282 results on '"Omholt, Stig"'
Search Results
2. Aging as a consequence of selection to reduce the environmental risk of dying
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Omholt, Stig W. and Kirkwood, Thomas B. L.
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- 2021
3. Interstitial solute transport in 3D reconstructed neuropil occurs by diffusion rather than bulk flow
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Holter, Karl Erik, Kehlet, Benjamin, Devor, Anna, Sejnowski, Terrence J, Dale, Anders M, Omholt, Stig W, Ottersen, Ole Petter, Nagelhus, Erlend Arnulf, Mardal, Kent-André, and Pettersen, Klas H
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Neurosciences ,Animals ,Biological Transport ,Blood-Brain Barrier ,Body Fluids ,Cerebrospinal Fluid ,Computer Simulation ,Diffusion ,Extracellular Fluid ,Hippocampus ,Humans ,Imaging ,Three-Dimensional ,Lymphatic Vessels ,Microscopy ,Electron ,Neuropil ,glymphatic ,interstitial fluid ,extracellular space ,simulation ,AQP4 - Abstract
The brain lacks lymph vessels and must rely on other mechanisms for clearance of waste products, including amyloid [Formula: see text] that may form pathological aggregates if not effectively cleared. It has been proposed that flow of interstitial fluid through the brain's interstitial space provides a mechanism for waste clearance. Here we compute the permeability and simulate pressure-mediated bulk flow through 3D electron microscope (EM) reconstructions of interstitial space. The space was divided into sheets (i.e., space between two parallel membranes) and tunnels (where three or more membranes meet). Simulation results indicate that even for larger extracellular volume fractions than what is reported for sleep and for geometries with a high tunnel volume fraction, the permeability was too low to allow for any substantial bulk flow at physiological hydrostatic pressure gradients. For two different geometries with the same extracellular volume fraction the geometry with the most tunnel volume had [Formula: see text] higher permeability, but the bulk flow was still insignificant. These simulation results suggest that even large molecule solutes would be more easily cleared from the brain interstitium by diffusion than by bulk flow. Thus, diffusion within the interstitial space combined with advection along vessels is likely to substitute for the lymphatic drainage system in other organs.
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- 2017
4. Containing pandemics through targeted testing of households
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Voigt, André, Martyushenko, Nikolay, Karlsen, Emil, Hall, Martina, Nyhamar, Kristen, Omholt, Stig William, and Almaas, Eivind
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- 2021
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5. Correction to: Containing pandemics through targeted testing of households
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Voigt, André, Martyushenko, Nikolay, Karlsen, Emil, Hall, Martina, Nyhamar, Kristen, Omholt, Stig William, and Almaas, Eivind
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- 2021
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6. Arterial stiffening provides sufficient explanation for primary hypertension
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Pettersen, Klas H., Bugenhagen, Scott M., Nauman, Javaid, Beard, Daniel A., and Omholt, Stig W.
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Quantitative Biology - Tissues and Organs ,92C30 - Abstract
Hypertension is one of the most common age-related chronic diseases and by predisposing individuals for heart failure, stroke and kidney disease, it is a major source of morbidity and mortality. Its etiology remains enigmatic despite intense research efforts over many decades. By use of empirically well-constrained computer models describing the coupled function of the baroreceptor reflex and mechanics of the circulatory system, we demonstrate quantitatively that arterial stiffening seems sufficient to explain age-related emergence of hypertension. Specifically, the empirically observed chronic changes in pulse pressure with age, and the impaired capacity of hypertensive individuals to regulate short-term changes in blood pressure, arise as emergent properties of the integrated system. Results are consistent with available experimental data from chemical and surgical manipulation of the cardio-vascular system. In contrast to widely held opinions, the results suggest that primary hypertension can be attributed to a mechanogenic etiology without challenging current conceptions of renal and sympathetic nervous system function. The results support the view that a major target for treating chronic hypertension in the elderly is the reestablishment of a proper baroreflex response., Comment: 19 pages, 4 figures
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- 2013
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7. Electrodiffusive model for astrocytic and neuronal ion concentration dynamics
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Halnes, Geir, Østby, Ivar, Pettersen, Klas H., Omholt, Stig W., and Einevoll, Gaute T.
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Quantitative Biology - Cell Behavior ,Quantitative Biology - Subcellular Processes ,92C05 - Abstract
Electrical neural signalling typically takes place at the time-scale of milliseconds, and is typically modeled using the cable equation. This is a good approximation for processes when ionic concentrations vary little during the time course of a simulation. During periods of intense neural signalling, however, the local extracellular K+ concentration may increase by several millimolars. Clearance of excess K+ likely depends partly on diffusion in the extracellular space, partly on local uptake by- and intracellular transport within astrocytes. This process takes place at the time scale of seconds, and can not be modeled accurately without accounting for the spatiotemporal variations in ion concentrations. The work presented here consists of two main parts: First, we developed a general electrodiffusive formalism for modeling ion concentration dynamics in a one-dimensional geometry, including both an intra- and extracellular domain. The formalism was based on the Nernst-Planck equations. It ensures (i) consistency between the membrane potential and ion concentrations, (ii) global particle/charge conservation, and (iii) accounts for diffusion and concentration dependent variations in resistivities. Second, we applied the formalism to model how astrocytes exchange ions with the ECS, and identified the key astrocytic mechanisms involved in K+ removal from high concentration regions. We found that a local increase in extracellular K\textsuperscript{+} evoked a local depolarization of the astrocyte membrane, which at the same time (i) increased the local astrocytic uptake of K\textsuperscript{+}, (ii) suppressed extracellular transport of K+, (iii) increased transport of K+ within astrocytes, and (iv) facilitated astrocytic relase of K+ in extracellular low concentration regions. In summary, these mechanisms seem optimal for shielding the extracellular space from excess K+., Comment: 19 pages, 5 figures, 1 table (Equations 37 & 38 and the two first equations in Figure 2 were corrected May 30th 2013)
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- 2013
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8. Social Exploitation of Vitellogenin
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Amdam, Gro V., Norberg, Kari, Hagen, Arne, and Omholt, Stig W.
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- 2003
9. Wearable technology and the cardiovascular system: the future of patient assessment
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Williams, Gareth J., Al-Baraikan, Abdulaziz, Rademakers, Frank E., Ciravegna, Fabio, van de Vosse, Frans N., Lawrie, Allan, Rothman, Alexander, Ashley, Euan A., Wilkins, Martin R., Lawford, Patricia V., Omholt, Stig W., Wisløff, Ulrik, Hose, D. Rodney, Chico, Timothy J.A., Gunn, Julian P., Morris, Paul D., Williams, Gareth J., Al-Baraikan, Abdulaziz, Rademakers, Frank E., Ciravegna, Fabio, van de Vosse, Frans N., Lawrie, Allan, Rothman, Alexander, Ashley, Euan A., Wilkins, Martin R., Lawford, Patricia V., Omholt, Stig W., Wisløff, Ulrik, Hose, D. Rodney, Chico, Timothy J.A., Gunn, Julian P., and Morris, Paul D.
- Abstract
The past decade has seen a dramatic rise in consumer technologies able to monitor a variety of cardiovascular parameters. Such devices initially recorded markers of exercise, but now include physiological and health-care focused measurements. The public are keen to adopt these devices in the belief that they are useful to identify and monitor cardiovascular disease. Clinicians are therefore often presented with health app data accompanied by a diverse range of concerns and queries. Herein, we assess whether these devices are accurate, their outputs validated, and whether they are suitable for professionals to make management decisions. We review underpinning methods and technologies and explore the evidence supporting the use of these devices as diagnostic and monitoring tools in hypertension, arrhythmia, heart failure, coronary artery disease, pulmonary hypertension, and valvular heart disease. Used correctly, they might improve health care and support research.
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- 2023
10. The Atlantic salmon genome provides insights into rediploidization
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Lien, Sigbjørn, Koop, Ben F., Sandve, Simen R., Miller, Jason R., Kent, Matthew P., Nome, Torfinn, Hvidsten, Torgeir R., Leong, Jong S., Minkley, David R., Zimin, Aleksey, Grammes, Fabian, Grove, Harald, Gjuvsland, Arne, Walenz, Brian, Hermansen, Russell A., von Schalburg, Kris, Rondeau, Eric B., Di Genova, Alex, Samy, Jeevan K. A., Olav Vik, Jon, Vigeland, Magnus D., Caler, Lis, Grimholt, Unni, Jentoft, Sissel, Inge Våge, Dag, de Jong, Pieter, Moen, Thomas, Baranski, Matthew, Palti, Yniv, Smith, Douglas R., Yorke, James A., Nederbragt, Alexander J., Tooming-Klunderud, Ave, Jakobsen, Kjetill S., Jiang, Xuanting, Fan, Dingding, Hu, Yan, Liberles, David A., Vidal, Rodrigo, Iturra, Patricia, Jones, Steven J. M., Jonassen, Inge, Maass, Alejandro, Omholt, Stig W., and Davidson, William S.
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- 2016
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11. Genetically controlled mtDNA deletions prevent ROS damage by arresting oxidative phosphorylation
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Stenberg, Simon, primary, Li, Jing, additional, Gjuvsland, Arne B, additional, Persson, Karl, additional, Demitz-Helin, Erik, additional, González Peña, Carles, additional, Yue, Jia-Xing, additional, Gilchrist, Ciaran, additional, Ärengård, Timmy, additional, Ghiaci, Payam, additional, Larsson-Berglund, Lisa, additional, Zackrisson, Martin, additional, Smits, Silvana, additional, Hallin, Johan, additional, Höög, Johanna L, additional, Molin, Mikael, additional, Liti, Gianni, additional, Omholt, Stig W, additional, and Warringer, Jonas, additional
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- 2022
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12. Life-History Evolution and the Polyphenic Regulation of Somatic Maintenance and Survival
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Flatt, Thomas, Amdam, Gro V., Kirkwood, Thomas B. L., and Omholt, Stig W.
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- 2013
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13. Genetically controlled mtDNA deletions prevent ROS damage by arresting oxidative phosphorylation
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Stenberg, Ulf Simon, Li, Jing, Gjuvsland, Arne Bjørke, Persson, Karl, Demitz-Helin, Erik, Gonzalez-Pena, Carles, Yue, Jia-Xing, Gilchrist, Ciaran, Ärengård, Timmy, Ghiaci, Payam, Larsson-Berglund, Lisa, Zackrisson, Martin, Smits, Silvana, Hallin, Johan, Höög, Johanna L., Molin, Mikael, Liti, Gianni, Omholt, Stig William, and Warringer, Jonas
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- 2022
14. Bestandsestimering av hjort ved bruk av jegerrapporterte data - Presentasjon av en kjønns- og stadium-strukturert dynamisk populasjonsmodell
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Omholt, Stig William and Meisingset, Erling L.
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Hjort ,hjortebestand ,Viltøkologi ,population modelling ,hunting ,modellering ,jakt ,Red deer - Abstract
I denne rapporten viser vi at jegerrapporterte data gir mulighet for robust bestandsestimering av hjort basert på modellgenererte populasjonsforløp og derved mulighet for framskriving av bestandsutvikling som funksjon av jaktuttak. Tidsseriedataene, populasjonsmodellen og metoden for sammenstilling definerer til sammen en estimeringsmodell. Med utgangspunkt i data fra kommunene Averøy, Tingvoll, Surnadal og Sunndal i Møre og Romsdal viser vi hvordan en slik estimeringsmodell kan brukes til å få robuste anslag for størrelse og sammensetning av hjortebestandene på lokalt nivå. Bestandsestimering av hjort ved bruk av jegerrapporterte data - Presentasjon av en kjønns- og stadium-strukturert dynamisk populasjonsmodell
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- 2022
15. A vision and strategy for the virtual physiological human in 2010 and beyond
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Hunter, Peter, Coveney, Peter V., de Bono, Bernard, Diaz, Vanessa, Fenner, John, Frangi, Alejandro F., Harris, Peter, Hose, Rod, Kohl, Peter, Lawford, Pat, McCormack, Keith, Mendes, Miriam, Omholt, Stig, Quarteroni, Alfio, Skår, John, Tegner, Jesper, Thomas, S. Randall, Tollis, Ioannis, Tsamardinos, Ioannis, VAN Beek, Johannes H. G. M., and Viceconti, Marco
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- 2010
16. Disentangling genetic and epigenetic determinants of ultrafast adaptation
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Gjuvsland, Arne B, Zörgö, Enikö, Samy, Jeevan KA, Stenberg, Simon, Demirsoy, Ibrahim H, Roque, Francisco, Maciaszczyk‐Dziubinska, Ewa, Migocka, Magdalena, Alonso‐Perez, Elisa, Zackrisson, Martin, Wysocki, Robert, Tamás, Markus J, Jonassen, Inge, Omholt, Stig W, and Warringer, Jonas
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- 2016
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17. Comparing the impact of vaccination strategies on the spread of COVID-19, including a novel household-targeted vaccination strategy
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Voigt, André, primary, Omholt, Stig, additional, and Almaas, Eivind, additional
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- 2022
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18. Genetic Variation in Putative Regulatory Loci Controlling Gene Expression in Breast Cancer
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Kristensen, Vessela N., Edvardsen, Hege, Tsalenko, Anya, Nordgard, Silje H., Sørlie, Therese, Sharan, Roded, Vailaya, Aditya, Ben-Dor, Amir, Lønning, Per Eystein, Lien, Sigbjørn, Omholt, Stig, Syvänen, Ann-Christine, Yakhini, Zohar, and Børresen-Dale, Anne-Lise
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- 2006
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19. Concerted Evolution of Life Stage Performances Signals Recent Selection on Yeast Nitrogen Use
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Ibstedt, Sebastian, Stenberg, Simon, Bagés, Sara, Gjuvsland, Arne B., Salinas, Francisco, Kourtchenko, Olga, Samy, Jeevan K.A., Blomberg, Anders, Omholt, Stig W., Liti, Gianni, Beltran, Gemma, and Warringer, Jonas
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- 2015
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20. Additional file 1 of Containing pandemics through targeted testing of households
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Voigt, André, Martyushenko, Nikolay, Karlsen, Emil, Hall, Martina, Nyhamar, Kristen, Omholt, Stig William, and Almaas, Eivind
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Data_FILES ,ComputingMethodologies_DOCUMENTANDTEXTPROCESSING - Abstract
Additional file 1 Supplementary text. An additional text file that describes the software in detail, contains parameter tables, software availability, and additional figures.
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- 2021
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21. Evolution evolves: physiology returns to centre stage
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Noble, Denis, Jablonka, Eva, Joyner, Michael J., Müller, Gerd B., and Omholt, Stig W.
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- 2014
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22. When parameters in dynamic models become phenotypes: a case study on flesh pigmentation in the chinook salmon (Oncorhynchus tshawytscha)
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Rajasingh, Hannah, Gjuvsland, Arne B., Vage, Dag Inge, and Omholt, Stig W.
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Phenotype -- Identification and classification ,Chinook salmon -- Genetic aspects ,Allelomorphism -- Identification and classification ,Gene expression -- Research ,Biological sciences - Abstract
The Pacific chinook salmon occurs as both white- and red-fleshed populations, with the flesh color type (red or white) seemingly under strong genetic influence. Previously published data on crosses between red- and white-fleshed individuals cannot be reconciled with a simple Mendelian two-locus, two-allele model, pointing to either a more complex inheritance pattern or the existence of gene interactions. Here we show that a standard single-locus, three-allele model can fully explain these data. Moreover, by implementing the single-locus model at the parameter level of a previously developed mathematical model describing carotenoid dynamics in salmon, we show that variation at a single gene involved in the muscle uptake of carotenoids is able to explain the available data. This illustrates how such a combined approach can generate biological understanding that would not be possible in a classical population genetic explanatory structure. An additional asset of this approach is that by allowing parameters to become phenotypes obeying a given genetic model, biological interpretations of mechanisms involved at a resolution level far beyond what is built into the original dynamic model are made possible. These insights can in turn be exploited in experimental studies as well as in construction of more detailed models.
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- 2008
23. Statistical epistasis is a generic feature of gene regulatory networks
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Gjuvsland, Arne B., Hayes, Ben J., Omholt, Stig W., and Carlborg, Orjan
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Quantitative trait loci -- Research ,Genetic epistasis -- Research ,Genetic regulation -- Research ,Biological sciences - Abstract
Functional dependencies between genes are a defining characteristic of gene networks underlying quantitative traits. However, recent studies show that the proportion of the genetic variation that can be attributed to statistical epistasis varies from almost zero to very high. It is thus of fundamental as well as instrumental importance to better understand whether different functional dependency patterns among polymorphic genes give rise to distinct statistical interaction patterns or not. Here we address this issue by combining a quantitative genetic model approach with genotype-phenotype models capable of translating allelic variation and regulatory principles into phenotypic variation at the level of gene expression. We show that gene regulatory networks with and without feedback motifs can exhibit a wide range of possible statistical genetic architectures with regard to both type of effect explaining phenotypic variance and number of apparent loci underlying the observed phenotypic effect. Although all motifs are capable of harboring significant interactions, positive feedback gives rise to higher amounts and more types of statistical epistasis. The results also suggest that the inclusion of statistical interaction terms in genetic models will increase the chance to detect additional QTL as well as functional dependencies between genetic loci over a broad range of regulatory regimes. This article illustrates how statistical genetic methods can fruitfully be combined with nonlinear systems dynamics to elucidate biological issues beyond reach of each methodology in isolation.
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- 2007
24. Bridging the genotype–phenotype gap: what does it take?
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Gjuvsland, Arne B., Vik, Jon Olav, Beard, Daniel A., Hunter, Peter J., and Omholt, Stig W.
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- 2013
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25. Is the brain water channel aquaporin-4 a pathogenetic factor in idiopathic intracranial hypertension? Results from a combined clinical and genetic study in a Norwegian cohort
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Kerty, Emilia, Heuser, Kjell, Indahl, Ulf G., Berg, Paul R., Nakken, Sigve, Lien, Sigbjrn, Omholt, Stig W., Ottersen, Ole P., and Nagelhus, Erlend A.
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- 2013
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26. Life History Shapes Trait Heredity by Accumulation of Loss-of-Function Alleles in Yeast
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Zörgö, Enikö, Gjuvsland, Arne, Cubillos, Francisco A., Louis, Edward J., Liti, Gianni, Blomberg, Anders, Omholt, Stig W., and Warringer, Jonas
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- 2012
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27. The genome sequence of Atlantic cod reveals a unique immune system
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Star, Bastiaan, Nederbragt, Alexander J., Jentoft, Sissel, Grimholt, Unni, Malmstrøm, Martin, Gregers, Tone F., Rounge, Trine B., Paulsen, Jonas, Solbakken, Monica H., Sharma, Animesh, Wetten, Ola F., Lanzén, Anders, Winer, Roger, Knight, James, Vogel, Jan-Hinnerk, Aken, Bronwen, Andersen, Øivind, Lagesen, Karin, Tooming-Klunderud, Ave, Edvardsen, Rolf B., Tina, Kirubakaran G., Espelund, Mari, Nepal, Chirag, Previti, Christopher, Karlsen, Bård Ove, Moum, Truls, Skage, Morten, Berg, Paul R., Gjøen, Tor, Kuhl, Heiner, Thorsen, Jim, Malde, Ketil, Reinhardt, Richard, Du, Lei, Johansen, Steinar D., Searle, Steve, Lien, Sigbjørn, Nilsen, Frank, Jonassen, Inge, Omholt, Stig W., Stenseth, Nils Chr., and Jakobsen, Kjetill S.
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- 2011
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28. Life-history evolution and the polyphenic regulation of somatic maintenance and survival
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Flatt, Thomas, Amdam, Gro V., Kirkwood, Thomas B. L., Omholt, Stig W., Flatt, Thomas, Amdam, Gro V., Kirkwood, Thomas B. L., and Omholt, Stig W.
- Abstract
Here we discuss life-history evolution from the perspective of adaptive phenotypic plasticity, with a focus on polyphenisms for somatic maintenance and survival. Polyphenisms are adaptive discrete alternative phenotypes that develop in response to changes in the environment. We suggest that dauer larval diapause and its associated adult phenotypes in the nematode (Caenorhabditis elegans), reproductive dormancy in the fruit fly (Drosophila melanogaster) and other insects, and the worker castes of the honey bee (Apis mellifera) are examples of what may be viewed as the polyphenic regulation of somatic maintenance and survival. In these and other cases, the same genotype can—depending upon its environment—express either of two alternative sets of life-history phenotypes that differ markedly with respect to somatic maintenance, survival ability, and thus life span. This plastic modulation of somatic maintenance and survival has traditionally been underappreciated by researchers working on aging and life history. We review the current evidence for such adaptive life-history switches and their molecular regulation and suggest that they are caused by temporally and/or spatially varying, stressful environments that impose diversifying selection, thereby favoring the evolution of plasticity of somatic maintenance and survival under strong regulatory control. By considering somatic maintenance and survivorship from the perspective of adaptive life-history switches, we may gain novel insights into the mechanisms and evolution of aging.
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- 2019
29. A dense SNP-based linkage map for Atlantic salmon (Salmo salar) reveals extended chromosome homeologies and striking differences in sex-specific recombination patterns
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Lien Sigbjørn, Gidskehaug Lars, Moen Thomas, Hayes Ben J, Berg Paul R, Davidson William S, Omholt Stig W, and Kent Matthew P
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Biotechnology ,TP248.13-248.65 ,Genetics ,QH426-470 - Abstract
Abstract Background The Atlantic salmon genome is in the process of returning to a diploid state after undergoing a whole genome duplication (WGD) event between 25 and100 million years ago. Existing data on the proportion of paralogous sequence variants (PSVs), multisite variants (MSVs) and other types of complex sequence variation suggest that the rediplodization phase is far from over. The aims of this study were to construct a high density linkage map for Atlantic salmon, to characterize the extent of rediploidization and to improve our understanding of genetic differences between sexes in this species. Results A linkage map for Atlantic salmon comprising 29 chromosomes and 5650 single nucleotide polymorphisms (SNPs) was constructed using genotyping data from 3297 fish belonging to 143 families. Of these, 2696 SNPs were generated from ESTs or other gene associated sequences. Homeologous chromosomal regions were identified through the mapping of duplicated SNPs and through the investigation of syntenic relationships between Atlantic salmon and the reference genome sequence of the threespine stickleback (Gasterosteus aculeatus). The sex-specific linkage maps spanned a total of 2402.3 cM in females and 1746.2 cM in males, highlighting a difference in sex specific recombination rate (1.38:1) which is much lower than previously reported in Atlantic salmon. The sexes, however, displayed striking differences in the distribution of recombination sites within linkage groups, with males showing recombination strongly localized to telomeres. Conclusion The map presented here represents a valuable resource for addressing important questions of interest to evolution (the process of re-diploidization), aquaculture and salmonid life history biology and not least as a resource to aid the assembly of the forthcoming Atlantic salmon reference genome sequence.
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- 2011
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30. Characterisation of a novel paralog of scavenger receptor class B member I (SCARB1) in Atlantic salmon (Salmo salar)
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Omholt Stig W, Baranski Matthew, Helgeland Hanna, Sundvold Hilde, and Våge Dag
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Genetics ,QH426-470 - Abstract
Abstract Background Red flesh colour is a unique trait found in some salmonid genera. Carotenoid pigments are not synthesized de novo in the fish, but are provided by dietary uptake. A better understanding of the molecular mechanisms underlying the cellular uptake and deposition of carotenoids could potentially be used to improve the low muscle deposition rate that is typically found in farmed Atlantic salmon. In addition, from an evolutionary point of view, the establishment and maintenance of this trait is still poorly understood. It has been demonstrated in several species that scavenger receptor class B, member 1 (SCARB1) is involved in intestinal absorption of carotenoids, which makes this gene a possible source of genetic variation in salmonid flesh pigmentation. Results In this study, a novel paralog of SCARB1 (SCARB1-2) was detected through screening for genetic variation in Atlantic salmon SCARB1. Full length SCARB1-2 encodes a protein with 89% identity to Atlantic salmon SCARB1, except for the C-terminal cytoplasmic tail that shows only 12% identity. The most prominent site of SCARB1 mRNA expression was in the mid gut, while a five-fold lower level was detected in Atlantic salmon skeletal muscle and liver. The SCARB1-2 mRNA was equally expressed in liver, muscle and mid gut, and at a lower level than SCARB1 mRNA. A total of seven different SCARB1-2 alleles comprising repetitive enhancer of zeste motifs (EZH2) were identified in the founding parents of a resource Atlantic salmon population. We mapped the SCARB1-2 paralog to a region on Atlantic salmon chromosome 1, containing a putative QTL for flesh colour. Addition of the SCARB1-2 marker increased the significance of this QTL, however the large confidence interval surrounding the QTL precludes confirmation of SCARB1-2 as a causative gene underlying variation in this trait. Conclusion We have characterised a novel paralog of SCARB1 (SCARB1-2), have mapped it to Atlantic salmon chromosome 1 and have described its expression in various tissues. Mapping with SCARB1-2 alleles added further evidence for a QTL affecting flesh colour on this chromosome, however further studies are needed to confirm a functional role for this gene in flesh colour pigmentation.
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- 2011
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31. A linkage map of the Atlantic salmon (Salmo salar) based on EST-derived SNP markers
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Kjøglum Sissel, Berg Paul R, Baranski Matthew, Hayes Ben, Moen Thomas, Koop Ben F, Davidson Willie S, Omholt Stig W, and Lien Sigbjørn
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Biotechnology ,TP248.13-248.65 ,Genetics ,QH426-470 - Abstract
Abstract Background The Atlantic salmon is a species of commercial and ecological significance. Like other salmonids, the species displays residual tetrasomy and a large difference in recombination rate between sexes. Linkage maps with full genome coverage, containing both type I and type II markers, are needed for progress in genomics. Furthermore, it is important to estimate levels of linkage disequilibrium (LD) in the species. In this study, we developed several hundred single nucleotide polymorphism (SNP) markers for the Atlantic salmon, and constructed male and female linkage maps containing SNP and microsatellite markers. We also investigated further the distribution of male and female recombination events across the genome, and estimated levels of LD between pairs of markers. Results The male map had 29 linkage groups and was 390 cM long. The female map had 30 linkage groups as was 1983 cM long. In total, the maps contained 138 microsatellite markers and 304 SNPs located within genes, most of which were successfully annotated. The ratio of male to female recombination events was either close to zero or very large, indicating that there is little overlap between regions in which male and female crossovers occur. The female map is likely to have close to full genome coverage, while the majority of male linkage groups probably lack markers in telomeric regions where male recombination events occur. Levels of r2 increased with decreasing inter-marker distance in a bimodal fashion; increasing slowly from ~60 cM, and more rapidly more from ~12 cM. Long-ranging LD may be consequence of recent admixture in the population, the population being a 'synthetic' breeding population with contributions from several distinct rivers. Levels of r2 dropped to half its maximum value (above baseline) within 15 cM, and were higher than 0.2 above baseline for unlinked markers ('useful LD') at inter-marker distances less than 5 cM. Conclusion The linkage map presented here is an important resource for genetic, comparative, and physical mapping of the Atlantic salmon. The female map is likely to have a map coverage that is not far from complete, whereas the male map length is likely to be significantly shorter than the true map, due to suboptimal marker coverage in the apparently small physical regions where male crossovers occur. 'Useful LD' was found at inter-marker distances less than 5 cM.
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- 2008
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32. Carotenoid dynamics in Atlantic salmon
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Omholt Stig W, Våge Dag, Øyehaug Leiv, and Rajasingh Hannah
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Biology (General) ,QH301-705.5 - Abstract
Abstract Background Carotenoids are pigment molecules produced mainly in plants and heavily exploited by a wide range of organisms higher up in the food-chain. The fundamental processes regulating how carotenoids are absorbed and metabolized in vertebrates are still not fully understood. We try to further this understanding here by presenting a dynamic ODE (ordinary differential equation) model to describe and analyse the uptake, deposition, and utilization of a carotenoid at the whole-organism level. The model focuses on the pigment astaxanthin in Atlantic salmon because of the commercial importance of understanding carotenoid dynamics in this species, and because deposition of carotenoids in the flesh is likely to play an important life history role in anadromous salmonids. Results The model is capable of mimicking feed experiments analyzing astaxanthin uptake and retention over short and long time periods (hours, days and years) under various conditions. A sensitivity analysis of the model provides information on where to look for possible genetic determinants underlying the observed phenotypic variation in muscle carotenoid retention. Finally, the model framework is used to predict that a specific regulatory system controlling the release of astaxanthin from the muscle is not likely to exist, and that the release of the pigment into the blood is instead caused by the androgen-initiated autolytic degradation of the muscle in the sexually mature salmon. Conclusion The results show that a dynamic model describing a complex trait can be instrumental in the early stages of a project trying to uncover underlying determinants. The model provides a heuristic basis for an experimental research programme, as well as defining a scaffold for modelling carotenoid dynamics in mammalian systems.
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- 2006
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33. Disruption of vitellogenin gene function in adult honeybees by intra-abdominal injection of double-stranded RNA
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Norberg Kari, Guidugli Karina R, Simões Zilá LP, Amdam Gro V, and Omholt Stig W
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Biotechnology ,TP248.13-248.65 - Abstract
Abstract Background The ability to manipulate the genetic networks underlying the physiological and behavioural repertoires of the adult honeybee worker (Apis mellifera) is likely to deepen our understanding of issues such as learning and memory generation, ageing, and the regulatory anatomy of social systems in proximate as well as evolutionary terms. Here we assess two methods for probing gene function by RNA interference (RNAi) in adult honeybees. Results The vitellogenin gene was chosen as target because its expression is unlikely to have a phenotypic effect until the adult stage in bees. This allowed us to introduce dsRNA in preblastoderm eggs without affecting gene function during development. Of workers reared from eggs injected with dsRNA derived from a 504 bp stretch of the vitellogenin coding sequence, 15% had strongly reduced levels of vitellogenin mRNA. When dsRNA was introduced by intra-abdominal injection in newly emerged bees, almost all individuals (96 %) showed the mutant phenotype. An RNA-fragment with an apparent size similar to the template dsRNA was still present in this group after 15 days. Conclusion Injection of dsRNA in eggs at the preblastoderm stage seems to allow disruption of gene function in all developmental stages. To dissect gene function in the adult stage, the intra-abdominal injection technique seems superior to egg injection as it gives a much higher penetrance, it is much simpler, and it makes it possible to address genes that are also expressed in the embryonic, larval or pupal stages.
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- 2003
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34. Roadmap for cardiovascular circulation model
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Safaei, Soroush, Bradley, Christopher P., Suresh, Vinod, Mithraratne, Kumar, Muller, Alexandre, Ho, Harvey, Ladd, David, Hellevik, Leif R., Omholt, Stig W., Chase, J. Geoffrey, Müller, Lucas O., Watanabe, Sansuke M., Blanco, Pablo J., de Bono, Bernard, and Hunter, Peter J.
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Cardiovascular Physiological Phenomena ,Special section reviews: The Cardiac Physiome Project ,Blood Circulation ,Hemodynamics ,Models, Cardiovascular ,Humans ,Software - Abstract
Computational models of many aspects of the mammalian cardiovascular circulation have been developed. Indeed, along with orthopaedics, this area of physiology is one that has attracted much interest from engineers, presumably because the equations governing blood flow in the vascular system are well understood and can be solved with well-established numerical techniques. Unfortunately, there have been only a few attempts to create a comprehensive public domain resource for cardiovascular researchers. In this paper we propose a roadmap for developing an open source cardiovascular circulation model. The model should be registered to the musculo-skeletal system. The computational infrastructure for the cardiovascular model should provide for near real-time computation of blood flow and pressure in all parts of the body. The model should deal with vascular beds in all tissues, and the computational infrastructure for the model should provide links into CellML models of cell function and tissue function. In this work we review the literature associated with 1D blood flow modelling in the cardiovascular system, discuss model encoding standards, software and a model repository. We then describe the coordinate systems used to define the vascular geometry, derive the equations and discuss the implementation of these coupled equations in the open source computational software OpenCMISS. Finally, some preliminary results are presented and plans outlined for the next steps in the development of the model, the computational software and the graphical user interface for accessing the model.
- Published
- 2016
35. Functional Analysis of All Salmonid Genomes (FAASG): an international initiative supporting future salmonid research, conservation and aquaculture
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Macqueen, Daniel J., Primmer, Craig R., Houston, Ross D., Nowak, Barbara F., Bernatchez, Louis, Bergseth, Steinar, Davidson, William S., Gallardo-Escárate, Cristian, Goldammer, Tom, Guiguen, Yann, Iturra, Patricia, Kijas, James W., Koop, Ben F., Lien, Sigbjørn, Maass, Alejandro, Martin, Samuel A.M., McGinnity, Philip, Montecino, Martin, Naish, Kerry A., Nichols, Krista M., Ólafsson, Kristinn, Omholt, Stig W., Palti, Yniv, Plastow, Graham S., Rexroad, Caird E., Rise, Matthew L., Ritchie, Rachael J., Sandve, Simen R., Schulte, Patricia M., Tello, Alfredo, Vidal, Rodrigo, Vik, Jon O., Wargelius, Anna, and Yáñez, José Manuel
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salmonidae ,biologie comparative ,génomique fonctionnelle ,production aquacole ,reproduction ,analyse de génome ,phénotype ,séquençage du génome ,poisson ,aquaculture ,variation phénotypique ,comparative biology ,data sharing ,evolution ,functional annotation ,genome biology ,phenotyping ,standardized data and metadata ,salmonid fish ,whole genome duplication ,évolution génomique des poissons ,sélection génomique ,évolution génomique ,annotation fonctionnelle ,conservation des espèces ,duplication des génomes ,expression des gènes - Abstract
We describe an emerging initiative - the 'Functional Annotation of All Salmonid Genomes' (FAASG), which will leverage the extensive trait diversity that has evolved since a whole genome duplication event in the salmonid ancestor, to develop an integrative understanding of the functional genomic basis of phenotypic variation. The outcomes of FAASG will have diverse applications, ranging from improved understanding of genome evolution, to improving the efficiency and sustainability of aquaculture production, supporting the future of fundamental and applied research in an iconic fish lineage of major societal importance.
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- 2016
36. How to organise and run an ISBE modelling service
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Vik, Jon Olav, Omholt, Stig, van Nieuwpoort, Frans, Snoep, Jacky, Mone, Martijn, Westerhoff, Hans, Nickerson, David, Juty, Nick, Goble, Carole, Stanford, Natalie, Hoefer, Thomas, Martins dos Santos. Vitor, Hermjakob, Henning, and La Novere, Nicolas
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ISBE, systems biology, infrastructure, modelling - Abstract
ISBE will empower the experimental research community to make modelling part of their lab routine. Here we discuss how to define and structure ISBE modelling services, building on D8.2's review of the purpose and overall design principles for modelling services. We identify the components of ISBE modelling services and propose an organizational structure to achieve uniform coverage of services from a heterogeneous network of expertises. A roadmap concludes the report, proposing initial low-budget services for selected modelling frameworks, then outlining a strategy for growth and scalability of ISBE modelling services. How to define and structure ISBE modelling services is a many-faceted question. First and foremost, one must identify the purpose of each service (what will it achieve?), which also entails specifying its inputs and outputs. It can be useful to group kinds of services into broader categories, either based on their function, or based on their organizational structure including staffing and funding. Modelling services will include automated analyses of published or user-provided models, fitting of parameters to user data, and refinement and adaptation of existing models. However, it also makes sense to include related services such as stewardship and training in the broad term "modelling services". A coordinating Systems Biology Centre (cSBC) will interconnect national Systems Biology Centres (nSBCs) to make the collective expertise of participating nations easily accessible for all European researchers. Chapter 2.3 concretizes this with illustrations of the variety of modelling services that ISBE is likely to offer, and how to route requests from clients to ISBE tools and expertise. Levels of service may range from fully automatic tools to long-term personal involvement, with access to more demanding services prioritized in cooperation with funders. Likewise, there will be several kinds and levels of documentation and user support. We advocate a focus on user needs in prioritizing what ISBE is to offer, in specifying services, and in routing expertise to clients. Clear descriptions of the data requirements for each modelling approach helps clients figure out their options and see what additional data they might require to open more options for modelling. Standardized virtual experiments can form an articulated link between modellers and experimentalists, and can be used to streamline the confrontation of models with data, e.g. in parameter estimation and model selection. As candidates for pilot services to be offered by the interim "ISBE light", we have identified modelling frameworks that span a wide range of biologically interesting questions within a well-defined set of user inputs. These include ordinary differential equations (where the rates-of-change of state variables is a function of the current value of those state variables) and constraint-based models (based on stoichiometry in biochemical reaction networks). The demand for modelling services is anticipated to increase sharply once ISBE succeeds in transforming the practice of biological research and application. To meet this demand, we identify five key issues of scalability: Recruitment of providers, routing of clients to providers, strategic focusing of effort, training and education of users, and standardization and curation to streamline knowledge management, each of which is detailed in Chapter 5.2.
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- 2015
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37. ISBE - resource assessment for a European modelling service: Report detailing all the findings and activities on Task 2
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Vik, Jon Olav, Omholt, Stig, Moné, Martijn J., Van Nieuwpoort, Frans, Van Driel, Roel, Skene, Barbara, Fitzmaurice, William, Juty, Nick, Goble, Carole, Stanford, Natalie, Hoefer, Thomas, Martins dos Santos, Vitor, Westerhoff, Hans, Hermjakob, Hennig, and La Novere, Nicolas
- Subjects
ISBE, systems biology, infrastructure, modelling - Abstract
A distinguishing feature of ISBE is its ambition to provide modelling as a service, making it easier for biologists to integrate mathematical modelling in their scientific work. In this deliverable we review the rationale for modelling in systems biology, develop concepts to describe modelling needs and competences, cite the chief demands voiced by respondents in ISBE surveys, and propose design principles for ISBE modelling services.
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- 2015
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38. Intermediate report on the definition of criteria and preliminary map of ISBE centres
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van Driel, Roel, van Nieuwpoort, Frans, Moné, Martijn, Westerhoff, Hans, Regierer, Babette, Martins dos Santos, Vitor, Hohmann, Stefan, Pugh, Adrian, Pastori, Gabriela, Goble, Carol, Wolstencroft, Katy, Omholt, Stig, Vik, Jon Olav, McKiernan, Eadaoin, Fitzmaurice, William, Gruden, Kristina, and Thanos, Dimitris
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ISBE, systems biology, biology, infrastructure - Abstract
This report summarises the vision of the ISBE Steering Committee on the contours of the three types of ISBE expertise centres. It represents the shared vision on ISBE centres that will be used by the work packages in developing the ISBE infrastructure.
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- 2015
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39. The gene csd is the primary signal for sexual development in the honeybee and encodes an SR-type protein
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Beye, Martin, Hasselmann, Martin, Fondrk, M. Kim, Page, Robert E. Jr., and Omholt, Stig W.
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Sex determination, Genetic -- Genetic aspects ,Gene expression -- Analysis ,Honeybee -- Genetic aspects ,Haploidy -- Genetic aspects ,Biological sciences - Abstract
The complementary sex determiner (csd) in honeybees is the primary sex- determining signal. At the csd locus males are hemizygous, while females are heterozygous. The csd alleles vary substatially with no transcription differences between sexes. It encodes a serine-arginine-rich protein.
- Published
- 2003
40. A novel role for pigment genes in the stress response in rainbow trout (Oncorhynchus mykiss)
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Khan, Uniza Wahid, Øverli, Øyvind, Hinkle, Patricia M, Pasha, Farhan Ahmad, Johansen, Ida Beitnes, Berget, Ingunn, Silva, Patricia I M, Kittilsen, Silje, Höglund, Erik, Omholt, Stig W, Våge, Dag Inge, Khan, Uniza Wahid, Øverli, Øyvind, Hinkle, Patricia M, Pasha, Farhan Ahmad, Johansen, Ida Beitnes, Berget, Ingunn, Silva, Patricia I M, Kittilsen, Silje, Höglund, Erik, Omholt, Stig W, and Våge, Dag Inge
- Abstract
In many vertebrate species visible melanin-based pigmentation patterns correlate with high stress- and disease-resistance, but proximate mechanisms for this trait association remain enigmatic. Here we show that a missense mutation in a classical pigmentation gene, melanocyte stimulating hormone receptor (MC1R), is strongly associated with distinct differences in steroidogenic melanocortin 2 receptor (MC2R) mRNA expression between high- (HR) and low-responsive (LR) rainbow trout (Oncorhynchus mykiss). We also show experimentally that cortisol implants increase the expression of agouti signaling protein (ASIP) mRNA in skin, likely explaining the association between HR-traits and reduced skin melanin patterning. Molecular dynamics simulations predict that melanocortin 2 receptor accessory protein (MRAP), needed for MC2R function, binds differently to the two MC1R variants. Considering that mRNA for MC2R and the MC1R variants are present in head kidney cells, we hypothesized that MC2R activity is modulated in part by different binding affinities of the MC1R variants for MRAP. Experiments in mammalian cells confirmed that trout MRAP interacts with the two trout MC1R variants and MC2R, but failed to detect regulation of MC2R signaling, possibly due to high constitutive MC1R activity.
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- 2016
41. Gene Regulatory Networks Generating the Phenomena of Additivity, Dominance and Epistasis
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Omholt, Stig W., Plahte, Erik, Oyehaug, Leiv, and Xiang, Kefang
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Genetic regulation -- Research ,Molecular genetics -- Research ,Biological control systems -- Genetic aspects ,Dominance (Genetics) ,Biological sciences - Abstract
We show how the phenomena of genetic dominance, overdominance, additivity, and epistasis are generic features of simple diploid gene regulatory networks. These regulatory network models are together sufficiently complex to catch most of the suggested molecular mechanisms responsible for generating dominant mutations. These include reduced gene dosage, expression or protein activity (haploinsufficiency), increased gene dosage, ectopic or temporarily altered mRNA expression, increased or constitutive protein activity, and dominant negative effects. As classical genetics regards the phenomenon of dominance to be generated by intralocus interactions, we have studied two one-locus models, one with a negative autoregulatory feedback loop, and one with a positive autoregulatory feedback loop. To include the phenomena of epistasis and downstream regulatory effects, a model of a three-locus signal transduction network is also analyzed. It is found that genetic dominance as well as overdominance may he an intra-as well as interlocus interaction phenomenon. In the latter case the dominance phenomenon is intimately connected to either feedback-mediated epistasis or downstream-mediated epistasis. It appears that in the intra- as well as the interlocus case there is considerable room for additive gene action, which may explain to some degree the predictive power of quantitative genetic theory, with its emphasis on this type of gene action. Furthermore, the results illuminate and reconcile the prevailing explanations of heterosis, and they support the old conjecture that the phenomenon of dominance may have an evolutionary explanation related to life history strategy.
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- 2000
42. ISBE portfolio of showcases illustrating the impact of modelling
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Höfer, Thomas, Weiser, Anne, Westerhoff, Hans, Mone, Martijn, Martins dos Santos, Vitor, Fitzmaurice, Will, Omholt, Stig, and Vik, Jon Olav
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ISBE, systems biology, research, modelling ,3. Good health - Abstract
This document identifies showcases illustrating the impact of modelling on biological discovery and the added-value of integrated theoretical-experimental research. It illustrates the impact of modelling through existing showcases by providing examples of existing modelling methodologies where they have led to a quantum increase in understanding of biology or medicine. There are also examples how experimental data have driven the development of new modelling approaches capable of delivering the required methodology. It illustrates outstanding, representative, examples of the added value of integrated theoretical-experimental research programmes and documents how modelling will have to guide the development of a mature phenomics discipline.
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- 2014
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43. Electrodiffusion in neural tissue at long timescales
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Pettersen Klas, T. Einevoll Gaute, Østby Ivar, Halnes Geir, and W Omholt Stig
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Biomedical Engineering ,Neuroscience (miscellaneous) ,Computer Science Applications - Published
- 2014
44. Roadmap for cardiovascular circulation model
- Author
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Safaei, Soroush, primary, Bradley, Christopher P., additional, Suresh, Vinod, additional, Mithraratne, Kumar, additional, Muller, Alexandre, additional, Ho, Harvey, additional, Ladd, David, additional, Hellevik, Leif R., additional, Omholt, Stig W., additional, Chase, J. Geoffrey, additional, Müller, Lucas O., additional, Watanabe, Sansuke M., additional, Blanco, Pablo J., additional, de Bono, Bernard, additional, and Hunter, Peter J., additional
- Published
- 2016
- Full Text
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45. Scan-o-matic: High-Resolution Microbial Phenomics at a Massive Scale
- Author
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Zackrisson, Martin, primary, Hallin, Johan, additional, Ottosson, Lars-Göran, additional, Dahl, Peter, additional, Fernandez-Parada, Esteban, additional, Ländström, Erik, additional, Fernandez-Ricaud, Luciano, additional, Kaferle, Petra, additional, Skyman, Andreas, additional, Stenberg, Simon, additional, Omholt, Stig, additional, Petrovič, Uroš, additional, Warringer, Jonas, additional, and Blomberg, Anders, additional
- Published
- 2016
- Full Text
- View/download PDF
46. A novel role for pigment genes in the stress response in rainbow trout (Oncorhynchus mykiss)
- Author
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Khan, Uniza Wahid, primary, Øverli, Øyvind, additional, Hinkle, Patricia M., additional, Pasha, Farhan Ahmad, additional, Johansen, Ida Beitnes, additional, Berget, Ingunn, additional, Silva, Patricia I. M., additional, Kittilsen, Silje, additional, Höglund, Erik, additional, Omholt, Stig W., additional, and Våge, Dag Inge, additional
- Published
- 2016
- Full Text
- View/download PDF
47. The Human Physiome: a necessary key for the creative destruction of medicine
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Omholt, Stig W., primary and Hunter, Peter J., additional
- Published
- 2016
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48. Monotonicity is a key feature of genotype-phenotype maps
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Gjuvsland, Arne Bjørke, Wang, Yunpeng, Plahte, Erik, and Omholt, Stig W
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epistasis ,systems genetics ,Genetics ,Molecular Medicine ,variance component analysis ,genetic modeling ,Original Research Article ,genetic variance ,genotype-phenotype map ,monotonicity ,gene regulatory networks ,Genetics (clinical) - Abstract
It was recently shown that monotone gene action, i.e., order-preservation between allele content and corresponding genotypic values in the mapping from genotypes to phenotypes, is a prerequisite for achieving a predictable parent-offspring relationship across the whole allele frequency spectrum. Here we test the consequential prediction that the design principles underlying gene regulatory networks are likely to generate highly monotone genotype-phenotype maps. To this end we present two measures of the monotonicity of a genotype-phenotype map, one based on allele substitution effects, and the other based on isotonic regression. We apply these measures to genotype-phenotype maps emerging from simulations of 1881 different 3-gene regulatory networks. We confirm that in general, genotype-phenotype maps are indeed highly monotonic across network types. However, regulatory motifs involving incoherent feedforward or positive feedback, as well as pleiotropy in the mapping between genotypes and gene regulatory parameters, are clearly predisposed for generating non-monotonicity. We present analytical results confirming these deep connections between molecular regulatory architecture and monotonicity properties of the genotype-phenotype map. These connections seem to be beyond reach by the classical distinction between additive and non-additive gene action. © 2013 Gjuvsland, Wang, Plahte and Omholt. This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). This Document is Protected by copyright and was first published by Frontiers. All rights reserved. it is reproduced with permission.
- Published
- 2013
49. Towards causally cohesive genotype–phenotype modelling for characterization of the soft-tissue mechanics of the heart in normal and pathological geometries
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Nordbø, Øyvind, primary, Gjuvsland, Arne B., additional, Nermoen, Anders, additional, Land, Sander, additional, Niederer, Steven, additional, Lamata, Pablo, additional, Lee, Jack, additional, Smith, Nicolas P., additional, Omholt, Stig W., additional, and Vik, Jon Olav, additional
- Published
- 2015
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50. High-Throughput Biochemical Fingerprinting of Saccharomyces cerevisiae by Fourier Transform Infrared Spectroscopy
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Kohler, Achim, primary, Böcker, Ulrike, additional, Shapaval, Volha, additional, Forsmark, Annabelle, additional, Andersson, Mats, additional, Warringer, Jonas, additional, Martens, Harald, additional, Omholt, Stig W., additional, and Blomberg, Anders, additional
- Published
- 2015
- Full Text
- View/download PDF
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