Global ETD Search

1	Role of yeast ArsA homologue ARR4 in thermotolerance of Saccharomyces cerevisiae Kuo, Ya-Po 24 July 2002 (has links) The ArsA homologue ARR4 in Saccharomyces cerevisiae, encoded by YDL100C. Homologues of the E. coli ArsA are found in S. cerevisiae about 29 % from Genetic Computer Group (GCG). The ARR4 gene product contains an ATP binding site that is similar to protein ArsA from E. coli Disruption of ARR4 in yeast is not lethal but the disrupted strain was unable to grow at 40¢J, suggesting that the possible cause of cell death in KO strain at 40¢J was investigated. The accumulation of trehalose and the in vivo molecular oxidation level are higher in KO strain than that in WT strain under heat stress condition. These suggest that the increased reactive oxygen species (ROS) but not the amount of thermoprotectant trehalose is most likely to be the reason for cell death in KO strain. In this report ROS scavenger system show that the activities of ROS scavenger system are lower in KO compared to that in WT strain at 30¢J or 40¢J. This suggests that ARR4 is involved in the heat stress ¡Boxidative stress and osmatic stress triggers activation of the STRE ( stress tolerance response element) regulon. Further studies involvement ARR4 of CTT1, SOD1, and TSL1 gene of STRE-drive gene by RT-PCR. Here the report that the KO strain exhibits a thermosensitivity phenotype in comparison to wild-type strain, indicating that ARR4 may act as a component of a stress tolerance network. STRE ROS Thermotolerance ARR4 yeast Heat stress
2	Use of plant growth promoting endophytic bacteria to alleviate the effects of individual and combined abiotic stresses on plants as an innovative approach to discover new delivery strategies for bacterial bio-stimulants Tufail, Muhammad Aammar 19 May 2021 (has links) Bacterial endophytes are the organisms that live inside the plant for a full or a part of their life cycle. Endophytic bacteria have captured the interest of agriculture industry due to their plant beneficial properties, such as synthesis of phytohormones, solubilization of soil nutrients, and alleviation of biotic and abiotic stresses. Several studies have reported that stress tolerant endophytic bacteria can work with a similar performance as non-stressed conditions when inoculated to the plants under stressed conditions. Combination of abiotic stresses such as salinity, drought and low nitrogen stress can have additive or agonistic effects on bacterial and plant growth, and their interactions. However, very few studies have reported the impact of combined stress on endophytic bacterial assisted plant growth promotion. Therefore, understanding the underlying mechanisms of endophytic bacterial assisted plant’s tolerance abiotic stresses may provide the means of better exploiting the beneficial abilities of endophytic bacteria in agricultural production. Thus, the aim of this thesis was to study the stress tolerance mechanisms, beneficial characteristics, and plant growth promotion characteristics of endophytic bacteria under individual and combined abiotic stresses. Transcriptome analysis of endophytic bacteria revealed that tolerance mechanisms to deal with one kind of stress is different than concurrent stresses. Salinity and drought stress largely modulated the genes involved in flagellar assembly and membrane transport, showing reduced motility under stress conditions to preserve the energy. Additionally, bacterial endophyte that can fix nitrogen was studied with maize plant growth promotion under drought and low nitrogen stress conditions. The results suggested that diazotrophic bacterial endophyte can promote plant growth under moderate individual and combined stress conditions. Plant growth promoting endophytic bacteria can be utilized as an efficient tool to increase crop production under individual and concurrent abiotic stresses. plant growth endophyte endophytic bacteria salinity salt tolerance salt stre abiotic stre transcriptome drought combined stre low nitrogen nitrogen fixing bacteria meta-analysi RNAseq Settore AGR/16 - Microbiologia Agraria Settore BIO/04 - Fisiologia Vegetale Settore BIO/11 - Biologia Molecolare
3	Pharmacotherapy for Social Anxiety Disorder and Posttraumatic Stress Disorder: New Meta-Analytic Approaches to Synthesising the Evidence Williams,Taryn Amos 23 November 2022 (has links) (PDF) Background Social anxiety disorder (SAD) and posttraumatic stress disorder (PTSD) are prevalent, disabling and highly comorbid disorders. SAD is the most prevalent of the anxiety disorders, and PTSD is the central disorder in the DSM-5 section on trauma- and stressor-related disorders. Given the growing need to consider the totality of evidence for pharmacological treatment for SAD, the publication of systematic reviews and of novel meta-analytic approaches have become of interest for the use of medication in their treatment and decision making. This dissertation has three objectives 1) To update Cochrane reviews of pharmacotherapy for SAD and PTSD, 2) To conduct a qualitative systematic review of network meta-analyses for pharmacological treatment of common mental disorders, 3) To conduct network meta-analyses for SAD and for PTSD and to compare findings to standard pairwise meta-analytic methods. Methods To obtain eligible trials to answer each aim, trials were identified through a systematic search of a variety of electronic databases: the Cochrane Common Mental Disorders Controlled Trials Register (CCMDCTR-Studies and CCMDCTR-References), MEDLINE, EMBASE, PsycINFO, Google Scholar, Scopus, PubMed Central, the International Clinical Trials Registry Platform (ICTRP) (apps.who.int/trialsearch), clinicaltrials.gov, the National PTSD Center Pilots database and the metaRegister module [mRCT] of the Controlled Trials database, specific to each aim. RCTs of pharmacological treatments comparing active drug versus active drug or active drug versus placebo for SAD and PTSD were considered for inclusion in the respective chapters, and in answering the aims, with the inclusion of add on trials in the SAD and PTSD NMA reviews. Adult participants (18-65 years) diagnosed with SAD and PTSD according to the Diagnostic Statistical Manual for Mental Disorders (DSM, all versions) were included in the individual reviews (i.e. for chapter two, three, five and six). In chapter three adolescents and adults with common mental disorders (depression, GAD, PD, OCD, PTSD, SAD and specific phobia) diagnosed according to the DSM or the International Classification of Diseases ((ICD- 10) were included. The primary and secondary outcomes across aims and reviews include clinical response rates (i.e. the Clinical Global Impressions Improvement scale (CGI-I) or similar) and acceptability (i.e. dropouts due to side effects); and the investigation of symptom severity for SAD with the Liebowitz Social Anxiety Scale (LSAS) and PTSD with the Clinician Administered PTSD Scale (CAPS). In addition, the proportion of dropouts due to any cause were also assessed. The quality of each trial was assessed according to the Cochrane Risk of Bias Tool. GRADE was also used to grade the quality of evidence for the Cochrane reviews and NMAs and the International Society for Pharmacoeconomics and Outcomes Research checklist of good research practices for indirect treatment-comparison in assessing studies for aim two. For aim one, the extracted data for the SAD and PTSD Cochrane reviews was exported into RevMan 5.3.5. Software, which was used to conduct a meta-analysis for SAD and PTSD separately. Pre-planned subgroup and sensitivity analyses were conducted for each review, as well as the generation of funnel plots to assess publication bias with the Eggers' regression test using the R statistical computing platform for the SAD review. In answering aim three, standard pairwise meta-analyses were performed using a random effects model and Frequentist method in RStudio version 3.5 for the SAD NMA review, and Bayesian method using Markov chain Monte Carlo methods in WinBUGS version 1.4.3 for the PTSD NMA. The P-score, an analogue to the surface under the cumulative ranking curves (SUCRA), was used to rank the treatments on a continuous scale for all pairwise comparisons for the SAD NMA, and for the PTSD review, ranking probabilities using the surface under the cumulative ranking curve (SUCRA) and mean ranks were assessed. Results For aim one, the evidence for the standard pairwise Cochrane reviews of SAD and PTSD were most convincing for the treatment efficacy of SSRIs (number of studies (k) = 24, risk ratio (RR) 1.65; 95% confidence interval (CI) 1.48 to 1.85, N = 4984 and k = 8, RR 1.61; 95% CI 1.41 to 1.84, N = 1078, respectively), and was based on very low quality evidence. Evidence of a benefit for the SSRIs was also observed for the reduction of social anxiety symptoms on the LSAS (k = 14, mean difference (MD) −10.14 points, 95% CI −14.05 to −6.22, N = 1990) and posttraumatic symptoms on the CAPS (k = 14, MD −4.69 points, 95% CI −7.18 to −2.20, N = 2709). Other medications such as SSRIs, the serotonin–norepinephrine reuptake inhibitor (SNRI) venlafaxine, monoamine oxidase inhibitors (MAOIs), reversible monoamine oxidase inhibitors (RIMAs), benzodiazepines, the antipsychotic olanzapine, and the noradrenergic and specific serotonergic antidepressant (NaSSA) atomoxetine were also effective in reducing SAD symptoms, with evidence of a treatment response for anticonvulsants with gamma-amino butyric acid (GABA) analogues, the MAOIs, the RIMAs and the benzodiazepines. For the treatment of PTSD, the alpha-blocker prazosin and antipsychotics reduced symptom severity, and the alpha-blocker prazosin and the tricyclic antidepressant amitriptyline improved number of responders. Overall, SSRIs were less well tolerated than placebo in both reviews (SAD Review: k = 5131, RR 2.59; 95% CI 1.97 to 3.39, N = 5131; PTSD Review: (k = 15, RR 1.41; 95% CI 1.07 to 1.87, N = 2493), but there were low absolute rates of withdrawal compared to placebo (16% and 14%, respectively). There were no significant differences in dropouts due to any cause in both reviews for the SSRI intervention arms (SAD Review: k = 26, RR 1.01; 95% CI 0.90 to 1.14, N = 5208; ; PTSD Review: k = 21, RR 1.13; 95% CI 0.93 to 1.38, N = 3206). Twenty NMAs (i.e. investigating depressive disorder, GAD, SAD, PTSD and OCD) were found in answering aim three, and antidepressants were found to be the most efficacious and tolerable agents for these disorders based on rankings (45% of NMAs) or statistical significance (55% of NMAs). The quality of the reporting of each NMA was high. Seventy percent of the NMAs included a network diagram and 75% of the included NMAs assessed consistency, made use of a random effects model, provided information on the model used to fit the data and adjusted for covariates. The review also revealed that few NMAs reported rankings of treatments. The SAD and PTSD NMA provided similar findings to the Cochrane reviews, discussed in aim one. For aim three (the SAD NMA), the SSRI paroxetine was significantly more effective than placebo in reducing the number of responders (odds ratio (OR) 2.64; CI 1.97 to 3.54) and anxiety symptoms (mean difference (MD) -15.89; CI -29.94 to -1.84) yet performed worse in comparison to placebo for dropouts due to adverse events. Most of the medications (i.e.12 out of 19 comparisons) reported a decrease in dropout rates relative to placebo, but no statistically significant difference was found. There was also evidence that venlafaxine is efficacious in treating SAD symptoms. According to the rankings of individual treatments olanzapine performed better than the rest of the treatments in terms of treatment efficacy and buspirone for dropouts due to any cause. Bromazepam performed well in treating the number of responders due to adverse events. Similarly, for the PTSD NMA, paroxetine was also effective in the treatment of PTSD symptoms (MD -15.89; CI -29.94 to -1.84). Evidence was also observed for phenelzine, desipramine and risperidone for the treatment of PTSD symptoms. Mirtazapine yielded a relatively high rank for efficacy, but the respective value for acceptability was not among the best treatments. Most evidence from both NMAs was associated with low to very low-quality evidence. Conclusion Different meta-analytic approaches are useful in presenting, synthesising, and reporting data. The evidence discussed here suggest that SSRIs are effective in the treatment and reduction of SAD and PTSD symptoms, even though the tolerability of SSRIs was lower than placebo for each disorder. It is noteworthy that similar estimates were found across the different approaches to synthesising data and across the different patient groups (i.e. SAD and PTSD). In addition, the NMAs found in this dissertation show high quality of reporting and that study limitations do not impact on the network estimate. The quality of reporting of individual RCTs included across the review however remain low, and so additional research is needed in this area. common metal disorders medication network meta-analyses NMAs pharmacotherapy posttraumatic stre
4	Reduced-Dimension Hierarchical Statistical Models for Spatial and Spatio-Temporal Data Kang, Lei January 2009 (has links) No description available. Statistics Aerosol optical depth (AOD) Fixed Rank Filtering (FRF) Fixed Rank Kriging (FRK) Givens angles regional climate models (RCMs)
5	The Rtg1 and Rtg3 proteins are novel transcription factors regulated by the yeast hog1 mapk upon osmotic stress Noriega Esteban, Núria 27 February 2009 (has links) La adaptación de la levadura Saccharomyces cerevisiae a condiciones de alta osmolaridad está mediada por la vía de HOG ((high-osmolarity glycerol). La activación de esta vía induce una serie de respuestas que van a permitir la supervivencia celular en respuesta a estrés. La regulación génica constituye una respuesta clave para dicha supervivencia. Se han descrito cinco factores de transcripción regulados por Hog1 en respuesta a estrés osmótico. Sin embargo, éstos no pueden explicar la totalidad de los genes regulados por la MAPK Hog1. En el presente trabajo describimos cómo el complejo transcripcional formado por las proteínas Rtg1 y Rtg3 regula, a través de la quinasa Hog1, la expresión de un conjunto específico de genes. Hog1 fosforila Rtg1 y Rtg3, aunque ninguna de estas fosforilaciones son esenciales para regulación transcripcional en respuesta a estrés. Este trabajo también muestra cómo la deleción de proteínas RTG provoca osmosensibilidad celular, lo que indica que la integridad de la vía de RTG es esencial para la supervivencia celular frente a un estrés osmótico. / In Saccharomyces cerevisiae the adaptation to high osmolarity is mediated by the HOG (high-osmolarity glycerol) pathway, which elicits different cellular responses required for cell survival upon osmostress. Regulation of gene expression is a major adaptative response required for cell survival in response to osmotic stress. At least five transcription factors have been reported to be controlled by the Hog1 MAPK. However, they cannot account for the regulation of all of the genes under the control of the Hog1 MAPK. Here we show that the Rtg1/3 transcriptional complex regulates the expression of specific genes upon osmostress in a Hog1-dependent manner. Hog1 phosphorylates both Rtg1 and Rtg3 proteins. However, none of these phosphorylations are essential for the transcriptional regulation upon osmostress. Here we also show that the deletion of RTG proteins leads to osmosensitivity at high osmolarity, suggesting that the RTG-pathway integrity is essential for cell survival upon stress. OD: optical density NAD+: nicotinamide adenine dinucleotide MAPK: mitogen activated protein kinase HOG: high osmolarity glycerol ERC: extrachromosomal rDNA circles CDK: cyclin dependent kinase DNA: desoxirribobucleic acid ATP: adenosine triphosphate AMP: adenosine monophosphate TOR: Diana de la rapamicina STRE element de resposta a l'estrés ROS: especies reactives de l'oygen rDNA: DNA risbosomal OD: densitat òptica NAD+: nicotinàmida adenina dinucleòtid HOG: osmolaritat elevada de glicerol rDNA: risbosomal DNA ERC: cercle d'rDNA extracromosòmic DNA: àcid desoxirriblonucleic CDK: Kinassa dependent de ciclines ATP: trifosfat d'adenosina AMP: monofosfat d'adenosina ROS: reactive oxygen species SAPK: stress activated protein kinase STRE: stress response element TOR: target of rapamycin 575 58
6	SCF cdc4 regulates msn2 and msn4 dependent gene expression to counteract hog1 induced lethality Vendrell Arasa, Alexandre 16 January 2009 (has links) L'activació sostinguda de Hog1 porta a una inhibició del creixement cel·lular. En aquest treball, hem observat que el fenotip de letalitat causat per l'activació sostinguda de Hog1 és parcialment inhibida per la mutació del complexe SCFCDC4. La inhibició de la mort causada per l'activació sostinguda de Hog1 depèn de la via d'extensió de la vida. Quan Hog1 s'activa de manera sostinguda, la mutació al complexe SCFCDC4 fa que augmenti l'expressió gènica depenent de Msn2 i Msn4 que condueix a una sobreexpressió del gen PNC1 i a una hiperactivació de la deacetilassa Sir2. La hiperactivació de Sir2 és capaç d'inhibir la mort causada per l'activació sostinguda de Hog1. També hem observat que la mort cel·lular causada per l'activació sostinguda de Hog1 és deguda a una inducció d'apoptosi. L'apoptosi induïda per Hog1 és inhibida per la mutació al complexe SCFCDC4. Per tant, la via d'extensió de la vida és capaç de prevenir l'apoptosi a través d'un mecanisme desconegut. / Sustained Hog1 activation leads to an inhibition of cell growth. In this work, we have observed that the lethal phenotype caused by sustained Hog1 activation is prevented by SCFCDC4 mutants. The prevention of Hog1-induced cell death by SCFCDC4 mutation depends on the lifespan extension pathway. Upon sustained Hog1 activation, SCFCDC4 mutation increases Msn2 and Msn4 dependent gene expression that leads to a PNC1 overexpression and a Sir2 deacetylase hyperactivation. Then, hyperactivation of Sir2 is able to prevent cell death caused by sustained Hog1 activation. We have also observed that cell death upon sustained Hog1 activation is due to an induction of apoptosis. The apoptosis induced by Hog1 is decreased by SCFCDC4 mutation. Therefore, lifespan extension pathway is able to prevent apoptosis by an unknown mechanism. STRE: stress response element TOR: target of rapamycin SAPK: stress activated protein kinase ROS: reactive oxygen species PCD: programmed cell death rDNA: risbosomal DNA PAK: p21 activated kinase NAM: nicotinamide OD: optical density MEF2C: myocyte enhancer factor 2C NAD+: nicotinamide adenine dinucleotide MAPK: mitogen activated protein kinase SRF from homo sapiens agamous fromaArabidopsis thaliana saccharomyces cerevisiae IAP: inhibitor of apoptosis proteins HOG: high osmolarity glycerol FACS: fluorescent-activated cell sorting ERC: extrachromosomal rDNA circles DUBs: deubiquitinases CR: caloric restriction DNA: desoxirribobucleic acid CDK: cyclin dependent kinase ATP: adenosine triphosphate AMP: adenosine monophosphate AIF: apoptosis-inducing factor TOR: Diana de la rapamicina STRE element de resposta a l'estrés ROS: especies reactives de l'oygen rDNA: DNA risbosomal PCD: mort cel·lular programada PAK: kinassa activada per p21 OD: densitat òptica NAM: nicotinàmida NAD+: nicotinàmida adenina dinucleòtid MEF2C: factor 2C activador del miócits i SRF d'Homo sapiens del rèptil Antirrhinum majus AGAMOUS d'Arabidopsis thaliana DEFICIENS Saccharomyces cerevisiae IAP: inhibidor de proteins d'apoptosi HOG: Osmolaritat elevada de glicerol ERC: cercle d'rDNA extracromosòmic DUB: deubiquitinassa DNA: Àcid desoxirriblonucleic CR: restricció calòrica CDK: kinassa dependent de ciclines ATP: trifosfat d'adenosina AMP: monofosfat d'adenosina AIF: factor inductor d'apoptosi 576

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