Frida Ryttsén
University of Gothenburg
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Publication
Featured researches published by Frida Ryttsén.
Nature | 2001
Anders Karlsson; Roger Karlsson; Mattias Karlsson; Ann-Sofie Cans; Anette Strömberg; Frida Ryttsén; Owe Orwar
We have constructed complex two-dimensional microscopic networks of phospholipid bilayer nanotubes and containers in which we are able to control the connectivity, container size, nanotube length, and angle between the nanotube extensions. Containers within these networks can be chemically differentiated and materials successfully routed between two containers connected by a common nanotube. These networks will enable model systems to be devised for studying confined biochemical reactions, intracellular transport phenomena and chemical computations.
Current Opinion in Biotechnology | 2003
Jessica Olofsson; Kerstin Nolkrantz; Frida Ryttsén; Bradley A. Lambie; Stephen G. Weber; Owe Orwar
Electroporation is a widely used method for the introduction of polar and charged agents such as dyes, drugs, DNA, RNA, proteins, peptides, and amino acids into cells. Traditionally, electroporation is performed with large electrodes in a batch mode for treatment of a large number of cells in suspension. Recently, microelectrodes that can produce extremely localized electric fields, such as solid carbon fiber microelectrodes, electrolyte-filled capillaries and micropipettes as well as chip-based microfabricated electrode arrays, have proven useful to electroporate single cells and subcellular structures. Single-cell electroporation opens up a new window of opportunities in manipulating the genetic, metabolic, and synthetic contents of single targeted cells in tissue slices, cell cultures, in microfluidic channels or at specific loci on a chip-based device.
Biophysical Journal | 2000
Frida Ryttsén; Cecilia Farre; Carrie Brennan; Stephen G. Weber; Kerstin Nolkrantz; Kent Jardemark; Daniel T. Chiu; Owe Orwar
Electroporation of single NG108-15 cells with carbon-fiber microelectrodes was characterized by patch-clamp recordings and fluorescence microscopy. To minimize adverse capacitive charging effects, the patch-clamp pipette was sealed on the cell at a 90(o) angle with respect to the microelectrodes where the applied potential reaches a minimum. From transmembrane current responses, we determined the electric field strengths necessary for ion-permeable pore formation and investigated the kinetics of pore opening and closing as well as pore open times. From both patch-clamp and fluorescence microscopy experiments, the threshold transmembrane potentials for dielectric breakdown of NG108-15 cells, using 1-ms rectangular waveform pulses, was approximately 250 mV. The electroporation pulse preceded pore formation, and analyte entry into the cells was dictated by concentration, and membrane resting potential driving forces. By stepwise moving a cell out of the focused field while measuring the transmembrane current response during a supramaximal pulse, we show that cells at a distance of approximately 30 microm from the focused field were not permeabilized.
Molecular and Cellular Neuroscience | 2001
Maria A.I. Åberg; Frida Ryttsén; Gunnel Hellgren; Kajsa Lindell; Lars Rosengren; A. J. MacLennan; Björn Carlsson; Owe Orwar; Peter Eriksson
We have developed a novel method in which antisense DNA is selectively electroporated into individual adult neural progenitor cells. By electroporation of antisense oligonucleotides against signal transducer and activator of transcription 3 (STAT3) we demonstrate that ciliary neurotrophic factor (CNTF) is an instructive signal for astroglial type 2 cell fate specifically mediated via activation of STAT3. Activation of the mitogen-activated protein kinase (MAPK) signaling pathway induced only a transient increase in glial fibrillary acidic protein (GFAP) expression, and inhibition of this signaling pathway did not block the induction by CNTF of glial differentiation in progenitor cells. In addition we show that microelectroporation is a new powerful method for introducing antisense agents into single cells in complex cellular networks.
Chemical Physics | 1999
Daniel T. Chiu; Clyde F. Wilson; Anders Karlsson; Anna Danielsson; Anders Lundqvist; Anette Strömberg; Frida Ryttsén; Maximilian Davidson; Sture Nordholm; Owe Orwar; Richard N. Zare
A method to study single-molecule reactions confined in a biomimetic container is described. The technique combines rapid vesicle preparation, optical trapping and fluorescence confocal microscopy for performing simultaneous single-vesicle trapping and single-molecule detection experiments. The collisional environment between a single enzyme and substrate inside a vesicle is characterized by a Brownian dynamics Monte Carlo simulation. q 1999 Elsevier Science B.V. All rights reserved.
BiOS 2001 The International Symposium on Biomedical Optics | 2001
Daniel T. Chiu; Maximilian Davidson; Anette Stroemberg; Frida Ryttsén; Owe Orwar
This paper describes the use of focused electric fields and focused optical fields for the high-resolution manipulation of single cells. A focused electric field, obtained with the use of ultramicroelectrodes (tip diameter approximately 5 μm), is used to electroporate and electrofuse individual cells selectively and with high spatial resolution. A focused optical field, in the form of an optical tweezer, is used to isolate single organelles from a cell as well as to position liposomes incorporated with receptors and transporters along the cell for the high-resolution sampling and probing of the cellular microenvironment.
Science | 1999
Daniel T. Chiu; Clyde F. Wilson; Frida Ryttsén; Anette Strömberg; Cecilia Farre; Anders Karlsson; Sture Nordholm; Anuj Gaggar; Biren P. Modi; Alexander Moscho; Roberto A. Garza-López; Owe Orwar; Richard N. Zare
Analytical Chemistry | 2000
Mattias Karlsson; Kerstin Nolkrantz; Maximilian Davidson; Anette Strömberg; Frida Ryttsén; Björn Åkerman; Owe Orwar
Analytical Chemistry | 2001
Anette Strömberg; Anders Karlsson; Frida Ryttsén; Maximilian Davidson; Daniel T. Chiu; Owe Orwar
Archive | 2003
Frida Ryttsén; Owe Orwar; Mikael Levin; Eskil Sahlin; Joakim Wigström