Gotowa bibliografia na temat „Bioinformatics”
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Artykuły w czasopismach na temat "Bioinformatics"
Bottomley, S. "Bioinformatics: guide for evaluating bioinformatic software". Drug Discovery Today 4, nr 5 (1.05.1999): 240–43. http://dx.doi.org/10.1016/s1359-6446(99)01352-5.
Pełny tekst źródłaEldəniz qızı Əhmədova, Gülnarə. "Inclusion of bioinformatics in biological sciences". NATURE AND SCIENCE 22, nr 7 (17.07.2022): 82–86. http://dx.doi.org/10.36719/2707-1146/22/82-86.
Pełny tekst źródłaKangueane, Pandjassarame. "Biotechnology, Bioinformatics and BIOINFORMATION in an autobiography". Bioinformation 16, nr 1 (31.01.2020): 39–50. http://dx.doi.org/10.6026/97320630016039.
Pełny tekst źródłaKangueane, Pandjassarame. "Biotechnology, Bioinformatics and BIOINFORMATION in an autobiography". Bioinformation 16, nr 1 (31.01.2020): 39–50. http://dx.doi.org/10.6026/97320630016050.
Pełny tekst źródłaLee, Byung-Wook, In-Sun Chu, Nam-Shin Kim, Jin-Hyuk Lee, Seon-Yong Kim, Wan-Kyu Kim i Sang-Hyuk Lee. "Bioinformatics Resources of the Korean Bioinformation Center (KOBIC)". Genomics & Informatics 8, nr 4 (31.12.2010): 165–69. http://dx.doi.org/10.5808/gi.2010.8.4.165.
Pełny tekst źródłaPalsson, Bernhard O. "Bioinformatics: What lies beyond bioinformatics?" Nature Biotechnology 15, nr 1 (styczeń 1997): 3–4. http://dx.doi.org/10.1038/nbt0197-3.
Pełny tekst źródłaSantos, Sílvia Regina Cavani Jorge. "Bioinformatics". Brazilian Journal of Pharmaceutical Sciences 47, nr 1 (marzec 2011): 193. http://dx.doi.org/10.1590/s1984-82502011000100024.
Pełny tekst źródłaBrokaw, Stephen. "Bioinformatics:". Journal of Pharmaceutical Marketing & Management 16, nr 4 (13.10.2005): 65–80. http://dx.doi.org/10.1300/j058v16n04_04.
Pełny tekst źródłaPersidis, Aris. "Bioinformatics". Nature Biotechnology 17, nr 8 (sierpień 1999): 828–30. http://dx.doi.org/10.1038/11793.
Pełny tekst źródłaDoom, T., M. Raymerand i D. Krane. "Bioinformatics". IEEE Potentials 23, nr 1 (luty 2004): 24–27. http://dx.doi.org/10.1109/mp.2004.1266936.
Pełny tekst źródłaRozprawy doktorskie na temat "Bioinformatics"
Hvidsten, Torgeir R. "Predicting Function of Genes and Proteins from Sequence, Structure and Expression Data". Doctoral thesis, Uppsala : Acta Universitatis Upsaliensis : Univ.-bibl. [distributör], 2004. http://urn.kb.se/resolve?urn=urn:nbn:se:uu:diva-4490.
Pełny tekst źródłaHooper, Sean. "Dynamics of Microbial Genome Evolution". Doctoral thesis, Uppsala University, Molecular Evolution, 2003. http://urn.kb.se/resolve?urn=urn:nbn:se:uu:diva-3283.
Pełny tekst źródłaThe success of microbial life on Earth can be attributed not only to environmental factors, but also to the surprising hardiness, adaptability and flexibility of the microbes themselves. They are able to quickly adapt to new niches or circumstances through gene evolution and also by sheer strength of numbers, where statistics favor otherwise rare events.
An integral part of adaptation is the plasticity of the genome; losing and acquiring genes depending on whether they are needed or not. Genomes can also be the birthplace of new gene functions, by duplicating and modifying existing genes. Genes can also be acquired from outside, transcending species boundaries. In this work, the focus is set primarily on duplication, deletion and import (lateral transfer) of genes – three factors contributing to the versatility and success of microbial life throughout the biosphere.
We have developed a compositional method of identifying genes that have been imported into a genome, and the rate of import/deletion turnover has been appreciated in a number of organisms. Furthermore, we propose a model of genome evolution by duplication, where through the principle of gene amplification, novel gene functions are discovered within genes with weak- or secondary protein functions. Subsequently, the novel function is maintained by selection and eventually optimized. Finally, we discuss a possible synergic link between lateral transfer and duplicative processes in gene innovation.
Snøve, Jr Ola. "Hardware-accelerated analysis of non-protein-coding RNAs". Doctoral thesis, Norwegian University of Science and Technology, Faculty of Information Technology, Mathematics and Electrical Engineering, 2005. http://urn.kb.se/resolve?urn=urn:nbn:no:ntnu:diva-713.
Pełny tekst źródłaA tremendous amount of genomic sequence data of relatively high quality has become publicly available due to the human genome sequencing projects that were completed a few years ago. Despite considerable efforts, we do not yet know everything that is to know about the various parts of the genome, what all the regions code for, and how their gene products contribute in the myriad of biological processes that are performed within the cells. New high-performance methods are needed to extract knowledge from this vast amount of information.
Furthermore, the traditional view that DNA codes for RNA that codes for protein, which is known as the central dogma of molecular biology, seems to be only part of the story. The discovery of many non-proteincoding gene families with housekeeping and regulatory functions brings an entirely new perspective to molecular biology. Also, sequence analysis of the new gene families require new methods, as there are significant differences between protein-coding and non-protein-coding genes.
This work describes a new search processor that can search for complex patterns in sequence data for which no efficient lookup-index is known. When several chips are mounted on search cards that are fitted into PCs in a small cluster configuration, the system’s performance is orders of magnitude higher than that of comparable solutions for selected applications. The applications treated in this work fall into two main categories, namely pattern screening and data mining, and both take advantage of the search capacity of the cluster to achieve adequate performance. Specifically, the thesis describes an interactive system for exploration of all types of genomic sequence data. Moreover, a genetic programming-based data mining system finds classifiers that consist of potentially complex patterns that are characteristic for groups of sequences. The screening and mining capacity has been used to develop an algorithm for identification of new non-protein-coding genes in bacteria; a system for rational design of effective and specific short interfering RNA for sequence-specific silencing of protein-coding genes; and an improved algorithmic step for identification of new regulatory targets for the microRNA family of non-protein-coding genes.
Paper V, VI, and VII are reprinted with kind permision of Elsevier, sciencedirect.com
Björkholm, Patrik. "Method for recognizing local descriptors of protein structures using Hidden Markov Models". Thesis, Linköping University, The Department of Physics, Chemistry and Biology, 2008. http://urn.kb.se/resolve?urn=urn:nbn:se:liu:diva-11408.
Pełny tekst źródłaBeing able to predict the sequence-structure relationship in proteins will extend the scope of many bioinformatics tools relying on structure information. Here we use Hidden Markov models (HMM) to recognize and pinpoint the location in target sequences of local structural motifs (local descriptors of protein structure, LDPS) These substructures are composed of three or more segments of amino acid backbone structures that are in proximity with each other in space but not necessarily along the amino acid sequence. We were able to align descriptors to their proper locations in 41.1% of the cases when using models solely built from amino acid information. Using models that also incorporated secondary structure information, we were able to assign 57.8% of the local descriptors to their proper location. Further enhancements in performance was yielded when threading a profile through the Hidden Markov models together with the secondary structure, with this material we were able assign 58,5% of the descriptors to their proper locations. Hidden Markov models were shown to be able to locate LDPS in target sequences, the performance accuracy increases when secondary structure and the profile for the target sequence were used in the models.
Keller, Jens. "Clustering biological data using a hybrid approach : Composition of clusterings from different features". Thesis, University of Skövde, School of Humanities and Informatics, 2008. http://urn.kb.se/resolve?urn=urn:nbn:se:his:diva-1078.
Pełny tekst źródłaClustering of data is a well-researched topic in computer sciences. Many approaches have been designed for different tasks. In biology many of these approaches are hierarchical and the result is usually represented in dendrograms, e.g. phylogenetic trees. However, many non-hierarchical clustering algorithms are also well-established in biology. The approach in this thesis is based on such common algorithms. The algorithm which was implemented as part of this thesis uses a non-hierarchical graph clustering algorithm to compute a hierarchical clustering in a top-down fashion. It performs the graph clustering iteratively, with a previously computed cluster as input set. The innovation is that it focuses on another feature of the data in each step and clusters the data according to this feature. Common hierarchical approaches cluster e.g. in biology, a set of genes according to the similarity of their sequences. The clustering then reflects a partitioning of the genes according to their sequence similarity. The approach introduced in this thesis uses many features of the same objects. These features can be various, in biology for instance similarities of the sequences, of gene expression or of motif occurences in the promoter region. As part of this thesis not only the algorithm itself was implemented and evaluated, but a whole software also providing a graphical user interface. The software was implemented as a framework providing the basic functionality with the algorithm as a plug-in extending the framework. The software is meant to be extended in the future, integrating a set of algorithms and analysis tools related to the process of clustering and analysing data not necessarily related to biology.
The thesis deals with topics in biology, data mining and software engineering and is divided into six chapters. The first chapter gives an introduction to the task and the biological background. It gives an overview of common clustering approaches and explains the differences between them. Chapter two shows the idea behind the new clustering approach and points out differences and similarities between it and common clustering approaches. The third chapter discusses the aspects concerning the software, including the algorithm. It illustrates the architecture and analyses the clustering algorithm. After the implementation the software was evaluated, which is described in the fourth chapter, pointing out observations made due to the use of the new algorithm. Furthermore this chapter discusses differences and similarities to related clustering algorithms and software. The thesis ends with the last two chapters, namely conclusions and suggestions for future work. Readers who are interested in repeating the experiments which were made as part of this thesis can contact the author via e-mail, to get the relevant data for the evaluation, scripts or source code.
Chawade, Aakash. "Inferring Gene Regulatory Networks in Cold-Acclimated Plants by Combinatorial Analysis of mRNA Expression Levels and Promoter Regions". Thesis, University of Skövde, School of Humanities and Informatics, 2006. http://urn.kb.se/resolve?urn=urn:nbn:se:his:diva-20.
Pełny tekst źródłaUnderstanding the cold acclimation process in plants may help us develop genetically engineered plants that are resistant to cold. The key factor in understanding this process is to study the genes and thus the gene regulatory network that is involved in the cold acclimation process. Most of the existing approaches1-8 in deriving regulatory networks rely only on the gene expression data. Since the expression data is usually noisy and sparse the networks generated by these approaches are usually incoherent and incomplete. Hence a new approach is proposed here that analyzes the promoter regions along with the expression data in inferring the regulatory networks. In this approach genes are grouped into sets if they contain similar over-represented motifs or motif pairs in their promoter regions and if their expression pattern follows the expression pattern of the regulating gene. The network thus derived is evaluated using known literature evidence, functional annotations and from statistical tests.
Muhammad, Ashfaq. "Design and Development of a Database for the Classification of Corynebacterium glutamicum Genes, Proteins, Mutants and Experimental Protocols". Thesis, University of Skövde, School of Humanities and Informatics, 2006. http://urn.kb.se/resolve?urn=urn:nbn:se:his:diva-23.
Pełny tekst źródłaCoryneform bacteria are largely distributed in nature and are rod like, aerobic soil bacteria capable of growing on a variety of sugars and organic acids. Corynebacterium glutamicum is a nonpathogenic species of Coryneform bacteria used for industrial production of amino acids. There are three main publicly available genome annotations, Cg, Cgl and NCgl for C. glutamicum. All these three annotations have different numbers of protein coding genes and varying numbers of overlaps of similar genes. The original data is only available in text files. In this format of genome data, it was not easy to search and compare the data among different annotations and it was impossible to make an extensive multidimensional customized formal search against different protein parameters. Comparison of all genome annotations for construction deletion, over-expression mutants, graphical representation of genome information, such as gene locations, neighboring genes, orientation (direct or complementary strand), overlapping genes, gene lengths, graphical output for structure function relation by comparison of predicted trans-membrane domains (TMD) and functional protein domains protein motifs was not possible when data is inconsistent and redundant on various publicly available biological database servers. There was therefore a need for a system of managing the data for mutants and experimental setups. In spite of the fact that the genome sequence is known, until now no databank providing such a complete set of information has been available. We solved these problems by developing a standalone relational database software application covering data processing, protein-DNA sequence extraction and
management of lab data. The result of the study is an application named, CORYNEBASE, which is a software that meets our aims and objectives.
Chen, Lei. "Construction of Evolutionary Tree Models for Oncogenesis of Endometrial Adenocarcinoma". Thesis, University of Skövde, School of Humanities and Informatics, 2005. http://urn.kb.se/resolve?urn=urn:nbn:se:his:diva-25.
Pełny tekst źródłaEndometrial adenocarcinoma (EAC) is the fourth leading cause of carcinoma in woman worldwide, but not much is known about genetic factors involved in this complex disease. During the EAC process, it is well known that losses and gains of chromosomal regions do not occur completely at random, but partly through some flow of causality. In this work, we used three different algorithms based on frequency of genomic alterations to construct 27 tree models of oncogenesis. So far, no study about applying pathway models to microsatellite marker data had been reported. Data from genome–wide scans with microsatellite markers were classified into 9 data sets, according to two biological approaches (solid tumor cell and corresponding tissue culture) and three different genetic backgrounds provided by intercrossing the susceptible rat BDII strain and two normal rat strains. Compared to previous study, similar conclusions were drawn from tree models that three main important regions (I, II and III) and two subordinate regions (IV and V) are likely to be involved in EAC development. Further information about these regions such as their likely order and relationships was produced by the tree models. A high consistency in tree models and the relationship among p19, Tp53 and Tp53 inducible
protein genes provided supportive evidence for the reliability of results.
Dodda, Srinivasa Rao. "Improvements and extensions of a web-tool for finding candidate genes associated with rheumatoid arthritis". Thesis, University of Skövde, School of Humanities and Informatics, 2005. http://urn.kb.se/resolve?urn=urn:nbn:se:his:diva-26.
Pełny tekst źródłaQuantitativeTraitLocus (QTL) is a statistical method used to restrict genomic regions contributing to specific phenotypes. To further localize genes in such regions a web tool called “Candidate Gene Capture” (CGC) was developed by Andersson et al. (2005). The CGC tool was based on the textual description of genes defined in the human phenotype database OMIM. Even though the CGC tool works well, the tool was limited by a number of inconsistencies in the underlying database structure, static web pages and some gene descriptions without properly defined function in the OMIM database. Hence, in this work the CGC tool was improved by redesigning its database structure, adding dynamic web pages and improving the prediction of unknown gene function by using exon analysis. The changes in database structure diminished the number of tables considerably, eliminated redundancies and made data retrieval more efficient. A new method for prediction of gene function was proposed, based on the assumption that similarity between exon sequences is associated with biochemical function. Using Blast with 20380 exon protein sequences and a threshold E-value of 0.01, 639 exon groups were obtained with an average of 11 exons per group. When estimating the functional similarity, it was found that on the average 72% of the exons in a group had at least one Gene Ontology (GO) term in common.
Huque, Enamul. "Shape Analysis and Measurement for the HeLa cell classification of cultured cells in high throughput screening". Thesis, University of Skövde, School of Humanities and Informatics, 2006. http://urn.kb.se/resolve?urn=urn:nbn:se:his:diva-27.
Pełny tekst źródłaFeature extraction by digital image analysis and cell classification is an important task for cell culture automation. In High Throughput Screening (HTS) where thousands of data points are generated and processed at once, features will be extracted and cells will be classified to make a decision whether the cell-culture is going on smoothly or not. The culture is restarted if a problem is detected. In this thesis project HeLa cells, which are human epithelial cancer cells, are selected for the experiment. The purpose is to classify two types of HeLa cells in culture: Cells in cleavage that are round floating cells (stressed or dead cells are also round and floating) and another is, normal growing cells that are attached to the substrate. As the number of cells in cleavage will always be smaller than the number of cells which are growing normally and attached to the substrate, the cell-count of attached cells should be higher than the round cells. There are five different HeLa cell images that are used. For each image, every single cell is obtained by image segmentation and isolation. Different mathematical features are found for each cell. The feature set for this experiment is chosen in such a way that features are robust, discriminative and have good generalisation quality for classification. Almost all the features presented in this thesis are rotation, translation and scale invariant so that they are expected to perform well in discriminating objects or cells by any classification algorithm. There are some new features added which are believed to improve the classification result. The feature set is considerably broad rather than in contrast with the restricted sets which have been used in previous work. These features are used based on a common interface so that the library can be extended and integrated into other applications. These features are fed into a machine learning algorithm called Linear Discriminant Analysis (LDA) for classification. Cells are then classified as ‘Cells attached to the substrate’ or Cell Class A and ‘Cells in cleavage’ or Cell Class B. LDA considers features by leaving and adding shape features for increased performance. On average there is higher than ninety five percent accuracy obtained in the classification result which is validated by visual classification.
Książki na temat "Bioinformatics"
Andrew, French, i Westhead David R, red. Bioinformatics. Wyd. 2. Milton Park, Abingdon [Oxon]: Taylor & Francis, 2010.
Znajdź pełny tekst źródłaKeith, Jonathan M., red. Bioinformatics. New York, NY: Springer New York, 2017. http://dx.doi.org/10.1007/978-1-4939-6613-4.
Pełny tekst źródłaKeith, Jonathan M., red. Bioinformatics. New York, NY: Springer New York, 2017. http://dx.doi.org/10.1007/978-1-4939-6622-6.
Pełny tekst źródłaBaxevanis, Andreas D., i B. F. Francis Ouellette, red. Bioinformatics. New York, USA: John Wiley & Sons, Inc., 2001. http://dx.doi.org/10.1002/0471223921.
Pełny tekst źródłaKeith, Jonathan M., red. Bioinformatics. Totowa, NJ: Humana Press, 2008. http://dx.doi.org/10.1007/978-1-60327-159-2.
Pełny tekst źródłaHofestädt, Ralf, Thomas Lengauer, Markus Löffler i Dietmar Schomburg, red. Bioinformatics. Berlin, Heidelberg: Springer Berlin Heidelberg, 1997. http://dx.doi.org/10.1007/bfb0033198.
Pełny tekst źródłaEdwards, David, Jason Stajich i David Hansen, red. Bioinformatics. New York, NY: Springer New York, 2009. http://dx.doi.org/10.1007/978-0-387-92738-1.
Pełny tekst źródłaKeith, Jonathan M., red. Bioinformatics. Totowa, NJ: Humana Press, 2008. http://dx.doi.org/10.1007/978-1-60327-429-6.
Pełny tekst źródłaRamsden, Jeremy. Bioinformatics. London: Springer London, 2015. http://dx.doi.org/10.1007/978-1-4471-6702-0.
Pełny tekst źródłaBaxevanis, Andreas D., i B. F. Francis Ouellette, red. Bioinformatics. Hoboken, NJ, USA: John Wiley & Sons, Inc., 1998. http://dx.doi.org/10.1002/9780470110607.
Pełny tekst źródłaCzęści książek na temat "Bioinformatics"
Kangueane, Pandjassarame. "Bioinformatics for Bioinformation". W Bioinformation Discovery, 1–31. Cham: Springer International Publishing, 2018. http://dx.doi.org/10.1007/978-3-319-95327-4_1.
Pełny tekst źródłaMiguel Ortega, J., i Fabrício R. Santos. "Bioinformatics". W Omics in Plant Breeding, 167–85. Chichester, UK: John Wiley & Sons, Inc, 2014. http://dx.doi.org/10.1002/9781118820971.ch9.
Pełny tekst źródłaRoy, Somak, Liron Pantanowitz i Anil V. Parwani. "Bioinformatics". W Practical Informatics for Cytopathology, 175–80. New York, NY: Springer New York, 2013. http://dx.doi.org/10.1007/978-1-4614-9581-9_18.
Pełny tekst źródłaBastolla, Ugo. "Bioinformatics". W Encyclopedia of Astrobiology, 177–78. Berlin, Heidelberg: Springer Berlin Heidelberg, 2011. http://dx.doi.org/10.1007/978-3-642-11274-4_1751.
Pełny tekst źródłaMooney, Sean D., Jessica D. Tenenbaum i Russ B. Altman. "Bioinformatics". W Biomedical Informatics, 695–719. London: Springer London, 2013. http://dx.doi.org/10.1007/978-1-4471-4474-8_24.
Pełny tekst źródłaNahler, Gerhard. "bioinformatics". W Dictionary of Pharmaceutical Medicine, 16. Vienna: Springer Vienna, 2009. http://dx.doi.org/10.1007/978-3-211-89836-9_121.
Pełny tekst źródłaJuan, Hsueh-Fen, i Hsuan-Cheng Huang. "Bioinformatics". W Methods in Molecular Biology, 405–16. Totowa, NJ: Humana Press, 2007. http://dx.doi.org/10.1007/978-1-59745-304-2_25.
Pełny tekst źródłaFrenz, Christopher. "Bioinformatics". W Visual Basic and Visual Basic .NET for Scientists and Engineers, 285–304. Berkeley, CA: Apress, 2002. http://dx.doi.org/10.1007/978-1-4302-1139-6_14.
Pełny tekst źródłaBastolla, Ugo. "Bioinformatics". W Encyclopedia of Astrobiology, 286–87. Berlin, Heidelberg: Springer Berlin Heidelberg, 2015. http://dx.doi.org/10.1007/978-3-662-44185-5_1751.
Pełny tekst źródłaSticht, Heinrich. "Bioinformatics". W Chemoinformatics, 497–523. Weinheim, Germany: Wiley-VCH Verlag GmbH & Co. KGaA, 2018. http://dx.doi.org/10.1002/9783527816880.ch13.
Pełny tekst źródłaStreszczenia konferencji na temat "Bioinformatics"
Moore, Jason H. "Bioinformatics". W the 2007 GECCO conference companion. New York, New York, USA: ACM Press, 2007. http://dx.doi.org/10.1145/1274000.1274120.
Pełny tekst źródłaMoore, Jason H. "Bioinformatics". W the 12th annual conference comp. New York, New York, USA: ACM Press, 2010. http://dx.doi.org/10.1145/1830761.1830906.
Pełny tekst źródła"Bioinformatics track - bioinformatics track co-chairs". W 2007 2nd Bio-Inspired Models of Network, Information and Computing Systems. IEEE, 2007. http://dx.doi.org/10.1109/bimnics.2007.4610107.
Pełny tekst źródła"Bioinformatics track - chair: Bioinformatics track co-chairs". W 2007 2nd Bio-Inspired Models of Network, Information and Computing Systems. IEEE, 2007. http://dx.doi.org/10.1109/bimnics.2007.4610110.
Pełny tekst źródłaJones, Warren T., i Hasan M. Jamil. "Bioinformatics track". W the 2002 ACM symposium. New York, New York, USA: ACM Press, 2002. http://dx.doi.org/10.1145/508791.508821.
Pełny tekst źródłaHiew, Hong Liang, Matthew Bellgard, Tuan D. Pham i Xiaobo Zhou. "A Bioinformatics Reference Model: Towards a Framework for Developing and Organising Bioinformatic Resources". W COMPUTATIONAL MODELS FOR LIFE SCIENCES/CMLS '07. AIP, 2007. http://dx.doi.org/10.1063/1.2816640.
Pełny tekst źródłaWasnik, S., P. Donachy, T. Harmer, R. Perrott, P. V. Jithesh, M. McCurley, J. Johnston, M. Townsley i S. Mckee. "GeneGrid: From "Virtual" Bioinformatics Laboratory to "Smart" Bioinformatics Laboratory". W Proceedings. 19th IEEE International Symposium on Computer-Based Medical Systems. IEEE, 2006. http://dx.doi.org/10.1109/cbms.2006.90.
Pełny tekst źródłaGOLOVCO, Stela. "Bioinformatics and applications in genomic research". W Inter/transdisciplinary approaches in the teaching of the real sciences, (STEAM concept) = Abordări inter/transdisciplinare în predarea ştiinţelor reale, (concept STEAM). Ion Creangă Pedagogical State University, 2023. http://dx.doi.org/10.46727/c.steam-2023.p328-333.
Pełny tekst źródła"Applications II: Bioinformatics". W CLADE 2005. Proceedings Challenges of Large Applications in Distributed Environments, 2005. IEEE, 2005. http://dx.doi.org/10.1109/clade.2005.1520900.
Pełny tekst źródłaTENENBAUM, JESSICA D., SUBHA MADHAVAN, ROBERT R. FREIMUTH, JOSHUA C. DENNY i LEWIS FREY. "TRANSLATIONAL BIOINFORMATICS 101". W Proceedings of the Pacific Symposium. WORLD SCIENTIFIC, 2015. http://dx.doi.org/10.1142/9789814749411_0050.
Pełny tekst źródłaRaporty organizacyjne na temat "Bioinformatics"
Davenport, Karen Walston, Chien-Chi Lo, Po-E. Li, Migun Shakya i Patrick Sam Guy Chain. EDGE Bioinformatics. Office of Scientific and Technical Information (OSTI), marzec 2019. http://dx.doi.org/10.2172/1503175.
Pełny tekst źródłaCarr, Peter A., Darrell O. Ricke i Anna Shcherbina. Bioinformatics Challenge Days. Fort Belvoir, VA: Defense Technical Information Center, grudzień 2013. http://dx.doi.org/10.21236/ada591640.
Pełny tekst źródłaTarozzi, Martina Elena. Next Generation Sequencing Technologies, Bioinformatics and Artificial Intelligence: A Shared Time-line. MZB Standard Enterprise, lipiec 2024. http://dx.doi.org/10.57098/scirevs.biology.3.2.2.
Pełny tekst źródłaGary J. Olsen. Bioinformatics for Genome Analysis. Office of Scientific and Technical Information (OSTI), czerwiec 2005. http://dx.doi.org/10.2172/956994.
Pełny tekst źródłaRodriguez Muxica, Natalia. Open configuration options Bioinformatics for Researchers in Life Sciences: Tools and Learning Resources. Inter-American Development Bank, luty 2022. http://dx.doi.org/10.18235/0003982.
Pełny tekst źródłaHolm, Bruce. NYS Center of Excellence in Bioinformatics. Fort Belvoir, VA: Defense Technical Information Center, wrzesień 2005. http://dx.doi.org/10.21236/ada441201.
Pełny tekst źródłaLefkowitz, Elliot J. Development of a Viral Biological-Threat Bioinformatics Resource. Fort Belvoir, VA: Defense Technical Information Center, październik 2003. http://dx.doi.org/10.21236/ada419009.
Pełny tekst źródłaBrueggemeier, Robert W. Drug Discovery and Structural Bioinformatics in Breast Cancer. Fort Belvoir, VA: Defense Technical Information Center, grudzień 1999. http://dx.doi.org/10.21236/ada384146.
Pełny tekst źródłaFlanagan, Meg L., Terrance J. Leighton i Joseph P. Dudley. Anticipating Viral Species Jumps: Bioinformatics and Data Needs. Fort Belvoir, VA: Defense Technical Information Center, czerwiec 2011. http://dx.doi.org/10.21236/ada555216.
Pełny tekst źródłaPedelty, Jonah. Use of Bioinformatics to Prevent Injuries in Sports. Ames (Iowa): Iowa State University, grudzień 2023. http://dx.doi.org/10.31274/cc-20240624-1545.
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