[{"user_id":"48864","department":[{"_id":"302"}],"_id":"63436","language":[{"iso":"eng"}],"article_number":"acsanm.5c04857","type":"journal_article","publication":"ACS Applied Nano Materials","status":"public","author":[{"first_name":"Sivoney Ferreira","full_name":"de Souza, Sivoney Ferreira","last_name":"de Souza"},{"full_name":"Beresowski, Christina","last_name":"Beresowski","first_name":"Christina"},{"full_name":"Kosmella, Sabine","last_name":"Kosmella","first_name":"Sabine"},{"first_name":"João","full_name":"Ameixa, João","last_name":"Ameixa"},{"last_name":"Pothineni","full_name":"Pothineni, Bhanu Kiran","first_name":"Bhanu Kiran"},{"first_name":"Adrian Clemens","last_name":"Keller","orcid":"0000-0001-7139-3110","id":"48864","full_name":"Keller, Adrian Clemens"},{"full_name":"Hartlieb, Matthias","last_name":"Hartlieb","first_name":"Matthias"},{"full_name":"Taubert, Andreas","last_name":"Taubert","first_name":"Andreas"},{"first_name":"Ilko","last_name":"Bald","full_name":"Bald, Ilko"}],"date_created":"2026-01-05T08:23:24Z","publisher":"American Chemical Society (ACS)","date_updated":"2026-01-05T08:23:51Z","doi":"10.1021/acsanm.5c04857","title":"Nanocellulose Membranes for Plasmon-Enhanced Removal of Organic Pollutants from Water","publication_status":"published","publication_identifier":{"issn":["2574-0970","2574-0970"]},"citation":{"ama":"de Souza SF, Beresowski C, Kosmella S, et al. Nanocellulose Membranes for Plasmon-Enhanced Removal of Organic Pollutants from Water. ACS Applied Nano Materials. Published online 2026. doi:10.1021/acsanm.5c04857","ieee":"S. F. de Souza et al., “Nanocellulose Membranes for Plasmon-Enhanced Removal of Organic Pollutants from Water,” ACS Applied Nano Materials, Art. no. acsanm.5c04857, 2026, doi: 10.1021/acsanm.5c04857.","chicago":"Souza, Sivoney Ferreira de, Christina Beresowski, Sabine Kosmella, João Ameixa, Bhanu Kiran Pothineni, Adrian Clemens Keller, Matthias Hartlieb, Andreas Taubert, and Ilko Bald. “Nanocellulose Membranes for Plasmon-Enhanced Removal of Organic Pollutants from Water.” ACS Applied Nano Materials, 2026. https://doi.org/10.1021/acsanm.5c04857.","apa":"de Souza, S. F., Beresowski, C., Kosmella, S., Ameixa, J., Pothineni, B. K., Keller, A. C., Hartlieb, M., Taubert, A., & Bald, I. (2026). Nanocellulose Membranes for Plasmon-Enhanced Removal of Organic Pollutants from Water. ACS Applied Nano Materials, Article acsanm.5c04857. https://doi.org/10.1021/acsanm.5c04857","bibtex":"@article{de Souza_Beresowski_Kosmella_Ameixa_Pothineni_Keller_Hartlieb_Taubert_Bald_2026, title={Nanocellulose Membranes for Plasmon-Enhanced Removal of Organic Pollutants from Water}, DOI={10.1021/acsanm.5c04857}, number={acsanm.5c04857}, journal={ACS Applied Nano Materials}, publisher={American Chemical Society (ACS)}, author={de Souza, Sivoney Ferreira and Beresowski, Christina and Kosmella, Sabine and Ameixa, João and Pothineni, Bhanu Kiran and Keller, Adrian Clemens and Hartlieb, Matthias and Taubert, Andreas and Bald, Ilko}, year={2026} }","short":"S.F. de Souza, C. Beresowski, S. Kosmella, J. Ameixa, B.K. Pothineni, A.C. Keller, M. Hartlieb, A. Taubert, I. Bald, ACS Applied Nano Materials (2026).","mla":"de Souza, Sivoney Ferreira, et al. “Nanocellulose Membranes for Plasmon-Enhanced Removal of Organic Pollutants from Water.” ACS Applied Nano Materials, acsanm.5c04857, American Chemical Society (ACS), 2026, doi:10.1021/acsanm.5c04857."},"year":"2026"},{"publication":"Nanoscale","type":"journal_article","abstract":[{"text":"Surface-assisted DNA lattice assembly is used in the synthesis of functional surfaces and as a model of supramolecular network formation. Here, competitive DNA binding of different cation species is investigated...","lang":"eng"}],"status":"public","_id":"62726","department":[{"_id":"302"}],"user_id":"48864","language":[{"iso":"eng"}],"publication_identifier":{"issn":["2040-3364","2040-3372"]},"publication_status":"published","year":"2026","citation":{"ama":"Xu X, Pothineni BK, Grundmeier G, Tsushima S, Keller AC. On the role of cation-DNA interactions in surface-assisted DNA lattice assembly. Nanoscale. Published online 2026. doi:10.1039/d5nr03695j","ieee":"X. Xu, B. K. Pothineni, G. Grundmeier, S. Tsushima, and A. C. Keller, “On the role of cation-DNA interactions in surface-assisted DNA lattice assembly,” Nanoscale, 2026, doi: 10.1039/d5nr03695j.","chicago":"Xu, Xiaodan, Bhanu Kiran Pothineni, Guido Grundmeier, Satoru Tsushima, and Adrian Clemens Keller. “On the Role of Cation-DNA Interactions in Surface-Assisted DNA Lattice Assembly.” Nanoscale, 2026. https://doi.org/10.1039/d5nr03695j.","apa":"Xu, X., Pothineni, B. K., Grundmeier, G., Tsushima, S., & Keller, A. C. (2026). On the role of cation-DNA interactions in surface-assisted DNA lattice assembly. Nanoscale. https://doi.org/10.1039/d5nr03695j","bibtex":"@article{Xu_Pothineni_Grundmeier_Tsushima_Keller_2026, title={On the role of cation-DNA interactions in surface-assisted DNA lattice assembly}, DOI={10.1039/d5nr03695j}, journal={Nanoscale}, publisher={Royal Society of Chemistry (RSC)}, author={Xu, Xiaodan and Pothineni, Bhanu Kiran and Grundmeier, Guido and Tsushima, Satoru and Keller, Adrian Clemens}, year={2026} }","mla":"Xu, Xiaodan, et al. “On the Role of Cation-DNA Interactions in Surface-Assisted DNA Lattice Assembly.” Nanoscale, Royal Society of Chemistry (RSC), 2026, doi:10.1039/d5nr03695j.","short":"X. Xu, B.K. Pothineni, G. Grundmeier, S. Tsushima, A.C. Keller, Nanoscale (2026)."},"publisher":"Royal Society of Chemistry (RSC)","date_updated":"2026-01-06T10:42:32Z","author":[{"first_name":"Xiaodan","last_name":"Xu","full_name":"Xu, Xiaodan"},{"full_name":"Pothineni, Bhanu Kiran","last_name":"Pothineni","first_name":"Bhanu Kiran"},{"last_name":"Grundmeier","full_name":"Grundmeier, Guido","id":"194","first_name":"Guido"},{"full_name":"Tsushima, Satoru","last_name":"Tsushima","first_name":"Satoru"},{"id":"48864","full_name":"Keller, Adrian Clemens","orcid":"0000-0001-7139-3110","last_name":"Keller","first_name":"Adrian Clemens"}],"date_created":"2025-12-01T13:48:42Z","title":"On the role of cation-DNA interactions in surface-assisted DNA lattice assembly","doi":"10.1039/d5nr03695j"},{"abstract":[{"text":"Encoding information in molecular arrangements on DNA origami nanostructures (DONs) provides the basis for novel concepts in molecular data storage and computing. To preserve their integrity over long timescales, the information‐carrying DONs are often stored in a frozen state. Here, we investigate the effect of repeated freeze–thaw (F/T) cycles on the structural and functional integrity of DONs carrying biotin (Bt) modifications. Streptavidin (SAv) binding is used to visualize the stored information by atomic force microscopy (AFM) before and after 40 F/T cycles. Two strategies are compared by F/T cycling of (I) SAv‐bound DONs and (II) SAv‐free DONs that are exposed to SAv directly before AFM imaging. Our results reveal that while the DONs retain their overall shape, F/T cycling induces a small amount of damage, leading to slightly reduced SAv binding. Adding glycerol at mM concentrations efficiently protects the DONs and restores the original SAv binding yields. Nevertheless, SAv exposure after F/T cycling leads to slightly higher and more consistent SAv binding yields and a lower background of nonspecifically adsorbed SAv compared to Strategy I. This makes information readout by AFM more efficient and renders Strategy II more convenient for long‐term storage of information‐carrying DONs with repeated information readout.","lang":"eng"}],"status":"public","publication":"Chemistry–Methods","type":"journal_article","article_number":"e202500161","language":[{"iso":"eng"}],"_id":"65082","department":[{"_id":"302"}],"user_id":"48864","year":"2026","intvolume":" 6","citation":{"apa":"Li, X., Rabbe, L., Linneweber, J., Grundmeier, G., & Keller, A. C. (2026). Stability of Information‐Carrying DNA Origami Nanostructures During Repeated Freeze–Thaw Cycles. Chemistry–Methods, 6(3), Article e202500161. https://doi.org/10.1002/cmtd.202500161","bibtex":"@article{Li_Rabbe_Linneweber_Grundmeier_Keller_2026, title={Stability of Information‐Carrying DNA Origami Nanostructures During Repeated Freeze–Thaw Cycles}, volume={6}, DOI={10.1002/cmtd.202500161}, number={3e202500161}, journal={Chemistry–Methods}, publisher={Wiley}, author={Li, Xinyang and Rabbe, Lukas and Linneweber, Jacqueline and Grundmeier, Guido and Keller, Adrian Clemens}, year={2026} }","short":"X. Li, L. Rabbe, J. Linneweber, G. Grundmeier, A.C. Keller, Chemistry–Methods 6 (2026).","mla":"Li, Xinyang, et al. “Stability of Information‐Carrying DNA Origami Nanostructures During Repeated Freeze–Thaw Cycles.” Chemistry–Methods, vol. 6, no. 3, e202500161, Wiley, 2026, doi:10.1002/cmtd.202500161.","ama":"Li X, Rabbe L, Linneweber J, Grundmeier G, Keller AC. Stability of Information‐Carrying DNA Origami Nanostructures During Repeated Freeze–Thaw Cycles. Chemistry–Methods. 2026;6(3). doi:10.1002/cmtd.202500161","chicago":"Li, Xinyang, Lukas Rabbe, Jacqueline Linneweber, Guido Grundmeier, and Adrian Clemens Keller. “Stability of Information‐Carrying DNA Origami Nanostructures During Repeated Freeze–Thaw Cycles.” Chemistry–Methods 6, no. 3 (2026). https://doi.org/10.1002/cmtd.202500161.","ieee":"X. Li, L. Rabbe, J. Linneweber, G. Grundmeier, and A. C. Keller, “Stability of Information‐Carrying DNA Origami Nanostructures During Repeated Freeze–Thaw Cycles,” Chemistry–Methods, vol. 6, no. 3, Art. no. e202500161, 2026, doi: 10.1002/cmtd.202500161."},"publication_identifier":{"issn":["2628-9725","2628-9725"]},"publication_status":"published","issue":"3","title":"Stability of Information‐Carrying DNA Origami Nanostructures During Repeated Freeze–Thaw Cycles","doi":"10.1002/cmtd.202500161","publisher":"Wiley","date_updated":"2026-03-23T07:12:53Z","volume":6,"date_created":"2026-03-23T07:12:13Z","author":[{"first_name":"Xinyang","full_name":"Li, Xinyang","last_name":"Li"},{"last_name":"Rabbe","full_name":"Rabbe, Lukas","first_name":"Lukas"},{"first_name":"Jacqueline","full_name":"Linneweber, Jacqueline","last_name":"Linneweber"},{"full_name":"Grundmeier, Guido","id":"194","last_name":"Grundmeier","first_name":"Guido"},{"first_name":"Adrian Clemens","full_name":"Keller, Adrian Clemens","id":"48864","last_name":"Keller","orcid":"0000-0001-7139-3110"}]},{"type":"journal_article","publication":"Journal of Physics D: Applied Physics","abstract":[{"text":"Abstract\r\n Lithographic surface patterning is a cornerstone of modern materials and device fabrication. Although the available lithography techniques are constantly being advanced to push the feature sizes down to the few-nanometer scale, such developments are associated with many technological and economic challenges. Combining established top-down lithography with bottom-up self-assembly strategies has the potential to overcome those challenges and enable the manipulation of matter with molecular precision. One of the most exciting approaches in this regard is to harness the programmability of DNA self-assembly to create precise DNA nanostructure masks to be used in the lithographic patterning of diverse substrates. DNA nanotechnology has provided us with a versatile toolbox for the high-yield synthesis of 2D and 3D nanostructures with complex, user-defined shapes at unprecedented molecular accuracy. Consequently, the last decade has seen intense research efforts aimed at transferring such DNA nanostructure shapes into functional organic and inorganic materials and we have now arrived at a point where sophisticated molecular lithography approaches utilize DNA nanostructure masks for the fabrication of plasmonic surfaces for metamaterials and sensing applications. This review summarizes how the spatial information of such DNA nanostructure masks can be transferred into various organic and inorganic materials through selective etching and deposition steps. The review also discusses recent developments toward all-purpose molecular lithography schemes and highlights promising extensions of the discussed methods toward new materials systems and application fields.","lang":"eng"}],"status":"public","_id":"65108","user_id":"48864","department":[{"_id":"302"}],"language":[{"iso":"eng"}],"publication_status":"published","publication_identifier":{"issn":["0022-3727","1361-6463"]},"year":"2026","citation":{"ama":"Keller AC, Linko V. Molecular lithography with DNA nanostructures: Methods and applications. Journal of Physics D: Applied Physics. Published online 2026. doi:10.1088/1361-6463/ae5667","ieee":"A. C. Keller and V. Linko, “Molecular lithography with DNA nanostructures: Methods and applications,” Journal of Physics D: Applied Physics, 2026, doi: 10.1088/1361-6463/ae5667.","chicago":"Keller, Adrian Clemens, and Veikko Linko. “Molecular Lithography with DNA Nanostructures: Methods and Applications.” Journal of Physics D: Applied Physics, 2026. https://doi.org/10.1088/1361-6463/ae5667.","mla":"Keller, Adrian Clemens, and Veikko Linko. “Molecular Lithography with DNA Nanostructures: Methods and Applications.” Journal of Physics D: Applied Physics, IOP Publishing, 2026, doi:10.1088/1361-6463/ae5667.","bibtex":"@article{Keller_Linko_2026, title={Molecular lithography with DNA nanostructures: Methods and applications}, DOI={10.1088/1361-6463/ae5667}, journal={Journal of Physics D: Applied Physics}, publisher={IOP Publishing}, author={Keller, Adrian Clemens and Linko, Veikko}, year={2026} }","short":"A.C. Keller, V. Linko, Journal of Physics D: Applied Physics (2026).","apa":"Keller, A. C., & Linko, V. (2026). Molecular lithography with DNA nanostructures: Methods and applications. Journal of Physics D: Applied Physics. https://doi.org/10.1088/1361-6463/ae5667"},"date_updated":"2026-03-25T07:44:52Z","publisher":"IOP Publishing","author":[{"last_name":"Keller","orcid":"0000-0001-7139-3110","id":"48864","full_name":"Keller, Adrian Clemens","first_name":"Adrian Clemens"},{"last_name":"Linko","full_name":"Linko, Veikko","first_name":"Veikko"}],"date_created":"2026-03-25T07:43:24Z","title":"Molecular lithography with DNA nanostructures: Methods and applications","doi":"10.1088/1361-6463/ae5667"},{"author":[{"full_name":"Parikka, Johannes","last_name":"Parikka","first_name":"Johannes"},{"full_name":"Pothineni, Bhanu Kiran","last_name":"Pothineni","first_name":"Bhanu Kiran"},{"full_name":"Järvinen, Heini","last_name":"Järvinen","first_name":"Heini"},{"first_name":"Kosti","last_name":"Tapio","full_name":"Tapio, Kosti"},{"first_name":"Adrian","id":"48864","full_name":"Keller, Adrian","last_name":"Keller","orcid":"0000-0001-7139-3110"},{"last_name":"Toppari","full_name":"Toppari, J. Jussi","first_name":"J. Jussi"}],"date_created":"2025-04-08T09:06:14Z","date_updated":"2025-04-08T09:06:34Z","publisher":"Springer US","doi":"10.1007/978-1-0716-4394-5_7","title":"Surface-Assisted Assembly of DNA Origami Lattices on Silicon Wafers","publication_identifier":{"isbn":["9781071643938","9781071643945"],"issn":["1064-3745","1940-6029"]},"publication_status":"published","citation":{"ama":"Parikka J, Pothineni BK, Järvinen H, Tapio K, Keller A, Toppari JJ. Surface-Assisted Assembly of DNA Origami Lattices on Silicon Wafers. In: Methods in Molecular Biology. Springer US; 2025. doi:10.1007/978-1-0716-4394-5_7","ieee":"J. Parikka, B. K. Pothineni, H. Järvinen, K. Tapio, A. Keller, and J. J. Toppari, “Surface-Assisted Assembly of DNA Origami Lattices on Silicon Wafers,” in Methods in Molecular Biology, New York, NY: Springer US, 2025.","chicago":"Parikka, Johannes, Bhanu Kiran Pothineni, Heini Järvinen, Kosti Tapio, Adrian Keller, and J. Jussi Toppari. “Surface-Assisted Assembly of DNA Origami Lattices on Silicon Wafers.” In Methods in Molecular Biology. New York, NY: Springer US, 2025. https://doi.org/10.1007/978-1-0716-4394-5_7.","apa":"Parikka, J., Pothineni, B. K., Järvinen, H., Tapio, K., Keller, A., & Toppari, J. J. (2025). Surface-Assisted Assembly of DNA Origami Lattices on Silicon Wafers. In Methods in Molecular Biology. Springer US. https://doi.org/10.1007/978-1-0716-4394-5_7","short":"J. Parikka, B.K. Pothineni, H. Järvinen, K. Tapio, A. Keller, J.J. Toppari, in: Methods in Molecular Biology, Springer US, New York, NY, 2025.","mla":"Parikka, Johannes, et al. “Surface-Assisted Assembly of DNA Origami Lattices on Silicon Wafers.” Methods in Molecular Biology, Springer US, 2025, doi:10.1007/978-1-0716-4394-5_7.","bibtex":"@inbook{Parikka_Pothineni_Järvinen_Tapio_Keller_Toppari_2025, place={New York, NY}, title={Surface-Assisted Assembly of DNA Origami Lattices on Silicon Wafers}, DOI={10.1007/978-1-0716-4394-5_7}, booktitle={Methods in Molecular Biology}, publisher={Springer US}, author={Parikka, Johannes and Pothineni, Bhanu Kiran and Järvinen, Heini and Tapio, Kosti and Keller, Adrian and Toppari, J. Jussi}, year={2025} }"},"year":"2025","place":"New York, NY","department":[{"_id":"302"}],"user_id":"48864","_id":"59421","language":[{"iso":"eng"}],"publication":"Methods in Molecular Biology","type":"book_chapter","status":"public"},{"_id":"59847","user_id":"48864","department":[{"_id":"302"}],"article_number":"77","language":[{"iso":"eng"}],"type":"journal_article","publication":"Discover Nano","abstract":[{"lang":"eng","text":"Abstract\r\n The surface-assisted assembly of DNA origami lattices is a potent method for creating molecular lithography masks. Lattice quality and assembly kinetics are controlled by various environmental parameters, including the employed surface, the assembly temperature, and the ionic composition of the buffer, with optimized parameter combinations resulting in highly ordered lattices that can span surface areas of several cm2. Established assembly protocols, however, employ assembly times ranging from hours to days. Here, the assembly of highly ordered hexagonal DNA origami lattices at mica surfaces is observed within few minutes using high-speed atomic force microscopy (HS-AFM). A moderate increase in the DNA origami concentration enables this rapid assembly. While forming a regular lattice takes 10 min at a DNA origami concentration of 4 nM, this time is shortened to about 2 min at a concentration of 6 nM. Increasing the DNA origami concentration any further does not result in shorter assembly times, presumably because DNA origami arrival at the mica surface is diffusion-limited. Over short length scales up to 1 µm, lattice order is independent of the DNA origami concentration. However, at larger length scales of a few microns, a DNA origami concentration of 10 nM yields slightly better order than lower and higher concentrations. Therefore, 10 nM can be considered the optimum concentration for the rapid assembly of highly ordered DNA origami lattices. These results thus represent an important step toward the industrial-scale application of DNA origami-based lithography masks."}],"status":"public","publisher":"Springer Science and Business Media LLC","date_updated":"2025-05-08T07:17:54Z","date_created":"2025-05-08T07:17:29Z","author":[{"full_name":"Pothineni, Bhanu Kiran","last_name":"Pothineni","first_name":"Bhanu Kiran"},{"first_name":"Jörg","last_name":"Barner","full_name":"Barner, Jörg"},{"first_name":"Guido","full_name":"Grundmeier, Guido","id":"194","last_name":"Grundmeier"},{"first_name":"David","last_name":"Contreras","full_name":"Contreras, David"},{"full_name":"Castro, Mario","last_name":"Castro","first_name":"Mario"},{"first_name":"Adrian","last_name":"Keller","orcid":"0000-0001-7139-3110","full_name":"Keller, Adrian","id":"48864"}],"volume":20,"title":"Rapid assembly of highly ordered DNA origami lattices at mica surfaces","doi":"10.1186/s11671-025-04254-2","publication_status":"published","publication_identifier":{"issn":["2731-9229"]},"issue":"1","year":"2025","citation":{"mla":"Pothineni, Bhanu Kiran, et al. “Rapid Assembly of Highly Ordered DNA Origami Lattices at Mica Surfaces.” Discover Nano, vol. 20, no. 1, 77, Springer Science and Business Media LLC, 2025, doi:10.1186/s11671-025-04254-2.","bibtex":"@article{Pothineni_Barner_Grundmeier_Contreras_Castro_Keller_2025, title={Rapid assembly of highly ordered DNA origami lattices at mica surfaces}, volume={20}, DOI={10.1186/s11671-025-04254-2}, number={177}, journal={Discover Nano}, publisher={Springer Science and Business Media LLC}, author={Pothineni, Bhanu Kiran and Barner, Jörg and Grundmeier, Guido and Contreras, David and Castro, Mario and Keller, Adrian}, year={2025} }","short":"B.K. Pothineni, J. Barner, G. Grundmeier, D. Contreras, M. Castro, A. Keller, Discover Nano 20 (2025).","apa":"Pothineni, B. K., Barner, J., Grundmeier, G., Contreras, D., Castro, M., & Keller, A. (2025). Rapid assembly of highly ordered DNA origami lattices at mica surfaces. Discover Nano, 20(1), Article 77. https://doi.org/10.1186/s11671-025-04254-2","ama":"Pothineni BK, Barner J, Grundmeier G, Contreras D, Castro M, Keller A. Rapid assembly of highly ordered DNA origami lattices at mica surfaces. Discover Nano. 2025;20(1). doi:10.1186/s11671-025-04254-2","ieee":"B. K. Pothineni, J. Barner, G. Grundmeier, D. Contreras, M. Castro, and A. Keller, “Rapid assembly of highly ordered DNA origami lattices at mica surfaces,” Discover Nano, vol. 20, no. 1, Art. no. 77, 2025, doi: 10.1186/s11671-025-04254-2.","chicago":"Pothineni, Bhanu Kiran, Jörg Barner, Guido Grundmeier, David Contreras, Mario Castro, and Adrian Keller. “Rapid Assembly of Highly Ordered DNA Origami Lattices at Mica Surfaces.” Discover Nano 20, no. 1 (2025). https://doi.org/10.1186/s11671-025-04254-2."},"intvolume":" 20"},{"department":[{"_id":"302"}],"user_id":"48864","_id":"59992","language":[{"iso":"eng"}],"publication":"RSC Applied Interfaces","type":"journal_article","status":"public","abstract":[{"text":"The immobilization of DNA origami nanostructures on solid surfaces is an important prerequisite for their application in many biosensors. So far, DNA origami immobilization has been investigated in detail only...","lang":"eng"}],"date_created":"2025-05-19T09:30:44Z","author":[{"full_name":"Xu, Xiaodan","last_name":"Xu","first_name":"Xiaodan"},{"id":"69524","full_name":"Golebiowska, Sandra Alicja","last_name":"Golebiowska","first_name":"Sandra Alicja"},{"last_name":"de los Arcos","full_name":"de los Arcos, Teresa","first_name":"Teresa"},{"first_name":"Guido","full_name":"Grundmeier, Guido","id":"194","last_name":"Grundmeier"},{"first_name":"Adrian","full_name":"Keller, Adrian","id":"48864","orcid":"0000-0001-7139-3110","last_name":"Keller"}],"publisher":"Royal Society of Chemistry (RSC)","date_updated":"2025-05-19T09:32:05Z","doi":"10.1039/d5lf00109a","title":"DNA origami adsorption at single-crystalline TiO2 surfaces","publication_identifier":{"issn":["2755-3701"]},"publication_status":"published","citation":{"ama":"Xu X, Golebiowska SA, de los Arcos T, Grundmeier G, Keller A. DNA origami adsorption at single-crystalline TiO2 surfaces. RSC Applied Interfaces. Published online 2025. doi:10.1039/d5lf00109a","ieee":"X. Xu, S. A. Golebiowska, T. de los Arcos, G. Grundmeier, and A. Keller, “DNA origami adsorption at single-crystalline TiO2 surfaces,” RSC Applied Interfaces, 2025, doi: 10.1039/d5lf00109a.","chicago":"Xu, Xiaodan, Sandra Alicja Golebiowska, Teresa de los Arcos, Guido Grundmeier, and Adrian Keller. “DNA Origami Adsorption at Single-Crystalline TiO2 Surfaces.” RSC Applied Interfaces, 2025. https://doi.org/10.1039/d5lf00109a.","bibtex":"@article{Xu_Golebiowska_de los Arcos_Grundmeier_Keller_2025, title={DNA origami adsorption at single-crystalline TiO2 surfaces}, DOI={10.1039/d5lf00109a}, journal={RSC Applied Interfaces}, publisher={Royal Society of Chemistry (RSC)}, author={Xu, Xiaodan and Golebiowska, Sandra Alicja and de los Arcos, Teresa and Grundmeier, Guido and Keller, Adrian}, year={2025} }","mla":"Xu, Xiaodan, et al. “DNA Origami Adsorption at Single-Crystalline TiO2 Surfaces.” RSC Applied Interfaces, Royal Society of Chemistry (RSC), 2025, doi:10.1039/d5lf00109a.","short":"X. Xu, S.A. Golebiowska, T. de los Arcos, G. Grundmeier, A. Keller, RSC Applied Interfaces (2025).","apa":"Xu, X., Golebiowska, S. A., de los Arcos, T., Grundmeier, G., & Keller, A. (2025). DNA origami adsorption at single-crystalline TiO2 surfaces. RSC Applied Interfaces. https://doi.org/10.1039/d5lf00109a"},"year":"2025"},{"author":[{"first_name":"Bhanu Kiran","full_name":"Pothineni, Bhanu Kiran","last_name":"Pothineni"},{"last_name":"Theile-Rasche","full_name":"Theile-Rasche, Chantal","first_name":"Chantal"},{"first_name":"Hendrik","full_name":"Müller, Hendrik","last_name":"Müller"},{"first_name":"Guido","last_name":"Grundmeier","full_name":"Grundmeier, Guido","id":"194"},{"full_name":"de los Arcos de Pedro, Maria Teresa","id":"54556","orcid":"0000-0002-8684-273X ","last_name":"de los Arcos de Pedro","first_name":"Maria Teresa"},{"full_name":"Keller, Adrian","id":"48864","last_name":"Keller","orcid":"0000-0001-7139-3110","first_name":"Adrian"}],"date_created":"2025-02-12T14:49:48Z","date_updated":"2025-06-10T09:10:16Z","doi":"10.1002/chem.202404108","title":"DNA Origami Adsorption and Lattice Formation on Different SiOx Surfaces","citation":{"apa":"Pothineni, B. K., Theile-Rasche, C., Müller, H., Grundmeier, G., de los Arcos de Pedro, M. T., & Keller, A. (2025). DNA Origami Adsorption and Lattice Formation on Different SiOx Surfaces. Chemistry – A European Journal, e202404108. https://doi.org/10.1002/chem.202404108","short":"B.K. Pothineni, C. Theile-Rasche, H. Müller, G. Grundmeier, M.T. de los Arcos de Pedro, A. Keller, Chemistry – A European Journal (2025) e202404108.","bibtex":"@article{Pothineni_Theile-Rasche_Müller_Grundmeier_de los Arcos de Pedro_Keller_2025, title={DNA Origami Adsorption and Lattice Formation on Different SiOx Surfaces}, DOI={10.1002/chem.202404108}, journal={Chemistry – A European Journal}, author={Pothineni, Bhanu Kiran and Theile-Rasche, Chantal and Müller, Hendrik and Grundmeier, Guido and de los Arcos de Pedro, Maria Teresa and Keller, Adrian}, year={2025}, pages={e202404108} }","mla":"Pothineni, Bhanu Kiran, et al. “DNA Origami Adsorption and Lattice Formation on Different SiOx Surfaces.” Chemistry – A European Journal, 2025, p. e202404108, doi:10.1002/chem.202404108.","ieee":"B. K. Pothineni, C. Theile-Rasche, H. Müller, G. Grundmeier, M. T. de los Arcos de Pedro, and A. Keller, “DNA Origami Adsorption and Lattice Formation on Different SiOx Surfaces,” Chemistry – A European Journal, p. e202404108, 2025, doi: 10.1002/chem.202404108.","chicago":"Pothineni, Bhanu Kiran, Chantal Theile-Rasche, Hendrik Müller, Guido Grundmeier, Maria Teresa de los Arcos de Pedro, and Adrian Keller. “DNA Origami Adsorption and Lattice Formation on Different SiOx Surfaces.” Chemistry – A European Journal, 2025, e202404108. https://doi.org/10.1002/chem.202404108.","ama":"Pothineni BK, Theile-Rasche C, Müller H, Grundmeier G, de los Arcos de Pedro MT, Keller A. DNA Origami Adsorption and Lattice Formation on Different SiOx Surfaces. Chemistry – A European Journal. Published online 2025:e202404108. doi:10.1002/chem.202404108"},"page":"e202404108","year":"2025","user_id":"48864","department":[{"_id":"302"}],"_id":"58613","language":[{"iso":"eng"}],"type":"journal_article","publication":"Chemistry – A European Journal","status":"public","abstract":[{"text":"Self-assembled DNA origami lattices on silicon oxide surfaces have great potential to serve as masks in molecular lithography. However, silicon oxide surfaces come in many different forms and the type and history of the silicon oxide has a large effect on its physicochemical surface properties. Therefore, we here investigate DNA origami lattice formation on differently fabricated SiOx films on silicon wafers after wet-chemical oxidation by RCA1. Despite having similar oxide compositions and hydroxylation states, of all surfaces tested, only thermally grown SiOx performs similarly well as native oxide. For the other SiOx films deposited by plasma-enhanced chemical vapor deposition and magnetron sputtering, DNA origami adsorption is strongly suppressed. This is attributed to an increased surface roughness and a lower oxide density, respectively. Our results demonstrate that the employed SiOx surface may decide over the outcome of an experiment and should be considered as an additional parameter that may require optimization and fine-tuning before high-quality lattices can be assembled. In particular, our observations suggest that efficient DNA origami lattice assembly on SiOx surfaces requires a low surface roughness and a high oxide density.","lang":"eng"}]},{"year":"2025","intvolume":" 2","page":"61–75","citation":{"apa":"Keller, A. (2025). DNA origami nanostructures in biomedicine and the issue of stability. Nucleic Acid Insights, 2(2), 61–75. https://doi.org/10.18609/nuc.2025.011","bibtex":"@article{Keller_2025, title={DNA origami nanostructures in biomedicine and the issue of stability}, volume={2}, DOI={10.18609/nuc.2025.011}, number={2}, journal={Nucleic Acid Insights}, author={Keller, Adrian}, year={2025}, pages={61–75} }","short":"A. Keller, Nucleic Acid Insights 2 (2025) 61–75.","mla":"Keller, Adrian. “DNA Origami Nanostructures in Biomedicine and the Issue of Stability.” Nucleic Acid Insights, vol. 2, no. 2, 2025, pp. 61–75, doi:10.18609/nuc.2025.011.","ieee":"A. Keller, “DNA origami nanostructures in biomedicine and the issue of stability,” Nucleic Acid Insights, vol. 2, no. 2, pp. 61–75, 2025, doi: 10.18609/nuc.2025.011.","chicago":"Keller, Adrian. “DNA Origami Nanostructures in Biomedicine and the Issue of Stability.” Nucleic Acid Insights 2, no. 2 (2025): 61–75. https://doi.org/10.18609/nuc.2025.011.","ama":"Keller A. DNA origami nanostructures in biomedicine and the issue of stability. Nucleic Acid Insights. 2025;2(2):61–75. doi:10.18609/nuc.2025.011"},"has_accepted_license":"1","issue":"2","title":"DNA origami nanostructures in biomedicine and the issue of stability","doi":"10.18609/nuc.2025.011","oa":"1","date_updated":"2025-06-10T09:09:28Z","volume":2,"date_created":"2025-06-01T08:53:58Z","author":[{"last_name":"Keller","orcid":"0000-0001-7139-3110","id":"48864","full_name":"Keller, Adrian","first_name":"Adrian"}],"status":"public","file":[{"relation":"main_file","content_type":"application/pdf","file_size":701125,"file_id":"60083","access_level":"open_access","file_name":"Keller_nai25.pdf","date_updated":"2025-06-01T08:53:35Z","creator":"adke","date_created":"2025-06-01T08:53:35Z"}],"publication":"Nucleic Acid Insights","type":"journal_article","ddc":["570"],"language":[{"iso":"eng"}],"file_date_updated":"2025-06-01T08:53:35Z","_id":"60082","department":[{"_id":"302"}],"user_id":"48864"},{"abstract":[{"text":"Abstract\r\n While being a promising approach for the treatment of infections caused by drug-resistant, pathogenic bacteria, the clinical implementation of phage therapy still faces several challenges. One of these challenges lies in the high strain-specificity of most bacteriophages, which makes it necessary to screen large phage collections against the target pathogens in order to identify suitable candidates for the formulations of personalized therapeutic phage cocktails. In this work, we evaluate the potential of quartz crystal microbalance with dissipation monitoring (QCM-D) to identify and detect phage infection and subsequent lysis of bacteria immobilized on the surfaces of the QCM-D sensors. Using lytic Escherichia coli phage T7 as a model, we show that phage infection of E. coli cells results in various unique alterations in the behaviors of the frequency (Δf) and dissipation (ΔD) signals, which are not observed during exposure of the E. coli strain to non-infectious Bacillus subtilis phage phi29 at similar concentration. To aid future phage screening campaigns, we furthermore identify a single measurement parameter, i.e., the spread between the different overtones of ΔD, that can be used to detect phage-induced lysis. For T7 infection of E. coli, this is achieved within 4 h after inoculation, including immobilization and growth of the bacteria on the sensor surface, as well as the completed phage propagation cycle. Given the commercial availability of highly automated multichannel systems and the fact that this approach does not require any sensor modifications, QCM-D has the potential to become a valuable tool for screening medium-sized phage collections against target pathogens.\r\n \r\n Graphical Abstract\r\n ","lang":"eng"}],"status":"public","publication":"Analytical and Bioanalytical Chemistry","type":"journal_article","language":[{"iso":"eng"}],"_id":"58853","department":[{"_id":"302"}],"user_id":"48864","year":"2025","citation":{"ama":"Pothineni BK, Probst R, Kiefer D, et al. Monitoring phage infection and lysis of surface-immobilized bacteria by QCM-D. Analytical and Bioanalytical Chemistry. Published online 2025. doi:10.1007/s00216-025-05803-5","ieee":"B. K. Pothineni et al., “Monitoring phage infection and lysis of surface-immobilized bacteria by QCM-D,” Analytical and Bioanalytical Chemistry, 2025, doi: 10.1007/s00216-025-05803-5.","chicago":"Pothineni, Bhanu K., René Probst, Dorothee Kiefer, Verena Dobretzberger, Ivan Barišić, Guido Grundmeier, and Adrian Keller. “Monitoring Phage Infection and Lysis of Surface-Immobilized Bacteria by QCM-D.” Analytical and Bioanalytical Chemistry, 2025. https://doi.org/10.1007/s00216-025-05803-5.","apa":"Pothineni, B. K., Probst, R., Kiefer, D., Dobretzberger, V., Barišić, I., Grundmeier, G., & Keller, A. (2025). Monitoring phage infection and lysis of surface-immobilized bacteria by QCM-D. Analytical and Bioanalytical Chemistry. https://doi.org/10.1007/s00216-025-05803-5","mla":"Pothineni, Bhanu K., et al. “Monitoring Phage Infection and Lysis of Surface-Immobilized Bacteria by QCM-D.” Analytical and Bioanalytical Chemistry, Springer Science and Business Media LLC, 2025, doi:10.1007/s00216-025-05803-5.","bibtex":"@article{Pothineni_Probst_Kiefer_Dobretzberger_Barišić_Grundmeier_Keller_2025, title={Monitoring phage infection and lysis of surface-immobilized bacteria by QCM-D}, DOI={10.1007/s00216-025-05803-5}, journal={Analytical and Bioanalytical Chemistry}, publisher={Springer Science and Business Media LLC}, author={Pothineni, Bhanu K. and Probst, René and Kiefer, Dorothee and Dobretzberger, Verena and Barišić, Ivan and Grundmeier, Guido and Keller, Adrian}, year={2025} }","short":"B.K. Pothineni, R. Probst, D. Kiefer, V. Dobretzberger, I. Barišić, G. Grundmeier, A. Keller, Analytical and Bioanalytical Chemistry (2025)."},"publication_identifier":{"issn":["1618-2642","1618-2650"]},"publication_status":"published","title":"Monitoring phage infection and lysis of surface-immobilized bacteria by QCM-D","doi":"10.1007/s00216-025-05803-5","date_updated":"2025-02-26T09:23:43Z","publisher":"Springer Science and Business Media LLC","date_created":"2025-02-26T09:23:19Z","author":[{"last_name":"Pothineni","full_name":"Pothineni, Bhanu K.","first_name":"Bhanu K."},{"full_name":"Probst, René","last_name":"Probst","first_name":"René"},{"last_name":"Kiefer","full_name":"Kiefer, Dorothee","first_name":"Dorothee"},{"full_name":"Dobretzberger, Verena","last_name":"Dobretzberger","first_name":"Verena"},{"full_name":"Barišić, Ivan","last_name":"Barišić","first_name":"Ivan"},{"last_name":"Grundmeier","id":"194","full_name":"Grundmeier, Guido","first_name":"Guido"},{"first_name":"Adrian","full_name":"Keller, Adrian","id":"48864","orcid":"0000-0001-7139-3110","last_name":"Keller"}]},{"publication":"Nanoscale","type":"journal_article","status":"public","abstract":[{"lang":"eng","text":"DNA origami nanostructures are powerful molecular tools for the controlled arrangement of functional molecules and thus have important applications in biomedicine, sensing, and materials science. The fabrication of DNA origami..."}],"department":[{"_id":"302"}],"user_id":"48864","_id":"60507","language":[{"iso":"eng"}],"publication_identifier":{"issn":["2040-3364","2040-3372"]},"publication_status":"published","citation":{"ama":"Tomm E, Grundmeier G, Keller A. Cost-efficient folding of functionalized DNA origami nanostructures via staple recycling. Nanoscale. Published online 2025. doi:10.1039/d5nr01435b","chicago":"Tomm, Emilia, Guido Grundmeier, and Adrian Keller. “Cost-Efficient Folding of Functionalized DNA Origami Nanostructures via Staple Recycling.” Nanoscale, 2025. https://doi.org/10.1039/d5nr01435b.","ieee":"E. Tomm, G. Grundmeier, and A. Keller, “Cost-efficient folding of functionalized DNA origami nanostructures via staple recycling,” Nanoscale, 2025, doi: 10.1039/d5nr01435b.","mla":"Tomm, Emilia, et al. “Cost-Efficient Folding of Functionalized DNA Origami Nanostructures via Staple Recycling.” Nanoscale, Royal Society of Chemistry (RSC), 2025, doi:10.1039/d5nr01435b.","short":"E. Tomm, G. Grundmeier, A. Keller, Nanoscale (2025).","bibtex":"@article{Tomm_Grundmeier_Keller_2025, title={Cost-efficient folding of functionalized DNA origami nanostructures via staple recycling}, DOI={10.1039/d5nr01435b}, journal={Nanoscale}, publisher={Royal Society of Chemistry (RSC)}, author={Tomm, Emilia and Grundmeier, Guido and Keller, Adrian}, year={2025} }","apa":"Tomm, E., Grundmeier, G., & Keller, A. (2025). Cost-efficient folding of functionalized DNA origami nanostructures via staple recycling. Nanoscale. https://doi.org/10.1039/d5nr01435b"},"year":"2025","date_created":"2025-07-03T11:26:30Z","author":[{"last_name":"Tomm","full_name":"Tomm, Emilia","id":"68157","first_name":"Emilia"},{"first_name":"Guido","last_name":"Grundmeier","full_name":"Grundmeier, Guido","id":"194"},{"orcid":"0000-0001-7139-3110","last_name":"Keller","full_name":"Keller, Adrian","id":"48864","first_name":"Adrian"}],"publisher":"Royal Society of Chemistry (RSC)","date_updated":"2025-07-03T11:27:19Z","doi":"10.1039/d5nr01435b","title":"Cost-efficient folding of functionalized DNA origami nanostructures via staple recycling"},{"type":"journal_article","status":"public","_id":"60606","department":[{"_id":"302"}],"user_id":"48864","publication_identifier":{"issn":["2046-2069"]},"publication_status":"published","intvolume":" 15","page":"24536-24543","citation":{"apa":"Rabbe, L., Tomm, E., Grundmeier, G., & Keller, A. (2025). Toward high-density streptavidin arrays on DNA origami nanostructures. RSC Advances, 15(30), 24536–24543. https://doi.org/10.1039/d5ra03393d","short":"L. Rabbe, E. Tomm, G. Grundmeier, A. Keller, RSC Advances 15 (2025) 24536–24543.","bibtex":"@article{Rabbe_Tomm_Grundmeier_Keller_2025, title={Toward high-density streptavidin arrays on DNA origami nanostructures}, volume={15}, DOI={10.1039/d5ra03393d}, number={30}, journal={RSC Advances}, publisher={Royal Society of Chemistry (RSC)}, author={Rabbe, Lukas and Tomm, Emilia and Grundmeier, Guido and Keller, Adrian}, year={2025}, pages={24536–24543} }","mla":"Rabbe, Lukas, et al. “Toward High-Density Streptavidin Arrays on DNA Origami Nanostructures.” RSC Advances, vol. 15, no. 30, Royal Society of Chemistry (RSC), 2025, pp. 24536–43, doi:10.1039/d5ra03393d.","ama":"Rabbe L, Tomm E, Grundmeier G, Keller A. Toward high-density streptavidin arrays on DNA origami nanostructures. RSC Advances. 2025;15(30):24536-24543. doi:10.1039/d5ra03393d","chicago":"Rabbe, Lukas, Emilia Tomm, Guido Grundmeier, and Adrian Keller. “Toward High-Density Streptavidin Arrays on DNA Origami Nanostructures.” RSC Advances 15, no. 30 (2025): 24536–43. https://doi.org/10.1039/d5ra03393d.","ieee":"L. Rabbe, E. Tomm, G. Grundmeier, and A. Keller, “Toward high-density streptavidin arrays on DNA origami nanostructures,” RSC Advances, vol. 15, no. 30, pp. 24536–24543, 2025, doi: 10.1039/d5ra03393d."},"date_updated":"2025-07-15T06:07:16Z","volume":15,"author":[{"first_name":"Lukas","full_name":"Rabbe, Lukas","last_name":"Rabbe"},{"first_name":"Emilia","id":"68157","full_name":"Tomm, Emilia","last_name":"Tomm"},{"first_name":"Guido","last_name":"Grundmeier","full_name":"Grundmeier, Guido","id":"194"},{"first_name":"Adrian","id":"48864","full_name":"Keller, Adrian","last_name":"Keller","orcid":"0000-0001-7139-3110"}],"doi":"10.1039/d5ra03393d","publication":"RSC Advances","abstract":[{"lang":"eng","text":"Streptavidin binding to DNA origami-supported high-density biotin arrays is investigated for selected experimental parameters. While bidentate binding and steric hindrance can be minimized, molecular crowding limits the binding yields in 2D arrays."}],"language":[{"iso":"eng"}],"issue":"30","year":"2025","publisher":"Royal Society of Chemistry (RSC)","date_created":"2025-07-15T06:06:48Z","title":"Toward high-density streptavidin arrays on DNA origami nanostructures"},{"date_updated":"2025-07-22T07:18:04Z","publisher":"Royal Society of Chemistry (RSC)","date_created":"2025-07-22T07:17:24Z","author":[{"last_name":"Omoboye","full_name":"Omoboye, Adekunle","first_name":"Adekunle"},{"last_name":"Pothineni","full_name":"Pothineni, Bhanu","first_name":"Bhanu"},{"first_name":"Guido","id":"194","full_name":"Grundmeier, Guido","last_name":"Grundmeier"},{"first_name":"Zhe","last_name":"She","full_name":"She, Zhe"},{"id":"48864","full_name":"Keller, Adrian","orcid":"0000-0001-7139-3110","last_name":"Keller","first_name":"Adrian"}],"title":"Surface potential-dependent assembly of DNA origami lattices at SiO2 surfaces","doi":"10.1039/d5lf00169b","publication_identifier":{"issn":["2755-3701"]},"publication_status":"published","year":"2025","citation":{"ama":"Omoboye A, Pothineni B, Grundmeier G, She Z, Keller A. Surface potential-dependent assembly of DNA origami lattices at SiO2 surfaces. RSC Applied Interfaces. Published online 2025. doi:10.1039/d5lf00169b","chicago":"Omoboye, Adekunle, Bhanu Pothineni, Guido Grundmeier, Zhe She, and Adrian Keller. “Surface Potential-Dependent Assembly of DNA Origami Lattices at SiO2 Surfaces.” RSC Applied Interfaces, 2025. https://doi.org/10.1039/d5lf00169b.","ieee":"A. Omoboye, B. Pothineni, G. Grundmeier, Z. She, and A. Keller, “Surface potential-dependent assembly of DNA origami lattices at SiO2 surfaces,” RSC Applied Interfaces, 2025, doi: 10.1039/d5lf00169b.","bibtex":"@article{Omoboye_Pothineni_Grundmeier_She_Keller_2025, title={Surface potential-dependent assembly of DNA origami lattices at SiO2 surfaces}, DOI={10.1039/d5lf00169b}, journal={RSC Applied Interfaces}, publisher={Royal Society of Chemistry (RSC)}, author={Omoboye, Adekunle and Pothineni, Bhanu and Grundmeier, Guido and She, Zhe and Keller, Adrian}, year={2025} }","short":"A. Omoboye, B. Pothineni, G. Grundmeier, Z. She, A. Keller, RSC Applied Interfaces (2025).","mla":"Omoboye, Adekunle, et al. “Surface Potential-Dependent Assembly of DNA Origami Lattices at SiO2 Surfaces.” RSC Applied Interfaces, Royal Society of Chemistry (RSC), 2025, doi:10.1039/d5lf00169b.","apa":"Omoboye, A., Pothineni, B., Grundmeier, G., She, Z., & Keller, A. (2025). Surface potential-dependent assembly of DNA origami lattices at SiO2 surfaces. RSC Applied Interfaces. https://doi.org/10.1039/d5lf00169b"},"_id":"60709","department":[{"_id":"302"}],"user_id":"48864","language":[{"iso":"eng"}],"publication":"RSC Applied Interfaces","type":"journal_article","abstract":[{"lang":"eng","text":"Self-assembled DNA origami lattices have promising applications in the fabrication of functional surfaces for sensing and plasmonics via molecular lithography. While surface-assisted DNA origami lattice assembly at mica surfaces is..."}],"status":"public"},{"publication":"Small Structures","type":"journal_article","status":"public","abstract":[{"text":"The specific binding of DNA origami nanostructures (DONs) to bacteria is an important prerequisite for their application in pathogen targeting and antimicrobial drug delivery. So far, targeting bacteria with DONs has been achieved exclusively via aptamers, which suffer from drawbacks such as sensitivity toward environmental conditions and reduced binding after immobilization or conjugation. Here, an alternative approach is presented based on the modification of DONs with the cell wall‐binding glycopeptide antibiotic vancomycin. Using strain‐promoted azide‐alkyne cycloaddition, azide‐modified vancomycin is conjugated to selected staple strands and subsequently incorporated into 2D DON triangles. The resulting constructs show specific binding to the Gram‐positive species Bacillus subtilis (B. subtilis) and Staphylococcus capitis (S. capitis), and remarkably, to Gram‐negative Escherichia coli (E. coli), but no antimicrobial activity at vancomycin concentrations up to at least 2.91 μM. For B. subtilis and E. coli, DONs with vancomycin modifications on both sides exhibit better binding than DONs modified on only one side. However, both variants bind equally well to S. capitis. These results demonstrate the great potential of small molecule drug compounds for the robust, broad‐spectrum targeting of bacteria with DONs. Targeting a ubiquitous cell wall component of most pathogenic bacteria, vancomycin‐modified DONs have many potential applications in the prevention and treatment of nosocomial infections.","lang":"eng"}],"department":[{"_id":"302"}],"user_id":"48864","_id":"60973","language":[{"iso":"eng"}],"article_number":"2500246","publication_identifier":{"issn":["2688-4062","2688-4062"]},"publication_status":"published","citation":{"apa":"Coşkuner Leineweber, Ö., Pothineni, B. K., Schumann, N., Hofmann, U., Möser, C., Smith, D. M., Grundmeier, G., Zhang, Y., & Keller, A. (2025). Vancomycin‐Modified DNA Origami Nanostructures for Targeting Bacterial Pathogens. Small Structures, Article 2500246. https://doi.org/10.1002/sstr.202500246","bibtex":"@article{Coşkuner Leineweber_Pothineni_Schumann_Hofmann_Möser_Smith_Grundmeier_Zhang_Keller_2025, title={Vancomycin‐Modified DNA Origami Nanostructures for Targeting Bacterial Pathogens}, DOI={10.1002/sstr.202500246}, number={2500246}, journal={Small Structures}, publisher={Wiley}, author={Coşkuner Leineweber, Özge and Pothineni, Bhanu K. and Schumann, Nils and Hofmann, Ulrike and Möser, Christin and Smith, David M. and Grundmeier, Guido and Zhang, Yixin and Keller, Adrian}, year={2025} }","short":"Ö. Coşkuner Leineweber, B.K. Pothineni, N. Schumann, U. Hofmann, C. Möser, D.M. Smith, G. Grundmeier, Y. Zhang, A. Keller, Small Structures (2025).","mla":"Coşkuner Leineweber, Özge, et al. “Vancomycin‐Modified DNA Origami Nanostructures for Targeting Bacterial Pathogens.” Small Structures, 2500246, Wiley, 2025, doi:10.1002/sstr.202500246.","ieee":"Ö. Coşkuner Leineweber et al., “Vancomycin‐Modified DNA Origami Nanostructures for Targeting Bacterial Pathogens,” Small Structures, Art. no. 2500246, 2025, doi: 10.1002/sstr.202500246.","chicago":"Coşkuner Leineweber, Özge, Bhanu K. Pothineni, Nils Schumann, Ulrike Hofmann, Christin Möser, David M. Smith, Guido Grundmeier, Yixin Zhang, and Adrian Keller. “Vancomycin‐Modified DNA Origami Nanostructures for Targeting Bacterial Pathogens.” Small Structures, 2025. https://doi.org/10.1002/sstr.202500246.","ama":"Coşkuner Leineweber Ö, Pothineni BK, Schumann N, et al. Vancomycin‐Modified DNA Origami Nanostructures for Targeting Bacterial Pathogens. Small Structures. Published online 2025. doi:10.1002/sstr.202500246"},"year":"2025","author":[{"last_name":"Coşkuner Leineweber","full_name":"Coşkuner Leineweber, Özge","first_name":"Özge"},{"first_name":"Bhanu K.","last_name":"Pothineni","full_name":"Pothineni, Bhanu K."},{"first_name":"Nils","full_name":"Schumann, Nils","last_name":"Schumann"},{"last_name":"Hofmann","full_name":"Hofmann, Ulrike","first_name":"Ulrike"},{"first_name":"Christin","last_name":"Möser","full_name":"Möser, Christin"},{"last_name":"Smith","full_name":"Smith, David M.","first_name":"David M."},{"last_name":"Grundmeier","full_name":"Grundmeier, Guido","id":"194","first_name":"Guido"},{"full_name":"Zhang, Yixin","last_name":"Zhang","first_name":"Yixin"},{"full_name":"Keller, Adrian","id":"48864","last_name":"Keller","orcid":"0000-0001-7139-3110","first_name":"Adrian"}],"date_created":"2025-08-22T06:02:45Z","date_updated":"2025-08-22T06:04:06Z","publisher":"Wiley","doi":"10.1002/sstr.202500246","title":"Vancomycin‐Modified DNA Origami Nanostructures for Targeting Bacterial Pathogens"},{"status":"public","abstract":[{"text":"AbstractControlling the surface orientation of DNA origami nanostructures (DON) is crucial for applications in nanotechnology and materials science. While previous work utilized various DON modifications, simple methods for controlling their landing orientation remain scarce. Here, we demonstrate a straightforward approach to control the adsorption orientation of chiral double‐L (CDL) DON on mica by tuning magnesium ion (Mg2⁺) concentration and exploiting global shape distortions. Using atomic force microscopy (AFM), we analyzed the resulting distribution of the mirror‐image orientations, referred to as S and Z orientations, at both buffer/mica and air/mica interfaces and identified conditions resulting in homogenous CDL orientation of 100% S. These results demonstrate how DON conformation and ionic environments influence DON orientation, offering insights for precise nanostructure deposition.","lang":"eng"}],"publication":"Angewandte Chemie International Edition","type":"journal_article","language":[{"iso":"eng"}],"article_number":"e202507613","department":[{"_id":"302"}],"user_id":"48864","_id":"61821","citation":{"ieee":"G. Velpula, E. Tomm, B. Shen, K. S. Mali, A. C. Keller, and S. De Feyter, “Breaking of the Up‐Down Symmetry of DNA Origami on a Solid Substrate,” Angewandte Chemie International Edition, Art. no. e202507613, 2025, doi: 10.1002/anie.202507613.","chicago":"Velpula, Gangamallaiah, Emilia Tomm, Boxuan Shen, Kunal S. Mali, Adrian Clemens Keller, and Steven De Feyter. “Breaking of the Up‐Down Symmetry of DNA Origami on a Solid Substrate.” Angewandte Chemie International Edition, 2025. https://doi.org/10.1002/anie.202507613.","ama":"Velpula G, Tomm E, Shen B, Mali KS, Keller AC, De Feyter S. Breaking of the Up‐Down Symmetry of DNA Origami on a Solid Substrate. Angewandte Chemie International Edition. Published online 2025. doi:10.1002/anie.202507613","bibtex":"@article{Velpula_Tomm_Shen_Mali_Keller_De Feyter_2025, title={Breaking of the Up‐Down Symmetry of DNA Origami on a Solid Substrate}, DOI={10.1002/anie.202507613}, number={e202507613}, journal={Angewandte Chemie International Edition}, publisher={Wiley}, author={Velpula, Gangamallaiah and Tomm, Emilia and Shen, Boxuan and Mali, Kunal S. and Keller, Adrian Clemens and De Feyter, Steven}, year={2025} }","mla":"Velpula, Gangamallaiah, et al. “Breaking of the Up‐Down Symmetry of DNA Origami on a Solid Substrate.” Angewandte Chemie International Edition, e202507613, Wiley, 2025, doi:10.1002/anie.202507613.","short":"G. Velpula, E. Tomm, B. Shen, K.S. Mali, A.C. Keller, S. De Feyter, Angewandte Chemie International Edition (2025).","apa":"Velpula, G., Tomm, E., Shen, B., Mali, K. S., Keller, A. C., & De Feyter, S. (2025). Breaking of the Up‐Down Symmetry of DNA Origami on a Solid Substrate. Angewandte Chemie International Edition, Article e202507613. https://doi.org/10.1002/anie.202507613"},"year":"2025","publication_identifier":{"issn":["1433-7851","1521-3773"]},"publication_status":"published","doi":"10.1002/anie.202507613","title":"Breaking of the Up‐Down Symmetry of DNA Origami on a Solid Substrate","date_created":"2025-10-13T13:53:22Z","author":[{"last_name":"Velpula","full_name":"Velpula, Gangamallaiah","first_name":"Gangamallaiah"},{"first_name":"Emilia","full_name":"Tomm, Emilia","last_name":"Tomm"},{"full_name":"Shen, Boxuan","last_name":"Shen","first_name":"Boxuan"},{"full_name":"Mali, Kunal S.","last_name":"Mali","first_name":"Kunal S."},{"first_name":"Adrian Clemens","id":"48864","full_name":"Keller, Adrian Clemens","orcid":"0000-0001-7139-3110","last_name":"Keller"},{"first_name":"Steven","full_name":"De Feyter, Steven","last_name":"De Feyter"}],"publisher":"Wiley","date_updated":"2025-10-13T13:55:05Z"},{"publication_identifier":{"issn":["1439-4227","1439-7633"]},"publication_status":"published","citation":{"ama":"Garcia-Diosa JA, Grundmeier G, Keller A. Effect of DNA Origami Nanostructures on Bacterial Growth. ChemBioChem. Published online 2024. doi:10.1002/cbic.202400091","apa":"Garcia-Diosa, J. A., Grundmeier, G., & Keller, A. (2024). Effect of DNA Origami Nanostructures on Bacterial Growth. ChemBioChem. https://doi.org/10.1002/cbic.202400091","mla":"Garcia-Diosa, Jaime Andres, et al. “Effect of DNA Origami Nanostructures on Bacterial Growth.” ChemBioChem, Wiley, 2024, doi:10.1002/cbic.202400091.","short":"J.A. Garcia-Diosa, G. Grundmeier, A. Keller, ChemBioChem (2024).","bibtex":"@article{Garcia-Diosa_Grundmeier_Keller_2024, title={Effect of DNA Origami Nanostructures on Bacterial Growth}, DOI={10.1002/cbic.202400091}, journal={ChemBioChem}, publisher={Wiley}, author={Garcia-Diosa, Jaime Andres and Grundmeier, Guido and Keller, Adrian}, year={2024} }","chicago":"Garcia-Diosa, Jaime Andres, Guido Grundmeier, and Adrian Keller. “Effect of DNA Origami Nanostructures on Bacterial Growth.” ChemBioChem, 2024. https://doi.org/10.1002/cbic.202400091.","ieee":"J. A. Garcia-Diosa, G. Grundmeier, and A. Keller, “Effect of DNA Origami Nanostructures on Bacterial Growth,” ChemBioChem, 2024, doi: 10.1002/cbic.202400091."},"year":"2024","author":[{"first_name":"Jaime Andres","full_name":"Garcia-Diosa, Jaime Andres","last_name":"Garcia-Diosa"},{"first_name":"Guido","id":"194","full_name":"Grundmeier, Guido","last_name":"Grundmeier"},{"last_name":"Keller","orcid":"0000-0001-7139-3110","id":"48864","full_name":"Keller, Adrian","first_name":"Adrian"}],"date_created":"2024-02-03T12:41:16Z","date_updated":"2024-02-03T12:42:48Z","publisher":"Wiley","doi":"10.1002/cbic.202400091","title":"Effect of DNA Origami Nanostructures on Bacterial Growth","publication":"ChemBioChem","type":"journal_article","status":"public","abstract":[{"lang":"eng","text":"DNA origami nanostructures are a powerful tool in biomedicine and can be used to combat drug‐resistant bacterial infections. However, the effect of unmodified DNA origami nanostructures on bacteria is yet to be elucidated. With the aim to obtain a better understanding of this phenomenon, the effect of three DNA origami shapes, i.e., DNA origami triangles, six‐helix bundles (6HBs), and 24‐helix bundles (24HBs), on the growth of Gram‐negative Escherichia coli and Gram‐positive Bacillus subtilis is investigated. These results reveal that while triangles and 24HBs can be used as a source of nutrients by E. coli and thereby promote population growth, their effect is much smaller than that of genomic single‐ and double‐stranded DNA. However, no effect on E. coli population growth is observed for the 6HBs. On the other hand, B. subtilis does not show any significant changes in population growth when cultured with the different DNA origami shapes or genomic DNA. The detailed effect of DNA origami nanostructures on bacterial growth thus depends on the competence signals and uptake mechanism of each bacterial species, as well as the DNA origami shape. This should be considered in the development of antimicrobial DNA origami nanostructures."}],"department":[{"_id":"302"}],"user_id":"48864","_id":"51121","language":[{"iso":"eng"}],"keyword":["Organic Chemistry","Molecular Biology","Molecular Medicine","Biochemistry"]},{"abstract":[{"text":"The coupling of structural transitions to heat capacity changes leads to destabilization of macromolecules at both, elevated and lowered temperatures. DNA origami not only exhibit this property but also provide...","lang":"eng"}],"status":"public","type":"journal_article","publication":"Chemical Communications","keyword":["Materials Chemistry","Metals and Alloys","Surfaces","Coatings and Films","General Chemistry","Ceramics and Composites","Electronic","Optical and Magnetic Materials","Catalysis"],"language":[{"iso":"eng"}],"_id":"53621","user_id":"48864","department":[{"_id":"302"}],"year":"2024","citation":{"ama":"Dornbusch D, Hanke M, Tomm E, et al. Cold denaturation of DNA origami nanostructures. Chemical Communications. Published online 2024. doi:10.1039/d3cc05985e","chicago":"Dornbusch, Daniel, Marcel Hanke, Emilia Tomm, Charlotte Kielar, Guido Grundmeier, Adrian Keller, and Karim Fahmy. “Cold Denaturation of DNA Origami Nanostructures.” Chemical Communications, 2024. https://doi.org/10.1039/d3cc05985e.","ieee":"D. Dornbusch et al., “Cold denaturation of DNA origami nanostructures,” Chemical Communications, 2024, doi: 10.1039/d3cc05985e.","apa":"Dornbusch, D., Hanke, M., Tomm, E., Kielar, C., Grundmeier, G., Keller, A., & Fahmy, K. (2024). Cold denaturation of DNA origami nanostructures. Chemical Communications. https://doi.org/10.1039/d3cc05985e","short":"D. Dornbusch, M. Hanke, E. Tomm, C. Kielar, G. Grundmeier, A. Keller, K. Fahmy, Chemical Communications (2024).","bibtex":"@article{Dornbusch_Hanke_Tomm_Kielar_Grundmeier_Keller_Fahmy_2024, title={Cold denaturation of DNA origami nanostructures}, DOI={10.1039/d3cc05985e}, journal={Chemical Communications}, publisher={Royal Society of Chemistry (RSC)}, author={Dornbusch, Daniel and Hanke, Marcel and Tomm, Emilia and Kielar, Charlotte and Grundmeier, Guido and Keller, Adrian and Fahmy, Karim}, year={2024} }","mla":"Dornbusch, Daniel, et al. “Cold Denaturation of DNA Origami Nanostructures.” Chemical Communications, Royal Society of Chemistry (RSC), 2024, doi:10.1039/d3cc05985e."},"publication_status":"published","publication_identifier":{"issn":["1359-7345","1364-548X"]},"title":"Cold denaturation of DNA origami nanostructures","doi":"10.1039/d3cc05985e","date_updated":"2024-04-23T08:21:05Z","publisher":"Royal Society of Chemistry (RSC)","author":[{"last_name":"Dornbusch","full_name":"Dornbusch, Daniel","first_name":"Daniel"},{"full_name":"Hanke, Marcel","last_name":"Hanke","first_name":"Marcel"},{"id":"68157","full_name":"Tomm, Emilia","last_name":"Tomm","first_name":"Emilia"},{"first_name":"Charlotte","full_name":"Kielar, Charlotte","last_name":"Kielar"},{"first_name":"Guido","id":"194","full_name":"Grundmeier, Guido","last_name":"Grundmeier"},{"first_name":"Adrian","last_name":"Keller","orcid":"0000-0001-7139-3110","full_name":"Keller, Adrian","id":"48864"},{"full_name":"Fahmy, Karim","last_name":"Fahmy","first_name":"Karim"}],"date_created":"2024-04-23T08:20:05Z"},{"citation":{"ama":"Garcia-Diosa JA, Grundmeier G, Keller A. Highly Efficient Quenching of Singlet Oxygen by DNA Origami Nanostructures. Chemistry – A European Journal. Published online 2024. doi:10.1002/chem.202402057","chicago":"Garcia-Diosa, Jaime Andres, Guido Grundmeier, and Adrian Keller. “Highly Efficient Quenching of Singlet Oxygen by DNA Origami Nanostructures.” Chemistry – A European Journal, 2024. https://doi.org/10.1002/chem.202402057.","ieee":"J. A. Garcia-Diosa, G. Grundmeier, and A. Keller, “Highly Efficient Quenching of Singlet Oxygen by DNA Origami Nanostructures,” Chemistry – A European Journal, 2024, doi: 10.1002/chem.202402057.","mla":"Garcia-Diosa, Jaime Andres, et al. “Highly Efficient Quenching of Singlet Oxygen by DNA Origami Nanostructures.” Chemistry – A European Journal, Wiley, 2024, doi:10.1002/chem.202402057.","short":"J.A. Garcia-Diosa, G. Grundmeier, A. Keller, Chemistry – A European Journal (2024).","bibtex":"@article{Garcia-Diosa_Grundmeier_Keller_2024, title={Highly Efficient Quenching of Singlet Oxygen by DNA Origami Nanostructures}, DOI={10.1002/chem.202402057}, journal={Chemistry – A European Journal}, publisher={Wiley}, author={Garcia-Diosa, Jaime Andres and Grundmeier, Guido and Keller, Adrian}, year={2024} }","apa":"Garcia-Diosa, J. A., Grundmeier, G., & Keller, A. (2024). Highly Efficient Quenching of Singlet Oxygen by DNA Origami Nanostructures. Chemistry – A European Journal. https://doi.org/10.1002/chem.202402057"},"year":"2024","publication_identifier":{"issn":["0947-6539","1521-3765"]},"publication_status":"published","doi":"10.1002/chem.202402057","title":"Highly Efficient Quenching of Singlet Oxygen by DNA Origami Nanostructures","author":[{"first_name":"Jaime Andres","last_name":"Garcia-Diosa","full_name":"Garcia-Diosa, Jaime Andres"},{"first_name":"Guido","id":"194","full_name":"Grundmeier, Guido","last_name":"Grundmeier"},{"last_name":"Keller","orcid":"0000-0001-7139-3110","full_name":"Keller, Adrian","id":"48864","first_name":"Adrian"}],"date_created":"2024-06-07T07:53:50Z","publisher":"Wiley","date_updated":"2024-06-07T07:54:02Z","status":"public","abstract":[{"lang":"eng","text":"DNA origami nanostructures (DONs) are able to scavenge reactive oxygen species (ROS) and their scavenging efficiency toward ROS radicals was shown to be comparable to that of genomic DNA. Herein, we demonstrate that DONs are highly efficient singlet oxygen quenchers outperforming double‐stranded (ds) DNA by several orders of magnitude. To this end, a ROS mixture rich in singlet oxygen is generated by light irradiation of the photosensitizer methylene blue and its cytotoxic effect on Escherichia coli cells is quantified in the presence and absence of DONs. DONs are found to be vastly superior to dsDNA in protecting the bacteria from ROS‐induced damage and even surpass established ROS scavengers. At a concentration of 15 nM, DONs are about 50 000 times more efficient ROS scavengers than dsDNA at an equivalent concentration. This is attributed to the dominant role of singlet oxygen, which has a long diffusion length and reacts specifically with guanine. The dense packing of the available guanines into the small volume of the DON increases the overall quenching probability compared to a linear dsDNA with the same number of base pairs. DONs thus have great potential to alleviate oxidative stress caused by singlet oxygen in diverse therapeutic settings."}],"publication":"Chemistry – A European Journal","type":"journal_article","language":[{"iso":"eng"}],"department":[{"_id":"302"}],"user_id":"48864","_id":"54644"},{"year":"2024","citation":{"short":"L. Rabbe, J.A. Garcia‐Diosa, G. Grundmeier, A. Keller, Small Structures (2024).","mla":"Rabbe, Lukas, et al. “Ion‐Dependent Stability of DNA Origami Nanostructures in the Presence of Photo‐Generated Reactive Oxygen Species.” Small Structures, Wiley, 2024, doi:10.1002/sstr.202400094.","bibtex":"@article{Rabbe_Garcia‐Diosa_Grundmeier_Keller_2024, title={Ion‐Dependent Stability of DNA Origami Nanostructures in the Presence of Photo‐Generated Reactive Oxygen Species}, DOI={10.1002/sstr.202400094}, journal={Small Structures}, publisher={Wiley}, author={Rabbe, Lukas and Garcia‐Diosa, Jaime Andres and Grundmeier, Guido and Keller, Adrian}, year={2024} }","apa":"Rabbe, L., Garcia‐Diosa, J. A., Grundmeier, G., & Keller, A. (2024). Ion‐Dependent Stability of DNA Origami Nanostructures in the Presence of Photo‐Generated Reactive Oxygen Species. Small Structures. https://doi.org/10.1002/sstr.202400094","ieee":"L. Rabbe, J. A. Garcia‐Diosa, G. Grundmeier, and A. Keller, “Ion‐Dependent Stability of DNA Origami Nanostructures in the Presence of Photo‐Generated Reactive Oxygen Species,” Small Structures, 2024, doi: 10.1002/sstr.202400094.","chicago":"Rabbe, Lukas, Jaime Andres Garcia‐Diosa, Guido Grundmeier, and Adrian Keller. “Ion‐Dependent Stability of DNA Origami Nanostructures in the Presence of Photo‐Generated Reactive Oxygen Species.” Small Structures, 2024. https://doi.org/10.1002/sstr.202400094.","ama":"Rabbe L, Garcia‐Diosa JA, Grundmeier G, Keller A. Ion‐Dependent Stability of DNA Origami Nanostructures in the Presence of Photo‐Generated Reactive Oxygen Species. Small Structures. Published online 2024. doi:10.1002/sstr.202400094"},"publication_identifier":{"issn":["2688-4062","2688-4062"]},"publication_status":"published","title":"Ion‐Dependent Stability of DNA Origami Nanostructures in the Presence of Photo‐Generated Reactive Oxygen Species","doi":"10.1002/sstr.202400094","date_updated":"2024-07-18T09:03:49Z","publisher":"Wiley","author":[{"last_name":"Rabbe","full_name":"Rabbe, Lukas","first_name":"Lukas"},{"full_name":"Garcia‐Diosa, Jaime Andres","last_name":"Garcia‐Diosa","first_name":"Jaime Andres"},{"first_name":"Guido","last_name":"Grundmeier","id":"194","full_name":"Grundmeier, Guido"},{"first_name":"Adrian","last_name":"Keller","orcid":"0000-0001-7139-3110","full_name":"Keller, Adrian","id":"48864"}],"date_created":"2024-07-18T09:03:17Z","abstract":[{"text":"DNA origami nanostructures are promising carries for drug delivery applications. However, their limited stability under relevant conditions often presents a challenge. Herein, the structural stability of DNA origami nanostructures is investigated in a setting compatible with their application in photodynamic therapy (PDT). To this end, DNA origami triangles and six‐helix bundles (6HBs) are loaded with the clinically tested photosensitizer methylene blue, which upon irradiation with red light generates reactive oxygen species (ROS) that attack the DNA origami nanostructures. ROS‐induced structural damage is observed to depend on the ionic composition of the surrounding medium and becomes more severe at low ionic strength. Mg2+ ions can efficiently protect the DNA origami nanostructures from ROS‐induced damage and may even heal some of the damage obtained under Mg2+‐free conditions when added after irradiation. Finally, the employed DNA origami 6HBs are more resistant toward ROS‐induced structural damage than the triangles, which is attributed to their markedly different mechanical properties. These results thus provide some fundamental insights into the stabilizing role of DNA origami superstructure that may guide the selection or design of DNA origami nanocarriers with optimized stability for their application in PDT.","lang":"eng"}],"status":"public","publication":"Small Structures","type":"journal_article","language":[{"iso":"eng"}],"_id":"55310","department":[{"_id":"302"}],"user_id":"48864"},{"volume":15,"author":[{"first_name":"Hendrik","last_name":"Müller","full_name":"Müller, Hendrik"},{"full_name":"Stadler, Hartmut","last_name":"Stadler","first_name":"Hartmut"},{"orcid":"0000-0002-8684-273X ","last_name":"de los Arcos de Pedro","id":"54556","full_name":"de los Arcos de Pedro, Maria Teresa","first_name":"Maria Teresa"},{"first_name":"Adrian","last_name":"Keller","orcid":"0000-0001-7139-3110","full_name":"Keller, Adrian","id":"48864"},{"first_name":"Guido","id":"194","full_name":"Grundmeier, Guido","last_name":"Grundmeier"}],"date_created":"2025-02-12T14:48:49Z","date_updated":"2025-02-12T14:56:14Z","doi":"10.3762/bjnano.15.51","title":"AFM-IR investigation of thin PECVD SiO x films on a polypropylene substrate in the surface-sensitive mode","issue":"1","publication_identifier":{"issn":["2190-4286"]},"intvolume":" 15","page":"603–611","citation":{"mla":"Müller, Hendrik, et al. “AFM-IR Investigation of Thin PECVD SiO x Films on a Polypropylene Substrate in the Surface-Sensitive Mode.” Beilstein Journal of Nanotechnology, vol. 15, no. 1, 2024, pp. 603–611, doi:10.3762/bjnano.15.51.","short":"H. Müller, H. Stadler, M.T. de los Arcos de Pedro, A. Keller, G. Grundmeier, Beilstein Journal of Nanotechnology 15 (2024) 603–611.","bibtex":"@article{Müller_Stadler_de los Arcos de Pedro_Keller_Grundmeier_2024, title={AFM-IR investigation of thin PECVD SiO x films on a polypropylene substrate in the surface-sensitive mode}, volume={15}, DOI={10.3762/bjnano.15.51}, number={1}, journal={Beilstein Journal of Nanotechnology}, author={Müller, Hendrik and Stadler, Hartmut and de los Arcos de Pedro, Maria Teresa and Keller, Adrian and Grundmeier, Guido}, year={2024}, pages={603–611} }","apa":"Müller, H., Stadler, H., de los Arcos de Pedro, M. T., Keller, A., & Grundmeier, G. (2024). AFM-IR investigation of thin PECVD SiO x films on a polypropylene substrate in the surface-sensitive mode. Beilstein Journal of Nanotechnology, 15(1), 603–611. https://doi.org/10.3762/bjnano.15.51","ama":"Müller H, Stadler H, de los Arcos de Pedro MT, Keller A, Grundmeier G. AFM-IR investigation of thin PECVD SiO x films on a polypropylene substrate in the surface-sensitive mode. Beilstein Journal of Nanotechnology. 2024;15(1):603–611. doi:10.3762/bjnano.15.51","ieee":"H. Müller, H. Stadler, M. T. de los Arcos de Pedro, A. Keller, and G. Grundmeier, “AFM-IR investigation of thin PECVD SiO x films on a polypropylene substrate in the surface-sensitive mode,” Beilstein Journal of Nanotechnology, vol. 15, no. 1, pp. 603–611, 2024, doi: 10.3762/bjnano.15.51.","chicago":"Müller, Hendrik, Hartmut Stadler, Maria Teresa de los Arcos de Pedro, Adrian Keller, and Guido Grundmeier. “AFM-IR Investigation of Thin PECVD SiO x Films on a Polypropylene Substrate in the Surface-Sensitive Mode.” Beilstein Journal of Nanotechnology 15, no. 1 (2024): 603–611. https://doi.org/10.3762/bjnano.15.51."},"year":"2024","department":[{"_id":"302"}],"user_id":"54556","_id":"58611","language":[{"iso":"eng"}],"publication":"Beilstein Journal of Nanotechnology","type":"journal_article","status":"public","abstract":[{"lang":"eng","text":"AFM-IR investigation of thin PECVD SiOx films on a polypropylene substrate in the surface-sensitive mode"}]}]