Cd44-Hyaluronic Acid Interactions in Il-2 Induced Vascular Leak Syndrome

Mustafa, Amjad

02 July 2001

Immunotherapy with IL-2 is accompanied by severe toxicity leading to development of vascular leak syndrome (VLS). Previous studies from our laboratory demonstrated that CD44 knockout mice exhibit marked decrease in IL-2 induced VLS, thereby suggesting a role for CD44 in VLS. In the current study we tested whether use of mAbs against CD44 or hyaluronic acid (HA), the ligand for CD44, can abrogate IL-2 induced VLS. Administration of IL-2 (75,000 U/mouse, three times a day for 4 days) into C57BL/6 mice triggered significant VLS in the lungs and liver. Interestingly, HA caused a marked increase in IL-2-induced VLS in the lungs and liver. In contrast, use of anti-CD44 mAbs reduced IL-2-induced VLS in the lungs and liver. The change in VLS seen following HA or anti-CD44 mAbs treatment was not due to any defect in lymphocyte migration or homing to various organs because histopathological studies in these mice demonstrated significant and often greater perivascular infiltration of lymphocytes when compared to mice treated with IL-2 alone. However, HA treatment exhibited a marked increase in IL-2-induced lymphokine-activated killer (LAK) cell activity while anti-CD44 mAbs treatment led to a significant decrease in IL-2-induced LAK cell activity. These studies demonstrate that HA or anti CD44 mAbs may serve as a useful tool to selectively alter the LAK activity as well as to prevent the toxicity induced by IL-2. Altering CD44-HA interactions in vivo may offer a novel therapeutic approach to prevent endothelial cell injury by cytotoxic lymphocytes in a variety of clinical diseases. / Master of Science

Vascular Leak Syndrome

CD44

Hyaluronate

Role of CD44 in Immune Functions and Endothelial Cell Injury

Rafi-Janajreh, Asimah

02 October 1998

In addition to the antigen-specific receptors, the T and B cells also express a variety of adhesion molecules, which are known to participate in cell-cell interaction, migration, homing and signal transduction. CD44 is a widely distributed cell surface glycoprotein whose principal ligand has been identified as hyaluronic acid (HA), a major component of the extracellular matrix. In the current study, we investigated whether HA or mAbs against CD44 would induce a proliferative response in mouse lymphocytes. Spleen cells from normal and nude but not severe combined immunodeficient mice, exhibited strong proliferative responsiveness to stimulation with soluble HA or anti-CD44 mAbs. Furthermore, purified B cells but not T cells were found to respond to HA. These data demonstrated that interaction between HA and CD44 can regulate murine B cell effector functions and that such interactions may play a critical role during normal or autoimmune responsiveness of B cells. Endothelial cell injury resulting in vascular leak syndrome (VLS) is one of the most widely noted phenomenons in a variety of clinical diseases, however, the underlying reason for which remains unclear. We used interleukin-2 induced VLS as a model to investigate the role of cytolytic lymphocytes in the direct cytotoxicity of endothelial cells. BL/6 wild-type mice developed significant VLS in the lungs, liver and spleen following IL-2 administration. Interestingly, perforin-knockout mice exhibited marked decrease in VLS in all three organs tested. Also, FasL-defective (gld) mice and Fas-deficient (lpr) mice exhibited decreased VLS in the liver and spleen, but not in the lungs. These results demonstrated for the first time that perforin and FasL may actively participate in endothelial cell injury and induction of VLS in a variety of organs. Inasmuch as, CD44 also plays a major role in the lymphocyte adhesion to the endothelial cells, we used CD44-knockout mice and observed that such mice exhibited markedly diminished VLS following IL-2-treatment. Our data also suggested that blocking CD44 helps in reducing the IL-2-induced VLS and therefore such an approach may serve as a useful tool to prevent endothelial cell damage seen in a variety of clinical disorders. / Ph. D.

Vascular Leak Syndrome

Hyaluronate

CD44

Assemblages de copolymères à blocs pour la vectorisation de siRNA

Bui, Laurent

20 December 2011

Les « siRNA » sont des molécules double brin d’acide ribonucléique capables d’inhiber l’expression d’un gène spécifique, présentant ainsi un fort potentiel thérapeutique pour les maladies génétiques, les cancers et les infections virales. Cependant, son utilisation in vivo est restreinte par sa sensibilité à la dégradation enzymatique. Le projet de thèse consiste à créer un système de vectorisation des siRNA pour des applications in vivo. Nous avons synthétisé des copolymères à blocs amphiphiles biocompatibles et biodégradables capable de s’auto-assembler en diverses structures et d’encapsuler les siRNA. Les propriétés physico-chimiques des assemblages formées et l’évaluation cellulaire préliminaire est réalisée / Amphiphilic block copolymers are molecules composed of hydrophilic and hydrophobic segments having the capacity to spontaneously self-assemble into a variety of supramolecular structures like micelles and vesicles. Here, we propose an original way to self-assemble amphiphilic block copolymers into a supported bilayer membrane for defined coating of nanoparticles. The heart of the method rests on a change of the amphiphilicity of the copolymer that can be turned off and on by varying the polarity of the solvent. In this condition, the assembly process can take advantage of specific molecular interactions in both organic solvent and water. The higher gene silencing activity of the copolymer-modified complexes over the complexes alone shows the potential of this new type of nanoconstructs for biological applications, especially for the delivery of therapeutic biomolecules.

Copolymère

Amphiphile

Vectoristaion

SiRNA

Hyaluronate

Polysacharide

Copolymer

Amphiphilic

SiRNA

Fluorescently Labeled Sodium Hyaluronate: Synthesis, Characterization and Solution Properties

MacEwan Gracie, Kimberley D.

09 1900

<p> Fluorescence spectroscopy has been proven to be a useful technique for the investigation of the structural, physical and solution properties of polymers. A polymer system containing a photo physical probe can be investigated using fluorescence quenching and polarization. We have randomly labeled sodium hyaluronate (HA) chains with fluorescent dyes such as 1-(1-pyrenyl)methyl amine and N-ε-dansyl-L-lysine, and studied their physical, structural and solution properties, including interactions with surfactants using the above fluorescence techniques.</p> / Thesis / Master of Science (MSc)

DIFFERENTIATION OF NEURAL STEM CELL USING SMALL MOLECULES IN 2D AND 3D CULTURE SYSTEM

Shi, Xinglong

January 2015

The neuronal differentiation of neural stem cells (NSCs) has received much attention due to its potential for the treatment of neurodegenerative diseases (i.e., Parkinson’s and Alzheimer’s diseases). In this regard, discovering compounds that direct differentiation of NSCs is highly required to facilitate therapeutic applications. In this study, we examined various bioactive compounds (SA1, SA2, LiCl, compound B, and DHED) to induce the neuronal differentiation of human neural stem cells (hNSCs). The study was conducted on the cells grown in three dimensional (3D) hydrogel or two dimensional (2D) environment since 3D hydrogel mimics the extracellular matrix and provides physiologically more relevant environment than 2D cell culture system. Three-dimensional (3D) hydrogel systems in this study involve polysaccharides such as alginate and hyaluronic acid. Neuronal differentiation of hNSCs was monitored in genetic level and protein level by quantitative reverse transcription polymerase chain reaction (RT-qPCR) and immunocytochemistry (ICC), respectively. This study will show the effect of bioactive compounds on hNSCs differentiation in 2D and 3D culture systems. / Bioengineering

Engineering, Biomedical

Alginate

Differentiation

Hyaluronate

Neural Stem Cells

Peptide Amphiphile

Role of CD44, Fas Ligand, and Perforin in the Cytotoxicity Mediated by Natural Killer Cells

Bradley, Michael Joseph

16 June 1997

Two important mechanisms of lymphocyte-mediated cytotoxicity, one perforin based and the other Fas ligand (FasL) based, have been characterized recently. It has also been shown that CD44, an adhesion molecule, can participate in signaling cytotoxic activity of cytotoxic T lymphocytes (CTLs). In the current study we tested the hypothesis that activation of natural killer (NK) or lymphokine activated killer (LAK) cells induces the expression of FasL, perforin, and CD44 which together contribute towards increased cytolytic activity. To this effect, we used wild-type mice, perforin-knockout mice, and mice lacking a functional FasL. We observed that both interleukin-2 (IL-2) and Poly I:C triggered NK/LAK cells to lyse targets through the perforin- and FasL- pathways. In addition, Fas+ tumor targets were more susceptible to lysis by poly I:C and IL-2 activated NK/LAK cells when compared to Fas- targets. Furthermore, Fas- tumor cells injected subcutaneously into syngeneic mice could grow and induce tumors, whereas, Fas+ tumors were rejected. IL-2 treatment increased the CD44 expression on NK cells, which was responsible for the lysis of endothelial cells through its ligand, hyaluronate. Upregulation of perforin and FasL in activated NK/LAK cells may explain why such cells can kill a wide variety of tumor cells efficiently. On the other hand, activated NK/LAK cells express increase increased levels of CD44 and use this molecule to mediate cytotoxicity of endothelial cells, which may account for the vascular leak seen during IL-2 therapy. / Master of Science

Hyaluronate

Apoptosis

Natural Killer Cells

CD44

Perforin

Fas Ligand

Pokročilé mikroreologické techniky ve výzkumu hydrogelů / Advanced microrheological techniques in the research of hydrogels

Kábrtová, Petra

January 2017

This diploma thesis deals with the use of fluorescence correlation spectroscopy technique for microrheological characterization of hydrogel in a system of hyaluronate-cetyltrimethylammonium bromide. Fluorescently labelled particles were used for microrheological FCS analysis. To optimize the method the most appropriate size of particles was chosen on the basis of Newtonian glycerol solutions analysis. Among other things, the discussion was focused on the influence of refractive index change of analysed solutions on analysis results. After hyaluronate solutions analysis it was possible to assess the biopolymer concentration and molecular weight impact on the FCS microrheology results, which could then be compared with analysis results of model hydrogels of hyaluronate and CTAB. Finally, usability and limitations of FCS microrheology have been discussed.

Fluorescence ve výzkumu hydrofilních oblastí asociativních koloidů / Fluorescence study of hydrophilic domains of associating colloids

Londinová, Monika

January 2008

The properties of the hyaluronan were investigated by using different fluorescence probes, because hyaluronan is a hopeful carrier of an active matter in medicine and cosmetics. Selected fluorescence probes were: cationic acridine orange, Nile Blue A, methylene blue, amphiphilic 4-Di-2-ASP and anionic fluorescein. Except from fluorescence and absorption spectra of the probes were observed electrostatic and hydrophobic interactions as well. The probes in solvents with different polarity (MeOH, EtOH, DMSO) showed the bathochromic shift in the emission maximum and quenching of the fluorescence with the increasing polarity of the solvents. The influence of the ionic strength on fluorescence properties of the probe acridine orange and 4-Di-2-ASP was investigated in aqueous solutions of chlorides. The formation of acridine orange dimer is inhibited with increasing ionic strength. CaCl2 increased the ionic strength the most, then prevented repulsion of carboxylate groups, so it means the expansion of hyaluronan cluster into the solution. However, the emission of the probe 4-Di-2-ASP was quenched with the addition of CaCl2 the most. The first additions of COO– groups cause the formation of dimers of AO shown as decreasing in extinction coefficient and fluorescence intensity. Next addition of the hyaluronan caused a depolymerization of formed dimers and the increase of the emission intensity. The repolymerization caused the decrease and then again the increase. In case of 4-Di-2-ASP was the pattern of the fluorescence (the intensity and the position of the emission) firstly the same, but at the concentration of 1 g dm-3 the emission intensity increased. The probes MB and F were used for spectroscopic studies of the interaction between methylene blue-fluorescein complex and anionic and cationic surfactants. The absorbance of separate MB and F changed only with the addition of surfactants with the opposite electric charge. Absorbance of the mixture MB-F changed with the addition of the CTAC surfactant, while the addition of SDS into the mixture caused only the change of MB absorption spectra.

Etude et modulation du microenvironnement des purinorécepteurs de mort P2X7 par des formulations lipidiques et biopolymères afin de réguler les mécanismes de prolifération et de dégénérescence cellulaire sur des modèles dermatologiques : cicatrisation et mélanome / Study and modulation of P2X7 purinoceptors cell death microenvironment by lipid formulations and biopolymers to regulate the mechanisms of cell proliferation and degeneration of dermatological models : healing and melanoma

Ghazi, Kamelia

19 November 2012

Le purinorécepteur P2X7 joue un rôle majeur dans les phénomènes de dégénérescences (Alzheimer, DMLA) et mort cellulaires. Récemment des études ont montré que l’activation basale de ce récepteur est indispensable dans le processus de cicatrisation et de prolifération cellulaire. Nous avons essayé de mieux comprendre le paradoxe de cette activation du récepteur P2X7 qui oriente vers la prolifération et même les métastases tumorales, mais aussi vers les mécanismes de dégénérescence cellulaire. L'influence du microenvironnement (Lipides, matrice extracellulaire, oxygène) apparait essentielle pour comprendre ces différents effets. Notre premier objectif a été d’étudier l’impact de la modulation du microenvironnement du récepteur P2X7 par des composants de la matrice extracellulaire. Ainsi, sur un modèle de cicatrisation cutanée, nous avons mis en évidence l’impact de la taille des fragments du hyaluronate de sodium (composant prédominant dans la matrice extracellulaire). Nos résultats ont montré que l’activation du récepteur P2X7 dépend du poids moléculaire du hyaluronate de sodium. Notre deuxième objectif a été de moduler le microenvironnement lipidique du récepteur P2X7. Nous avons sélectionné une huile riche en acides gras insaturés et avons ainsi étudié son effet sur l’activation du récepteur P2X7. Sur nos modèles de cicatrisation, nous avons mis en évidence qu’une modulation du microenvironnement lipidique du récepteur P2X7 influence son activation. D’autre part la modulation du microenvironnement lipidique sur des cellules tumorale de mélanome active les voies de dégénérescence ouvrant la perspective de nouvelles stratégies thérapeutiques. / The purinoceptor P2X7 plays a role in cytotoxic degenerative processus (Alzheimer, AMD) and cell death. Recent studies have shown that basal activation of this receptor is essential in the healing process and cell proliferation. We tried to understand the paradox that activation of P2X7 receptor that directs to the same proliferation and tumor metastasis, but also to the mechanisms of cell degeneration. The influence of the microenvironment (lipids, extracellular matrix, oxygen) appears essential to understand these effects. Our first objective was to study the impact of the modulation of P2X7 receptor microenvironment by extracellular matrix components. On cell monolayer model of wound healing we have highlighted the impact hyaluronan molecular weight (predominant component in the extracellular matrix). Our results showed that activation of P2X7 receptor is dependent on hyaluronan molecular weight. Our second objective was to modulate lipid microenvironment P2X7 receptor. We selected an oil rich in unsaturated fatty acids and thus have studied its effect on the activation of P2X7 receptor. In our models of healing and melanoma cell, we have demonstrated that modulation of lipid microenvironment affects P2X7 activation.

Hyaluronate de sodium

Matrice extracellulaire

Microenvironnement

Lipides

In vitro

Récepteur P2X7

Cicatrisation

Mélanome

Hyaluronan

Extracellular matrix

Microenvironment

Lipids

In vitro

P2X7 receptor

Wound healing

Melanoma

616.55

Reologie jakožto účinný nástroj ke komplexní charakterizaci hydrogelových systémů / Rheology as a powerful tool for the complex characterization of hydrogels

Kadlec, Martin

January 2020

This diploma thesis investigates the suitability of relaxation tests as a part of complex characterization of hydrogel materials using classical rheology methods. With respect to the current research, creep and three interval thixotropy tests were taken into account. For them, general optimization was done aiming to find an ideal parameter settings. The optimization was performed using physically crosslinked agarose (AG) hydrogel and the tuned tests were also applied to two more samples: hyaluronan (HyA) and polyvinyl alcohol (PVAl) gel. These materials were selected due to their mutually different crosslinking principle. The experiments showed, the AG gel proved to have the best ability to recover after deformation of all studied samples. On the other hand, the HyA gel relaxed the worst. Although the final results of both tests were comparable, the regeneration process itself was different. Hence, the complex relaxation characteristics cannot be described using one of the performed tests alone and both the creep and three interval thixotropy tests have great importance in the scope of complex relaxation behaviour. The obtained results may lead to more precise description of deformation and relaxation, which are frequent phenomena occurring during treatment and application of hydrogel materials.