Mechanisms and modulation of experimental allergic encephalomyelitis as basis for treatment of multiple sclerosis /

Xu, Ling-Yun,

January 1900

Diss. (sammanfattning) Stockholm : Karol. inst. / Härtill 6 uppsatser.

Investigating the role of heat shock proteins (Hsps) 40, 70 and 90 in the life cycle of Theiler's murine encephalomyelitis virus (TMEV) / Investigating the role of heat shock proteins 40, 70 and 90 in the life cycle of a picornavirus, Theiler's murine encephalomyelitis virus

Mutsvunguma, Lorraine Zvichapera

January 2011

Introduction: Picornaviruses are a family of RNA viruses which are economically and clinically significant. Like many other viruses, picornaviruses utilise host cell machinery to facilitate their replication and assembly, including heat shock proteins (Hsps). The aim of this research was to investigate the role of Hsp40, Hsp70 and Hsp90 during picornavirus infection using the cardiovirus, Theiler’s murine encephalomyelitis virus (TMEV), as a study model. Methodology: Picornavirus VP1 capsid proteins were analysed by multiple sequence alignment and multiple structural comparisons. Protein domain architecture was used to analyse Hsp90 cellular and viral client proteins. Effects of Hsp90 inhibitors, novobiocin and geldanamycin, on TMEV growth in BHK-21 cells was observed over a 48hr period. Localisation of Hsp40, Hsp90 and Hsp70 in TMEV-infected BHK-21 cells was investigated by indirect immunofluorescence and confocal microscopy. Results and Discussion: VP1 proteins of picornaviruses are highly divergent within the family at the amino acid level, which might be linked to the protein’s function in determining virus tropism and antibody neutralisation. An eight-stranded anti-parallel beta-barrel structure was found conserved in the VP1 protein structures which might be linked to the highly conserved picornavirus capsid assembly process. Absence of a common protein domain between Hsp90 viral and cellular client proteins that might be functionally connected to Hsp90, suggests that Hsp90 most likely recognises surface features rather than sequence motifs/patterns. The Hsp90 inhibitors, novobiocin and geldanamycin, had a negative effect on virus growth as virus-induced cytopathic effect was not observed in treated cell after 48hrs. TMEV 2C protein was detected by Western analysis in infected cell lysates treated with geldanamycin but not novobiocin, suggesting novobiocin affects the translation or processing of TMEV 2C. Immunofluorescence analysis of TMEV-infected cells showed a relocalisation of Hsp40 into the nucleus during infection. Overlap of Hsp40 and TMEV P1 was observed in the perinuclear region, suggesting colocalisation between these proteins. Hsp70 converged around the replication complex during infection but did not overlap with TMEV 2C. Hsp90 concentrated in the region of the replication complex where it overlapped with TMEV 2C and this redistribution was found to be dependent on the stage of infection. The overlap between Hsp90 and TMEV 2C signals observed, suggested colocalisation between the two proteins. Conclusion: This study identified Hsp90, Hsp70 and Hsp40 as possible host factors required in TMEV replication.

Heat shock proteins

Picornaviruses

Encephalomyelitis

Generation of polyclonal antibodies against Theiler's Murine Encephalomyelitis virus protein 2C, and their use in investigating localisation of the protein in infected cells

Jauka, Tembisa Innocencia

January 2010

The Picornavirus family of positive sense RNA viruses includes some significant human and animal pathogens including Poliovirus (PV), Foot-and-Mouth disease virus (FMDV) and Human Rhinovirus (HRV). The genome is translated within the host cell into a polyprotein that is proteolytically cleaved into the structural and nonstructural proteins. The highly conserved, non-structural protein 2C has numerous roles during the virus life cycle and is essential for virus replication. Although the protein has been well studied in the case of PV, its interactions with the host cell during picornavirus infection is poorly understood. Theiler’s Encephalomyelitis virus (TMEV) is a picornavirus that infects mice, and is being used in our laboratory as a model in which to study the 2C protein. In this study, polyclonal antibodies against the TMEV 2C protein were generated and used to localise the protein in infected cells by indirect immunofluorescence. To produce antigen for immunisation purposes, the TMEV-2C protein sequence was analysed to identify hydrophilic and antigenic regions. An internal region of the 2C representing amino acid residues 31-210 was selected, expressed in bacteria and purified by nickel NTA affinity chromatography. Time course analysis of 2C (31-210) showed that the peptide was maximally expressed at 5 hours post induction. The peptide was solubilised using a mild detergent and 1.5 mg of purified antigen was used for immunisation of rabbits. Western blot analysis confirmed that the antibodies could detect both bacteriallyexpressed antigen, and virally-expressed 2C. Examination of virus-infected baby hamster kidney cells by immunofluorescence and confocal microscopy using the antiserum (anti-TMEV 2C antibodies) showed that the protein had a diffuse distribution upon early infection and at later stages it was located in a large perinuclear structure representing the viral replication complex. Furthermore, 2C localised to the Golgi apparatus as revealed by dual-label immunofluorescence using anti-TMEV 2C antibodies and wheat germ agglutinin (WGA). Furthermore, it was shown that TMEV infection results in changes in cell morphology and a redistribution of the cytoskeletal protein, β-actin. The successful production of antibodies that recognise TMEV 2C opens the way for further studies to investigate interactions between 2C and hostencoded factors.

Picornaviruses

RNA viruses

Immunoglobulins

Encephalomyelitis

Natural and experimental infections of eastern equine encephalomyelitis and other arborviruses in colonial bats (Chiroptera: Vespertilionidae) of New England.

Main, Andrew James

01 January 1970

No description available.

Bats Diseases

Encephalomyelitis

Rabies Research.

Studies of the pathogenesis of encephalomyelitis in gnotobiotic dogs induced by canine distemper virus /

Higgins, Robert James

January 1980

No description available.

Biology

Encephalomyelitis

Canine distemper virus

Gangliosides suppress the proliferation of autoreactive cells in experimental allergic encephalomyelitis : the effects of gangliosides on interleukin 2 activity /

Jackson, Kelly Michael

January 1986

No description available.

Health Sciences

Gangliosides

Encephalomyelitis

Interleukins

Studies on encephalitis

Cover, Morris Seifert.

January 1943

Call number: LD2668 .T4 1943 C6 / Master of Science

Communicable diseases in animals.

Equine encephalomyelitis.

Masters theses

Attempts to adapt avian encephalomyelitis virus to suckling mice with preliminary observations on serodiagnostic methods

Madden, David L.(David Larry),1932-

January 1958

Call number: LD2668 .T4 1958 M32

Avian encephalomyelitis.

Virology--Research.

Masters theses

Molekulare Mechanismen und zelluläre Kooperationen tolerogener Dendritischer Zellen bei der Experimentellen Autoimmun-Enzephalomyelitis / Molecular mechanism and cellular cooperations of tolerogenic dendritic cells in the experimental autoimmune enzephalomyelitis

Brandl, Carolin

January 2010

Aus Vorarbeiten in der Arbeitsgruppe war bekannt, dass Mäuse durch Injektion von tolerogenen, TNF-gereiften und MOG-beladenen DZ vor EAE geschützt werden können. Eines der Ziele dieser Arbeit war es zu untersuchen, ob das koinhibitorische Molekül B7-H1 auf der Oberfläche der DZ einen Einfluss auf das tolerogene Potential der DZ hat. Dazu wurden B7-H1-defiziente DZ generiert, mit TNF gereift, mit MOG-Peptid beladen und intravenös in Mäuse injiziert, bevor die EAE induziert wurde. Es zeigte sich, dass diese DZ die Tiere sogar noch besser vor der Krankheit schützen konnten als die WT DZ. Die Injektion der B7-H1-/- DZ bewirkte eine verstärkte Produktion von IL-10 and IL-13 nach Restimulation der Milz-Zellen in vitro und eine erhöhte Menge von protektiven Serum-Zytokinen (IL-4 und IL-13), welche von NKT-Zellen produziert wurden. Versuche mit CD1d-/- und Jα281-/- Mäusen haben ergeben, dass diese Zytokine von Typ II NKT-Zellen produziert wurden. Weitere Versuche mit Typ I und II NKT-Zell-Linien haben bestätigt, dass nur die Typ II NKT-Zellen von einem endogenen CD1d-Ligand der DZ stimuliert werden können. Außerdem wird dies über B7-H1 reguliert, da die NKT-Zell-Reaktion in Abwesenheit von B7-H1 stärker ist. Des Weiteren konnte gezeigt werden, dass neben den NKT-Zellen MZ B-Zellen nötig sind, um die Mäuse vor der EAE-Entwicklung zu schützen. Versuche mit CD22-/- Mäusen, welche eine Reduktion in der MZ B-Zell-Population zeigen, haben ergeben, dass in Abwesenheit von MZ B-Zellen keine EAE-Protektion mehr möglich ist. In dieser Arbeit wurde auch der Effekt von Glykolipid-Antigenen, welche einen Großteil der Myelinscheide des ZNS ausmachen, auf DZ untersucht. Ausgewählte Lipide führen zu einer Reifung der DZ, welche sich in der verstärkten MHC II- und CD86-Expression, jedoch nicht in der Produktion von Zytokinen äußert. Außerdem sind diese Lipid-gereiften DZ in der Lage T-Zellen zu stimulieren. Als letzter Punkt wurde in dieser Arbeit der Zusammenhang zwischen Masern-Virus-Infektionen und EAE untersucht. Es konnte gezeigt werden, dass eine cerebrale Masern-Infektion zusammen mit einer EAE-Induktion einen dramatischen Effekt auf die Tiere hat. Für diese Versuche wurde ein Maus-Modell einer persistierenden Masern-Infektion im Gehirn verwendet. Diese Tiere leben nach der Virus-Behandlung ohne Symptome. Nach der EAE-Induktion starben diese Tiere jedoch bereits wenige Tage später aufgrund einer MOG-Peptid-spezifischen Reaktion. / From previous studies in our group it was known that tolerogenic, TNF-matured and MOG-loaded DC could protect mice from developing EAE. One issue of this thesis was to investigate the effect of the co-inhibitory molecule B7-H1 on the tolerogenic potential of the DC. Therefore B7-H1-deficient DC were generated, matured with TNF, loaded with MOG peptide and injected intravenously before inducing EAE. It could be shown that the B7-H1-/- DC were even better in protecting mice from EAE. The injection of B7-H1-/- DC induced an increased production of IL-10 and IL-13 after restimulation of splenic cells in vitro and an increased amount of the protective serum-cytokines (IL-4 and IL-13) which were produced by NKT cells. Experiments with CD1d-/- and Jα281-/- mice showed that these cytokines were produced by Type II NKT cells. Futher experiments with Type I and II NKT cell lines confirmed that only Type II NKT cells could be stimulated by an endogenous CD1d-Ligand on the DC. Futhermore this mechanism is regulated by B7-H1 because the NKT cell reaction is stronger in the absence of B7-H1. This study also showed that besides the NKT cells the MZ B cells are necessary to protect mice from EAE. Experiments with CD22-/- mice which have a reduction in MZ B cells showed that EAE protection in the absence of MZ B cells is not possible. Another issue of this work was to study the effect of glycolipid antigens on DC. These lipids are a major part of the myelin sheath of the CNS. Some lipids induce DC maturation which is indicated by an increased MHC II and CD86 expression but not by cytokine production. Futhermore these lipid-matured DC are able to stimulate T cells. The last point of this study was to investigate the connection between measles virus infections and EAE. It could be shown that a cerebral measles infection together with EAE has an dramatic effect on the mice. For these experiments the mouse model of an persistant measles infection in the brain was used. These animals live without symptoms after treatment with the virus alone but after EAE induction these mice died rapidly because of an MOG specific reaction.

Encephalomyelitis

Dendritische Zelle

Immuntoleranz

Autoimmunität

ddc:570

An analysis of the relationship between coping strategies used and incidence of relapse in myalgic encephalomyelitis

Biccard, Anne-Marie

20 July 2016

Dissertation Submitted to the Faculty of Science, University of the Witwatersrand, Johannesburg, for the degree of Master of Science. Johannesburg 1993 / This dissertation studies the relationship between the use of certain coping strategies and the relapse of'illness, Eighty subjects with 1\'{yalgicEncephalomyelitis (M.E.) were followed OVera nine month period, initially completing a biographical questionnaire which showed some interesting common features, but these characteristics may be attributed to the narrow population from which the sample was drawn. The subjects then completed a battery of tests every eight weeks. These tests monitored appraisal of stressors, ways of coping and general health over the eight weeks since the previous test. Results were analysed using a Pearson's product moment correlation and a principal components factor analysis with a varimax rotation. The subjects were expected to show a positive correlat'on between certain coping techniques (such as denial, avoidance, and self- blame) and the relapse of M.B., while a zero or negative correlation between other coping techniques (such as seeking social support and problem solving when the stressor is controllable) and relapse. Neither of these hypotheses was supported by the data gathered. However, the subjects showed a remarkable consistency inthe types of'coping used, rather than adapting the mode of coping to the type of stressor experienced. It was concluded that the subjects used abnormal coping techniques and that these techniques Weresomehow related to their illness. However, the exact causal relationship between the coping techniques and the illness could not be assessed. It is possible that the subjects' poor coping mechanisms contributed to the development and exacerbation of the illness but it in also possible that the illness limited the repertoire of coping techniques available to the p"atient.

Stress (Psychology)

Stress (Physiology)

Myalgic encephalomyelitis.