Biskanewin Ishkode (The Fire that is Beginning to Stand): Exploring Indigenous Health and Healing Concepts and Practices for Addressing Sexual Traumas

Reeves, Allison

14 January 2014

Multiple traumas, including sexual vulnerabilities, sexual abuse, and sexualized violence, remain substantially higher among Indigenous peoples in Canada than among non-Indigenous peoples. These trends are rooted in a colonial history that includes systemic racism, a deprivation of lands and culture and other intergenerational traumas. Mental health sequelae following sexual vulnerabilities such as abuse and violence may include mood disorders, low self-worth, posttraumatic stress and a range of issues related to anxiety—yet Western mental health services are typically under-used by Indigenous peoples managing these issues. Indigenous mental health and healing services are explored as a more culturally appropriate and successful alternative for Indigenous clients experiencing multiple traumas.

Indigenous healing

Trauma

6021

Biskanewin Ishkode (The Fire that is Beginning to Stand): Exploring Indigenous Health and Healing Concepts and Practices for Addressing Sexual Traumas

Reeves, Allison

14 January 2014

Multiple traumas, including sexual vulnerabilities, sexual abuse, and sexualized violence, remain substantially higher among Indigenous peoples in Canada than among non-Indigenous peoples. These trends are rooted in a colonial history that includes systemic racism, a deprivation of lands and culture and other intergenerational traumas. Mental health sequelae following sexual vulnerabilities such as abuse and violence may include mood disorders, low self-worth, posttraumatic stress and a range of issues related to anxiety—yet Western mental health services are typically under-used by Indigenous peoples managing these issues. Indigenous mental health and healing services are explored as a more culturally appropriate and successful alternative for Indigenous clients experiencing multiple traumas.

Indigenous healing

Trauma

6021

Open Source, Distributed IS Development : A Study of the Development and Implementation of a Hospital Information System in India

Valland, Samson, Øygard, Per Øyvind

January 2011

Open-Source software has become increasingly more common in IT-organisations. Despite this the focus of studies on open-source has largely been focused on large system software. In our thesis we have worked on a software development project in Shimla, India, to create a hospital management system for the district hospitals in the state of Himachal Pradesh. Through our studies we have looked at the challenges of developing and implementing an open-source IS system in low-resource environment. Our results show that such an undertaking can be successful, but that distributed development poses a lot of challenges, and that the use of open-source software, while free, still necessitates a lot of work and close communication with the community.

ntnudaim:6021

MTDT datateknikk

Program- og informasjonssystemer

To Which of Thine Selves be True? Changes in Viscerosomatic Neural Activity with Mindfulness Meditation Training Reflect Improved Present-moment Self-awareness

Farb, Norman A. S.

26 July 2013

Mindfulness training cultivates momentary awareness, a form of attention directed to non-evaluative, immediate sensation. This form of attention stands in contrast to a more temporally extended awareness, which allows for the evaluative organization of experience into a personal narrative. The neural mechanisms underlying such awareness, and their role in regulating emotions, are poorly understood. Thus, in three functional magnetic resonance imaging (fMRI) experiments, I explored the thesis that momentary and extended awareness represent dissociable modes of self-reference, with momentary self-reference reducing ruminative elaboration of events by biasing attention towards interoceptive signals from the body. I compared individuals who were randomly-assigned to either an 8-week Mindfulness-Based Stress Reduction (MBSR) training course against a waitlisted group (Controls). Three distinct studies examined the impact of Mindfulness on: 1) the contrast between explicitly directed momentary and extended self referential processing; 2) reactions to an induced sadness challenge; and 3) the contrast between interoceptive (breath-monitoring) and exteroceptive (visual) attention. In all three studies MBSR led to a shift in neural activity away from cortical midline structures, such as the medial prefrontal and posterior cingulate cortices, to predominantly right-lateralized viscerosomatic structures, and specifically the insular cortex. Cortical midline activity is thought to support habitual patterns of evaluation, and stands as the neural correlate of a narrated, extended self, while right-lateralized insula activity is thought to represent the recurrent integration of present moment context, the neural correlate of the momentary self. These data revealed that MBSR may enhance the distinction between momentary and extended self-reference, reducing cortical midline responses and recruiting a novel, right-lateralized viscerosomatic network. Additionally, MBSR graduates demonstrated reduced emotional reactivity to a film-based sadness mood induction, reducing cortical midline activity and inhibition of the right insula. Moreover, the MBSR group demonstrated enhanced right middle insula recruitment during the monitoring of sensory experience associated with breath monitoring, a core mindfulness practice. The data from this final study also suggest that MBSR promoted an integration of posterior insular sensory representations with anterior insular subjective representations of present moment status. Preserved viscerosomatic activity in the face of emotional challenge may be a predictor of enhanced well-being following mindfulness training.

Cognitive Neuroscience

Mindfulness

Meditation

fMRI

Insula

Self-Reference

6021

0623

0349

0317

Beteiligung der Indolamin 2,3-Dioxygenase (IDO) an Immunregulation des zentralen Nervensystems

Kwidzinski, Erik

13 February 2006

In Europa stellt die Multiple Sklerose (MS) die häufigste neuroimmunologische Erkrankung des zentralen Nervensystems (ZNS) dar. Relevante Daten zum Krankheitsverlauf der MS wurden durch Untersuchungen im Tiermodell der experimentellen autoimmunen Enzephalomyelits (EAE) gewonnen. Nach gegenwärtigem Kenntnisstand wandern autoreaktive T-Zellen vom T-Helfer-1 (Th-1) Typ in das ZNS ein und lösen eine gegen Bestandteile der Markscheide gerichtete Entzündung aus. Diese Zellen exprimieren große Mengen des für sie typischen Zytokin Interferon-gamma (IFN-gamma), was in zahlreichen Zelltypen die Expression des Tryptophan degradierenden Enzyms Indolamin 2,3-Dioxygenase (IDO) induziert. Seit 1998 ist bekannt, dass die Inhibition der IDO zu einer durch T-Zellen vermittelten Abstoßung allogener Feten führt. Diese immunregulatorische Funktion von IDO konnte auf den schnellen Abbau der essentiellen Aminosäure Tryptophan und der im folgenden Abbauweg synthetisierten T-Zell-toxischen Metabolite zurückgeführt werden. Da im entzündeten ZNS-Gewebe während der MS und der EAE das IDO induzierende Zytokin IFN-gamma ebenfalls exprimiert wird, sollte in der vorliegenden Arbeit untersucht werden in wie weit die IDO an der Immunregulation des ZNS unter autoimmuner Neuroinflammation während EAE, beteiligt ist. Mittels HPLC konnte gezeigt werden, dass die relative IDO Aktivität im ZNS während der akuten und der Erholungsphase der Erkrankung signifikant gesteigert ist. Erfolgte ab dem Ausbruch der Erkrankung die systemische Inhibition der IDO Aktivität mit dem spezifischen IDO-Inhibitor 1-Methyl-Tryptophan, so führte dies zu einem signifikant schwereren Krankheitsverlauf im Vergleich zu Kontrolltieren. Mittels Immunzytochemie wurde gezeigt, dass aktivierte Mikroglia IDO im entzündeten ZNS und in Zellkultur nach IFN-gamma Stimulation exprimieren. Aufgrund von RT-PCR Analysen weiterer Enzyme des Kynureninweges konnte dessen Regulation während EAE nachgewiesen werden Entlang dieses Stoffwechselweges werden T-zell-toxische Tryptophanmetabolite gebildet die an der Eliminierung autoreaktiver T-Zellen im ZNS während der Erholungsphase der EAE beteiligt sein könnten und somit die aktivierten Th1 Zellen im ZNS einen antiinflammatorischen Rückkopplungsmechanismus auslösen. / Multiple sclerosis (MS) is the most widespread neuroimmunological disease of the central nervous system (CNS) in Europe. By applying the animal model of MS, experimental autoimmune encephalomyelitis (EAE), important insights into the disease course of MS have been gained. At present it is accepted that at the onset of the disease myelin-reactive T helper type 1 (Th1) cells infiltrate the CNS and induce autoimmune neuroinflammation. Activated Th1 cells express high amounts of the cytokine interferon-gamma (IFN-gamma). This pro-inflammatory signaling molecule is known to induce the expression of the tryptophan-degrading enzyme Indolmaine 2,3- Dioxygenase (IDO) in several cell types. Since 1998 it is known that inhibition of IDO induces the T cell-mediated rejection of allogeneic concepti in mice. The mechanism of this immunregulatory function of IDO was shown to be due to the degradation of the essential amino acid tryptophan and the subsequent synthesis of T cell toxic metabolites. Since the IDO-inducing cytokine IFN-gamma is also expressed within inflamed CNS tissue during MS and EAE, the present work investigated the role of IDO in immunregulation of the CNS during autoimmune neuroinflammation in the EAE model. A significant increase in relative IDO activity within the CNS during the acute and remission phases of EAE was identified by HPLC analysis. Systemic inhibition of IDO activity by the specific IDO inhibitor 1-methyl-tryptophan reduced the remission and exacerbated the progression of the disease in comparison to control animals. Activated microglia were identified by immunocytochemistry as IDO-expressing cells within the acute inflamed CNS and in cell culture after IFN-gamma stimulation. Enzymes following IDO in the kynurenine pathway were shown by RT-PCR to be up-regulated in the disease course. The analyzed enzymes are known to produce T cell toxic tryptophan metabolites and might therefore be involved in the elimination of autoreactive T cells from CNS tissue. In conclusion, the presented data support the view that autoreactive Th1 cells in the CNS induce a self-limiting negative feedback mechanism which limits the spread of inflammation, thereby reducing bystander damage in the CNS.

Autoimmunität

IDO

ZNS

EAE

Multiple Sklerose

autoimmunity

IDO

CNS

EAE

multiple sclerosis

610 Medizin

33 Medizin

XG 8804

YG 6004

YG 6021

YG 6093

ddc:610

Die Bedeutung löslicher TNF-Familienmitglieder für die multiple Sklerose

Ehrlich, Stefan

13 June 2006

Bei Autoimmunkrankheiten wie der Multiplen Sklerose (MS) kommt es zu einer fehlgesteuerten Immunantwort mit Aktivierung und Persistenz autoreaktiver T-Zellen. Apoptose-regulierende Mechanismen wie das CD95-Rezeptor/CD95-Ligand- und TRAIL-Rezeptor/TRAIL-System könnten dabei eine wichtige Rolle spielen. Die lösliche Form des CD95-Rezeptor (sCD95) kann an CD95L binden und so die Apoptose aktivierter T-Zellen verhindern. Die systemische Blockade von TRAIL führt zur Exazerbation von Autoimmunerkrankungen in Tierversuchen. In der vorliegenden Arbeit wurden deshalb die Expression, Regulation und Bedeutung sowohl von sCD95 als auch von löslichem TRAIL (sTRAIL) und membranständigem TRAIL bei gesunden Probanden und Patienten mit schubförmig remittierender MS (RRMS) untersucht. Zytokine wurden mit ELISAs, Zelloberflächenproteine sowie Apoptose im Durchflusszytometer gemessen. Die Untersuchungen mit magnetisch gereinigten humanen Leukozytensubpopulationen und Zelllinien zeigten, dass sCD95 lediglich von zelltyp-spezifisch aktivierten humanen T-Zellen, sezerniert wird. TRAIL wurde vor allem von Monozyten, die mit IFN-beta stimuliert waren, sezerniert und auf der Zelloberfläche exprimiert. Zellkulturüberstände, die sTRAIL enthielten, lösten Apoptose in suszeptiblen Tumorzellen aus. TRAIL führte zu einer signifikanten Inhibition der Proliferation und der Produktion von Th1- und Th2-spezifischen Zytokinen bei humanen (auto)antigenspezifischen T-Zellen. Weder für die sCD95- noch für die TRAIL-Expression wurden Unterschiede zwischen RRMS-Patienten und gesunden Probanden nachgewiesen. Die Ergebnisse dieser Arbeit zeigen ein komplexes Regulations- und Expressionsmuster von sCD95 und TRAIL, ohne jedoch Anhaltspunkte für Unterschiede zwischen MS-Patienten und Gesunden zu liefern. Es ergaben sich wichtige Hinweise darauf, dass der protektive immunomodulatorische Effekt einer systemischen IFN-beta-Therapie bei MS durch TRAIL vermittelt werden könnte. / Autoimmune disorders such as Multiple Sclerosis (MS) are characterized by an aberrant immune response with activation and persistence of autoreactive T-cells. Apoptosis-regulating mechanism such as the CD95-Rezeptor/CD95-Ligand- and the TRAIL-Rezeptor/TRAIL-System may play a major role in this process. The soluble CD95 receptor (sCD95) can bind to CD95L and subsequently inhibit apoptosis of activated T-cells. The systemic blockade of TRAIL leads to the exacerbation of autoimmune disease in animal experiments. In this work I investigated the expression, regulation and significance of sCD95, soluble TRAIL (sTRAIL) and membrane-bound TRAIL in patients with remitting-relapsing MS (RRMS), and in healthy controls. Cytokines were measured by ELISA, membrane bound proteins and apoptosis were measured by flow cytometry. The experiments with magnetically sorted human leucocyte subpopulations and cell lines showed, that only cell-type specific activated human T-cells secrete sCD95. Both forms of TRAIL were expressed by monocytes stimulated with IFN-beta. Cell supernatants containing sTRAIL induced apoptosis in susceptible tumour cells. Furthermore TRAIL inhibited proliferation of (auto)antigen-specific T cells and the production of Th-1 and Th-2 specific cytokines. There were no differences in the expression of sCD95 and TRAIL between RRMS patients and healthy controls. This work shows a complex regulation pattern of sCD95 and TRAIL without being able to detect differences between MS patients and healthy controls. However, results point out that TRAIL could be an important mediator of the immunomodulatory effects of systemic IFN-beta therapy in MS.

Multiple Sklerose

Apoptose

sCD95

IFN-beta

T-Zelle

B-Zelle

Monozyt

Multiple Sclerosis

Apoptosis

sCD95

IFN-beta

T-cell

B-cell

Monocyte

610 Medizin

33 Medizin

YG 6004

YG 6018

YG 6021

ddc:610