Class I histone deacetylases (HDAC1–3) are histone lysine delactylases

Moreno–Yruela, Carlos; Zhang, Di; Wei, Wei; Bæk, Michael; Li, Wenchao; Gao, Jinjun; Danková, Daniela; Nielsen, Alexander L.; Bolding, Julie E.; Yang, Lu; Jameson, Samuel T; Wong, Jiemin; Olsen, Christian A.; Zhao, Yingming

doi:10.1126/sciadv.abi6696

Cited by 194 publications

(204 citation statements)

References 78 publications

(140 reference statements)

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“…The sulfonates (5,6), sulfonamide (7), phosphonate (8), boronates (9)(10)(11), and fluorophenols (12,13) all exhibited poor inhibition of SIRT5. Among the series of heterocycles in our array of compounds (14)(15)(16)(17)(18)(19)(20)(21)(22)(23)(24)(25)(26), on the other hand, the 1,2,4-oxadiazol-5(4H)-one ( 16) and the tetrazole (24) exhibited similar IC 50 values to the parent compound (1), while the 2-hydroxy-isoxazole ( 22) also had a sub-micromolar IC 50 value (Figure 1). Finally, substituting the carboxylic acid for a hydroxamic acid (27) resulted in substantial loss of potency.…”

Section: Resultsmentioning

confidence: 93%

“…[3][4][5][6] Sirtuins 1-3 and 6 have exhibited preference for aliphatic acyl chains of different length ranging from ɛ-N-acetyllysine (Kac) to ɛ-N-myristoyllysine (Kmyr), [7][8][9] which is also reflected by hydrophobic binding pockets. [10][11][12][13] Moreover, SIRT1-3 has recently been reported to cleave both the D and L stereoisomers of ɛ-N-lactyllysine (Klac); [14,15] albeit, with lower efficiency than the zinc-dependent histone deacetylases (HDACs) 1-3. [15] Sirtuin 4 has been reported to cleave negatively charged modifications, such as ɛ-N-methylglutaconyllysine (Kmgc) and ɛ-N-(3-hydroxy-3-methylglutaryl)lysine (Khmg), [16,17] as well as ɛ-N-lipoyllysine (Klip) and ɛ-N-biotinyllysine (Kbio).…”

Section: Introductionmentioning

confidence: 99%

“…[10][11][12][13] Moreover, SIRT1-3 has recently been reported to cleave both the D and L stereoisomers of ɛ-N-lactyllysine (Klac); [14,15] albeit, with lower efficiency than the zinc-dependent histone deacetylases (HDACs) 1-3. [15] Sirtuin 4 has been reported to cleave negatively charged modifications, such as ɛ-N-methylglutaconyllysine (Kmgc) and ɛ-N-(3-hydroxy-3-methylglutaryl)lysine (Khmg), [16,17] as well as ɛ-N-lipoyllysine (Klip) and ɛ-N-biotinyllysine (Kbio). [18] Sirtuin 7 has been reported to cleave long chain acyl groups [19,20] and ɛ-Nglutaryllysine (Kglut), [21] and has been reported to be activated by oligonucleotides.…”

Section: Introductionmentioning

confidence: 99%

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Investigation of Carboxylic Acid Isosteres and Prodrugs for Inhibition of the Human SIRT5 Lysine Deacylase Enzyme**

et al. 2022

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Sirtuin 5 (SIRT5) is a protein lysine deacylase enzyme that regulates diverse biology by hydrolyzing ϵ‐N‐carboxyacyllysine posttranslational modifications in the cell. Inhibition of SIRT5 has been linked to potential treatment of several cancers but potent compounds with activity in cells have been lacking. Here we developed mechanism‐based inhibitors that incorporate isosteres of a carboxylic acid residue that is important for high‐affinity binding to the enzyme active site. By masking of the tetrazole moiety of the most potent candidate from our initial SAR study, we achieved potent and cytoselective growth inhibition for the treatment of SIRT5‐dependent leukemic cancer cell lines in culture. Thus, we provide an efficient, cellularly active small molecule that targets SIRT5, which can help elucidate its function and potential as a future drug target. This work shows that masked isosteres of carboxylic acids are viable chemical motifs for the development of inhibitors that target mitochondrial enzymes, which may have applications beyond the sirtuin field.

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Section: Resultsmentioning

confidence: 93%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Investigation of Carboxylic Acid Isosteres and Prodrugs for Inhibition of the Human SIRT5 Lysine Deacylase Enzyme**

et al. 2022

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“…These results therefore suggest that protein lactylation is reversible and likely regulated by the HDAC family, consistent with a very recent report. 8 Furthermore, we examined the applicability and generality of YnLac for the metabolic labelling of proteins in various cell lines. Robust protein labelling by YnLac was observed for all cell types tested (Fig.…”

Section: Resultsmentioning

confidence: 99%

A bioorthogonal chemical reporter for the detection and identification of protein lactylation

2022

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“…Further pull-down experiments with cell lysates allowed the successful identification of 475 and 472 putative substrates of p300 and GCN5, respectively. Among them, two novel substrates of GCN5, Kcr p300 [28] CBP, PCAF hMOF [29] WB; IP/WB Sirt1 [44] Sirt1-3 [46] HDAC1 & 3 [29] HDAC1-3 & 8 [44] IF/WB AfBP IP/WB IF/WB AF9 [89] YEATS2 [91] MOZ/DPF2 [92] Taf14 [90] ITC/Microarray/X-ray/IP X-ray/NMR/Pull-Down Ksucc GCN5 [30] p300 [34] IP-MS WB Sirt5 [20] Sirt7 [21] LC-MS/MS/X-ray IP/LC-MS/MS GAS41 [93] Pull-Down/X-ray Kmal NA NR Sirt5 [20] LC-MS/MS/X-ray NA NR Kglu GCN5 [35] IP/WB Sirt5 [47] Sirt7 [35] FL probe/LC-MS/WB MCR/WB/LC-MS/MS NA NR Khib p300 [31] Tip60 [32] WB/IF WB/MS HDAC2 [32] HDAC3 [32] WB/MS NA NR Kbhb p300 [33] WB HDAC1 & 2 [33] Sirt3 [53] WB/LC X-ray/WB NA NR Klip LIPT1-2 [22][23] WB Sirt4 [8] Sirt2 [48] IP/LC-MS/MS AfBP NA NR Kmyr NMT1-2 [24] LC-MS/X-ray /MCR HDAC8 [50] , Sirt2 [25] Sirt6 [26] , Sirt7 [52] MCR NA NR Kbz NA NR Sirt2 [4] LC-MS/WB DPF, YEATS [27] ITC/Microarray/X-ray/IF Kla p300 [2] LC-MS/WB HDAC1 & 3 [126] FL Probe/WB NA NR Kinic CBP, p300 [5] WB HDAC3 [5] IF namely the structural...…”

Section: Coa-based Activity-based Probesmentioning

confidence: 99%

Chemical Biology Tools for Protein Lysine Acylation

Xie

Liu

et al. 2022

Angewandte Chemie

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Lysine acylation plays pivotal roles in cell physiology, including DNA transcription and repair, signal transduction, immune defense, metabolism, and many other key cellular processes. Molecular mechanisms of dysregulated lysine acylation are closely involved in the pathophysiological progress of many human diseases, most notably cancers. In recent years, chemical biology tools have become instrumental in studying the function of post‐translational modifications (PTMs), identifying new “writers”, “erasers” and “readers”, and in targeted therapies. Here, we describe key developments in chemical biology approaches that have advanced the study of lysine acylation and its regulatory proteins (2016–2021). We further discuss the discovery of ligands (inhibitors and PROTACs) that are capable of targeting regulators of lysine acylation. Next, we discuss some current challenges of these chemical biology probes and suggest how chemists and biologists can utilize chemical probes with more discriminating capacity. Finally, we suggest some critical considerations in future studies of PTMs from our perspective.

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Class I histone deacetylases (HDAC1–3) are histone lysine delactylases

Cited by 194 publications

References 78 publications

Investigation of Carboxylic Acid Isosteres and Prodrugs for Inhibition of the Human SIRT5 Lysine Deacylase Enzyme**

Investigation of Carboxylic Acid Isosteres and Prodrugs for Inhibition of the Human SIRT5 Lysine Deacylase Enzyme**

A bioorthogonal chemical reporter for the detection and identification of protein lactylation

Chemical Biology Tools for Protein Lysine Acylation

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