Global ETD Search

301	L’effet d’une potentialisation cholinergique sur la régionalisation et la synchronisation corticale d’un conditionnement visuel Laliberté, Guillaume 12 1900 (has links) Cette thèse démontre qu’une potentialisation cholinergique durant un conditionnement visuel typique permet de raffiner la réponse et la connectivité des neurones des aires corticales visuelles ainsi que des aires associatives supérieures via un phénomène plastique. Afin de déterminer cet effet sur un conditionnement visuel monoculaire sur la réponse corticale, nous avons utilisé un système d’imagerie calcique à large champ sur des souris adultes exprimant le rapporteur calcique GCaMP6s. La potentialisation cholinergique était causée par l’administration de donepezil (DPZ), un inhibiteur de l’acétylcholinestérase qui dégrade l’acétylcholine. Cette technique, possédant de bonnes résolutions spatiale et temporelle, a permis l’observation de l’activité neuronale dans les couches supra granulaires du cortex visuel primaire (V1), des aires secondaires (A, AL, AM, LM, PM, RL) ainsi que dans le cortex retrosplénial (RSC). Il a été alors possible de mesurer les modifications d’activité neuronale de ces aires au repos et lors de la présentation de stimulations visuelles, composées de réseaux sinusoïdaux d’orientation et de contraste varié. La réponse corticale des animaux naïfs est similaire en matière d’amplitude et de sensibilité au contraste pour chacune des orientations de stimulations visuelles présentées. Le conditionnement visuel accompagné de l’administration de DPZ diminue significativement la réponse neuronale évoquée par le stimulus conditionné dans la majorité des aires observés alors qu’il ne modifie pas la réponse à la stimulation non conditionnée. Cet effet n’est pas présent sans potentialisation cholinergique. Il est intéressant de noter qu’un effet sur la corrélation d’activation est observé exclusivement dans les aires de la voie visuelle ventrale. Finalement, le conditionnement monoculaire diminue la corrélation au repos entre les aires visuelles monoculaire et binoculaire de chacun des hémisphères, un effet qui disparaît lors de l’administration du DPZ durant le conditionnement. En conclusion, nos résultats démontrent une diminution de l’amplitude et de l’étalement de la réponse corticale dans les couches supra-granulaires de PM et de V1 en réponse à notre traitement. Nous suggérons que ces résultats démontrent une diminution de la réponse excitatrice causée par l’augmentation de l’activité inhibitrice en réponse à la stimulation conditionnée. / The cholinergic system of the basal forebrain modulates the visual cortex and enhances visual acuity and discrimination when activated during visual conditioning. As wide-field calcium imaging provides cortical maps with a fine regional and temporal resolution, we used this technique to determine the effects of the cholinergic potentiation of visual conditioning on cortical activity and connectivity in the visual cortex and higher associative areas. Mesoscopic calcium imaging was performed in head-fixed GCaMP6s adult mice during resting state or monocular presentation of conditioned (0.03 cpd, 30°, 100% contrast) or non-conditioned 1Hz-drifting gratings (30°, 50 and 75% contrast; 90°, 50, 75 and 100% contrast), before and after conditioning. The conditioned stimulus was presented 10 min daily for a week. Donepezil (DPZ, 0.3 mg/kg, s.c.), a cholinesterase inhibitor that potentiates cholinergic transmission, or saline were injected prior to each conditioning session and compared to a sham-conditioned group. Cortical maps were established, then amplitude, duration, and latency of the peak response, as well as size of activation were measured in the primary visual cortex (V1), secondary visual areas (AL, A, AM, PM, LM, RL), the retrosplenial cortex (RSC) , and higher cortical areas. Visual stimulation increased calcium signaling in all primary and secondary visual areas, but no other cortices (except RSC). The cortical responses were sensitive to contrast but not to grating orientation. There were no significant effects of sham-conditioning or conditioning alone, but DPZ treatment during conditioning significantly decreased the evoked neuronal activity response for the conditioned stimulus in V1, AL, PM, and LM. The size of activated area and signal-to-noise ratio were affected in some cortical areas. There was no effect for the non-conditioned stimuli. Interestingly, signal correlation appeared only between V1 and the ventral visual pathway and RSC and was decreased by DPZ administration. The resting state activity was slightly correlated and rarely affected by treatments, except between binocular and monocular V1 in both hemispheres. In conclusion, despite the previously observed enhancement of the cortical response of layer 4 after visual conditioning with cholinergic potentiation, mesoscale cortical calcium imaging showed that cholinergic potentiation diminished the cortical activation in layer 2/3 and sharpened the responses to the conditioned visual stimulus in V1 and PM, via a layer-dependent effect. Potentialisation cholinergique Imagerie calcique à larges champs Conditionnement visuel Inhibiteur de l’acétylcholinestérase Cortex visuel Cholinergic potentiation Mesoscale calcium imaging Visual conditioning Acetylcholinesterase inhibitors Visual cortex
302	Age-Related Differences in In-vitro Sensitivity to Inhibition of Human Red Blood Cell Acetylcholinesterase and Plasma Butyrylcholinesterase by the Cholinesterase Inhibitors Physostigmine (PHYS), Pyridostigmine (PYR), Donepezil (DON) and Galantamine (GAL) Lee, David 31 July 2009 (has links) Alzheimer’s disease (AD) is a chronic, progressive neurodegenerative disorder, characterized clinically by a progressive loss of memory, cognitive function, ability to care for oneself and psychiatric symptoms. First-line agents for the treatment of AD are ChE inhibitors (DON, GAL), whose modest clinical efficacy and the high incidence of dose-limiting toxicities limit their clinical utility. In addition to AD, ChE inhibitors (PYR) are used for other medical conditions, such as myasthenia gravis (MG). Furthermore, ChE inhibitors (PYR) are used by military personnel prophylactically if impending exposure to chemical warfare agents, e.g., soman, is suspected. The purpose of this research project was to understand the effect of age on the in-vitro sensitivity of ChE inhibitors in human RBCs and plasma. Understanding possible covariates, such as age and gender, may assist in optimizing dosing regimens of ChE inhibitors and/or developing newer ChE inhibitors with better adverse effect profiles. Plasma PHYS concentrations were measured by a validated HPLC-FD method. RBC AChE activity and plasma BuChE activity were measured by a modified Ellman’s colorimetric method using the model substrates, acetylthiocholine and butyrylthiocholine, respectively. The kinetics of RBC and plasma ChE activity followed Michaelis-Menten kinetics. Acetylthiocholine was found to be a nonselective substrate (RBC AChE Km = 73 μM; plasma BuChE Km = 117 μM); while butyrylthiocholine was a selective substrate for plasma BuChE (RBC AChE Km = 130,000 μM; plasma BuChE Km = 72 μM). For the following studies, RBC AChE activity was measured using acetylthiocholine as the substrate and plasma BuChE activity was measured using butyrylthiocholine as the substrate. This research project was performed in two parts: First, mechanistic studies of PHYS, PYR, DON and GAL, explored and determined the mechanism of in-vitro inhibition of RBC AChE and plasma BuChE inhibition, as well as the in-vitro degradation of PHYS in human whole blood, plasma and RBC. PHYS was rapidly degraded in human whole blood, RBC and plasma and followed Michaelis-Menten kinetics but its degradation clearance - scaled to whole blood clearance - was only predicted to account for 4-6% (i.e., 195-261 ml/min) of the reported total body clearance for PHYS (4500 ml/min). RBCs were responsible for 60% of the whole blood clearance while plasma accounted for 40% of the whole blood clearance. Inhibition results indicated that both PHYS and PYR were nonselective and rapid suicide ChE inactivators. PYR inactivated RBC AChE more rapidly at low concentrations and inactivated plasma BuChE more rapidly at high concentrations, but inactivated both more rapidly than PHYS. PHYS was a more potent inactivator than PYR with a Ki for RBC AChE of 0.011 μM and 0.063 μM, respectively, and 0.023 μM and 0.036 μM, respectively for plasma BuChE. DON was found to be a noncompetitive inhibitor for RBC AChE (Ki,noncomp = 114 μM), but a competitive inhibitor for plasma BuChE (Ki,comp = 213 μM). GAL was found to be a competitive inhibitor for both RBC AChE (Ki,comp = 66 μM) and plasma BuChE (Ki,comp = 358 μM). The second part involved a clinical study with ten young and nine elderly healthy subjects, balanced for gender, who donated blood for an in-vitro study in order to assess any age- and gender-related differences in in-vitro sensitivity to RBC AChE and plasma BuChE inhibition to all four ChE inhibitors. Elderly adults were found to be 2-3-fold less sensitive compared to the young adults for PHYS (BuChE Ki,pss; 0.010 and 0.015 μM, young and elderly, respectively) and PYR (AChE Ki,pss; 0.12 and 0.25 μM, young and elderly, respectively) only, while neither DON nor GAL showed any age-related differences in sensitivity. The observed differences for PHYS and PYR may be due to kinetic differences in ChE inactivation between young and aged adults, rather then a difference in binding affinities/potencies. These carbamate ChE inhibitors, presumably, have a slower decarbamoylation rate in younger adults than elderly adults, which leads to the observed difference in in-vitro sensitivity. The above in-vitro results were consistent with results of a meta-analysis: In a study by Knapp et al. (1991), young males (n=6), receiving 18 mg, 24 mg and 30 mg PHYS tablets, showed similar ex-vivo plasma BuChE sensitivity to (28 %/(ng/ml)) as the in-vitro sensitivity for young males in the current study (33 %/(ng/ml)). On the other hand, in the study by Men (2004), elderly males (n=8) and females (n=8), receiving 6.7 μg/kg PHYS as 30-minute infusion, showed similar ex-vivo RBC AChE sensitivity (12 %/(ng/ml)) as the in-vitro sensitivity for elderly subjects in the current study (9.7 %/(ng/ml)). This suggests that in-vitro measurement of ChE sensitivity is predictive of ex-vivo sensitivity in clinical studies. The study results suggest that elderly adults may require a 2-3-fold higher blood concentration than young adults to achieve the same ChE inhibition. This may explain why for epistigmine, an investigational carbamate ChE inhibitor for the treatment of AD, the maximum tolerated dose observed in young adults (40 mg single dose) was lower than for older adults (90 mg/day). Higher sensitivity in young adults prevented further dose escalation, while all elderly subjects tolerated higher doses. This research may have implications for other diseases and conditions, most notably MG and as a prophylaxis of nerve gases poisoning. As patients with MG age, they may become less sensitive to PYR, the most common symptomatic treatment for MG, and an increase in dose may be required. Further, older military personnel assigned to receive PYR, may require increased doses to achieve the targeted 10% RBC AChE inhibition, necessary to protect against nerve gas poisoning. acetylcholinesterase butyrylcholinesterase cholinesterase inhibitors aging in-vitro sensitivity physostigmine galantamine donepezil pyridostigmine red blood cell plasma age-related suicide inactivator competitive inhibitors noncompetitive inhibitors mechanism-based inhibitor inhibitor models enzyme kinetics inhibitor kinetics Alzheimer’s disease myathenia gravis Medicine and Health Sciences Pharmacy and Pharmaceutical Sciences
303	Screening of traditional Chinese medicine for anti-Alzheimer's disease drugs. January 2005 (has links) by Wong Kin Kwan Kelvin. / Thesis submitted in: September 2004. / Thesis (M.Phil.)--Chinese University of Hong Kong, 2005. / Includes bibliographical references (leaves 91-101). / Abstracts in English and Chinese. / Acknowledgements --- p.i / Abstract --- p.ii / 摘要 --- p.iv / Abbreviations --- p.x / List of Figures --- p.xiii / List of Tables --- p.xiv / Chapter Chapter 1 --- Intorduction --- p.1 / Chapter 1.1 --- Alzheimer，s disease --- p.1 / Chapter 1.2 --- Histopathological features --- p.1 / Chapter 1.3 --- Tau protein pathology and AD --- p.4 / Chapter 1.4 --- Tau protein kinase I (TPKI)- GSK-3β --- p.6 / Chapter 1.5 --- Tau protein kinase II (TPKII)- Cyclin dependent kinase 5 (Cdk5) --- p.8 / Chapter 1.6 --- Available treatment --- p.9 / Chapter 1.7 --- Objectives of the present study --- p.12 / Chapter Chapter 2 --- Screening for GSK-3p inhibitors from Traditional Chinese Medicine (TCM) --- p.13 / Chapter 2.1 --- Introduction --- p.13 / Chapter 2.1.1 --- Phosphorylation of tau in AD --- p.13 / Chapter 2.1.2 --- Gsk-3p inhibitors --- p.14 / Chapter 2.1.3 --- Screening of GSK-3β inhibitor from TCM --- p.16 / Chapter 2.2 --- Material and Methods --- p.18 / Chapter 2.2.1 --- Preparation of extracts and fractions (AOF1-5) --- p.18 / Chapter 2.2.2 --- General cell culture techniques --- p.21 / Chapter 2.2.3 --- "3-(4,5-dimethyltiazoI-2-yl)-2, 5-diphenyl-tetrazolium (MTT) assay of AOF" --- p.23 / Chapter 2.2.4 --- Recombinant DNA techniques --- p.23 / Chapter 2.2.5 --- Transfection of GSK-3β and tau cDNA into COS7 cells --- p.28 / Chapter 2.2.6 --- Extraction of total proteins from culture cells --- p.28 / Chapter 2.2.7 --- Quantitation of protein by the Bradford method --- p.29 / Chapter 2.2.8 --- Protein separation by sodium dodecylsulphate polyacrylamide gel electrophoresis (SDS-PAGE) --- p.29 / Chapter 2.2.9 --- Western blot analysis --- p.31 / Chapter 2.2.10 --- GSK-3β kinase assay --- p.32 / Chapter 2.2.11 --- Determination of lithium content by atomic adsorption spectrophotometry --- p.34 / Chapter 2.3 --- Results --- p.35 / Chapter 2.3.1 --- Establishment of a co-transfected cell model for GSK-3β induced tau hyperphosphorylation --- p.35 / Chapter 2.3.2 --- Preliminary screening results of aqueous and ethanol extracts (AOF1 and AOF2) --- p.37 / Chapter 2.3.3 --- Ethanol extract of AOF inhibits GSK-3p induced tau phosphorylation in COS-7 cells --- p.40 / Chapter 2.3.5 --- Effect of the essential oils of AOF on GSK-3P induced tau phosphorylation --- p.46 / Chapter 2.3.6 --- The effect of AOF essential oil on GSK-3P activity in COS7 --- p.50 / Chapter 2.3.7 --- Lithium content of AOF extracts --- p.52 / Chapter 2.4 --- Discussion --- p.54 / Chapter Chapter 4 --- Evaluation of the in vivo efficacy of cryptotenshinone (CT) in Morris Water Maze Task (WMT) --- p.59 / Chapter 4.1 --- Introduction --- p.59 / Chapter 4.1.1 --- Involvement of Cholinergic system in cognitive dysfunction in AD --- p.59 / Chapter 4.1.2 --- Animal model for Alzheimer's disease --- p.60 / Chapter 4.1.3 --- Morris Watermaze Task (WMT) --- p.61 / Chapter 4.2 --- MATERIAL AND METHODS --- p.64 / Chapter 4.2.1 --- Morris Water maze setup --- p.64 / Chapter 4.2.2 --- Animal model --- p.66 / Chapter 4.2.3 --- Drug preparation --- p.67 / Chapter 4.2.4 --- Toxicity test of CT --- p.67 / Chapter 4.2.5 --- Water maze task (WMT) --- p.68 / Chapter 4.2.6 --- Visual acuity test --- p.73 / Chapter 4.3 --- RESULTS --- p.74 / Chapter 4.3.1 --- Chronic crytotanshinone treatment does not cause hepatic damages to the mice --- p.74 / Chapter 4.3.2 --- Training Session --- p.76 / Chapter 4.4 --- DISCUSSION --- p.85 / Chapter Chapter 5 --- General Discussion and Future Directions --- p.87 / Chapter 5.1 --- "AOF, the potential GSK-3 inhibitor" --- p.87 / Chapter 5.2 --- CT´ؤthe AChEI --- p.88 / References --- p.91 / Appendix --- p.102 / Chapter A1 --- Reagents for SDS-PAGE --- p.103 / Chapter A3 --- Solution components provided by QIAGEN Plasmid Maxipreps kit --- p.108 / Chapter A4 --- Reagents and medium for cell culture --- p.109 / Chapter A5 --- Reagents for kinase assay --- p.110 / Chapter A6 --- Raw data of figures --- p.112 / Chapter A7 --- Plasmid map of PCI-neo --- p.119 Glycogen synthase kinase-3 Glycogen synthase kinase-3--Inhibitors Acetylcholinesterase--Inhibitors Plant extracts Medicine, Chinese Alzheimer's disease--Chemotherapy Cholinesterase Inhibitors Protein-Serine-Threonine Kinases Medicine, Chinese Traditional Alzheimer Disease--drug therapy
304	Fitohemijska karakterizacija i biohemijska ispitivanja plodova vrsta roda Sorbus L. 1753 (Rosaceae, Maloideae) kao izvora prirodnih nutraceutika / Phytochemical characterization and biochemical activity of fruits of genus Sorbus L. 1753 (Rosaceae, Maloideae) as natural source of nutraceutics Mrkonjić Zorica 02 October 2017 (has links) <p>   Cilj ove doktorske disertacije predstavljao je ispitivanje fitohemijskog sastava i biolo&scaron;ke aktivnosti vodenih i metanolnih ekstrakata svežih i suvih plodova, kao  i pekmeza  pripremljenog  po tradicionalnoj recepturi od plodova  četiri (od kojih se jedna javlja u dve forme)  samonike  vrsta  roda  <em>Sorbus</em>  L.:  S.<em> aucuparia</em>, S.<em> domestica</em>, S. <em>torminalis</em>  f.  t<em>orminalis</em>, S. <em>torminalis</em>  f. <em>semitorminalis</em>  i  S. intermedia Ispitivanje fitohemijskog sastava obuhvatalo je LC-MS/MS analizu  44 odabrana fenolna jedinjenja  i  hinske kiseline (organska  kiselina). Takođe, spektrofotometrijski je  određen  sadržaj  ukupnih fenolnih i flavonoidnih jedinjenja, kao i  sadržaj askorbinske kiseline. Evaluacija biolo&scaron;ke aktivnosti obuhvatala je  <em>in vitro  </em>ispitivanja antioksidantne aktivnosti, kao i ispitivanje uticaja ekstrakata odabranih vrsta  roda <em> Sorbus</em>  na aktivnost enzima acetilholinesteraze, antimikrobni, kao i antiproliferativni potencijal.</p><p>   Sumiranjem dobijenih rezultata može se zaključiti da sveži i suvi plodovi ispitivanih vrsta  <em>Sorbus</em>,  kao i  pekmezi  predstavljaju  umeren izvor  fenolnih jedinjenja.  Kao najzastupljenije fenolne kiseline izdvojile su se protokatehinska i  ferulna, a među flavonoidima amentoflavon i kvercetin-3<em>-O-</em>glukozid.  Pored toga, hinska kiselina je zabeležena u značajnoj količini u svim analiziranim ekstraktima.</p><p>    Ekstrakti ispitivanih vrsta pokazali su  umeren  antioksidantni potencijal koji se ogleda u njihovoj sposobnosti neutralizacije nekoliko radikalskih vrsta, redukcionom potencijalu i sposobnosti inhibicije lipidne peroksidacije.  Ispitivanjem uticaja ekstrakata odabranih vrsta <em> Sorbus</em>  naaktivnost  enzima  acetilholinesteraze  dokazana  je  jedino  umerena aktivnost  ekstrakata vrste  <em>S. aucuparia</em>.  Takođe, ispitivani ekstrakti  vrsta roda  <em>Sorbus</em>  ispoljili su umerenu  antimikrobnu  aktivnost u pogledu inhibicije  rasta Gram pozitivne bakterije,  <em>Staphylococcus aureus</em>, i Gram negativne bakterije, <em> Escherichia coli</em>.  Vodeni i metanolni ekstrakti svežih i suvih plodova vrste  <em>S. aucuparia</em>  pokazali su umeren i inhibitorni potencijal prema rastu tumorskih (HeLa, MCF7, HT-29), ali i netumorskih ćelijskih linija (MRC-5).  Rezultati dobijeni u ovoj doktorskoj distertaciji  ukazuju na značajan  biopotencijal plodova i pekmeza  ispitivanih vrsta <em> Sorbus</em>  i ukazuju na njihovu primenu u prehrambenoj industriji u vidu funkcionalne hrane.</p> / <p>The aim of presented  PhD  thesis was investigation of phytochemical composition and biological activity of water and methanol extracts of fresh and air-dried  fruits, as   well  as  jam,  made according to traditional recipe,  of fruits  of four  (one of them occurs in two forms)  wild growing  <em>Sorbus</em>  L. species:  <em>S. aucuparia, S. domestica, S. torminalis  f. torminalis, S. torminalis f. semitorminalis</em> and <em>S. intermedia</em>. Examination of phytochemical composition included LC-MS/MS analysis of 44 selected phenolic compounds  and  quinic acid (organic acid).  Also, total phenolic and flavonoid contents, as well as  ascorbic acid  content,  were determined spectrophotometrically. Biological activity evaluation of extracts of<em>  Sorbus</em>  species included <em> in vitro </em> investigation of antioxidant, anti-acetylcholinesterase, antimicrobial  and cytotoxic activity.</p><p>   According to obtained results, fresh and air-dried  fruits, as well as jam  present  moderate  source of phenolic compounds. Amongs examined phenolic acids protocatechuic  and ferulic acids were the most abundant, and amongs investigated flavonoids amentoflavone and quercetin-3-<em>O</em>-glucoside wete present in noticeable amount.  Furthermore, high concentration of quinic acid was present in all examined extracts.</p><p>   Extracts of all examined species showed  moderate   antioxidant activity in terms of radical scavenging ability, reduction potential and inhibition of lipid peroxidation.  Also, investigation of  anti-acetylcholinesterase activity revealed moderate activity only of extracts of <em>S. aucuparia</em>. Furthermore, examinated extracts of<em> Sorbus</em> species showedmoderate antimicrobial activity against Gram–positive bacteria, <em>Staphylococcus aureus</em>, and Gram-negative bacteria, <em> Escherichia coli</em>.  In addition, water  and methanol  extracts of fresh and air-dried  fruits of <em> S.aucuparia</em>  showed  inhibitory activity toward  tumor (HeLa, MCF7, HT-29), and also non-tumor (MRC-5) cell lines. Presented results indicate significant  biopotential of examined  fruits of  <em>Sorbus </em> species  and  support their use in food industry as functional food.</p>
305	Toxicidad volátil de monoterpenoides y mecanismos bioquímicos en insectos plaga del arroz almacenado López Belchí, María Dolores 23 October 2008 (has links) Algunas plagas causan daños importantes en productos y granos almacenados, lo cual conlleva consecuentemente a pérdidas de producción y calidad en estos productos.Las principales plagas del arroz almacenado en España son, Sitophilus oryzae L. (Coleoptera Curculionidae), Rhyzopertha dominica Fabricius (Coleoptera: Bostrichidae), y Cryptolestes pusillus Schönherr (Coleoptera: Cucujidae). Las dos primeras son plagas primarias que atacan directamente el grano y resultan bastante destructivas debido a que sus larvas se alimentan y desarrollan dentro de él. C.pusillus es, sin embargo, una plaga secundaria que se beneficia de granos que ya están dañados y rotos.Actualmente, el uso de fumigantes e insecticidas de síntesis sigue siendo el principal método de lucha para controlar las plagas de almacén, si bien recientemente (dadas las continuas restricciones al uso de agroquímicos) existe un gran interés en la utilización de otras alternativas tales como el control biológico, el almacenamiento a bajas temperaturas, o los tratamientos con calor entre otros.Igualmente muchos productos obtenidos principalmente de plantas y que derivan del metabolismo secundario de las mismas ofrecen una fuente de bioinsecticidas que podrían representar una alternativa ecológica frente a los insecticidas de síntesis ya que su uso masivo e indiscriminado ha ocasionado problemas tales como la aparición de resistencias en determinadas especies de insectos frente a diferentes materias activas, desequilibrios ecológicos y problemas medioambientales sin olvidar el riesgo que entrañan para la salud humana.Con este trabajo se ha pretendido estudiar la actividad plaguicida de los aceites esenciales extraídos de tres plantas: Coriandrum sativum L. (Umbelliferae), Carum carvii L. (Umbelliferae) y Ocimum basilicum L. (Labiatae) y su posterior fraccionamiento para identificar dentro de estos aceites los compuestos químicos responsables de esta actividad insecticida sobre tres plagas de almacén de arroz (S. oryzae, R.dominica y C.pusillus).Del estudio de estos monoterpenoides, linalol, S-carvona y estragol resultaron tener una alta actividad insecticida sobre estas plagas. Sin embargo el E-anetol fue más selectivo para R.dominica y C.pusillus, así como el limoneno, γ-terpineno, geraniol y eucaliptol sólo resultaron activos frente a C.pusillus.Algunos monoterpenoides podrían actuar de sinergistas potenciando la actividad de otros, como podría ser el caso del alcanfor, acetato de geranilo y E-anetol con linalol en R.dominica y C.pusillus, o el caso del metoxicinamaldehido, p-anisaldehido y linalol que pueden tener efecto sinergista sobre el estragol.Este trabajo también abarcó el estudio de un posible modo de acción de estos monoterpenoides, la inhibición de la acetilcolinesterasa, para alcanzar un mayor entendimiento del comportamiento de estas sustancias en el interior del insecto.Así se pudo observar como la mayoría de monoterpenoides estudiados inhibían en cierta medida esta enzima, siendo fenchona, S-carvona y linalol los monoterpenoides que mayor inhibición originaron.Del mismo modo se observó como fenchona, γ-terpineno, geraniol y linalol inhibían competitivamente la acetilcolinesterasa, mientras que S-carvona, estragol y alcanfor producían una inhibición mixta para esta enzima.Sin embargo no se observó inhibición de la acetilcolinesterasa por parte del E-anetol a las concentraciones de monoterpenoides ensayadas.Para completar este trabajo se examinó de igual forma la capacidad que tenían estos bioinsecticidas de generar resistencia en estas tres plagas así como el mecanismo de resistencia implicado en el desarrollo de este proceso. Para ello se fueron seleccionando las poblaciones de insectos mediante la aplicación de los diferentes monoterpenoides a dosis crecientes durante 7 generaciones. De este modo se pudo calcular el factor de resistencia en cada una de las plagas y para cada uno de los monoterpenoides comparando las concentraciones letales 50 de las poblaciones seleccionadas con las poblaciones iniciales (sensibles).A continuación se analizaron tres posibles sistemas de detoxificación enzimáticos gracias al uso de sinergistas para estudiar el mecanismo de resistencia que podría estar involucrado.De tal forma se observó como estos monoterpenoides inducían lentamente resistencias resultando ventajosos en un futuro para el control de estas plagas.Esta Tesis ha englobado un estudio íntegro y profundo de estos insecticidas ecológicos desde la extracción de los aceites esenciales, seguido de la identificación de compuestos puros (CG-EM) con actividad insecticida junto con el estudio de un modo de acción de estos insecticidas, la selección de resistencia en las poblaciones de insectos y los posibles mecanismos de resistencia que pudieran estar implicados en este proceso. / Some pests cause serious damage to stored grains and stored products and consequently production and quality losses in these products.The rice weevil, Sitophilus oryzae L. (Coleoptera: Curculionidae), the lesser grain borer, Rhyzopertha dominica Fabricius (Coleoptera: Bostrichidae) and Cryptolestes pusillus Schönherr (Coleoptera: Cucujidae) were the main damaging pests found in stored rice in Spain.S.oryzae and R.dominica are primary pests attacking directly the intact grain and are quite destructive because their larvi feed and develop inside the grain whereas C.pusillus is a secondary pest which benefits from grains previously damaged.At the present time, organic synthetic pesticides are still the main method to control stored grain pests, however, recently (due to restriction in agrochemicals use) there is a great interest in using other altenatives such as biological control, storage at low-temperatures, or heat treatment.Likewise, many products obtained mainly from plants and derived from secondary metabolism have insecticidal activity against insects, such as monoterpenoids, which present a broad variety of bioinsecticide products which could turn out to be an ecologic alternative to synthetic pesticides since the majority of alternative products are not harmful for the human healthy and they become less environmentally damaging, exhibiting a low impact on the environment.In addition, it cannot be ignored the different difficulties related to resistance due to several active compounds from organic pesticides found in some species of insects.With this work, we have considered remarkable to study the insecticide activity of essential oils extracted from three plants: Coriandrum sativum L. (Umbelliferae), Carum carvii L. (Umbelliferae) and Ocimum basilicum L. (Labiatae) and carry out a bioassay-guided fractionation of their essential oils to identify which compounds were responsible for the volatile toxicity shown on three stored rice pests (S. oryzae, R. dominica and C. pusillus).Linalool, S-carvone and estragole turned out to have a high insecticide activity on these pests. Nevertheless E-anetol was more selective to R. dominica and C. pusillus, being only active on C. pusillus limonene, γ-terpinene, geraniol and eucalyptol.Some monoterpenoids were found as synergists, increasing the activity of the other ones, like for instance, camphor, geranyl acetate and E-anethole with linalool in R.dominica and C.pusillus or metoxycinnamaldehyde, p-anysaldehyde and linalool which could activate to estragole.In this work, the inhibition of acetylcholinesterase as a posible mode of action was studied as well, to reach a clear understanding about the action of these products inside the insects.The majority of monoterpenoids inhibited the enzyme acetylcholinesterase being fenchone, S-carvone and linalool the monoterpenoids that produced a higher inhibition.Furthermore, it was observed how fenchone, γ-terpinene, geraniol and linalool showed a competitive inhibition whereas S-carvone, estragole and camphor produced a mixed inhibition for this enzyme. However the enzyme acetylcholinesterase was not inhibited by E-anethole.To finish up this work, the selection for monoterpenoid resistance on these pests as well as the metabolic mechanisms implicated was studied.The resistant strains were selected from susceptible insect populations and survivors were reared separately for each monoterpenoid and successive generations were treated with higher concentrations. These populations were selected until seven times.As a result we could calculate the resistance factor on each pest (comparing lethal concentration 50 values of susceptible and resistant strains).Next, three enzymatic systems detoxifying these monoterpenoids were analysed to study the metabolic mechanism implicated.In this way we could realize that all monoterpenoids induced resistance slowly, concluding that these pesticides will be appropriated to control these pests in the future.This Thesis has concerned a study in depth about ecological insecticides from extraction of essential oils, identification of compounds (GC-MS) with insecticide activity, mode of action and study of resistance and mechanism of insecticide resistance involved in this process. Sitophilus oryzae Rhyzopertha dominica Coriandrum sativum Carum carvii Ocimum basilicum Botanical Insecticides Fenchone E-Anethole Estragole S-Carvone Linalool Acetilcolinesterasa Resistencia a monoterpenoides Coleoptera Cryptolestes pusillus Rhyzopertha dominica Sitophilus oryzae Coriandrum sativum Carum carvii Ocimum basilicum Insecticidas de origen natural Fenchona E-Anetol Estragol S-Carvona : Linalol Cryptolestes pusillus Coleoptera Acetylcholinesterase Monoterpenoid Resistance Química Agrícola 54 577 63 631
306	Novel molecular mechanisms of neuronal and vascular protection in experimental glaucoma Almasieh, Mohammadali 04 1900 (has links) Le glaucome est la deuxième cause de cécité irréversible dans le monde. La perte de vision qui se produit lors du glaucome s’explique par une dégénérescence du nerf optique et une mort progressive et sélective des cellules ganglionnaires de la rétine (CRG). L'hypertension oculaire est un facteur de risque majeur dans le glaucome, mais des défauts du champ visuel continuent à se développer chez un contingent de patients malgré l'administration de médicaments qui abaissent la pression intraoculaire (PIO). Par conséquent, bien que la PIO représente le seul facteur de risque modifiable dans le développement du glaucome, son contrôle ne suffit pas à protéger les CRGs et préserver la fonction visuelle chez de nombreux patients. Dans ce contexte, j'ai avancé l'hypothèse centrale voulant que les stratégies de traitement du glaucome visant à promouvoir la protection structurale et fonctionnelle des CRGs doivent agir sur les mécanismes moléculaires qui conduisent à la mort des ces neurones. Dans la première partie de ma thèse, j'ai caractérisé l'effet neuroprotecteur de la galantamine, un inhibiteur de l'acétylcholinestérase qui est utilisé cliniquement dans le traitement de la maladie d'Alzheimer. Cette étude s’est basée sur l'hypothèse que la galantamine, en modulant l'activité du récepteur de l'acétylcholine, puisse améliorer la survie des CRGs lors du glaucome. Nous avons utilisé un modèle expérimental bien caractérisé d'hypertension oculaire induite par l’administration d'une solution saline hypertonique dans une veine épisclérale de rats Brown Norway. Les résultats de cette étude (Almasieh et al. Cell Death and Disease, 2010) ont démontré que l'administration quotidienne de galantamine améliore de manière significative la survie des corps cellulaires et des axones CRGs. La protection structurelle des CRGs s’accompagne d’une préservation remarquable de la fonction visuelle, évaluée par l'enregistrement des potentiels évoqués visuels (PEV) dans le collicule supérieur, la cible principale des CRGs chez le rongeur. Une autre constatation intéressante de cette étude est la perte substantielle de capillaires rétiniens et la réduction du débit sanguin associé à la perte des CRGs dans le glaucome expérimental. Il est très intéressant que la galantamine ait également favorisé la protection de la microvascularisation et amélioré le débit sanguin rétinien des animaux glaucomateux (Almasieh et al. en préparation). J'ai notamment démontré que les neuro-et vasoprotections médiées par la galantamine se produisent par iv l'activation des récepteurs muscariniques de l'acétylcholine. Dans la deuxième partie de ma thèse, j'ai étudié le rôle du stress oxydatif ainsi que l'utilisation de composés réducteurs pour tester l'hypothèse que le blocage d'une augmentation de superoxyde puisse retarder la mort des CRG lors du glaucome expérimental. J'ai profité d'un composé novateur, un antioxydant à base de phosphineborane (PB1), pour tester sur son effet neuroprotecteur et examiner son mécanisme d'action dans le glaucome expérimental. Les données démontrent que l'administration intraoculaire de PB1 entraîne une protection significative des corps cellulaire et axones des CRGs. Les voies moléculaires conduisant à la survie neuronale médiée par PB1 ont été explorées en déterminant la cascade de signalisation apoptotique en cause. Les résultats démontrent que la survie des CRGs médiée par PB1 ne dépend pas d’une inhibition de signalisation de protéines kinases activées par le stress, y compris ASK1, JNK ou p38. Par contre, PB1 induit une augmentation marquée des niveaux rétiniens de BDNF et une activation en aval de la voie de survie des ERK1 / 2 (Almasieh et al. Journal of Neurochemistry, 2011). En conclusion, les résultats présentés dans cette thèse contribuent à une meilleure compréhension des mécanismes pathologiques qui conduisent à la perte de CRGs dans le glaucome et pourraient fournir des pistes pour la conception de nouvelles stratégies neuroprotectrices et vasoprotectrices pour le traitement et la gestion de cette maladie. / Glaucoma is the second cause of irreversible blindness worldwide. Loss of vision in glaucoma is accompanied by progressive optic nerve degeneration and selective loss of retinal ganglion cells (RGCs). Ocular hypertension is a major risk factor in glaucoma, but visual field defects continue to progress in a large group of patients despite the use of drugs that lower intraocular pressure (IOP). Therefore, although IOP is the sole modifiable risk factor in the development of glaucoma, its regulation is not sufficient to protect RGCs and preserve visual function in many affected patients. To address this issue, I put forward the central hypothesis that effective therapeutic strategies for glaucoma must interfere with molecular mechanisms that lead to RGC death to successfully promote structural and functional protection of these neurons. In the first part of my thesis, I characterized the neuroprotective effect of galantamine, an acetylcholinesterase inhibitor that is clinically used for the treatment of Alzheimer’s disease. The specific hypothesis of this study was that galantamine, by modulating acetylcholine receptor activity, can improve the survival of injured RGCs in glaucoma. A well characterized experimental model of ocular hypertension induced by administration of a hypertonic saline into an episcleral vein of Brown Norway rats was used. The results of this study (Almasieh et al. Cell Death and Disease, 2010) demonstrated that daily administration of galantamine significantly improved the survival of RGC soma and axons in this model. Structural protection of RGCs correlated with substantial preservation of visual function, assessed by recording visual evoked potentials (VEPs) from the superior colliculus, the primary target of RGCs in the rodent brain. An interesting finding during the course of my thesis was that there is a substantial loss of retinal capillaries and a reduction in retinal blood that correlates with RGC loss in experimental glaucoma. Interestingly, galantamine also promoted the protection of the microvasculature and improved retinal blood flow in ocular hypertensive animals (Almasieh et al. in preparation). Importantly, I demonstrated that galantamine-mediated neuro- and vasoprotection occur through activation of muscarinic acetylcholine receptors. In the second part of my thesis, I investigated the role of oxidative stress and the use of reducing compounds to test the hypothesis that blockade of a superoxide burst may delay RGC death in experimental glaucoma. I took advantage of a novel phosphinevi borane based antioxidant compound available to us (PB1) to investigate its neuroprotective effect and mechanism of action in experimental glaucoma. The data demonstrate that intraocular administration of PB1 resulted in significant protection of RGC soma and axons. I also explored the molecular pathways leading to PB1-mediated neuronal survival by analyzing the components of survival and apoptotic signaling pathways involved in this response. My results show that PB1-mediated RGC survival did not correlate with inhibition of stress-activated protein kinase signaling, including ASK1, JNK or p38. Instead, PB1 led to a striking increase in retinal BDNF levels and downstream activation of the pro-survival ERK1/2 pathway (Almasieh et al. Journal of Neurochemistry, 2011). In conclusion, the findings presented in this thesis contribute to a better understanding of the pathological mechanisms underlying RGC loss in glaucoma and might provide insights into the design of novel neuroprotective and vasoprotective strategies for the treatment and management of this disease. Glaucome Cellule ganglionnaire de la rétine Neuroprotection Inhibiteur de l'acétylcholinestérase muscarinique superoxyde microvascularisation rétinienne débit sanguin rétinien Glaucoma Retinal ganglion cell Neuroprotection Acetylcholinesterase inhibitor Muscarinic Superoxide Brain-derived neurotrophic factor Extracellular signalregulated kinase 1/2 Retinal microvasculature Retinal blood flow
307	Μελέτη της νευροπροστατευτικής δράσης του εκχυλίσματος του φυτού Sideritis clandestina subsp. clandestina Βασιλοπούλου, Αικατερίνη 27 December 2010 (has links) "Το τσάι του βουνού" (στο οποίο ανήκουν πολλά είδη του γένους Sideritis) καταναλώνεται παραδοσιακά στην Ελλάδα ως ηρεμιστικό αλλά και ενάντια του κρυολογήματος και αλλεργιών. Η παρούσα μελέτη διερευνά την πιθανή νευροπροστατευτική δράση του ανωτέρω φυτού και εστιάζεται: α) στην επίδραση του αφεψήματος του φυτού Sideritis clandestina subsp. clandestina σε συμπεριφερικές παραμέτρους ενηλίκων μυών (άγχος/φόβος, μνήμη/μάθηση), β) στην επίδραση του αφεψήματος του ανωτέρω φυτού σε βιοχημικές παραμέτρους και πιο συγκεκριμένα στη συγκέντρωση της ανηγμένης γλουταθειόνης, στην υπεροξείδωση λιπιδίων και στην ενεργότητα δυο ισομορφών του ενζύμου της ακετυλοχολινεστεράσης (AChE) και γ) στην in vitro πιθανή αντιχολινεστερασική και αντιαμυλοειδική δράση του υδατικού εκχυλίσματος του φυτού. Το φυτικό αφέψημα σε συγκέντρωση 4% w/v χορηγoόταν καθημερινά σε αρσενικούς Balb-c μύες για περίοδο 40 ημερών. Για την εκτίμηση του άγχους/φόβου χρησιμοποιήθηκε α) η δοκιμασία του Υπερυψωμένου Λαβυρίνθου (χρόνος παραμονής των μυών στους ανοιχτούς βραχίονες ως προς το συνολικό χρόνο παραμονής στους ανοιχτούς και κλειστούς βραχίονες της συσκευής) και β) η δοκιμασία του Θιγμοτακτισμού (τάση παραμονής των μυών πλησίον των τοιχωμάτων του ειδικού κλωβού). Η μνήμη-μάθηση μελετήθηκε με τη δοκιμασία της Παθητικής Αποφυγής η οποία βασίζεται στην παρατήρηση ότι τα πειραματόζωα θα θυμούνται ότι μια συγκεκριμένη αντίδρασή τους θα έχει αρνητικές συνέπειες (εφαρμογή επώδυνου ηλεκτρικού ερεθίσματος στα άκρα). Οι οξειδωτικές/αντιοξειδωτικές ιδιότητες του φυτικού αφεψήματος προσδιορίστηκαν με εκτίμηση α) της συγκέντρωσης του αντιοξειδωτικού δείκτη της ανηγμένης γλουταθειόνης, η οποία στηρίζεται στο σχηματισμό ενός φθορίζοντος συμπλόκου μετά την αντίδραση της ο-φθαλαλδεϋδης με τη γλουταθειόνη και υστιδύλ-ενώσεις και β) τα επίπεδα λιπιδικής υπεροξείδωσης μέσω προσδιορισμού των επιπέδων του οξειδωτικού δείκτη της μηλονικής διαλδεΰδης που στηρίζεται στο σχηματισμό του φθορίζοντος συμπλόκου που δημιουργείται όταν η μηλονική αλδεΰδη αντιδρά με το θειοβαρβιτουρικό οξύ. Η ενεργότητα του ενζύμου της ακετυλοχολινεστεράσης (AChE) τόσο ex vivo όσο και in vitro προσδιορίστηκε με τη χρήση της χρωματομετρικής μεθόδου του Ellman, όπου ως υπόστρωμα του ενζύμου χρησιμοποιήθηκε η ιωδιούχος ακετυλοθειοχολίνη. Κατά τον προσδιορισμό της ενεργότητας του ενζύμου in vitro ως εσωτερικό πρότυπο χρησιμοποιήθηκε η γαλανταμίνη, ένας ισχυρός αναστολέας του ενζύμου. Η πιθανή αντιαμυλοειδκή δράση του φυτικού εκχυλίσματος μελετήθηκε με τη μέθοδο της θειοφλαβίνης-Τ. Τα αποτελέσματα της δοκιμασίας του Υπερυψωμένου Λαβύρινθου έδειξαν ότι ο χρόνος παραμονής στους ανοιχτούς βραχίονες ως προς το συνολικό χρόνο παραμονής στους ανοιχτούς και κλειστούς βραχίονες της συσκευής είναι στατιστικώς σημαντικά αυξημένος για την ομάδα των ζώων που κατανάλωσαν το φυτικό αφέψημα σε σύγκριση με τους μάρτυρες. Από τη δοκιμασία του Θιγμοτακτισμού για την πειραματική ομάδα φάνηκε ότι ο χρόνος θιγμοτακτισμού μειώνεται και ο αριθμός των εισόδων στην κεντρική περιοχή του ανοιχτού πεδίου αυξάνεται για κάθε 5 λεπτά παραμονής (εκ του συνολικού διαστήματος των 30 λεπτών) στη συσκευή εν συγκρίσει με την ομάδα των μαρτύρων. Τέλος, κατά τη δοκιμασία της Παθητικής Αποφυγής ο αρχικός και τελικός λανθάνων χρόνος (IL, STL αντίστοιχα) φάνηκε να μη διαφέρουν μεταξύ των δυο ομάδων πειραματοζώων. Η πόση του φυτικού αφεψήματος επηρέασε με ιστοειδικό τρόπο τις υπό μελέτη βιοχημικές παραμέτρους, καθώς παρατηρήθηκε αύξηση των επιπέδων της ανηγμένης γλουταθειόνης και μείωση της υπεροξείδωσης λιπιδίων στον ολικό εγκέφαλο (-παρ/δας) των ενηλίκων μυών, η οποία συνοδευόταν από αλλαγές στις επιμέρους εγκεφαλικές περιοχές της παρεγκεφαλίδας και του μεσεγκεφάλου ενώ ο εγκεφαλικός φλοιός ακολούθησε το πρότυπο του ήπατος και έδειξε να μην επηρεάζεται. Σε σχέση με την ενεργότητα των δυο ισομορφών του ενζύμου της AChE παρατηρήθηκε αναστολή στον ολικό εγκέφαλο (-παρ/δας) της πειραματικής ομάδας συγκρινόμενη με τους μάρτυρες, η οποία συνοδεύτηκε από μείωση στις επιμέρους περιοχές του εγκεφαλικού φλοιού, του ραβδωτού και του ιπποκάμπου. Το υδατικό εκχύλισμα του Sideritis clandestina subsp. clandestina παρουσίασε: 10% αντιχολινεστερασική δράση in vitro σε αντίθεση με τον αναστολέα της γαλανταμίνης ο οποίος ανέστειλλε το ένζυμο σε ποσοστό 85%. Τέλος, το φυτικό εκχυλίσματος σε συγκέντρωση 0,3mg/mL ανέστειλε τη συσσωμάτωση του Αβ πεπτιδίου σε ποσοστό περίπου 85%. Με βάση τα ανωτέρω το «τσάι του βουνού» επιδεικνύει τάση για αγχόλυση, ενισχύει την αντιοξειδωτική άμυνα, έχει αντιχολινεστερασικές ιδιότητες και επιφέρει ανασταλτικό αποτέλεσμα στη συσσωμάτωση του Αβ αμυλοειδούς. Οι δράσεις του αυτές οφείλονται πιθανόν στην πολυφαινολική του σύσταση και οι μηχανισμοί που εμπλέκονται χρήζουν περαιτέρω διερεύνησης. / “Mountain tea” (various species of Sideritis) has been traditionally consumed in Greece as a calmative and against common cold and allergies. The aim of the present study was to examine the neuroprotective role of the above plant and focus on: a) the effect of tea drinking in behavioral parameters of adult mice (fear/anxiety, learning and memory), b) the effect of tea drinking in antioxidative biochemical parameters of adult mice brain and liver, i.e. the concentration of reduced glutathione (GSH), the levels of lipid peroxidation and the activity of the two acetylcholinesterase (AChE) isoforms, and c) in vitro putative anticholinesterase and antiamyloid actions of Sideritis clandestina subsp. clandestina infusion. The beverage was provided (4g/100 mL, daily) for 40 days to adult male Balb-c/jice. Fear/anxiety was assessed by the measurement of i) the percentage of time spent in the open arms of the elevated plus maze apparatus and ii) the thigmotactic response (the tendency to remain close to vertical surfaces) of adult mice in an open-field. Learning and memory was assessed using the step-through passive avoidance task which is based on the obseravation that the experimental mice remember that a specific reaction has negative effects (electric foot shock). The oxidant/antioxidant properties of tea drinking was determined via measurement of a) the concentration of GSH (antioxidant marker), which is based on the formation of a fluorescent complex after the reaction of o-pthalaldehyde with glutathione and hystidyl compounds and b) the levels of malondialdehyde (MDA) (oxidant marker) by monitoring thiobarbituric acid reactive substance formation. The ex vivo and in vitro AChE activity was measured using the colorimetric method of Ellman where acetylthiocholine iodide was used as a substrate. Galantamine, a strong inhibitor of AChE, was used as a standard during in vitro determination of the enzyme activity. The effect of the infusion on amyloid-beta aggregation was studied in vitro with a thioflavine T - based fluorescence assay. Tea drinking caused statistically significant a) increase of the time percentage that animals spent into the open arms of the elevated plus maze apparatus and b) decrease of thigmotaxis time and increase of the time that animals entered to the central area of open field. Initial and Step-Through Latency showed no significant difference between two animal groups. The beverage also affected the biochemical parameters examined in the present study, in a tissue specific manner. More specifically, adult mice whole brain (-Ce) displayed increased reduced glutathione content and decreased lipid peroxidation levels compared to the controls. Similar changes were also observed in cerebellum and midbrain while cerebral cortex and liver were not affected. Regarding the activity of the two AChE isoforms, tea intake caused significant inhibition of these enzymes’ activity in whole brain (-Ce), compared with the control group. In agreement, cerebral cortex, striatum and hippocampus dispayed similar inhibition in both AChE isoforms activity after tea consuming. Sideritis clandestina subsp. clandestina infusion exhibited 10% in vitro anticholinesterase activity while galantamine inhibited the enzyme in a percentage of 85%. Moreover, tea infusion in a concentration of 0,3 mg/mL exhibited 85% inhibition of Ab1-40 fibrillogenesis in vitro, indicating, thus, strongly a putative antiamyloid action of Sideritis clandestina subsp. clandestinα. Conclusively, our results suggest that mountain tea infusion exhibits anxiolytic-like action, antioxidant and anticholintesterase properties and a strong, in vitro, inhibitory effect on amyloid-beta’s aggregation. These activities are most probably due to the polyphenols contained in Sideritis clandestina subsp. clandestina infusion; the underlying mechanisms need, though, further, in deep investigation. Οξειδωτικό στρες Νευροεκφύλιση Νόσος Alzheimer Χολινεργικό σύστημα Ακετυλοχολινεστεράση Εγκέφαλος μυών Ήπαρ Συμπεριφορά Φόβος/άγχος Μάθηση-μνήμη 583.96 Sideritis clandestina subsp. clandestina Oxidative stress Reduced gluthatione Lipid peroxidation Neurodegeneration Alzheimer disease Cholinergic system Acetylcholinesterase Mice brain Liver Behavior Fear/anxiety Learning-memory
308	Μελέτη της επίδρασης αφεψήματος του φυτού Crocus sativus στην από το μόλυβδο επαγόμενη νευροτοξικότητα σε σχέση με συμπεριφορικές παραμέτρους ενήλικων αρσενικών μυών και βιοχημικούς δείκτες των εγκεφαλικών τους περιοχών Αυγουστάτος, Διονύσιος 04 December 2012 (has links) Πολλοί περιβαλλοντικοί παράγοντες μελετώνται εδώ και δεκαετίες για τις επιπτώσεις τους στο νευρικό σύστημα. Περιβαλλοντικοί παράγοντες όπως ο μόλυβδος (Pb) έχει δειχθεί ότι εμπλέκονται στην παθοφυσιολογία ασθενειών όπως η νόσος Alzheimer προκαλώντας νευροεκφύλιση σε ενήλικους αλλά και αναπτυσσόμενους οργανισμούς. Το περιβάλλον όμως είναι επιπλέον πλούσιο σε προστατευτικούς παράγοντες όπως τα εκχυλίσματα διαφόρων φυτών της ελληνικής επικράτειας τα οποία μάλιστα αποτελούν και σημαντική πηγή εσόδων σε περιπτώσεις όπως του κρόκου της Κοζάνης. Σκοπός της παρούσας εργασίας ήταν η διερεύνηση της επίδρασης της πόσης μολύβδου (500ppm) για 14 και 28 ημέρες, η πόση αφεψήματος του φυτού Crocus sativous για 28 ημέρες και η χορήγησή τους σε σειρά για 14 και 14 μέρες αντίστοιχα, από ενήλικους αρσενικούς μύες. Συγκεκριμένα διερευνήθηκαν οι συμπεριφορικές καταστάσεις άγχος/φόβος και τάση για κατάθλιψη καθώς και οι βιοχημικοί δείκτες ενεργότητα της ακετυλοχολινεστεράση (AChE), συγκέντρωση της γλουταθειόνης (GSH) και υπεροξείδοση των λιπιδίων μέσω της συγκέντρωσης της μηλονικής διαλδεΰδης (MDA). Αναλυτικά, οι συμπεριφορικές καταστάσεις άγχος φόβος μελετήθηκαν με τη χρήση των δοκιμασιών του υπερυψωμένου λαβυρίνθου και του θιγμοτακτισμού και η επαγωγή καταθλιπτικής τάσης με τη χρήση της δοκιμασίας της εξαναγκασμένης κολύμβησης. Η ενεργότητα του ενζύμου AChE μετρήθηκε με τη χρήση της χρωματομετρικής μεθόδου του Ellman σε διαλυτό σε άλας κλάσμα (SS) [περιέχει κυρίως την G1 ισομορφή του ενζύμου] και διαλυτό σε απορρυπαντικό κλάσμα (DS) [περιέχει κυρίως την G4 ισομορφή του ενζύμου] του ιστού. Η συγκέντρωση της γλουταθειόνης προσδιορίστικέ με τη φθορισμομετρική μέθοδο των Mokrasch LC. & Teschke EJ. (1984), η οποία βασίζεται στο σχηματισμό φθορίζοντος συμπλόκου μετά την αντίδραση της ο- φθαλαλδεΰδης με την γλουταθειόνη και ιστιδυλ- ενώσεις. Τέλος η υπεροξείδωση των λιπιδίων μελετήθηκε μέσω της μηλονικής διαλδεΰδης (MDA), η οποία αποτελεί το κύριο προϊόν της υπεροξείδωσης των πολυακόρεστων λιπαρών οξέων. Ο προσδιορισμός της έγινε φθορισμομετρικά λόγω του συμπλόκου που δημιουργείται όταν η ίδια αντιδρά με το θειοβαρβιτουρικό οξύ. Οι παραπάνω μελέτες έγιναν στους ιστούς φλοιός, παρεγκεφαλίδα, μεσεγκέφαλος, ιππόκαμπος, ραβδωτό και ήπαρ ενήλικων αρσενικών μυών. Τα αποτελέσματά μας έδειξαν ότι το βάρος των πειραματοζώων δεν επηρεάζεται κατά τη διάρκεια του χειρισμού, η πόση του Pb για 28 και 14 ημέρες προκάλεσε αγχογενή συμπεριφορά και επαγωγή του φόβου στα πειραματόζωα καθώς και επαγωγή καταθλιπτικής τάσης. Η χορήγηση του κρόκου στους μύες μάρτυρες σχετίζεται με αγχολυτική δράση αλλά όχι με αντικαταθλιπτική δράση. Αντικαταθλιπτική του δράση παρατηρείται μόνο στην περίπτωση που ακολούθησε τη χορήγηση του μολύβδου για 14 ημέρες. Επίσης η χορήγηση Pb προκάλεσε αναστολή της ενερότητας και των δύο ισομορφών του ενζύμου με ιστοειδικό τρόπο, η πόση του αφεψήματος του φυτού οδήγησε σε θετική δράση σε σχέση με την ενεργότητά του τόσο όταν χορηγήθηκε μόνο του όσο και κατά τη χορήγηση του μετά από το Pb (με ιστοειδικό τρόπο δράσης). Αξίζει να σημειωθεί ότι η δράση του μολύβδου μπορεί να είναι άμεση προκαλώντας νευροεκφύλιση είτε έμμεση επεμβαίνοντας σε διάφορα μεταβολικά μονοπάτια που επειρεάζουν την ενεργότητα του ενζύμου. Αναφορικά με τη συγκέντρωση της γλουταθειόνης ο μόλυβδος όταν χορηγήθηκε έδρασε ιστοειδικά, προκαλώντας μείωση της ενεργότητας του ενζύμου ενώ δεν παρατηρήθηκε δράση του φυτικού αφεψήματος επι του ενζύμου. Τέλος η υπεροξείδωση των λιπιδίων αυξήθηκε ιστοειδικά από την χορήγηση του Pb ενώ αντίθετα περιορίστηκε από την πόση του αφεψήματος με επίσης ιστοειδικό τρόπο. Συνοψίζοντας, στην παρούσα εργασία παρατηρήθηκε αρνητική δράση του μολύβδου σε συμπεριφορικό και βιοχημικό επίπεδο, θετική δράση του κρόκου στις παραπάνω διεργασίες καθώς επίσης θετική δράση κατά περίπτωση και της σε σειρά χορήγησης του αφεψήματος κρόκου μετά από χορήγηση μολύβδου. / Various environmental factors have been studied decades ago due to their effects on nervous system. It has been shown that lead (Pb) is implicated in the pathophysiology of diseases such as Alzheimer’s disease, resulting in neurodegeneration in adult and developing organisms. Also, the environment is rich in protective agents, such as various plant extracts of the Greek flora (e.g. Greek saffron which is cultivated at Kozani region in northern Greece) that present simultaneous financial interest. Aim of the present study was to investigate the effects of oral administration of lead (500ppm) for 14 and 28 days, Crocus sativous infusion for 28 days and lead (for 14 days) plus Crocus sativous infusion (for 14 days), in adult male mice. Briefly, behavioral parameters of anxiety/fear and depression-like and acetylcholinesterase (AChE) activity, glutathione (GSH) and lipid peroxidation (malondialdehyde, MDA) levels, were evaluated. In detail, anxiety/fear and depression-like behavior were assessed by using the elevated plus maze and thigmotaxis tests and forced swimming test, respectively. AChE activity was determined in salt soluble (SS) [contains mainly G1 isoform of the enzyme] and detergent soluble (DS) [contains mainly the G4 isoform of the enzyme] fractions of tissue homogenates, by Ellman’s colorimetric method. Glutathione content was measured fluorometrically according to the procedure of Mokrasch LC. & Teschke EJ. (1984), which is based on the formation of a fluorescent complex after reaction with o-phthalaldehyde and histidyl compounds. Also, lipid peroxidation levels were determined fluorometrically by measuring malondialdehyde (MDA) concentration after its reaction with thiobarbituric acid, as MDA is the main product of polyunsaturated fatty acid peroxidation. The biochemical assessments were performed in cortex, cerebellum, midbrain, hippocampus, striatum and liver of adult male mice. Our results showed that there were no effects on mouse body weight during the experimental period and Pb intake for 28 and 14 days induced anxiety/fear and depression-like behavior. Saffron administration to control mice is associated with anxiolytic but not antidepressant efficacy. Antidepressant effects of saffron were observed only in mice pre-treated with lead for 14 days. Also, Pb intake caused inhibition of both AChE isoforms’ activity and saffron infusion that was administered either alone or under Pb toxicity, beneficially affected enzyme activity, in a tissue-specific way. It should be noticed that lead may act directly, inducing neurodegeneration or indirectly, interfering with various metabolic pathways that influences AChE activity. Moreover, Pb intake reduced glutathione content in a tissue-specific way, while no effect was observed after saffron administration. Finally, lipid peroxidation levels were increased and decreased tissue specifically, after Pb and saffron administration, respectively. Conclusively, the current study presents adverse effects of lead on behavioral and biochemical parameters and beneficial effects of saffron infusion when it was administered either alone or under Pb toxicity. Νευροεκφύλιση Νευροπροστασία Μόλυβδος (Pb) Χολινεργικό σύστημα Οξειδωτικό στρες Ακετυλοχολινεστεράση Άγχος / Φόβος Καταθλιπτική τάση Συμπεριφορά Εγκέφαλος 615.53 616.804 610 724 Neurodegeneration Neuroprotection Lead (Pb) Cholinergic system Oxidative stress Acetylcholinesterase Reduced glutathion Lipid peroxidation Anxiety / Fear Like depression Behavior Brain Crocus sativus
309	Filogenia da sensibilidade da acetilcolinesterase cerebral de peixes ao metil-paraoxon como um possível marcador ambiental / Phylogeny of the sensitivity of fish brain acetylcholinesterase to methyl-paraoxon as a possible marker Environmental Freitas, Amanda Pereira de January 2009 (has links) Made available in DSpace on 2011-05-04T12:36:17Z (GMT). No. of bitstreams: 0 Previous issue date: 2009 / Todos os animais com células nervosas e musculares possuem a enzima acetilcolinesterase (EC 3.1.1.7, AChE) e essa seqüência de aminoácidos está presente em muitas outras proteínas, com ou sem atividade catalítica, fato que permite que essa proteína seja utilizada em estudos de filogenia e de evolução. A grande diferença de afinidade entre substratos e inibidores é utilizada como um biomarcador para estudos genéticos de vários grupos de animais, especialmente insetos. Peixes possuem uma grande diferença na sensibilidade da AChE ao metil-paraoxon (MP) em relação aos animais terrestres e essa diferença pode estar relacionada à evolução. As constantes cinéticas de inibição (CCI) para o mecanismo de inibição progressivamente irreversível da AChE cerebral ao MP foram determinadas em duas fontes de AChE como um modelo para avaliação do potencial de uso das CCI como biomarcador para estudos evolucionários e filogenéticos. As CCI da AChE cerebral de seis exemplares de tainha (Mugil liza), coletados em duas lagoas da costa do Estado do Rio de Janeiro (Araruama e Saquarema), em tempos diferentes (2005 e 2007, respectivamente), foram determinadas em dois laboratórios distintos (CESTEH - FIOCRUZ e Dept. Bioquímica - UERJ). As CCI, medidas separadamente em cada exemplar, indicaram que essas constantes são preservadas em todos os exemplares de uma mesma espécie e que a metodologia empregada pode ser conduzida em laboratórios distintos sem grandes variações. A AChE cerebral de tainha foi tomada como um exemplo de enzima menos sensível (IC50 = 2118nM) e a de galinha comercial (Gallus gallus domesticus) como um exemplo de uma enzima muito mais sensível ao MP (IC50 = 26nM). Alguns testes foram feitos para a validação dessa metodologia. A AChE cerebral dessas duas fontes de enzima foi parcialmente purificada descartando o sobrenadante do homogeneizadoe solubilizando o sedimento com o detergente Triton X-100. A inibição da atividade de AChE nessas preparações pelo substrato acetiltiocolina, comportamento típico da AChE, comprovou a homogeneidade dessa atividade enzimática como representativa da AChE verdadeira em cada animal. A utilização do MP permitiu aferir as soluções de inibidorcom métodos colorimétricos no momento do uso e a preparação solúvel de AChE eliminou artefatos insolúveis que atrapalham a quantificação da enzima. Algumas características matemáticas do cálculo das CCI foram discutidas e um modelo foi validado para ser utilizado em estudos de evolução e filogenia de peixes marinhos da costa brasileira. Como a AChE cerebral de todos os animais terrestres, cujos resultados estão disponíveis, é muito mais sensível ao MP, exemplares de uma espécie de baiacu (baiacu-arara, Lagocephaluslaevigatus) foram testados como um exemplo de peixe mais jovem na escala evolutiva. Os resultados das CCI da AChE cerebral para essa espécie (IC50 = 2243nM) indicaram que entre os peixes a idade evolutiva não está correlacionada com a sensibilidade aos organofosforados. A AChE mais sensível entre os peixes testados foi a de um tipo de bagre (bagre-branco, Genidens barbus, IC50 = 606nM) e a enzima do cação-frango (Rhizoprionodonporosus), exemplo de um peixe mais antigo na evolução, apresentou uma sensibilidade intermediária (IC50 = 1280nM). Estudos com outras espécies correlacionadas com aquelas que se mostraram mais sensíveis ao MP terão que ser feitos para uma resposta mais adequada sobre o uso das CCI de inibição da AChE cerebral por MP como possível marcador evolutivo e filogenético. / The enzyme acetylcholinesterase (EC 3.1.1.7, AChE) is present in all animals with neurons and muscle cells, and many other proteins have the same sequence, with or without catalytic activity, allowing them to be used for phylogenetic and evolutionary studies. The great difference between substrates and inhibitor affinities makes it useful as a biomarker for genetic studies of various animals groups, especially insects. There are great differences among fish in AChE sensitivity to methyl-paraoxon (MP) in relation to terrestrial animals, and these differences can be related to evolution. The inhibition kinetic constants (IKC) for progressive irreversible inhibition of brain AChE with MP were determined in these two AChE sources as models for evaluating IKC as potential biomarkers in evolutionary and phylogenetic studies, especially among fish. IKC of brain AChE from six specimens of Mugil liza, a very common coastal fish, was collected from two of Brazil's lagoons in Rio de Janeiro State during 2005 at Araruama and 2007 at Saquarema. First samples were assayed at CESTEH - Fundação Oswaldo Cruz and the latter at Dept. Bioquímica - Universidade do Estado do Rio de Janeiro. The IKC was measured separately for each fish showing that these constants were maintained for all animals of the same species and that this methodology can be used in different laboratories without variations. The cerebral AChE of tainha was used as an example of a less sensitive enzyme (Concentration which inhibits 50% of enzyme activity after 30 minutes of incubation, or IC50, = 2118nM). The commercial hen (Gallus gallus domesticus) was used an example of a very highly sensitive enzyme to MP (IC50 = 26nM). Some tests were carried out to validate this methodology. The cerebral AChE of these two sources of enzyme was partially purified discarding the supernatant of the homogenate and solubilizing the pellet with Triton X-100 detergent. The AChE activity inhibition in these preparations by excess of the substrate acetylthiocholine, a typical AChE behaviour, proved the homogeneity of this preparation and that it is representative of the real AChE of each animal. Using MP allows checking out the solutions of inhibitor with colorimetric methods in the moment of use. The preparation of soluble AChE eliminates insoluble matters which confound the enzyme quantification. Some characteristics of mathematical calculations of IKC were defined to create a valid model that is able to be used for evolutionary and phylogenic studies of fish and other animals. The cerebral AChE of all terrestrial animals, whose results are available, is highly sensitive to MP. To compare with a similar recently evolved fish, a sample of baiacu (baiacu-arara, Lagocephalus laevigatus) was tested for IKC and the results (IC50 = 2243nM) indicated that evolutionary age of the fish does not correlate with sensitivity to organophosphorus compounds. The most sensitive AChE among the fish tested was a type of catfish (bagre-branco, Genidens barbus, IC50 = 606nM) and the enzyme of an older evolved fish, a small shark (cação-frango, Rhizoprionodon porosus), had an intermediate sensitivity (IC50 = 1280nM). Studies with other species correlated to those being more sensitive to MP have to be made to get adequate answers about the use of IKC for cerebral AChE inhibition by MP as a possible evolutionary and phylogenetic marker. Acetilcolinesterase Filogenia Metil-paraoxon Biomarcador Monitoramento Ambiental Filogenia Peixes/fisiologia Marcadores Biológicos Acetylcholinesterase Phylogeny ethyl-paraoxon Biomarker Monitoramento Ambiental Filogenia Peixes/fisiologia -Marcadores Biológicos
310	Etudes des propriétés antiplasmodiales, antitrypanosomales et inhibitrices d'acétylcholinestérase de triclisia sacleuxii (Pierre) Diels "Menispermaceae" / Study of antiplasmodial, antitrypanosomal and acetylcholinesterase inhibatory properties of triclisia sacleuxii (Pierre) Diels "Menispermaceae" Murebwayire, Sengabo 09 June 2008 (has links) Le paludisme, la maladie la plus dévastatrice des régions tropicales fait l’objet de nombreuses recherches ayant pour but de trouver des médicaments préventifs, du matériel de protection, de nouveaux traitements, des vaccins, …<p>Notre travail s’est inscrit dans la recherche des composés naturels actifs sur l’agent pathogène, le Plasmodium. Nos investigations phytochimiques et pharmacologiques ont porté sur Triclisia sacleuxii, une plante utilisée en médecine traditionnelle pour traiter diverses maladies dont deux parasitaires: la schistosomiase et l’ascardiose. Elle est aussi employée dans la préparation du poison de flèche. De plus, T. sacleuxii appartient à la famille des Menispermaceae, une famille riche en alcaloïdes bisbenzylisoquinoléiques (BBIQ). Ces composés ont de nombreuses propriétés biologiques dont l’activité antipaludique et trypanocide. Plusieurs autres espèces appartenant au genre Triclisia sont utilisées en médecine traditionnelle pour traiter la fièvre, le paludisme et d’autres pathologies. Ces éléments ont motivé la recherche dans cette plante des composés à activité antiplasmodiale. En effet, la plupart des composés que nous en avons isolés (p 12) sont actifs aussi bien sur la souche chloroquino-sensible (3D7) que sur la souche chloroquino-résistante (W2) que nous avons testées.<p>Deux d’entre eux ont en plus une activité plus élevée vis-à-vis de la souche choroquino-résistante.<p>Les composés actifs sur Plasmodium falciparum ont également montré une toxicité à l’égard de Trypanosoma brucei brucei, une sous-espèce apparentée à celles qui sont à la base de la maladie du sommeil en Afrique Centrale et de l’Est.<p>A part les usages mentionnés précédemment, T. sacleuxii est en plus employée comme antidote contre les morsures de serpents. Ce qui voudrait dire qu’elle pourrait renfermer des inhibiteurs d’enzymes.<p>Aussi, des BBIQ ont déjà démontré une activité inhibitrice de l’acétylcholinéstérase (AChE) et des phospholipases A2. Sur base de ces informations, nous avons assigné un troisième objectif à notre investigation qui cible l’AChE en correlation avec la maladie d’Alzheimer (MA). La MA est une pathologie neurodégénérative qui affecte en général les personnes âgées de plus de 60 ans, caractérisée entre autres par une perte progressive de la mémoire, une détérioration de plusieurs fonctions cognitives, de troubles neurologiques et du comportement, … Les différents extraits alcaloïdiques ont montré un degré d’inhibition de l’AChE élevé ( 80 - 90%) à une concentration de 100 μg/ml. Avec les composés purs, l’inhibition est très variable (30 - 90 %) suivant la structure. Enfin, nous avons effectué des investigations pour déterminer le mode d’action antiplasmodiale des BBIQ majeurs isolés de T. sacleuxii. Il apparaît que non seulement toutes les BBIQ n’agissent pas par un même mode d’action, mais aussi un même composé pourrait agir simultanément suivant deux ou plusieurs mécanismes différents.<p><p><p>Malaria, the most devastating disease in tropical areas, is currently a target of numerous researches, aiming to find preventive medicines, protective tools, new treatments and vaccines. In a search for antiplasmodial natural compounds, we have undertaken phytochemical and pharmacological investigations on Triclisia sacleuxii, used in traditional medicine to treat various ailments including two parasitological diseases; schistosomiasis and ascariasis. It is also used as an arrow poison.<p>Triclisia sacleuxii belongs to the Menispermaceae family, which is known to contain bisbenzylisoquinolines. These components have shown various biological activities among which antimalarial and trypanocidal activity. Furthermore, many Triclisia species are used in traditional medicine for treating fever and malaria along with other disorders.<p>With this background the research was set out to investigate on possible antiparasitic compounds active against Plasmodium falciparum.<p>Most of the compounds isolated in this work were active towards both chloroquine sensitive strain (3D7) and chloroquine resistant Plasmodium strain (W2). Interestingly some of them demonstrated selectivity for the resistant strain.<p>The compounds which displayed antiplasmodial activity also showed toxicity against Trypanosoma brucei brucei, a parasite related to those which cause sleeping sickness.<p>Besides Triclisia sacleuxii traditional uses mentioned above, it is also used as a snakebites antidote. This suggests that it might contain enzymes inhibitors. Additionally, in previous works, bisbenzylisoquinolines which are believed to be present in T. sacleuxii, have displayed phospholipases A2 and acetylcholinesterase inhibitory activity. On the basis of these informations, the third aim of our investigation targeted acetylcholinesterase (AChE), an enzyme involved in Alzheimer’s disease (AD). AD is a neurodegenerative disease occurring mostly in people aged beyond 60 years, characterised by a progressive loss of memory, impairement of multiple cognitive functions, neurological and behavior disorders, Our results have demonstrated that leaves, stems and roots alkaloidal fractions have high anti-AChE activity. Pure compounds exhibited a structure-dependent activity ranging from 30 up to 90% at a concentration of 100μg/ml).<p>Finally, we have undertaken an investigation on the antiplasmodial mode of action of the major alkaloids. It appears that not only the BBIQ do not act by a same mechanism, but also a single compound may act by more than one mode of action. / Doctorat en Sciences biomédicales et pharmaceutiques / info:eu-repo/semantics/nonPublished Sciences pharmaceutiques Plasmodium Menispermaceae -- Therapeutic use Malaria -- Chemotherapy Antimalarials Acetylcholinesterase Plasmodium Paludisme -- Chimiothérapie Antipaludiques Acétylcholinestérase beta-hematine / beta-hematine.

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