Hesperadin hydrochloride
Chemical Name: N-[2,3-Dihydro-2-oxo-3-[(3Z)-phenyl[[4-(1-piperidinylmethyl)phenyl]amino]methylene]-1H-indol-5-yl]-ethanesulfonamide hydrochloride
Purity: ≥99%
Biological Activity
Hesperadin hydrochloride is an ATP-competitive inhibitor of Aurora B kinase (IC50 = 250 nM). Prevents chromosome alignment and segregation; also induces polyploidy and prevents histone H3-Ser10 phosphorylation. Overrides the spindle assembly checkpoint and induces mitotic exit in monastrol- and taxol-treated HeLa cells. Inhibits replication of influenza A and B viral strains (IC50 values range from 0.22 μM to 1.8 μM, dependant on strain), by inhibiting viral RNA transcription and translationTechnical Data
The technical data provided above is for guidance only.
For batch specific data refer to the Certificate of Analysis.
Tocris products are intended for laboratory research use only, unless stated otherwise.
Background References
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The small molecule Hesperadin reveals a role for Aurora B in correcting kinetochore-microtubule attachment and in maintaining the spindle assembly checkpoint.
Hauf, S et al.
J Cell Biol;161(2):281-94. -
The cell cycle as a therapeutic target against Trypanosoma brucei: Hesperadin inhibits Aurora kinase-1 and blocks mitotic progression in bloodstream forms.
Jetton et al.
Mol.Microbiol., 2009;72:442 -
Mechanism of Aurora B activation by INCENP and inhibition by Hesperadin.
Sessa et al.
Mol.Cell., 2005;18:379 -
Chemical genomics approach leads to the identification of hesperadin, an aurora B kinase inhibitor, as a broad-spectrum influenza antiviral.
Hu et al.
Int.J.Mol.Sci., 2017;18:1929
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Citations for Hesperadin hydrochloride
The citations listed below are publications that use Tocris products. Selected citations for Hesperadin hydrochloride include:
2 Citations: Showing 1 - 2
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Histone variant H3.3 residue S31 is essential for Xenopus gastrulation regardless of the deposition pathway.
Authors: Damarys Et al.
Nat Commun 2020;11:1256
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DGAT2 partially compensates for lipid-induced ER stress in human DGAT1-deficient intestinal stem cells.
Authors: Judith Et al.
J Lipid Res 2019;60:1787-1800
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