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Literature DB >> 19746508

Syringolin A selectively labels the 20 S proteasome in murine EL4 and wild-type and bortezomib-adapted leukaemic cell lines.

Jérôme Clerc¹, Bogdan I Florea, Marianne Kraus, Michael Groll, Robert Huber, André S Bachmann, Robert Dudler, Christoph Driessen, Herman S Overkleeft, Markus Kaiser.

Abstract

The natural product syringolin A (SylA) is a potent proteasome inhibitor with promising anticancer activities. To further investigate its potential as a lead structure, selectivity profiling with cell lysates was performed. At therapeutic concentrations, a rhodamine-tagged SylA derivative selectively bound to the 20 S proteasome active sites without detectable off-target labelling. Additional profiling with lysates of wild-type and bortezomib-adapted leukaemic cell lines demonstrated the retention of this proteasome target and subsite selectivity as well as potency even in clinically relevant cell lines. Our studies, therefore, propose that further development of SylA might indeed result in an improved small molecule for the treatment of leukaemia.

Entities: Chemical Disease Gene Species

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Year: 2009 PMID： 19746508 DOI： 10.1002/cbic.200900411

Source DB: PubMed Journal: Chembiochem ISSN： 1439-4227 Impact factor: 3.164

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Cited

15 in total

1. Enzymatic timing and tailoring of macrolactamization in syringolin biosynthesis.

Authors: William M Wuest; Daniel Krahn; Markus Kaiser; Christopher T Walsh
Journal: Org Lett Date: 2011-08-03 Impact factor: 6.005

2. Proteasome activity imaging and profiling characterizes bacterial effector syringolin A.

Authors: Izabella Kolodziejek; Johana C Misas-Villamil; Farnusch Kaschani; Jérôme Clerc; Christian Gu; Daniel Krahn; Sherry Niessen; Martijn Verdoes; Lianne I Willems; Hermen S Overkleeft; Markus Kaiser; Renier A L van der Hoorn
Journal: Plant Physiol Date: 2010-11-02 Impact factor: 8.340

3. Syrbactin Structural Analog TIR-199 Blocks Proteasome Activity and Induces Tumor Cell Death.

Authors: André S Bachmann; John Opoku-Ansah; Tannya R Ibarra-Rivera; Lisette P Yco; Sudhakar Ambadi; Christopher C Roberts; Chia-En A Chang; Michael C Pirrung
Journal: J Biol Chem Date: 2016-02-23 Impact factor: 5.157

4. Syrbactin proteasome inhibitor TIR-199 overcomes bortezomib chemoresistance and inhibits multiple myeloma tumor growth in vivo.

Authors: Marquicia R Pierce; Reeder M Robinson; Tannya R Ibarra-Rivera; Michael C Pirrung; Nathan G Dolloff; André S Bachmann
Journal: Leuk Res Date: 2019-11-12 Impact factor: 3.156

5. Discovery of a potent and highly β1 specific proteasome inhibitor from a focused library of urea-containing peptide vinyl sulfones and peptide epoxyketones.

Authors: Wouter A van der Linden; Lianne I Willems; Tamer B Shabaneh; Nan Li; Mark Ruben; Bogdan I Florea; Gijs A van der Marel; Markus Kaiser; Alexei F Kisselev; Herman S Overkleeft
Journal: Org Biomol Chem Date: 2011-11-22 Impact factor: 3.876

10. Activity-based probes for studying the activity of flavin-dependent oxidases and for the protein target profiling of monoamine oxidase inhibitors.

Authors: Joanna M Krysiak; Johannes Kreuzer; Peter Macheroux; Albin Hermetter; Stephan A Sieber; Rolf Breinbauer
Journal: Angew Chem Int Ed Engl Date: 2012-06-11 Impact factor: 15.336

Syringolin A selectively labels the 20 S proteasome in murine EL4 and wild-type and bortezomib-adapted leukaemic cell lines.

1. Enzymatic timing and tailoring of macrolactamization in syringolin biosynthesis.

2. Proteasome activity imaging and profiling characterizes bacterial effector syringolin A.

3. Syrbactin Structural Analog TIR-199 Blocks Proteasome Activity and Induces Tumor Cell Death.

4. Syrbactin proteasome inhibitor TIR-199 overcomes bortezomib chemoresistance and inhibits multiple myeloma tumor growth in vivo.

5. Discovery of a potent and highly β1 specific proteasome inhibitor from a focused library of urea-containing peptide vinyl sulfones and peptide epoxyketones.

6. SylC catalyzes ureido-bond formation during biosynthesis of the proteasome inhibitor syringolin A.

Review 7. Activity-based imaging probes of the proteasome.

8. Development of Proteasome Inhibitors as Therapeutic Drugs.

9. The antimalarial natural product symplostatin 4 is a nanomolar inhibitor of the food vacuole falcipains.

10. Activity-based probes for studying the activity of flavin-dependent oxidases and for the protein target profiling of monoamine oxidase inhibitors.