Analyse genetischer Stabilität in den Nachkommen bestrahlter Zellen mittels klassischer Chromosomenbänderung und verschiedener Hochdurchsatz-Techniken / Analysis of genetic stability in the clonal descendants of irradiated cells using conventional chromosome banding and various high-throughput methods

Flunkert, Julia

January 2018

Ionisierende Strahlung (IR) ist in der medizinischen Diagnostik und in der Tumortherapie von zentraler Bedeutung, kann aber Genominstabilität und Krebs auslösen. Strahleninduzierte Genominstabilität (RIGI) ist in den klonalen Nachkommen bestrahlter Zellen zu beobachten, die zugrundeliegenden Mechanismen sind jedoch noch unverstanden. Zur Erforschung von verzögerten Strahleneffekten wurden primäre embryonale Fibroblastenkulturen mit 2 Gray bestrahlt und für 20 Populationsverdopplungen klonal expandiert. Zellen, die keiner Strahlung ausgesetzt waren, dienten als Kontrolle für normale Alterungsprozesse. Die Klone wurden durch klassische Chromosomenbänderungstechniken analysiert und in Abhängigkeit der Stabilität ihres Genoms in Gruppen eingeteilt. Ein Klon wurde als stabil gewertet, wenn die analysierten Metaphasen keinerlei Auffälligkeiten zeigten, während instabile Klone ein Mosaik aus normalen und abnormalen Metaphasen waren. Die Zellen von zwei Spendern wurden untersucht, um interindividuelle Strahleneffekte zu beurteilen. Nach Bestrahlung hatten mehr als die Hälfte der Klone Metaphasen mit strukturellen Aberrationen und wurden dementsprechend als instabil eingestuft. Drei Klone zeigten zudem numerische Aberrationen, die ausschließlich das Y Chromosom betrafen. Fluoreszenz in situ Hybridisierungen verifizierten diese Beobachtung in weiteren Klonen und deuteten an, dass der Verlust des Y Chromosoms mit RIGI assoziiert ist. Molekulare Karyotypisierungen mit SNP Arrays ergaben, dass IR in den Klonen Veränderungen der Kopienzahl auslöst. Ein Unterschied zwischen chromosomal stabilen und instabilen Klonen konnte jedoch nicht detektiert werden. Chromosomale Regionen, in denen sich bekanntermaßen fragile Stellen befinden, zeigten eine Anhäufung von CNVs. Ein RIGI Effekt konnte für die fragile Stelle 3B, in der sich das Gen FHIT befindet, identifiziert werden. Exom Sequenzierungen von Klonen und der entsprechenden Massenkultur zeigten eine alterungsassoziierte Entstehung von Varianten. Der Effekt wurde durch die Einwirkung von Strahlung erhöht. Auf Ebene von einzelnen Nukleotiden konnten ebenfalls Anhäufungen von Schäden in bestimmten genomischen Bereichen detektiert werden, dieser Effekt ging ohne die typischen RIGI Endpunkte einher. Die Ergebnisse der vorliegenden Arbeit zeigen, dass strahlenbedingte Veränderungen auf verschiedenen Ebenen (Chromosomen, Genkopienzahl und einzelnen Nukleotiden) beobachtet werden können, welche, unabhängig von RIGI, die Tumorentstehung begünstigen. Speziell Veränderungen im FRA3B Lokus und der Verlust des Y Chromosoms scheinen jedoch über die Destabilisierung des Genoms zur Krebsentstehung beizutragen. / Ionizing radiation is important in medical diagnosis and cancer treatment but can lead to genomic instability and secondary malignancies as a late effect. Radiation induced genomic instability (RIGI) can be observed in the progeny of irradiated cells but the underlying cellular processes remain to be elucidated. To study delayed genetic radiation effects, single cell fibroblast clones from two different male donors were established after a single X ray dose of 2 Gray. Non irradiated cells were used as controls to account for aging related effects. Clones were characterized using chromosome banding analysis. Stable clones were endowed with no karyotype abnormalities in all analysed metaphases after 20 Population doublings, whereas unstable clones showed both normal and abnormal metaphases. Two fibroblast strains were used to detect differences in radiation sensitivity. More than half of the irradiated clones were chromosomally abnormal and thus classified as unstable. Both banding analysis and fluorescence in situ hybridization revealed an increased rate of Y chromosome loss in irradiated clones which might be associated with RIGI. Using SNP Arrays, an increased rate of de novo copy number variations (CNVs) was detected in the progeny of irradiated cells when compared to non irradiated controls. However, a significant difference between chromosomally stable and unstable clones was not found. CNVs clustered in chromosomal regions that are associated with known fragile sites. The fragile site 3B, which encompasses the gene FHIT, was found to be affected by CNVs in unstable clones suggesting a RIGI related effect. Exome sequencing of clones and the respective primary cultures revealed an increased rate of variants during in vitro aging. This effect was further increased by radiation exposure. Analysis of single nucleotides showed a RIGI independent accumulation of damage in specific regions. The results of the present study show that radiation induced changes can manifest as chromosomal abnormalities, copy number variations and DNA sequence mutations promoting tumorigenesis independent from RIGI. However, changes in FRA3B and loss of Y chromosome might trigger cancer through destabilizing the genome.

Ionisierende Strahlung

High throughput screening

Instabilität

Genom

ddc:576

Re-annotation of Camponotus floridanus Genome and Characterization of Innate Immunity Transcriptome Responses to Bacterial Infections / Re-Annotation des Camponotus floridanus Genoms und Charakterisieren der unspezifischen Immun-Transkriptom-Antwort auf bakterielle Infektionen

Gupta, Shishir Kumar

January 2018

The sequencing of several ant genomes within the last six years open new research avenues for understanding not only the genetic basis of social species but also the complex systems such as immune responses in general. Similar to other social insects, ants live in cooperative colonies, often in high densities and with genetically identical or closely related individuals. The contact behaviours and crowd living conditions allow the disease to spread rapidly through colonies. Nevertheless, ants can efficiently combat infections by using diverse and effective immune mechanisms. However, the components of the immune system of carpenter ant Camponotus floridanus and also the factors in bacteria that facilitate infection are not well understood. To form a better view of the immune repository and study the C. floridanus immune responses against the bacteria, experimental data from Illumina sequencing and mass-spectrometry (MS) data of haemolymph in normal and infectious conditions were analysed and integrated with the several bioinformatics approaches. Briefly, the tasks were accomplished in three levels. First, the C. floridanus genome was re-annotated for the improvement of the existing annotation using the computational methods and transcriptomics data. Using the homology based methods, the extensive survey of literature, and mRNA expression profiles, the immune repository of C. floridanus were established. Second, large-scale protein-protein interactions (PPIs) and signalling network of C. floridanus were reconstructed and analysed and further the infection induced functional modules in the networks were detected by mapping of the expression data over the networks. In addition, the interactions of the immune components with the bacteria were identified by reconstructing inter-species PPIs networks and the interactions were validated by literature. Third, the stage-specific MS data of larvae and worker ants were analysed and the differences in the immune response were reported. Concisely, all the three omics levels resulted to multiple findings, for instance, re-annotation and transcriptome profiling resulted in the overall improvement of structural and functional annotation and detection of alternative splicing events, network analysis revealed the differentially expressed topologically important proteins and the active functional modules, MS data analysis revealed the stage specific differences in C. floridanus immune responses against bacterial pathogens. Taken together, starting from re-annotation of C. floridanus genome, this thesis provides a transcriptome and proteome level characterization of ant C. floridanus, particularly focusing on the immune system responses to pathogenic bacteria from a biological and a bioinformatics point of view. This work can serve as a model for the integration of omics data focusing on the immuno-transcriptome of insects. / Das Sequenzieren mehrerer Ameisen Genome innerhalb der letzten 6 Jahre eröffnete neue Forschungswege, um nicht nur die genetische Grundlade sozialer Arten, sondern auch komplexere Systeme wie generelle Immunantworten zu untersuchen. Ähnlich zu anderen sozialen Insekten leben Ameisen in Kolonien, oft mit einer sehr hohen Dichte mit genetisch übereinstimmenden oder nah verwandten Individuen. Das Sozialverhalten und die engen Lebensumstände führen dazu, dass sich Krankheiten in Kolonien schnell ausbreiten können. Dennoch können Ameisen mit der Nutzung ihrer komplexen Immunsystemmechanismen Infektionen effektiv abwehren. Die Zusammensetzung des Immunsystems der Rossameise Camponotus floridanus (C. floridanus) und die Faktoren der Bakterien, welche die Infektionen verursachen sind noch nicht gut untersucht. Um einen besseren Überblick über die verschiedenen Gruppen der Immun- Gene zu bekommen und um die Immunantworten von C. floridanus gegen Bakterien zu untersuchen haben wir experimentelle Daten der Illumina Sequenzierung und der Massenspektrometrie (MS) aus der Hämolymphe unter normalen und unter infizierten Bedingungen analysiert und über verschiedene bioinformatische Ansätzen zusammengefasst. Die Aufgabe wurde in drei Ebenen unterteilt. Zuerst wurde das Genom von C. floridanus neu annotiert, die Verbesserung der existierenden Annotation wurde rechnerisch und mit Transkriptom- Daten erreicht. Mit der Nutzung der auf Homologie- basierenden Methoden, der umfassenden Überprüfung der Literatur und der Nutzung von mRNA Genexpressionsanalysen wurde für C. floridanus dieser Überblick erstellt. Anschließend wurden größere Protein- Protein- Interaktionen (PPI) und Signalnetzwerke von C. floridanus rekonstruiert und analysiert und daraufhin wurden die Infektions-induzierten funktionalen Module im Netzwerk entdeckt und die Expressionsdaten über Netzwerke abgebildet. Zusätzlich wurden die Anteile der Immunantwort bei der Interaktion mit Bakterien mittels der Rekonstruktion von zwischenartlichen PPI Netzwerken identifiziert und diese Interaktionen wurden mit Literaturwerten validiert. In der dritten und letzten Phase wurden Daten der Stadium- spezifischen Massenspektrometrie (MS) von Larven- und Arbeiterameisen analysiert und die Unterschiede in den Immunantworten aufgezeichnet. Zusammengefasst lieferten alle drei Omiks- Ebenen jeweils viele Ergebnisse, zum Beispiel führte die neue Annotation und das Transkription- Profil zu einer generellen Verbesserung der strukturellen und funktionalen Annotation und dem Aufspüren von alternativen Splicing- Ereignissen. Die Netzwerkanalyse deckte die unterschiedlich exprimierten topologisch wichtigen Proteine und die aktiven funktionalen Module auf, die Analyse der MS- Daten erbrachte Ergebnisse über die Stadium- spezifischen Unterschiede in der Immunantwort von C. floridanus gegen bakterielle Pathogene. Rundum, beginnend mit der neuen Annotation des Genoms von C. floridanus stellt diese Arbeit eine Transkriptom- und Protein Charakterisierung der Ameise C. floridanus dar. Besonders lag der Fokus auf die Antworten des Immunsystems auf Pathogene Bakterien aus biologischer- und bioinformatischer Sicht. Diese Arbeit kann als Vorlage für die Integration von Omiks Daten dienen, welche sich auf die Immun- Transkriptome von Insekten fokussieren.

Camponotus floridanus

Genom

Transkription <Genetik>

Immunreaktion

ddc:570

An Investigation of Migraine Candidate Genes and Genomic Susceptibility Regions

Lea, Rod A., n/a

January 2003

Typical migraine, comprised of migraine with aura (MA) and migraine without aura (MO), is a chronic, painful and debilitating neurovascular disease which is generally characterised by recurrent attacks of severe headache usually accompanied by nausea, vomiting, photo and phonophobia. Migraine has been shown to affect a large proportion of Caucasian populations with a recent comprehensive study indicating that around 25% of women and 8% of men suffer from the disease. Strong familial aggregation of typical migraine and an increased concordance for the disease in MZ twins over DZ twins, suggests that it has a significant genetic component. Heritability estimates are calculated to be between 40% and 60%, indicating that disease variation, in part, is explained by environmental determinants. The mode of transmission of typical migraine is not clear but is most likely multifactorial. Although the MA and MO subtypes exhibit some clinical heterogeneity, segregation analysis has suggested that there may be a common genetic aetiology for MA and MO, and a major gene contributing to typical migraine pathogenesis. This idea is substantiated by the fact that both subtypes of migraine can occur within the same family and even within the same individual, with up to 33% of sufferers experiencing both types of the disease. In addition, migraine prophylactics have been shown to result in similar effects in patients treated for both types of migraine. However, whether the two subtypes are truly separate entities or not remains unclear. At present, the type and number of genes involved in typical migraine is not known. Despite this, several studies into Familial Hemiplegic Migraine (FHM), a very severe subtype of MA, have led to the discovery that mutations in a brain specific calcium channel subunit gene (CACNA1A) located on chromosome 19, cause FHM in about 50% of affected families. FHM is a rare disease and is distinguished from typical migraine by its association with hemiparesis and clear autosomal dominant mode of inheritance. However, certain clinical features are common to both FHM and typical migraine including similarities in headache characteristics and triggers. Hence, FHM genetic studies provide a valuable model for investigating the genes involved in the more prevalent types of migraine with and without aura. For this reason the Genomics Research Centre has been conducting linkage studies utilising large Australian migraine pedigrees with a focus on the known FHM (CACNA1A) gene region on chromosome 19p13. Our results to date have indicated suggestive linkage to the FHM region on 19p13 in a large multigenerational pedigree (MF1) affected with typical migraine, with a maximum parametric LOD score of 1.92 (P = 0.001) obtained for a triplet repeat polymorphism situated in exon 47 of the CACNA1A gene. Expansion of this repeat was not observed, but is possible that mutations elsewhere in the CACNA1A gene may be responsible for migraine in this pedigree. To investigate this possibility, the current research involved sequencing two patients carrying the critical susceptibility haplotype surrounding the CACNA1A gene. The results of this mutation screen revealed no disease causing mutations or polymorphisms in any of the 47 exons screened. To determine whether the CACNA1A genomic region was implicated in typical migraine susceptibility in the general Caucasian population, 82 independent pedigrees and a large case-control group were also analysed using highly polymorphic microsatellite markers. There was no linkage or association detected in these groups and thus, it was concluded that if CACNA1A plays a role in typical migraine it does not confer a major effect on the disease. However, subsequent case-control studies of SNPs in the INSR gene, which is located ~15cM telomeric from CACNA1A, provided evidence of association to typical migraine. Thus, the INSR gene may now emerge as the new migraine susceptibility gene in this genomic region on chromosome 19. Family linkage studies conducted by Gardner et al have implicated an additional FHM susceptibility region on chromsome 1q31. Furthermore, independent research carried out by Ducros et al. has indicated a second FHM locus at 1q21-23, which is ~ 30cM centromeric to the region reported by Gardner et al. At this stage it is not clear whether there is a single locus, or two distinct loci, on the chromosome 1q region. This research also involved a family-based linkage and association approach to investigating the FHM susceptibility region on chromosome 1q31 for involvement in typical migraine susceptibility in affected Australian pedigrees. Initial multipoint ALLEGRO analysis provided strong evidence for linkage of Chr1q31 markers to typical migraine in a large multigenerational pedigree. The 1-LOD* unit support interval for suggestive linkage spanned ~18cM with a maximum allele sharing LOD* score of 3.36 obtained for marker D1S2782, P = 0.00004. Subsequent analysis of an independent sample of 82 affected pedigrees added support to the initial findings with a maximum LOD* of 1.24 (P = 0.008). Utilising the independent sample of 82 pedigrees we also performed a family-based association test. Results of this analysis indicated distortion of allele transmission at marker D1S249 (global c2(5) of 15.00, P = 0.010) in these pedigrees. These positive linkage and association results will need further confirmation by independent researchers, but overall they provide good evidence for the existence of a typical migraine locus near these markers on Chr1q31, and reinforce the idea that an FHM gene in this genomic region may also contribute to susceptibility to the more common forms of migraine. The serotonergic system has long been implicated in the pathophysiology of migraine. Researchers have therefore focused on the serotonin receptors and the genes that code for them when investigating this disease. Although serotonin receptor agonists have proven to be effective in the treatment of migraine, there has been little evidence of a serotonin receptor gene being associated with the disorder. However, in 1998, Ogilvie et al reported that a VNTR in the serotonin transporter gene (SERT) showed altered allelic distributions in a Danish migraine population. In addition to serotonin, there has been renewed interest in the involvement of the dopaminergic pathways in migraine. This interest has gained impetus since the study of Peroutka et al who reported an allelic association between the dopamine receptor gene DRD2 and migraine with aura. Another dopamine related gene, the dopamine beta-hydroxylase gene (DBH), has been localised to Chr 9q34 and codes for the enzyme that catalyses the conversion of dopamine to norepinephrine. It therefore plays an important role in dopaminergic and noradrenergic neurotransmission. Serum levels of DbH enzyme have been reported to be elevated in migrainous patients during the headache phase of an attack. Also, significantly increased DbH enzyme activity has been observed in migraine patients during the headache-free interval. Thus, the DBH gene is another good candidate for involvement in migraine pathophysiology and, to our knowledge, has not been previously implicated in this disease. Candidate gene studies may be useful strategies for identifying genes involved in complex diseases such as migraine, especially if the gene being examined contributes only a minor effect to the overall phenotype. This research also involved a linkage and association approach to investigating neurotransmitter related migraine candidate genes. Specifically, polymorphisms within the serotonin transporter gene (SERT), the dopamine receptor gene (DRD2) and the dopamine beta-hydroxylase (DBH) gene were tested in unrelated Caucasian migraineurs and non-migraine control individuals. In addition, an independent sample of 82 families affected with migraine were examined. Unrelated case-control association analysis of a DBH intragenic dinucleotide polymorphism indicated altered allelic distribution between migraine and control groups (c2 = 16.53, P = 0.019). Furthermore, the transmission/disequilibrium test (TDT) which was implemented on the family data also indicated distortion of allele transmission for the same DBH marker (c2 = 4.44, P = 0.035). Together, these results provide evidence for allelic association of the DBH gene with typical migraine susceptibility (Fisher's Combined P-value = 0.006) and indicate that further research into the role of the DBH gene in migraine aetiology is warranted. Nitric oxide (NO) is emerging as a key molecule affecting the pain associated with migraine. Since nitric oxide synthase (NOS) enzymes catalyse the synthesis of NO, the genes that code for these enzymes are good candidates for migraine molecular genetic analysis. This research involved investigating the role of a functionally relevant bi-allelic tetranucleotide polymorphism located in the promoter region of the human inducible nitric oxide synthase (iNOS) gene in migraine aetiology. A large group of migraine affected individuals were genotyped and compared to an age and sex matched group of unaffected controls. Results of a chi-squared analysis indicated that allele distributions for both migraine cases and controls were not significantly different (c2 = 1.93, P = 0.16). These findings offer no evidence for an allelic association of the tested iNOS polymorphism with the common forms of the disease and therefore do not support a role for this gene in migraine pathogenesis. In summary, this research involved linkage and association analysis of migraine candidate genes and genomic susceptibility regions. Whilst, the known FHM gene (CACNA1A) was excluded for significant involvement in typical migraine the adjacent INSR gene has been associated. Migraine is genetically heterogeneous and the results of this research also provide good evidence that the DBH gene is involved in disease predisposition, whilst the DRD2, SERT and INOS gene were not shown to be implicated. An additional susceptibility region for typical migraine is also likely to localise to chromosome 1q31. Overall, the results presented in this thesis have contributed valuable data to the understanding of the molecular genetics of migraine with and without aura. Future research into the molecular pathophysiological mechanisms of migraine will greatly facilitate the development of more effective diagnosis and treatment strategies.

migraine

migraines

headache

headaches

genes

genetics

genom

ic susceptibility regions

-L,L,L,I,I - Står det liten här? : En studie om skriftspråksutveckling i förskolan. / -L,L,L,I,I - Does this mean little? : A study of written language development in pre-school

Jonsson, Alexandra, Sjölund, Anna-Karin

January 2012

Syftet med denna studie var att studera hur barn i tillrättalagda miljöer i förskolan utvecklar intresse för och stimuleras till skriftspråksinlärning. Våra frågeställningar har varit hur ser sampelet ut mellan pedagoger-barn och barn-barn i skriftspråkliga aktiviteter? Hur används förskolans miljö för att stimulera skriftspråksutveckling? Vilka redskap använder pedagogerna vid skriftspråksutveckling? Hur kan förskolan bidra till barns tidiga skriftspråksutveckling enligt pedagogerna? För att få en välgrundad uppfattning om ämnet har vi genomfört fyra observationer på två olika förskolor. De observerade barnen var fyra och fem år. Vi har även intervjuat fyra pedagoger som alla arbetade på de observerade avdelningarna. I studien användes en kvalitativ ansats. Studiens resultat har analyserats ur ett sociokulturellt perspektiv. Resultatet visade att barnen samspelade mer med varandra än med pedagogerna. Det visade även att förskolornas skriftspråksmiljö innefattade bokstavspussel, namnlappar och ABC-planscher. Varför används ABC-planscher när resultatet visade att ingen använde dem, de bara fanns där? De redskap som pedagogerna använde var memorykort med barnens namn, bokstäver i olika former och material samt kroppen för att träna ordrytm. För att stimulera skriftspråksutvecklingen tyckte de intervjuade pedagogerna att det var viktigt att ljuda fram bokstäver. Denna upptäckt var förvånande då ljudning är något vi kopplat ihop med förskoleklassens skriftspråksinlärning. Vissa barn har inte så bra finmotorik och för att ta hänsyn till att alla barn är olika användes magnetbokstäver för att underlätta skrivandet. Barnen fick skriva själva på papper och whiteboardtavla för att stimulera skriftspråket. Ett intressant resultat var att samtliga intervjuade talade om att skrivinlärning skedde i de planerade aktiviteterna som t ex samling och skapande vilket motsäger det läroplanen talar om nämligen att lära genom lek.

Förskolan

skriftspråksutveckling

samspel

miljö

lära genom lek

ljusning

Sång i förskola : Spontansångens påverkan på barnens språkutveckling

Johansson, Lyudmila

January 2011

No description available.

Spontansång

språkutveckling genom sång

förskolan

pedagoger

Aesthetic subjects

Estetiska ämnen

Låt oss se en film! : En undersökning om produktplacering inom svensk filmindustri

Kolari, Sandra

January 2014

När konsumenten får tillgång till ny teknologi möjliggörs nya sätt att se på tv och film, detta nya sätt att bestämma över reklamintag har ändrat sättet som konsumenten utsätts för reklam. När konsumtionsmarknaden ändras måste teknologin och marknadsföringstekniker följa efter. Produktplacering är ett sätt att integrera marknadsföring i kontext med kända aktörer och få konsumentens medvetenhet för produkter att öka. Produktplacering är inte ett nytt sätt att marknadsföra produkter men har blivit mer centralt då marknadens intolerans för reklam ökar. Undersökningen grundar sig på att beskriva hur filmindustrin använder sig av produktplacering inom svenskproducerade filmer. Genom att deskriptivt förklara vad produktplacering är och hur produkterna placeras genom produkttyp, tid, position i bild, aktörer och hur det genererar positiva och negativa effekter kan undersökningen skapa en bild över hur produktplaceringen i filmer används i Sverige. Produktplacering undersöks genom observation av två svenskproducerade filmer, Hundraåringen som klev ut genom fönstret och försvann samt Skumtimmen. Filmerna fungerar som en generalisering av den svenska filmindustrin genom att beskriva hur den såg ut år 2013. Företag kan gynnas av kunskapen inom produktplacering och använda teknikerna rätt för att generera avkastning, användningen av felaktiga tekniker kan i stället leda till förluster. I den svenska filmindustrin används vanligtvis produktplaceringstekniker genom att placera produkter medvetet genom visuell synlighet, i mitten av bilden och genom att integrerera produkterna med handlingen. Produkter som gör sig synliga i svenska produktioner varierar från stora produktioner till små, stora produkter har oftast en större variation av produkter än små produktioner men delar samma stora användning av produktplacering av livsmedel och dagligvaror. Mycket av de olikheter som stora och små produktioner har grundar sig på den tillgänglighet som filmen kommer nå ut i men även vilken form av genre filmen har. Det måste finnas en balans mellan filmindustrin och företagen för att största möjliga vinst skall kunna uppnås. Med denna undersökning hoppas jag som skribent kunna möjliggöra ett enklare sätt att undersöka produktplacering för att se att det används på det mest effektiva sättet.

Produktplacering

Filmindustrin

Sverige

Bioinformatic analysis of mutation and selection in the vertebrate non-coding genome /

Brandström, Mikael,

January 2007

Diss. (sammanfattning) Uppsala : Univ., 2007. / Härtill 5 uppsatser.

Approaching the three-dimensional organization of the human genome

Knoch, Tobias A.

January 2003

Heidelberg, Univ., Diss., 2002.

Vergleichende Sequenzanalyse der fünf Grundplastome der Sektion Oenothera (Gattung Oenothera) Analyse des Cytochrom-Komplexes /

Hupfer, Holger.

Unknown Date

Universiẗat, Diss., 2003--München.

Retrospektivism och biologi : Om begreppens natur genom evolutionens ögon / Retrospectivism and biology : On the nature of concepts through the eyes ofevolution

Forsberg, Erik

January 2018

Begreppsatomismen lär oss att den metafysiska strukturen hos lexikala begrepp beror påbegreppens relation till yttervärlden men är oklar i hur denna relation förverkligas. Avsiktenmed denna uppsats är därför att utveckla en metafysisk tes för uppkomsten av begreppsligstruktur som också närmare visar hur lexikala begrepp förhåller sig till världen. Utredningenbestår i att jämföra två filosofiska positioner som står nära begreppsatomismen: å ena sidanPutnams externalism för naturliga typer och å andra sidan biosemantiken, här representeradav Dennett och Millikan. Genom att utgå ifrån Putnams tankeexperiment tvillingjord ochhans syn på strukturen hos lexikala begrepp nås slutsatsen att biosemantiken når längre av detvå. Men en närmare granskning visar att biosemantik i förening med principen om evolutiongenom naturligt urval ger att strukturen hos lexikala begrepp står i ett metafysiskt beroendetill framtiden och förverkligas retrospektivt, varvid retrospektiv begreppsatomism föreslås.

Lexikala begrepp

biologi

evolution genom naturligt urval

Philosophy

Filosofi