Defining the minimal peptide sequence of the ING1b tumour suppressor capable of efficiently inducing apoptosis
Author:
Publisher
Springer Science and Business Media LLC
Subject
Cancer Research,Cell Biology,Cellular and Molecular Neuroscience,Immunology
Link
http://www.nature.com/articles/cddiscovery201548.pdf
Reference47 articles.
1. Coles AH, Jones SN . The ING gene family in the regulation of cell growth and tumorigenesis. J Cell Physiol 2009; 218: 45–57.
2. He GH, Helbing CC, Wagner MJ, Sensen CW, Riabowol K . Phylogenetic analysis of the ING family of PHD proteins. Mol Biol Evol 2005; 22: 104–116.
3. Doyon Y, Cayrou C, Ullah M, Landry AJ, Côté V, Selleck W et al. ING tumor suppressor proteins are critical regulators of chromatin acetylation required for genome expression and perpetuation. Mol Cell 2006; 21: 51–64.
4. Peña PV, Hom RA, Hung T, Lin H, Kuo AJ, Wong RPC et al. Histone H3K4me3 binding is required for the DNA repair and apoptotic activities of ING1 tumour suppressor. J Mol Biol 2008; 380: 303–312.
5. Schäfer A, Karaulanov E, Stapf U, Döderlein G, Niehrs C . Ing1 functions in DNA demethylation by directing Gadd45a to H3K4me3. Genes Dev 2013; 27: 261–273.
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1. A minimal ING1b fragment that improves the efficacy of HDAC-based cancer cell killing;Cell Death & Disease;2015-12
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