Natural Agents-Mediated Targeting of Histone Deacetylases

被引:0
|
作者
Ammad Ahmad Farooqi
Syed Kamran-ul-Hassan Naqvi
Aliye Aras Perk
Onur Yanar
Sobia Tabassum
Muhammad Sheeraz Ahmad
Qaisar Mansoor
Mohamed S. Ashry
Muhammad Ismail
George E. Naoum
Waleed O. Arafat
机构
[1] Institute of Biomedical and Genetic Engineering,Division of Botany, Department of Biology, Faculty of Science
[2] COMSATS Institute of Information Technology,Department of Bioinformatics and Biotechnology
[3] Istanbul University,Institute of Biochemistry and Biotechnology
[4] International Islamic University,Department of radiation Oncology
[5] PMAS Arid Agriculture University,Clinical Oncology Department
[6] Alexandria Comprehensive Cancer Center,Clinical Oncology Department
[7] Harvard Medical School,undefined
[8] Massachusetts General Hospital,undefined
[9] Alexandria University,undefined
[10] Mansoura University,undefined
来源
Archivum Immunologiae et Therapiae Experimentalis | 2018年 / 66卷
关键词
Histone deacetylase (HDAC); Transcription regulation; TRAIL; Natural agents; Cancer;
D O I
暂无
中图分类号
学科分类号
摘要
In the past few years, basic and clinical scientists have witnessed landmark achievements in many research projects, such as those conducted by the US National Institutes of Health Roadmap Epigenomics Mapping Consortium, the International Human Epigenome Consortium, The Cancer Genome Atlas Network and the International Cancer Genome Consortium, which have provided near-complete resolution of epigenetic landscape in different diseases. Furthermore, genome sequencing of tumors has provided compelling evidence related to frequent existence of mutations in readers, erasers and writers of epigenome in different cancers. Histone acetylation is an intricate mechanism modulated by two opposing sets of enzymes and deeply studied as a key biological phenomenon in 1964 by Vincent Allfrey and colleagues. The research group suggested that this protein modification contributed substantially in transcriptional regulation. Subsequently, histone deacetylases (HDACs), histone acetyltransferases and acetyl-Lys-binding proteins were identified as transcriptional mediators, which further deepened our comprehension regarding biochemical modifications. Overwhelmingly increasing high-impact research is improving our understanding of this molecularly controlled mechanism; moreover, quantification and identification of lysine acetylation by mass spectrometry has added new layers of information. We partition this multi-component review into how both activity and expression of HDAC are targeted using natural agents. We also set spotlight on how oncogenic fusion proteins tactfully utilize HDAC-associated nano-machinery to modulate expression of different genes and how HDAC inhibitors regulate TRAIL-induced apoptosis in cancer cells. HDAC inhibitors have been reported to upregulate expression of TRAIL receptors and protect TRAIL from proteasomal degradation. Deeper understanding of HDAC biology will be useful for stratification and selection of patients who are responders, non-responders and poor-responders for HDACi therapy, and for the rational design of combination studies using HDACi.
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页码:31 / 44
页数:13
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