The duplication of the Hox gene clusters in teleost fishes

Prohaska, Sonja, Stadler, Peter F.

23 October 2018

Higher teleost fishes, including zebrafish and fugu, have duplicated their Hox genes relative to the gene inventory of other gnathostome lineages. The most widely accepted theory contends that the duplicate Hox clusters orginated synchronously during a single genome duplication event in the early history of ray-finned fishes. In this contribution we collect and re-evaluate all publicly available sequence information. In particular, we show that the short Hox gene fragments from published PCR surveys of the killifish Fundulus heteroclitus, the medaka Oryzias latipes and the goldfish Carassius auratus can be used to determine with little ambiguity not only their paralog group but also their membership in a particular cluster. Together with a survey of the genomic sequence data from the pufferfish Tetraodon nigroviridis we show that at least percomorpha, and possibly all eutelosts, share a system of 7 or 8 orthologous Hox gene clusters. There is little doubt about the orthology of the two teleost duplicates of the HoxA and HoxB clusters. A careful analysis of both the coding sequence of Hox genes and of conserved non-coding sequences provides additional support for the “duplication early” hypothesis that the Hox clusters in teleosts are derived from eight ancestral clusters by means of subsequent gene loss; the data remain ambiguous, however, in particular for the HoxC clusters. Assuming the “duplication early” hypothesis we use the new evidence on the Hox gene complements to determine the phylogenetic positions of gene-loss events in the wake of the cluster duplication. Surprisingly, we find that the resolution of redundancy seems to be a slow process that is still ongoing. A few suggestions on which additional sequence data would be most informative for resolving the history of the teleostean Hox genes are discussed.

info:eu-repo/classification/ddc/572.8

ddc:572.8

Models and Algorithms for Sorting Permutations with Tandem Duplication and Random Loss

Hartmann, Tom

25 April 2019

A central topic of evolutionary biology is the inference of phylogeny, i. e., the evolutionary history of species. A powerful tool for the inference of such phylogenetic relationships is the arrangement of the genes in mitochondrial genomes. The rationale is that these gene arrangements are subject to different types of mutations in the course of evolution. Hence, a high similarity in the gene arrangement between two species indicates a close evolutionary relation. Metazoan mitochondrial gene arrangements are particularly well suited for such phylogenetic studies as they are available for a wide range of species, their gene content is almost invariant, and usually free of duplicates. With these properties gene arrangements of mitochondrial genomes are modeled by permutations in which each element represents a gene, i. e., a specific genetic sequence. The mutations that shape the gene arrangement of genomes are then represented by operations that rearrange elements in permutations, so-called genome rearrangements, and thereby bridge the gap between evolutionary biology and optimization. Many problems of phylogeny inference can be formulated as challenging combinatorial optimization problems which makes this research area especially interesting for computer scientists. The most prominent examples of such optimization problems are the sorting problem and the distance problem. While the sorting problem requires a minimum length sequence of rearrangements that transforms one given permutation into another given permutation, i. e., it aims for a hypothetical scenario of gene order evolution, the distance problem intends to determine only the length of such a sequence. This minimum length is called distance and used as a (dis)similarity measure quantifying the evolutionary relatedness. Most evolutionary changes occurring in gene arrangements of mitochondrial genomes can be explained by the tandem duplication random loss (TDRL) genome rearrangement model. A TDRL consists of a duplication of a consecutive set of genes in tandem followed by a random loss of one copy of each duplicated gene. In spite of the importance of the TDRL genome rearrangement in mitochondrial evolution, its combinatorial properties have rarely been studied. In addition, models of genome rearrangements which include all types of rearrangement that are relevant for mitochondrial genomes, i. e., inversions, transpositions, inverse transpositions, and TDRLs, while admitting computational tractability are rare. Nevertheless, especially for metazoan gene arrangements the TDRL rearrangement should be considered for the reconstruction of phylogeny. Realizing that a better understanding of the TDRL model is indispensable for the study of mitochondrial gene arrangements, the central theme of this thesis is to broaden the horizon of TDRL genome rearrangements with respect to mitochondrial genome evolution. For this purpose, this thesis provides combinatorial properties of the TDRL model and its variants as well as efficient methods for a plausible reconstruction of rearrangement scenarios between gene arrangements. The methods that are proposed consider all types of genome rearrangements that predominately occur during mitochondrial evolution. More precisely, the main points contained in this thesis are as follows: The distance problem and the sorting problem for the TDRL model are further examined in respect to circular permutations, a formal concept that reflects the circular structure of mitochondrial genomes. As a result, a closed formula for the distance is provided. Recently, evidence for a variant of the TDRL rearrangement model in which the duplicated set of genes is additionally inverted have been found. Initiating the algorithmic study of this new rearrangement model on a certain type of permutations, a closed formula solving the distance problem is proposed as well as a quasilinear time algorithm that solves the corresponding sorting problem. The assumption that only one type of genome rearrangement has occurred during the evolution of certain gene arrangements is most likely unrealistic, e. g., at least three types of rearrangements on top of the TDRL rearrangement have to be considered for the evolution metazoan mitochondrial genomes. Therefore, three different biologically motivated constraints are taken into account in this thesis in order to produce plausible evolutionary rearrangement scenarios. The first constraint is extending the considered set of genome rearrangements to the model that covers all four common types of mitochondrial genome rearrangements. For this 4-type model a sharp lower bound and several close additive upper bounds on the distance are developed. As a byproduct, a polynomial-time approximation algorithm for the corresponding sorting problem is provided that guarantees the computation of pairwise rearrangement scenarios that deviate from a minimum length scenario by at most two rearrangement operations. The second biologically motivated constraint is the relative frequency of the different types of rearrangements occurring during the evolution. The frequency is modeled by employing a weighting scheme on the 4-type model in which every rearrangement is weighted with respect to its type. The resulting NP-hard sorting problem is then solved by means of a polynomial size integer linear program. The third biologically motivated constraint that has been taken into account is that certain subsets of genes are often found in close proximity in the gene arrangements of many different species. This observation is reflected by demanding rearrangement scenarios to preserve certain groups of genes which are modeled by common intervals of permutations. In order to solve the sorting problem that considers all three types of biologically motivated constraints, the exact dynamic programming algorithm CREx2 is proposed. CREx2 has a linear runtime for a large class of problem instances. Otherwise, two versions of the CREx2 are provided: The first version provides exact solutions but has an exponential runtime in the worst case and the second version provides approximated solutions efficiently. CREx2 is evaluated by an empirical study for simulated artificial and real biological mitochondrial gene arrangements.

info:eu-repo/classification/ddc/500

ddc:500

Role Kit ligandů v hematopoeze Danio rerio / The role of Kit ligands in hematopoiesis of Danio rerio

Oltová, Jana

January 2020

Hematopoiesis is a precisely regulated process, dependent on the activity of hematopoietic cytokines and their receptors. Due to an extra round of whole genome duplication in teleost fish, two paralogs of many important genes, including some hematopoietic cytokines and their receptors, are present in the zebrafish (Danio rerio) genome. In this project, we have been investigating the role of zebrafish Kit ligands in hematopoiesis. Kit ligand is a pleiotropic cytokine, which is essential for vertebrate erythropoiesis; however, in zebrafish, no such role has been reported so far. To determine the function of zebrafish paralogs of Kit ligand (Kitlga and Kitlgb) in hematopoiesis, we performed in vivo and ex vivo gain- and loss-of-function experiments. Strikingly, we were the first to report the synergistic cooperation of zebrafish Kitlga with erythropoietin and dexamethasone, enabling the growth of kidney marrow-derived suspension cells and providing optimal conditions for the expansion of adult erythroid progenitors. We assume that by using different cytokine combinations, optimal conditions for the growth of other hematopoietic cell types can be established, and therefore, this new approach now available for the...

The Statistical Fate of Genomic DNA : Modelling Match Statistics in Different Evolutionary Scenarios / Le devenir statistique de l'ADN génomique : Modélisation des statistiques d'appariement dans différents scénarios évolutifs

Massip, Florian

02 October 2015

Le but de cette thèse est d'étudier la distribution des tailles des répétitions au sein d'un même génome, ainsi que la distribution des tailles des appariements obtenus en comparant différents génomes. Ces distributions présentent d'importantes déviations par rapport aux prédictions des modèles probabilistes existants. Étonnamment, les déviations observées sont distribuées selon une loi de puissance. Afin d'étudier ce phénomène, nous avons développé des modèles mathématiques prenant en compte des mécanismes évolutifs plus complexes, et qui expliquent les distributions observées. Nous avons aussi implémenté des modèles d'évolution de séquences in silico générant des séquences ayant les mêmes propriétés que les génomes étudiés. Enfin, nous avons montré que nos modèles permettent de tester la qualité des génomes récemment séquencés, et de mettre en évidence la prévalence de certains mécanismes évolutifs dans les génomes eucaryotes. / In this thesis, we study the length distribution of maximal exact matches within and between eukaryotic genomes. These distributions strongly deviate from what one could expect from simple probabilistic models and, surprisingly, present a power-law behavior. To analyze these deviations, we develop mathematical frameworks taking into account complex mechanisms and that reproduce the observed deviations. We also implemented in silico sequence evolution models that reproduce these behaviors. Finally, we show that we can use our framework to assess the quality of sequences of recently sequenced genomes and to highlight the importance of unexpected biological mechanisms in eukaryotic genomes.

Propriétés statistiques des Génomes

Distributions en loi Puissance

Duplications

Modèles évolutifs

Satistical properties of Genome

Scale free distributions

Duplication

Evolutionary models

Differential expression of recent gene duplicates in developmental tissues of <i>Arabidopsis thaliana</i>

Owens, Sarah Marie

14 August 2009

No description available.

Botany

Genetics

Molecular Biology

Gene duplication

recent gene duplicates

differential expression

gene expression

unlinked duplicates

expression divergence

Acquisitions done innovatively: streamlining workflows within the Acquisitions department

Husain, Amjad

January 2017

Yes / In the last 10 years the University of Bradford Library Acquisitions Department has shrunk from 13 members of staff to 5. This has led to us embracing new technology to help streamline workflows within the department. As well as utilising EDI functionality, changing processing workflows and using shelf-ready books, we have devised innovative ways of dealing with everyday tasks. Topics included cover: PDA deduplication; spine labelling on a large scale; the weeding of discarded books; using saved global updates on incoming MARC records and using load profiles innovatively.

Acquisitions

Workflow

Efficiency

Load profiles

Saved global updates

PDA title de-duplication

Spine labelling

Weeding books

Bradford University

Library

Etude du phénomène didactique : le dédoublement des milieux dans l'enseignement ordinaire et dans des ingénieries / Studying the didactic phenomenon : The "duplication of milieu" in ordinary classes and engineering

Kazan, Elie

10 February 2014

Cette thèse s'appuie sur un recueil de données empiriques portant sur l'observation de bifurcations au sein des milieux dans trois situations didactiques : au cycle primaire et au collège, dans des classes ordinaires et dans des ingénieries en France (CE1) et au Liban (EB6/Sixième et EB7/Cinquième). Le cadre théorique mobilisé est celui de la théorie anthropologique du didactique (TAD). Nous nous sommes intéressés aux origines des dédoublements de milieux en observant, d'une part, les rapports du professeur et des élèves à un même milieu, et d'autre part, le rapport de chacun à des milieux différents. Nous avons analysé les praxéologies mobilisées par les professeurs et leurs élèves. Nous avons repéré sur l'échelle des niveaux de codétermination didactique la distance mésogénétique entre le milieu institutionnel du savoir et les milieux personnels activés. La thèse définit quelques-unes des caractéristiques du phénomène didactique « dédoublement des milieux » et étudie certains facteurs génériques qui agissent sur son apparition au sein d'une institution. Ce travail ouvre des perspectives sur la recherche d'autres facteurs à l'origine du phénomène et sur la possibilité de réaliser un critère d'évaluation de la distance entre le milieu institutionnel et les milieux personnels évoqués. / This thesis focus on a report of empirical data talking about the observation of bifurcates within the milieu in three didactic situations: at the primary cycle and the college, in ordinary classes and engineering in France (CE1) and in Lebanon (EB6/ 6th grade and EB7/ 7th grade). The theoric mobilized setting in the one of the anthropological theory of didactics (TAD) of the observer, from one hand, the relationships between the teacher and the students in the same milieu, and in another hand, the relationships of each one on the different milieu. We analyzed the mobilized praxeologies by the teacher and their students. We reported on the levels scab of the didactic codetermination the mesogenetic distance between the institutional milieu of knowing and the personal activated milieu. The thesis define some of the characteristics of the didactic phenomenon « duplication of milieu » and study some generic factors that act on its appearance within an institution.This work opens perspectives on the research of other factors at the origin of the phenomenon and on the possibility of realizing an evaluation criteria of the distance between the institutional milieu and the evocated personal milieu.

Dédoublement des milieux

Bifurcations

Distance mésogénétique

Théorie anthropologique de didactique

Praxéologies

Duplication of the milieu

Mesogenetic distance

Anthropological theory of didactic

Praxeologies.

An Evaluation of Digital Methods in Reverse Engineering Using Selected Medical Applications

Parrott, Andrew Mark

17 November 2006

Student Number : 9710738R - MSc (Eng) dissertation - Faculty of Engineering and the Built Environment / This dissertation investigates the use of digital modeling methods for selected medical applications. The digital methods include the design of a cranial implant, auricular prosthesis and the duplication of an oral prosthesis. The digital process includes imaging, image processing, design and fabrication steps. Three types of imaging used are contact and non-contact measurement systems and CT scanning. The investigation uses a Phantom haptic device for digital design. The implants and prostheses are fabricated using a Thermojet printer and investment casting. Traditional and digital processes are compared using four case studies on selected criteria. The conclusions of the investigation are that a digital process can be used and is equal to or better than traditional methods in prosthesis and implant design.

digital modeling methods

medical applications

cranial implant

auricular prosthesis

duplication of an oral prosthesis

imaging

image processing

design

fabrication steps

Phantom haptic device

Avaliação genotípica de pacientes com polineuropatia inflamatória desmielinizante crônica: estudo da duplicação/deleção do gene PMP22 / Genotypic evaluation of patients with chronic inflammatory demyelinating polyneuropathy: study of the PMP22 gene duplication/delection.

Silva, Alex Eduardo da

09 October 2014

Introdução: Polineuropatias são doenças do sistema nervoso periférico com etiologias variadas. Dentre elas são freqüentes as inflamatórias e as hereditárias, com prevalência de 0,67-7,7/100000 e 7,9-82,3/100000 para polineuropatia inflamatória desmielinizante crônica (PIDC) e Doença de Charcot-Marie-Tooth (CMT), respectivamente. Existem poucas evidências de sobreposição entre estas duas doenças e também algumas dificuldades diagnósticas em situações específicas. Objetivos: Estudar a freqüência de mutações (duplicações e deleções) do gene PMP22 em uma coorte de pacientes inicialmente diagnosticados como PIDC ou suspeitos de apresentarem as duas condições, os sinais e sintomas sugestivos da sobreposição e os fatores implicados em erro de classificação da neuropatia. Métodos: 111 pacientes com diagnóstico de PIDC foram estudados. DNA foi isolado a partir de leucócitos de sangue periférico segundo protocolo padrão. Duplicações e deleções do gene PMP22 foram avaliadas através de marcadores polimórficos do DNA localizados dentro do cromossomo 17p11.2-12, o qual contém o gene PMP22. Achados clínicos e laboratoriais também foram estudados e comparados entre os grupos. Resultados: Dentre os 111 pacientes estudados, mutações no PMP22 foram encontradas em 10 (9%), sendo duplicações em 9 pacientes e deleção em 1 paciente. Concomitância entre PIDC e CMT foi verificada em 4 pacientes (3,6%), todos com duplicação do PMP22. Os outros 6 pacientes foram diagnosticados como CMT puro (5) ou Neuropatia Hereditária Susceptível à Compressão (1), visto que não apresentaram melhora com o uso de tratamento imunomodulador e/ou imunossupressor (5 casos) ou foi estabelecido diagnóstico alternativo associado (1). Os outros 101 pacientes não tiveram duplicação nem deleção deste gene e, portanto, tinham PIDC apenas. Idade média dos pacientes com PIDC/CMT foi de 23,8±18,0 anos e 43,6±19,3 anos para pacientes sem mutações (p=0,04). Houve diferença estatísticamente significativa na resposta ao tratamento entre os grupos PIDC/CMT X CMT (p=0,008) e PIDC X CMT (p=0,00). Ausência de história familiar e presença de doenças e hábitos ligados ao desenvolvimento de neuropatias periféricas, como diabetes mellitus e ingesta de bebidas alcoólicas, por exemplo, bem como achados atípicos na eletroneuromiografia e na biópsia de nervo podem ter contribuído para a confusão diagnóstica nos casos de CMT puro. Conclusões: Alguns pacientes podem desenvolver PIDC em associação com CMT e se beneficiam do tratamento. A neuropatia hereditária poderia predispor à neuropatia inflamatória, uma vez que estes pacientes tendem a apresentar essa condição em idades mais precoces. Cautela deve ser dispensada àqueles pacientes com suspeita diagnóstica de PIDC que não têm os achados clássicos ou não melhoram com o tratamento, uma vez que podem apresentar outras etiologias para a neuropatia, dentre elas uma neuropatia hereditária, como a CMT. / Introduction: Polyneuropathies are peripheral nervous system disorders with a wide range of etiologies. Among them, inflammatory and hereditary are frequent with prevalence of 0.67-7.7/100000 and 7.9-82.3/100000, for chronic inflammatory demyelinating polyneuropathy (CIDP) and Charcot-Marie-Tooth disease (CMT), respectively. There are a few evidence of ovelapping between these two conditions and also some diagnostic difficulties in specific situations. Objectives: To study the frequency of mutations in PMP22 gene (duplications and delections) among a cohort of patients initially diagnosed as CIDP or suspected to have both conditions, the signs and symptoms related to this ovelapping and factors implicated in misdiagnose. Methods: 111 patients with an initially CIDP suspected diagnosis were studied. DNA was isolated from peripheral blood leucocytes following a standard salting-out protocol. Duplications and delections in the PMP22 gene were analysed by polymorphic DNA markers located within the chromosome 17p11.2-12, wich contains the PMP22 gene. Clinical and laboratory findings were also studied and compared within groups. Results: Among 111 patients studied, 10 (9%) were found to harbor mutations in PMP22 gene, specifically duplications in nine and delection in one. We therefore diagnosed CIDP plus CMT in four patients (3.6%), all of them with a duplicated PMP22 gene. The other six patients were diagnosed as pure CMT (5) or Hereditary Neuropathy with liability to Pressure Palsy (1), as they did not improved with the use of immunomodulatory and/or immunosupressive treatment (five cases) or were found to have alternative associated diagnosis (one patient). The other 101 patients did not show duplication nor delection in this gene, so they had CIDP. Mean age of patients with CIDP/CMT were 23.8±18.0 years and 43.6±19.3 years for patients without mutations (p=0.04). There were statistically significant difference in treatmet response between groups CIDP/CMT X CMT (p=0.008) and CIDP X CMT (p=0.00). The lack of family history and presence of other diseases and habits linked to the development of peripheral neuropathies, as diabetes mellitus and alcohol intake, for instance, as well as atypical findings in electrodiagnostic studies and nerve biopsy may have contributed to misdiagnose in the pure CMT cases. Conclusions: Some patients may develop CIDP in association with CMT and have benefit from treatment. The hereditary neuropathy may predispose to the inflammatory neuropathy as these patients tend to show this condition at younger ages. Caution should be dispensed to those patients with a suspected diagnose of CIDP who do not have the classical disease findings or do not improve with treatment, as they can have alternative etiologies for the neuropathy, among them a hereditary neuropathy as CMT disease.

Charcot-Marie-Tooth disease

deleção

delection

doença de Charcot-Marie-Tooth

duplicação

duplication

gene PMP22

overlap

PMP22 gene

polineuropatia

polyneuropathy

sobreposição.

O narrador e seus duplos em Nenhum olhar e em Cemitério de pianos, de José Luís Peixoto / The narrator and his double in Nenhum olhar and Cemitério de pianos, by José Luís Peixoto

Suelotto, Kátia Cristina Franco de Medeiros

24 September 2012

O principal objetivo desta tese é a investigação do foco narrativo nos romances Nenhum olhar e Cemitério de pianos, de José Luís Peixoto, com vistas a defender a hipótese de que o narrador em primeira pessoa promove a assunção de duplos. Ambas as obras trazem personagens que contam a sua história e, no processo da narração, entram em contato consigo mesmas, sob uma perspectiva pautada nas deformações intrínsecas à passagem do tempo. Nesse sentido, a faculdade da memória assume um papel fundamental na relativização do passado. Trata-se, em primeiro lugar, de uma análise do plano da expressão. Concomitante à questão do narrador e seus duplos, observamos que o conteúdo de ambos os romances evoca o tema da busca da salvação. Compreendemos que a concepção de mundo que permeia as referidas obras está pautada na jornada de Cristo na Terra e, em especial, ao drama da Paixão. Concluímos, pois, que, ao desejo do narrador em primeira pessoa de contar a sua história, estão intimamente relacionados o fenômeno do duplo e a negação da morte. Desse modo, por meio da duplicação, as personagens entram em contato com uma realidade supratemporal, fundada no mito. / The main objective of this thesis is the investigation of narrative focus on novels Nenhum olhar and Cemitério de pianos, by José Luís Peixoto, in order to defend the hypothesis that the first-person narrator promotes the assumption of doubles. Both works bring characters to tell their story and in the process of narration, get in touch with themselves, a perspective based on the deformations intrinsic to the passage of time. In this sense, the faculty of memory plays a key role in the relativization of the past. It is, firstly, an analysis of the level of expression. Concomitant with the question of the narrator and his double, we observed that the contents of both novels evoke the theme of the quest for salvation. We understand that the world view that permeates these works is based on the journey of Christ on Earth and in particular the drama of the Passion. Therefore we conclude that the desire of the first-person narrator to tell his story, are closely related to the phenomenon of the double and the denial of death. Thus, by duplicating the characters come into contact with supratemporal reality, founded on myth.

Christocentric worldview

Cosmovisão cristocêntrica

Duplicação

Duplication

First-person narrative focus

Foco narrativo em primeira pessoa

José Luís Peixoto

José Luís Peixoto

Mito

Myth