| Literature DB >> 27572818 |
Alokta Chakrabarti1, Jelena Melesina2, Fiona R Kolbinger3, Ina Oehme3, Johanna Senger1, Olaf Witt3,4, Wolfgang Sippl2, Manfred Jung1,5.
Abstract
Histone deacetylase 8 (HDAC8), a unique class I zinc-dependent HDAC, is an emerging target in cancer and other diseases. Its substrate repertoire extends beyond histones to many nonhistone proteins. Besides being a deacetylase, HDAC8 also mediates signaling via scaffolding functions. Aberrant expression or deregulated interactions with transcription factors are critical in HDAC8-dependent cancers. Many potent HDAC8-selective inhibitors with cellular activity and anticancer effects have been reported. We present HDAC8 as a druggable target and discuss inhibitors of different chemical scaffolds with cellular effects. Furthermore, we review HDAC8 activators that revert activity of mutant enzymes. Isotype-selective HDAC8 targeting in patients with HDAC8-relevant cancers is challenging, however, is promising to avoid adverse side effects as observed with pan-HDAC inhibitors.Entities:
Keywords: HDAC8; SMC3; T-cell; cancer; druggable; hydroxamic acid; inhibitor; stem cell; therapy
Mesh:
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Year: 2016 PMID: 27572818 DOI: 10.4155/fmc-2016-0117
Source DB: PubMed Journal: Future Med Chem ISSN: 1756-8919 Impact factor: 3.808