A new approach for a physicochemical characterization of nanoparticles in complex media: a pilot study

Présentation PosterInternational audienceCurrent techniques used to measure the phys-icochemical characteristics of nanoparticles in simple media are poorly predictive of their behavior observed during in vivo experi-ments1. As a consequence, some pharmaco-kinetic or toxicokinetic issues are detected too late. In this contribution, we are proposing an innovative approach to tackle this challenge2. The goal is to develop a generic characteriza-tion process that could be used in any labora-tory with different categories of measurement technologies. The proposed solution is com-posed of three main steps:1.Sample preparation;2.Measurement phase;3.Statistical analysis.The sample preparation relies on a set of n serum-free media initially designed for cell culture but used herein to mimic heterogenei-ty of biological context. Each culture medium is composed of a large number (p), around a hundred, of biological compounds (proteins, vitamins, mineral salts, etc.), which may indi-vidually and synergistically interact with the nanoparticle surface. The nanoparticle to be characterized is added to each medium of the kit with the same concentration.The resulting mixtures are then analyzed by an appropriate technology compatible with complex media to measure the size distribu-tion of constitutive nano-objects. In a third step, all the experimental data com-ing from the n series of measurement are used to solve a “ large p small n” regression problem. This statistical analysis informs about the most likely medium compounds to affect the size distribution of nanoparticles compared to their initial dimensions. This communication presents the first results of a pilot study in which the proposed approach was tested on gold nanoparticles mixed in n=8 cell free culture media provided by Thermo Fisher Scientific. The nanoparticle size distributions were measured by a Dy-namic light scattering system (Nanosight, Malvern). A partial least squares method was used to solve the “ large p small n” regression problem. Preliminary results confirms signifi-cant changes of the size distribution between the culture media and the feasibility of the statistical method to identify a set of medium compounds that may explain those variations

Monte Carlo simulations guided by imaging to predict the in vitro ranking of radiosensitizing nanoparticles

International audienceThis article addresses the in silico–in vitro prediction issue of organometallic nanoparticles (NPs)-based radiosensitization enhancement. The goal was to carry out computational experiments to quickly identify efficient nanostructures and then to preferentially select the most promising ones for the subsequent in vivo studies. To this aim, this interdisciplinary article introduces a new theoretical Monte Carlo computational ranking method and tests it using 3 different organometallic NPs in terms of size and composition. While the ranking predicted in a classical theoretical scenario did not fit the reference results at all, in contrast, we showed for the first time how our accelerated in silico virtual screening method, based on basic in vitro experimental data (which takes into account the NPs cell biodistribution), was able to predict a relevant ranking in accordance with in vitro clonogenic efficiency. This corroborates the pertinence of such a prior ranking method that could speed up the preclinical development of NPs in radiation therapy

Are the anti-EGFR targeted therapies having an anti-angiogenic effect? In vitro study of angiogenesis induced by head and neck squamous cell carcinoma exposed to cetuximab

La surexpression du récepteur EGFR a un rôle majeur dans le développement des carcinomes des voies aérodigestives supérieures (VADS) et son inhibition par les anticorps anti-EGFR (cetuximab) induit un effet anti-tumoral mais pourrait également avoir un effet anti-angiogénique. Cependant, les effets de ces agents sur l'angiogenèse et les cellules endothéliales (CE) n'ont pas réellement été évalués. L'objectif de ce travail est d'étudier l'angiogenèse induite par les molécules libérées par les cellules tumorales des VADS (Cal27, FaDu) dans les milieux de culture en présence ou non de cetuximab, appelés milieux conditionnés (CM). Le cetuximab n'a pas d'effet direct significatif sur les CE. Il induit une diminution de la sécrétion de VEGF par les cellules tumorales mais paradoxalement, les CM obtenus induisent un effet pro-angiogénique. L'analyse de la composition des CM ne permet pas d'identifier de molécule clé responsable de cet effet, le cetuximab diminuant à la fois la sécrétion tumorale des facteurs pro- et anti-angiogéniques. Pour expliquer ce paradoxe et en accord avec la littérature, nous avons mis en évidence une libération de microvésicules par nos cellules tumorales (TMV), TMV exprimant EGFR et TF, et une régulation de cette libération et de leur contenu par le cetuximab. Ces TMV peuvent interagir avec les CE et le cetuximab favoriserait cette interaction. La caractérisation de ces TMV et leur rôle dans le processus angiogénique en réponse ou non au cetuximab permettront dans le futur de comprendre la réelle activité des anticorps anti-EGFR sur l'angiogenèseOverexpression of EGFR has a major role in the development of head and neck squamous cell carcinoma (HNSCC) and its inhibition by anti-EGFR antibodies (cetuximab) induced an anti-tumor effect but could also induce an anti-angiogenic effect. However, the effects of these agents onto angiogenesis and endothelial cells (EC) have not really been evaluated. The objective of this work is to study angiogenesis induced by mediators released by head and neck squamous carcinoma cells (Cal27, FaDu) in culture media with or without cetuximab exposure, known as conditioned media (CM). Cetuximab has no significant direct effect on EC. It induces a decrease in the secretion of VEGF by tumor cells but, paradoxically, the CM induces a pro-angiogenic effect. The analysis of the composition of the CM does not allow us to identify a key molecule responsible for this effect because cetuximab decreases the secretion of both pro- and anti-angiogenic factors by tumor cells. To explain this paradox and in agreement with the literature, we highlighted the release of microvesicles by our tumor cells (TMV), TMV which express EGFR and TF, and regulation of this release and the content of TMV after cetuximab exposure. These TMV may interact with the EC and cetuximab increases this interaction. Further characterization of TMV and studying their role in the angiogenic process in response to cetuximab will allow us in the future to understand the real activity of anti-EGFR antibodies onto angiogenesi

Les thérapies ciblées anti-EGFR ont-elles un réel effet anti-angiogénique ? Etude in vitro de l'angiogenèse induite par des cellules cancéreuses des VADS traitées ou non par le Cetuximab

Overexpression of EGFR has a major role in the development of head and neck squamous cell carcinoma (HNSCC) and its inhibition by anti-EGFR antibodies (cetuximab) induced an anti-tumor effect but could also induce an anti-angiogenic effect. However, the effects of these agents onto angiogenesis and endothelial cells (EC) have not really been evaluated. The objective of this work is to study angiogenesis induced by mediators released by head and neck squamous carcinoma cells (Cal27, FaDu) in culture media with or without cetuximab exposure, known as conditioned media (CM). Cetuximab has no significant direct effect on EC. It induces a decrease in the secretion of VEGF by tumor cells but, paradoxically, the CM induces a pro-angiogenic effect. The analysis of the composition of the CM does not allow us to identify a key molecule responsible for this effect because cetuximab decreases the secretion of both pro- and anti-angiogenic factors by tumor cells. To explain this paradox and in agreement with the literature, we highlighted the release of microvesicles by our tumor cells (TMV), TMV which express EGFR and TF, and regulation of this release and the content of TMV after cetuximab exposure. These TMV may interact with the EC and cetuximab increases this interaction. Further characterization of TMV and studying their role in the angiogenic process in response to cetuximab will allow us in the future to understand the real activity of anti-EGFR antibodies onto angiogenesisLa surexpression du récepteur EGFR a un rôle majeur dans le développement des carcinomes des voies aérodigestives supérieures (VADS) et son inhibition par les anticorps anti-EGFR (cetuximab) induit un effet anti-tumoral mais pourrait également avoir un effet anti-angiogénique. Cependant, les effets de ces agents sur l'angiogenèse et les cellules endothéliales (CE) n'ont pas réellement été évalués. L'objectif de ce travail est d'étudier l'angiogenèse induite par les molécules libérées par les cellules tumorales des VADS (Cal27, FaDu) dans les milieux de culture en présence ou non de cetuximab, appelés milieux conditionnés (CM). Le cetuximab n'a pas d'effet direct significatif sur les CE. Il induit une diminution de la sécrétion de VEGF par les cellules tumorales mais paradoxalement, les CM obtenus induisent un effet pro-angiogénique. L'analyse de la composition des CM ne permet pas d'identifier de molécule clé responsable de cet effet, le cetuximab diminuant à la fois la sécrétion tumorale des facteurs pro- et anti-angiogéniques. Pour expliquer ce paradoxe et en accord avec la littérature, nous avons mis en évidence une libération de microvésicules par nos cellules tumorales (TMV), TMV exprimant EGFR et TF, et une régulation de cette libération et de leur contenu par le cetuximab. Ces TMV peuvent interagir avec les CE et le cetuximab favoriserait cette interaction. La caractérisation de ces TMV et leur rôle dans le processus angiogénique en réponse ou non au cetuximab permettront dans le futur de comprendre la réelle activité des anticorps anti-EGFR sur l'angiogenès

Les thérapies ciblées anti-EGFR ont-elles un réel effet anti-angiogénique ? Etude in vitro de l'angiogenèse induite par des cellules cancéreuses des VADS traitées ou non par le Cetuximab

La surexpression du récepteur EGFR a un rôle majeur dans le développement des carcinomes des voies aérodigestives supérieures (VADS) et son inhibition par les anticorps anti-EGFR (cetuximab) induit un effet anti-tumoral mais pourrait également avoir un effet anti-angiogénique. Cependant, les effets de ces agents sur l'angiogenèse et les cellules endothéliales (CE) n'ont pas réellement été évalués. L'objectif de ce travail est d'étudier l'angiogenèse induite par les molécules libérées par les cellules tumorales des VADS (Cal27, FaDu) dans les milieux de culture en présence ou non de cetuximab, appelés milieux conditionnés (CM). Le cetuximab n'a pas d'effet direct significatif sur les CE. Il induit une diminution de la sécrétion de VEGF par les cellules tumorales mais paradoxalement, les CM obtenus induisent un effet pro-angiogénique. L'analyse de la composition des CM ne permet pas d'identifier de molécule clé responsable de cet effet, le cetuximab diminuant à la fois la sécrétion tumorale des facteurs pro- et anti-angiogéniques. Pour expliquer ce paradoxe et en accord avec la littérature, nous avons mis en évidence une libération de microvésicules par nos cellules tumorales (TMV), TMV exprimant EGFR et TF, et une régulation de cette libération et de leur contenu par le cetuximab. Ces TMV peuvent interagir avec les CE et le cetuximab favoriserait cette interaction. La caractérisation de ces TMV et leur rôle dans le processus angiogénique en réponse ou non au cetuximab permettront dans le futur de comprendre la réelle activité des anticorps anti-EGFR sur l'angiogenèseOverexpression of EGFR has a major role in the development of head and neck squamous cell carcinoma (HNSCC) and its inhibition by anti-EGFR antibodies (cetuximab) induced an anti-tumor effect but could also induce an anti-angiogenic effect. However, the effects of these agents onto angiogenesis and endothelial cells (EC) have not really been evaluated. The objective of this work is to study angiogenesis induced by mediators released by head and neck squamous carcinoma cells (Cal27, FaDu) in culture media with or without cetuximab exposure, known as conditioned media (CM). Cetuximab has no significant direct effect on EC. It induces a decrease in the secretion of VEGF by tumor cells but, paradoxically, the CM induces a pro-angiogenic effect. The analysis of the composition of the CM does not allow us to identify a key molecule responsible for this effect because cetuximab decreases the secretion of both pro- and anti-angiogenic factors by tumor cells. To explain this paradox and in agreement with the literature, we highlighted the release of microvesicles by our tumor cells (TMV), TMV which express EGFR and TF, and regulation of this release and the content of TMV after cetuximab exposure. These TMV may interact with the EC and cetuximab increases this interaction. Further characterization of TMV and studying their role in the angiogenic process in response to cetuximab will allow us in the future to understand the real activity of anti-EGFR antibodies onto angiogenesisNANCY1-Bib. numérique (543959902) / SudocSudocFranceF

Effect of cetuximab treatment on induction of angiogenesis by HNSCC cell line depending on PTEN expression

International audienceOur work aimed to identify the ability of the HNSCC cell line Cal 27 to induce angiogenesis, regarding PTEN expression and anti-EGFR treatment. Cal 27, a human HNSCC cell line expressing PTEN has been transfected by a PTEN-siRNA and exposed to cetuximab for 48 hours. The culture media were then collected to be used as conditionned media for HUVEC and aortic rings culture. Aortic rings sprouting and tubular structures from HUVEC have been investigated by microscopy and quantified by AngioQuant software. The conditioned media have been also characterized by an analysis of key factors involved in angiogenesis regulation using Proteome Profiler Array. The anti-angiogenic effect of cetuximab in HNSCC seems to result from a direct effect of the anti-EGFR on endothelial cells rather than an effect mediated by tumoral cells, despite a VEGF concentration significantly lower due to cetuximab exposure. PTEN is involved in the regulation of vasculature in HNSCC. But surprisingly, loss of PTEN expression in Cal 27 leads to a reduction of the tumoral cells ability to induce angiogenesis. This process is not linked to the VEGF concentration changes but is mediated by a global change in the molecular constitution of conditioned media

Photomolecular beacon ciblant LRP-1, activables par les MMPs pour traiter le glioblastome par thérapie photodynamique.

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New targeted gold nanorods for the treatment of glioblastoma by photodynamic therapy

International audienceThis study describes the employment of gold nanorods (AuNRs), known for their good reputation in hyperthermia-based cancer therapy, in a hybrid combination of photosensitizers (PS) and peptides (PP). We report here, the design and the synthesis of this nanosystem and its application as a vehicle for the selective drug delivery and the efficient photodynamic therapy (PDT). AuNRs were functionalized by polyethylene glycol, phototoxic pyropheophorbide-a (Pyro) PS, and a “KDKPPR” peptide moiety to target neuropilin-1 receptor (NRP-1). The physicochemical characteristics of AuNRs, the synthesized peptide and the intermediate PP-PS conjugates were investigated. The photophysical properties of the hybrid AuNRs revealed that upon conjugation, the AuNRs acquired the characteristic properties of Pyro concerning the extension of the absorption profile and the capability to fluoresce (Φf = 0.3) and emit singlet oxygen (ΦΔ = 0.4) when excited at 412 nm. Even after being conjugated onto the surface of the AuNRs, the molecular affinity of “KDKPPR” for NRP-1 was preserved. Under irradiation at 652 nm, in vitro assays were conducted on glioblastoma U87 cells incubated with different PS concentrations of free Pyro, intermediate PP-PS conjugate and hybrid AuNRs. The AuNRs showed no cytotoxicity in the absence of light even at high PS concentrations. However, they efficiently decreased the cell viability by 67% under light exposure. This nanosystem possesses good efficiency in PDT and an expected potential effect in a combined photodynamic/photothermal therapy guided by NIR fluorescence imaging of the tumors due to the presence of both the hyperthermic agent, AuNRs, and the fluorescent active phototoxic PS

Inclusion complex vs. conjugation of hydrophobic photosensitizers with β-cyclodextrin: Improved disaggregation and photodynamic therapy efficacy against glioblastoma cells

International audienceSelf-aggregation of hydrophobic porphyrin-based photosensitizers (PSs) in aqueous biological environment decreases their bioavailability and in vivo therapeutic efficacy, which hampers their clinical use in photodynamic therapy (PDT). In the current study, we explore three new supramolecular systems based of hydrophobic PSs (i.e. 5,10,15,20-tetrakis(3-hydroxyphenyl)porphyrin (mTHPP) or 5-(4-carboxyphenyl)-10,15,20-triphenylporphyrin (P1COOH)) non-covalently or covalently attached to β-CD. The two non-covalent solid inclusion complexes (β-CD)2/mTHPP and [(β-CD)/P1COOH]4 are prepared by a new co-precipitation@lyophilization combined method and the covalent conjugate β-CD-P1 by click chemistry. The binding type effect and effectiveness on the disaggregation in aqueous medium and in vitro PDT efficacy against glioblastoma cancer cells of PSs are investigated for the three β-CD/PS systems. The findings reveal a remarkable improvement of the disaggregation and in vitro PDT activity of these β-CD/PS systems compared to the free PSs, except for [(β-CD)/P1COOH]4 inclusion complex caused by J-type self-aggregation of the inclusion complex in tetrameric form. β-CD-P1 conjugate shows the higher in vitro PDT efficacy compared to the other β-CD/PS systems. Overall, the results indicate that the disaggregation in aqueous medium and in vitro PDT activity of hydrophobic PSs can be improved by their binding to β-CD and the covalent binding is the best approach

Pouvoir radiopotentialisant in vitro de nanoparticules hybrides à base de métaux.

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