-Petteri), Ala-Korpela, M. (Mika), Lehtimäki, T. (Tero), Kähönen, M. (Mika), Viikari, J. (Jorma), Perola, M. (Markus), Salomaa, V. (Veikko), Kettunen, J. (Johannes), Raitakari, O. T. (Olli T.), and Mäkinen, V.-P. (Ville-Petteri)

Abstract

Context: Aging varies between individuals, with profound consequences for chronic diseases and longevity. One hypothesis to explain the diversity is a genetically regulated molecular clock that runs differently between individuals. Large human studies with long enough follow-up to test the hypothesis are rare due to practical challenges, but statistical models of aging are built as proxies for the molecular clock by comparing young and old individuals cross-sectionally. These models remain untested against longitudinal data. Objective: We applied novel methodology to test if cross-sectional modeling can distinguish slow vs accelerated aging in a human population. Methods: We trained a machine learning model to predict age from 153 clinical and cardiometabolic traits. The model was tested against longitudinal data from another cohort. The training data came from cross-sectional surveys of the Finnish population (n = 9708; ages 25–74 years). The validation data included 3 time points across 10 years in the Young Finns Study (YFS; n = 1009; ages 24–49 years). Predicted metabolic age in 2007 was compared against observed aging rate from the 2001 visit to the 2011 visit in the YFS dataset and correlation between predicted vs observed metabolic aging was determined. Results: The cross-sectional proxy failed to predict longitudinal observations (R2 = 0.018%, P = 0.67). Conclusion: The finding is unexpected under the clock hypothesis that would produce a positive correlation between predicted and observed aging. Our results are better explained by a stratified model where aging rates per se are similar in adulthood but differences in starting points explain diverging metabolic fates.

Published

2023

14. Effect of common pregnancy and perinatal complications on offspring metabolic traits across the life course:a multi-cohort study

Author

Elhakeem, A. (Ahmed), Ronkainen, J. (Justiina), Mansell, T. (Toby), Lange, K. (Katherine), Mikkola, T. M. (Tuija M.), Mishra, B. H. (Binisha H.), Wahab, R. J. (Rama J.), Cadman, T. (Tim), Yang, T. (Tiffany), Burgner, D. (David), Eriksson, J. G. (Johan G.), Järvelin, M.-R. (Marjo-Riitta), Gaillard, R. (Romy), Jaddoe, V. W. (Vincent W. V.), Lehtimäki, T. (Terhoi), Raitakari, O. T. (Olli T.), Saffery, R. (Richard), Wake, M. (Melissa), Wright, J. (John), Sebert, S. (Sylvain), Lawlor, D. A. (Deborah A.), Elhakeem, A. (Ahmed), Ronkainen, J. (Justiina), Mansell, T. (Toby), Lange, K. (Katherine), Mikkola, T. M. (Tuija M.), Mishra, B. H. (Binisha H.), Wahab, R. J. (Rama J.), Cadman, T. (Tim), Yang, T. (Tiffany), Burgner, D. (David), Eriksson, J. G. (Johan G.), Järvelin, M.-R. (Marjo-Riitta), Gaillard, R. (Romy), Jaddoe, V. W. (Vincent W. V.), Lehtimäki, T. (Terhoi), Raitakari, O. T. (Olli T.), Saffery, R. (Richard), Wake, M. (Melissa), Wright, J. (John), Sebert, S. (Sylvain), and Lawlor, D. A. (Deborah A.)

Abstract

Background: Common pregnancy and perinatal complications are associated with offspring cardiometabolic risk factors. These complications may influence multiple metabolic traits in the offspring and these associations might differ with offspring age. Methods: We used data from eight population-based cohort studies to examine and compare associations of pre-eclampsia (PE), gestational hypertension (GH), gestational diabetes (GD), preterm birth (PTB), small (SGA) and large (LGA) for gestational age (vs. appropriate size for gestational age (AGA)) with up to 167 plasma/serum-based nuclear magnetic resonance-derived metabolic traits encompassing lipids, lipoproteins, fatty acids, amino acids, ketones, glycerides/phospholipids, glycolysis, fluid balance, and inflammation. Confounder-adjusted regression models were used to examine associations (adjusted for maternal education, parity age at pregnancy, ethnicity, pre/early pregnancy body mass index and smoking, and offspring sex and age at metabolic trait assessment), and results were combined using meta-analysis by five age categories representing different periods of the offspring life course: neonates (cord blood), infancy (mean ages: 1.1–1.6 years), childhood (4.2–7.5 years); adolescence (12.0–16.0 years), and adulthood (22.0–67.8 years). Results: Offspring numbers for each age category/analysis varied from 8925 adults (441 PTB) to 1181 infants (135 GD); 48.4% to 60.0% were females. Pregnancy complications (PE, GH, GD) were each associated with up to three metabolic traits in neonates (P≤0.001) with some evidence of persistence to older ages. PTB and SGA were associated with 32 and 12 metabolic traits in neonates respectively, which included an adjusted standardised mean difference of −0.89 standard deviation (SD) units for albumin with PTB (95% CI: −1.10 to −0.69, P=1.3×10⁻¹⁷) and −0.41 SD for total lipids in medium HDL with SGA (95% CI: −0.56 to −0.25, P=2.6×10⁻⁷), with some evidence of persistence to older a

Published

2023

15. The effect of nuclear factor 1B polymorphisms and valproate use on clozapine metabolism

Author

Rask, S.M., primary, Solismaa, A., additional, Ahola-Olli, A., additional, Lyytikäinen, L.P., additional, Mononen, N., additional, Lehtimäki, T., additional, and Kampman, O., additional

Published

2023

16. Comparing the Efficacy of Electrocardiographic Leads in Recovery Phase in Detecting Coronary Artery Disease in Women

Author

Beyene, S. D., Nikus, K. C., Lehtimäki, T. J., Kähönen, M. A., Viik, J. J., Tampere University, BioMediTech, Clinical Medicine, TAYS Heart Centre, and Department of Clinical Physiology and Nuclear Medicine

Subjects

217 Medical engineering, 3121 Internal medicine

Abstract

acceptedVersion

Published

2022

17. Changes in BMI and physical activity from youth to adulthood distinguish normal-weight, metabolically obese adults from those who remain healthy

Author

Viitasalo, A., primary, Pahkala, K., additional, Lehtimäki, T., additional, Viikari, JSA., additional, Tammelin, TH., additional, Raitakari, O., additional, and Kilpeläinen, TO., additional

Published

2022

18. Viridans streptococcal immunopositivity associates with calcified coronary plaque area and coronary stenosis severity. The Tampere Sudden Death Study (TSDS)

Author

Karhunen, P., primary, Hörkkö, S., additional, Hakamaa, E., additional, Tuomisto, S., additional, Sundström, K., additional, Pessi, T., additional, Karhunen, V., additional, Iivonen, T., additional, Oksala, A., additional, Louhelainen, A.-M., additional, Goebeler, S., additional, Martiskainen, M., additional, and Lehtimäki, T., additional

Published

2022

19. Age-dependent differences in coronary atherosclerosis between women and men who died suddenly out-of-hospital

Author

Hakamaa, E., primary, Karhunen, P., additional, Goebeler, S., additional, Martiskainen, M., additional, Louhelainen, A.-M., additional, Ahinko, K., additional, and Lehtimäki, T., additional

Published

2022

20. Genetic and epigenetic regulation of nc886 RNA levels and their association to cardiometabolic phenotypes

Author

Rajic, S., primary, Marttila, S., additional, Mishra, P., additional, Mononen, N., additional, Raitakari, O., additional, Lyytikäinen, L.-P., additional, Kähönen, M., additional, Hutri-Kähönen, N., additional, Waldenberger, M., additional, Lehtimäki, T., additional, and Raitoharju, E., additional

Published

2022

21. Childhood Cardiovascular Risk Factors and Adult Cardiovascular Events

Author

Jacobs, DR, Woo, JG, Sinaiko, AR, Daniels, SR, Ikonen, J, Juonala, M, Kartiosuo, N, Lehtimäki, T, Magnussen, CG, Viikari, JSA, Zhang, N, Bazzano, LA, Burns, TL, Prineas, RJ, Steinberger, J, Urbina, EM, Venn, AJ, Raitakari, OT, Dwyer, T, Tampere University, Clinical Medicine, and Department of Clinical Chemistry

Subjects

Adult, Male, Adolescent, General Medicine, Middle Aged, Article, Young Adult, Cholesterol, Cardiovascular Diseases, Heart Disease Risk Factors, Risk Factors, Child, Preschool, Humans, Female, 3111 Biomedicine, Prospective Studies, Child

Abstract

BACKGROUND: Childhood cardiovascular risk factors predict subclinical adult cardiovascular disease, but links to clinical events are unclear. METHODS: In a prospective cohort study involving participants in the International Childhood Cardiovascular Cohort (i3C) Consortium, we evaluated whether childhood risk factors (at the ages of 3 to 19 years) were associated with cardiovascular events in adulthood after a mean follow-up of 35 years. Body-mass index, systolic blood pressure, total cholesterol level, triglyceride level, and youth smoking were analyzed with the use of i3C-derived age- and sex-specific z scores and with a combined-risk z score that was calculated as the unweighted mean of the five risk z scores. An algebraically comparable adult combined-risk z score (before any cardiovascular event) was analyzed jointly with the childhood risk factors. Study outcomes were fatal cardiovascular events and fatal or nonfatal cardiovascular events, and analyses were performed after multiple imputation with the use of proportional-hazards regression. RESULTS: In the analysis of 319 fatal cardiovascular events that occurred among 38,589 participants (49.7% male and 15.0% Black; mean [±SD] age at childhood visits, 11.8±3.1 years), the hazard ratios for a fatal cardiovascular event in adulthood ranged from 1.30 (95% confidence interval [CI], 1.14 to 1.47) per unit increase in the z score for total cholesterol level to 1.61 (95% CI, 1.21 to 2.13) for youth smoking (yes vs. no). The hazard ratio for a fatal cardiovascular event with respect to the combined-risk z score was 2.71 (95% CI, 2.23 to 3.29) per unit increase. The hazard ratios and their 95% confidence intervals in the analyses of fatal cardiovascular events were similar to those in the analyses of 779 fatal or nonfatal cardiovascular events that occurred among 20,656 participants who could be evaluated for this outcome. In the analysis of 115 fatal cardiovascular events that occurred in a subgroup of 13,401 participants (31.0±5.6 years of age at the adult measurement) who had data on adult risk factors, the adjusted hazard ratio with respect to the childhood combined-risk z score was 3.54 (95% CI, 2.57 to 4.87) per unit increase, and the mutually adjusted hazard ratio with respect to the change in the combined-risk z score from childhood to adulthood was 2.88 (95% CI, 2.06 to 4.05) per unit increase. The results were similar in the analysis of 524 fatal or nonfatal cardiovascular events. CONCLUSIONS: In this prospective cohort study, childhood risk factors and the change in the combined-risk z score between childhood and adulthood were associated with cardiovascular events in midlife. (Funded by the National Institutes of Health.)

Published

2022

22. Associations of Polymorphisms in the Peroxisome Proliferator-Activated Receptor Gamma Coactivator-1 Alpha Gene With Subsequent Coronary Heart Disease: An Individual-Level Meta-Analysis

Author

Schillemans, T., Tragante, V., Maitusong, B., Gigante, B., Cresci, S., Laguzzi, F., Vikström, M., Richards, M., Pilbrow, A., Cameron, V., Foco, L., Doughty, R.N., Kuukasjärvi, P., Allayee, H., Hartiala, J.A., Tang, W.H., Lyytikäinen, L.P., Nikus, K., Laurikka, J.O., Srinivasan, S., Mordi, I.R., Trompet, S., Kraaijeveld, A., Setten, J. van, Gijsberts, C.M., Maitland-van der Zee, A.H., Saely, C.H., Gong, Y., Johnson, J.A., Cooper-DeHoff, R.M., Pepine, C.J., Casu, G., Leiherer, A., Drexel, H., Horne, B.D., Laan, S.W. van der, Marziliano, N., Hazen, S.L., Sinisalo, J., Kähönen, M., Lehtimäki, T., Lang, C.C., Burkhardt, R., Scholz, M., Jukema, J.W., Eriksson, N., Åkerblom, A., James, S., Held, C., Hagström, E., Spertus, J.A., Algra, A., Faire, U. de, Åkesson, A., Asselbergs, F.W., Patel, R.S., Leander, K., Schillemans, T., Tragante, V., Maitusong, B., Gigante, B., Cresci, S., Laguzzi, F., Vikström, M., Richards, M., Pilbrow, A., Cameron, V., Foco, L., Doughty, R.N., Kuukasjärvi, P., Allayee, H., Hartiala, J.A., Tang, W.H., Lyytikäinen, L.P., Nikus, K., Laurikka, J.O., Srinivasan, S., Mordi, I.R., Trompet, S., Kraaijeveld, A., Setten, J. van, Gijsberts, C.M., Maitland-van der Zee, A.H., Saely, C.H., Gong, Y., Johnson, J.A., Cooper-DeHoff, R.M., Pepine, C.J., Casu, G., Leiherer, A., Drexel, H., Horne, B.D., Laan, S.W. van der, Marziliano, N., Hazen, S.L., Sinisalo, J., Kähönen, M., Lehtimäki, T., Lang, C.C., Burkhardt, R., Scholz, M., Jukema, J.W., Eriksson, N., Åkerblom, A., James, S., Held, C., Hagström, E., Spertus, J.A., Algra, A., Faire, U. de, Åkesson, A., Asselbergs, F.W., Patel, R.S., and Leander, K.

Abstract

Contains fulltext : 283506.pdf (Publisher’s version ) (Open Access), Background: The knowledge of factors influencing disease progression in patients with established coronary heart disease (CHD) is still relatively limited. One potential pathway is related to peroxisome proliferator-activated receptor gamma coactivator-1 alpha (PPARGC1A), a transcription factor linked to energy metabolism which may play a role in the heart function. Thus, its associations with subsequent CHD events remain unclear. We aimed to investigate the effect of three different SNPs in the PPARGC1A gene on the risk of subsequent CHD in a population with established CHD. Methods: We employed an individual-level meta-analysis using 23 studies from the GENetIcs of sUbSequent Coronary Heart Disease (GENIUS-CHD) consortium, which included participants (n = 80,900) with either acute coronary syndrome, stable CHD, or a mixture of both at baseline. Three variants in the PPARGC1A gene (rs8192678, G482S; rs7672915, intron 2; and rs3755863, T528T) were tested for their associations with subsequent events during the follow-up using a Cox proportional hazards model adjusted for age and sex. The primary outcome was subsequent CHD death or myocardial infarction (CHD death/myocardial infarction). Stratified analyses of the participant or study characteristics as well as additional analyses for secondary outcomes of specific cardiovascular disease diagnoses and all-cause death were also performed. Results: Meta-analysis revealed no significant association between any of the three variants in the PPARGC1A gene and the primary outcome of CHD death/myocardial infarction among those with established CHD at baseline: rs8192678, hazard ratio (HR): 1.01, 95% confidence interval (CI) 0.98-1.05 and rs7672915, HR: 0.97, 95% CI 0.94-1.00; rs3755863, HR: 1.02, 95% CI 0.99-1.06. Similarly, no significant associations were observed for any of the secondary outcomes. The results from stratified analyses showed null results, except for significant inverse associations between rs7672915 (intro

Published

2022

23. Does social intolerance vary according to cognitive styles, genetic cognitive capacity, or education?

Author

Saarinen, A. (Aino), Keltikangas-Järvinen, L. (Liisa), Dobewall, H. (Henrik), Cloninger, C. R. (C. Robert), Ahola-Olli, A. (Ari), Lehtimäki, T. (Terho), Hutri-Kähönen, N. (Nina), Raitakari, O. (Olli), Rovio, S. (Suvi), Ravaja, N. (Niklas), Saarinen, A. (Aino), Keltikangas-Järvinen, L. (Liisa), Dobewall, H. (Henrik), Cloninger, C. R. (C. Robert), Ahola-Olli, A. (Ari), Lehtimäki, T. (Terho), Hutri-Kähönen, N. (Nina), Raitakari, O. (Olli), Rovio, S. (Suvi), and Ravaja, N. (Niklas)

Abstract

Background: Low education, low cognitive abilities, and certain cognitive styles are suggested to predispose to social intolerance and prejudices. Evidence is, however, restricted by comparatively small samples, neglect of confounding variables and genetic factors, and a narrow focus on a single sort of prejudice. We investigated the relationships of education, polygenic cognitive potential, cognitive performance, and cognitive styles with social intolerance in adulthood over a 15-year follow-up. Methods: We used data from the prospective population-based Young Finns Study (n = 960‒1679). Social intolerance was evaluated with the Social Intolerance Scale in 1997, 2001, and 2011; cognitive performance with the Cambridge Neuropsychological Test Automated Battery in 2011; cognitive styles in 1997; and socioeconomic factors in 1980 (childhood) and 2011 (adulthood); and polygenic cognitive potential was calculated based on genome-wide association studies. Results: We found that nonrational thinking, polygenic cognitive potential, cognitive performance, or socioeconomic factors were not related to social intolerance. Regarding cognitive styles, low flexibility (B = –0.759, p < .001), high perseverance (B = 1.245, p < .001), and low persistence (B = –0.329, p < .001) predicted higher social intolerance consistently in the analyses. Discussion: When developing prejudice-reduction interventions, it should be considered that educational level or cognitive performance may not be crucial for development of social intolerance. Adopting certain cognitive styles may play more important roles in development of social intolerance.

Published

2022

24. Pancreatic secretory trypsin inhibitor (SPINK1) gene mutation in patients with acute alcohol pancreatitis (AAP) compared to healthy controls and heavy alcohol users without pancreatitis

Author

Nikkola, A. (Anssi), Mäkelä, K. A. (Kari Antero), Herzig, K.-H. (Karl-Heinz), Mutt, S. J. (Shivaprakash Jagalur), Prasannan, A. (Aishwarya), Seppänen, H. (Hanna), Lehtimäki, T. (Terho), Kähönen, M. (Mika), Raitakari, O. (Olli), Seppälä, I. (Ilkka), Pakkanen, P. (Pihla), Nordback, I. (Isto), Sand, J. (Juhani), Laukkarinen, J. (Johanna), Nikkola, A. (Anssi), Mäkelä, K. A. (Kari Antero), Herzig, K.-H. (Karl-Heinz), Mutt, S. J. (Shivaprakash Jagalur), Prasannan, A. (Aishwarya), Seppänen, H. (Hanna), Lehtimäki, T. (Terho), Kähönen, M. (Mika), Raitakari, O. (Olli), Seppälä, I. (Ilkka), Pakkanen, P. (Pihla), Nordback, I. (Isto), Sand, J. (Juhani), and Laukkarinen, J. (Johanna)

Abstract

Only 3–5% of heavy alcohol users develop acute alcohol pancreatitis (AAP). This suggests that additional triggers are required to initiate the inflammatory process. Genetic susceptibility contributes to the development of AAP, and SPINK1 mutation is a documented risk factor. We investigated the prevalence of the SPINK1(N34S) mutation in patients with AAP compared to heavy alcohol users who had never suffered an episode of pancreatitis. Blood samples for the mutational analysis from patients with first episode (n = 60) and recurrent AAP (n = 43) and from heavy alcohol users without a history of AAP (n = 98) as well as from a control population (n = 1914) were obtained. SPINK1 mutation was found in 8.7% of the patients with AAP. The prevalence was significantly lower in healthy controls (3.4%, OR 2.72; 1.32–5.64) and very low in alcoholics without pancreatitis (1.0%, OR 9.29; 1.15–74.74). In a comparison adjusted for potential cofounders between AAP patients and alcoholics, SPINK1 was found to be an independent marker for AAP. The prevalence of the SPINK1 mutation is overrepresented in AAP patients and very low in alcoholics without pancreatitis. This finding may play a role in understanding the variable susceptibility to AAP found in heavy alcohol users.

Published

2022

25. Genome-wide analysis of 102,084 migraine cases identifies 123 risk loci and subtype-specific risk alleles

Author

Hautakangas, H. (Heidi), Winsvold, B. S. (Bendik S.), Ruotsalainen, S. E. (Sanni E.), Bjornsdottir, G. (Gyda), Harder, A. V. (Aster V. E.), Kogelman, L. J. (Lisette J. A.), Thomas, L. F. (Laurent F.), Noordam, R. (Raymond), Benner, C. (Christian), Gormley, P. (Padhraig), Artto, V. (Ville), Banasik, K. (Karina), Bjornsdottir, A. (Anna), Boomsma, D. I. (Dorret, I), Brumpton, B. M. (Ben M.), Burgdorf, K. S. (Kristoffer Solvsten), Buring, J. E. (Julie E.), Chalmer, M. A. (Mona Ameri), de Boer, I. (Irene), Dichgans, M. (Martin), Erikstrup, C. (Christian), Färkkilä, M. (Markus), Garbrielsen, M. E. (Maiken Elvestad), Ghanbari, M. (Mohsen), Hagen, K. (Knut), Häppölä, P. (Paavo), Hottenga, J.-J. (Jouke-Jan), Hrafnsdottir, M. G. (Maria G.), Hveem, K. (Kristian), Johnsen, M. B. (Marianne Bakke), Kähönen, M. (Mika), Kristoffersen, E. S. (Espen S.), Kurth, T. (Tobias), Lehtimäki, T. (Terho), Lighart, L. (Lannie), Magnusson, S. H. (Sigurdur H.), Malik, R. (Rainer), Pedersen, O. B. (Ole Birger), Pelzer, N. (Nadine), Penninx, B. W. (Brenda W. J. H.), Ran, C. (Caroline), Ridker, P. M. (Paul M.), Rosendaal, F. R. (Frits R.), Sigurdardottir, G. R. (Gudrun R.), Skogholt, A. H. (Anne Heidi), Sveinsson, O. A. (Olafur A.), Thorgeirsson, T. E. (Thorgeir E.), Ullum, H. (Henrik), Vijfhuizen, L. S. (Lisanne S.), Widen, E. (Elisabeth), van Dijk, K. W. (Ko Willems), International Headache Genetics Consortium, HUNT All-in Headache, Danish Blood Donor Study Genomic Cohort, Aromaa, A. (Arpo), Belin, A. C. (Andrea Carmine), Freilinger, T. (Tobias), Ikram, M. A. (M. Arfan), Järvelin, M.-R. (Marjo-Riitta), Raitakari, O. T. (Olli T.), Terwindt, G. M. (Gisela M.), Kallela, M. (Mikko), Wessman, M. (Maija), Olesen, J. (Jes), Chasman, D. I. (Daniel, I), Nyholt, D. R. (Dale R.), Stefansson, H. (Hreinn), Stefansson, K. (Kari), van den Maagdenberg, A. M. (Arn M. J. M.), Hansen, T. F. (Thomas Folkmann), Ripatti, S. (Samuli), Zwart, J.-A. (John-Anker), Palotie, A. (Aarno), Pirinen, M. (Matti), Hautakangas, H. (Heidi), Winsvold, B. S. (Bendik S.), Ruotsalainen, S. E. (Sanni E.), Bjornsdottir, G. (Gyda), Harder, A. V. (Aster V. E.), Kogelman, L. J. (Lisette J. A.), Thomas, L. F. (Laurent F.), Noordam, R. (Raymond), Benner, C. (Christian), Gormley, P. (Padhraig), Artto, V. (Ville), Banasik, K. (Karina), Bjornsdottir, A. (Anna), Boomsma, D. I. (Dorret, I), Brumpton, B. M. (Ben M.), Burgdorf, K. S. (Kristoffer Solvsten), Buring, J. E. (Julie E.), Chalmer, M. A. (Mona Ameri), de Boer, I. (Irene), Dichgans, M. (Martin), Erikstrup, C. (Christian), Färkkilä, M. (Markus), Garbrielsen, M. E. (Maiken Elvestad), Ghanbari, M. (Mohsen), Hagen, K. (Knut), Häppölä, P. (Paavo), Hottenga, J.-J. (Jouke-Jan), Hrafnsdottir, M. G. (Maria G.), Hveem, K. (Kristian), Johnsen, M. B. (Marianne Bakke), Kähönen, M. (Mika), Kristoffersen, E. S. (Espen S.), Kurth, T. (Tobias), Lehtimäki, T. (Terho), Lighart, L. (Lannie), Magnusson, S. H. (Sigurdur H.), Malik, R. (Rainer), Pedersen, O. B. (Ole Birger), Pelzer, N. (Nadine), Penninx, B. W. (Brenda W. J. H.), Ran, C. (Caroline), Ridker, P. M. (Paul M.), Rosendaal, F. R. (Frits R.), Sigurdardottir, G. R. (Gudrun R.), Skogholt, A. H. (Anne Heidi), Sveinsson, O. A. (Olafur A.), Thorgeirsson, T. E. (Thorgeir E.), Ullum, H. (Henrik), Vijfhuizen, L. S. (Lisanne S.), Widen, E. (Elisabeth), van Dijk, K. W. (Ko Willems), International Headache Genetics Consortium, HUNT All-in Headache, Danish Blood Donor Study Genomic Cohort, Aromaa, A. (Arpo), Belin, A. C. (Andrea Carmine), Freilinger, T. (Tobias), Ikram, M. A. (M. Arfan), Järvelin, M.-R. (Marjo-Riitta), Raitakari, O. T. (Olli T.), Terwindt, G. M. (Gisela M.), Kallela, M. (Mikko), Wessman, M. (Maija), Olesen, J. (Jes), Chasman, D. I. (Daniel, I), Nyholt, D. R. (Dale R.), Stefansson, H. (Hreinn), Stefansson, K. (Kari), van den Maagdenberg, A. M. (Arn M. J. M.), Hansen, T. F. (Thomas Folkmann), Ripatti, S. (Samuli), Zwart, J.-A. (John-Anker), Palotie, A. (Aarno), and Pirinen, M. (Matti)

Abstract

Migraine affects over a billion individuals worldwide but its genetic underpinning remains largely unknown. Here, we performed a genome-wide association study of 102,084 migraine cases and 771,257 controls and identified 123 loci, of which 86 are previously unknown. These loci provide an opportunity to evaluate shared and distinct genetic components in the two main migraine subtypes: migraine with aura and migraine without aura. Stratification of the risk loci using 29,679 cases with subtype information indicated three risk variants that seem specific for migraine with aura (in HMOX2, CACNA1A and MPPED2), two that seem specific for migraine without aura (near SPINK2 and near FECH) and nine that increase susceptibility for migraine regardless of subtype. The new risk loci include genes encoding recent migraine-specific drug targets, namely calcitonin gene-related peptide (CALCA/CALCB) and serotonin 1F receptor (HTR1F). Overall, genomic annotations among migraine-associated variants were enriched in both vascular and central nervous system tissue/cell types, supporting unequivocally that neurovascular mechanisms underlie migraine pathophysiology.

Published

2022

26. Bidirectional pathways between psychosocial risk factors and paranoid ideation in a general nonclinical population

Author

Saarinen, A. (Aino), Granö, N. (Niklas), Hintsanen, M. (Mirka), Lehtimäki, T. (Terho), Cloninge, C. R. (C. Robert), Keltikangas-Järvinen, L. (Liisa), Saarinen, A. (Aino), Granö, N. (Niklas), Hintsanen, M. (Mirka), Lehtimäki, T. (Terho), Cloninge, C. R. (C. Robert), and Keltikangas-Järvinen, L. (Liisa)

Abstract

We investigated (a) whether psychosocial factors (experienced stress, anticipatory worry, social detachment, sleeping disturbances, alcohol use) predict the course of paranoid ideation between the ages of 24 to 50 years and (b) whether the predictive relationships are more likely to proceed from the psychosocial factors to paranoid ideation, or vice versa. The participants (N = 1534–1553) came from the population-based Young Finns study. Paranoid ideation and psychosocial factors were assessed by reliable self-report questionnaires in 2001, 2007, and 2011/2012. The data were analyzed using growth curve and structural equation models. High experienced stress, anticipatory worry, social detachment, frequent sleeping disturbances, and frequent alcohol use predicted more paranoid ideation. More risk factors predicted increasing paranoid ideation. There were bidirectional predictive relationships of paranoid ideation with experienced stress, anticipatory worry, social detachment, and sleeping disturbances. The link between alcohol use and paranoid ideation was only correlative. In conclusion, paranoid ideation increases by reciprocal interactions with stress, worry, social detachment, and sleeping disturbances. The findings support the threat–anticipation model of paranoid ideation, providing important implications for treatment of paranoia.

Published

2022

27. The relationship between temperament, polygenic score for intelligence and cognition:a population-based study of middle-aged adults

Author

Tölli, P. (Pekka), Keltikangas-Järvinen, L. (Liisa), Lehtimäki, T. (Terho), Ravaja, N. (Niklas), Hintsanen, M. (Mirka), Ahola-Olli, A. (Ari), Pahkala, K. (Katja), Kähönen, M. (Mika), Hutri-Kähönen, N. (Nina), Laitinen, T. T. (Tomi T.), Tossavainen, P. (Päivi), Taittonen, L. (Leena), Dobewall, H. (Henrik), Jokinen, E. (Eero), Raitakari, O. (Olli), Cloninger, C. R. (C. Robert), Rovio, S. (Suvi), Saarinen, A. (Aino), Tölli, P. (Pekka), Keltikangas-Järvinen, L. (Liisa), Lehtimäki, T. (Terho), Ravaja, N. (Niklas), Hintsanen, M. (Mirka), Ahola-Olli, A. (Ari), Pahkala, K. (Katja), Kähönen, M. (Mika), Hutri-Kähönen, N. (Nina), Laitinen, T. T. (Tomi T.), Tossavainen, P. (Päivi), Taittonen, L. (Leena), Dobewall, H. (Henrik), Jokinen, E. (Eero), Raitakari, O. (Olli), Cloninger, C. R. (C. Robert), Rovio, S. (Suvi), and Saarinen, A. (Aino)

Abstract

We investigated whether temperament modifies an association between polygenic intelligence potential and cognitive test performance in midlife. The participants (n = 1647, born between 1962 and 1977) were derived from the Young Finns Study. Temperament was assessed with Temperament and Character Inventory over a 15-year follow-up (1997, 2001, 2007, 2012). Polygenic intelligence potential was assessed with a polygenic score for intelligence. Cognitive performance (visual memory, reaction time, sustained attention, spatial working memory) was assessed with CANTAB in midlife. The PGSI was significantly associated with the overall cognitive performance and performance in visual memory, sustained attention and working memory tests but not reaction time test. Temperament did not correlate with polygenic score for intelligence and did not modify an association between the polygenic score and cognitive performance, either. High persistence was associated with higher visual memory (B = 0.092; FDR-adj. p = 0.007) and low harm avoidance with higher overall cognitive performance, specifically better reaction time (B = −0.102; FDR-adj; p = 0.007). The subscales of harm avoidance had different associations with cognitive performance: higher “anticipatory worry,” higher “fatigability,” and lower “shyness with strangers” were associated with lower cognitive performance, while the role of “fear of uncertainty” was subtest-related. In conclusion, temperament does not help or hinder one from realizing their genetic potential for intelligence. The overall modest relationships between temperament and cognitive performance advise caution if utilizing temperament-related information e.g. in working-life recruitments. Cognitive abilities may be influenced by temperament variables, such as the drive for achievement and anxiety about test performance, but they involve distinct systems of learning and memory.

Published

2022

28. Evolution of genetic networks for human creativity

Author

Zwir, I. (I.), Del-Val, C. (C.), Hintsanen, M. (Mirka), Cloninger, K. M. (K. M.), Romero-Zaliz, R. (R.), Mesa, A. (A.), Arnedo, J. (J.), Salas, R. (R.), Poblete, G. F. (G. F.), Raitoharju, E. (E.), Raitakari, O. (O.), Keltikangas-Järvinen, L. (L.), de Erausquin, G. A. (G. A.), Tattersall, I. (I.), Lehtimäki, T. (T.), Cloninger, C. R. (C. R.), Zwir, I. (I.), Del-Val, C. (C.), Hintsanen, M. (Mirka), Cloninger, K. M. (K. M.), Romero-Zaliz, R. (R.), Mesa, A. (A.), Arnedo, J. (J.), Salas, R. (R.), Poblete, G. F. (G. F.), Raitoharju, E. (E.), Raitakari, O. (O.), Keltikangas-Järvinen, L. (L.), de Erausquin, G. A. (G. A.), Tattersall, I. (I.), Lehtimäki, T. (T.), and Cloninger, C. R. (C. R.)

Abstract

The genetic basis for the emergence of creativity in modern humans remains a mystery despite sequencing the genomes of chimpanzees and Neanderthals, our closest hominid relatives. Data-driven methods allowed us to uncover networks of genes distinguishing the three major systems of modern human personality and adaptability: emotional reactivity, self-control, and self-awareness. Now we have identified which of these genes are present in chimpanzees and Neanderthals. We replicated our findings in separate analyses of three high-coverage genomes of Neanderthals. We found that Neanderthals had nearly the same genes for emotional reactivity as chimpanzees, and they were intermediate between modern humans and chimpanzees in their numbers of genes for both self-control and self-awareness. 95% of the 267 genes we found only in modern humans were not protein-coding, including many long-non-coding RNAs in the self-awareness network. These genes may have arisen by positive selection for the characteristics of human well-being and behavioral modernity, including creativity, prosocial behavior, and healthy longevity. The genes that cluster in association with those found only in modern humans are over-expressed in brain regions involved in human self-awareness and creativity, including late-myelinating and phylogenetically recent regions of neocortex for autobiographical memory in frontal, parietal, and temporal regions, as well as related components of cortico-thalamo-ponto-cerebellar-cortical and cortico-striato-cortical loops. We conclude that modern humans have more than 200 unique non-protein-coding genes regulating co-expression of many more protein-coding genes in coordinated networks that underlie their capacities for self-awareness, creativity, prosocial behavior, and healthy longevity, which are not found in chimpanzees or Neanderthals.

Published

2022

29. Genetic and observational evidence:no independent role for cholesterol efflux over static high-density lipoprotein concentration measures in coronary heart disease risk assessment

Author

Kuusisto, S. (Sanna), Karjalainen, M. K. (Minna K.), Tillin, T. (Therese), Kangas, A. J. (Antti J.), Holmes, M. V. (Michael V.), Kähönen, M. (Mika), Lehtimäki, T. (Terho), Viikari, J. (Jorma), Perola, M. (Markus), Chaturvedi, N. (Nishi), Salomaa, V. (Veikko), Raitakari, O. T. (Olli T.), Järvelin, M.-R. (Marjo-Riitta), Kettunen, J. (Johannes), Ala-Korpela, M. (Mika), Kuusisto, S. (Sanna), Karjalainen, M. K. (Minna K.), Tillin, T. (Therese), Kangas, A. J. (Antti J.), Holmes, M. V. (Michael V.), Kähönen, M. (Mika), Lehtimäki, T. (Terho), Viikari, J. (Jorma), Perola, M. (Markus), Chaturvedi, N. (Nishi), Salomaa, V. (Veikko), Raitakari, O. T. (Olli T.), Järvelin, M.-R. (Marjo-Riitta), Kettunen, J. (Johannes), and Ala-Korpela, M. (Mika)

Abstract

Background: Observational findings for high-density lipoprotein (HDL)-mediated cholesterol efflux capacity (HDL-CEC) and coronary heart disease (CHD) appear inconsistent, and knowledge of the genetic architecture of HDL-CEC is limited. Objectives: A large-scale observational study on the associations of HDL-CEC and other HDL-related measures with CHD and the largest genome-wide association study (GWAS) of HDL-CEC. Participants/Methods: Six independent cohorts were included with follow-up data for 14,438 participants to investigate the associations of HDL-related measures with incident CHD (1,570 events). The GWAS of HDL-CEC was carried out in 20,372 participants. Results: HDL-CEC did not associate with CHD when adjusted for traditional risk factors and HDL cholesterol (HDL-C). In contradiction, almost all HDL-related concentration measures associated consistently with CHD after corresponding adjustments. There were no genetic loci associated with HDL-CEC independent of HDL-C and triglycerides. Conclusions: HDL-CEC is not unequivocally associated with CHD in contrast to HDL-C, apolipoprotein A-I, and most of the HDL subclass particle concentrations.

Published

2022

30. Circulating inflammatory cytokines and risk of five cancers: a Mendelian randomization analysis

Author

Bouras, E. (Emmanouil), Karhunen, V. (Ville), Gill, D. (Dipender), Huang, J. (Jian), Haycock, P. C. (Philip C.), Gunter, M. J. (Marc J.), Johansson, M. (Mattias), Brennan, P. (Paul), Key, T. (Tim), Lewis, S. J. (Sarah J.), Martin, R. M. (Richard M.), Murphy, N. (Neil), Platz, E. A. (Elizabeth A.), Travis, R. (Ruth), Yarmolinsky, J. (James), Zuber, V. (Verena), Martin, P. (Paul), Katsoulis, M. (Michail), Freisling, H. (Heinz), Nost, T. H. (Therese Haugdahl), Schulze, M. B. (Matthias B.), Dossus, L. (Laure), Hung, R. J. (Rayjean J.), Amos, C. I. (Christopher, I), Ahola-Olli, A. (Ari), Palaniswamy, S. (Saranya), Mannikko, M. (Minna), Auvinen, J. (Juha), Herzig, K.-H. (Karl-Heinz), Keinänen-Kiukaanniemi, S. (Sirkka), Lehtimäki, T. (Terho), Salomaa, V. (Veikko), Raitakari, O. (Olli), Salmi, M. (Marko), Jalkanen, S. (Sirpa), Järvelin, M.-R. (Marjo-Riitta), Dehghan, A. (Abbas), Tsilidis, K. K. (Konstantinos K.), Bouras, E. (Emmanouil), Karhunen, V. (Ville), Gill, D. (Dipender), Huang, J. (Jian), Haycock, P. C. (Philip C.), Gunter, M. J. (Marc J.), Johansson, M. (Mattias), Brennan, P. (Paul), Key, T. (Tim), Lewis, S. J. (Sarah J.), Martin, R. M. (Richard M.), Murphy, N. (Neil), Platz, E. A. (Elizabeth A.), Travis, R. (Ruth), Yarmolinsky, J. (James), Zuber, V. (Verena), Martin, P. (Paul), Katsoulis, M. (Michail), Freisling, H. (Heinz), Nost, T. H. (Therese Haugdahl), Schulze, M. B. (Matthias B.), Dossus, L. (Laure), Hung, R. J. (Rayjean J.), Amos, C. I. (Christopher, I), Ahola-Olli, A. (Ari), Palaniswamy, S. (Saranya), Mannikko, M. (Minna), Auvinen, J. (Juha), Herzig, K.-H. (Karl-Heinz), Keinänen-Kiukaanniemi, S. (Sirkka), Lehtimäki, T. (Terho), Salomaa, V. (Veikko), Raitakari, O. (Olli), Salmi, M. (Marko), Jalkanen, S. (Sirpa), Järvelin, M.-R. (Marjo-Riitta), Dehghan, A. (Abbas), and Tsilidis, K. K. (Konstantinos K.)

Abstract

Background: Epidemiological and experimental evidence has linked chronic inflammation to cancer aetiology. It is unclear whether associations for specific inflammatory biomarkers are causal or due to bias. In order to examine whether altered genetically predicted concentration of circulating cytokines are associated with cancer development, we performed a two-sample Mendelian randomisation (MR) analysis. Methods: Up to 31,112 individuals of European descent were included in genome-wide association study (GWAS) meta-analyses of 47 circulating cytokines. Single nucleotide polymorphisms (SNPs) robustly associated with the cytokines, located in or close to their coding gene (cis), were used as instrumental variables. Inverse-variance weighted MR was used as the primary analysis, and the MR assumptions were evaluated in sensitivity and colocalization analyses and a false discovery rate (FDR) correction for multiple comparisons was applied. Corresponding germline GWAS summary data for five cancer outcomes (breast, endometrial, lung, ovarian, and prostate), and their subtypes were selected from the largest cancer-specific GWASs available (cases ranging from 12,906 for endometrial to 133,384 for breast cancer). Results: There was evidence of inverse associations of macrophage migration inhibitory factor with breast cancer (OR per SD = 0.88, 95% CI 0.83 to 0.94), interleukin-1 receptor antagonist with endometrial cancer (0.86, 0.80 to 0.93), interleukin-18 with lung cancer (0.87, 0.81 to 0.93), and beta-chemokine-RANTES with ovarian cancer (0.70, 0.57 to 0.85) and positive associations of monokine induced by gamma interferon with endometrial cancer (3.73, 1.86 to 7.47) and cutaneous T-cell attracting chemokine with lung cancer (1.51, 1.22 to 1.87). These associations were similar in sensitivity analyses and supported in colocalization analyses. Conclusions: Our study adds to current knowledge on the role of specific inflammatory biomarker pathways in cancer aetiolog

Published

2022

31. Glycoprotein acetyls:a novel inflammatory biomarker of early cardiovascular risk in the young

Author

Chiesa, S. T. (Scott T.), Charakida, M. (Marietta), Georgiopoulos, G. (Georgios), Roberts, J. D. (Justin D.), Stafford, S. J. (Simon J.), Park, C. (Chloe), Mykkänen, J. (Juha), Kähönen, M. (Mika), Lehtimäki, T. (Terho), Ala‐Korpela, M. (Mika), Raitakari, O. (Olli), Pietiäinen, M. (Milla), Pussinen, P. (Pirkko), Muthurangu, V. (Vivek), Hughes, A. D. (Alun D.), Sattar, N. (Naveed), Timpson, N. J. (Nicholas J.), Deanfield, J. E. (John E.), Chiesa, S. T. (Scott T.), Charakida, M. (Marietta), Georgiopoulos, G. (Georgios), Roberts, J. D. (Justin D.), Stafford, S. J. (Simon J.), Park, C. (Chloe), Mykkänen, J. (Juha), Kähönen, M. (Mika), Lehtimäki, T. (Terho), Ala‐Korpela, M. (Mika), Raitakari, O. (Olli), Pietiäinen, M. (Milla), Pussinen, P. (Pirkko), Muthurangu, V. (Vivek), Hughes, A. D. (Alun D.), Sattar, N. (Naveed), Timpson, N. J. (Nicholas J.), and Deanfield, J. E. (John E.)

Abstract

Background: Low‐grade inflammation in the young may contribute to the early development of cardiovascular disease. We assessed whether circulating levels of glycoprotein acetyls (GlycA) were better able to predict the development of adverse cardiovascular disease risk profiles compared with the more commonly used biomarker high‐sensitivity CRP (C‐reactive protein). Methods: A total of 3306 adolescents and young adults from the Avon Longitudinal Study of Parents and Children (mean age, 15.4±0.3; n=1750) and Cardiovascular Risk in Young Finns Study (mean age, 32.1±5.0; n=1556) were included. Baseline associations between inflammatory biomarkers, body composition, cardiovascular risk factors, and subclinical measures of vascular dysfunction were assessed cross‐sectionally in both cohorts. Prospective risk of developing hypertension and metabolic syndrome during 9‐to‐10‐year follow‐up were also assessed as surrogate markers for future cardiovascular risk. GlycA showed greater within‐subject correlation over 9‐to‐10‐year follow‐up in both cohorts compared with CRP, particularly in the younger adolescent group (r=0.36 versus 0.07). In multivariable analyses, GlycA was found to associate with multiple lifestyle‐related cardiovascular disease risk factors, cardiometabolic risk factor burden, and vascular dysfunction (eg, mean difference in flow‐mediated dilation=−1.2 [−1.8, −0.7]% per z‐score increase). In contrast, CRP levels appeared predominantly driven by body mass index and showed little relationship to any measured cardiovascular risk factors or phenotypes. In both cohorts, only GlycA predicted future risk of both hypertension (risk ratio [RR], ≈1.1 per z‐score increase for both cohorts) and metabolic syndrome (RR, ≈1.2–1.3 per z‐score increase for both cohorts) in 9‐to‐10‐year follow‐up. Conclusions: Low‐grade inflammation captured by the novel biomarker GlycA is associated with adverse cardiovascular risk profiles from as early as adolescence and predicts f

Published

2022

32. Outcome and biomarker supervised deep learning for survival prediction in two multicenter breast cancer series

Author

Bychkov, D. (Dmitrii), Joensuu, H. (Heikki), Nordling, S. (Stig), Tiulpin, A. (Aleksei), Kücükel, H. (Hakan), Lundin, M. (Mikael), Sihto, H. (Harri), Isola, J. (Jorma), Lehtimäki, T. (Tiina), Kellokumpu-Lehtinen, P.-L. (Pirkko-Liisa), von Smitten, K. (Karl), Lundin, J. (Johan), Linder, N. (Nina), Bychkov, D. (Dmitrii), Joensuu, H. (Heikki), Nordling, S. (Stig), Tiulpin, A. (Aleksei), Kücükel, H. (Hakan), Lundin, M. (Mikael), Sihto, H. (Harri), Isola, J. (Jorma), Lehtimäki, T. (Tiina), Kellokumpu-Lehtinen, P.-L. (Pirkko-Liisa), von Smitten, K. (Karl), Lundin, J. (Johan), and Linder, N. (Nina)

Abstract

Background: Prediction of clinical outcomes for individual cancer patients is an important step in the disease diagnosis and subsequently guides the treatment and patient counseling. In this work, we develop and evaluate a joint outcome and biomarker supervised (estrogen receptor expression and ERBB2 expression and gene amplification) multitask deep learning model for prediction of outcome in breast cancer patients in two nation-wide multicenter studies in Finland (the FinProg and FinHer studies). Our approach combines deep learning with expert knowledge to provide more accurate, robust, and integrated prediction of breast cancer outcomes. Materials and Methods: Using deep learning, we trained convolutional neural networks (CNNs) with digitized tissue microarray (TMA) samples of primary hematoxylin-eosin-stained breast cancer specimens from 693 patients in the FinProg series as input and breast cancer-specific survival as the endpoint. The trained algorithms were tested on 354 TMA patient samples in the same series. An independent set of whole-slide (WS) tumor samples from 674 patients in another multicenter study (FinHer) was used to validate and verify the generalization of the outcome prediction based on CNN models by Cox survival regression and concordance index (c-index). Visual cancer tissue characterization, i.e., number of mitoses, tubules, nuclear pleomorphism, tumor-infiltrating lymphocytes, and necrosis was performed on TMA samples in the FinProg test set by a pathologist and combined with deep learning-based outcome prediction in a multitask algorithm. Results: The multitask algorithm achieved a hazard ratio (HR) of 2.0 (95% confidence interval [CI] 1.30–3.00), P < 0.001, c-index of 0.59 on the 354 test set of FinProg patients, and an HR of 1.7 (95% CI 1.2–2.6), P = 0.003, c-index 0.57 on the WS tumor samples from 674 patients in the independent FinHer series. The multitask CNN remained a statistically independent predictor of survival in bot

Published

2022

33. Changes in BMI and physical activity from youth to adulthood distinguish normal-weight, metabolically obese adults from those who remain healthy

Author

Viitasalo, A., Pahkala, K., Lehtimäki, T., Viikari, J. S.A., Tammelin, T. H., Raitakari, O., Kilpeläinen, T. O., Viitasalo, A., Pahkala, K., Lehtimäki, T., Viikari, J. S.A., Tammelin, T. H., Raitakari, O., and Kilpeläinen, T. O.

Abstract

Highlights: Adults with MONW have a lower BMI during youth until young adulthood, but higher BMI after this than adults with metabolically healthy normal weight. Adults with MONW have a greater decrease in physical activity from youth to adulthood than other adults. Healthy lifestyle is important in the prevention of metabolic disorders, particularly in individuals who are slim in childhood. Background: Individuals with metabolically obese normal-weight (MONW) have higher risk of cardiovascular events than those with obesity but a metabolically healthy status. Etiological factors leading to MONW are not well known. We hypothesized distinct trajectories of changes in BMI and physical activity may modify metabolic risk and distinguish individuals with MONW from those who remain healthy. Methods: We compared the mean levels of BMI and physical activity at eight time points (1980, 1983, 1986, 1989, 1992, 2001, 2007, 2011) between MONW and healthy normal-weight adults using linear mixed-model analysis. The analyses included 1180 participants of the Cardiovascular Risk in Young Finns study, a population-based study that represents six different age cohorts 3, 6, 9, 12, 15 and 18 years of age at baseline. Results: Individuals with adult MONW had significantly lower BMI in childhood and young adulthood, but their BMI increased more than in other adults after this age (p<0.001for interaction between time and MONW status). Physical activity decreased relatively more since youth in individuals with adult MONW (p<0.001). Conclusions: Relative leanness in youth and subsequent weight gain in young adulthood, and a gradual decrease in physical activity levels from youth to adulthood, predispose normal-weight individuals to metabolic impairments. The results highlight the importance of a healthy lifestyle in the prevention of metabolic disorders, particularly in individuals who are slim in childhood.

Published

2022

34. Intraductal Papillary Neoplasia of the Pancreas (IPMN) under Surveillance

Author

Kaprio, T., primary, Johansson, K., additional, Nieminen, H., additional, Lehtimäki, T., additional, Lantto, E., additional, Haglund, C., additional, and Seppänen, H., additional

Published

2022

35. Low-Density Lipoprotein Cholesterol Level Distributions Across Different Ages: Implications for Screening Children for Severe and Familial Hypercholesterolemia.

Author

Liu J, Bellows BK, Jacobs DR Jr, Woo JG, Urbina EM, Balte PP, Oelsner EC, Kazi DS, Siscovick D, Allen NB, Rana JS, Wilkins JT, Hall ME, Bazzano LA, Burns TL, Daniels SR, Dwyer T, Juonala M, Raitakari OT, Sinaiko AR, Steinberger J, Venn AJ, Kartiosuo N, Lehtimäki T, Magnussen CG, Viikari JSA, de Ferranti SD, Moran AE, and Zhang Y

Abstract

Competing Interests: None.

Published

2024

36. Leptin and leptin receptor gene polymorphisms and depression treatment response.

Author

Tavast IM, Solismaa A, Lyytikäinen LP, Mononen N, Moilanen E, Hämäläinen M, Lehtimäki T, and Kampman O

Abstract

Objective: Associations between leptin ( LEP ) and leptin receptor ( LEPR ) gene polymorphisms and mood disorders have been found but not yet confirmed in multiple studies. The aim of our study was to study the associations between LEP and LEPR single nucleotide polymorphisms (SNPs) and treatment response of depression. Associations between leptin levels and depression severity were also investigated., Methods: The data included 242 depressed patients in secondary psychiatric care. Symptoms of depression were assessed with the Montgomery–Åsberg Depression Rating Scale (MADRS). Previously found LEP and LEPR SNPs associated with depression and other mood disorders were studied. Furthermore, all available LEP and LEPR SNPs were clumped using proxy SNPs to represent gene areas in r 2 > 0.2 linkage disequilibrium and their association with treatment response was analysed with logistic regression., Results: Two proxy SNPs of LEPR gene, rs12564738 and rs12029311, were associated with MADRS response at 6 weeks ( p adjusted = 0.024, p adjusted = 0.024). SNPs from previous studies were not associated with MADRS response, but LEPR rs12145690 from a previous study was strongly associated with rs12564738 ( r 2 = 0.94). The positive association between leptin levels and MADRS score at baseline after adjusting with age, sex, body mass index (BMI), Alcohol Use Disorders Identification Test score, and smoking was found ( p = 0.011)., Conclusion: Our findings suggest that LEPR polymorphisms are associated with depression treatment response. We also found associations between leptin levels and depression independently of BMI. Further studies and meta-analyses are needed to confirm the significance of found SNPs and the role of leptin in depression.

Published

2024

37. Genetic risk score for coronary artery calcification and its predictive ability for coronary artery disease.

Author

Mishra PP, Mishra BH, Lyytikäinen LP, Goebeler S, Martiskainen M, Hakamaa E, Kleber ME, Delgado GE, März W, Kähönen M, Karhunen PJ, and Lehtimäki T

Abstract

Aim: The modest added predictive value of the existing genetic risk scores (GRSs) for coronary artery disease (CAD) could be partly due to missing genetic components, hidden in the genetic architecture of intermediate phenotypes such as coronary artery calcification (CAC). In this study, we investigated the predictive ability of CAC GRS for CAD., Materials and Methods: We investigated the association of CAC GRSs with CAD and coronary calcification among the participants in the Ludwigshafen Risk and Cardiovascular Health study (LURIC) ( n = 2742), the Tampere Vascular Study (TVS) ( n = 133), and the Tampere Sudden Death Study (TSDS) ( n = 660) using summary data from the largest multi-ancestry GWAS meta-analysis of CAC to date. Added predictive value of the CAC GRS over the traditional CVD risk factors as well as metaGRS, a GRS for CAD constructed with 1.7 million genetic variants, was tested with standard train-test machine learning approach using the LURIC data, which had the largest sample size., Results: CAC GRS was significantly associated with CAD in LURIC (OR=1.41, 95 % CI [1.28-1.55]), TVS (OR=1.79, 95 % CI [1.05-3.21]) as well as in TSDS (OR=4.20, 95 % CI [1.74-10.52]). CAC GRS showed strong association with calcification areas in left (OR=1.78, 95 % CI [1.16-2.74]) and right (OR=1.71, 95 % CI [1.98-2.67]) coronary arteries. There was statistically significant added predictive value of the CAC GRS for CAD over the used traditional CVD risk factors (AUC 0.734 vs 0.717, p-value = 0.02). Furthermore, CAC GRS improved the prediction accuracy for CAD when combined with metaGRS., Conclusions: This study showed that CAC GRS is a new risk marker for CAD in three European cohorts, with added predictive value over the traditional CVD risk factors., Competing Interests: The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (© 2024 The Authors.)

Published

2024

38. Bias in O-Information Estimation.

Author

Gehlen J, Li J, Hourican C, Tassi S, Mishra PP, Lehtimäki T, Kähönen M, Raitakari O, Bosch JA, and Quax R

Abstract

Higher-order relationships are a central concept in the science of complex systems. A popular method of attempting to estimate the higher-order relationships of synergy and redundancy from data is through the O-information. It is an information-theoretic measure composed of Shannon entropy terms that quantifies the balance between redundancy and synergy in a system. However, bias is not yet taken into account in the estimation of the O-information of discrete variables. In this paper, we explain where this bias comes from and explore it for fully synergistic, fully redundant, and fully independent simulated systems of n=3 variables. Specifically, we explore how the sample size and number of bins affect the bias in the O-information estimation. The main finding is that the O-information of independent systems is severely biased towards synergy if the sample size is smaller than the number of jointly possible observations. This could mean that triplets identified as highly synergistic may in fact be close to independent. A bias approximation based on the Miller-Maddow method is derived for the O-information. We find that for systems of n=3 variables the bias approximation can partially correct for the bias. However, simulations of fully independent systems are still required as null models to provide a benchmark of the bias of the O-information.

Published

2024

39. Association of Serum Trimethylamine-N-Oxide Concentration from Childhood to Early Adulthood with Age and Sex.

Author

Almer G, Enko D, Kartiosuo N, Niinikoski H, Lehtimäki T, Munukka E, Viikari J, Rönnemaa T, Rovio SP, Mykkänen J, Lagström H, Jula A, Herrmann M, Raitakari OT, Meinitzer A, and Pahkala K

Subjects

Humans, Female, Male, Child, Adolescent, Adult, Young Adult, Age Factors, Sex Factors, Child, Preschool, Infant, Biomarkers blood, Methylamines blood, Gastrointestinal Microbiome

Abstract

Background: Primary prevention is the cornerstone of cardiometabolic health. In the randomized, controlled Special Turku Coronary Risk Factor Intervention Project (STRIP), dietary counseling intervention was given to children from infancy to 20 years of age and a follow-up was completed at age 26 years. We investigated the associations of age, sex, gut microbiome, and dietary intervention with the gut metabolite and the cardiac biomarker trimethylamine-N-oxide (TMAO)., Methods: Overall, 592 healthy participants (females 46%) from STRIP were investigated. Compared to the control group, the intervention group had received dietary counseling between ages 7 months and 20 years focused on low intakes of saturated fat and cholesterol and the promotion of fruit, vegetable, and whole-grain consumption. TMAO serum concentrations were measured by a liquid chromatography-tandem mass spectrometry method at ages 11, 13, 15, 17, 19, and 26 years. Microbiome composition was assessed using 16S rRNA gene sequencing at 26 years of age., Results: TMAO concentrations increased from age 11 to 26 years in both sexes. At all measurement time points, males showed significantly higher serum TMAO concentrations compared to females, but concentrations were similar between the intervention and control groups. A direct association between TMAO concentrations and reported fiber intake was found in females. Gut microbiome analysis did not reveal associations with TMAO., Conclusions: TMAO concentration increased from childhood to early adulthood but was not affected by the given dietary intervention. In females, TMAO concentrations could be directly associated with higher fiber intake suggesting sex-specific differences in TMAO metabolism., (© Association for Diagnostics & Laboratory Medicine 2024.)

Published

2024

40. Prediction of Sudden Cardiac Death With Ultra-Short-Term Heart Rate Fluctuations.

Author

Hernesniemi JA, Pukkila T, Molkkari M, Nikus K, Lyytikäinen LP, Lehtimäki T, Viik J, Kähönen M, and Räsänen E

Subjects

Humans, Male, Female, Middle Aged, Prospective Studies, Aged, Risk Factors, Adult, Predictive Value of Tests, Death, Sudden, Cardiac epidemiology, Heart Rate physiology, Electrocardiography, Exercise Test

Abstract

Background: Conventional measures of heart rate variability (HRV) have shown only modest associations with sudden cardiac death (SCD). Detrended fluctuation analysis (DFA), with novel methodological developments to evaluate the short-term scaling exponent, is a potentially superior method compared to conventional HRV tools., Objectives: In this study, the authors studied the analysis of the association between DFA and SCD., Methods: The investigators studied the predictive value of ultra-short-term heart rate fluctuations (1-minute electrocardiogram samples) with DFA at rest and during different stages of physical exertion for incident SCD among 2,794 participants undergoing clinical exercise testing in the prospective FINCAVAS (Finnish Cardiovascular Study). The novel key DFA measure, the short-scale scaling exponent computed with second-order detrending (DFA2 α 1 ), was the main exposure variable. SCDs were defined by American Heart Association/European Society of Cardiology criteria using death certificates with written accounts of the events., Results: During a median follow-up of 8.3 years (Q1-Q3: 6.4-10.5), 83 SCDs occurred. DFA2 α 1 measured at rest (but not in exercise) associated highly significantly with the risk of SCD, with 1-SD lower values associating with a 2.4-fold (Q1-Q3: 2.0-3.0) risk (P < 0.001). The results persisted when adjusting for other major risk factors for SCD, including age, cardiovascular morbidities, cardiorespiratory fitness, heart rate reduction, and left ventricular ejection fraction. Associations between conventional HRV parameters (measured at any stage of exercise or at rest) and SCD were substantially weaker and statistically nonsignificant after adjusting for other risk factors., Conclusions: Ultra-short-term DFA2 α 1 , when measured at rest, is a powerful and independent predictor of SCD. The association between DFA2 α 1 and SCD is modified by physical exertion., Competing Interests: Funding Support and Author Disclosures FINCAVAS has been financially supported by the Competitive Research Funding of Tampere University Hospital (grants 9M048 and 9N035); the Finnish Cultural Foundation; the Finnish Foundation for Cardiovascular Research (to T.L); the Emil Aaltonen Foundation; the Tampere Tuberculosis Foundation, EU Horizon 2020 (grants 755320 for TAXINOMISIS and 848146 for To Aition); and the Academy of Finland (grant 322098). Additional funding has been also granted by Business Finland, R2B Funding 2022-23 (to E.R). The authors have reported that they have no relationships relevant to the contents of this paper to disclose., (Copyright © 2024 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2024

41. Childhood family environment and systemic haemodynamics in adulthood: the Cardiovascular Risk in Young Finns Study.

Author

KÄhÖnen E, LehtimÄki T, Raitakari OT, KÄhÖnen M, Hutri N, Keltikangas-JÄrvinen L, and Saarinen A

Abstract

Aims: Childhood family environment is associated with adulthood health behaviours and cardiovascular health, but limited data are available concerning the relationship between childhood family environment and adulthood haemodynamic determinants of blood pressure. We evaluated how childhood family environment predicts adulthood systemic haemodynamics., Methods: The sample came from the Cardiovascular Risk in Young Finns Study ( n =1554-1620). Childhood family environment (1980) was assessed with four cumulative risk scores: socioeconomic family risk, risky emotional family atmosphere, stressful life events, and parents' risky health behaviours. Haemodynamic outcomes in 2007 (participants being 30-45 year-olds) included stroke volume index, systemic vascular resistance index, cardiac output index and heart rate. Analyses were adjusted for childhood (1980) cardiovascular risk factors (high-density lipoprotein and low-density lipoprotein cholesterol, triglycerides, insulin, body mass index and systolic blood pressure); and adulthood (2007) health behaviours (alcohol consumption, smoking, physical activity); and finally for adulthood cardiovascular risk factors., Results: When adjusted for age and sex, high socioeconomic family risk predicted lower stroke volume index ( P =0.001), higher heart rate ( P =0.001) and higher systemic vascular resistance index ( P =0.030). These associations remained after controlling for childhood cardiovascular covariates or adulthood health behaviours ( P ⩽0.02 for all) but diluted after controlling for adulthood cardiovascular risk factors. The other childhood cumulative risk scores (stressful life events, risky emotional atmosphere, or parents' risky health behaviour) did not predict adulthood haemodynamic outcomes., Conclusions: High childhood socioeconomic family risk predicted adulthood haemodynamic outcomes independently of childhood cardiovascular risk factors and adulthood health behaviours, while other childhood psychosocial adversities were not associated with cardiovascular function in adulthood., Competing Interests: Declaration of conflicting interestsThe author(s) declared no potential conflicts of interest with respect to the research, authorship, and/or publication of this article.

Published

2024

42. Association of inflammatory cytokines with lung function, chronic lung diseases, and COVID-19.

Author

Rontogianni MO, Gill D, Bouras E, Asimakopoulos AG, Tzoulaki I, Karhunen V, Lehtimäki T, Raitakari O, Wielscher M, Salomaa V, Jalkanen S, Salmi M, Timonen M, Yarmolinsky J, Chen J, Tobin MD, Izquierdo AG, Herzig KH, Ioannides AE, Jarvelin MR, Dehghan A, and Tsilidis KK

Abstract

We investigated the effects of 35 inflammatory cytokines on respiratory outcomes, including COVID-19, asthma (atopic and non-atopic), chronic obstructive pulmonary disease (COPD), and pulmonary function indices, using Mendelian randomization and colocalization analyses. The emerging associations were further explored using observational analyses in the UK Biobank. We found an inverse association between genetically predicted macrophage colony stimulating factor (MCSF), soluble intercellular adhesion molecule-1 (sICAM), and soluble vascular cell adhesion molecule-1 with risk of COVID-19 outcomes. sICAM was positively associated with atopic asthma risk, whereas tumor necrosis factor-alfa showed an inverse association. A positive association was shown between interleukin-18 and COPD risk (replicated in observational analysis), whereas an inverse association was shown for interleukin-1 receptor antagonist (IL-1ra). IL-1ra and monocyte chemotactic protein-3 were positively associated with lung function indices, whereas inverse associations were shown for MCSF and interleukin-18 (replicated in observational analysis). Our results point to these cytokines as potential pharmacological targets for respiratory traits., Competing Interests: The authors declare the following competing interests: Salomaa Veikko was funded by the Finnish Foundation for Cardiovascular Research and by the Juho Vainio Foundation. Salomaa Veikko has received an honorarium from Sanofi for consulting and has ongoing research collaboration with Bayer Ltd. (All outside the present study). These companies had no role in study design, data collection and analysis, decision to publish, or preparation of the article. Sirpa Jalkanen, Marko Salmi: Financial support for cytokine analyses has come from the Finnish Academy. Abril Izquierdo and Martin Tobin were supported for the present article by Wellcome Trust grants (WT202849/Z/16/Z, WT225221/Z/22/Z) and the National Institute of Health and Care Research (NIHR) Leicester Biomedical Research Center. Martin Tobin has also received an NIHR Senior Investigator Award and had a funded research collaboration with Orion Pharma (the latter outside the scope of this work). Markku Timonen has received payment for one lecture for Otsuka Pharmaceutical and payment for two lectures for H. Lundbeck A/S. Marjo-Ritta Jarvelin is partly funded by the Medical Research Council (MR/S019669/1). James Yarmolinsky is supported by a Cancer Research UK Population Research Postdoctoral Fellowship (C68933/A28534). The remaining authors have no competing interests to declare., (© 2024 The Author(s).)

Published

2024

43. Predicting early-stage coronary artery disease using machine learning and routine clinical biomarkers improved by augmented virtual data.

Author

Koloi A, Loukas VS, Hourican C, Sakellarios AI, Quax R, Mishra PP, Lehtimäki T, Raitakari OT, Papaloukas C, Bosch JA, März W, and Fotiadis DI

Abstract

Aims: Coronary artery disease (CAD) is a highly prevalent disease with modifiable risk factors. In patients with suspected obstructive CAD, evaluating the pre-test probability model is crucial for diagnosis, although its accuracy remains controversial. Machine learning (ML) predictive models can help clinicians detect CAD early and improve outcomes. This study aimed to identify early-stage CAD using ML in conjunction with a panel of clinical and laboratory tests., Methods and Results: The study sample included 3316 patients enrolled in the Ludwigshafen Risk and Cardiovascular Health (LURIC) study. A comprehensive array of attributes was considered, and an ML pipeline was developed. Subsequently, we utilized five approaches to generating high-quality virtual patient data to improve the performance of the artificial intelligence models. An extension study was carried out using data from the Young Finns Study (YFS) to assess the results' generalizability. Upon applying virtual augmented data, accuracy increased by approximately 5%, from 0.75 to -0.79 for random forests (RFs), and from 0.76 to -0.80 for Gradient Boosting (GB). Sensitivity showed a significant boost for RFs, rising by about 9.4% (0.81-0.89), while GB exhibited a 4.8% increase (0.83-0.87). Specificity showed a significant boost for RFs, rising by ∼24% (from 0.55 to 0.70), while GB exhibited a 37% increase (from 0.51 to 0.74). The extension analysis aligned with the initial study., Conclusion: Accurate predictions of angiographic CAD can be obtained using a set of routine laboratory markers, age, sex, and smoking status, holding the potential to limit the need for invasive diagnostic techniques. The extension analysis in the YFS demonstrated the potential of these findings in a younger population, and it confirmed applicability to atherosclerotic vascular disease., Competing Interests: Conflict of interest: none declared., (© The Author(s) 2024. Published by Oxford University Press on behalf of the European Society of Cardiology.)

Published

2024

44. Polymorphisms in ERBB4 and TACR1 associated with dry mouth in clozapine-treated patients.

Author

Puolakka H, Solismaa A, Lyytikäinen LP, Viikki M, Seppälä N, Mononen N, Lehtimäki T, and Kampman O

Subjects

Humans, Female, Male, Adult, Middle Aged, Genotype, Schizophrenia drug therapy, Schizophrenia genetics, Clozapine adverse effects, Polymorphism, Single Nucleotide, Antipsychotic Agents adverse effects, Receptor, ErbB-4 genetics, Xerostomia chemically induced, Xerostomia genetics, Sialorrhea chemically induced, Sialorrhea genetics, Receptors, Neurokinin-1 genetics, Receptors, Neurokinin-1 metabolism

Abstract

Background: Sialorrhea is a common and uncomfortable adverse effect of clozapine, and its severity varies between patients. The aim of the study was to select broadly genes related to the regulation of salivation and study associations between sialorrhea and dry mouth and polymorphisms in the selected genes., Methods: The study population consists of 237 clozapine-treated patients, of which 172 were genotyped. Associations between sialorrhea and dry mouth with age, sex, BMI, smoking, clozapine dose, clozapine and norclozapine serum levels, and other comedication were studied. Genetic associations were analyzed with linear and logistic regression models explaining sialorrhea and dry mouth with each SNP added separately to the model as coefficients., Results: Clozapine dose, clozapine or norclozapine concentration and their ratio were not associated with sialorrhea or dryness of mouth. Valproate use ( p = 0.013) and use of other antipsychotics ( p = 0.015) combined with clozapine were associated with excessive salivation. No associations were found between studied polymorphisms and sialorrhea. In analyses explaining dry mouth with logistic regression with age and sex as coefficients, two proxy-SNPs were associated with dry mouth: epidermal growth factor receptor 4 (ERBB4) rs3942465 (adjusted p = 0.025) and tachykinin receptor 1 (TACR1) rs58933792 (adjusted p = 0.029)., Conclusion: Use of valproate or antipsychotic polypharmacy may increase the risk of sialorrhea. Genetic variations in ERBB4 and TACR1 might contribute to experienced dryness of mouth among patients treated with clozapine.

Published

2024

45. A Large-Scale Genome-Wide Study of Gene-Sleep Duration Interactions for Blood Pressure in 811,405 Individuals from Diverse Populations.

Author

Wang H, Nagarajan P, Winkler T, Bentley A, Miller C, Kraja A, Schwander K, Lee S, Wang W, Brown M, Morrison J, Giri A, O'Connell J, Bartz T, de las Fuentes L, Gudmundsdottir V, Guo X, Harris S, Huang Z, Kals M, Kho M, Lefevre C, Luan J, Lyytikäinen LP, Mangino M, Milaneschi Y, Palmer N, Rao V, Rauramaa R, Shen B, Stadler S, Sun Q, Tang J, Thériault S, van der Graaf A, van der Most P, Wang Y, Weiss S, Westerman K, Yang Q, Yasuharu T, Zhao W, Zhu W, Altschul D, Ansari MAY, Anugu P, Argoty-Pantoja A, Arzt M, Aschard H, Attia J, Bazzano L, Breyer M, Brody J, Cade B, Chen HH, Chen YI, Chen Z, de Vries P, Dimitrov L, Do A, Du J, Dupont C, Edwards T, Evans M, Faquih T, Felix S, Fisher-Hoch S, Floyd J, Graff M, Charles Gu C, Gu D, Hairston K, Hanley A, Heid I, Heikkinen S, Highland H, Hood M, Kähönen M, Karvonen-Gutierrez C, Kawaguchi T, Kazuya S, Tanika K, Komulainen P, Levy D, Lin H, Liu P, Marques-Vidal P, McCormick J, Mei H, Meigs J, Menni C, Nam K, Nolte I, Pacheco N, Petty L, Polikowsky H, Province M, Psaty B, Raffield L, Raitakari O, Rich S, Riha R, Risch L, Risch M, Ruiz-Narvaez E, Scott R, Sitlani C, Smith J, Sofer T, Teder-Laving M, Völker U, Vollenweider P, Wang G, van Dijk KW, Wilson O, Xia R, Yao J, Young K, Zhang R, Zhu X, Below J, Böger C, Conen D, Cox S, Dörr M, Feitosa M, Fox E, Franceschini N, Gharib S, Gudnason V, Harlow S, He J, Holliday E, Kutalik Z, Lakka T, Lawlor D, Lee S, Lehtimäki T, Li C, Liu CT, Mägi R, Matsuda F, Morrison A, Penninx BWJH, Peyser P, Rotter J, Snieder H, Spector T, Wagenknecht L, Wareham N, Zonderman A, North K, Fornage M, Hung A, Manning A, Gauderman W, Chen H, Munroe P, Rao D, van Heemst D, Redline S, and Noordam R

Abstract

Although both short and long sleep duration are associated with elevated hypertension risk, our understanding of their interplay with biological pathways governing blood pressure remains limited. To address this, we carried out genome-wide cross-population gene-by-short-sleep and long-sleep duration interaction analyses for three blood pressure traits (systolic, diastolic, and pulse pressure) in 811,405 individuals from diverse population groups. We discover 22 novel gene-sleep duration interaction loci for blood pressure, mapped to 23 genes. Investigating these genes' functional implications shed light on neurological, thyroidal, bone metabolism, and hematopoietic pathways that necessitate future investigation for blood pressure management that caters to sleep health lifestyle. Non-overlap between short sleep (12) and long sleep (10) interactions underscores the plausible nature of distinct influences of both sleep duration extremes in cardiovascular health. Several of our loci are specific towards a particular population background or sex, emphasizing the importance of addressing heterogeneity entangled in gene-environment interactions, when considering precision medicine design approaches for blood pressure management., Competing Interests: Declarations CONFLICT OF INTEREST C.L.M. has received funding from AstraZeneca not related to the current study. B.M.P. serves on the steering committee of the Yale Open Data Access Project funded by Johnson & Johnson. D.C. receives consultancy fees from Roche Diagnostics and Trimedics and speaker fees from Servier. D.A.L. has received support from Medtronic LTD and Roche Diagnostics for biomarker research not related to the current study. The remaining authors declare no competing interests.

Published

2024

46. Gene expression networks regulated by human personality.

Author

Del Val C, Díaz de la Guardia-Bolívar E, Zwir I, Mishra PP, Mesa A, Salas R, Poblete GF, de Erausquin G, Raitoharju E, Kähönen M, Raitakari O, Keltikangas-Järvinen L, Lehtimäki T, and Cloninger CR

Subjects

Humans, Adult, Female, Male, Transcriptome genetics, MicroRNAs genetics, MicroRNAs metabolism, Gene Expression Profiling methods, Young Adult, Gene Expression Regulation genetics, Gene Regulatory Networks genetics, Personality genetics, Personality physiology, Brain metabolism, Genome-Wide Association Study methods

Abstract

Genome-wide association studies of human personality have been carried out, but transcription of the whole genome has not been studied in relation to personality in humans. We collected genome-wide expression profiles of adults to characterize the regulation of expression and function in genes related to human personality. We devised an innovative multi-omic approach to network analysis to identify the key control elements and interactions in multi-modular networks. We identified sets of transcribed genes that were co-expressed in specific brain regions with genes known to be associated with personality. Then we identified the minimum networks for the co-localized genes using bioinformatic resources. Subjects were 459 adults from the Young Finns Study who completed the Temperament and Character Inventory and provided peripheral blood for genomic and transcriptomic analysis. We identified an extrinsic network of 45 regulatory genes from seed genes in brain regions involved in self-regulation of emotional reactivity to extracellular stimuli (e.g., self-regulation of anxiety) and an intrinsic network of 43 regulatory genes from seed genes in brain regions involved in self-regulation of interpretations of meaning (e.g., production of concepts and language). We discovered that interactions between the two networks were coordinated by a control hub of 3 miRNAs and 3 protein-coding genes shared by both. Interactions of the control hub with proteins and ncRNAs identified more than 100 genes that overlap directly with known personality-related genes and more than another 4000 genes that interact indirectly. We conclude that the six-gene hub is the crux of an integrative network that orchestrates information-transfer throughout a multi-modular system of over 4000 genes enriched in liquid-liquid-phase-separation (LLPS)-related RNAs, diverse transcription factors, and hominid-specific miRNAs and lncRNAs. Gene expression networks associated with human personality regulate neuronal plasticity, epigenesis, and adaptive functioning by the interactions of salience and meaning in self-awareness., (© 2024. The Author(s).)

Published

2024

47. Association of Ideal Cardiovascular Health in Youth with Cancer Risk in Adulthood: A Cardiovascular Risk in Young Finns Study.

Author

Niemelä J, Nuotio J, Laitinen TT, Kähönen M, Hutri N, Lehtimäki T, Jokinen E, Tossavainen P, Laitinen TP, Heinonen OJ, Dwyer T, Pahkala K, Rovio SP, Viikari J, Raitakari O, and Juonala M

Subjects

Humans, Female, Male, Adolescent, Young Adult, Finland epidemiology, Incidence, Child, Exercise, Risk Factors, Adult, Life Style, Follow-Up Studies, Neoplasms epidemiology, Neoplasms etiology, Cardiovascular Diseases epidemiology, Cardiovascular Diseases etiology

Abstract

Background: Lifestyle factors may affect cancer risk. This study aimed to identify whether the American Heart Association ideal cardiovascular health (ICH) score and its individual variables in youth are associated with subsequent cancer incidence., Methods: This study comprised participants of the Cardiovascular Risk in Young Finns Study free of cancer at the analysis baseline in 1986 (n = 1,873). The baseline age was 12 to 24 years, and the follow-up occurred between 1986 and 2018., Results: Among 1,873 participants (mean age 17.3 ± 4.1 years; 53.4% females at baseline), 72 incident cancer cases occurred during the follow-up (mean follow-up time 31.4 ± 3.4 years). Baseline ICH score was not associated with future cancer risk (HR, 0.96; 95% confidence interval, 0.78-1.12 per 1-point increment). Of individual ICH score variables, ideal physical activity (PA) was inversely associated with cancer incidence [age- and sex-adjusted HR, 0.45 (0.23-0.88) per 1-category change (nonideal/ideal)] and remained significant in the multivariable-adjusted model, including body mass index, smoking, diet, and socioeconomic status. A continuous PA index at ages 9 to 24 years and moderate-to-vigorous PA in youth were also related to decreased cancer incidence (P < 0.05). Body mass index, smoking, diet, total cholesterol, glucose, and blood pressure were not related to cancer risk. Of the dietary components, meat consumption was associated with cancer incidence (P = 0.023)., Conclusions: These findings indicate that higher PA levels in youth are associated with a reduced subsequent cancer incidence, whereas the American Heart Association's ICH score in youth does not., Impact: This finding supports efforts to promote a healthy lifestyle and encourages PA during childhood, yielding a subsequent healthier life., (©2024 American Association for Cancer Research.)

Published

2024

48. NMR metabolomic modeling of age and lifespan: A multicohort analysis.

Author

Lau CE, Manou M, Markozannes G, Ala-Korpela M, Ben-Shlomo Y, Chaturvedi N, Engmann J, Gentry-Maharaj A, Herzig KH, Hingorani A, Järvelin MR, Kähönen M, Kivimäki M, Lehtimäki T, Marttila S, Menon U, Munroe PB, Palaniswamy S, Providencia R, Raitakari O, Schmidt AF, Sebert S, Wong A, Vineis P, Tzoulaki I, and Robinson O

Subjects

Humans, Aged, Middle Aged, Aged, 80 and over, Adult, Male, Female, Longevity, Cohort Studies, Young Adult, Risk Factors, Finland epidemiology, Metabolomics methods, Aging, Magnetic Resonance Spectroscopy methods

Abstract

Metabolomic age models have been proposed for the study of biological aging, however, they have not been widely validated. We aimed to assess the performance of newly developed and existing nuclear magnetic resonance spectroscopy (NMR) metabolomic age models for prediction of chronological age (CA), mortality, and age-related disease. Ninety-eight metabolic variables were measured in blood from nine UK and Finnish cohort studies (N ≈31,000 individuals, age range 24-86 years). We used nonlinear and penalized regression to model CA and time to all-cause mortality. We examined associations of four new and two previously published metabolomic age models, with aging risk factors and phenotypes. Within the UK Biobank (N ≈102,000), we tested prediction of CA, incident disease (cardiovascular disease (CVD), type-2 diabetes mellitus, cancer, dementia, and chronic obstructive pulmonary disease), and all-cause mortality. Seven-fold cross-validated Pearson's r between metabolomic age models and CA ranged between 0.47 and 0.65 in the training cohort set (mean absolute error: 8-9 years). Metabolomic age models, adjusted for CA, were associated with C-reactive protein, and inversely associated with glomerular filtration rate. Positively associated risk factors included obesity, diabetes, smoking, and physical inactivity. In UK Biobank, correlations of metabolomic age with CA were modest (r = 0.29-0.33), yet all metabolomic model scores predicted mortality (hazard ratios of 1.01 to 1.06/metabolomic age year) and CVD, after adjustment for CA. While metabolomic age models were only moderately associated with CA in an independent population, they provided additional prediction of morbidity and mortality over CA itself, suggesting their wider applicability., (© 2024 The Authors. Aging Cell published by Anatomical Society and John Wiley & Sons Ltd.)

Published

2024

49. Polygenic risk for schizophrenia predicting social trajectories in a general population sample.

Author

Saarinen A, Hietala J, Lyytikäinen LP, Hamal Mishra B, Sormunen E, Lavonius V, Kähönen M, Raitakari O, Lehtimäki T, and Keltikangas-Järvinen L

Subjects

Humans, Male, Female, Adult, Adolescent, Young Adult, Finland epidemiology, Middle Aged, Genetic Predisposition to Disease, Psychotic Disorders genetics, Psychotic Disorders epidemiology, Depressive Disorder, Major genetics, Depressive Disorder, Major epidemiology, Risk Factors, Child, Schizophrenia genetics, Multifactorial Inheritance, Social Support

Abstract

Background: We investigated (a) whether polygenic risk for schizophrenia predicts different trajectories of social development among those who have not developed psychoses and (b) whether possible associations are PRS SCZ -specific or evident also for any polygenic risk for mental disorders, e.g. for major depression., Methods: Participants came from the population-based Young Finns Study ( n = 2377). We calculated a polygenic risk score for schizophrenia (PRS SCZ ) and for major depression (PRS DEP ). Diagnoses of psychotic disorders were derived from the hospital care register. Social development from adolescence to middle age was measured by (a) perceived social support from friends, family, and a close other, (b) perceived sociability, and (c) family structure (partnership status, number of children, age of first-time parenthood)., Results: Among those without manifest psychoses, high PRS SCZ predicted lower experienced support from friends ( B = -0.04, p = 0.009-0.035) and family ( B = -0.04, p = 0.009-0.035) especially after early adulthood, and also lower perceived sociability ( B = -0.05, p = 0.010-0.026). PRS SCZ was not related to family structure. PRS DEP did not predict any domain of social development., Conclusions: Individuals at high PRS SCZ (not converted to psychosis) seem to experience a lower preference to be with others over being alone. Individuals with high ( v. low) PRS SCZ seem to have a similar family structure in terms of partnership status or number of children but, nevertheless, they experience less support from their family. Among those not converted to psychosis in a typical age period, high PRS SCZ may predict a 'later risk phase' and reduced functional resilience when approaching middle age.

Published

2024

50. Metabolic syndrome and epigenetic aging: a twin study.

Author

Föhr T, Hendrix A, Kankaanpää A, Laakkonen EK, Kujala U, Pietiläinen KH, Lehtimäki T, Kähönen M, Raitakari O, Wang X, Kaprio J, Ollikainen M, and Sillanpää E

Subjects

Humans, Middle Aged, Female, Male, Adult, Aged, DNA Methylation genetics, Young Adult, Life Style, Aging, Premature genetics, Metabolic Syndrome genetics, Metabolic Syndrome epidemiology, Epigenesis, Genetic, Aging genetics, Aging physiology

Abstract

Background: Metabolic syndrome (MetS) is associated with premature aging, but whether this association is driven by genetic or lifestyle factors remains unclear., Methods: Two independent discovery cohorts, consisting of twins and unrelated individuals, were examined (N = 268, aged 23-69 years). The findings were replicated in two cohorts from the same base population. One consisted of unrelated individuals (N = 1 564), and the other of twins (N = 293). Participants' epigenetic age, estimated using blood DNA methylation data, was determined using the epigenetic clocks GrimAge and DunedinPACE. The individual-level linear regression models for investigating the associations of MetS and its components with epigenetic aging were followed by within-twin-pair analyses using fixed-effects regression models to account for genetic factors., Results: In individual-level analyses, GrimAge age acceleration was higher among participants with MetS (N = 56) compared to participants without MetS (N = 212) (mean 2.078 [95% CI = 0.996,3.160] years vs. -0.549 [-1.053,-0.045] years, between-group p = 3.5E-5). Likewise, the DunedinPACE estimate was higher among the participants with MetS compared to the participants without MetS (1.032 [1.002,1.063] years/calendar year vs. 0.911 [0.896,0.927] years/calendar year, p = 4.8E-11). An adverse profile in terms of specific MetS components was associated with accelerated aging. However, adjustments for lifestyle attenuated these associations; nevertheless, for DunedinPACE, they remained statistically significant. The within-twin-pair analyses suggested that genetics explains these associations fully for GrimAge and partly for DunedinPACE. The replication analyses provided additional evidence that the association between MetS components and accelerated aging is independent of the lifestyle factors considered in this study, however, suggesting that genetics is a significant confounder in this association., Conclusions: The results of this study suggests that MetS is associated with accelerated epigenetic aging, independent of physical activity, smoking or alcohol consumption, and that the association may be explained by genetics., (© 2024. The Author(s).)

Published

2024