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Computational Exploration of Zinc Binding Groups for HDAC Inhibition
Abstract
Histone deacetylases (HDACs) have emerged as important drug targets in epigenetics. The most common HDAC inhibitors use hydroxamic acids as zinc binding groups despite unfavorable pharmacokinetic properties. A two-stage protocol of M05-2X calculations of a library of 48 fragments in a small model active site, followed by QM/MM hybrid calculations of the full enzyme with selected binders, is used to prospectively select potential bidentate zinc binders. The energetics and interaction patterns of several zinc binders not previously used for the inhibition of HDACs are discussed- Dataset
- Dataset
- Biophysics
- Biochemistry
- Cell Biology
- Genetics
- Molecular Biology
- Pharmacology
- Cancer
- Chemical Sciences not elsewhere classified
- calculation
- HDAC InhibitionHistone deacetylases
- interaction patterns
- drug targets
- HDAC inhibitors use hydroxamic acids
- 48 fragments
- pharmacokinetic properties
- Zinc Binding Groups
- Computational Exploration
- bidentate zinc binders
- zinc binding groups
- QM
- zinc binders
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Last time updated on 12/02/2018
This paper was published in The Francis Crick Institute.
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Licence: CC BY-NC 4.0