Effects of Electrical Stimulation of the Pontine A5 Cell Group on Blood Pressure and Heart Rate in the Rabbit

Woodruff, Michael L., Baisden, Ronald H., Whittington, Dennis L.

30 July 1986

The effects of electrical stimulation of the A5 noradrenergic cell group of the ventrolateral pons was assessed in rabbits. Stimulation administered through either concentric bipolar or monopolar electrodes produced current-intensity related increases in mean arterial pressure (MAP). Decreases in heart rate (HR) accompanied the increases in MAP, but were essentially eliminated by bilateral vagotomy or destruction of the nucleus and tractus solitarii (NTS), thereby indicating that the HR decelerations were secondary to activation of baroreceptor reflexes. Neither vagotomy nor midcollicular section of the brainstem altered the MAP response to A5 stimulation. Bilateral destruction of the NTS slightly enhanced the response. Several rabbits received microinjections of 6-hydroxydopamine (6-OHDA) into the A5 region 2 weeks before the experiment. Other rabbits received vehicle injections and served as control subjects for the non-specific effects of the 6-OHDA injections. 6-OHDA injections, but not vehicle injections, prevented the vasopressor effects of A5 stimulation. However, stimulation of the A1 noradrenergic nucleus of the ventrolateral medulla produced decreases in MAP in rabbits given prior microinjections of 6-OHDA into A5. These observations are interpreted to indicate that the 6-OHDA injections produced neurotoxic effects which were relatively restricted to the A5 region. Furthermore, the data from all of these experiments are interpreted as indicating that the vasopressor effects observed as a consequence of electrical stimulation of A5 are due to excitation of the noradrenaline-containing neuron cell bodies of this region and that this effect is mediated via pathways arising from this region and terminating in the intermediolateral cell column of the spinal cord.

A5 noradrenergic nucleus

blood pressure

electrical stimulation

pons

rabbit

Biomedical Sciences

Bioremediation potential of 1,1,1-trichloro-2,2-bis(p-chlorophenyl) ethane (DDT) from a sandy-loam soil using aerobic bacteria Alcaligenes eutrophus A5, Corynebacterium sp. and a mixed culture

Erdem, Ziya

04 October 2016

No description available.

Environmental Engineering

Microbiology

DDT

chloropesticide

soil bioremediation

Alcaligenes eutrophus A5

Corynebacterium sp

Etude cinétique de la liaison élémentaire entre Annexine-A5 et membranes et mise au point d’un test de quantification des microparticules plasmatiques pro-coagulantes, par cytométrie en flux / Kinetics of Annexin-A5 binding to model membranes studied by Flow Cytometry and development of a new method for quantifying Plasmatic Microparticles

Arraud, Nicolas

19 December 2011

L’Annexine A5 (AnxA5) est une protéine soluble se liant aux membranes contenant de la phosphatidylsérine (PS) en présence de calcium (Ca2+). Le rôle central joué par l’AnxA5 dans les processus de réparation membranaire a été récemment mis en évidence. L’AnxA5 possède une très forte affinité pour les membranes biologiques contenant de la PS, cependant son mode de liaison aux membranes n’est pas encore élucidé.La première partie de mon travail de thèse a concerné le développement d’une approche originale d’étude de la liaison de l’AnxA5 à des microsphères de silice fonctionnalisées par une bicouche lipidique (µPSiO2@SLB pour supported lipid bilayer), par cytométrie en flux (FCM). Cette approche m’a permis d’étudier la liaison à l’équilibre et en cinétique à très faible concentration en AnxA5, de l’ordre du picomolaire. Cette approche représente une des méthodes les plus sensibles d’étude de liaison à l’équilibre et la première permettant d’accéder aux constantes cinétiques d’interaction pour l’AnxA5. Cette étude m’a également permis de mettre au point une stratégie de dosage indirect de liposomes contenant de la PS avec une sensibilité de l’ordre du nanogramme de lipides par millilitre.La seconde partie de ma thèse a concerné l’étude de microparticules (MP), fragments de membranes cellulaires présents dans les fluides biologiques. Dans le plasma sanguin la majorité des MP sont d’origine plaquettaire et exposent de la PS. Il existe une corrélation entre la concentration en MP plasmatiques exposant de la PS et le développement de pathologies thrombotiques. La FCM est la méthode de référence dans l’étude des MP cependant leur détection est rendue difficile par leur petite taille. J’ai appliqué aux MP plasmatiques le test de dosage développé pour les liposomes. Les résultats obtenus sont prometteurs et permettent d’envisager le développement d’un test de dosage de l’ensemble des MP exposant de la PS. / Annexin-A5 (AnxA5) is a soluble membrane binding protein that binds to phosphatidylserine (PS) containing membranes in a calcium dependent manner and plays a central role in cell membrane repair processes. AnxA5 has a remarkably high affinity for PS containing membranes, but its binding mechanism remains unclear.The first part of my PhD work was to develop a new method for studying AnxA5 binding using supported lipid bilayer functionalized silica microspheres (µPSiO2@SLB) and Flow Cytometry (FCM). This approach allowed me to describe in details both equilibrium and kinetics of AnxA5 binding at picomolar concentrations in AnxA5. This study is one of the most sensitive for equilibrium binding studies and the first allowing to measure binding kinetics constants for AnxA5. This study also led to the development of a new strategy for determination of liposome concentration with sensitivity in the range of one nanogram of lipid per milliliter. The second part of my work focused on microparticles (MP) that are cell membrane fragments found in biological fluids. In plasma, the vast majority of MP originates from platelets and expresses PS at their surface. There is a correlation between MP concentration in plasma and thrombotic risk. FCM is the “golden standard” of hæmatologic analysis but the majority of MPs are too small to be detected. I have applied the test developed with liposomes for the quantification of MP. The results are promising and allow foreseeing the development of a test able to give the absolute quantity of PS exposing MPs in plasma samples.

Annexine A5

Cinétique de liaison

Cytométrie en flux

Bicouche lipidique supportée

Microsphères de silice

Phosphatidylsérine

Microparticules plasmatiques

Quantification

Annexin A5

Binding kinetics

Flow cytometry

Supported lipid bilayer

Silica microspheres

Phosphatidylserine

Plasmatic microparticles

Quantification

"for to knowen here sicknesse and to do the lechecraft there fore" : animal ailments and their treatment in late-mediaeval England

Aitchison, Briony Louise

January 2010

Veterinary medicine in late-mediaeval England has thus far received little attention. This study therefore aims to partly fill this gap by providing an insight into English veterinary practices at this time. The introduction places the animals under discussion into context, from the noble war-horse to the lowly pig. Also discussed are the sources, with their intended audience and evidence for use. The first chapter concentrates on those who were responsible for treating animals when ill, examining the qualities sought in such people, and the source of their learning. In the second chapter the ailments suffered by mediaeval animals are discussed, together with the causes of illness and methods of diagnosis. The third, and final, chapter examines the treatment meted out to animals. Firstly the factors influencing this are explored, followed by surgical intervention, then therapeutic methods of treatment. The precautions taken when treating animals are looked at, as too is the efficacy of the remedies, whilst finally the preparation of medicines, the instruments used, and the materia medica employed are discussed. The aim of this study is not only to provide an insight into the state of veterinary medicine in late-mediaeval England, but also to adopt a broader and more comparative approach than has hitherto been undertaken. It therefore draws upon veterinary texts, hawking and hunting manuals, husbandry treatises, and recipe collections, in order to compare and contrast the ailments and treatment meted out to a variety of animals. Another important facet is to examine the reality of care, which is achieved through an examination of sources such as household and manorial accounts. By marrying the actuality of care with the theory and recommendations of treatises and recipe collections, our understanding of animal welfare is more greatly enhanced.

942.03

Extending ionothermal synthesis

Aidoudi, Farida Himeur

January 2012

An exploration of some organic-inorganic hybrid metal fluorides and lanthanide containing metal organic frameworks (Ln-MOFs) has been carried out under ionothermal conditions. In this synthesis technique an ionic liquid (IL) or deep eutectic mixture (DES) is used as the solvent and in many cases as the provider of the organic structure directing agent. A wide range of ILs and DESs have been investigated as the reaction solvent for the synthesis of organically templated vanadium fluorides and oxyfluorides (VOFs), and initially this has proved to be successful with the isolation of 13 phases, including eight new materials. In the VOFs synthesis the IL acts as a solvent, however the DES acts as a solvent and also as a template delivery agent, where the expected template is provided by the partial breakdown of the urea derivative component. Interestingly, it has been shown that the same structure can be accessible via two different ways; either by using IL with an added templating source, or simply through the use of a DES without any other additive; since the template is provided by the in situ breakdown of the DES. The synthesis of VOFs with extended structures was achieved by the use of the hydrophobic IL 1-ethyl-3-methylimidazolium bis(trifluoromethylsulfonyl)imide (EMIM Tf₂N) as the solvent. [HNC₅H₅][V₂O₂F₅] represents the first VOF with a 2D network that contains exclusively V⁴⁺. This material may be considered as arising via condensation of the previously known ladder-like chains. Furthermore, using imidazole as an added template has produced another layer material that has significant similarities to the [HNC₅H₅][V₂O₂F₅] structure, but with some key differences. Within the same system three other phases were also isolated, including two novel materials displaying the known ladder-type building units. Further investigations in the ionothermal synthesis of VOF using EMIM Tf₂N resulted in a successful synthesis of [NH₄]₂[HNC₇H₁₃][V₇O₆F₁₈], a novel material displaying a unique double layered topology featuring a S = ½ kagome type lattice of V⁴⁺ ions (d¹). Two of the V⁴⁺ based kagome sheets are pillared by V³⁺ ions to form a double layered structure templated by both ammonium and quinuclidinium cations. This compound exhibits a high degree of magnetic frustration, with significant antiferromagnetic interactions but no long range ordering was observed above 2 K. This material presents an interesting comparison to the famous Herbertsmithite, ZnCu₃(OH)₆Cl₂, and may provide an excellent candidate for realising a quantum spin liquid (QSL) ground state. Interestingly, in this system the use of EMIM Tf₂2N as a solvent produces mainly V⁴⁺-containing materials, despite the high reaction temperature (170 °C). This characteristic is unprecedented in VOFs synthesis, as rising the reaction temperature above 150 °C in other techniques (i.e. hydrothermal synthesis) would often result in further reduction of V⁴⁺ to V³⁺. Using the ionothermal technique in the synthesis of hybrid iron fluorides resulted in the isolation of three chain-type materials. Again, the IL acts as the solvent and the DES acts as the solvent and also as the template provider where the expected template is released by the partial breakdown of the urea derivative component of the DES. The synthesis of Ln-MOF using a choline chloride/ 1,3-dimethylurea deep eutectic mixture has produced three novel isostructural materials. Usually, in ionothermally prepared materials (i.e. zeolites) the urea portion of the DES is unstable and breaks down in situ to form ammonium or alkylammonium cations. In the ionothermal synthesis of Ln-MOF, 1,3-dimethyurea (DMU) remains intact and is occluded in the final structure. Using a choline chloride/ethylene glycol deep eutectic solvent led to the isolation of a Ln-MOF with interesting structural properties, however none of the DES components appeared in the final structure. These results demonstrate once more the usefulness and applicability of the ionothermal synthesis method and emphasise how this synthesis technique can be further extended and applied in the preparation of important structures with unique properties and functionalities.

546.3

Apolipoprotein A5 Genetic Polymorphisms In Turkish Population And The Risk Of Ischemic Stroke

Sahin, Esra

01 September 2008

Stroke is the third leading cause of death and the most common cause of disabilities worldwide. Apolipoprotein A5 gene (APO A5), which encodes a 369 amino acid protein called Apolipoprotein AV (apo AV), has several single nucleotide polymorphisms (SNPs) found to be associated with altered triglyceride (TG) levels. Atherosclerosis is a major cause of ischemic stroke and this pathology may be associated with variability of TG levels. The main objective of this study was to investigate the coding region (c.553G&gt / T) and promoter region (-1131T/C) polymorphisms of the APO A5 gene as a risk factor for ischemic stroke. The study group in Turkish population consisted of 198 unrelated ischemic stroke patients and 130 control subjects. There was no statistically significant difference between the groups with respect to age and gender. Total blood samples were obtained from G&uuml / lhane Military Medical Academy Hospital, Neurology Department, Ankara. In stroke patients, hypertension and diabetes were 2.5 times more common and high-density lipoprotein cholesterol (HDL-C) was significantly lower than controls. Logistic regression analysis showed that hypertension, diabetes and smoking were significant predictors of stroke. The frequency of risky alleles c.553T and -1131C were 0.003 and 0.098, respectively, in patients and were nearly the same with controls. The risk of hypertensive and diabetic individuals having ischemic stroke was higher in -1131C allele carriers (Odds ratio / OR= 3.4 and 6.4, respectively) than -1131TT individuals (OR= 2.3 and 1.9, respectively). Stroke patients with -1131C allele had significantly higher TG levels (1.70 mmol/L) and lower HDL-C levels (1.05 mmol/L) when compared to controls (1.35 mmol/L and 1.20 mmol/L, respectively) with the same genotype. Logistic regression analysis revealed elevated TG level to be associated with 2.2-fold and low levels of HDL-C to be associated with 1.8-fold increase in the risk of ischemic stroke versus control status. This is the first study investigating the relation between APO A5 c.553G&gt / T polymorphism and stroke risk. Additionally, in Turkish population -1131T/C polymorphism was analyzed for the first time in terms of its relation to ischemic stroke. The present study demonstrated that the frequency of risky alleles c.553T and-1131C were nearly the same in stroke patients and control subjects. Consequently, we decided that carrying minor alleles of c.553G&gt / T and-1131T/C polymorphisms do not constitute a risk for ischemic stroke.

QH Genetics 426-470

T, -1131T/C, Turkish Population.

Kryptoanalýza šifer používaných v GSM telefonech / Cryptanalysis of ciphers used in GSM phones

Barboriková, Jana

January 2012

The aim of this thesis is to introduce the family of A5 algorithm which is used in data encryption and decryption in GSM phones. It is focused on real time cryptanalysis of the stream cipher A5/1. It describes in detail the known plaintext attack published by A. Biryukov, A. Shamir and D. Wagner. Both the attack and the cipher are implemented. The implementation proves that the preprocessing stage of the attack is very time consuming, but the actual attack can be carried out in real time on a single PC. Then the problem of finding a good statistical model for the process of generating tree of predecessors of internal states of A5/1 is studied. We present reasons why the singletype Galton-Watson process is not suitable for the problem and introduce a multitype Galton-Watson process and a macro process. The models are applied to the process of generating predecessors and their predictions are compared with experimental data.

Synthese molekularer Bildgebungssonden für die molekulare Magnetresonanztomographie

Figge, Lena

01 July 2014

Zweck der molekularen Bildgebung ist es, biologische Prozesse auf zellulärer und molekularer Ebene zu messen und zu charakterisieren, um so die Ursachen von Krankheiten und Veränderungen im Organismus zu diagnostizieren. Sie basiert auf dem Einsatz molekularer Bildgebungssonden, welche einen spezifischen biologischen Vorgang darstellen oder sich spezifisch in dem zu untersuchenden Gewebe anreichern oder aktiviert werden. Ziel dieser Arbeit war die Entwicklung und Analyse neuer Bildgebungssonden für die spezifische in-vivo-Bildgebung der Apoptose und von Enzymaktivitäten mittels Magnetresonanztomographie (MRT) auf der Grundlage sehr kleiner Eisenoxidnanopartikel (very small iron oxide particles, VSOP). VSOP sind superparamagnetisch und durch ihre negativ geladene Citrathülle elektrostatisch stabilisiert. Für die Apoptose-Bildgebung sollte durch Bindung des Proteins Annexin A5 (AnxA5) an die Citrathülle der VSOP eine zielgerichtete Sonde hergestellt werden (AnxA5-VSOP). Für die Bildgebung von Enzymaktivitäten sollte eine durch die Matrixmetalloproteinase-9 (MMP-9) aktivierbare Sonde hergestellt werden (Protease-spezifische Eisenoxidpartikel, PSOP). / The goal of molecular imaging is to characterize and measure biological processes at cellular and molecular levels for the purpose of diagnosing the cause of diseases and molecular abnormalities. Molecular imaging is based on the use of probes with a high affinity to the target tissue and / or which are specifically activated. The aim of this study was to develop and analyze new molecular imaging probes for the in vivo imaging of apoptosis and enzyme activity using magnetic resonance imaging (MRI), based on very small iron oxide particles (VSOP). VSOP are superparamagnetic and electrostatically stabilized due to their negatively charged citrate surface. For the imaging of apoptosis the protein annexin A5 (AnxA5) was coupled to the citrate surface (AnxA5-VSOP). For the imaging of enzyme activities an activatable imaging probe with a cleavage site for the matrix metalloproteinase 9 (MMP-9) was synthesized (protease-specific iron oxide particles, PSOP).

Magnetresonanztomographie

Apoptose

Enzymaktivitäten

molekulare Bildgebungssonde

superparamagnetisch

VSOP

Annexin A5

PSOP

Matrixmetalloproteinase

magnetic resonance imaging

apoptosis

enzyme activity

molecular imaging probe

superparamagnetic

very small iron oxide particles

VSOP

Annexin A5

protease-specific iron oxide particles

PSOP

matrix metalloproteinase

540 Chemie

30 Chemie

YR 2404

YR 2520

ddc:540

Caractérisation, quantification et isolation de vésicules extracellulaires du plasma sanguin à l’aide de nanoparticules d’or ou magnétiques conjuguées à des protéines / Phenotyping, quantification and isolation of extracellular vesicles from blood plasma using gold or magnetic nanoparticles conjugated to proteins

Linares, Romain

02 December 2016

Les vésicules extracellulaires (VEs) sont des vésicules membranaires de taille majoritairement submicrométrique présentes dans les fluides biologiques et émises par les cellules en réponse à divers stimuli. Les VEs sont impliquées dans de nombreux phénomènes physiologiques mais également dans des pathologies telles que cancers ou maladies cardiovasculaires. Elles pourraient donc être utilisées comme biomarqueurs de ces pathologies. Bien que les VEs soient aujourd’hui largement étudiées, nos connaissances sur le sujet demeurent limitées. Ceci est principalement dû aux difficultés de caractérisation des VEs et à l’absence de standardisation de leurs méthodes d’étude et d’isolation. La première partie de mon travail de thèse a porté sur le développement d’une méthode de thiolation de protéines. Des anticorps ont été modifiés pour exposer des thiols et ont été conjugués à des nanoparticules d’or fonctionnalisées par des maléimides. Le couplage des anticorps thiolés aux nanoparticules d’or a été étudié de manière quantitative et des conditions de conjugaison optimales ont été déterminées par des approches biochimiques. La seconde partie de ce travail a concerné la caractérisation des VEs du plasma sanguin de sujets sains par microscopie électronique à transmission (MET). La morphologie, la taille et le phénotype des VEs ont été déterminés par cryo- MET combinée au marquage par des nanoparticules d’or conjuguées à des protéines. La quantification objective des VEs du plasma sanguin a été réalisée à l’aide d’une méthode originale de MET basée sur la sédimentation de VEs sur grille de MET. La troisième partie de cette étude a consisté à mettre au point une méthode d’isolation de VEs à l’aide de particules magnétiques conjuguées à de l’AnxA5. Des conditions permettant d’extraire la totalité des VEs exposant la phosphatidylsérine contenues dans un plasma sanguin ont été déterminées par cytométrie en flux (CF). Ce travail a permis d’apporter une caractérisation détaillée des VEs du plasma sanguin du sujet sain et peut servir de référence pour des études ultérieures concernant les VEs contenues dans des plasmas ou autres liquides biologiques pathologiques. / Extracellular vesicles (EVs) are submicrometric membrane vesicles found in body fluids and produced by cells in response to various stimuli. EVs are involved in numerous physiological processes but also in pathologies as cancers or cardiovascular diseases. Even if EVs are largely studied, our knowledge about them remains limited. This is mainly caused by the difficulties to characterize EVs and by the lack of standardized methods allowing their characterization. The first part of my PhD work focused on the development and optimization of a protein thiolation method. Antibodies modified to expose few thiols were conjugated to gold nanoparticles functionalized with maleimides. The binding of thiolated antibodies to gold nanoparticles was quantitatively studied and optimal conjugation conditions were determined using biochemical methods. The second part of my PhD work concerned the characterization of blood plasma EVs from healthy subjects using transmission electron microscopy (TEM). EVs morphology, size and phenotype were determined by cryo-TEM combined with labelling with protein-conjugated gold nanoparticles. The near-absolute quantification of blood plasma EVs was achieved using an original TEM method based on the direct sedimentation of EVs onto TEM grids. The third part of this study consisted in developing an EV isolation method using AnxA5-conjugated magnetic particles. Conditions allowing total extraction of blood plasma phosphatidylserine-exposing EVs were determined using flow cytometry (FC). This study presents a detailed characterization of blood plasma EVs from healthy subjects and can serve as a reference for future studies on EVs contained in pathological plasmas or other body fluids.

Vésicules extracellulaires

Plasma sanguin

Thiolation de protéines

Immunomarquage à l’or

Extraction magnétique

Annexine- A5

Phosphatidylsérine

Microscopie électronique

Cytométrie en flux

Extracellular vesicles

Blood plasma

Protein thiolation

Protein-conjugated gold nanoparticles

Immunogold labelling

Magnetic extraction

Annexin-A5

Phosphatidylserine

Electron microscopy

Flow cytometry

Assemblages 2D de l'Annexine A5 : Applications biotechnologiques & Aspects fonctionnels

Berat, Rémi

12 December 2007

L'Annexine A5 (Anx5) est une protéine de la famille des annexines qui présente la propriété de s'organiser à la surface des bicouches lipidiques en trimères et en assemblages bidimensionnels (2D) de trimères. Ce travail de thèse concerne le développement d'applications biotechnologiques des assemblages 2D d'Anx5 ainsi qu'une étude des propriétés fonctionnelles de ces assemblages. Ces travaux ont été réalisés principalement à l'aide des méthodes de la microbalance à cristal de quartz avec mesure de dissipation (QCM-D) et de la microscopie à force atomique (AFM). <br />La première partie de cette thèse concerne le développement de plates-formes d'ancrage basées sur des assemblages 2D de protéines dérivées de l'Anx5. Des complexes covalents entre l'Anx5 et des peptides d'adhésion cellulaire pour la réalisation de plates-formes d'ancrage de cellules. Des protéines de fusion entre l'Anx5 et un fragment de la protéine A ont d'autre part servi au développement de plates-formes 2D pour l'immobilisation contrôlée d'anticorps et de protéines. <br />La seconde partie de cette thèse concerne l'étude des propriétés fonctionnelles des assemblages 2D d'Anx5. L'étude de l'interaction d'un anticorps anti-phospholipide avec les assemblages 2D d'Anx5 montre que cet anticorps ne perturbe pas l'organisation 2D de l'Anx5. La seconde étude concernant l'influence des assemblages 2D de l'Anx5 sur la dynamique des bicouches lipidiques établie une corrélation entre la formation de trimères et le ralentissement de la dynamique des membranes.<br />Ces travaux contribuent à notre compréhension des propriétés des assemblages 2D d'Anx5 et permettent d'envisager le développement de biocapteurs pour cellules ou molécules.

Annexine A5

Bicouche lipidique supportée (SLB)

Microscopie à force atomique (AFM)

biocapteur

adhésion cellulaire

syndrome anti-phospholipide