Systematic analysis of human lysine acetylation proteins and accurate prediction of human lysine acetylation through bi-relative adapted binomial score Bayes feature representation

Shao, Jiahui; Xu, Dong; Hu, Landian; Kwan, Yiu Wa; Wang, Yifei; Kong, Xiangyin; Ngai, Sai-Ming

doi:10.1039/c2mb25251a

Cited by 62 publications

(54 citation statements)

References 78 publications

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“…It is worth considering that the identification of the acetylated sites can be influenced by the antibodies used for immunoaffinity enrichment of the modified peptides. However, the observations in bacteria seem to contrast other eukaryotic acetylation motifs, such as the glycine-rich histone acetylation motifs and the reported enrichment for aromatic and basic residues in other linear nuclear motifs (1,2,(73)(74)(75)(76). There are two possibilities for the significance of the enrichment in acidic residues in the vicinity of an acetylation site in bacteria.…”

mentioning

confidence: 79%

Regulation, Function, and Detection of Protein Acetylation in Bacteria

2017

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N -Lysine acetylation is now recognized as an abundant posttranslational modification (PTM) that influences many essential biological pathways. Advancements in mass spectrometry-based proteomics have led to the discovery that bacteria contain hundreds of acetylated proteins, contrary to the prior notion of acetylation events being rare in bacteria. Although the mechanisms that regulate protein acetylation are still not fully defined, it is understood that this modification is finely tuned via both enzymatic and nonenzymatic mechanisms. The opposing actions of Gcn5-related N-acetyltransferases (GNATs) and deacetylases, including sirtuins, provide the enzymatic control of lysine acetylation. A nonenzymatic mechanism of acetylation has also been demonstrated and proven to be prominent in bacteria, as well as in mitochondria. The functional consequences of the vast majority of the identified acetylation sites remain unknown. From studies in mammalian systems, acetylation of critical lysine residues was shown to impact protein function by altering its structure, subcellular localization, and interactions. It is becoming apparent that the same diversity of functions can be found in bacteria. Here, we review current knowledge of the mechanisms and the functional consequences of acetylation in bacteria. Additionally, we discuss the methods available for detecting acetylation sites, including quantitative mass spectrometry-based methods, which promise to promote this field of research. We conclude with possible future directions and broader implications of the study of protein acetylation in bacteria.

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confidence: 79%

Regulation, Function, and Detection of Protein Acetylation in Bacteria

2017

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“…Two in silico online programs, LAceP and BRABSB-PHKA, both predicted potential lysine (K) acetylation sites in human LSD1, including K432 and K436 (http://www.scbit.org/iPTM) (Hou et al, 2014;Shao et al, 2012). Global proteomics also uncovered acetylation of LSD1 K432, K433, and K436 (http://www.…”

Section: Mof Directly Acetylates Lsd1 At Lysine Residues 432 433 Anmentioning

confidence: 98%

MOF Acetylates the Histone Demethylase LSD1 to Suppress Epithelial-to-Mesenchymal Transition

Luo

Shenoy

et al. 2016

Cell Reports

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The histone demethylase LSD1 facilitates epithelial-to-mesenchymal transition (EMT) and tumor progression by repressing epithelial marker expression. However, little is known about how its function may be modulated. Here, we report that LSD1 is acetylated in epithelial but not mesenchymal cells. Acetylation of LSD1 reduces its association with nucleosomes, thus increasing histone H3K4 methylation at its target genes and activating transcription. The MOF acetyltransferase interacts with LSD1 and is responsible for its acetylation. MOF is preferentially expressed in epithelial cells and is downregulated by EMT-inducing signals. Expression of exogenous MOF impedes LSD1 binding to epithelial gene promoters and histone demethylation, thereby suppressing EMT and tumor invasion. Conversely, MOF depletion enhances EMT and tumor metastasis. In human cancer, high MOF expression correlates with epithelial markers and a favorable prognosis. These findings provide insight into the regulation of LSD1 and EMT and identify MOF as a critical suppressor of EMT and tumor progression.

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“…10 different algorithms were used; KacePred [48], PAIL [49], ASEB [50,51], Predmod [52], BRABSB-PHKA [53], PSKAcePred [54], PLMLA [55], PHOSIDA [56], EnsemblePail [57] and Lys Acet [58], which are, to our knowledge, the most frequently and widely used/cited methods for prediction of lysine acetylation sites. Threshold values were taken as stringent as possible for all predictions (Supplementary Table 1).…”

Section: Prediction Of Acetylated Lysines Of Nfat5mentioning

confidence: 99%