Étude de la tomodensitométrie spectrale quantitative et ses applications en radiothérapie

Simard, Mikaël

02 1900

La tomodensitométrie par rayons-X (CT) est une modalité d’imagerie produisant une carte tridimensionnelle du coefficient d’atténuation des rayons-X d’un objet. En radiothérapie, le CT fournit de l’information anatomique et quantitative sur le patient afin de permettre la planification du traitement et le calcul de la dose de radiation à livrer. Le CT a plusieurs problèmes, notamment (1) une limitation au niveau de l’exactitude des paramètres physiques quantitatifs extraits du patient, et (2) une sensibilité aux biais causés par des artéfacts de durcissement du faisceau. Enfin, (3) dans le cas où le CT est fait en présence d’un agent de contraste pour améliorer la planification du traitement, il est nécessaire d’effectuer un deuxième CT sans agent de contraste à des fins de calcul de dose, ce qui augmente la dose au patient. Ces trois problèmes limitent l’efficacité du CT pour certaines modalités de traitement qui sont plus sensibles aux incertitudes comme la protonthérapie. Le CT spectral regroupe un ensemble de méthodes pour produire plusieurs cartes d’atténuation des rayons-X moyennées sur différentes plages énergétiques. L’information supplémentaire, pondérée en énergie qui est obtenue permet une meilleure caractérisation des matériaux analysés. Le potentiel de l’une de ces modalités spectrales, le CT bi-énergie (DECT), est déjà bien démontré en radiothérapie, alors qu’une approche en plein essor, le CT spectral à comptage de photons (SPCCT), promet davantage d’information spectrale à l’aide de détecteurs discriminateurs en énergie. Par contre, le SPCCT souffre d’un bruit plus important et d’un conditionnement réduit. Cette thèse investigue la question suivante : y a-t-il un bénéfice à utiliser plus d’information résolue en énergie, mais de qualité réduite pour la radiothérapie ? La question est étudiée dans le contexte des trois problèmes ci-haut. Tout d’abord, un estimateur maximum a posteriori (MAP) est introduit au niveau de la caractérisation des tissus post-reconstruction afin de débruiter les données du CT spectral. L’approche est validée expérimentalement sur un DECT. Le niveau de bruit du pouvoir d’arrêt des protons diminue en moyenne d’un facteur 3.2 à l’aide de l’estimateur MAP. Celui-ci permet également de conserver généralement le caractère quantitatif des paramètres physiques estimés, le pouvoir d’arrêt variant en moyenne de 0.9% par rapport à l’approche conventionnelle. Ensuite, l’estimateur MAP est adapté au contexte de l’imagerie avec agent de contraste. Les résultats numériques démontrent un bénéfice clair à utiliser le SPCCT pour l’imagerie virtuellement sans contraste par rapport au DECT, avec une réduction de l’erreur RMS sur le pouvoir d’arrêt des protons de 2.7 à 1.4%. Troisièmement, les outils développés ci-haut sont validés expérimentalement sur un micro-SPCCT de la compagnie MARS Bioimaging, dont le détecteur à comptage de photons est le Medipix 3, qui est utilisé pour le suivi de particules au CERN. De légers bénéfices au niveau de l’estimation des propriétés physiques à l’aide du SPCCT par rapport au DECT sont obtenus pour des matériaux substituts à des tissus humains. Finalement, une nouvelle paramétrisation du coefficient d’atténuation pour l’imagerie pré-reconstruction est proposée, dans le but ultime de corriger les artéfacts de durcissement du faisceau. La paramétrisation proposée élimine les biais au niveau de l’exactitude de la caractérisation des tissus humains par rapport aux paramétrisations existantes. Cependant, aucun avantage n’a été obtenu à l’aide du SPCCT par rapport au DECT, ce qui suggère qu’il est nécessaire d’incorporer l’estimation MAP dans l’imagerie pré-reconstruction via une approche de reconstruction itérative. / X-ray computed tomography (CT) is an imaging modality that produces a tridimensional map of the attenuation of X-rays by the scanned object. In radiation therapy, CT provides anatomical and quantitative information on the patient that is required for treatment planning. However, CT has some issues, notably (1) a limited accuracy in the estimation of quantitative physical parameters of the patient, and (2) a sensitivity to biases caused by beam hardening artifacts. Finally, (3) in the case where contrast-enhanced CT is performed to help treatment planning, a second scan with no contrast agent is required for dose calculation purposes, which increases the overall dose to the patient. Those 3 problems limit the efficiency of CT for some treatment modalities more sensitive to uncertainties, such as proton therapy. Spectral CT regroups a set of methods that allows the production of multiple X-ray attenuation maps evaluated over various energy windows. The additional energy-weighted information that is obtained allows better material characterization. The potential of one spectral CT modality, dual-energy CT (DECT), is already well demonstrated for radiation therapy, while an upcoming method, spectral photon counting CT (SPCCT), promises more spectral information with the help of energy discriminating detectors. Unfortunately, SPCCT suffers from increased noise and poor conditioning. This thesis thus investigates the following question: is there a benefit to using more, but lower quality energy-resolved information for radiotherapy? The question is studied in the context of the three problems discussed earlier. First, a maximum a posteriori (MAP) estimator is introduced for post-reconstruction tissue characterization for denoising purposes in spectral CT. The estimator is validated experimentally using a commercial DECT. The noise level on the proton stopping power is reduced, on average, by a factor of 3.2 with the MAP estimator. The estimator also generally con- serves the quantitative accuracy of estimated physical parameters. For instance, the stopping power varies on average by 0.9% with respect to the conventional approach. Then, the MAP estimation framework is adapted to the context of contrast-enhanced imaging. Numerical results show clear benefits when using SPCCT for virtual non-contrast imaging compared to DECT, with a reduction of the RMS error on the proton stopping power from 2.7 to 1.4%. Third, the developed tools are validated experimentally on a micro-SPCCT from MARS Bioimaging, which uses the Medipix 3 chip as a photon counting detector. Small benefits in the accuracy of physical parameters of tissue substitutes materials are obtained. Finally, a new parametrization of the attenuation coefficient for pre-reconstruction imaging is pro- posed, whose ultimate aim is to correct beam hardening artifacts. In a simulation study, the proposed parametrization eliminates all biases in the estimated physical parameters of human tissues, which is an improvement upon existing parametrizations. However, no ad- vantage has been obtained with SPCCT compared to DECT, which suggests the need to incorporate MAP estimation in the pre-reconstruction framework using an iterative reconstruction approach.

Tomodensitométrie par rayons-X

Tomodensitométrie multi-énergie

Radiothérapie

Tomodensitométrie spectrale

Détecteur à comptage de photons

Protonthérapie

Imagerie par agents de contraste

Imagerie virtuellement sans contraste

MARS Bioimaging

Medipix 3

X-ray computed tomography

Multi-energy computed tomography

Radiation therapy

Spectral computed tomography

Photon counting detector

Proton therapy

Contrast-enhanced imaging

Virtual non-contrast imaging

MARS Bioimaging

Medipix 3

Structural integrity of highly ionized peptides

Eliah Dawod, Ibrahim

January 2019

In order to understand the behaviour and function of proteins, their three dimensional structure needs to be known. Determination of macro-molecules’ structures is done using X-ray diffraction or electron microscopy, where the resulting diffraction pattern is used for molecular reconstruction. These methods are however limited by radiation damage.The aim of this work is to study radiation damage of peptides in proteins using computer simulations. Increased understanding of the atomic and molecular dynamics can contribute to an improvement of the method ofimaging biological molecules. To be able to describe the processes that take place as accurately as possible, the problem must treated quantum mechanically.Thus, the simulations are performed with molecular dynamics based on first principles. In order to capture the dynamics of the excited states of the molecule when exposed to X-rays, time-dependent density functional theory with delta self-consistent field is used. These simulations are compared to ground state simulations. The results of the thesis conclude that the excited and ground state simulations result in differences in the dynamics, which are most pronounced for lager molecules.

X-ray free-electron laser

X-ray imaging

XFEL

Computer simulations

Radiation damage

Ab-initio molecular dynamics

DFT

TDDFT

Excited states

Femtosecond

Bioimaging

Atom and Molecular Physics and Optics

Atom- och molekylfysik och optik

Interação de pontos quânticos com fotossensibilizadores orgânicos na presença de estruturas nano-organizadas / Interaction of quantum dots with organic photosensitizers in the presence of nano-organized structures

Parra, Gustavo Gimenez

19 January 2015

O sucesso de tratamento de câncer depende do seu diagnóstico e tratamento nas etapas iniciais da doença. Isso estimula a busca de novos métodos de diagnóstico e de tratamento sensíveis e tecnicamente simples. Entre esses métodos, o diagnóstico por fluorescência (DPF) e a fotoquimioterapia (FQT) atraem uma atenção especial, sendo não invasivos, sensíveis e fácil de usar. Os fotossensibilizadores (FS) atualmente utilizados em DPF e FQT são corantes orgânicos, os quais possuem algumas desvantagens, tais como instabilidade fotoquímica e baixa seletividade. Os pontos quânticos (PQ) são candidatos promissores para substituírem os FS clássicos por serem fotoestáveis, apresentarem amplo e intenso espectro de absorção óptica e luminescência com alto rendimento quântico. Contudo a iteração entre FS clássicos e os PQ pode aumentar a eficiência de ambos devido a transferência de energia entre eles. O objetivo geral deste trabalho foi estudar os processos da interação de FS orgânicos (as porfirinas PPh, TMPyP e TPPS4) com PQs (CdTe e CdSe/ZnS), funcionalizados com diferentes grupos, em solução aquosa e na presença de modelos nano-organizados de estruturas biológicas com a finalidade de avaliar seu potencial para aplicação em Fotoquimioterapia e Diagnóstico por Fluorescência. Dedicamos especial atenção aos processos de transferência de energia e de carga entre os PQs e os FS. Os PQs interagem efetivamente com as PPh, cuja interação se manifesta pelas mudanças da intensidade e do perfil dos espectros e das curvas de decaimento da luminescência de PQ e da porfirina, do tamanho das partículas espalhadoras na solução, do potencial zeta dentre outros parâmetros espectroscópicos e físico-químicos. Dentro das soluções aquosas homogêneas, o PQ e as PPh podem formar agregados mistos (PQ&PPh&PQ) ou simples (PQ&PPh) e a interação entre eles realiza-se através de mecanismos de curto e/ou longo alcance, dependendo do grupo funcional do PQ. Entretanto, a interação eletrostática repulsiva entre o PQ e outro composto pode estimular a desagregação dos PQs induzindo o aumento na intensidade da sua luminescência e do seu tempo de vida, provocando um aumento na contribuição dos tempos longos do decaimento da luminescência associados com a superfície do PQ. Essas relações entre o tipo de interação do PQ e da PPh podem ser extrapoladas aos sistemas que contêm PQ na presença de estruturas nano-organizadas. / The success of cancer treatment depends on the diagnosis and treatment in the early stages of the disease. This stimulates the research for new methods of sensitive diagnosis and technically simple treatment. Among these methods, the Optical Bioimaging by fluorescence (OBI) and Photochemotherapy (PCT) attract special attention, being non-invasive, sensitive and friendly use. The photosensitizers (PS) currently used in the OBI-PCT are organic dyes, which have some drawbacks such as photochemical instability and low selectivity. Quantum Dots (QD) are promising candidates to replace the classic PS being photostable, present broad and intensive spectrum of optical absorption and luminescence and, high quantum yield. Therefore the interaction between QDPS and the classic PS can increase the efficiency of both due to energy transfer between them. The aim of this work was to study the processes of organic PS interaction (porphyrins PPh, TMPyP and TPPS4) with QDs (CdTe and CdSe/ZnS), functionalized with different groups in aqueous solution and in the presence of nano-organized models of biological structures with order to evaluate its potential for use in Photochemotherapy and Optical Bioimaging. We devote special attention to energy transfer processes and cargo between the QDs and PS. The QDs effectively interact with PPh, whose interaction is manifested by changes in the intensity and profile of spectra and luminescence decay curves of QD and the porphyrin, the linear size of the scattering particles in the solution, the zeta potential among other spectroscopic and physical chemistry parameters. Within the homogeneous aqueous solutions, QD and Pph can form mixed aggregates (QD&PPh&QD) or simple (QD&PPh) and the interaction between them is carried out through short mechanisms and/or long range, depending on the functional group of the QD. However, the repulsive electrostatic interaction between the QD and another compound may stimulate the breakdown of QDs inducing the increase in the intensity of their luminescence and its lifetime, causing an increase in the contribution of long time decay of the luminescence associated with the surface of QD. These relationships between the type of interaction of the QD and PPh can be extrapolated to systems containing QD in the presence of nano-organized structures.

Charge transfer

Energy transfer

Fotossensibilizador orgânico

Nano-organized system

Photochemotherapy and Optical bioimaging

Photosensitizer

Ponto quântico

Quantum Dots

Sistema biomimético nano-organizado

Transferência de carga

Transferência de energia

Matériaux Hybrides nanostructures photoactifs pour des applications optiques et biomédicales / Photoactive Nanostructured Hybrid Materials for Optical and Biomedical Applications

Epelde Elezcano, Nerea

20 May 2016

Dans ce manuscrit, la synthèse et la caractérisation complète de différents matériaux hybrides dédiés à des applications dans le domaine optique ou thérapeutique sont décrites. Dans un premier temps, des systèmes macroscopiquement ordonnés sont obtenus par intercalation de colorants tels que le Styryl 722 ou la pyronine-Y dans plusieurs films à base d’argile de type smectite. Les films d’argile sont élaborés par spin-coating et les colorants intercalés par immersion des films dans les solutions de ces colorants. Les effets de l’argile sur les propriétés des colorants sont analysés en détail et leur orientation préférentielle dans l’espace inter-couches est étudié grâce à la réponse anisotropique des films en lumière linéairement polarisée. Dans la deuxième partie, la synthèse par chimie sol-gel de monolithes de silice de grande dimension contenant des colorants laser présentant une forte absorption et une émission de fluorescence dans le visible est abordée. Des colorants laser à l’état solide (SSDL) avec de bonnes stabilités photochimique, thermique et chimique sont ainsi proposés. Dans le troisième chapitre, la synthèse par voie sol-gel de nanoparticules de silice (NP) d’environ 50 nm de diamètre fonctionnalisées sur leur surface externe est ensuite décrite. Grâce à l’encapsulation de molécules de colorants fluorescents dans leur cœur et le greffage de photosensibilisateurs sur leur écorce, des nanoparticules biocompatibles adaptées à la bio-imagerie et la thérapie photodynamique (PDT) ont été préparées. Pour optimiser leurs performances, les propriétés photophysiques et plus particulièrement la production d’oxygène singulet d’une nouvelle série de photosensibilisateurs basés sur les chromophores de type PODIPY ont d’abord été étudiées en détail. A partir de ces résultats, des BODIPY particulièrement efficaces ont été greffés sur les nanoparticules de silice afin de les utiliser pour la PDT. Les propriétés photophysiques de ces matériaux ont été analysées par spectroscopie d’absorption et de fluorescence (stationnaire ou résolue en temps) et les rendements quantiques de production d’oxygène singulet déterminés par des méthodes directe (émission de luminescence de l’oxygène singulet à 1270 nm) ou indirecte (utilisation de sondes chimiques spécifiques à l’oxygène singulet). Par ailleurs les matériaux hybrides ont été complètement caractérisés par plusieurs techniques (SEM, TEM, XRD, XPS, IR, DLS, BET). / Along this manuscript different hybrid materials are synthesized and extensively characterized for several uses: from optical to therapeutic applications. First, by the intercalation of different dyes, styryl 722 and pyronine-Y into several smectite clay films, macroscopically ordered system are obtained. Clay films are elaborated by spin-coating technique and the dyes are intercalated by the immersion of clay thin films into dye solutions. The effect of clay on the dye properties is deeply analyzed and its preferential orientation in the interlayer space of the clay is studied by the anisotropic response of the films to the linear polarized light. Second, large silica monoliths with embedded laser dyes with strong absorption and fluorescence bands in different region of the Visible spectrum are attained by sol-gel chemistry to obtain solid-state dye laser (SSDL) with good photo, thermal and chemical stabilities. Third, silica nanoparticles (NP) with suitable size (50 nm) and functionalized external surface are also synthesised by sol-gel chemistry. Through the encapsulation of fluorescent dye molecules in their core and by the grafting of photosensitizers on their shell, biocompatible nanoparticles for bio-imaging and Photodynamic Therapy (PDT) applications are prepared. In order to optimize their properties, a careful investigation of the photophysical properties and mainly the singlet oxygen generation of a large range of new photosensitizers based on chromophores known as BODIPYs, is previously carried out. Based on these results, some efficient BODIPYs are selected for grafting on silica nanoparticles in order to use them for PDT. The photophysical properties of all these hybrid materials are analyzed by absorption and fluorescence (steady-state and time correlated) spectroscopies, and the singlet oxygen measurements are monitored by direct method (recording the singlet oxygen luminescence at 1270 nm) and by indirect method (using selective chemical probe). Moreover, the hybrid materials are fully characterized by several techniques such as, SEM, TEM, XRD, XPS, IR, DLS, BET.

Matériaux hybrides

Colorants laser

, Photosensibilisateurs

Nanoparticules de silice

Thérapie Photodynamique

Minéraux argileux

Bio-imagerie

Monolithes de silice

Oxygène singulet

Photophysique

Calculs théoriques

Hybrid materials

Laser dyes

Photosensitizer

Silica nanoparticle

Photodynemic Therapy

Bioimaging

Clay minerals

Silica Monoliths

Singlet oxygen

Photophysics

Theoretical calculations

Nanotubes de carbonne ultracourts pour la bioimagerie / Ultrashort carbon nanotubes for bioimaging applications

Faes, Romain

18 February 2014

Les travaux de recherche effectués lors de cette thèse portent sur l’obtention de nanotubes de carbone ultracourts et leur biofonctionnalisation pour une utilisation comme biomarqueur proche infrarouge. Des dispersions de nanotubes de carbone en milieux aqueux ont été formulées à l’aide de différents tensioactifs. Un traitement chimique oxydant préalable et/ou l’application d’ultrasons aux nanotubes ont permis de réduire leur longueur de façon significative, la sélection des plus courts étant effectuée par ultracentrifugation en gradient de densité. Les différentes fractions sélectionnées à l’issu de ce processus ont été caractérisées par spectroscopie Raman et spectroscopie d’absorption ainsi que par microscopie à force atomique. Il est ainsi montré la sélection de nanotubes d’une longueur inférieure à 20 nm. Nous montrons également leur fonctionnalisation à l’aide d’anticorps monoclonaux et leur visualisation par imagerie photothermique hétérodyne. Des résultats prometteurs ont été obtenus avec la fixation spécifique de nanotubes de carbone ultracourts sur des cellules. Ces travaux ouvrent de nombreuses perspectives en bioimagerie et en particulier l’étude de la plasticité synaptique au sein de neurones vivants. / This thesis reports the achievement of ultrashort carbon nanotubes and their biofunctionalization for applications as near-infrared biomarker. Dispersions of carbon nanotubes in aqueous media have been formulated with various surfactants. Oxidizing chemical treatments combined with the application of ultrasounds allowed significant shortening of the carbon nanotubes. Sorting and selection of the shortest nanotubes was done by density gradient ultracentrifugation. The different fractions selected at the end of this process have been characterized by Raman spectroscopy, UV-vis absorption spectroscopy and atomic force microscopy. Selection of nanotubes of a length below 20 nm is demonstrated. We also show functionalization by antibodies and the visualization of ultrashort functionalized nanotubes by photothermal heterodyne imaging. Promising results were obtained with the specific binding of ultrashort carbon nanotubes to cells. This work open route towards bioimaging applications and in particular towards the study of the synapsis plasticity within alive neurons.

Nanotubes de carbone

Ultracourts

Bioimagerie

Dispersion

Imagerie photothermique hétérodyne

Microscopie à force atomique

Spectroscopie d’absorption

Spectroscopie Raman

Traitement chimique oxydant

Biofonctionnalisation

Carbon nanotubes

Ultrashort

Bioimaging

Dispersion

Photothermal heterodyne imaging

Atomic force microscopy

Absorption spectroscopy

Raman spectroscopy

Oxidizing chemical treatment

Biofunctionalization

DIFFUSE OPTICAL MEASUREMENTS OF HEAD AND NECK TUMOR HEMODYNAMICS FOR EARLY PREDICTION OF CHEMO-RADIATION THERAPY OUTCOMES

Dong, Lixin

01 January 2015

Chemo-radiation therapy is a principal modality for the treatment of head and neck cancers, and its efficacy depends on the interaction of tumor oxygen with free radicals. In this study, we adopted a novel hybrid diffuse optical instrument combining a commercial frequency-domain tissue oximeter (Imagent) and a custom-made diffuse correlation spectroscopy (DCS) flowmeter, which allowed for simultaneous measurements of tumor blood flow and blood oxygenation. Using this hybrid instrument we continually measured tumor hemodynamic responses to chemo-radiation therapy over the treatment period of 7 weeks. We also explored monitoring dynamic tumor hemodynamic changes during radiation delivery. Blood flow data analysis was improved by simultaneously extracting multiple parameters from one single autocorrelation function curve measured by DCS. Patients were classified into two groups based on clinical outcomes: a complete response (CR) group and an incomplete response (IR) group with remote metastasis and/or local recurrence within one year. Interestingly, we found human papilloma virus (HPV-16) status largely affected tumor homodynamic responses to therapy. Significant differences in tumor blood flow index (BFI) and reduced scattering coefficient (μs’) between the IR and CR groups were observed in HPV-16 negative patients at Week 3. Significant differences in oxygenated hemoglobin concentration ([HbO2]) and blood oxygen saturation (StO2) between the two groups were found in HPV-16 positive patients at Week 1 and Week 3, respectively. Receiver operating characteristic curves were constructed and results indicated high sensitivities and specificities of these hemodynamic parameters for early (within the first three weeks of the treatment) prediction of one-year treatment outcomes. Measurement of tumor hemodynamics may serve as a predictive tool allowing treatment selection based on biologic tumor characteristics. Ultimately, reduction of side effects in patients not benefiting from radiation treatment may be feasible.

near-infrared

diffuse optics

head and neck cancer

papilloma virus status

radiation therapy

tumor hemodynamics

prediction of treatment outcomes

Bioimaging and Biomedical Optics

Biomedical Devices and Instrumentation

Biostatistics

Synthesis of fluorescent organic nanoparticles for biological applications / Synthèse de nanoparticules organiques fluorescentes en vue d'applications biologiques

Shulov, Ievgen

05 January 2016

Boîtes quantiques (QDs) et nanoparticules fluorescentes de silice (NPs) ont influencé le domaine de la bioimagerie de par leur forte luminosité et photostabilité. Par rapport aux QDs, les NPs organiques peuvent s’avérer être encore plus brillantes et entièrement biodégradables, avec une bonne biocompatibilité et sans contenir aucun élément toxique. Nous avons développé quatre types de ces NPs : en premier, des nano-gouttelettes lipidiques chargées de colorants lipophiles (flavone et Nil Rouge) pour l'imagerie in vivo chez le poisson zèbre ; en second, l’association ionique entre rhodamine B alkylée et tétraphénylborate fluoré (TPB) donne des NPs de 11-20 nm avec un rendement quantique de ~60% ; une troisième type de NPs consiste en des micelles de 7 nm obtenus par co-assemblage de cyanine amphiphiles et contre-ions TPB ; enfin, la polymérisation de micelles de calix[4]arène par agents de réticulation bi-fonctionnels à base de cyanine donne des NPs de 7 nm présentant un comportement fluorogène et une bonne stabilité en milieu intracellulaire. Ces NPs plus brillantes et de taille inférieure aux QDs apparaissent comme des outils prometteurs en bioimagerie. / Quantum dots (QDs) and fluorescent silica nanoparticles (NPs) have impacted the domain of bioimaging by their high brightness and robust photostability. In comparison to QDs, organic NPs can be even brighter and fully biodegradable, as well biocompatible and not containing toxic elements inside. Herein, we developed four types of these NPs. At first, lipid nano-droplets loaded with lipophilic flavone and Nile Red dyes for in vivo imaging in zebrafish; second, ion-association of alkyl rhodamine B with fluorinated tetraphenylborate (TPB) counterions result in 11-20 nm NPs with fluorescence quantum yield up to 60%; third, 7 nm micellar NPs obtained by co-assembly of cyanine amphiphiles with TPB counterions; finally, polymerization of calix[4]arene micelles using bi-functional cyanine crosslinkers giving 7 nm NPs, that show fluorogenic behavior and high intracellular stability. These NPs, being of smaller size and brighter than QDs, have emerged as promising tools for bioimaging.

Nanoparticules organiques

Fluorescence

Auto-assemblage

Calix[4]arène

Imagerie biologique

Contre-ion

Stabilité colloïdale

Transfert d'énergie

Organic nanoparticles

Fluorescence

Self-assembly

Calix[4]arene

Bioimaging

Counterion

Colloidal stability

Energy transfer

571.4

547.2

Interação de pontos quânticos com fotossensibilizadores orgânicos na presença de estruturas nano-organizadas / Interaction of quantum dots with organic photosensitizers in the presence of nano-organized structures

Gustavo Gimenez Parra

19 January 2015

O sucesso de tratamento de câncer depende do seu diagnóstico e tratamento nas etapas iniciais da doença. Isso estimula a busca de novos métodos de diagnóstico e de tratamento sensíveis e tecnicamente simples. Entre esses métodos, o diagnóstico por fluorescência (DPF) e a fotoquimioterapia (FQT) atraem uma atenção especial, sendo não invasivos, sensíveis e fácil de usar. Os fotossensibilizadores (FS) atualmente utilizados em DPF e FQT são corantes orgânicos, os quais possuem algumas desvantagens, tais como instabilidade fotoquímica e baixa seletividade. Os pontos quânticos (PQ) são candidatos promissores para substituírem os FS clássicos por serem fotoestáveis, apresentarem amplo e intenso espectro de absorção óptica e luminescência com alto rendimento quântico. Contudo a iteração entre FS clássicos e os PQ pode aumentar a eficiência de ambos devido a transferência de energia entre eles. O objetivo geral deste trabalho foi estudar os processos da interação de FS orgânicos (as porfirinas PPh, TMPyP e TPPS4) com PQs (CdTe e CdSe/ZnS), funcionalizados com diferentes grupos, em solução aquosa e na presença de modelos nano-organizados de estruturas biológicas com a finalidade de avaliar seu potencial para aplicação em Fotoquimioterapia e Diagnóstico por Fluorescência. Dedicamos especial atenção aos processos de transferência de energia e de carga entre os PQs e os FS. Os PQs interagem efetivamente com as PPh, cuja interação se manifesta pelas mudanças da intensidade e do perfil dos espectros e das curvas de decaimento da luminescência de PQ e da porfirina, do tamanho das partículas espalhadoras na solução, do potencial zeta dentre outros parâmetros espectroscópicos e físico-químicos. Dentro das soluções aquosas homogêneas, o PQ e as PPh podem formar agregados mistos (PQ&PPh&PQ) ou simples (PQ&PPh) e a interação entre eles realiza-se através de mecanismos de curto e/ou longo alcance, dependendo do grupo funcional do PQ. Entretanto, a interação eletrostática repulsiva entre o PQ e outro composto pode estimular a desagregação dos PQs induzindo o aumento na intensidade da sua luminescência e do seu tempo de vida, provocando um aumento na contribuição dos tempos longos do decaimento da luminescência associados com a superfície do PQ. Essas relações entre o tipo de interação do PQ e da PPh podem ser extrapoladas aos sistemas que contêm PQ na presença de estruturas nano-organizadas. / The success of cancer treatment depends on the diagnosis and treatment in the early stages of the disease. This stimulates the research for new methods of sensitive diagnosis and technically simple treatment. Among these methods, the Optical Bioimaging by fluorescence (OBI) and Photochemotherapy (PCT) attract special attention, being non-invasive, sensitive and friendly use. The photosensitizers (PS) currently used in the OBI-PCT are organic dyes, which have some drawbacks such as photochemical instability and low selectivity. Quantum Dots (QD) are promising candidates to replace the classic PS being photostable, present broad and intensive spectrum of optical absorption and luminescence and, high quantum yield. Therefore the interaction between QDPS and the classic PS can increase the efficiency of both due to energy transfer between them. The aim of this work was to study the processes of organic PS interaction (porphyrins PPh, TMPyP and TPPS4) with QDs (CdTe and CdSe/ZnS), functionalized with different groups in aqueous solution and in the presence of nano-organized models of biological structures with order to evaluate its potential for use in Photochemotherapy and Optical Bioimaging. We devote special attention to energy transfer processes and cargo between the QDs and PS. The QDs effectively interact with PPh, whose interaction is manifested by changes in the intensity and profile of spectra and luminescence decay curves of QD and the porphyrin, the linear size of the scattering particles in the solution, the zeta potential among other spectroscopic and physical chemistry parameters. Within the homogeneous aqueous solutions, QD and Pph can form mixed aggregates (QD&PPh&QD) or simple (QD&PPh) and the interaction between them is carried out through short mechanisms and/or long range, depending on the functional group of the QD. However, the repulsive electrostatic interaction between the QD and another compound may stimulate the breakdown of QDs inducing the increase in the intensity of their luminescence and its lifetime, causing an increase in the contribution of long time decay of the luminescence associated with the surface of QD. These relationships between the type of interaction of the QD and PPh can be extrapolated to systems containing QD in the presence of nano-organized structures.

Fotossensibilizador orgânico

Ponto quântico

Sistema biomimético nano-organizado

Transferência de carga

Transferência de energia

Charge transfer

Energy transfer

Nano-organized system

Photochemotherapy and Optical bioimaging

Photosensitizer

Quantum Dots

Organic-inorganic composite materials for specific recognition and optical detection of environmental, food and biomedical analytes / Matériaux composites organiques-inorganiques pour la reconnaissance spécifique et la détection optique des analytes environnementaux, alimentaires et biomédicaux

Panagiotopoulou, Maria

09 December 2016

Cette thèse décrit l'état de l'art des sondes et nanoparticules fluorescents traditionnels utilisés en imagerie de fluorescence ainsi que le développement de nouveaux nanomatériaux à base de polymère à empreinte moléculaire, aussi dénommé ‘anticorps plastique’, pour le ciblage et la bioimagerie. En biologie et en médecine, il y a un besoin constant de diagnostiquer diverses maladies pour leur éventuel traitement et prévention. Une distribution anormale et un taux élévé de glycosylation (e.g. acides hyaluronique et sialique) à la surface ou dans les cellules sont indicateurs d’une infection ou d’un cancer. Généralement, l’imagerie par fluorescence permet de visualiser, localiser et quantifier les biomarqueurs de pathologie mais à l’heure actuelle, il n’existe pas d’outil analytique fiable pour cibler spécifiquement les molécules de glycosylation car les anticorps et les lectines vendus dans le commerce ont une faible affinité et sélectivité vis-à-vis de ces cibles. Dans ce contexte, les polymères à empreintes moléculaires (MIPs) pourraient apporter une solution. Les MIPs sont des récepteurs synthétiques possédant des affinités et sélectivités comparables à ceux des anticorps, mais exhibant une stabilité physique, thermique et chimique bien plus accrue. De plus, leur fabrication est peu coûteuse et ne nécessite pas de tuer des animaux comme pour l’obtention des anticorps biologiques. Dans cette thèse, nous avons optimisé et synthétisé des MIPs biocompatibles pour leur utilisation en bioimagerie afin de détecter et quantifier l’acide hyaluronique et l’acide sialique sur les cellules et les tissus de peau humaine. L’acide glucuronique, une composante de l’acide hyaluronique et l’acide N-acétylneuraminique, l’acide sialique le plus commun, ont été utilisés comme molécules ‘patron’, générant des MIPs très sélectifs envers leur cible en milieu aqueux. Deux types de nanoparticules de MIPs fluorescents ont été synthétisés: (1) en incorporant un colorant rhodamine polymérisable dans la solution de pré-polymérisation et (2) en encapsulant des boîtes quantiques InP/ZnS générant ainsi des MIPs de type cœur-coquille. Pour cela, nous avons adopté une stratégie innovante qui consiste à synthétiser les coquilles de MIPs directement autour des boîtes quantiques en utilisant l’énergie de l’onde fluorescente émise par l’excitation des points quantiques, pour initier la polymérisation. Un protocole d'immunocoloration standard a ensuite été optimisé afin d’imager des kératinocytes humains fixés et vivants ainsi que des tissus de peau, par microscopie à épifluorescence et confocale. Les résultats étaient similaires à ceux obtenus par la méthode de référence utilisant une protéine biotinylée reconnaissant l'acide hyaluronique. L'imagerie multiplex en combinant deux MIPs couplés à deux couleurs de boîtes quantiques et l’imagerie des cellules cancéreuses ont également été démontrées. Bien que les MIPs n’étaient pas cytotoxiques aux concentrations utilisées pour la bioimagerie, la toxicité des différentes composantes du MIP pourrait être un frein à leur utilisation dans le domaine biomédical. Afin de rendre ces MIPs plus ‘inoffensifs’, nous avons supprimé l’amorceur de polymérisation, une molécule considérée comme toxique. Les MIPs ont été synthétisés en employant des monomères qui s’auto-initient sous l’effet de l’UV ou de la chaleur. La spécificité et la sélectivité des MIPs obtenus étaient similaires à ceux préparés avec des amorceurs. En conclusion, cette thèse décrit la première utilisation des MIPs comme anticorps synthétique pour la bioimagerie de fluorescence. Ce travail ouvre la voie à de nouvelles applications en détection, diagnostique et thérapie par des MIPs. / This thesis describes the state of the art in nanomaterials-based targeted bioimaging and introduces molecularly imprinted polymers, also termed ‘plastic antibodies’ as novel biorecognition agents for labeling and imaging of cells and tissues. In fundamental biology and medical diagnostics, there is a constant need to localize and quantify specific molecular targets. Abnormal glycosylation levels or distributions of hyaluronan or sialic acids on cells are indicators of infection or malignancy. In general, bioimaging with fluorescent probes enables the localization and qualitative or quantitative determination of these pathological biomarkers. However, no reliable tools for the recognition of glycosylation sites on proteins exist, because the commercially available antibodies or lectins have poor affinity and selectivity for these targets. In this context, tailor-made molecularly imprinted polymers (MIPs) are promising synthetic receptor materials since they present a series of advantages over their natural counterparts such as the ease and low cost of preparation and their physical and chemical stability. Thus, MIPs could provide a robust and specific imaging tool for revealing the location/distribution, time of appearance and structure of glycosylation sites on/in cells, which would lead to a better insight of the tremendously diverse biological processes in which these molecules are involved. Herein, we describe the synthesis of water-compatible MIPs for the molecular imaging of hyaluronan and sialylation sites on cells and tissues. Since molecular imprinting of entire biomacromolecules like oligosaccharides is challenging, we opted for what is commonly called the ‘epitope approach’, which was inspired by nature. The monosaccharides, glucuronic acid and N-acetylneuraminic acid were imprinted, and the resulting MIPs were able to bind these molecules when present and accessible on the terminal unit of hyaluronan and sialylation sites. Fluorescent MIPs were synthesized as rhodamine-labeled nanoparticles and as MIP-coated InP/ZnS core-shell quantum dot (QD) particles. For the coating of the QDs, a novel versatile solubilization and functionalization strategy was proposed, which consists of creating polymer shells directly on QDs by photopolymerization using the particles as individual internal light sources. A standard immunostaining protocol was then successfully adapted for the application of the fluorescently labeled MIPs to image fixed and living human keratinocytes and skin tissues, by epifluorescence and confocal fluorescence microscopy. The results were comparable to those obtained with a reference method where staining was done with a biotinylated hyaluronic acid binding protein. Multiplexed and cancer cell imaging were also performed, demonstrating the potential of molecularly imprinted polymers as a versatile biolabeling and bioimaging tool. Although the MIPs were not cytotoxic at the concentrations used for bioimaging, in order to render them generally applicable in biomedicine, where toxicity of the polymerization precursors is a matter of concern, we suppressed the initiator, a toxic chemical. Initiator-free MIPs were thus synthesized by using monomers that can self-initiate under UV irradiation or heat. The specificity and selectivity of the obtained MIPs were as good as the ones prepared with initiators. In conclusion, we have demonstrated for the first time the great potential of MIPs as synthetic antibody mimics for bioimaging. The possibility to associate other functionalities such as QDs and additionally attach drugs to the same material appears rather straightforward due to the synthetic polymeric nature of MIPs, which paves the way to new potential applications in theranostics.

Bioimagerie

Anticorps plastique

Boîte quantique

Monomère auto-initiant

Imagerie par fluorescence

Nanomatériaux

Bioimaging

Multiplexing

Glycosylation

Hyaluronan

Sialic acid

Molecularly imprinted polymer (MIP)

Plastic antibody

Quantum dot

Initiator-free polymerization

Self-initiated monomer

Development and Testing of a Second Generation Hand-held Optical Imager

Gonzalez, Jean

22 March 2012

Hand-held optical imagers are developed towards clinical breast cancer imaging. Herein, a Gen-2 hand-held optical imager has been developed with unique features: (i) image curved breast tissues with ~86% surface contact, and (ii) perform reflectance and transillumination imaging using the novel forked probe heads. Extensive phantom studies were performed using 1% Liposyn solution (background, ~ 300 ml and 1000 ml volumes) and 0.45 cc India Ink (absorption) targets, under different target:background contrast ratios and target depths. Two-dimensional surface images detected target(s) up to 2.5 cm deep via reflectance imaging, and up to 5 cm deep via transillumination imaging. Preliminary studies on gel-based breast phantoms (~700 ml) detected targets via reflectance and transillumination imaging. Preliminary in-vivo reflectance studies on normal and cancerous breast tissues also detected targets, although with artifacts. In future, the portable Gen-2 imager has potential for clinical breast imaging via reflectance and transillumination approach after extensive in-vivo studies.

Optical

imaging

breast

hand-held

bed-based

spectroscopic

spectroscopy

near-infrared imaging

NIR

imager

Development

testing of optical device

device

human subject

subject

human

preliminary invivo

invivo

in-vivo

phantom

extensive phantom

biomedical

optics

bioimaging