Role of the nuclear lamina for stem cell mediated homeostasis

Petrovsky, Roman

02 December 2015

No description available.

572

Ageing

Lamina

Stem cells

HGPS

Drosophila

Lamin Dm0

Kugelkern

Homeostasis

Biologie (PPN619462639)

A influência da emissão sonora nos constituintes da lâmina própria da prega ventricular / The influence of the sound emission on the lamina propria of the ventricular fold

Armani, Andre

18 December 2015

As pregas vocais (PV) são estruturas únicas, altamente especializadas na vibração para a produção sonora. Em grande parte, decorrente da estruturação em camadas da lâmina própria (LP). Essa estruturação não está presente ao nascimento, somente após anos de uso vibratório e fonatório da PV é que a LP está finalmente estruturada. As pregas ventriculares (PVT) não são, habitualmente, estruturas vibratórias na produção sonora, e possuem a LP menos organizada em estratos, sendo menos especializadas para a vibração. Até o presente momento, não se tem conhecimento do que ocorre com os constituintes da LP de PVTs de pessoas que as utilizam como fonte produtora de voz. No presente estudo, foram comparados os constituintes colágenos e as fibras elásticas da LP de PVTs de indivíduos que as utilizam como principal fonte vibratória na produção de voz com o grupo controle. Foram selecionados seis indivíduos que utilizavam pelo menos uma das PVTs como fonte de vibração para a produção sonora por ao menos seis anos. Delas, colheu-se pequeno fragmento (0,5 cm2), que após processamento histológico, as fibras colágenas foram coradas com Picrosirus Red e as fibras elásticas com Weigert resorcina-fucsina. Foram obtidas 54 imagens da camada mais superficial da LP de cada PVT para cada coloração. Após a aquisição das imagens, as fibras colágenas tipo I e tipo III, colágenas totais e fibras elásticas foram quantificadas utilizando-se o software Image-Pro Plus, e comparadas com as PVTs dos controles. A análise estatística foi realizada por meio do teste T de Student para amostras não pareadas. A porcentagem de colágeno total na camada mais superficial da LP de PVT utilizada como fonte vibratória para a produção de som foi significativamente maior em relação aos controles. O mesmo ocorreu com a quantidade de colágeno tipo I. Não houve diferenças na quantidade de colágeno tipo III e de fibras elásticas. Como conclusão, pode-se afirmar que a utilização da PVT como fonte vibratória produtora de som leva ao aumento da quantidade de fibras colágenas totais e do tipo I na camada mais superficial da sua LP / The vocal folds (VF) are unique structures, highly specialized in vibrating for sound production. This specialization is mainly due to a layered structure of the lamina propria (LP). This layered structure is not present at birth, and develops only after a several years of phonation. The LP of the mature vocal fold consists of three layers. The ventricular folds (VTF) are not originally vibrating structures for sound production, and in its LP the layers are poorly organized. It is not known what happens to the constituents of the LP in the VTF in subjects that use VTF vibration as a source of voice production. In the present study, the distribution and quantity of collagen and elastic fibers of the lamina propria from VTF of patients that use it as the main source of vibration for voice production were compared with the VTF from control subjects. Six individuals that used at least one of the VTF as source of vibration for sound production for minimum of six years were selected. A small fragment of VTF (0.5 cm2) used as vibration source of sound production was collected from each subject. The samples were processed for histological analysis. Collagen fibers were stained with Picrosirus Red and elastic fibers were stained with Weigert\'s Resorcin-Fuchsin. A total of 54 images were obtained from the superficial layer of the LP from each VTF for each stain. After image acquisition, collagen type I, III, total collagen and elastic fibers were quantified and compared with the VTF from the control group. Quantification was done using Image-Pro Plus software. Statistics were performed using an unpaired Student T test. The amount of total collagen in the most superficial layer of LP when the VTF was used as the source of vibration for the production of sound was significantly higher when compared to controls. The same result was seen for the amount of type I collagen in both groups. There was no difference in the quantity of type III collagen and elastic fibers between the two groups. Vibration of the VTF as a source of sound, for at least six years, leads to an increase in the amount of total collagen fibers and an increase in type I collagen, but does not increase the amount of type III collagen and elastic fibers in the most superficial layer of LP. These results may help elucidate the unique development of the lamina propria of the vocal fold

Colágeno

Collagen

Elastic fibres

Fibras elásticas

Lamina propria

Lâmina própria

Prega ventricular

Ventricular fold

Defining the role of the nuclear lamina LEM Domain protein Otefin in germline stem cells

Barton, Lacy Jo

01 August 2014

The contents of nuclei are highly organized. Nuclear organization is facilitated by a dense protein network, called the nuclear lamina, which underlies the nuclear envelope. The nuclear lamina is composed of filamentous lamins and more than eighty lamin-associated proteins (LAPs). Among the first LAPs identified are LEM Domain (LEM-D) proteins, named after LAP2, emerin and MAN1. LEM-D proteins have many shared and unique functions that include providing structural support to the nucleus, regulating signal transduction pathways and gene expression, facilitating proper progression through the cell cycle and maintaining chromatin attachments at the nuclear periphery. Despite requirements for these processes in all cell types, loss of globally expressed LEM-D proteins causes tissue-restricted defects. Identification of the primary function in tissues susceptible to LEM-D protein loss is a persistent challenge in the nuclear lamina field. Research described here uses Drosophila as a model to understand LEM-D protein function. Loss of the Drosophila emerin homologue Otefin (Ote) causes a complex phenotype in the ovary wherein both somatic and germline cells are compromised. Using tissue-restricted expression experiments, it was determined that Ote function is only required in germline stem cells (GSCs) to maintain all cells in the ovary. Developmental, molecular and genetic analyses revealed that the primary defect in ote mutant ovaries is an early block in germline differentiation, followed by GSC death. Genetic rescue experiments revealed that both of these GSC defects are due to the activation of the DNA Damage Response (DDR) proteins ATR and Chk2. Interestingly, activation of ATR and Chk2 occurs independent of detectable canonical DDR triggers, including DNA damage. Immunohistochemical analyses suggest that Ote might be regulating chromatin condensation and/or heterochromatin organization in GSCs. Through studies of Ote, a rescue method was discovered that involves culturing animals at elevated temperatures. This novel rescue strategy, termed hyperthermia, acts independent of ATR or Chk2 inhibition. Interestingly, elevated temperatures leads to chromatin decondensation in Drosophila, suggesting that hyperthermia may rescue oogenesis by alleviating chromatin defects observed in ote mutant germ cells. Together, results from experiments discussed herein dissect a complex ovary phenotype to reveal the critical requirement for a nuclear lamina LEM-D protein. Investigations into Ote function have revealed several aspects of GSC biology. The ATR/Chk2 checkpoint activated in the absence of Ote uncovered a previously unidentified cause of female GSC death. Further, findings that ATR and Chk2 are activated in the absence of canonical triggers suggest that GSCs possess a system to monitor defects or changes in the nucleus that do not involve DNA damage. Therefore, studies of Ote function and ote mutant phenotypes have uncovered valuable insights into LEM-D protein function and revealed the existence of novel conditions required for GSC maintenance.

DNA Damage Response

Drosophila

Germline Stem Cells

LEM Domain

nuclear lamina

Otefin

Biochemistry

Distribution and frequency of myeloid and t cell populations in the small intestine of newborn and weaned calves

Fries, Patrick Norbert

25 August 2011

The development of mucosal dendritic cells (DCs) in cattle is poorly understood and an analysis of myeloid cells in the bovine small intestine is required to increase our knowledge in this area. The phenotype, frequency and distribution of mucosal myeloid and lymphoid lamina propria leukocytes (LPL) and intraepithelial leukocytes (IEL) in the ileum and jejunum of newborn calves (3-5 weeks old) were analyzed using flow cytometry and immunohistochemistry (IHC). LPL and IEL were isolated through the use of chemical and enzymatic incubations. Costaining with a CD45-specific monoclonal antibody allowed us to exclude all non-leukocytic cells from our analysis of IEL and LPL. The morphology of CD45+CD11c+MHC Class II+ cells isolated from the lamina propria (LP) of ileum and jejunum showed myeloid characteristics, validating the use of CD11c and MHC Class II co-expression to identify myeloid cells. Regional differences in the frequency and number of leukocytes isolated from the IEL and LP compartments of the ileum and jejunum were analyzed in newborn calves. The CD11cHiCD14+ and CD335+ NK cell populations were significantly more abundant in the ileum than the jejunum. IHC was then used to identify the distribution of myeloid cells within the intestine. This analysis confirmed the presence of a variety of myeloid cell populations within the LP. Furthermore, CD11c+ cells were uniquely distributed within the jejunal, but not the ileal IEL compartment. In contrast, CD11b+ cells were present in the ileal, but absent from the jejunal, IEL compartment. A comparison of myeloid cell populations isolated from jejunum and blood dentified distinct mucosal DC populations, such as CD11c+CD13+ cells, which were present in he jejunum but absent from blood. The phenotype, frequency and distribution of IEL and LPL in the ileum and jejunum of weaned calves (6 months old) were then investigated. Significant regional differences were observed when comparing mucosal T cell populations with CD8+ and γδ T cells more abundant in the ileum and CD4+ T cells more abundant in the jejunum. Proportionally, there were no significant differences between the frequency and number of myeloid populations in the two regions. IHC was, once again, used to confirm these unique distributions of cells within each region. CD11b+ cells were present in the LP of both the ileum and jejunum, although a small number of CD11b+ cells were found in the ileal epithelium. CD4+ T cells were restricted to the LP, while CD8+ and γδ T cells were restricted to the IEL compartment. Significant age-related changes were observed when comparing mucosal leukocyte populations in the ileum and jejunum of newborn and 6 month old calves. In the ileum there was an age-related enrichment of CD8+ and γδ T cells, while in the jejunum there was enrichment in CD4+ and CD8+ T cells. In contrast, total myeloid (CD11c+MHC Class II+) cells number remained unchanged but there was a significant age-related enrichment of DC subpopulations (CD13, CD26, CD205). In conclusion, the ileum and jejunum of the newborn calf was populated by diverse myeloid subpopulations, some of which were distinct from myeloid subpopualtions identified in blood. Furthermore, the total number of CD11cHiMHC Class II+ myeloid cells isolated from a 10 cm segment of intestine did not change with age. If neonatal DCs are functionally equivalent to DCs present in weaned calves then the neonatal mucosal immune system appears to have an equivalent capacity to acquire and present antigens acquired from diet, commensal microflora, or pathogens. The one limitation to this conclusion may be the marked difference in the distribution of intraepithelial DC and macrophage distribution when comparing newborn and weaned calves.

lamina propria leukocytes

intraepithelial lymphocytes

dendritic cells

cellular immunology

bovine

small intestine

mucosal immunity

Distribution and frequency of myeloid and t cell populations in the small intestine of newborn and weaned calves

Fries, Patrick Norbert

25 August 2011

The development of mucosal dendritic cells (DCs) in cattle is poorly understood and an analysis of myeloid cells in the bovine small intestine is required to increase our knowledge in this area. The phenotype, frequency and distribution of mucosal myeloid and lymphoid lamina propria leukocytes (LPL) and intraepithelial leukocytes (IEL) in the ileum and jejunum of newborn calves (3-5 weeks old) were analyzed using flow cytometry and immunohistochemistry (IHC). LPL and IEL were isolated through the use of chemical and enzymatic incubations. Costaining with a CD45-specific monoclonal antibody allowed us to exclude all non-leukocytic cells from our analysis of IEL and LPL. The morphology of CD45+CD11c+MHC Class II+ cells isolated from the lamina propria (LP) of ileum and jejunum showed myeloid characteristics, validating the use of CD11c and MHC Class II co-expression to identify myeloid cells. Regional differences in the frequency and number of leukocytes isolated from the IEL and LP compartments of the ileum and jejunum were analyzed in newborn calves. The CD11cHiCD14+ and CD335+ NK cell populations were significantly more abundant in the ileum than the jejunum. IHC was then used to identify the distribution of myeloid cells within the intestine. This analysis confirmed the presence of a variety of myeloid cell populations within the LP. Furthermore, CD11c+ cells were uniquely distributed within the jejunal, but not the ileal IEL compartment. In contrast, CD11b+ cells were present in the ileal, but absent from the jejunal, IEL compartment. A comparison of myeloid cell populations isolated from jejunum and blood dentified distinct mucosal DC populations, such as CD11c+CD13+ cells, which were present in he jejunum but absent from blood. The phenotype, frequency and distribution of IEL and LPL in the ileum and jejunum of weaned calves (6 months old) were then investigated. Significant regional differences were observed when comparing mucosal T cell populations with CD8+ and γδ T cells more abundant in the ileum and CD4+ T cells more abundant in the jejunum. Proportionally, there were no significant differences between the frequency and number of myeloid populations in the two regions. IHC was, once again, used to confirm these unique distributions of cells within each region. CD11b+ cells were present in the LP of both the ileum and jejunum, although a small number of CD11b+ cells were found in the ileal epithelium. CD4+ T cells were restricted to the LP, while CD8+ and γδ T cells were restricted to the IEL compartment. Significant age-related changes were observed when comparing mucosal leukocyte populations in the ileum and jejunum of newborn and 6 month old calves. In the ileum there was an age-related enrichment of CD8+ and γδ T cells, while in the jejunum there was enrichment in CD4+ and CD8+ T cells. In contrast, total myeloid (CD11c+MHC Class II+) cells number remained unchanged but there was a significant age-related enrichment of DC subpopulations (CD13, CD26, CD205). In conclusion, the ileum and jejunum of the newborn calf was populated by diverse myeloid subpopulations, some of which were distinct from myeloid subpopualtions identified in blood. Furthermore, the total number of CD11cHiMHC Class II+ myeloid cells isolated from a 10 cm segment of intestine did not change with age. If neonatal DCs are functionally equivalent to DCs present in weaned calves then the neonatal mucosal immune system appears to have an equivalent capacity to acquire and present antigens acquired from diet, commensal microflora, or pathogens. The one limitation to this conclusion may be the marked difference in the distribution of intraepithelial DC and macrophage distribution when comparing newborn and weaned calves.

lamina propria leukocytes

intraepithelial lymphocytes

dendritic cells

cellular immunology

bovine

small intestine

mucosal immunity

Integrated reservoir study of the 8 reservoir of the Green Canyon 18 field

Aniekwena, Anthony Udegbunam

15 November 2004

The move into deeper waters in the Gulf of Mexico has produced new opportunities for petroleum production, but it also has produced new challenges as different reservoir problems are encountered. This integrated reservoir characterization effort has provided useful information about the behavior and characteristics of a typical unconsolidated, overpressured, fine-grained, turbidite reservoir, which constitutes the majority of the reservoirs present in the Outer Continental Shelf of the Gulf of Mexico. Reservoirs in the Green Canyon 18 (GC 18) field constitute part of a turbidite package with reservoir quality typically increasing with depth. Characterization of the relatively shallow 8 reservoir had hitherto been hindered by the difficulty in resolving its complex architecture and stratigraphy. Furthermore, the combination of its unconsolidated rock matrix and abnormal pore pressure has resulted in severe production-induced compaction. The reservoir's complex geology had previously obfuscated the delineation of its hydrocarbon accumulation and determination of its different resource volumes. Geological and architectural alterations caused by post-accumulation salt tectonic activities had previously undermined the determination of the reservoir's active drive mechanisms and their chronology. Seismic interpretation has provided the reservoir geometry and topography. The reservoir stratigraphy has been defined using log, core and seismic data. With well data as pilot points, the spatial distribution of the reservoir properties has been defined using geostatistics. The resulting geological model was used to construct a dynamic flow model that matched historical production and pressure data.. The reservoir's pressure and production behavior indicates a dominant compaction drive mechanism. The results of this work show that the reservoir performance is influenced not only by the available drive energy, but also by the spatial distribution of the different facies relative to well locations. The study has delineated the hydrocarbon bearing reservoir, quantified the different resource categories as STOIIP/GIIP = 19.8/26.2 mmstb/Bscf, ultimate recovery = 9.92/16.01 mmstb/Bscf, and reserves (as of 9/2001) = 1.74/5.99 mmstb/Bscf of oil and gas, respectively. There does not appear to be significant benefit to infill drilling or enhanced recovery operations.

Turbidite

Geopressured

Fine-grained

8 reservoir

GC-18

Green Canyon

Compensational stacking

lamina

thin-bedded

The use of polarized light for biomedical applications

Baba, Justin Shekwoga

15 November 2004

Polarized light has the ability to increase the specificity of the investigation of biomedical samples and is finding greater utilization in the fields of medical diagnostics, sensing, and measurement. In particular, this dissertation focuses on the application of polarized light to address a major obstacle in the development of an optical based polarimetric non-invasive glucose detector that has the potential to improve the quality of life and prolong the life expectancy of the millions of people afflicted with the disease diabetes mellitus. By achieving the mapping of the relative variations in rabbit corneal birefringence, it is hoped that the understanding of the results contained herein will facilitate the development of techniques to eliminate the effects of changing corneal birefringence on polarimetric glucose measurement through the aqueous humor of the eye. This dissertation also focuses on the application of polarized light to address a major downside of cardiovascular biomechanics research, which is the utilization of toxic chemicals to prepare samples for histological examination. To this end, a polarization microscopy image processing technique is applied to non-stained cardiovascular samples as a means to eliminate, for certain cardiac samples, the necessity for staining using toxic chemicals. The results from this work have the potential to encourage more investigators to join the field of cardiac biomechanics, which studies the remodeling processes responsible for cardiovascular diseases such as myocardial infarct (heart attacks) and congestive heart failure. Cardiovascular disease is epidemic, particularly amongst the population group older than 65 years, and the number of people affected by this disease is expected to increase appreciably as the baby boomer generation transitions into this older, high risk population group. A better understanding of the responsible mechanisms for cardiac tissue remodeling will facilitate the development of better prevention and treatment regimens by improving the early detection and diagnosis of this disease.

polarization microscopy

corneal birefringence

noninvasive glucose measurement

polarimetry

polarization imaging

myo-lamina sheet angle

cardiovascular measurements

Endometriale periglandulär akzentuierte mononukleäre Entzündungszellinfiltrate beim Pferd – Physiologischer Befund oder Initialstadium einer Endometrose?

Klose, Kristin

26 June 2015

Im Rahmen der Routinediagnostik von Endometriumbioptaten der Stute fielen regel-mäßig periglanduläre mononukleäre Entzündungszellinfiltrate (PAME) auf. Ziel der vorliegenden Studie war die histomorphologische und immunhistologische Charakterisierung der PAME im klinisch-gynäkologischen, jahreszeitlichen und endometrialen Kontext. Insbesondere sollte geklärt werden, ob das Phänomen der periglandulären Entzündungszellakkumulation Ausdruck eines physiologischen endometrialen Befundes, Frühstadium (Trigger) der Endometrose oder Begleitsymptom einer Endometritis ist. Zu diesem Zweck wurden alle im Jahr 2009 mittels einer Übersichtsfärbung (H.-E.-Färbung) im Institut für Veterinär-Pathologie der Universität Leipzig untersuchten Endometriumbioptate von Stuten (n = 754) hinsichtlich des Vorkommens einer PAME überprüft. Es konnten 133 Bioptate von 131 Stuten identifiziert werden, die ausführlich histopathologisch ausgewertet wurden. 72 Bioptate wurden zusätzlich anhand einer Methylgrün-Pyronin-Färbung (MGP) und immunhistologischer Verfahren beurteilt: Neben der Differenzierung der an der PAME beteiligten Zellpopulationen (CD3, CD79 A, MAC 387, MGP), wurde das Vorkommen der Intermediärfilamente Vimentin und Desmin sowie von α-GMA in den beteiligten Epithel- und Stromazellen untersucht. Die glanduläre Basallamina wurde anhand der Basallaminakomponente Laminin dargestellt und charakterisiert. PAME kamen in 18 % aller im Jahr 2009 untersuchten Bioptate vor, bevorzugt (96 %) in entzündlich und/oder fibrotisch alterierten Endometrien. Der Entzündungszellcharakter der begleitenden Endometritis stimmte in 29 % der Fälle nicht mit dem Entzündungszellbild der PAME (mononukleär) überein. Während im übrigen Endometrium häufig (95 %) eine gering- bis mittelgradige Endometrose nachweisbar war, wiesen die PAME-Drüsen mehrheitlich (71 %) keine periglanduläre Fibrose auf. Bei der Endometrose um Drüsen mit einer PAME handelt es sich überwiegend (67 %) um die destruierende und zu 50 % um die aktive/gemischte Form. In 48 % der PAME-Lokalisationen wurde eine Infiltration der periglandulären Entzündungszellen zwischen die Drüsenepithelzellen beobachtet. Die PAME bestanden hauptsächlich aus T-Lymphozyten (CD3-positiv). Daneben fanden sich, in geringerer und variierender Anzahl, Plasmazellen (MGP), B-Zellen (CD79A-positiv) und Makrophagen (MAC 387-positiv). Anhand der Expression der Basallaminakomponente Laminin wurden in allen untersuchten PAME-Lokalisationen Alterationen der Basallamina nachgewiesen. Die Läsionen der Basallamina waren bei mittel- und hochgradigen PAME graduell stärker ausgeprägt und standen häufig (43 %) mit einer intraepithelialen Infiltration der Entzündungszellen im Zusammenhang. Vimentin wurde vereinzelt (4 %) in intraläsionalen Drüsenepithelzellen nachgewiesen. Periläsionale Stromazellen exprimieren zu 60 % Vimentin, zu 17 % Desmin und zu 28 % α-GMA. Bei der PAME handelt es sich sehr wahrscheinlich nicht ausschließlich um ein „histopathologisches Symptom“ einer chronischen nicht-eitrigen Endometritis. Die Interpretation der PAME als physiologischer Bestandteil eines Schleimhaut-assoziierten lymphatischen Gewebes (MALT) im equinen Endometrium hingegen ist denkbar und bedarf in Folgeuntersuchungen der Klärung. Hinsichtlich der Strukturfilamente wurden in den involvierten Epithel- und Stromazellen immunhistologische Expressionsmuster nachgewiesen, die mit denen in frühen Stadien der equinen Endometrose vergleichbar sind. Darüber hinaus wiesen die periläsionalen Stromazellen Differenzierungsmerkmale von Myofibroblasten auf. PAME waren eng mit dem Vorliegen von Basallaminaalterationen verknüpft, die im Entstehungsprozess der equinen Endometrose eine zentrale Bedeutung besitzen. Es ist vorstellbar, dass es sich bei der PAME möglicherweise um einen auslösenden Faktor der Endometrose handelt. Außerdem ist eine intrinsische Aufrechterhaltung im Rahmen der zytokinvermittelten Interaktion (IL-4, IL-13, MCP-1), zwischen den periglandulären Entzündungszellen und den an einer Fibrose beteiligten Stromazellen, mit daraus resultierender progredienter Fibrose denkbar. Zukünftig sollte in weiteren Untersuchungen eine diesbezügliche Analyse der potentiellen Regelkreise erfolgen.

Endometrose

Endometritis

Basallamina

Immunhistologie

Entzündungszellen

Endometrium

endometrosis

endometritis

basal lamina

immunohistochemistry

inflammatory cells

endometrium

ddc:610

Distribution and frequency of myeloid and t cell populations in the small intestine of newborn and weaned calves

07 1900

The development of mucosal dendritic cells (DCs) in cattle is poorly understood and an analysis of myeloid cells in the bovine small intestine is required to increase our knowledge in this area. The phenotype, frequency and distribution of mucosal myeloid and lymphoid lamina propria leukocytes (LPL) and intraepithelial leukocytes (IEL) in the ileum and jejunum of newborn calves (3-5 weeks old) were analyzed using flow cytometry and immunohistochemistry (IHC). LPL and IEL were isolated through the use of chemical and enzymatic incubations. Costaining with a CD45-specific monoclonal antibody allowed us to exclude all non-leukocytic cells from our analysis of IEL and LPL. The morphology of CD45+CD11c+MHC Class II+ cells isolated from the lamina propria (LP) of ileum and jejunum showed myeloid characteristics, validating the use of CD11c and MHC Class II co-expression to identify myeloid cells. Regional differences in the frequency and number of leukocytes isolated from the IEL and LP compartments of the ileum and jejunum were analyzed in newborn calves. The CD11cHiCD14+ and CD335+ NK cell populations were significantly more abundant in the ileum than the jejunum. IHC was then used to identify the distribution of myeloid cells within the intestine. This analysis confirmed the presence of a variety of myeloid cell populations within the LP. Furthermore, CD11c+ cells were uniquely distributed within the jejunal, but not the ileal IEL compartment. In contrast, CD11b+ cells were present in the ileal, but absent from the jejunal, IEL compartment. A comparison of myeloid cell populations isolated from jejunum and blood dentified distinct mucosal DC populations, such as CD11c+CD13+ cells, which were present in he jejunum but absent from blood. The phenotype, frequency and distribution of IEL and LPL in the ileum and jejunum of weaned calves (6 months old) were then investigated. Significant regional differences were observed when comparing mucosal T cell populations with CD8+ and γδ T cells more abundant in the ileum and CD4+ T cells more abundant in the jejunum. Proportionally, there were no significant differences between the frequency and number of myeloid populations in the two regions. IHC was, once again, used to confirm these unique distributions of cells within each region. CD11b+ cells were present in the LP of both the ileum and jejunum, although a small number of CD11b+ cells were found in the ileal epithelium. CD4+ T cells were restricted to the LP, while CD8+ and γδ T cells were restricted to the IEL compartment. Significant age-related changes were observed when comparing mucosal leukocyte populations in the ileum and jejunum of newborn and 6 month old calves. In the ileum there was an age-related enrichment of CD8+ and γδ T cells, while in the jejunum there was enrichment in CD4+ and CD8+ T cells. In contrast, total myeloid (CD11c+MHC Class II+) cells number remained unchanged but there was a significant age-related enrichment of DC subpopulations (CD13, CD26, CD205). In conclusion, the ileum and jejunum of the newborn calf was populated by diverse myeloid subpopulations, some of which were distinct from myeloid subpopualtions identified in blood. Furthermore, the total number of CD11cHiMHC Class II+ myeloid cells isolated from a 10 cm segment of intestine did not change with age. If neonatal DCs are functionally equivalent to DCs present in weaned calves then the neonatal mucosal immune system appears to have an equivalent capacity to acquire and present antigens acquired from diet, commensal microflora, or pathogens. The one limitation to this conclusion may be the marked difference in the distribution of intraepithelial DC and macrophage distribution when comparing newborn and weaned calves.

lamina propria leukocytes

intraepithelial lymphocytes

dendritic cells

cellular immunology

bovine

small intestine

mucosal immunity

The role of lamin A and emerin in mediating genome organisation

Godwin, Lauren Sarah

January 2010

The nuclear matrix (NM) is proposed to be a permanent network of core filaments underlying thicker fibres, present regardless of transcriptional activity. It is found to be both RNA and protein rich; indeed, numerous important nuclear proteins are components of the structure. In addition to mediating the organisation of entire chromosomes, the NM has also been demonstrated to tether telomeres via their TTAGGG repeats. In order to examine telomeric interactions with the NM, a technique known as the DNA halo preparation has been employed. Regions of DNA that are tightly attached to the structure are found within a so-called residual nucleus, while those sequences forming lesser associations produce a halo of DNA. Coupled with various FISH methodologies, this technique allowed the anchorage of genomic regions by the NM, to be analysed. In normal fibroblasts, the majority of chromosomes and telomeres were extensively anchored to the NM. Such interactions did not vary significantly in proliferating and senescent nuclei. However, a decrease in NM-associated telomeres was detected in quiescence. Since lamin A is an integral component of the NM, it seemed pertinent to examine chromosome and telomere NM-anchorage in Hutchinson-Gilford Progeria Syndrome (HGPS) fibroblasts, which contain mutant forms of lamin A. Indeed, genome tethering by the NM was perturbed in HGPS. In immortalised HGPS fibroblasts, this disrupted anchorage appeared to be rescued; the implications of this finding will be discussed. This study also suggested that telomere-NM interactions are aberrant in X-linked Emery-Dreifuss Muscular Dystrophy (X-EDMD), which is caused by mutant forms of emerin, another NM-associated protein. The positioning of selected genes in control and X-EDMD cell lines was examined in un-extracted nuclei using 2D and 3D FISH. Subtle shifts in the organisation of these genes were detected in diseased cells; however, their expression levels remained unaltered. Furthermore, in order to examine the architectural integrity of the nuclear lamina in lamin A and emerin mutant cell lines, scanning electron microscopy (SEM) was employed. This work revealed that such structures were indeed compromised in disease. The findings presented in this thesis highlight the importance of lamin A and emerin in mediating the organisation of the genome and taken together, promote the hypothesis that dysfunctional NM dynamics may well contribute to disease pathology.

610