Nanoparticules hybrides thermosensibles pour la théranostique / Hybrid and thermosensitive nanoparticles for theranostic applications

Louguet, Stéphanie

05 April 2011

Cette étude concerne le développement de nanoparticules hybrides offrant de nouvelles stratégies pour la thérapie et le diagnostic médical. Elles sont constituées d’un cœur magnétique jouant le rôle d’agent de contraste pour l’IRM et d’inducteur de chaleur par hyperthermie, d’une couronne de polymère thermosensible permettant d’encapsuler des principes actifs et de peptides de reconnaissance biologique. Une grande partie de l’étude a consisté à étudier les processus d'adsorption de copolymères poly(éther)-b-poly(L-lysine) de composition variable sur les particules magnétiques et à comprendre le rôle de la conformation des chaînes polymère à la surface des particules sur la stabilité des colloïdes en milieu physiologique. Un agent antitumoral a été encapsulé puis libéré de façon contrôlée sous l’effet d’un champ magnétique alternatif en exploitant le caractère thermosensible des blocs polyéthers. Des séquences peptidiques ciblant les zones d’inflammation de la barrière hémato-encéphalique ont été greffées sur les copolymères. L’efficacité du ciblage a été validée par IRM et fluorescence sur un modèle animal démontrant ainsi la multifonctionnalité des nanoparticules. / This work deals with the development of hybrid nanoparticles that could offer new strategies for therapy and diagnostic. These are based on a magnetic core which can play the role of contrast agent for MRI as well as heat inductor in AC magnetic field. This inorganic core is surrounded by a thermo-responsive polymeric brush that controls the loading and the release of drugs, and can be functionalized by specific ligands ensuring the targeting specificity. A large part of this work consists in studying the adsorption mechanism of poly(ether)-b-poly(L-lysine) based block copolymers onto magnetic particle and to better understand the influence of the polymer chain conformation at particles surface on the colloidal stability under physiological conditions. An anticancer drug has been loaded and released in a controlled manner under alternative magnetic field by taking advantage from the thermosensitivity of the polyether block. Targeting peptides specific of inflammation sites at the blood brain barrier have been grafted onto copolymers. The targeting specificity has been demonstrated by MRI and fluorescence imaging in rats attesting the multifunctionality of such nanoparticles.

Théranostique

Nanoparticules magnétiques

Oxyde de manganèse

Copolymères à blocs

Polypeptides

Peg

Polymère thermosensible

Délivrance contrôlée

Hyperthermie

Irm

Agents de contraste

Nanoparticules multifonctionnelles

Theranostic

Magnetic nanoparticles

Manganese oxide

Block copolymers

Polypeptides

Peg

Thermosensitive polymer

Controlled release

Hyperthermia

Mri

Contrast agents

Multifunctional nanoparticles

Estudos conformacionais em compostos contendo íons lantanídeos

Oliveira, Maria Weruska Pereira de

13 November 2008

Made available in DSpace on 2015-05-14T13:21:13Z (GMT). No. of bitstreams: 1 arquivototal.pdf: 1246890 bytes, checksum: d8de4e92a3d9c573a9ad39ccb546aa71 (MD5) Previous issue date: 2008-11-13 / Coordenação de Aperfeiçoamento de Pessoal de Nível Superior - CAPES / Lanthanide macrocyclic complexes, especially containing Gd(III) ions, are largely used as contrast agents in the medical diagnostic technique named Magnetic Resonance Imaging (MRI). Theoretical investigation of these compounds by molecular modeling methods is an emerging research area today. In this work we have performed a conformational study of the following supramolecular compounds: the macrocyclic ligands 1,4,7,10- tetraazacyclododecane (DOTA) and 1,4,7,10-tetraazacyclododecane- 1,4,7,10-tetraacetic acid (H4DOTA) and the macrocyclic complexes [Gd(DOTA).H2O]- and Gd(PhenHDO3A).H2O, where PhenHDO3A is (rel-10- [(5R,6R)-5,6-dihydro-6-hydroxy-1,10-Phenanthroline-5-yl)-1,4,7,10- tetraazacyclododecane-1,4,7-triacetic acid). For this, we have developed and carried out a procedure that involves: (1) the sampling of the conformation space of these compounds through some short molecular dynamics at different temperatures and (2) full geometry optimization in the geometries obtained in the previous stage using semi-empirical AM1 method for the macrocyclic ligands and Sparkle/AM1 model for the macrocyclic lanthanide complexes. Our results revealed that the high flexibility of non-coordinated macrocyclic ligands DOTA and H4DOTA, helped us to test the ability of our methodology to sample different regions of conformation space of these compounds. For the [Gd(DOTA).H2O]- complex, we were capable to find the same conformational isomers which were reported in published works as well as to comprehend relevant details about the mobility of the coordinated water molecule. Furthermore, we also were capable to identify some intermediate local minima related to the dynamics of rotation of the coordinated acetate groups in the studied complexes as well as to the dynamics of ring inversion of the coordinated tetraazadodecane moiety in the Gd(PhenHDO3A).H2O. In conclusion, we possess now an interesting strategy to conduct the search for conformational isomers of these compounds. This knowledge is very important to be applied in the rational design of new molecules to act as contrast agent in MRI. / Complexos macrocíclicos de lantanídeos, em especial com o íon Gd(III), são cada vez mais utilizados como agentes de contrastes na técnica médica de diagnóstico, imagem por ressonância magnética nuclear (MRI). O estudo teórico de novos agentes de contrastes através de modelagem molecular é uma área de pesquisa em grande expansão. No nosso trabalho fizemos um estudo conformacional dos seguintes compostos supramoleculares: os ligantes macrocíclicos 1,4,7,10- tetraazaciclododecano (DOTA) e ácido 1,4,7,10-tetraazaciclododecano- 1,4,7,10-tetraacético (H4DOTA), o complexo macrocíclico [Gd(DOTA)H2O]- e o complexo macrocíclico Gd(PhenHDO3A).H2O, onde PhenHDO3A é (rel-10-[(5R,6R)-5,6-dihidro-6-hidroxi-1,10-fenantrolina-5- il)-1,4,7,10-tetraazaciclododecano-1,4,7-ácido triacético). Para isso, elaboramos e executamos um procedimento que envolve o mapeamento ou amostragem do espaço conformacional desses compostos através de dinâmicas moleculares curtas em diferentes temperaturas para em seguida, essas geometrias serem usadas como pontos de partida para otimização de geometria usando tanto o método semi-empírico AM1 quanto o modelo Sparkle/AM1. Como resultado, podemos citar que a elevada flexibilidade dos ligantes macrocíclicos não coordenados DOTA e H4DOTA, serviu para testar a capacidade da nossa metodologia de visitar regiões distintas do espaço conformacional. Para o complexo [Gd(DOTA)H2O]-, conseguimos encontrar os mesmos isômeros conformacionais que já são reportados em outros estudos, bem como revelar detalhes relativos à mobilidade da molécula de água coordenada. Além disso, conseguimos identificar mínimos locais intermediários que estão relacionados com a dinâmica de rotação dos grupos acetato em ambos os complexos e a dinâmica de inversão do anel tetraazadodecano no complexo Gd(PhenHDO3A).H2O. A relevância desse trabalho está apoiada no fato de que agora temos uma estratégia interessante para realizar a busca de isômeros conformacionais desses compostos, sendo essas informações, muito importantes quando se deseja projetar uma nova molécula para atuar como agente de contraste em MRI.

Análise conformacional

Agentes de contraste em MRI

Dinâmica molecular

Métodos semi-empíricos

Modelo sparkle/AM1

Conformational analysis

MRI contrast agents

Molecular dynamics

Semi-empirical methods

Sparkle/AM1 model

CIENCIAS EXATAS E DA TERRA::QUIMICA

Nanoparticles functionalized with human antibodies for multimodal molecular imaging of atherosclerosis / Nanoparticules fonctionnalisées avec des anticorps humains pour l'imagerie moléculaire multimodale de l'athérosclérose

Larivière, Mélusine

19 December 2016

L'athérosclérose, à l’origine de la plupart des maladies cardiovasculaires telles que l'infarctus du myocarde ou l'AVC, est la principale cause de décès dans le monde. Les cliniciens ont donc besoin de techniques d'imagerie fiables pour identifier les patients «vulnérables» porteur d’athérome à haut risque d'occlusion thrombotique. Cette pathologie est une maladie inflammatoire qui implique beaucoup d'acteurs cellulaires et moléculaires, parmi lesquels les cellules endothéliales et immunitaires, les lipoprotéines, les cellules apoptotiques et les plaquettes. L'imagerie moléculaire visant à détecter ces acteurs avant la survenue d'événements cardiovasculaires dramatiques est en plein essor. Des anticorps humains (HuAbs) sélectionnés par phage-display pour reconnaître des biomarqueurs de la pathologies ont ici proposés comme ligands servant à fonctionnaliser des vecteurs pour l'imagerie IRM, de fluorescence ou TEP. Les HuAbs ont été modifiés, en introduisant soit des Cystéines soit un site de reconnaissance pour la Sortase, afin de développer un greffage site-spécifique. Les agents ciblant ont été validés in vitro et ex vivo sur des coupes d'athérome de modèles animaux. Des résultats prometteurs ontété obtenus en injectant dans des souris ApoE-/- l’anticorps antiplaquettaire TEG4, apportant ainsi de nouvelles connaissances sur la biologie de l'athérome et la preuve de concept d'une possible détection des plaques à haut risque riches en plaquettes. Des améliorations sont en cours pour développer des agents de contraste multi-fonctionnalisés avec des HuAbs et permettant de réaliser une imagerie moléculaire multimodale de l'athérosclérose facilement transposable en clinique. / Because cardiovascular diseases are the leading cause of death in the world, providing clinicians with reliable and straightforward imaging techniques to identify "vulnerable" patients from the general population appears like the Holy Grail of the cardiovascular field. Atherosclerosis, identified as the underlying condition for most acute cardiovascular events, is characterized by the constitution of a lipidrich atheroma plaque, driven both by excess cholesterol and inflammation, which eventual rupture triggers clotting into the blood flow. It involves a wealth of cellular and molecular actors, which are so many potential markers for molecular imaging, aiming at deciphering how to warn clinicians about the possible occurrence of myocardial infarction or stroke. Here, human antibodies (HuAbs) selected by phage-display for their recognition of over-expressed biomarkers of the pathology are proposed as targeting ligands. They were further engineered for site-specific grafting, either by introducing Cysteine or Sortase recognition tags, and used to target contrast agents for MRI, fluorescence, or PET imaging. In vitro and ex vivo validation studies were carried out on atheroma sections of animal models. In vivo studies in the ApoE-/- mouse model were realized with the anti-platelet TEG4 HuAb using MRI, which provided insights on the biological relevance and feasibility to detect platelets-rich, high-risk atheroma plaques. The development of contrast agents useful in multi-modality imaging, and multi-functionalized with HuAbs is underway. It should serve as an accurate molecular imaging method for atherosclerosis, further more easily translated into the clinical arena.

Athérosclérose

Anticorps humains

Ingénierie d’anticorps

Agents de contraste ciblés

Fonctionnalisation site-spécifique

Imagerie de résonance magnétique

Fluorescence proche-infrarouge

Atherosclerosis

Human antibodies

Antibodies engineering

Targeted contrast agents

Sitespecific functionalization

Magnetic resonance imaging

Near-infrared fluorescence

Tissue harmonic reduction : application to ultrasound contrast harmonic imaging / Imagerie ultrasonore non linéaire : réduction des harmoniques tissulaire en imagerie de contraste

Pašović, Mirza

11 May 2010

Les agents de contraste sont de petites bulles qui répondent non linéairement lorsqu’ils sont exposés à ultrasons. La réponse non-linéaire donne la possibilité d’images échographiques harmoniques qui a beaucoup d’avantages sur l’imagerie fondamentale. Toutefois, afin d’accroître l’échographie de contraste d’imagerie harmonique de performance nous devons d’abord comprendre la propagation non linéaire d’ultrasons. La non-linéarité du milieu déforme l’onde qui se propage, tels que les harmoniques commencent à se développer. La théorie qui a été prévue est la mise en œuvre, qui a permis une nouvelle méthode de modélisation de propagation des ultrasons non-linéaire. La connaissance acquise au cours de ce processus a été utilisée pour construire un deuxième signal à composantes multiples pour la réduction des harmoniques générées en raison des non-linéarités des tissus. En conséquence, la détection d’agents de contraste ultrasonore aux harmoniques a été augmentée. Une puissante technique d’imagerie échographique (Pulse inversion) a été renforcée avec le deuxième signal pour la réduction des harmoniques. Qu’est-ce qui a été appris pendant l’investigation : le pulse inversion technique a donné une nouvelle phase codée, appelée inversion de seconde harmonique. En outre, il a été noté que pour différents types de médias le niveau de distorsion de l’impulsion à ultrasons est différent. Cela dépend en grande partie du paramètre non linéaire B / A. Les travaux sur ce paramètre n’a pas été fini, mais il est quand même important de continuer dans cette direction puisque B / A imagerie avec des agents de contraste ultrasonore a beaucoup de potentiel. / Ultrasound contrast agents are small micro bubbles that respond nonlinearly when exposed to ultrasound wave. The nonlinear response gives possibility of harmonic ultrasound images which has many advantages over fundamental imaging. However, to increase ultrasound contrast harmonic imaging performance we must first understand nonlinear propagation of ultrasound wave. Nonlinear propagation distorts the propagating wave such that higher harmonics appear as the wave is propagating. The theory that was laid down, was allowed implementing a new method of modelling nonlinear ultrasound propagation. The knowledge obtained during this process was used to construct a multiple component second harmonic reduction signal for reduction of their harmonics generated due to the tissue nonlinearities. As a consequence detection of ultrasound contrast agents at higher harmonics was increased. Further more, a powerful ultrasound imaging technique called Pulse Inversion, was further enhanced with multiple component second harmonic reduction signal. What was learned during investigation of the Pulse Inversion, technique lead to a new phase coded ultrasound contrast harmonic method called second harmonic inversion;. Also it was noted that for different type of media the level of distortion of ultrasound pulse is different. It depends largely on the nonlinear parameter B / A. Although the work on this parameter has not been finished it is very important to continue in this direction since B / A imaging with ultrasound contrast agents has a lot of potential.

Propagation non linéaire

Agents de contraste

Réduction de deuxième harmonique

Pulse inversion

Inversion de seconde harmonique

Paramètre du non linéaire

Nonlinear propagation

Ultrasound contrast agents

Second harmonic reduction

Pulse inversion

Second harmonic inversion

Nonlinear parameter

534

534.5

DCE-MRI assessment of hepatic uptake and efflux of the contrast agent, gadoxetate, to monitor transporter-mediated processes and drug-drug interactions : in vitro and in vivo studies

Georgiou, Leonidas

January 2015

Dynamic contrast-enhanced magnetic resonance imaging (DCE-MRI) techniques offer the opportunity to understand the physiological processes involved in the distribution of the contrast agent in vivo. This work utilises a liver specific contrast agent (gadoxetate) and demonstrates the potential use of these techniques to study transporter-mediated process in vivo. In vitro experiments investigated gadoxetate’s interaction with uptake and efflux transporters at the cellular level, ideally a prerequisite to understand the contribution of transporter proteins in in vivo pharmacokinetics. MRI was used to measure the accumulation of gadoxetate in fresh rat hepatocytes. Furthermore, LC-MS/MS methodology was optimised in conjunction with two in vitro systems to determine the role of transporters in gadoxetate uptake and efflux. HEK-OATP1B1 transfected cells were used to optimise the LC-MS/MS technique and Caco-2 cell monolayers were used to examine whether gadoxetate is a substrate of the efflux transporters, Pgp and BCRP. Subsequent studies demonstrated the use of DCE-MRI techniques to study transporter-mediated processes. Two pharmacokinetic models were proposed to quantify the uptake and efflux of gadoxetate in vivo. The suitability of the models in describing the liver concentration profiles of gadoxetate was assessed in pre-clinical and clinical reproducibility studies. Further pre-clinical experiments demonstrated the ability of the proposed DCE-MRI techniques to monitor changes in the uptake and efflux rate estimates of gadoxetate into hepatocytes, through co-administration of the transporter inhibitor, rifampicin, at two doses. The work presented demonstrates the potential use of DCE-MRI techniques as a diagnostic probe to assess transporter-mediated processes and drug-drug interactions (DDIs) in vivo.

615.7

Registrace obrazů - aplikace v oftalmologii a ultrasonografii / Image Registration - Application in ophthalmology and ultrasonography

Harabiš, Vratislav

January 2014

Image registration is widely used in clinical practice. However image registration and its~evaluation is still challenging especially with regards to new possibilities of various modalities. One of these areas is contrast-enhanced ultrasound imaging. The time-dependent image contrast, low signal-to-noise ratio and specific speckle pattern make preprocessing and image registration difficult. In this thesis a method for registration of images in ultrasound contrast-enhanced sequences is proposed. The method is based on automatic fragmentation into image subsequences in which the images with similar characteristics are registered. The new evaluation method based on comparison of perfusion model is proposed. Registration and evaluation method was tested on a flow phantom and real patient data and compared with a standard methods proposed i literature. The second part of this thesis contains examples of application of image registration in~ophthalmology and proposition for its improvement. In this area the image registration methods are widely used, especially landmark based image registration method. In this thesis methods for landmark detection and its correspondence estimation are proposed.

Akvizice, modelování a analýza signálů v ultrazvukovém perfúzním zobrazování / Acquisition, Modeling and Signal Processing in Ultrasound Perfusion Imaging

Mézl, Martin

January 2017

This work deals with possibilities of ultrasound perfusion analysis for the absolute quantification of perfusion parameters. In the theoretical part of this work are discussed possibilities of using of the ultrasound contrast agents and approaches for the perfusion analysis. New methods for the perfusion analysis are suggested and tested in the practical part of this work. The methods are based on convolutional model in which the concentration of the contrast agent is modeled as aconvolution of the arterial input function and the tissue residual function. The feasibility of these methods for the absolute quantification of perfusion parameters is shown on data from phantom studies, simulations and also preclinical and clinical studies. The software for the whole process of the perfusion analysis was developed for using in hospitals.

Modelování v perfúzním ultrazvukovém zobrazování / Modelling for ultrasound perfusion imaging

Jakubík, Juraj

January 2017

This master thesis deals with the contrast agents and their application in the ultrasound perfusion analysis. It is focused on Bolus & Burst method which, as a combination of two approaches that have been used so far, allows an absolute quantification of perfusion parameters in the region of interest. Contrast agent concentration time sequence is modeled as a convolution of the parametrically defined arterial input function and the tissue residual funkction. Thesis discusses different mathematical models of these functions as well as the methods of the parameters estimation. The methods functionality is validated on simulated and also preclinical data.

Impacts environnementaux des agents de contraste à base de Gadolinium : situation locale, approche cellulaire et in vivo / Environmental impacts of Gadolinium-based contrast agents : local situation, cellular and in vivo approaches

Perrat, Emilie

12 December 2017

L’utilisation de plus en plus fréquente des agents de contraste à base de Gd (AC-Gd) au cours des examens d’Imagerie par Résonnance Magnétique (IRM), engendre le rejet de ces produits pharmaceutiques dans les eaux usées retraitées en STation d’EPuration (STEP). En l’absence de retraitement spécifique de ces AC-Gd en STEP, ils sont rejetés dans le milieu aquatique, où de nombreuses études ont relevé leur présence aussi bien dans les eaux de surface que dans les eaux souterraines et jusqu’à l’eau du robinet. Le manque de connaissances concernant les effets des AC-Gd suite à leur rejet a mis en évidence la nécessité d’étudier leurs impacts environnementaux sur les organismes vivants dans les milieux aquatiques. Dans ce contexte, nous avons choisi de déterminer les concentrations en Gd d’origine anthropique à proximité de rejets de STEP et de zones de captage en eau potable situés en région Lorraine. Nos mesures ont permis de montrer la présence Gd d’origine anthropique sur l’ensemble des échantillons prélevés, avec des concentrations mesurées comprises de quelques ng(Gd)/L à quelques dizaines de µg(Gd)/L. Ces concentrations de Gd anthropique seraient dues à la présence d’AC-Gd. Nous nous sommes plus particulièrement intéressés aux effets de l’AC-Gd le plus stable et l’un des plus fréquemment commercialisé : le Gd-DOTA (Dotarem®). Pour cela, nous avons choisis plusieurs espèces représentatives des taxons rencontrés dans les cours d’eau Lorrains. Des essais ont été menés en conditions contrôlées de laboratoire afin de mesurer l’accumulation du Gd-DOTA dans les tissus et les effets de l’AC-Gd ont été appréhendés au travers de mesures de croissance, de reproduction et de mortalité au niveau individuel chez les microalgues vertes unicellulaires (Chlorella vulgaris et Pseudokirchneriella subcapitata), chez un microcrustacé (Daphnia magna) et chez un vertébré aquatique (Danio rerio) exposés à des concentrations en Gd-DOTA réalistes d’un point de vue environnemental. L’accumulation du Gd-DOTA a aussi été mesurée chez les bivalves (Corbicula fluminea et Dresseina rostriformis bugensis) et comparée à des mesures d’accumulation du Gd in situ. Les réponses physiologiques des bivalves ont été évaluées à l’aide d’une batterie de 11 biomarqueurs dans leurs branchies et leur glande digestive. Les effets de l’AC-Gd ont également été étudiés in vitro sur des fibroblastes de D. rerio (cellules ZF4 - ATCC-2050). Nos travaux ont montré que les AC-Gd et le Gd-DOTA en particulier étaient responsables d’effets écotoxiques indirects à différents niveaux d’organisation biologiques. Seuls les bivalves accumulent le Gd-DOTA mais tous les individus semblent mettre en place des mécanismes de dépuration pour parer à la toxicité de l’AC-Gd. Les résultats obtenus au cours de cette recherche ont confirmé la nécessité d’un suivi des concentrations en AC-Gd dans le milieu aquatique et la nécessité d’approfondir les études de l’écotoxicité de ces produits pharmaceutiques. Ceci pourra aboutir à une évaluation pertinente de leur risque environnemental et de proposer des solutions pour la gestion environnementale de ces composés / The increasing use of Gadolinium-based Contrast Agents (Gd-CA) for Magnetic Resonance Imaging (MRI) results in their rejection in Waste Water Treatment Plants (WWTPs). Due to the lack of specific recycling process in European WWTPs, these pharmaceutical produces enter the aquatic environment from river to tap water. The effects of Gd-CA in aquatic media have been not studied yet. The lack of knowledge about these effects highlighted the need to study their environmental impacts on aquatic organisms. In this context, we decided to measure anthropogenic concentrations of Gd in the aquatic environment in the Lorraine region (France) closed to WWTPs outputs and catchment areas used for drinking water. Our measurements underlined the presence of anthropogenic Gd on all the collected samples at concentrations ranging from few ng/L to several dozen of µg/L. In this research we focused on the effects of the most frequently used Gd-CA, the gadoteric acid (Gd-DOTA - Dotarem®) which is also the most stable one. Several representative species of aquatic environment were selected for ecotoxicological assays: i.e. unicellular green microalgae (Chlorella vulgaris and Pseudokirchneriella subcapitata), microcrustacean (Daphnia magna) and aquatic vertebrate (Danio rerio). Assays were conducted in laboratory under controlled conditions as well as in situ. Gd-DOTA accumulation was measured in the tissues of the different organisms. Environmental realistic concentrations of Gd-CA were used to assess their effects at the individual level by means of growth, reproduction and mortality measurements. The Gd-DOTA accumulation was also measured in bivalves’ tissues (Corbicula fluminea and Dresseina rostriformis bugensis) and compared to Gd ones in situ in these organisms. Physiological responses were assessed based on a battery of 11 complementary biomarkers measured in the digestive gland and in the gills of both bivalve species. At cellular level, the effects of Gd-DOTA were studied in vitro on D. rerio fibroblasts (ZF4 – ATCC-2050). Indirect ecotoxicological effects of Gd-CA and of Gd-DOTA especially have been highlighted at all biological levels. Accumulation of Gd-DOTA was observed in bivalves only, but defense systems were mobilized in all organisms to limit toxicity. Our results demonstrated that following both research on ecotoxicological effects of the Gd-CA and evolution of their concentrations in aquatic ecosystem are necessary to assess more precisely their environmental risk and to propose solutions for their environmental management

Gd-DOTA (Dotarem®)

Bioaccumulation

Biomarqueurs

Gadolinium d’origine anthropique

Analyses ICP-MS

Gd-DOTA (Dotarem®)

Bioaccumulation

Biomarkers

Anthropogenic Gadolinium

ICP-MS analysis

571.95

Nanobubble Ultrasound-Contrast Agents as a Strategy to Assess Tumor Microenvironment Characteristics and Nanoparticle Extravasation

Cooley, Michaela Briana

26 May 2023

No description available.

Biomedical Engineering

Medicine

Medical Imaging

Nanoscience

Nanotechnology

Oncology

Radiology

Nanobubbles

ultrasound

ultrasound contrast agents

cancer

medical imaging

vascular permeability

red blood cells

microfluidics

companion nanoparticle

decorrelation time

acoustic radiation force

patient stratification