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  • About
  • The Global ETD Search service is a free service for researchers to find electronic theses and dissertations. This service is provided by the Networked Digital Library of Theses and Dissertations.
    Our metadata is collected from universities around the world. If you manage a university/consortium/country archive and want to be added, details can be found on the NDLTD website.
31

Kvantitativt sensoriskt test - tröskelvärden vid olika hudtemperaturer

Ranta, Isabella January 2018 (has links)
No description available.
32

Metodutvärdering och mervärde av Treponema pallidum IgM analys vid diagnostik av syfilis

Aronsson, Ulrika January 2018 (has links)
No description available.
33

Extremitetelektrodernas inverkan på QRS-amplituden och den elektriska axeln i ett elektrokardiogram

Dobos, Rebecca January 2018 (has links)
No description available.
34

Insamling av referensvärden för Visual evoked potentials (VEP) hos friska individer vid Centralsjukhuset i Karlstad

Pinsanor, Preeyanun January 2018 (has links)
No description available.
35

Parathyreoideascintigrafi och parathyreoideaektomi: En jämförelse av resultat vid Centralsjukhuset i Karlstad

Evehäll, Martin January 2018 (has links)
No description available.
36

Temperaturens inverkan på sensoriska delen av nervus medianus förmåga att leda elektriska signaler

Palmbrandt, Linda January 2018 (has links)
No description available.
37

Detektion av cashewnötsprotein i livsmedel

Fan, Ying January 2018 (has links)
No description available.
38

Screening Swedish bees for pahogens shines new light on the parasite Gregarine

Svedin, Nellie January 2017 (has links)
are under pressure from habitat loss, environmental stress and pathogens including viruses. Research have shown viral infections to be one of the major causes of colony losses. The purpose of this study was to screen three viruses; Deformed wing virus, Slow bee paralysis virus and Acute bee paralysis virus but also three parasites; Nosema spp., Crithidia spp., and Gregarine spp. due to their mortality and the lack of knowledge regarding some of the pathogens’ habitat and hosts. During the years of 2015 and 2016 three bee species were collected in a number of 156 samples including honeybees, bumblebees and solitary bees equally divided. Extraction of RNA and DNA was done using only the abdomen which was homogenised by the use of MixerMill and later extracted on a QIAcube. Real-time qPCR was used in this study as a qualitative screening method. DWV was detected primarily in honeybees, infecting as much as 70 %. The parasite known to have bumblebees as its host, namely Crithidia spp. was detected in 23 % of the honeybees collected, 15 % of the bumblebees and 2 % of the solitary bees. According to the results; Crithidia spp. is no longer a specific parasite found in bumblebees but have broaden its host spectrum to both honeybees and solitary bees. Furthermore, the parasite detected in most samples was Gregarine spp. and was detected in 50 % out of the bees collected suggesting that this parasite is common in Swedish bees.
39

The correlation between consumption of benzodiazipines and fall-tendency in elderly people : A literature study

Hadi, Hadi January 2016 (has links)
No description available.
40

Mechanistic modelling - a BOLD response to the fMRI information loss problem

Lundengård, Karin January 2017 (has links)
Functional Magnetic Resonance Imaging (fMRI) is a common technique for imaging brain activity in humans. However, the fMRI signal stems from local changes in oxygen level rather than from neuronal excitation. The change in oxygen level is referred to as the Blood Oxygen Level Dependent (BOLD) response, and is connected to neuronal excitation and the BOLD response are connected by the neurovascular coupling. The neurons affect the oxygen metabolism, blood volume and blood flow, and this in turn controls the shape of the BOLD response. This interplay is complex, and therefore fMRI analysis often relies on models. However, none of the previously existing models are based on the intracellular mechanisms of the neurovascular coupling. Systems biology is a relatively new field where mechanistic models are used to integrate data from many different parts of a system in order to holistically analyze and predict system properties. This thesis presents a new framework for analysis of fMRI data, based on mechanistic modelling of the neurovascular coupling, using systems biology methods.  Paper I presents the development of the first intracellular signaling model of the neurovascular coupling. Using models, a feed-forward and a feedback hypothesis are tested against each other. The resulting model can mechanistically explain both the initial dip, the main response and the post-peak undershoot of the BOLD response. It is also fitted to estimation data from the visual cortex and validated against variations in frequency and intensity of the stimulus. In Paper II, I present a framework for separating activity from noise by investigating the influence of the astrocytes on the blood vessels via release of vasoactive sub- stances, using observability analysis. This new method can recognize activity in both measured and simulated data, and separate differences in stimulus strength in simulated data. Paper III investigates the effects of the positive allosteric GABA modulator diazepam on working memory in healthy adults. Both positive and negative BOLD was measured during a working memory task, and activation in the cingulate cortex was negatively correlated to the plasma concentration of diazepam. In this area, the BOLD response had decreased below baseline in test subjects with >0.01 mg/L diazepam in the blood. Paper IV expands the model presented in Paper I with a GABA mechanism so that it can describe neuronal inhibition and the negative BOLD response. Sensitization of the GABA receptors by diazepam was added, which enabled the model to explain how changes to the BOLD response described in Paper III could occur without a change in the balance between the GABA and glutamate concentrations. The framework presented herein may serve as the basis for a new method for identification of both brain activity and useful potential biomarkers for brain diseases and disorders, which will bring us a deeper understanding of the functioning of the human brain.

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