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Dive into the research topics where Stephan Güttinger is active.

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Featured researches published by Stephan Güttinger.


Journal of the American Chemical Society | 2010

Anguinomycins and Derivatives: Total Syntheses, Modeling, and Biological Evaluation of the Inhibition of Nucleocytoplasmic Transport

Simone Bonazzi; Oliv Eidam; Stephan Güttinger; Jean-Yves Wach; Ivo Zemp; Ulrike Kutay; Karl Gademann

The preparation of the polyketide natural products anguinomycin C and D is reported based on key steps such as Negishi stereoinversion cross coupling, Jacobsen Cr(III)-catalyzed Hetero Diels-Alder reaction, Evans B-mediated syn-aldol chemistry, and B-alkyl Suzuki-Miyaura cross coupling. The configuration of both natural products was established as (5R,10R,16R,18S,19R,20S). Biological evaluation demonstrated that these natural products are inhibitors of the nuclear export receptor CRM1, leading to shutdown of CRM1-mediated nuclear protein export at concentrations above 10 nM. Analogues of anguinomycin and leptomycin B (LMB) have been prepared, and the simple alpha,beta-unsaturated lactone analogue 4 with a truncated polyketide chain retains most of the biological activity (inhibition above 25 nM). The structural basis for this inhibition has been demonstrated by modeling the transport inhibitors into X-ray crystal structures, thus highlighting key points for successful and strong biological action of anguinomycin and LMB.


FEBS Letters | 2006

Nuclear envelope localization of human UNC84A does not require nuclear lamins.

Sameez Hasan; Stephan Güttinger; Petra Mühlhäusser; Fabian Anderegg; Simone Bürgler; Ulrike Kutay

The SUN proteins are a conserved family of proteins in eukaryotes. Human UNC84A (Sun1) is a homolog of Caenorhabditis elegans UNC‐84, a protein involved in nuclear anchorage and migration. We have analyzed targeting of UNC84A to the nuclear envelope (NE) and show that the N‐terminal 300 amino acids are crucial for efficient NE localization of UNC84A whereas the conserved C‐terminal SUN domain is not required. Furthermore, we demonstrate by combining RNA interference with immunofluorescence and fluorescence recovery after photobleaching analysis that localization and anchoring of UNC84A is not dependent on the lamin proteins, in contrast to what had been observed for C. elegans UNC‐84.


RNA | 2013

The double-stranded RNA binding domain of human Dicer functions as a nuclear localization signal

Michael Doyle; Lukas Badertscher; Lukasz Jaskiewicz; Stephan Güttinger; Sabine Jurado; Tabea Hugenschmidt; Ulrike Kutay; Witold Filipowicz

Dicer is a key player in microRNA (miRNA) and RNA interference (RNAi) pathways, processing miRNA precursors and double-stranded RNA into ∼21-nt-long products ultimately triggering sequence-dependent gene silencing. Although processing of substrates in vertebrate cells occurs in the cytoplasm, there is growing evidence suggesting Dicer is also present and functional in the nucleus. To address this possibility, we searched for a nuclear localization signal (NLS) in human Dicer and identified its C-terminal double-stranded RNA binding domain (dsRBD) as harboring NLS activity. We show that the dsRBD-NLS can mediate nuclear import of a reporter protein via interaction with importins β, 7, and 8. In the context of full-length Dicer, the dsRBD-NLS is masked. However, duplication of the dsRBD localizes the full-length protein to the nucleus. Furthermore, deletion of the N-terminal helicase domain results in partial accumulation of Dicer in the nucleus upon leptomycin B treatment, indicating that CRM1 contributes to nuclear export of Dicer. Finally, we demonstrate that human Dicer has the ability to shuttle between the nucleus and the cytoplasm. We conclude that Dicer is a shuttling protein whose steady-state localization is cytoplasmic.


Bioorganic & Medicinal Chemistry Letters | 2010

The cytotoxic styryl lactone goniothalamin is an inhibitor of nucleocytoplasmic transport

Jean-Yves Wach; Stephan Güttinger; Ulrike Kutay; Karl Gademann

An in vivo nuclear export assay (immunostaining of Rio2 in HeLa cells) demonstrated that (R)-goniothalamin is an inhibitor of nucleocytoplasmic transport above 500 nM, which was rationalized also by molecular modeling. The cytotoxic styryl lactone natural product was prepared via an enantioselective Cr(III) catalyzed hetero Diels-Alder reaction and a Sonogashira coupling. A series of analogs was synthesized and only the oxidized goniothalamin derivative featuring an alkyne spacer was found active. Unsaturated lactones of natural origin other than leptomycin (LMB) are thus suggested to operate via a similar mechanism targeting the CRM1 nuclear receptor.


Science | 2004

Nuclear export of microRNA precursors.

Elsebet Lund; Stephan Güttinger; Angelo Calado; James E. Dahlberg; Ulrike Kutay


Trends in Cell Biology | 2005

Leucine-rich nuclear-export signals: born to be weak

Ulrike Kutay; Stephan Güttinger


Nature Reviews Molecular Cell Biology | 2009

Orchestrating nuclear envelope disassembly and reassembly during mitosis

Stephan Güttinger; Eva Laurell; Ulrike Kutay


Molecular Cell | 2006

The Conserved Transmembrane Nucleoporin NDC1 Is Required for Nuclear Pore Complex Assembly in Vertebrate Cells

Jörg Mansfeld; Stephan Güttinger; Lisa A. Hawryluk-Gara; Nelly Panté; Moritz Mall; Vincent Galy; Uta Haselmann; Petra Mühlhäusser; Richard W. Wozniak; Iain W. Mattaj; Ulrike Kutay; Wolfram Antonin


Proceedings of the National Academy of Sciences of the United States of America | 2004

Transportin2 functions as importin and mediates nuclear import of HuR.

Stephan Güttinger; Petra Mühlhäusser; Roland Koller-Eichhorn; Julius Brennecke; Ulrike Kutay


Angewandte Chemie | 2007

Total Synthesis, Configuration, and Biological Evaluation of Anguinomycin C†

Simone Bonazzi; Stephan Güttinger; Ivo Zemp; Ulrike Kutay; Karl Gademann

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Simone Bonazzi

École Polytechnique Fédérale de Lausanne

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Jean-Yves Wach

École Polytechnique Fédérale de Lausanne

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