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Factors associated with the development of drug resistant tuberculosis in EthiopiaHenock Bekele Keto 01 1900 (has links)
PURPOSE: The purpose of this study was to assess factors associated with the development of drug resistant tuberculosis in Ethiopia.
DESIGN: A quantitative case-control study was conducted to determine if there were any significant differences in prevalence of pre-defined factors between cases and controls.
METHODS: Cases were patients with drug resistant tuberculosis who had a confirmed diagnosis by culture drug-susceptibility or gene expert tests. Successfully treated, tuberculosis symptom free patients who had been on first-line tuberculosis treatment and who were registered as cured or treatment completed were taken as controls. An equal number of cases (N=181) and controls (N=181) was selected using a systematic random sampling method and was used in the study. A structured questionnaire developed by the researcher was used to collect data. Odds ratio and multiple logistic regression were used to quantify the strength of association between dependent and independent variables.
RESULTS: The development of drug resistant tuberculosis was significantly associated with two or more previous episodes of tuberculosis illness (adjusted odds ratio (AOR): 14.84; 95% CI 8.90 –24.75), previous first-line tuberculosis treatment not directly observed by a health worker for 7 to 8 weeks (AOR: 13.41; 95% CI 8.06 – 22.29) and previous first-line tuberculosis treatment outcome of failure (AOR: 39.19; 95% CI 12.05 -127.46). Interruption of first-line tuberculosis treatment for one day or more (AOR = 4.28; 95% CI 2.76 – 6.64) and history of treatment in the first-line tuberculosis treatment category for previously treated patients (AOR: 3.70; 95% CI 2.40 – 5.72) were also significantly associated with the development of drug resistant tuberculosis in the current study.
CONCLUSION: Patients with a history of previous first-line tuberculosis treatment, patients who interrupted previous first-line tuberculosis treatment and patients with previous first-line tuberculosis treatment outcome of failure were at high risk of developing drug resistant tuberculosis. Therefore, the full course of first-line tuberculosis treatment should be given, following the Directly Observed Treatment (DOT) guide. Patients with recurrent tuberculosis and unfavourable first-line tuberculosis treatment outcome should be tested for drug susceptibility. / Health Studies / D. Litt. et Phil. (Health Studies)
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Ototoxicity Monitoring using Automated Extended High-Frequency Audiometry and the Sensitive Range of Ototoxicity in Patients with MDR-TBGreeff, Wildine Marion 26 January 2021 (has links)
Background: Disabling hearing loss is a global burden. This burden is worsened by the emergence of multi-drug resistant tuberculosis (MDR-TB). Some of the medications used to treat MDR-TB are damaging to the cochlea and auditory nerve (ototoxic) and can lead to permanent hearing loss and/or balance disorders. Ototoxicity monitoring aims to reduce this burden by preventing or minimising the damage caused by ototoxic treatment as it can progress and worsen speech perception difficulties. However, the proposed test battery for ototoxicity monitoring is lengthy and demands active participation which is not ideal for ill patients (such as those on MDR-TB treatment). The Sensitive Range of Ototoxicity (SRO) technique is recommended to shorten the test time. The SRO consists of seven consecutive relatively high frequencies determined from the highest frequency the participant responded to. The SRO technique is time efficient. Although the SRO technique provides the prospect of a shortened test battery, there is still a global lack of audiologists. Automated audiometry is a vital application for testing especially when audiologists are not available to physically do the test. Automated audiometry has been previously validated. Clinically, automated audiometry is objective and allows for standardisation. Even though automated audiometry helps improve access to monitoring more patients, patient preference is an important factor when using automated audiometry to ensure patient-centred care is not compromised. Aims and Objectives: This study aimed to investigate the specificity and sensitivity of the SRO technique with automated audiometry compared to the gold standard (manual audiometry). This comparison was made by firstly, determining the testing time efficiency and the correlation of thresholds obtained with the different test methods and, secondly, testing the diagnostic value of automated audiometry using the SRO technique. The incidence of an ototoxicity-induced hearing loss was described by determining the time interval between starting ototoxic MDR-TB treatment and the onset of a significant threshold shift (STS) according to ASHA's criteria. Lastly, the test method preference of the participants with MDR-TB was described and compared using a short exit survey. Study Design: A prospective repeated-measures study design was used. Participants were chosen based on a risk factor (i.e. exposure to ototoxic medication) for an outcome of interest (i.e. the presence or absence of an STS). With a repeated measures study, multiple tests using different test methods can be compared with the same sample. Participants: Twenty-seven in-patients at Brooklyn Chest Hospital and DP Marais TB Hospital with normal hearing and on MDR-TB medication were included in the study. Their age range was from 19 to 51 years old with an average age of 33 years old. Non-probability convenience sampling was used as it was cost-effective, reduced data collection time and was relatively easy to execute. Data collection materials and procedures: The procedure for data collection included weekly follow-up testing for a maximum of four weeks. The test battery was as follows: an auditory symptom questionnaire, otoscopy examination, and manual and automated audiometry using the SRO technique with a fifteen-minute break in between. Participants were tested with the KUDUwave ™ in a non-sound treated room. The frequency range was determined with the SRO technique. If an STS was obtained, the patient was discharged from the study after completing an exit survey. Statistics: Analysis included descriptive statistics and inferential statistics. A Bonferroni corrected p-value (initially p ≤ 0.05) was used. Manual and automated audiometry thresholds were compared using the Pearson's Correlation Coefficient test. Manual and automated audiometry testing time and threshold means were compared using paired sample's t-tests. The diagnostic value of automated audiometry with the SRO technique was assessed with Receiver Operating Characteristics (ROC) Curves. Results: Manual audiometry was statistically more time-efficient compared to automated audiometry by an average of one minute and ten seconds (t (94) = -5.44; p< 0.003). There was a strong positive correlation for both left and right ears between the thresholds' obtained from manual and automated audiometry at 8kHz to 16 kHz (df> 28 = r > 0.70, p< 0.003). Automated audiometry was found to be a fair diagnostic test (area under the curve was 0.75; p= 0.002). Also, the ROC curve revealed that automated audiometry had a sensitivity of 61% and specificity of 90% when compared to manual audiometry (gold standard). Only participants that started data collection within 31 days after starting their MDR-TB treatment were included in the analysis of determining the incidence of an ototoxicity-induced hearing loss (n= 24 ears). This study found that 41.67% of ears (n= 10) had an ototoxicity-induced hearing loss. A box and whisker plot revealed that data was skewed to the right (i.e. more variation in data between the median and the maximum values) and that the median number of days for an ototoxicity-induced hearing loss to appear was 33 days. Secondly, 55.55% of participants (n=15 out of 27) reported auditory symptoms before data collection commencement. Aural fullness was the most reported symptom (n= eight out of 15). Ten out of 15 (66.66%) participants that reported auditory symptoms obtained an ototoxicity-induced hearing loss. Lastly, most participants (i.e. 13 out of 19; 68.42%) that completed the exit survey had no preference between manual or automated audiometry. The common rationale among these participants was “No difference noted.” Conclusion: This research study has revealed that manual audiometry was more time-efficient compared to automated audiometry in patients with MDR-TB. Also, automated audiometry was a fair diagnostic test. It may aid in reducing the disproportionate audiologist to patient ratio, especially in a developing country. However, manual audiometry (with the SRO technique) is more clinically appropriate in patients that are difficult-to-test. Secondly, audiometric settings can be changed to accommodate testing frequencies in 1/6 octaves so that the SRO technique can be clinically adopted. An ototoxicity-induced hearing loss seems to appear 33 days after ototoxic MDR-TB treatment commencement. Aural fullness was a commonly reported symptom among participants with MDRTB. Aural fullness is omnipresent in peripheral auditory pathologies. Therefore, auditory symptoms reported by patients' needs a comprehensive audiological investigation. Lastly, more research is needed on how patients (and clinicians) experience the advances in technology innovation especially in audiology where technology innovation is continuously evolving.
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Second Messenger Cyclic-di-GMP Regulation in Acinetobacter baumanniiDeal, Justin 01 May 2020 (has links)
Over time, “superbugs,” or bacteria that have become resistant to antibiotics, have become a great concern in modern medicine. Viable alternates are currently being looked into as effective and safe ways to prevent or treat infections caused by these superbugs. One such method is through the utilization of the second messenger molecule cyclic-di-GMP (c-di-GMP) that has been shown to regulate phenotypes within other bacteria that may control surface colonization in Acinetobacter baumannii. Through a series of experiments, the active enzymes that create c-di-GMP - diguanylate cyclases - and break down c-di- GMP - phosphodiesterases - have been inactivated in mutants to test phenotypes including biofilm formation, motility, antibiotic resistance, and desiccation survival. The research’s objective is to show that manipulation of c-di-GMP within the multi-drug resistant strain of Acinetobacter baumannii may serve as a means to control this bacteria.
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Molecular Mechanisms for Antiviral Activities and HIV-1 Resistance to Allosteric Integrase InhibitorsHoyte, Ashley Christopher January 2018 (has links)
No description available.
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MECHANISMS OF METHOTREXATE SECRETION AND DETOXIFICATION BY MALPIGHIAN TUBULES OF DROSOPHILA MELANOGASTERChahine, Sarah S. 10 1900 (has links)
<p>Insects are continually exposed to potentially toxic endogenous compounds and xenobiotics that require rapid elimination from the body. Xenobiotic resistance in insects has evolved predominantly by increasing the activity of detoxification enzymes and/or by increasing toxin excretion via the Malpighian (renal) tubules. The tubules have long been known to transport organic anions at high rates. This thesis examines the mechanisms of excretion and detoxification of the organic anion methotrexate (MTX) by isolated tissues of the fruit fly <em>Drosophila melanogaster</em>. A radioisotope tracer technique and the Ramsay assay were used to measure MTX secretion. Quantitative PCR (qPCR) was used to evaluate the expression of the genes for putative organic anion transporters. My results show that MTX transport across the Malpighian tubule epithelium is active, saturable, Na<sup>+</sup>-independent and inhibited by a wide range of organic anions including MK-571, probenecid and Texas Red. Pharmacological studies and qPCR analyses suggest multiple transporters are involved in the movement of MTX across the Malpighian tubules. Moreover, chronic exposure of larvae to dietary MTX or salicylate dramatically increases the transepithelial transport of MTX by isolated Malpighian tubules, suggesting that excretion of MTX is upregulated by exposure to these organic anions in the diet. In addition, treatments known to increase expression of specific detoxification enzymes, such as the P450 monoxygenases (P450s) and the glutathione-S-transferases (GSTs), also led to an increase in expression levels of multidrug efflux transporter (MET), multidrug resistance like protein 1 (dMRP) as well as to increased secretion of MTX by the tubules. This latter finding suggests a coordinated response to toxin exposure, so that when detoxification pathways are increased, there is a corresponding increase in the capacity for elimination of the products of P450 and GST enzymes. Finally, the last section of this thesis has shown that RNAi knockdown of a single organic anion transporter gene in the principal cells of <em>D. melanogaster</em> Malpighian tubules is associated with reductions in the expression of multiple, functionally-related genes. Importantly, these results indicate that dMRP andMET are not the dominantMTX transporters in the tubules when flies are reared onMTX-enriched diets. However, reductions in the expression of organic anion transporting polypeptide (OATP) are associated with reduced secretion of the organic anionsMTX, fluorescein and Texas Red. Taken together, these results suggest that OATP and at least one additional transporter, as yet unidentified, are required forMTX secretion. In conclusion, the results of my research contribute to our understanding of the mechanisms of organic anion detoxification and excretion in flies exposed to dietary toxins.</p> / Doctor of Science (PhD)
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The molecular epidemiology of mycobacterium tuberculosis : role in understanding disease dynamics in high prevalence settings in Southern Africa regionChihota, Violet 03 1900 (has links)
Thesis (PhD)--University of Stellenbosch, 2011. / ENGLISH ABSTRACT: The tuberculosis (TB) incidence has increased in Southern Africa and the situation
is worsened by the emergence of drug-resistant Mycobacterium tuberculosis strains.
Molecular biological techniques have been used to understand the disease dynamics of
TB. In a series of studies we describe the use of these techniques to understand the
disease dynamics of TB in Southern Africa.
Using spoligotyping and IS6110-restriction fragment length polymorphism (RFLP) to
characterize M. tuberculosis strains from TB patients in Zimbabwe, we identified a
genotype causing a disproportionate number of TB cases. The genotype belonged to the
Latin American Mediterranean (LAM) lineage and we named it the Southern Africa1
(SAF1) family and later renamed it SAF1/RDRio, also reflecting its predominance in
South America. To establish if this family of strains was predominant elsewhere in
Southern Africa, genotypes were compared to those from Western Cape, South Africa
and Zambia. The SAF1/RDRio strains were highly prevalent in Zambia but were only a
minor fraction of the strains in South Africa. The geographical distribution of
SAF1/RDRio strains was determined in Gweru, Zimbabwe, and was found to be spread in
high incidence areas. From these two studies it was hypothesized that certain host and
bacterial factors were associated with disease due to SAF1/RDRio.
Subsequently potential risk factors and clinical outcomes of disease due to SAF1/RDRio
strains were explored. An association was found with smoking and cavitary pulmonary
disease suggesting that SAF1/RDRio caused a more severe and highly transmissible
formof TB Using IS6110-RFLP, principal genetic grouping, spoligotyping, IS6110 insertion-site
mapping and variable-number tandem repeats (VNTR) typing, low IS6110 copy clade
(LCC) identified in Zimbabwe were characterized and compared to the strains from Cape
Town, South Africa and other regions. The LCC strains from Cape Town, South Africa,
were found to have close evolutionary relationship with strains from Zimbabwe and other
regions and were widely distributed suggesting they play an important role in the global
TB epidemic.
Observations from these studies and those from other studies led to the hypothesis that
specific genotypes of M. tuberculosis predominate in regions of Southern Africa. To gain
an insight on the population structure of M. tuberculosis strains in Southern Africa,
spoligotyping and/or IS6110-RFLP data from eight countries were compared. This is the
first study to describe the M. tuberculosis population structure in Southern Africa.
Distinct genotypes were associated with specific geographic regions. These findings have
important implications for TB diagnostics, anti-TB drug and vaccine development.
The population structure of multidrug-resistant (MDR), pre-extensively drug-resistant
(pre-XDR) and extensively drug-resistant (XDR) M. tuberculosis isolates from provinces
in South Africa was also determined. This is again the first study to describe the
population structure of drug-resistant M. tuberculosis in South Africa. The results also
showed geographic localization of genotypes and an association with resistance class.
However, decreasing strain diversity was observed as the isolates evolved from MDR-TB
to XDR-TB suggesting selection for the specific genotypes. These findings highlight the importance of identifying genetic markers in drug-resistant strains, to enhance early
detection of those at risk of developing XDR-TB. / AFIKAANSE OPSOMMING: Die voorkoms van tuberkulose (TB) in Suider Afrika word vererger deur stamme van
Mycobacterium tuberculosis wat weerstandig is teen die beskikbare anti-tuberkulose
middels. Molekulêre tegnieke word gebruik om in hierdie reeks studies die dinamika van
TB in Suider Afrika te ondersoek
Deur spoligotipering en IS6110 restriksie fragment lengte polimorfisme (RFLP) tegnieke
te gebruik om M. tuberculosis stamme van pasiente in Zimbabwe te beskryf, het ons ‘n
genotipe gevind wat ‘n buitengewone aantal TB gevalle veroorsaak het. Hierdie genotipe
is deel van die internasionaal beskryfde Latyns Amerikaase en Meditereense (LAM) stam
familie. Ons het dit die Suider Afrikaanse Familie1 (SAF1) genoem, maar later hernoem
na SAF1/RDRio, omdat dieselfde genotipe in ook volop is in Suid Amerika. Om vas te stel
of hierdie familie ook oorheesend is in die res van Suider Afrika, is dit vergelyk met
beskikbare databasisse van die Wes-Kaap, Suid-Afrika en Zambië. Alhoewel
SAF1/RDRio in die Wes-Kaap gevind is, dra dit slegs tot ‘n mindere mate by tot die
plaaslike TB epidemie. Aan die anderkant kom SAF1/RDRio baie algemeen in Zambië
voor. ‘n Verdere studie wys ook dat die SAF1/RDRio familie eweredig en wyd verspreid
voorkom in hoë insidensie gebiede in Gweru, Zimbabwe. Vanuit die bevindings van
hierdie 2 studies, kan ons aflei dat sekere gasheer- en bakteriële eienskappe geassosieer is
met SAF1/RDRio-TB-infeksie.
Hierna is potensiële risiko faktore en kliniese uitkomste van siekte as gevolg van infeksie
met SAF1/RDRio ondersoek. ‘n Assosiasie met rook en kaviterende pulmonale infeksie is gevind,wat daarop dui dat SAF1/RDRio erger vorm van TB veroorsaak en hoogs
oordraagbaar is.
Deur gebruik te maak van IS6110- (RFLP), hoof groep groepering, spoligotipering,
IS6110 invoegings kaartering en veranderlike getal tandem herhaling (VNTR) tipering
kon lae IS6110 invoeginsgetal (LCC) stamme van Kaapstad, Zimbabwe en ander gebiede
vergelyk word. Al die LCC stamme in die studie is evolusionêr naby verwant aan mekaar
en is wyd verspreid, wat dui op hulle belangrike rol in die wêreldwye TB epidemie.
Waarnemings in hierdie asook ander studies het tot die hipotese gely dat spesifieke
genotipes van M. tuberculosis dominant is in verskillende gebiede van Suider Afrika. Om
meer insig tot die populasie samestelling van M. tuberculosis stamme in Suider Afrika in
te win is spoligotipes en RFLP-data van 8 lande vergelyk. Hierdie is die eerste studie om
die populasie samestelling van M. tuberculosis in Suider Afrika te beskryf en is
belangrike fir toekomstige ontwikkeling van nuwe TB diagnose tegnieke, anti-TB
middels en TB entstowwe.
Die populasie samestelling van multiweerstandige (MDR), pre-ekstreme weerstandige
(pre-XDR) en ekstreme weerstandige (XDR) M. tuberculosis van verskillende provinsies
in Suid-Afrika is ook bepaal. Hierdie studie is ook die eerste wat die populasie
samestelling van weerstandige M. tuberculosis in Suid-Afrika beskryf. Die resultate wys
geografiese lokalisering van genotipes en ‘n assosiasie met weerstandigheidsklas. ‘n
Afname in stam diversiteit soos die isolate van MDR-TB tot XDR-TB ontwikkel, dui op seleksie van spesifieke genotipes. Hierdie bevinding lê die klem op die belangrikheid van
die identifisering van genetiese merkers in weerstandige stamme om die risiko vir die
ontwikkeling van XDR-TB te verminder deur vroë deteksie.
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EKT und unerwünschte Ereignisse – eine retrospektive Analyse an der Universitätsmedizin Göttingen / Electroconvulsive therapy and side effects - a retrospective analysis at the Universitätsmedizin GöttingenZottmann, Claudia 08 March 2017 (has links)
No description available.
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Synthesis, characterization and anti-bacterial studies or Hydrazide Schiff bases of Acetylacetonate metal complexesDikio, Charity Wokwu 06 1900 (has links)
M. Tech. (Chemistry, Department of Chemistry), Vaal University of Technology / Infectious diseases, a group of illnesses caused by specific pathogens or its toxins is a leading cause of death globally. Treatment with antibiotics is a key intervention in the control and management of many infectious disease. However, the increasing incidence of antibiotics failure, due to the emergence of drug resistant pathogens, is rendering the use of antibiotics chemotherapy ineffective. A possible solution is to synthesize new compounds with broad spectrum characteristics and superior drug performances as alternative to conventional antibiotics. Schiff Bases are biologically active ligands. They form metal complexes with superior biological activities. This research aims to synthesize some Schiff Base metal complexes and investigate their biological effects on Staphylococcus aureus and Enterococcus faecalis.
Metal acetylacetonates of Vanadium, Copper, Cobalt, Zinc, Magnesium, Manganese, Cadmium, Nickel and Iron were synthesized and characterized by Fourier transform infrared spectroscopy. Four Schiff bases, LI, L2, L3 and L4 were also synthesized by the condensation of 4- (diethylamino)-2-hydroxybenzaldehyde with 4-nitrobenzohydrazide and 4-methoxybenzohydrazide to form L1 and L2. 4-(dimethylamino) benzaldehyde was reacted with 4-nitrobenzohydrazide and 4-methoxybenzohydrazide to form L3 and L4 respectively.
The Schiff base ligands were then reacted with synthesized Vanadium, manganese, cobalt and magnesium acetylacetonates to form Schiff base complexes (SBC 1A to 4D).
Schiff bases ligands and complexes were characterized by FT-IR, 1H-NMR, 13C-NMR, TGA and DTA. Fourier Transform infrared spectroscopy (FTIR) of the acetylacetonates showed the formation of metal acetylacetonates as characterized by the absence of the carbonyl stretching n(C=O) vibration in metal acetylacetonate spectra as compared to pure acetylacetone. Metal acetylacetonates also showed the presence of metal oxygen vibration frequency, n(M-O-C), in the spectra obtained. Thermogravimetric analysis (TGA) and Derivative or Differential Thermogravimetric analysis (DTA) of the Schiff base ligands showed the presence of a single decomposition product in L1, L2, L3 and L4 indicating the formation of a single reaction product while those of Schiff base complexes showed the formation of several decomposition products. Proton and carbon thirteen Nuclear Magnetic Resonance (1H- and 13C-NMR) spectroscopy of the Schiff base ligands indicated the presence of hydrogen and carbon-13 in different environments.
The chemical shifts of the hydrogens and carbon-13 provided evidence that Schiff base ligands were formed. The strongest evidence is the presence of the azomethine hydrogen and carbon in the spectra of the Schiff base ligands. The presence of aromatic hydrogens and carbon at chemical shift environments found in literature also confirmed the formation of Schiff base ligand. The NMR spectra of Schiff base complexes showed the presence of azomethine (HC=N) and aromatic hydrogens at expected chemical shifts.
The synthesized Schiff bases and their corresponding metal complexes were screened for their invitro antibacterial activities against two Gram-positive (Staphylococcus aureues and Enterococcus feacalis) bacterial strains by the Agar-well diffusion methods.The ligands and complexes were tested against confirmed S. aureus and E. faecalis strains and only 4 exhibited antimicrobial activities. The ligands and complexes were effective against the S. aureusand E. faecalis isolates. / VUT
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Contrôle volontaire des crises et régulation des émotions dans l'épilepsie temporale pharmacorésistante : l’exemple d’une thérapie par GSR biofeedback / Voluntary control of seizures and emotional regulation in drug resistant temporal lobe epilepsy : an exemple of skin conductance biofeedbackKotwas, Iliana 28 September 2018 (has links)
Parmi les patients souffrant d'épilepsie, particulièrement du lobe temporal (ELT), 30% restent résistants aux médicaments malgré l'administration optimale des traitements pharmacologiques. Le caractère imprédictible des crises est l’un des aspects les plus invalidants de la maladie. De plus, les troubles dépressifs et anxieux sont des comorbidités psychiatriques fréquemment associées à l’épilepsie et impactent encore plus négativement la qualité de vie que les crises. Les approches par biofeedback, ont démontré leur efficacité dans le contrôle des crises. Une thérapie par biofeedback sur la conductance cutanée (GSR biofeedback) a montré son efficacité sur les symptômes psychiatriques. Cependant, les mécanismes sous-tendant l’efficacité sur ces symptômes restent peu connus. L’objectif de cette thèse est de mieux comprendre ces mécanismes. Deux pistes sont explorées : une physiologique dans laquelle il existerait un effet direct du GSR biofeedback sur la régulation physiologique des émotions ; une attentionnelle, dans laquelle il y aurait un effet indirect de l’entraînement sur le contrôle de l’attention. Les études menées ont permis de montrer que les patients avec ELT présentent des réponses électrodermales aux émotions plus faibles que des témoins, mais qu'elles ne sont pas plus élevées après des séances de GSR biofeedback. En revanche, l’amélioration des symptômes anxieux et dépressifs est liée à des modifications du traitement attentionnel des informations menaçantes. Le GSR biofeedback en améliorant le contrôle attentionnel induirait une diminution de la vigilance face à la menace, conduisant à une réduction de la vulnérabilité émotionnelle chez ces patients. / Among patients with epilepsy, particularly temporal lobe epilepsy (TLE), 30% remain drug-resistant despite optimal administration of pharmacological treatments. The unpredictability of seizures is one of the most disabling aspects of the disease. In addition, depressive and anxiety disorders are psychiatric comorbidities frequently associated with epilepsy and have a greater negative impact on quality of life than seizures. Biofeedback approaches have been shown to be effective in controlling seizures. A biofeedback therapy on skin conductance (GSR biofeedback) has shown its efficacy on psychiatric symptoms. However, the mechanisms underlying this efficacy remain poorly understood. The objective of this thesis is to better understand these mechanisms. Two tracks are explored: a physiological one in which there is a direct effect of GSR biofeedback on the physiological regulation of emotions; an attentional one, in which there would be an indirect effect of the training on the control of attention. The studies presented have shown that TLE patients have weaker electrodermal responses than controls but that they are not higher after GSR biofeedback sessions. In contrast, the improvement of anxiety and depressive symptoms is related to changes in the attentional processing of threatening information. GSR biofeedback by improving attentional control would lead to a decrease in alertness to threat, leading to a reduction in emotional vulnerability in these patients.
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Tuberculose multirresistente e extensivamente resistente em área metropolitana de elevada incidência - município de Santos (SP), Brasil / Multidrug and extensively drug-resistant tuberculosis in the metropolitan area of high incidence - the city of Santos (SP), BrazilCoelho, Andrea Gobetti Vieira 03 March 2015 (has links)
INTRODUÇÃO: A incidência de tuberculose (TB) em Santos (SP) situa-se em 73/100.000 habitantes-ano. A prevalência média de coinfecção TB/HIV é de 16%, taxas de cura e abandono de tratamento, entre casos novos são, respectivamente, 71% e 12%. Tais indicadores sugerem elevado risco para TB multidroga resistente (TBMR) no município, com incidência estimada em 1,9/100.000 habitantes-ano. OBJETIVO: Descrever e analisar o perfil de sensibilidade às drogas (TS) de primeira e segunda linha de tratamento entre pacientes com TB pulmonar (TBP), estimar a incidência de TBMR e a proporção de TB extensivamente resistente (TBXR); analisar aspectos moleculares, epidemiológicos e institucionais dos casos de TBP resistentes em Santos (SP). MÉTODOS: Estudo descritivo de uma coorte de pacientes de TBP, com início de tratamento ou retratamento entre 01 de janeiro de 2011 a 31 de dezembro de 2012. Definiu-se como caso de TBP, indivíduos com 15 anos ou mais, de ambos os sexos, residentes no município de Santos, com manifestações clínicas compatíveis com TBP e confirmação por cultura com isolamento de Mycobacterium tuberculosis. As variáveis de interesse para o estudo foram as características sociodemográficas, história atual e pregressa de TB, aspectos relativos ao tratamento, co-morbidades, ao diagnóstico e resistência a drogas. Para as análises comparativas entre proporções foram usados os testes qui-quadrado de Pearson e o Exato de Fisher e para variáveis contínuas o teste T de Student ou o de Kruskal - Wallis. Os perfis genéticos dos isoladas resistentes a ao menos uma droga foram obtidos pela técnica RLFP e analisados pelo programa Bionumerics versão 5.0 (Applied Maths - Bélgica). A descrição da distribuição espacial da TB resistentes e clusters foram feitas mediante a inserção dos casos no mapa de Santos, por endereço de residência, segundo o índice de vulnerabilidade social. RESULTADOS: Dos 263 casos de TBP selecionados, 68,4% (180/263) eram do sexo masculino, a mediana da idade foi de 38 anos, 8,7% (23/263) eram diabéticos; 20,4% (42/206) dos casos novos apresentavam ao menos um fator de risco para TBMR; destacando-se entre estes casos 10,7% (22/206) de confecção HIV/TB; 47,3% (123/260) tiveram tratamento supervisionado, 14,7% (91/617) dos contatos foram examinados, 18,6% (49/263) foram hospitalizados durante o tratamento, perfazendo uma média de 145,4 dias por paciente. Entre os casos resistentes a ao menos uma droga, a resistência à isoniazida foi 8,4% (22/263) e à rifampicina 3,8% (10/263) dos casos. A TBMR primária foi encontrada em 1,9% (4/206) dos casos e destes 25,0% (1/4) eram TBXR. A incidência média anual de TBMR foi de 0,57/100,000 habitantes. Dos 25 isolados resistentes ao menos uma droga, submetidos à RFLP, 12 (48,0%) foram agrupados em seis grupos genéticos, com dois pacientes em cada grupo. CONCLUSÕES: A elevada proporção TBMR primária, com um caso de TBXR enfatizam a necessidade de universalizar a cultura e TS, ampliar a cobertura do tratamento supervisionado, a investigação rotineira dos contatos e o monitoramento da resistência a drogas. O fortalecimento da vigilância da resistência às drogas é indispensável para o contínuo aperfeiçoamento do Programa de Controle da TB, especialmente em regiões de elevada carga da doença / INTRODUCTION: The incidence of tuberculosis (TB) in Santos (SP) is located around 73 / 100,000-year, approximately double that found on average in the country. The average prevalence of TB / HIV is 16% cure rates and treatment dropout among new cases are, respectively, 71% and 12%. Such indicators suggest high risk for multidrug-resistant TB (MR-TB) in the city, with the incidence estimated at 1.9 / 100,000-year. OBJECTIVE: To describe and analyze the sensitivity to drugs of first and second line treatment of patients with pulmonary TB (PTB) to estimate the incidence of MR-TB and extensively drugresistant TB (TBXR), describe molecular and institutional aspects, spatial distribution, epidemiological PTB resistant cases in the city of Santos (SP). METHODS: A descriptive study of a cohort of patients with PTB residing in the city who started treatment or retreatment in the period January 2011 to December 31, 2012. The case definition PTB individuals 15 years or more, both sexes, living in the city of Santos (SP), who present clinical manifestations compatible with PTB and whose confirmation was made by culture with isolation of M. tuberculosis. The variables of interest for the study were: bacteriological / laboratory socio-demographic characteristics, current and previous history of TB, aspects related to treatment, and comorbidities. For comparative analyzes of proportions the chi-squared tests and Fisher\'s exact were used for continuous variables and the Student t test or the Kruskal - Wallis. The genetic profiles of isolates resistant to at least one drug were obtained by RFLP (length polymorphism restriction fragment) and analyzed using version BioNumerics 5.0 (Applied Maths - Belgium) software. The description of the spatial distribution of resistant TB and the clusters was made by inserting the cases in Santos map, by address of residence, which was according to the index of social vulnerability. RESULTS: Of the 263 cases of PTB selected, 68.4% (180/263) were male, th median age was 38 years, 8.7% (23/263) were diabetes; 20.4% (42/206) of new cases had at least one risk factor for MR-TB, especially 10.7% (22/206) of making HIV / TB; 47.3% (123/260) underwent supervised treatment, 14.7% (91/617) of the contacts were examined, 18.6% (49/263) were hospitalized during treatment, totaling 7127 days of hospitalization with a mean 145.4 days per patient. Among the cases resistant to at least one drug resistance to isoniazid 8.4% (22/263) and rifampin 3.8% (10/263) of the cases was found. The primary MR-TB was found in 1.9% (4/206) of MR-TB cases and of these 25.0% (1/4) were TBXR. The average annual incidence of MDR-TB was 0.57/100,000 inhabitants. Of the 25 isolates resistant least one drug, subjected to molecular characterization of IS6110, 12 (48.0%) were grouped in six clusters, with each group including two isolates. CONCLUSIONS: A high proportion of primary MR-TB, including a case of TBXR emphasizes the need to universalize culture and TS, expand the coverage of supervised treatment, routine investigation of contacts and monitoring of drug resistance. The strengthening of the surveillance of drug resistance is essential for continuous improvement of the TB Control Program, especially in regions of high disease burden
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