Efeito da interação dipolar magnética na eficiência de aquecimento de nanopartículas: Implicações para magnetohipertermia / Effect of magnetic dipolar interactions on nanoparticle heating efficiency: Implications for magnetic hyperthermia

Branquinho, Luis Cesar

09 December 2014

Submitted by Erika Demachki (erikademachki@gmail.com) on 2017-04-27T17:01:46Z No. of bitstreams: 2 Tese - Luis Cesar Branquinho - 2014.pdf: 6091709 bytes, checksum: 2c59441af9866c02cd7a2cc3cc667b3e (MD5) license_rdf: 0 bytes, checksum: d41d8cd98f00b204e9800998ecf8427e (MD5) / Approved for entry into archive by Luciana Ferreira (lucgeral@gmail.com) on 2017-05-03T11:40:46Z (GMT) No. of bitstreams: 2 Tese - Luis Cesar Branquinho - 2014.pdf: 6091709 bytes, checksum: 2c59441af9866c02cd7a2cc3cc667b3e (MD5) license_rdf: 0 bytes, checksum: d41d8cd98f00b204e9800998ecf8427e (MD5) / Made available in DSpace on 2017-05-03T11:40:46Z (GMT). No. of bitstreams: 2 Tese - Luis Cesar Branquinho - 2014.pdf: 6091709 bytes, checksum: 2c59441af9866c02cd7a2cc3cc667b3e (MD5) license_rdf: 0 bytes, checksum: d41d8cd98f00b204e9800998ecf8427e (MD5) Previous issue date: 2014-12-09 / Coordenação de Aperfeiçoamento de Pessoal de Nível Superior - CAPES / Magnetic nanoparticles can generate heat when submitted to alternating magnetic fields of adequate amplitude and frequency. This phenomenon is named magnetic hyperthermia and has several therapeutic applications, as for example, in the treatment of cancer. In general, the theoretical models used to describe this neglect the effect of interparticle interaction. In this thesis we investigate the effect of magnetic dipolar interaction in the magnetothermal efficiency (named specific loss power – SLP) of bicompatible magnetic nanoparticles. Firstly, we develop a chain of magnetic particles model, where we prove that the interaction leads to a contribution to the uniaxial anisotropy. This term in the free energy density allowed us to extract from the electron magnetic resonance technique (EMR) information about the mean chain size in the colloid. Further, this additional magnetic nanoparticle anisotropy term was used to develop an analytical theoretical model that takes into account the effect of the dipolar interaction between nanoparticles to SLP, considering the case where the magnetization responds linearly to the field (Linear Response Theory). Our calculations indicate that depending on the particle parameters, specially the anisotropy, the effect can be to enhance or decrease the heat generation. Moreover, we showed that increasing the chain size (number of particles in the chain) the optimal particle size for hyperthermia can decrease up to 30% in comparison with non-interacting particles. This result has several clinical implications, which allowed us to suggest some strategies for improving the therapeutic efficacy. In order to investigate experimentally the effect, two magnetic fluids, one containing spherical nanoparticles based on manganese ferrite (MnF-citrate) in the superparamagnetic regime, and another commercial one (BNF-starch) magnetite-based with a shape of a parallellepiped and blocked, were selected and deeply characterized. We found a decrease of SLP increasing the chain size for the MnF sample, while for BNF-starch no effect was found at the same experimental conditions. The decrease of SLP in the MnF sample, within the particle concentration range, was explained considering in the model not only the effect in the anisotropy but also by an increase in the damping factor parameter, a term correlated to spin-phonon interaction. Data obtained using EMR and Monte Carlo simulations corroborate our hypothesis. The absence of concentration effect for the BNF sample was attributed to the higher anisotropy value and to the probable influence of brownian relaxation. In addition, the same chain model was used to investigate the behavior of blocked nanoparticles of Stoner-Wohlfarth type. In this case, we demonstrate that the chain formation increases the magnetic hyperthermia, as found in magnetosomes. Finally, we showed that a fluctuation of the dipolar interaction field between particles in the chain, which does not destroy the symmetry of this term, shows a Vogel-Fulcher behaviour in the weak coupling regime. / Nanopartículas magnéticas são capazes de gerar calor quando submetidas a campo magnético alternado de amplitude e frequência adequadas. Este fenômeno é conhecido como magnetohipertermia e possui aplicações terapêuticas como, por exemplo, no tratamento de câncer. Em geral, os modelos teóricos que descrevem o fenômeno não levam em conta efeitos associados à interação partícula-partícula. Nesta tese investigamos o efeito da interação dipolar magnética na eficiência magnetotérmica (SLP) de nanopartículas magnéticas biocompatíveis. Primeiramente desenvolvemos um modelo de cadeia de nanopartículas magnéticas, aonde provamos que a interação entre partículas que formam uma cadeia linear equivalem a uma contribuição uniaxial a anisotropia. Essa contribuição à densidade de energia permitiu que obtivéssemos por meio da técnica de ressonância magnética eletrônica (RME) informações acerca do tamanho médio de aglomerado na suspensão coloidal. Posteriormente utilizamos esse termo adicional da anisotropia efetiva da nanopartícula para propor um modelo teórico analítico que leve em consideração o efeito de tal interação na eficiência de aquecimento de nanopartículas magnéticas em um fluido para o caso em que a magnetização das nanopartículas responde linearmente ao campo (Teoria da Resposta Linear). Nossos cálculos indicaram que, dependendo de parâmetros da nanopartícula, em particular da anisotropia, este efeito pode aumentar ou diminuir a geração de calor. Além disso, mostramos que o aumento do número de partículas formando cadeias lineares reduz o diâmetro ótimo para hipertermia em até 30% em relação ao valor esperado para partículas isoladas. Este resultado possui fortes implicações clínicas, e permitiu que sugeríssemos algumas estratégias para aumentar a eficiência terapêutica. No intuito de investigar experimentalmente este efeito, dois fluidos magnéticos, um contendo nanopartículas esféricas de ferrita de Mn (MnF-citrato) no regime superparamagnético e outra comercial (BNF-starch) à base de magnetita com forma de nanoparalelepípedos e contendo partículas bloqueadas, foram selecionados e amplamente caracterizados. Observamos uma diminuição no SLP com o aumento de partículas na cadeia para a amostra MnF-citrato, para todos os valores de campo, enquanto que para a amostra BNF-starch não percebemos alteração do SLP. O decréscimo do SLP da amostra MnF, na faixa de concentração investigada, foi explicado incluindo não apenas o efeito na anisotropia efetiva, mas também o aumento no valor do fator de amortecimento. Dados de RME e simulação de Monte Carlo corroboraram tal hipótese. A ausência de efeito para amostra BNF-starch foi atribuída à alta anisotropia e provável influência de relaxação browniana. Adicionalmente, o modelo de cadeia foi usado para explicar o comportamento de nanopartículas bloqueadas do tipo Stoner-Wohlfarth. Neste caso demonstramos que a formação de cadeias aumenta a hipertermia magnética, como verificado em magnetossomos. Finalmente, mostramos que uma flutuação no campo dipolar interpartículas na cadeia, que não destrua a simetria desta contribuição, fornece um comportamento do tipo Vogel-Fulcher no regime fracamente interagente.

Hipertermia magnética

Interação interpartículas

Tratamento de câncer

Nanopartículas magnéticas

Aplicações biomédicas

Magnetic hyperthermia

Interparticle interactions

Cancer Therapy

Magnetic nanoparticles

Biomedical applications

CIENCIAS EXATAS E DA TERRA::FISICA

Cell penetrating and interfering peptides as new cancer therapy / Peptides pénétrants et interférants comme nouvelle thérapie contre le cancer

Zhang, Xiguang

30 November 2017

Les peptides pénétrants sont de petits peptides capables de se rentrer dans les cellules sans endommager la membrane, présentant un grand potentiel dans la délivrance de diverses cargaisons, y compris des peptides, pour le traitement du cancer ainsi que d'autres maladies. Les peptides comme médicaments, bénéficient d'être spécifiques, relativement sûrs, faciles à produire et faciles à modifier. Cependant, des défis significatifs demeurent concernant l'application de peptides en tant qu'agents thérapeutiques. L'identification des motifs de liaison des peptides est difficile et les peptides se comportent généralement avec une perméabilité cellulaire faible et une sensibilité à l'hydrolyse des proteases. Dans le présent travail, nous avons caractérisé deux interactions protéine-protéine Ras/Raf et PP2A/SET qui sont impliqués dans la régulation de la transformation tumorale et de l'apoptose. Nous avons identifié le site de liaison parmi ces protéines (peptides interférents). Ces peptides interférents ont été associés à une navette optimisée pour générer des peptides chimériques capables de dissocier ces interactions protéine/protéine. Les peptides chimeriques ont été testés in vitro et in vivo, montrant un effet anti-tumor. Ces peptides pourraient être considérés comme des candidats prometteurs pour des applications futures en tant que vecteurs pour la délivrance de médicaments intracellulaires. / Cell penetrating peptides are small peptides which are able to translocate into cells without causing membrane damage, presenting a great potential in the delivery of various cargos including peptides, for the treatment of cancer as well as other diseases. Peptides as drugs, benefit from being specific, relative safe, easy to produce and easy to modify. However, significant challenges remain regarding the application of peptides as therapeutic agents. Identification of the binding motifs of the peptides is difficult, and peptides generally behave low-cellular permeability and sensitivity to proteases hydrolysis. In the present work, we characterized two protein-protein interactions Ras/Raf and PP2A/SET that are involved in the regulation of tumor transformation and apoptosis. We have identified the binding site among these proteins (interfering peptides). These interfering peptides were associated to an optimized shuttle to generate chimeric peptides able to dissociate these protein/protein interactions. The chimeric peptides were tested in vitro an in vivo, showing an anti-tumor effect. These peptides could be considered as promising candidates for future applications as vectors for intracellular drugs delivery.

Peptides pénétrants

Interaction protéine-protéine

Thérapie contre le cancer

Internalisation des peptides

Stabilité du peptide

Livraison de médicaments

Cell penetrating peptides

Protein-protein interaction

Cancer therapy

571.6

Nouveaux systèmes nanométriques et ph dépendant pour le transport de médicaments contre les phénomènes de résistances / pH-responsive nanoscale drug delivery systems for overcoming drug resistance

Liu, Juan

22 November 2016

La résistance aux médicaments constitue un obstacle majeur pour le traitement du cancer. Les systèmes nanoparticulaires de délivrance de médicaments (nanoparticule drug delivery system, NDDS) sont pressentis pour apporter un nouvel espoir dans le traitement du cancer afin de surmonter la résistance aux médicaments en délivrant spécifiquement l’agent anticancéreux dans la lésion tumorale par effet EPR. Cela aura pour effet d’augmenter la concentration locale en médicaments et par conséquent d’améliorer l'efficacité thérapeutique tout en épargnant les tissus sains afin d'éviter les effets secondaires liés à la thérapie. Dans la mesure où la tumeur a souvent un microenvironnement acide, nous souhaiterions en outre doter nos nanoparticules NDDS d’une sensibilité pH-dépendante afin de permettre une délivrance spécifique dans la tumeur. Au cours de cette thèse, nous avons élaboré différents NDDSs sensibles aux variations de pH en employant des stratégies différentes. Ces NDDSs peuvent spécifiquement libérer le médicament au niveau du tissu tumoral et dans les cellules elles-mêmes à des valeurs de pH acides. En augmentant la concentration intracellulaire de médicament, l'objectif de surmonter la résistance aux médicaments pourrait ainsi être atteint. La présente étude a permis de fournir de nouvelles connaissances sur la conception de nano-transporteurs pour surmonter la résistance multidrogue par l’élaboration de NDDS sensibles au pH et constitue donc un exemple illustrant parfaitement le fait que les progrès des nanotechnologies peuvent être avantageusement mis en œuvre pour développer de nouvelles perspectives thérapeutiques. / Drug resistance presents a great hurdle to cancer treatment. Nanotechnology-based drug delivery systems (NDDSs) are widely expected to bring new hope for cancer therapy to overcome drug resistance by specifically delivering anticancer drugs to tumor lesions via the EPR effect, hence increasing local drug concentrations and consequently enhancing therapeutic efficacy, and at the same time, sparing healthy tissues to avoid side effects. As tumors often have an acidic microenvironment, we would like to further endow the NDDS with a pH-responsive drug releasing property for specific tumor targeting. In this thesis, we established different pH-responsive NDDSs by employing different strategies. These NDDSs could specifically control drug release at tumor tissues and within tumor cells in response to acidic pH. By increasing the intracellular drug concentration, the goal of circumventing drug resistance in cancer was achieved. The present study provides new insights into the design of nanocarriers to overcome drug resistance through pH-responsive drug delivery, and illustrates how advances in nanotechnology can be advantageously implemented to enhance therapeutic outcomes.

Traitement du cancer

Résistance aux médicaments

PH-Dépendance

Nano-Transporteur

Cancer therapy

Drug resistance

Nanoparticle-Based drug delivery system

PH-Response

Nanocarrier

540

Notch activation upon DNA damage : molecular characterisation and therapeutic applications in lung adenocarcinoma / Activation de la voie Notch en réponse aux dommages de l'ADN : caractérisation moléculaire et applications thérapeutiques dans l'adénocarcinome du poumon

Bernardo, Sara

15 November 2019

Le cancer du poumon est la principale cause de décès par cancer chez les hommes et les femmes dans le monde. Malgré les avancées majeures dans les traitements, les thérapies à base de platine restent la thérapie standard pour les patients atteints du cancer du poumon induit par la mutation KRAS. Bien que les composés de platine aient un premier effet sur ces patients, l’apparition d’une rechute constitue le principal défi au niveau clinique.Dans ce contexte, notre projet actuel vise à caractériser l’activation de la voie Notch dans la réponse aux sels de platines d’adénocarcinomes mutés pour K-Ras ainsi que son rôle dans l’acquisition de la résistance à ce traitement. Nous avons mis en évidence que la voie Notch est activée en réponse à divers agents induisant des dommages à l’ADN dans des lignées de cancer du poumon. Nous avons montré que cette activation est dépendante de la voie de checkpoint de Réponse aux Dommages de l’ADN (DDR) via ATM, ATM qui est une des principales kinases de la réponse cellulaire aux lésions de l’ADN telles que les cassures double-brin, causé notamment par la chimiothérapie conventionnelle. Parmi les nombreux substrats d’ATM en réponse à ces dommages, nous montrons un effet direct de MDM2 dans l’activation de la voie Notch en réponse aux dommages à l’ADN causé par le carboplatine. Nos données montrent une nouvelle interaction entre ATM, MDM2 et Notch, lors du traitement au carboplatine, qui pourrait jouer un rôle dans la cascade de signalisation favorisant la survie des cellules tumorales pulmonaires.En utilisant des xénogreffes dérivées de patients atteints d’adénocarcinomes du poumon, ainsi qu’un modèle cellulaire de xénogreffe résistant à la carboplatine, nous avons montré que l’association d’inhibiteurs de Notch et de MDM2 associé au traitement au carboplatine ont un effet accru sur le ralentissement de la croissance de la tumeur et sur la survie, en comparaison avec le traitement actuel de référence que représente le carboplatine.Nos résultats offrent une nouvelle possibilité de thérapie pour les adénocarcinomes de poumons mutés pour KRAS, et pourrait donc répondre à un besoin clinique urgent notamment pour contrecarrer la résistance aux chimiothérapies conventionnelles à base de sels de platine. / Lung cancer is the leading cause of cancer death among men and women worldwide. Despite the major advances in the treatments, platinum-based therapy remains the standard of care for patients affected by KRAS-driven lung cancer. Even though the platinum-compounds display an initial effect on these patients, the onset of the relapse constitutes the main challenge for the clinic. The molecular mechanisms underlying lung adenocarcinoma (LUAD) relapse are not completely elucidated yet, thus it is fundamental to understand them in order to improve survival of patients. Our data show that upon carboplatin treatment, the Notch pathway is activated in vitro. Since this effect was common for several other DNA damage insults, our driving hypothesis connected the DNA Damage Response (DDR) to the activation of the Notch pathway. Our data demonstrates that protein kinase ataxia telangiectasia-mutated (ATM) is a key mediator in the activation of the Notch pathway during DNA damage signalling. ATM is well-known as the chief mobilizer of the cellular response to the most toxic lesions to the DNA, the double-strand breaks which are also the type of damage caused by the conventional chemotherapy. Among the several substrates of ATM in response to the damage, there is the mouse double minute 2 protein (MDM2) that it is known to interact with the Notch pathway. Our data uncovered a new pathway connecting ATM, MDM2 and NICD during carboplatin treatment in LUAD cells.Using LUAD Patient-Derived Xenografts and a new generated carboplatin resistant cellular model, we show in vivo that the combination of Notch and MDM2 inhibitors with carboplatin showed a therapeutic benefit in tumour growth and survival compared to the standard of care, i.e. carboplatin.Our results can offer a new therapeutic window for KRAS-driven LUAD that become resistant to platinum-based therapy, hence tackling an urgent and unmet clinical need.

Cancer du poumon

Voie de signalisation Notch et DDR

Traitement du cancer bronchique

Résistance chimio-Induite

Lung cancer

Notch and DNA damage pathways;

Lung cancer therapy

Resistance to chemotherapy

Vitamin E Forms – Bioavailability and Protective Effects on Colitis and Colon Cancer

Kilia Y Liu (6623429)

12 October 2021

<p>Vitamin E is a natural lipophilic antioxidant contains eight structurally related forms, i.e., α-, β-, γ-, δ-tocopherols (αT, βT, γT, and δT) and corresponding tocotrienols. Recent research indicates that vitamin E forms are differentially metabolized to various carboxychromanols. Some these vitamin E metabolites have been shown to exhibit strong anti-inflammatory and anticancer effects, yet little is known about their bioavailability. Without this knowledge, it is impossible to assess the role of vitamin E metabolism in biological functions of vitamin E forms and their protective effects on chronic diseases. While αT and γT appear to improved gut health, the underlying mechanisms are not well understood. Furthermore, specific forms of vitamin E such as γT have been reported to have cancer-preventing effects, but their anticancer efficacy is relatively modest. For these reasons, this dissertation focused on the characterization of the pharmacokinetic formation of vitamin E metabolites after supplementation, and the investigation of the underlying mechanisms of the protective effect of vitamin E forms, αT and γT, on gut health, as well as anticancer efficacy of the combination of aspirin and γT on carcinogen-induced colon tumorigenesis.</p><p><br></p><p>The first project focuses on characterizing the pharmacokinetic formation of vitamin E metabolites after single dose supplementation of γ-tocopherol-rich mixed tocopherol (γTmT) and δ-tocotrienol (δTE). With our recently developed LC/MS/MS assay for quantifying vitamin E metabolites, we can simultaneously quantify the level of short-chain, long-chain, and sulfated carboxychromanols in plasma, urine, and fecal samples of supplemented animals. In this study, we investigated the pharmacokinetics including excretion of vitamin E forms and the formation of their metabolites after a single dose intragastric administration of tocopherols and tocotrienols in rats. We also measured vitamin E metabolites in the serum obtained from healthy humans after gT supplementation. In the plasma of rat, the pharmacokinetic profiles of γT and δTE are described as the following: γT, Cmax = 25.6 ± 9.1 μM, Tmax = 4 h; δTE, Cmax = 16.0 ± 2.3 μM, Tmax = 2 h. Sulfated CEHCs and sulfated 11’-COOHs were the predominant metabolites in the plasma of rat with Cmax of 0.4-0.5 μM (Tmax ~ 5-7 h) or ~0.3 μM (Tmax at 4.7 h), respectively. In 24-h urine, 2.7% of γT and 0.7% of dTE were excreted as conjugated CEHCs, the major identified urinary metabolites. In the feces, 17-45% of supplemented vitamers were excreted as un-metabolized forms and 4.9-9.2% as metabolites. The majority of metabolites excreted in feces were unconjugated carboxychromanols, among which 13’-COOHs constituted ~50% of total metabolites. Interestingly, 13’-COOHs derived from δTE were 2-fold higher than 13’-COOH from γT. Unlike rats, γ-CEHC is the predominant metabolites found in human plasma, although 11’-COOHs and 13’-COOHs (sulfated and unconjugated) were elevated by >20 folds responding to γT supplement. In this study, we found that tocopherols and tocotrienols, when taken as supplements, are mainly excreted as un-metabolized forms and long-chain carboxychromanols in feces. High fecal availability of 13’-COOHs may contribute to modulating effects on gut health.</p><p><br></p><p>The second project of my dissertation investigated the effect of vitamin E forms, αT and γT, on intestinal barrier function in a cellular model and a mouse colitis model. Inflammatory bowel diseases (IBD) are chronic idiopathic inflammatory conditions characterized by disruption of intestinal barrier integrity. Previous studies by others and us had demonstrated that vitamin E forms, αT and γT, can protect against chemical-induced colitis in animal models. However, the role of these vitamin E forms on intestinal barrier function has not been studied. Herein, we investigated the potential protective effects of vitamin E forms, αT and γT, on intestinal barrier function in a Caco-2 colon epithelial cell model and a dextran sodium sulfate (DSS)-induced colitis mouse model. In Caco-2 cells, pretreatment with 25mM αT and γT attenuated Caco-2 monolayer barrier dysfunction induced by 10 ng/mL TNF-α/IFN-γ, suggesting that these vitamin E forms protect intestinal barrier integrity in this cellular model. In male BALB/c mice, the supplementation of αT (0.05%) or γTmT (0.05%) when given 3 weeks before DSS treatment or at the same time as DSS treatment alleviated DSS-induced fecal bleeding and diarrhea symptoms in mice, and attenuated colon inflammation and colitis-associated damages. Additionally, αT and γTmT supplementation attenuated DSS-induced intestinal barrier dysfunction, as indicated by improving the level of occludin, a tight junction protein, in the colon and reducing lipopolysaccharide-binding protein (LBP) in the plasma. Furthermore, gut microbiota analysis demonstrated that αT and γTmT supplementation could modulate intestinal microbiome composition in mice with DSS treatment. DSS treatment reduced the relative abundance of Lachnospiraceae compared to healthy mice, and supplementation of αT and γT partially reversed this effect. Interestingly, the family Lachnospiraceae has been reported to decrease in IBD patients. Our study demonstrated the protective effects of vitamin E forms on intestinal barrier integrity in a cell-based model and a colitis model in mice. Furthermore, we demonstrated that these vitamin E forms caused favorable changes in the intestinal microbial population under colitis condition.</p><p><br></p><p>The third project of my dissertation evaluated the anticancer efficacy of the combination of aspirin and γT using an azoxymethane (AOM)-induced and colitis-promoted colon tumorigenesis mouse model. Extensive inflammation in the colon promotes the development of colorectal cancer (CRC). Eicosanoid production by pro-inflammatory enzymes, cyclooxygenases (COX-1 and COX-2) and 5-lipoxygenase (5-LOX) play a critical role in the initiation, progression, and invasion of CRC. Thus, nonsteroidal anti-inflammatory drugs (NSAIDs), such as aspirin, have been recommended for chemoprevention of CRC. However, long-term use of aspirin can cause many side effects, and the anticancer activity of aspirin is very modest. Previously, we have demonstrated that the combination of γT with aspirin prolonged the anti-inflammatory activity of aspirin and alleviated aspirin-associated adverse effects in a carrageenan-induced inflammation model in rats. Additionally, we found that the combination of γT and aspirin has stronger anticancer activity than aspirin or γT alone against HCT-116 human colorectal carcinoma cells. Therefore, we examined the anticancer effect of the combination of 0.025% aspirin and 0.05% γT against AOM-induced and DSS-promoted tumorigenesis in mice. In this study, we have found that the combination of aspirin and γT, but not aspirin or γT alone, suppressed colon tumorigenesis in mice, as indicated by 40% and 50% reduction in the multiplicity of total polyps (P < 0.05) and large adenomatous polyps (>2mm2, P < 0.05), respectively. More strikingly, the combination of aspirin and γT reduced the overall tumor area by 60% (P < 0.05). Noteworthy, the supplementation of γT also alleviated aspirin-induced stomach lesion and appeared to modulate intestinal microbial composition. Our study demonstrated that the combination of aspirin and γT has stronger anticancer activity than aspirin or γT alone while alleviates aspirin-associated adverse effect, suggesting that the combination of γT and aspirin is a more effective and safer chemopreventive agent for CRC than aspirin alone.</p>

Diseases

Gastroenterology and Hepatology

Nutritional Physiology

Inflammatory bowel diseases (IBD)

Cancer prevention

vitamin E treatment

pharmacokinetics

gut microbiota

Intestinal barrier function

RENCA macrobeads inhibit tumor cell growth via EGFR activation and regulation of MEF2 isoform expression

Martis, Prithy Caroline

12 August 2020

No description available.

Biomedical Research

RENCA macrobeads

cell-system anti-cancer therapy

systems-biological treatment approach

tumor inhibition

mechanism of action

EGFR

MEF2

reticulon-4

thrombospondin-1

tissue inhibitor of metalloproteinase-2

Induction of apoptosis in human cancer cells by targeting mitochondria with gold nanoparticles

Mkandawire, M. M., Lakatos, M., Springer, A., Clemens, A., Appelhans, D., Krause-Buchholz, U., Pompe, W., Rödel, G., Mkandawire, M.

16 December 2019

A major challenge in designing cancer therapies is the induction of cancer cell apoptosis, although activation of intrinsic apoptotic pathways by targeting gold nanoparticles to mitochondria is promising. We report an in vitro procedure targeting mitochondria with conjugated gold nanoparticles and investigating effects on apoptosis induction in the human breast cancer cell line Jimt-1. Gold nanoparticles were conjugated to a variant of turbo green fluorescent protein (mitoTGFP) harbouring an amino-terminal mitochondrial localization signal. Au nanoparticle conjugates were further complexed with cationic maltotriose-modified poly(propylene imine) third generation dendrimers. Fluorescence and transmission electron microscopy revealed that Au nanoparticle conjugates were directed to mitochondria upon transfection, causing partial rupture of the outer mitochondrial membrane, triggering cell death. The ability to target Au nanoparticles into mitochondria of breast cancer cells and induce apoptosis reveals an alternative application of Au nanoparticles in photothermal therapy of cancer.

info:eu-repo/classification/ddc/600

ddc:600

Využití rekombinantních virů vakcinie produkujících IGFBP3 pro terapii nádorů / IGFBP3 expressing rekombinant vaccinia virus used for tumor therapy

Musil, Jan

January 2010

IGFBP-3 expressing rekombinant vaccinia viruses used for tumor therapy Insulin-like growth factor-binding protein-3 (IGFBP-3) is a major regulator of endocrine effects of IGF and is capable to suppress the growth of variety of cancer. Several studies have shown that IGFBP-3 can induce the apoptosis of cancer cells via IGF-dependent and IGF-independent mechanisms. In our study, we have constructed recombinant vaccinia viruses (VACV) expressing IGFBP-3 under the control of the early H5 and synthetic early/late (E/L) promoter to investigate the potential effect on cancer growth in our cervical cancer model. We have shown that the expression of IGFBP-3 alone had no effect on tumor growth. On the other hand, the co-expression of IGFBP-3 enhanced the anti-cancer effect of immunization with the fusion protein SigE7LAMP, which gave rise to the anti-cancer immunity directed against HPV16 induced tumors. We have shown that the double-recombinant P13-SigE7LAMP-H5-IGFBP-3 can enhance the protective immune responses against MK16/ABC induced tumors. Furthermore, we have show that both double-recombinant viruses P13-SigE7LAMP-H5- IGFBP-3 and P13-SigE7LAMP-E/L-IGFBP-3 can increase the anti-cancer effect of SigE7LAMP expression in the therapy of TC-1 induced tumors. Key words: IGFBP-3, IGF, VACV, HPV16, E7 oncoprotein,...

Nové hybridní polymerní materiály na bázi polysacharidů využitelné v biomedicíně / Novel hybrid polysaccharide-based polymers for biomedicine

Loukotová, Lenka

January 2018

1 Abstract This doctoral thesis is focused on the synthesis and characterization of novel hybrid polysaccharide-based polymers applicable for biomedicine, specifically for a conceptually new bimodal cancer treatment - immunoradiotherapy. For this purpose, polysaccharides β-glucan from Auricularia auricula-judae and κ-carrageenan from Kappaphycus alvarezii, exhibiting immunostimulatory and anticancer activities, were chosen to be grafted with thermoresponsive poly(2-isopropyl-2-oxazoline-co-2-butyl-2-oxazoline)s (POXs) (with different graft lengths and grafting densities) that induced a lower critical solution temperature of the final polymers. The thermoresponsive behavior of resulting polymers was studied with temperature-dependent light scattering methods, fluorescence measurements and also nuclear magnetic spectroscopy to select a polymer material with the most suitable properties for the intended application, aiming at a polymer depot formation after the injection of a polymer solution into the body. The chosen polymer, β-glucan-graft-POX with graft length of 2500 Da, was then modified to bear 1,4,7,10-tetraazacyclododecane-1,4,7,10- tetraacetic acid and a fluorescent dye Dyomics-615 at the graft ends and tested first in vitro to investigate its immunostimulatory properties and also the cellular uptake....

Biomarker based therapies in high risk cancer patients - MACC1 as molecular target

Zincke, Fabian

13 January 2020

Das metastasierende kolorektale Karzinom stellt eine große Herausforderung in der Krebstherapie dar. Verlässliche und effiziente Biomarker zur Prognose des Krankheitsverlaufes oder der Therapieantwort (Prädiktion) sind rar. Metastasis-associated in colon cancer 1 (MACC1) ist ein prognostischer, prädiktiver und kausaler Biomarker für verschiedene Tumorentitäten. Durch die Induzierung von Zielgenen, wie z.B. MET, beeinflusst es Signalwege wie MEK/ERK und AKT/β-catenin und fördert so Zellproliferation und -motilität sowie Tumorprogression und Metastasierung in vivo. Diese Arbeit sollte neue Strategien erforschen diese Prozesse durch die Inhibition von MACC1 auf Transkriptions- und Signaltransduktionsebene zu unterbinden. Mit zwei verschiedenen Screeningmethoden konnten wir Statine als potente transkriptionelle Inhibitoren von MACC1 als auch phosphotyrosin (pY)-abhängige Interaktionen von MACC1 mit essentiellen Signalmolekülen identifizieren: SHP2, GRB2, SHC1, PLCG1 und STAT5B. Statine verringerten MACC1-spezifische Proliferation und Koloniebildung in vitro als auch Tumor Wachstum und Metastasierung in vivo bei Dosen äquivalent der humanen Standardtherapie zur Blutlipidsenkung. Mutation der pY-Bindungsstellen reduzierte die Aktivität des MACC1-induzierten ERK Signalwegs sowie Zellmigration und -proliferation. Anhand unserer Daten orchestriert MACC1, abhängig von MET und EGFR, neue SHP2/SRC/ERK und PKA/SRC/CREB Signalkaskaden zu einem malignen Phänotyp. Gezielte Intervention restringierte die MACC1-abhängige Koloniebildung, was neue therapeutische Interventionspunkte identifiziert und eine hervorragende Basis für Untersuchungen zur Kombinationstherapie darstellt. Die weitere Erforschung der spatiotemporalen Organisation des MACC1 Signalosoms und assoziierter Signalkaskaden soll das volle therapeutische Potential von MACC1 ausschöpfen. Wir empfehlen zudem Statine in der Krebstherapie bzw. -prävention, besonders bei MACC1-stratifzierten Patienten, anzuwenden. / Metastatic colorectal cancer still represents a major challenge in therapy. Reliable and efficient biomarkers for early prognosis of disease course or treatment response (prediction) remain scarce. Metastasis-associated in colon cancer 1 (MACC1) has been established as prognostic, predictive and causal biomarker for several tumor entities. Its induction of target genes such as MET affects several signaling pathways including MEK/ERK and AKT/β-catenin. Thus, it promotes cellular proliferation and motility as well as tumor progression and metastasis formation in vivo. This study intended to explore new strategies to inhibit these processes by targeting MACC1 on transcriptional and signaling level. By two distinct screening methods, we identified statins as potent MACC1 transcriptional inhibitors as well as phosphotyrosine (pY)-dependent interactions of MACC1 with crucial signaling molecules: SHP2, GRB2, SHC1, PLCG1 and STAT5B. Statins showed MACC1-specific reduction of proliferation and colony formation in vitro as well as restriction of tumor growth and metastasis formation in vivo at doses equivalent to human standard lipid reduction therapy. Mutation of the pY-interaction sites abrogated MACC1-dependent ERK signaling as well as cell migration and proliferation. Our data further suggest that MACC1 governs SHP2/SRC/ERK and PKA/SRC/CREB axes conferring a malignant phenotype in response to MET and EGFR. Targeted intervention restricted MACC1-dependent colony formation which indicates new drug intervention points for MACC1 signaling and provides an excellent baseline for further investigations of combinatorial treatments. Additional research about the spatiotemporal organization of MACC1 signalosome formation and downstream signaling will reveal the entire potential of MACC1 as therapeutic target, whereas statins should already be considered for cancer therapy or prevention, especially in patients stratified for MACC1 expression.

Biomarker

kolorektales Karzinom

transkriptionelle Inhibition

Signaltransduktion

Krebstherapie

MACC1

biomarker

colorectal cancer

transcriptional inhibition

signal transduction

cancer therapy

MACC1

570 Biowissenschaften; Biologie

XH 7212

XH 7215

ddc:570