Automated DNA Motif Discovery

Ensembl's human non-coding and protein coding genes are used to automatically find DNA pattern motifs. The Backus-Naur form (BNF) grammar for regular expressions (RE) is used by genetic programming to ensure the generated strings are legal. The evolved motif suggests the presence of Thymine followed by one or more Adenines etc. early in transcripts indicate a non-protein coding gene. Keywords: pseudogene, short and microRNAs, non-coding transcripts, systems biology, machine learning, Bioinformatics, motif, regular expression, strongly typed genetic programming, context-free grammar.Comment: 12 pages, 2 figure

Evolving DNA motifs to predict GeneChip probe performance

Background: Affymetrix High Density Oligonuclotide Arrays (HDONA) simultaneously measure expression of thousands of genes using millions of probes. We use correlations between measurements for the same gene across 6685 human tissue samples from NCBI's GEO database to indicated the quality of individual HG-U133A probes. Low correlation indicates a poor probe. Results: Regular expressions can be automatically created from a Backus-Naur form (BNF) context-free grammar using strongly typed genetic programming. Conclusion: The automatically produced motif is better at predicting poor DNA sequences than an existing human generated RE, suggesting runs of Cytosine and Guanine and mixtures should all be avoided. © 2009 Langdon and Harrison; licensee BioMed Central Ltd

CES-486 A Map of Human Gene Expression

We have calculated the correlation between most human genes, using thousands of public Affymetrix HG-U133 +2 high-density oligonucleotide array (HDONAs). The correspondences show highly structured interactions between EBI Ensembl exons across a wide range of tissues and disease states taken from NCBI GEO. Eigen values are used to find and display the principle components of the gene expression mRNA data. The PCA analysis suggests almost all genes interact in a connected graph. There are thousands of strongly interacting genes but the whole network is sparse, with many genes not correlating strongly. So far, few power laws typical of “small world” networks and anticipated in gene regulatory networks have been found. The �300 million correlations are organised by gene/exon and are available via a web interface

The amniotic fluid cell-free transcriptome in spontaneous preterm labor

The amniotic fluid (AF) cell-free RNA was shown to reflect physiological and pathological processes in pregnancy, but its value in the prediction of spontaneous preterm delivery is unknown. Herein we profiled cell-free RNA in AF samples collected from women who underwent transabdominal amniocentesis after an episode of spontaneous preterm labor and subsequently delivered within 24 h (n = 10) or later (n = 28) in gestation. Expression of known placental single-cell RNA-Seq signatures was quantified in AF cell-free RNA and compared between the groups. Random forest models were applied to predict time-to-delivery after amniocentesis. There were 2385 genes differentially expressed in AF samples of women who delivered within 24 h of amniocentesis compared to gestational age-matched samples from women who delivered after 24 h of amniocentesis. Genes with cell-free RNA changes were associated with immune and inflammatory processes related to the onset of labor, and the expression of placental single-cell RNA-Seq signatures of immune cells was increased with imminent delivery. AF transcriptomic prediction models captured these effects and predicted delivery within 24 h of amniocentesis (AUROC = 0.81). These results may inform the development of biomarkers for spontaneous preterm birth

Probabilistic analysis of the human transcriptome with side information

Understanding functional organization of genetic information is a major challenge in modern biology. Following the initial publication of the human genome sequence in 2001, advances in high-throughput measurement technologies and efficient sharing of research material through community databases have opened up new views to the study of living organisms and the structure of life. In this thesis, novel computational strategies have been developed to investigate a key functional layer of genetic information, the human transcriptome, which regulates the function of living cells through protein synthesis. The key contributions of the thesis are general exploratory tools for high-throughput data analysis that have provided new insights to cell-biological networks, cancer mechanisms and other aspects of genome function. A central challenge in functional genomics is that high-dimensional genomic observations are associated with high levels of complex and largely unknown sources of variation. By combining statistical evidence across multiple measurement sources and the wealth of background information in genomic data repositories it has been possible to solve some the uncertainties associated with individual observations and to identify functional mechanisms that could not be detected based on individual measurement sources. Statistical learning and probabilistic models provide a natural framework for such modeling tasks. Open source implementations of the key methodological contributions have been released to facilitate further adoption of the developed methods by the research community.Comment: Doctoral thesis. 103 pages, 11 figure

Single-cell immune profiling reveals markers of emergency myelopoiesis that distinguish severe from mild respiratory syncytial virus disease in infants

Whereas most infants infected with respiratory syncytial virus (RSV) show no or only mild symptoms, an estimated 3 million children under five are hospitalized annually due to RSV disease. This study aimed to investigate biological mechanisms and associated biomarkers underlying RSV disease heterogeneity in young infants, enabling the potential to objectively categorize RSV-infected infants according to their medical needs. Immunophenotypic and functional profiling demonstrated the emergence of immature and progenitor-like neutrophils, proliferative monocytes (HLA-DRLow, Ki67+), impaired antigen-presenting function, downregulation of T cell response and low abundance of HLA-DRLow B cells in severe RSV disease. HLA-DRLow monocytes were found as a hallmark of RSV-infected infants requiring hospitalization. Complementary transcriptomics identified genes associated with disease severity and pointed to the emergency myelopoiesis response. These results shed new light on mechanisms underlying the pathogenesis and development of severe RSV disease and identified potential new candidate biomarkers for patient stratification

Expression data dnalysis and regulatory network inference by means of correlation patterns

With the advance of high-throughput techniques, the amount of available data in the bio-molecular field is rapidly growing. It is now possible to measure genome-wide aspects of an entire biological system as a whole. Correlations that emerge due to internal dependency structures of these systems entail the formation of characteristic patterns in the corresponding data. The extraction of these patterns has become an integral part of computational biology. By triggering perturbations and interventions it is possible to induce an alteration of patterns, which may help to derive the dependency structures present in the system. In particular, differential expression experiments may yield alternate patterns that we can use to approximate the actual interplay of regulatory proteins and genetic elements, namely, the regulatory network of a cell. In this work, we examine the detection of correlation patterns from bio-molecular data and we evaluate their applicability in terms of protein contact prediction, experimental artifact removal, the discovery of unexpected expression patterns and genome-scale inference of regulatory networks. Correlation patterns are not limited to expression data. Their analysis in the context of conserved interfaces among proteins is useful to estimate whether these may have co-evolved. Patterns that hint on correlated mutations would then occur in the associated protein sequences as well. We employ a conceptually simple sampling strategy to decide whether or not two pathway elements share a conserved interface and are thus likely to be in physical contact. We successfully apply our method to a system of ABC-transporters and two-component systems from the phylum of Firmicute bacteria. For spatially resolved gene expression data like microarrays, the detection of artifacts, as opposed to noise, corresponds to the extraction of localized patterns that resemble outliers in a given region. We develop a method to detect and remove such artifacts using a sliding-window approach. Our method is very accurate and it is shown to adapt to other platforms like custom arrays as well. Further, we developed Padesco as a way to reveal unexpected expression patterns. We extract frequent and recurring patterns that are conserved across many experiments. For a specific experiment, we predict whether a gene deviates from its expected behaviour. We show that Padesco is an effective approach for selecting promising candidates from differential expression experiments. In Chapter 5, we then focus on the inference of genome-scale regulatory networks from expression data. Here, correlation patterns have proven useful for the data-driven estimation of regulatory interactions. We show that, for reliable eukaryotic network inference, the integration of prior networks is essential. We reveal that this integration leads to an over-estimate of network-wide quality estimates and suggest a corrective procedure, CoRe, to counterbalance this effect. CoRe drastically improves the false discovery rate of the originally predicted networks. We further suggest a consensus approach in combination with an extended set of topological features to obtain a more accurate estimate of the eukaryotic regulatory network for yeast. In the course of this work we show how correlation patterns can be detected and how they can be applied for various problem settings in computational molecular biology. We develop and discuss competitive approaches for the prediction of protein contacts, artifact repair, differential expression analysis, and network inference and show their applicability in practical setups.Mit der Weiterentwicklung von Hochdurchsatztechniken steigt die Anzahl verfügbarer Daten im Bereich der Molekularbiologie rapide an. Es ist heute möglich, genomweite Aspekte eines ganzen biologischen Systems komplett zu erfassen. Korrelationen, die aufgrund der internen Abhängigkeits-Strukturen dieser Systeme enstehen, führen zu charakteristischen Mustern in gemessenen Daten. Die Extraktion dieser Muster ist zum integralen Bestandteil der Bioinformatik geworden. Durch geplante Eingriffe in das System ist es möglich Muster-Änderungen auszulösen, die helfen, die Abhängigkeits-Strukturen des Systems abzuleiten. Speziell differentielle Expressions-Experimente können Muster-Wechsel bedingen, die wir verwenden können, um uns dem tatsächlichen Wechselspiel von regulatorischen Proteinen und genetischen Elementen anzunähern, also dem regulatorischen Netzwerk einer Zelle. In der vorliegenden Arbeit beschäftigen wir uns mit der Erkennung von Korrelations-Mustern in molekularbiologischen Daten und schätzen ihre praktische Nutzbarkeit ab, speziell im Kontext der Kontakt-Vorhersage von Proteinen, der Entfernung von experimentellen Artefakten, der Aufdeckung unerwarteter Expressions-Muster und der genomweiten Vorhersage regulatorischer Netzwerke. Korrelations-Muster sind nicht auf Expressions-Daten beschränkt. Ihre Analyse im Kontext konservierter Schnittstellen zwischen Proteinen liefert nützliche Hinweise auf deren Ko-Evolution. Muster die auf korrelierte Mutationen hinweisen, würden in diesem Fall auch in den entsprechenden Proteinsequenzen auftauchen. Wir nutzen eine einfache Sampling-Strategie, um zu entscheiden, ob zwei Elemente eines Pathways eine gemeinsame Schnittstelle teilen, berechnen also die Wahrscheinlichkeit für deren physikalischen Kontakt. Wir wenden unsere Methode mit Erfolg auf ein System von ABC-Transportern und Zwei-Komponenten-Systemen aus dem Firmicutes Bakterien-Stamm an. Für räumlich aufgelöste Expressions-Daten wie Microarrays enspricht die Detektion von Artefakten der Extraktion lokal begrenzter Muster. Im Gegensatz zur Erkennung von Rauschen stellen diese innerhalb einer definierten Region Ausreißer dar. Wir entwickeln eine Methodik, um mit Hilfe eines Sliding-Window-Verfahrens, solche Artefakte zu erkennen und zu entfernen. Das Verfahren erkennt diese sehr zuverlässig. Zudem kann es auf Daten diverser Plattformen, wie Custom-Arrays, eingesetzt werden. Als weitere Möglichkeit unerwartete Korrelations-Muster aufzudecken, entwickeln wir Padesco. Wir extrahieren häufige und wiederkehrende Muster, die über Experimente hinweg konserviert sind. Für ein bestimmtes Experiment sagen wir vorher, ob ein Gen von seinem erwarteten Verhalten abweicht. Wir zeigen, dass Padesco ein effektives Vorgehen ist, um vielversprechende Kandidaten eines differentiellen Expressions-Experiments auszuwählen. Wir konzentrieren uns in Kapitel 5 auf die Vorhersage genomweiter regulatorischer Netzwerke aus Expressions-Daten. Hierbei haben sich Korrelations-Muster als nützlich für die datenbasierte Abschätzung regulatorischer Interaktionen erwiesen. Wir zeigen, dass für die Inferenz eukaryotischer Systeme eine Integration zuvor bekannter Regulationen essentiell ist. Unsere Ergebnisse ergeben, dass diese Integration zur Überschätzung netzwerkübergreifender Qualitätsmaße führt und wir schlagen eine Prozedur - CoRe - zur Verbesserung vor, um diesen Effekt auszugleichen. CoRe verbessert die False Discovery Rate der ursprünglich vorhergesagten Netzwerke drastisch. Weiterhin schlagen wir einen Konsensus-Ansatz in Kombination mit einem erweiterten Satz topologischer Features vor, um eine präzisere Vorhersage für das eukaryotische Hefe-Netzwerk zu erhalten. Im Rahmen dieser Arbeit zeigen wir, wie Korrelations-Muster erkannt und wie sie auf verschiedene Problemstellungen der Bioinformatik angewandt werden können. Wir entwickeln und diskutieren Ansätze zur Vorhersage von Proteinkontakten, Behebung von Artefakten, differentiellen Analyse von Expressionsdaten und zur Vorhersage von Netzwerken und zeigen ihre Eignung im praktischen Einsatz

Automated retrieval and extraction of training course information from unstructured web pages

Web Information Extraction (WIE) is the discipline dealing with the discovery, processing and extraction of specific pieces of information from semi-structured or unstructured web pages. The World Wide Web comprises billions of web pages and there is much need for systems that will locate, extract and integrate the acquired knowledge into organisations practices. There are some commercial, automated web extraction software packages, however their success comes from heavily involving their users in the process of finding the relevant web pages, preparing the system to recognise items of interest on these pages and manually dealing with the evaluation and storage of the extracted results. This research has explored WIE, specifically with regard to the automation of the extraction and validation of online training information. The work also includes research and development in the area of automated Web Information Retrieval (WIR), more specifically in Web Searching (or Crawling) and Web Classification. Different technologies were considered, however after much consideration, Naïve Bayes Networks were chosen as the most suitable for the development of the classification system. The extraction part of the system used Genetic Programming (GP) for the generation of web extraction solutions. Specifically, GP was used to evolve Regular Expressions, which were then used to extract specific training course information from the web such as: course names, prices, dates and locations. The experimental results indicate that all three aspects of this research perform very well, with the Web Crawler outperforming existing crawling systems, the Web Classifier performing with an accuracy of over 95% and a precision of over 98%, and the Web Extractor achieving an accuracy of over 94% for the extraction of course titles and an accuracy of just under 67% for the extraction of other course attributes such as dates, prices and locations. Furthermore, the overall work is of great significance to the sponsoring company, as it simplifies and improves the existing time-consuming, labour-intensive and error-prone manual techniques, as will be discussed in this thesis. The prototype developed in this research works in the background and requires very little, often no, human assistance