26 results on '"Höppner, Marc"'
Search Results
2. Functional and evolutionary genomic inferences in Populus through genome and population sequencing of American and European aspen
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Lin, Yao-Cheng, Wang, Jing, Delhomme, Nicolas, Schiffthaler, Bastian, Sundström, Görel, Zuccolo, Andrea, Nystedt, Björn, Hvidsten, Torgeir R., de la Torre, Amanda, Cossu, Rosa M., Hoeppner, Marc P., Lantz, Henrik, Scofield, Douglas G., Zamani, Neda, Johansson, Anna, Mannapperuma, Chanaka, Robinson, Kathryn M., Mähler, Niklas, Leitch, Ilia J., Pellicer, Jaume, Park, Eung-Jun, Van Montagu, Marc, Van de Peer, Yves, Grabherr, Manfred, Jansson, Stefan, Ingvarsson, Pär K., and Street, Nathaniel R.
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- 2018
3. Inter-chromosomal coupling between vision and pigmentation genes during genomic divergence
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Hench, Kosmas, Vargas, Marta, Höppner, Marc P., McMillan, W. Owen, and Puebla, Oscar
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- 2019
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4. Phenotypic and genomic dissection of colour pattern variation in a reef fish radiation.
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Coulmance, Floriane, Akkaynak, Derya, Le Poul, Yann, Höppner, Marc P., McMillan, W. Owen, and Puebla, Oscar
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REEFS ,REEF fishes ,WHOLE genome sequencing ,GENOME-wide association studies ,SINGLE nucleotide polymorphisms ,UNDERWATER cameras - Abstract
Coral reefs rank among the most diverse species assemblages on Earth. A particularly striking aspect of coral reef communities is the variety of colour patterns displayed by reef fishes. Colour pattern is known to play a central role in the ecology and evolution of reef fishes through, for example, signalling or camouflage. Nevertheless, colour pattern is a complex trait in reef fishes—actually a collection of traits—that is difficult to analyse in a quantitative and standardized way. This is the challenge that we address in this study using the hamlets (Hypoplectrus spp., Serranidae) as a model system. Our approach involves a custom underwater camera system to take orientation‐ and size‐standardized photographs in situ, colour correction, alignment of the fish images with a combination of landmarks and Bézier curves, and principal component analysis on the colour value of each pixel of each aligned fish. This approach identifies the major colour pattern elements that contribute to phenotypic variation in the group. Furthermore, we complement the image analysis with whole‐genome sequencing to run a multivariate genome‐wide association study for colour pattern variation. This second layer of analysis reveals sharp association peaks along the hamlet genome for each colour pattern element and allows to characterize the phenotypic effect of the single nucleotide polymorphisms that are most strongly associated with colour pattern variation at each association peak. Our results suggest that the diversity of colour patterns displayed by the hamlets is generated by a modular genomic and phenotypic architecture. see also the Perspective by Bruno Frédérich [ABSTRACT FROM AUTHOR]
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- 2024
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5. Comparative analysis of amplicon and metagenomic sequencing methods reveals key features in the evolution of animal metaorganisms
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Rausch, Philipp, Rühlemann, Malte, Hermes, Britt M., Doms, Shauni, Dagan, Tal, Dierking, Katja, Domin, Hanna, Fraune, Sebastian, von Frieling, Jakob, Hentschel, Ute, Heinsen, Femke-Anouska, Höppner, Marc, Jahn, Martin T., Jaspers, Cornelia, Kissoyan, Kohar Annie B., Langfeldt, Daniela, Rehman, Ateequr, Reusch, Thorsten B. H., Roeder, Thomas, Schmitz, Ruth A., Schulenburg, Hinrich, Soluch, Ryszard, Sommer, Felix, Stukenbrock, Eva, Weiland-Bräuer, Nancy, Rosenstiel, Philip, Franke, Andre, Bosch, Thomas, and Baines, John F.
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- 2019
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6. Effect of Hyperbaric Oxygen and Inflammation on Human Gingival Mesenchymal Stem/Progenitor Cells.
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Tölle, Johannes, Koch, Andreas, Schlicht, Kristina, Finger, Dirk, Kaehler, Wataru, Höppner, Marc, Graetz, Christian, Dörfer, Christof, Schulte, Dominik M., and Fawzy El-Sayed, Karim
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PROGENITOR cells ,NUCLEOTIDE sequencing ,GENE expression profiling ,MESENCHYMAL stem cells ,GINGIVA ,GENE amplification - Abstract
The present study explores for the first time the effect of hyperbaric oxygen (HBO) on gingival mesenchymal stem cells' (G-MSCs) gene expression profile, intracellular pathway activation, pluripotency, and differentiation potential under an experimental inflammatory setup. G-MSCs were isolated from five healthy individuals (n = 5) and characterized. Single (24 h) or double (72 h) HBO stimulation (100% O2, 3 bar, 90 min) was performed under experimental inflammatory [IL-1β (1 ng/mL)/TNF-α (10 ng/mL)/IFN-γ (100 ng/mL)] and non-inflammatory micro-environment. Next Generation Sequencing and KEGG pathway enrichment analysis, G-MSCs' pluripotency gene expression, Wnt-/β-catenin pathway activation, proliferation, colony formation, and differentiation were investigated. G-MSCs demonstrated all mesenchymal stem/progenitor cells' characteristics. The beneficial effect of a single HBO stimulation was evident, with anti-inflammatory effects and induction of differentiation (TLL1, ID3, BHLHE40), proliferation/cell survival (BMF, ID3, TXNIP, PDK4, ABL2), migration (ABL2) and osteogenic differentiation (p < 0.05). A second HBO stimulation at 72 h had a detrimental effect, significantly increasing the inflammation-induced cellular stress and ROS accumulation through HMOX1, BHLHE40, and ARL4C amplification and pathway enrichment (p < 0.05). Results outline a positive short-term single HBO anti-inflammatory, regenerative, and differentiation stimulatory effect on G-MSCs. A second (72 h) stimulation is detrimental to the same properties. The current results could open new perspectives in the clinical application of short-termed HBO induction in G-MSCs-mediated periodontal reparative/regenerative mechanisms. [ABSTRACT FROM AUTHOR]
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- 2023
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7. Microbiomarkers in inflammatory bowel diseases: caveats come with caviar
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Sommer, Felix, Rühlemann, Malte Christoph, Bang, Corinna, Höppner, Marc, Rehman, Ateequr, Kaleta, Christoph, Schmitt-Kopplin, Phillippe, Dempfle, Astrid, Weidinger, Stephan, Ellinghaus, Eva, Krauss-Etschmann, Susanne, Schmidt-Arras, Dirk, Aden, Konrad, Schulte, Dominik, Ellinghaus, David, Schreiber, Stefan, Tholey, Andreas, Rupp, Jan, Laudes, Matthias, Baines, John F, Rosenstiel, Philip, and Franke, Andre
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- 2017
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8. Specificity of the innate immune system and diversity of C-type lectin domain (CTLD) proteins in the nematode Caenorhabditis elegans
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Schulenburg, Hinrich, Hoeppner, Marc P., Weiner, January, III, and Bornberg-Bauer, Erich
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- 2008
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9. Two different epigenetic information channels in wild three-spined sticklebacks are involved in salinity adaptation
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Heckwolf, Melanie J., Meyer, Britta S., Häsler, Robert, Höppner, Marc P., Eizaguirre, Christophe, and Reusch, Thorsten B. H.
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Epigenomics ,Evolutionary Biology ,Salinity ,Genome ,Acclimatization ,Adaptation, Biological ,SciAdv r-articles ,Computational Biology ,Genomics ,DNA Methylation ,Smegmamorpha ,Epigenesis, Genetic ,Gene Ontology ,Gene Expression Regulation ,Genetics ,Animals ,CpG Islands ,Research Articles ,Research Article - Abstract
Detection of both inducible and stable DNA methylation indicates two different epigenetic modes of salinity adaptation., Epigenetic inheritance has been proposed to contribute to adaptation and acclimation via two information channels: (i) inducible epigenetic marks that enable transgenerational plasticity and (ii) noninducible epigenetic marks resulting from random epimutations shaped by selection. We studied both postulated channels by sequencing methylomes and genomes of Baltic three-spined sticklebacks (Gasterosteus aculeatus) along a salinity cline. Wild populations differing in salinity tolerance revealed differential methylation (pop-DMS) at genes enriched for osmoregulatory processes. A two-generation experiment demonstrated that 62% of these pop-DMS were noninducible by salinity manipulation, suggesting that they are the result of either direct selection or associated genomic divergence at cis- or trans-regulatory sites. Two-thirds of the remaining inducible pop-DMS increased in similarity to patterns detected in wild populations from corresponding salinities. The level of similarity accentuated over consecutive generations, indicating a mechanism of transgenerational plasticity. While we can attribute natural DNA methylation patterns to the two information channels, their interplay with genomic variation in salinity adaptation is still unresolved.
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- 2020
10. Algal genomes reveal evolutionary mosaicism and the fate of nucleomorphs
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Curtis, Bruce A., Tanifuji, Goro, Burki, Fabien, Gruber, Ansgar, Irimia, Manuel, Maruyama, Shinichiro, Arias, Maria C., Ball, Steven G., Gile, Gillian H., Hirakawa, Yoshihisa, Hopkins, Julia F., Kuo, Alan, Rensing, Stefan A., Schmutz, Jeremy, Symeonidi, Aikaterini, Elias, Marek, Eveleigh, Robert J. M., Herman, Emily K., Klute, Mary J., Nakayama, Takuro, Oborník, Miroslav, Reyes-Prieto, Adrian, Armbrust, Virginia E., Aves, Stephen J., Beiko, Robert G., Coutinho, Pedro, Dacks, Joel B., Durnford, Dion G., Fast, Naomi M., Green, Beverley R., Grisdale, Cameron J., Hempel, Franziska, Henrissat, Bernard, Höppner, Marc P., Ishida, Ken-Ichiro, Kim, Eunsoo, Kořený, Luděk, Kroth, Peter G., Liu, Yuan, Malik, Shehre-Banoo, Maier, Uwe G., McRose, Darcy, Mock, Thomas, Neilson, Jonathan A. D., Onodera, Naoko T., Poole, Anthony M., Pritham, Ellen J., Richards, Thomas A., Rocap, Gabrielle, Roy, Scott W., Sarai, Chihiro, Schaack, Sarah, Shirato, Shu, Slamovits, Claudio H., Spencer, David F., Suzuki, Shigekatsu, Worden, Alexandra Z., Zauner, Stefan, Barry, Kerrie, Bell, Callum, Bharti, Arvind K., Crow, John A., Grimwood, Jane, Kramer, Robin, Lindquist, Erika, Lucas, Susan, Salamov, Asaf, McFadden, Geoffrey I., Lane, Christopher E., Keeling, Patrick J., Gray, Michael W., Grigoriev, Igor V., and Archibald, John M.
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- 2012
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11. Ultrafast dynamics and coherent order parameter oscillations under photo-excitation in the excitonic insulator Ta2NiSe5.
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Werdehausen, Daniel, Agustsson, Steinn Ymir, Kim, Minjae, Shabestari, Parmida, Huang, Emily, Pokharel, Amrit, Larkin, Timofei, Boris, Alexander, Takayama, Tomohiro, Yangfan Lu, Rost, Andreas W., Hao Chu, Yaresko, Alexander, Höppner, Marc, Schulz, Armin, Manske, Dirk, Keimer, Bernhard, Takagi, Hidenori, and Kaiser, Stefan
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- 2018
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12. Pseudomonas aeruginosa populations in the cystic fibrosis lung lose susceptibility to newly applied β-lactams within 3 days.
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Tueffers, Leif, Barbosa, Camilo, Bobis, Ingrid, Schubert, Sabine, Höppner, Marc, Rühlemann, Malte, Franke, Andre, Rosenstiel, Philip, Friedrichs, Anette, Krenz-Weinreich, Annegret, Fickenscher, Helmut, Bewig, Burkhard, Schreiber, Stefan, and Schulenburg, Hinrich
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PSEUDOMONAS aeruginosa ,CYSTIC fibrosis ,PULMONARY fibrosis ,PSEUDOMONAS aeruginosa infections ,LUNG infections ,CONDITIONED response - Abstract
Background: Chronic pulmonary infections by Pseudomonas aeruginosa require frequent intravenous antibiotic treatment in cystic fibrosis (CF) patients. Emergence of antimicrobial resistance is common in these patients, which to date has been investigated at long-term intervals only.Objectives: To investigate under close to real-time conditions the dynamics of the response by P. aeruginosa to a single course of antibiotic therapy and the potentially associated rapid spread of antimicrobial resistance, as well as the impact on the airway microbiome.Methods: We investigated a cohort of adult CF patients that were treated with a single course of antimicrobial combination therapy. Using daily sampling during treatment, we quantified the expression of resistance by P. aeruginosa (median of six isolates per daily sample, 347 isolates in total), measured bacterial load by P. aeruginosa-specific quantitative PCR and characterized the airway microbiome with a 16S rRNA-based approach. WGS was performed to reconstruct intrapatient strain phylogenies.Results: In two patients, we found rapid and large increases in resistance to meropenem and ceftazidime. Phylogenetic reconstruction of strain relationships revealed that resistance shifts are probably due to de novo evolution and/or the selection of resistant subpopulations. We observed high interindividual variation in the reduction of bacterial load, microbiome composition and antibiotic resistance.Conclusions: We show that CF-associated P. aeruginosa populations can quickly respond to antibiotic therapy and that responses are patient specific. Thus, resistance evolution can be a direct consequence of treatment, and drug efficacy can be lost much faster than usually assumed. The consideration of these patient-specific rapid resistance shifts can help to improve treatment of CF-associated infections, for example by deeper sampling of bacteria for diagnostics, repeated monitoring of pathogen susceptibility and switching between drugs. [ABSTRACT FROM AUTHOR]- Published
- 2019
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13. The evolution of microendemism in a reef fish (Hypoplectrus maya).
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Moran, Benjamin M., Hench, Kosmas, Waples, Robin S., Höppner, Marc P., Baldwin, Carole C., McMillan, William Owen, and Puebla, Oscar
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REEF fishes ,CENSUS ,ECOLOGICAL niche ,BIOLOGICAL evolution ,MARINE biodiversity - Abstract
Marine species tend to have extensive distributions, which are commonly attributed to the dispersal potential provided by planktonic larvae and the rarity of absolute barriers to dispersal in the ocean. Under this paradigm, the occurrence of marine microendemism without geographic isolation in species with planktonic larvae poses a dilemma. The recently described Maya hamlet (Hypoplectrus maya, Serranidae) is exactly such a case, being endemic to a 50‐km segment of the Mesoamerican Barrier Reef System (MBRS). We use whole‐genome analysis to infer the demographic history of the Maya hamlet and contrast it with the sympatric and pan‐Caribbean black (H. nigricans), barred (H. puella) and butter (H. unicolor) hamlets, as well as the allopatric but phenotypically similar blue hamlet (H. gemma). We show that H. maya is indeed a distinct evolutionary lineage, with genomic signatures of inbreeding and a unique demographic history of continuous decrease in effective population size since it diverged from congeners just ~3,000 generations ago. We suggest that this case of microendemism may be driven by the combination of a narrow ecological niche and restrictive oceanographic conditions in the southern MBRS, which is consistent with the occurrence of an unusually high number of marine microendemics in this region. The restricted distribution of the Maya hamlet, its decline in both census and effective population sizes, and the degradation of its habitat place it at risk of extinction. We conclude that the evolution of marine microendemism can be a fast and dynamic process, with extinction possibly occurring before speciation is complete. [ABSTRACT FROM AUTHOR]
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- 2019
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14. Spin Orientation of Two-Dimensional Electrons Driven by Temperature-Tunable Competition of Spin-Orbit and Exchange-Magnetic Interactions.
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Generalov, Alexander, Otrokov, Mikhail M., Chikina, Alla, Kliemt, Kristin, Kummer, Kurt, Höppner, Marc, Güttler, Monika, Seiro, Silvia, Fedorov, Alexander, Schulz, Susanne, Danzenbächer, Steffen, Chulkov, Evgueni V., Geibel, Christoph, Laubschat, Clemens, Dudin, Pavel, Hoesch, Moritz, Kim, Timur, Radovic, Milan, Ming Shi, and Plumb, Nicholas C.
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- 2017
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15. The genetic basis for ecological adaptation of the Atlantic herring revealed by genome sequencing.
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Barrio, Alvaro Martinez, Lamichhaney, Sangeet, Fan, Guangyi, Rafati, Nima, Pettersson, Mats, He Zhang, Dainat, Jacques, Ekman, Diana, Höppner, Marc, Jern, Patric, Martin, Marcel, Nystedt, Björn, Xin Liu, Wenbin Chen, Xinming Liang, Chengcheng Shi, Yuanyuan Fu, Kailong Ma, Xiao Zhan, and Chungang Feng
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- 2016
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16. Serendipitous Meta-Transcriptomics: The Fungal Community of Norway Spruce (Picea abies).
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Delhomme, Nicolas, Sundström, Görel, Zamani, Neda, Lantz, Henrik, Lin, Yao-Cheng, Hvidsten, Torgeir R., Höppner, Marc P., Jern, Patric, Van de Peer, Yves, Lundeberg, Joakim, Grabherr, Manfred G., and Street, Nathaniel R.
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FUNGAL communities ,RNA sequencing ,SERENDIPITY ,EPIPHYTES ,NORWAY spruce - Abstract
After performing de novo transcript assembly of >1 billion RNA-Sequencing reads obtained from 22 samples of different Norway spruce (Picea abies) tissues that were not surface sterilized, we found that assembled sequences captured a mix of plant, lichen, and fungal transcripts. The latter were likely expressed by endophytic and epiphytic symbionts, indicating that these organisms were present, alive, and metabolically active. Here, we show that these serendipitously sequenced transcripts need not be considered merely as contamination, as is common, but that they provide insight into the plant’s phyllosphere. Notably, we could classify these transcripts as originating predominantly from Dothideomycetes and Leotiomycetes species, with functional annotation of gene families indicating active growth and metabolism, with particular regards to glucose intake and processing, as well as gene regulation. [ABSTRACT FROM AUTHOR]
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- 2015
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17. Modular and configurable optimal sequence alignment software: Cola.
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Zamani, Neda, Sundström, Görel, Höppner, Marc P., and Grabherr, Manfred G.
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NUCLEOTIDE sequencing ,NUCLEOTIDES ,GENETIC algorithms ,COMPUTER software ,MATHEMATICAL analysis - Abstract
Background The fundamental challenge in optimally aligning homologous sequences is to define a scoring scheme that best reflects the underlying biological processes. Maximising the overall number of matches in the alignment does not always reflect the patterns by which nucleotides mutate. Efficiently implemented algorithms that can be parameterised to accommodate more complex non-linear scoring schemes are thus desirable. Results We present Cola, alignment software that implements different optimal alignment algorithms, also allowing for scoring contiguous matches of nucleotides in a nonlinear manner. The latter places more emphasis on short, highly conserved motifs, and less on the surrounding nucleotides, which can be more diverged. To illustrate the differences, we report results from aligning 14,100 sequences from 3' untranslated regions of human genes to 25 of their mammalian counterparts, where we found that a nonlinear scoring scheme is more consistent than a linear scheme in detecting short, conserved motifs. Conclusions Cola is freely available under LPGL from https://github.com/nedaz/cola. [ABSTRACT FROM AUTHOR]
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- 2014
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18. A universal genomic coordinate translator for comparative genomics.
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Zamani, Neda, Sundström, Görel, Meadows, Jennifer R. S., Höppner, Marc P., Dainat, Jacques, Lantz, Henrik, Haas, Brian J., and Grabherr, Manfred G.
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COMPARATIVE genomics ,DNA replication ,GRAPH theory ,PAIRED comparisons (Mathematics) ,DROSOPHILA ,CROSS-species amplification - Abstract
Background Genomic duplications constitute major events in the evolution of species, allowing paralogous copies of genes to take on fine-tuned biological roles. Unambiguously identifying the orthology relationship between copies across multiple genomes can be resolved by synteny, i.e. the conserved order of genomic sequences. However, a comprehensive analysis of duplication events and their contributions to evolution would require all-to-all genome alignments, which increases at N
2 with the number of available genomes, N. Results Here, we introduce Kraken, software that omits the all-to-all requirement by recursively traversing a graph of pairwise alignments and dynamically re-computing orthology. Kraken scales linearly with the number of targeted genomes, N, which allows for including large numbers of genomes in analyses. We first evaluated the method on the set of 12 Drosophila genomes, finding that orthologous correspondence computed indirectly through a graph of multiple synteny maps comes at minimal cost in terms of sensitivity, but reduces overall computational runtime by an order of magnitude. We then used the method on three well-annotated mammalian genomes, human, mouse, and rat, and show that up to 93% of protein coding transcripts have unambiguous pairwise orthologous relationships across the genomes. On a nucleotide level, 70 to 83% of exons match exactly at both splice junctions, and up to 97% on at least one junction. We last applied Kraken to an RNA-sequencing dataset from multiple vertebrates and diverse tissues, where we confirmed that brain-specific gene family members, i.e. one-to-many or many-to-many homologs, are more highly correlated across species than single-copy (i.e. one-to-one homologous) genes. Not limited to protein coding genes, Kraken also identifies thousands of newly identified transcribed loci, likely non-coding RNAs that are consistently transcribed in human, chimpanzee and gorilla, and maintain significant correlation of expression levels across species. Conclusions Kraken is a computational genome coordinate translator that facilitates cross-species comparisons, distinguishes orthologs from paralogs, and does not require costly all-to-all whole genome mappings. Kraken is freely available under LPGL from http://github.com/nedaz/kraken. [ABSTRACT FROM AUTHOR]- Published
- 2014
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19. Artificially designed promoters.
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Baumann, Martina, Höppner, Marc P., Meier, Michael, Pontiller, Jens, Ernst, Wolfgang, Grabherr, Reingard, Mauceli, Evan, and Grabherr, Manfred G.
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- 2012
20. Ascorbic Acid/Retinol and/or Inflammatory Stimuli's Effect on Proliferation/Differentiation Properties and Transcriptomics of Gingival Stem/Progenitor Cells.
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Fawzy El-Sayed, Karim M., Bittner, Amira, Schlicht, Kristina, Mekhemar, Mohamed, Enthammer, Kim, Höppner, Marc, Es-Souni, Martha, Schulz, Juliane, Laudes, Matthias, Graetz, Christian, Dörfer, Christof E., and Schulte, Dominik M.
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VITAMIN C ,CELL migration ,VITAMIN A ,PROGENITOR cells ,MESENCHYMAL stem cells ,GINGIVA - Abstract
The present study explored the effects of ascorbic-acid (AA)/retinol and timed inflammation on the stemness, the regenerative potential, and the transcriptomics profile of gingival mesenchymal stem/progenitor cells' (G-MSCs). STRO-1 (mesenchymal stem cell marker) immuno-magnetically sorted G-MSCs were cultured in basic medium (control group), in basic medium with IL-1β (1 ng/mL), TNF-α (10 ng/mL) and IFN-γ (100 ng/mL, inflammatory-medium), in basic medium with AA (250 µmol/L) and retinol (20 µmol/L) (AA/retinol group) or in inflammatory medium with AA/retinol (inflammatory/AA/retinol group; n = 5/group). The intracellular levels of phosphorylated and total β-Catenin at 1 h, the expression of stemness genes over 7 days, the number of colony-forming units (CFUs) as well as the cellular proliferation aptitude over 14 days, and the G-MSCs' multilineage differentiation potential were assessed. Next-generation sequencing was undertaken to elaborate on up-/downregulated genes and altered intracellular pathways. G-MSCs demonstrated all mesenchymal stem/progenitor cells characteristics. Controlled inflammation with AA/retinol significantly elevated NANOG (p < 0.05). The AA/retinol-mediated reduction in intracellular phosphorylated β-Catenin was restored through the effect of controlled inflammation (p < 0.05). Cellular proliferation was highest in the AA/retinol group (p < 0.05). AA/retinol counteracted the inflammation-mediated reduction in G-MSCs' clonogenic ability and CFUs. Amplified chondrogenic differentiation was observed in the inflammatory/AA/retinol group. At 1 and 3 days, the differentially expressed genes were associated with development, proliferation, and migration (FOS, EGR1, SGK1, CXCL5, SIPA1L2, TFPI2, KRATP1-5), survival (EGR1, SGK1, TMEM132A), differentiation and mineral absorption (FOS, EGR1, MT1E, KRTAP1-5, ASNS, PSAT1), inflammation and MHC-II antigen processing (PER1, CTSS, CD74) and intracellular pathway activation (FKBP5, ZNF404). Less as well as more genes were activated the longer the G-MSCs remained in the inflammatory medium or AA/retinol, respectively. Combined, current results point at possibly interesting interactions between controlled inflammation or AA/retinol affecting stemness, proliferation, and differentiation attributes of G-MSCs. [ABSTRACT FROM AUTHOR]
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- 2021
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21. An Improved Canine Genome and a Comprehensive Catalogue of Coding Genes and Non-Coding Transcripts
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Hoeppner, Marc P., Lundquist, Andrew, Pirun, Mono, Meadows, Jennifer R. S., Zamani, Neda, Johnson, Jeremy, Sundström, Görel, Cook, April, FitzGerald, Michael G., Swofford, Ross, Mauceli, Evan, Moghadam, Behrooz Torabi, Greka, Anna, Alföldi, Jessica, Abouelleil, Amr, Aftuck, Lynne, Bessette, Daniel, Berlin, Aaron, Brown, Adam, Gearin, Gary, Lui, Annie, Macdonald, J. Pendexter, Priest, Margaret, Shea, Terrance, Turner-Maier, Jason, Zimmer, Andrew, Lander, Eric S., di Palma, Federica, Lindblad-Toh, Kerstin, and Grabherr, Manfred G.
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Biology ,Biotechnology ,Computational Biology ,Evolutionary Biology ,Genetics ,Genomics ,Genome Analysis Tools ,Transcriptomes ,Genome Sequencing ,Microbiology ,Model Organisms ,Computer Science ,Computing Methods ,Software Engineering - Abstract
The domestic dog, Canis familiaris, is a well-established model system for mapping trait and disease loci. While the original draft sequence was of good quality, gaps were abundant particularly in promoter regions of the genome, negatively impacting the annotation and study of candidate genes. Here, we present an improved genome build, canFam3.1, which includes 85 MB of novel sequence and now covers 99.8% of the euchromatic portion of the genome. We also present multiple RNA-Sequencing data sets from 10 different canine tissues to catalog ∼175,000 expressed loci. While about 90% of the coding genes previously annotated by EnsEMBL have measurable expression in at least one sample, the number of transcript isoforms detected by our data expands the EnsEMBL annotations by a factor of four. Syntenic comparison with the human genome revealed an additional ∼3,000 loci that are characterized as protein coding in human and were also expressed in the dog, suggesting that those were previously not annotated in the EnsEMBL canine gene set. In addition to ∼20,700 high-confidence protein coding loci, we found ∼4,600 antisense transcripts overlapping exons of protein coding genes, ∼7,200 intergenic multi-exon transcripts without coding potential, likely candidates for long intergenic non-coding RNAs (lincRNAs) and ∼11,000 transcripts were reported by two different library construction methods but did not fit any of the above categories. Of the lincRNAs, about 6,000 have no annotated orthologs in human or mouse. Functional analysis of two novel transcripts with shRNA in a mouse kidney cell line altered cell morphology and motility. All in all, we provide a much-improved annotation of the canine genome and suggest regulatory functions for several of the novel non-coding transcripts.
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- 2014
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22. Free Air in the Abdomen.
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Kiehn, Felix K., Höppner, Marc, and Glatzle, Jörg
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The article describes the case of a 92-year-old woman who had lower abdominal peritoneal signs and presumed diagnosis of perforated sigmoid diverticulitis.
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- 2017
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23. Coherent order parameter oscillations in the ground state of the excitonic insulator Ta2NiSe5.
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Werdehausen, Daniel, Tomohiro Takayama, Höppner, Marc, Albrecht, Gelon, Rost, Andreas W., Yangfan Lu, Dirk Manske, Takagi, Hidenori, and Kaiser, Stefan
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- *
COLLECTIVE excitations , *ELECTRIC insulators & insulation , *GROUND state energy , *BAND gaps , *PHONONS - Abstract
The article presents a study of the collective excitations in Ta2NiSe5 to prove the coherent order parameter oscillations in the ground state of the bandgap semiconductor. It demonstrates the existence of a coherent amplitude response in the excitonic insulator (EI) Ta2NiSe5, identifying a phonon-coupled state of the condensate characterizing the transient order parameter of the EI as a function of excitation and temperature density.
- Published
- 2018
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24. Coherent order parameter oscillations in the ground state of the excitonic insulator Ta 2 NiSe 5 .
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Werdehausen D, Takayama T, Höppner M, Albrecht G, Rost AW, Lu Y, Manske D, Takagi H, and Kaiser S
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The excitonic insulator is an intriguing electronic phase of condensed excitons. A prominent candidate is the small bandgap semiconductor Ta
2 NiSe5 , in which excitons are believed to undergo a Bose-Einstein condensation-like transition. However, direct experimental evidence for the existence of a coherent condensate in this material is still missing. A direct fingerprint of such a state would be the observation of its collective modes, which are equivalent to the Higgs and Goldstone modes in superconductors. We report evidence for the existence of a coherent amplitude response in the excitonic insulator phase of Ta2 NiSe5 . Using nonlinear excitations with short laser pulses, we identify a phonon-coupled state of the condensate that can be understood as a novel amplitude mode. The condensate density contribution substantiates the picture of an electronically driven phase transition and characterizes the transient order parameter of the excitonic insulator as a function of temperature and excitation density.- Published
- 2018
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25. The genetic basis for ecological adaptation of the Atlantic herring revealed by genome sequencing.
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Martinez Barrio A, Lamichhaney S, Fan G, Rafati N, Pettersson M, Zhang H, Dainat J, Ekman D, Höppner M, Jern P, Martin M, Nystedt B, Liu X, Chen W, Liang X, Shi C, Fu Y, Ma K, Zhan X, Feng C, Gustafson U, Rubin CJ, Sällman Almén M, Blass M, Casini M, Folkvord A, Laikre L, Ryman N, Ming-Yuen Lee S, Xu X, and Andersson L
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- Animals, Atlantic Ocean, Fishes classification, Fishes physiology, Genetics, Population, Genomics, Saline Waters, Seawater, Adaptation, Biological, Fishes genetics, Genetic Variation
- Abstract
Ecological adaptation is of major relevance to speciation and sustainable population management, but the underlying genetic factors are typically hard to study in natural populations due to genetic differentiation caused by natural selection being confounded with genetic drift in subdivided populations. Here, we use whole genome population sequencing of Atlantic and Baltic herring to reveal the underlying genetic architecture at an unprecedented detailed resolution for both adaptation to a new niche environment and timing of reproduction. We identify almost 500 independent loci associated with a recent niche expansion from marine (Atlantic Ocean) to brackish waters (Baltic Sea), and more than 100 independent loci showing genetic differentiation between spring- and autumn-spawning populations irrespective of geographic origin. Our results show that both coding and non-coding changes contribute to adaptation. Haplotype blocks, often spanning multiple genes and maintained by selection, are associated with genetic differentiation.
- Published
- 2016
- Full Text
- View/download PDF
26. Artificially designed promoters: understanding the role of spatial features and canonical binding sites in transcription.
- Author
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Baumann M, Höppner MP, Meier M, Pontiller J, Ernst W, Grabherr R, Mauceli E, and Grabherr MG
- Subjects
- Base Sequence, Binding Sites genetics, Cell Line, Dinucleoside Phosphates genetics, Dinucleoside Phosphates metabolism, Gene Expression Regulation, HEK293 Cells, Humans, Molecular Sequence Data, NF-kappa B genetics, CpG Islands, NF-kappa B metabolism, Promoter Regions, Genetic
- Abstract
The promoter is a key element in gene transcription and regulation. We previously reported that artificial sequences rich in the dinucleotide CpG are sufficient to drive expression in vitro in mammalian cell lines, without requiring canonical binding sites for transcription factor proteins. Here, we report that introducing a promoter organization that alternates in CpGs and regions rich in A and T further increases expression strength, as well as how insertion of specific binding sites makes such sequences respond to induced levels of the transcription factor NFκB. Our findings further contribute to the mechanistic understanding of promoters, as well as how these sequences might be shaped by evolutionary pressure in living organisms.
- Published
- 2012
- Full Text
- View/download PDF
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