Davide Staedler
École Polytechnique Fédérale de Lausanne
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Featured researches published by Davide Staedler.
ACS Nano | 2012
Davide Staedler; Thibaud Magouroux; Rachid Hadji; Cécile Joulaud; Jérôme Extermann; Sebastian Schwung; Solène Passemard; Christelle Kasparian; Gareth Clarke; Mathias Gerrmann; Ronan Le Dantec; Yannick Mugnier; Daniel Rytz; Daniel Ciepielewski; Christine Galez; Sandrine Gerber-Lemaire; Lucienne Juillerat-Jeanneret; Luigi Bonacina; Jean-Pierre Wolf
Nonlinear optical nanocrystals have been recently introduced as a promising alternative to fluorescent probes for multiphoton microscopy. We present for the first time a complete survey of the properties of five nanomaterials (KNbO(3), LiNbO(3), BaTiO(3), KTP, and ZnO), describing their preparation and stabilization and providing quantitative estimations of their nonlinear optical response. In the light of their prospective use as biological and clinical markers, we assess their biocompatibility on human healthy and cancerous cell lines. Finally, we demonstrate the great potential for cell imaging of these inherently nonlinear probes in terms of optical contrast, wavelength flexibility, and signal photostability.
Angewandte Chemie | 2013
Reto Frei; Davide Staedler; Aruna Raja; Raimo Franke; Florenz Sasse; Sandrine Gerber-Lemaire; Jerome Waser
The first total synthesis of the alkaloid natural product jerantinine E is based on a selective cyclization of an aminocyclopropane. Preliminary investigations show that it inhibits the polymerization of tubulin, displaying significant cytotoxicity and antimigratory activity against both breast and lung cancer cell lines.
Bioconjugate Chemistry | 2011
Françoise Borcard; Aurélien Godinat; Davide Staedler; Horacio Comas Blanco; Anne-Laure Dumont; Catherine Chapuis-Bernasconi; Corinne Scaletta; Lee Ann Applegate; Franziska Krauss Juillerat; Urs T. Gonzenbach; Sandrine Gerber-Lemaire; Lucienne Juillerat-Jeanneret
The chemical functionalization of cell-surface proteins of human primary fetal bone cells with hydrophilic bioorthogonal intermediates was investigated. Toward this goal, chemical pathways were developed for click reaction-mediated coupling of alkyne derivatives with cellular azido-expressing proteins. The incorporation via a tetraethylene glycol linker of a dipeptide and a reporter biotin allowed the proof of concept for the introduction of cell-specific peptide ligands and allowed us to follow the reaction in living cells. Tuning the conditions of the click reaction resulted in chemical functionalization of living human fetal osteoblasts with excellent cell survival.
ACS Photonics | 2015
Andrii Rogov; Marie Irondelle; Fernanda Ramos Gomes; Julia Bode; Davide Staedler; Solène Passemard; Sébastien Courvoisier; Yasuaki Yamamoto; François Waharte; Daniel Ciepielewski; Philippe Rideau; Sandrine Gerber-Lemaire; Frauke Alves; Jean Salamero; Luigi Bonacina; Jean-Pierre Wolf
We investigate the use of bismuth ferrite (BFO) nanoparticles for tumor tissue labeling in combination with infrared multiphoton excitation at 1250 nm. We report the efficient and simultaneous generation of second- and third-harmonic signals by the nanoparticles. On this basis, we set up a novel imaging protocol based on the co-localization of the two harmonic signals and demonstrate its benefits in terms of increased selectivity against endogenous background sources in tissue samples. Finally, we discuss the use of BFO nanoparticles as mapping reference structures for correlative light–electron microscopy.
Journal of Applied Physics | 2014
Sebastian Schwung; Andrii Rogov; Gareth Clarke; Céline Joulaud; Thibaud Magouroux; Davide Staedler; Solène Passemard; Thomas Jüstel; Laurent Badie; Christine Galez; Jean-Pierre Wolf; Yuri Volkov; Adriele Prina-Mello; Sandrine Gerber-Lemaire; Daniel Rytz; Yannick Mugnier; Luigi Bonacina; Ronan Le Dantec
Second Harmonic Generation (SHG) from BiFeO3 nanocrystals is investigated for the first time to determine their potential as biomarkers for multiphoton imaging. Nanocrystals are produced by an auto-combustion method with 2-amino-2-hydroxymethyl-propane-1,3-diol as a fuel. Stable colloidal suspensions with mean particle diameters in the range 100–120 nm are then obtained after wet-milling and sonication steps. SHG properties are determined using two complementary experimental techniques, Hyper Rayleigh Scattering and nonlinear polarization microscopy. BiFeO3 shows a very high second harmonic efficiency with an averaged 〈d〉 coefficient of 79 ± 12 pm/V. From the nonlinear polarization response of individual nanocrystals, relative values of the independent dij coefficients are also determined and compared with recent theoretical and experimental studies. Additionally, the particles show a moderate magnetic response, which is attributed to γ-Fe2O3 impurities. A combination of high nonlinear optical efficiency and magnetic response within the same particle is of great interest for future bio-imaging and diagnostic applications.
Journal of Medicinal Chemistry | 2012
Davide Staedler; Catherine Chapuis-Bernasconi; Henrietta Dehmlow; Holger Fischer; Lucienne Juillerat-Jeanneret; Johannes Aebi
Ten oxidosqualene cyclase inhibitors with high efficacy as cholesterol-lowering agents and of different chemical structure classes were evaluated as potential anticancer agents against human cancer cells from various tissue origins and nontumoral human-brain-derived endothelial cells. Inhibition of cancer cell growth was demonstrated at micromolar concentrations, comparable to the concentrations of statins necessary for antitumor effect. Human glioblastoma cells were among the most sensitive cells. These compounds were also able to decrease the proliferation of angiogenic brain-derived endothelial cells, as a model of tumor-induced neovasculation. Additive effects in human glioblastoma cells were also demonstrated for oxidosqualene cyclase inhibitors in combination with atorvastatin while maintaining selectivity against endothelial cells. Thus, not only statins targeting the 3-hydroxy-3-methylglutaryl coenzyme A reductase but also inhibitors of oxidosqualene cyclase decrease tumor growth, suggesting new therapeutic opportunities of combined anti-cholesterol agents for dual treatment of glioblastoma.
Nanomedicine: Nanotechnology, Biology and Medicine | 2015
Davide Staedler; Solène Passemard; Thibaud Magouroux; Andrii Rogov; Ciaran Manus Maguire; Bashir M. Mohamed; Sebastian Schwung; Daniel Rytz; Thomas Jüstel; Stéphanie Hwu; Yannick Mugnier; Ronan Le Dantec; Yuri Volkov; Sandrine Gerber-Lemaire; Adriele Prina-Mello; Luigi Bonacina; Jean-Pierre Wolf
UNLABELLED Bismuth Ferrite (BFO) nanoparticles (BFO-NP) display interesting optical (nonlinear response) and magnetic properties which make them amenable for bio-oriented diagnostic applications as intra- and extra membrane contrast agents. Due to the relatively recent availability of this material in well dispersed nanometric form, its biocompatibility was not known to date. In this study, we present a thorough assessment of the effects of in vitro exposure of human adenocarcinoma (A549), lung squamous carcinoma (NCI-H520), and acute monocytic leukemia (THP-1) cell lines to uncoated and poly(ethylene glycol)-coated BFO-NP in the form of cytotoxicity, haemolytic response and biocompatibility. Our results support the attractiveness of the functional-BFO towards biomedical applications focused on advanced diagnostic imaging. FROM THE CLINICAL EDITOR Bismuth Ferrite nanoparticles (BFO-NP) have been recently successfully introduced as photodynamic tools and imaging probes. However, how these nanoparticles interact with various cells at the cellular level remains poorly understood. In this study, the authors performed in vitro experiments to assess the effects of uncoated and PEG-coated BFO-NP in the form of cytotoxicity, haemolytic response and biocompatibility.
Bioorganic & Medicinal Chemistry Letters | 2013
Solène Passemard; Davide Staedler; Lucia Učňová; Guillaume Stéphane Schneiter; Phally Kong; Luigi Bonacina; Lucienne Juillerat-Jeanneret; Sandrine Gerber-Lemaire
A straightforward route is proposed for the multi-gram scale synthesis of heterobifunctional poly(ethylene glycol) (PEG) oligomers containing combination of triethyloxysilane extremity for surface modification of metal oxides and amino or azido active end groups for further functionalization. The suitability of these PEG derivatives to be conjugated to nanomaterials was shown by pegylation of ultrasmall superparamagnetic iron oxide (USPIO) nanoparticles (NPs), followed by functionalization with small peptide ligands for biomedical applications.
Nanoscale | 2014
Davide Staedler; Thibaud Magouroux; Solène Passemard; Sebastian Schwung; Marc Dubled; Guillaume Stéphane Schneiter; Daniel Rytz; Sandrine Gerber-Lemaire; Luigi Bonacina; Jean-Pierre Wolf
A novel bio-photonics approach based on the nonlinear optical process of second harmonic generation by non-centrosymmetric nanoparticles is presented and demonstrated on malignant human cell lines. The proposed method allows to directly interact with DNA in absence of photosensitizing molecules, to enable independent imaging and therapeutic modalities switching between the two modes of operation by simply tuning the excitation laser wavelength, and to avoid any risk of spontaneous activation by any natural or artificial light source. ∗To whom correspondence should be addressed †Institute of Chemical Sciences and Engineering, EPFL, CH-1015, Lausanne, Switzerland ‡GAP-Biophotonics, Université de Genève, 22 chemin de Pinchat, CH-1211 Genève 4, Switzerland ¶FEE Gmbh, Struthstrasse 2, 55743 Idar-Oberstein, Germany §SYMME, Université de Savoie, BP 80439, 74944, Annecy Le Vieux Cedex, France ‖Contributed equally to this work. 1 ar X iv :1 30 6. 64 87 v1 [ ph ys ic s. bi oph ] 2 7 Ju n 20 13 We demonstrate here a novel diagnostic and therapeutic (theranostic) protocol based on the nonlinear optical process of non phase-matched second harmonic (SH) generation by non-centrosymmetric nanoparticles, referred to in the following as harmonic nanoparticles (HNPs).1,2 To date, the capability of these recently introduced nanometric probes of doubling any incoming frequency has not been employed for therapeutic use, although it presents several straightforward advantages, including i) the possibility to directly interact with DNA of malignant cells in absence of photosensitizing molecules, ii) fully independent access to imaging and therapeutic modalities, and iii) complete absence of risk of spontaneous activation by natural or artificial light sources other than pulsed femtosecond lasers. Given the unconstrained tunability of the HNPs nonlinear conversion process, this approach can be extended to selectively photo-activate molecules at the surface or in the vicinity of HNPs to further diversify the prospective therapeutic action.3 Here we show that by tuning the frequency of ultrashort laser pulses from infrared (IR) to visible (both harmless), SH generation leads respectively to diagnostics (imaging) and therapy (phototoxicity). Specifically, we report in situ generation of deep ultraviolet (DUV) radiation (270 nm) in human-derived lung cancer cells treated with bismuth ferrite (BiFeO3, BFO) HNPs upon pulsed laser irradiation in the visible spectrum, at 540 nm. We observe and quantify the appearance of double-strand breaks (DSBs) in the DNA and cell apoptosis, in the area of the laser beam. We show that DNA damages are dependent on irradiation-time, laser intensity, and NP concentration. We observe that apoptosis and genotoxic effects are only observed when visible light excitation is employed, being completely absent when IR excitation is used for imaging. HNPs, a family of NPs specifically conceived for multi-photon imaging, were introduced in 2005 for complementing fluorescence imaging labels.1,4,5 Although comparatively less bright than quantum dots, HNPs possess a series of advantageous optical properties, including complete absence of bleaching and blinking,1,6 spectrally narrow emission bands, fully coherent response,7–9 ,and UV to IR excitation wavelength tunability.10,11 These unique characteristics have been recently exploited in demanding bio-imaging applications12 including regenerative research.13 The possibility of working with long wavelengths presents clear advantages in terms of tissue pene-A biophotonics approach based on the nonlinear optical process of second harmonic generation is presented and demonstrated on malignant human cell lines labelled by harmonic nanoparticles. The method enables independent imaging and therapeutic action, selecting each modality by simply tuning the excitation laser wavelength from infrared to visible. In particular, the generation of deep ultraviolet radiation at 270 nm allows direct interaction with nuclear DNA in the absence of photosensitizing molecules.
International Journal of Nanomedicine | 2014
Catherine A. Schütz; Davide Staedler; Kieran Crosbie-Staunton; Dania Movia; Catherine Chapuis Bernasconi; Blanka Halamoda Kenzaoui; Adriele Prina-Mello; Lucienne Juillerat-Jeanneret
Therapeutic engineered nanoparticles (NPs), including ultrasmall superparamagnetic iron oxide (USPIO) NPs, may accumulate in the lower digestive tract following ingestion or injection. In order to evaluate the reaction of human colon cells to USPIO NPs, the effects of non-stabilized USPIO NPs (NS-USPIO NPs), oleic-acid-stabilized USPIO NPs (OA-USPIO NPs), and free oleic acid (OA) were compared in human HT29 and CaCo2 colon epithelial cancer cells. First the biophysical characteristics of NS-USPIO NPs and OA-USPIO NPs in water, in cell culture medium supplemented with fetal calf serum, and in cell culture medium preconditioned by HT29 and CaCo2 cells were determined. Then, stress responses of the cells were evaluated following exposure to NS-USPIO NPs, OA-USPIO NPs, and free OA. No modification of the cytoskeletal actin network was observed. Cell response to stress, including markers of apoptosis and DNA repair, oxidative stress and degradative/autophagic stress, induction of heat shock protein, or lipid metabolism was determined in cells exposed to the two NPs. Induction of an autophagic response was observed in the two cell lines for both NPs but not free OA, while the other stress responses were cell- and NP-specific. The formation of lipid vacuoles/droplets was demonstrated in HT29 and CaCo2 cells exposed to OA-USPIO NPs but not to NS-USPIO NPs, and to a much lower level in cells exposed to equimolar concentrations of free OA. Therefore, the induction of lipid vacuoles in colon cells exposed to OA utilized as a stabilizer for USPIO NPs is higly amplified compared to free OA, and is not observed in the absence of this lipid in NS-USPIO NPs.