Your search keyword '"DGKA"' showing total 13 results

1. Targeting diacylglycerol kinase α impairs lung tumorigenesis by inhibiting cyclin D3

Author

Dong Zhou, Tao Liu, Xinrui Rao, Xiaohua Jie, Yunshang Chen, Zilong Wu, Huilin Deng, Dan Zhang, Jian Wang, and Gang Wu

Subjects

DGKA, lung cancer, CCND3, tumorigenesis, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract Background Diacylglycerol kinase α (DGKA) is the first member discovered from the diacylglycerol kinase family, and it has been linked to the progression of various types of tumors. However, it is unclear whether DGKA is linked to the development of lung cancer. Methods We investigated the levels of DGKA in the lung cancer tissues. Cell growth assay, colony formation assay and EdU assay were used to examine the effects of DGKA‐targeted siRNAs/shRNAs/drugs on the proliferation of lung cancer cells in vitro. Xenograft mouse model was used to investigate the role of DGKA inhibitor ritanserin on the proliferation of lung cancer cells in vivo. The downstream target of DGKA in lung tumorigenesis was identified by RNA sequencing. Results DGKA is upregulated in the lung cancer cells. Functional assays and xenograft mouse model indicated that the proliferation ability of lung cancer cells was impaired after inhibiting DGKA. And cyclin D3(CCND3) is the downstream target of DGKA promoting lung cancer. Conclusions Our study demonstrated that DGKA promotes lung tumorigenesis by regulating the CCND3 expression and hence it can be considered as a potential molecular biomarker to evaluate the prognosis of lung cancer patients. What's more, we also demonstrated the efficacy of ritanserin as a promising new medication for treating lung cancer.

Published

2023

2. Targeting diacylglycerol kinase α impairs lung tumorigenesis by inhibiting cyclin D3.

Author

Zhou, Dong, Liu, Tao, Rao, Xinrui, Jie, Xiaohua, Chen, Yunshang, Wu, Zilong, Deng, Huilin, Zhang, Dan, Wang, Jian, and Wu, Gang

Subjects

*CARCINOGENESIS, *WESTERN immunoblotting, *LUNG tumors, *TRANSFERASES, *RESEARCH funding, *CELL lines

Abstract

Background: Diacylglycerol kinase α (DGKA) is the first member discovered from the diacylglycerol kinase family, and it has been linked to the progression of various types of tumors. However, it is unclear whether DGKA is linked to the development of lung cancer. Methods: We investigated the levels of DGKA in the lung cancer tissues. Cell growth assay, colony formation assay and EdU assay were used to examine the effects of DGKA‐targeted siRNAs/shRNAs/drugs on the proliferation of lung cancer cells in vitro. Xenograft mouse model was used to investigate the role of DGKA inhibitor ritanserin on the proliferation of lung cancer cells in vivo. The downstream target of DGKA in lung tumorigenesis was identified by RNA sequencing. Results: DGKA is upregulated in the lung cancer cells. Functional assays and xenograft mouse model indicated that the proliferation ability of lung cancer cells was impaired after inhibiting DGKA. And cyclin D3(CCND3) is the downstream target of DGKA promoting lung cancer. Conclusions: Our study demonstrated that DGKA promotes lung tumorigenesis by regulating the CCND3 expression and hence it can be considered as a potential molecular biomarker to evaluate the prognosis of lung cancer patients. What's more, we also demonstrated the efficacy of ritanserin as a promising new medication for treating lung cancer. [ABSTRACT FROM AUTHOR]

Published

2023

3. Light‐Induced Uncaging for Time‐Resolved Observations of Biochemical Reactions by MAS NMR Spectroscopy.

Author

Mos, Julian, Jakob, Andreas, Becker‐Baldus, Johanna, Heckel, Alexander, and Glaubitz, Clemens

Subjects

*NUCLEAR magnetic resonance spectroscopy, *MAGIC angle spinning, *MEMBRANE proteins, *BILAYER lipid membranes, *TIME-resolved spectroscopy, *LIPIDS

Abstract

Light‐induced activation of biomolecules by uncaging of photolabile protection groups has found many applications for triggering biochemical reactions with minimal perturbations directly within cells. Such an approach might also offer unique advantages for solid‐state NMR experiments on membrane proteins for initiating reactions within or at the membrane directly within the closed MAS rotor. Herein, we demonstrate that the integral membrane protein E. coli diacylglycerol kinase (DgkA), which catalyzes the phosphorylation of diacylglycerol, can be controlled by light under MAS‐NMR conditions. Uncaging of NPE‐ATP or of lipid substrate NPE‐DOG by in situ illumination triggers its enzymatic activity, which can be monitored by real‐time 31P‐MAS NMR. This proof‐of‐concept illustrates that combining MAS‐NMR with uncaging strategies and illumination methods offers new possibilities for controlling biochemical reactions at or within lipid bilayers. [ABSTRACT FROM AUTHOR]

Published

2020

4. BET-bromodomain inhibitors modulate epigenetic patterns at the diacylglycerol kinase alpha enhancer associated with radiation-induced fibrosis.

Author

Valinciute, Gintvile, Weigel, Christoph, Veldwijk, Marlon R., Oakes, Christopher C., Herskind, Carsten, Wenz, Frederik, Plass, Christoph, Schmezer, Peter, and Popanda, Odilia

Subjects

*FIBROSIS, *BROMODOMAIN-containing 1 gene, *RADIATION-induced abnormalities, *EPIGENETICS, *DIGLYCERIDES, *TREATMENT effectiveness, *THERAPEUTICS

Abstract

Background and purpose Fibrosis is a frequent adverse effect of radiotherapy and no effective treatments are currently available to prevent or reverse fibrotic disease. We have previously identified altered epigenetic patterns at a gene enhancer of the diacylglycerol kinase alpha ( DGKA ) locus in normal skin fibroblasts derived from fibrosis patients. An open chromatin pattern related to radiation-inducibility of DGKA is associated with onset of radiation-induced fibrosis. Here, we explore epigenetic modulation of DGKA as a way to mitigate predisposition to fibrosis. Material and methods We studied the effect of the BET-bromodomain inhibitors (JQ1, PFI-1) on DGKA inducibility in primary fibroblasts. Hence, DGKA transcription was additionally induced by the radiomimetic drug bleomycin, and DGKA mRNA expression, histone H3K27 acetylation and downstream markers of profibrotic fibroblast activation after BET-bromodomain inhibition were determined. Results BET-bromodomain inhibition suppressed induction of DGKA in bleomycin-treated fibroblasts, reduced H3K27ac at the DGKA enhancer and repressed collagen marker gene expression. Alterations in fibroblast morphology and reduction of collagen deposition were observed. Conclusion For the DGKA enhancer, we show that BET-bromodomain inhibitors can alter the epigenetic landscape of fibroblasts, thus counteracting profibrotic transcriptional events. Interference with epigenetic patterns of fibrosis predisposition may provide novel preventive therapies that improve radiotherapy. [ABSTRACT FROM AUTHOR]

Published

2017

5. Diacylglycerol Kinase α is a Pharmacologically Targetable Immune Regulator with a Newly Identified Role in Macrophage Activation

Subjects

DGKa, T-cell, immune regulation, diacylglycerol kinase, glioblastoma, melanoma, wound healing, macrophage, ritanserin, BMDM

Abstract

The diacylglycerol kinases (DGKs) are a family of lipid kinases whose primary function is the conversion of diacylglycerol (DAG) to phosphatidic acid (PA). There has been mounting evidence indicating that DGK enzymes are implicated in other physiologic processes, ranging from immune cell regulation to cancer progression. DGKα in particular is a known promoter of T-cell anergy, and has been demonstrated as a promising therapeutic target in multiple cancers including glioblastoma (GBM) and melanoma. Prior to these following studies, the only significant phenotype observed in DGKα knockout (KO) mice has been enhanced T-cell activity. Herein we reveal a novel, macrophage-specific, immune-regulatory function of DGKα. In bone marrow-derived macrophages (BMDMs) cultured from wild-type (WT) and KO mice, we observed increased responsiveness of KO macrophages to activating stimuli. Knockdown (KD) of Dgka in a murine macrophage cell line resulted in similar increased responsiveness. Demonstrating in vivo relevance, we observed significantly smaller wounds in Dgka-/- mice with full-thickness cutaneous burns, a complex wound healing process in which macrophages play a key role. The burned area also had increased numbers of macrophages. In a cortical stab wound model, Dgka-/- brains show increased Iba1+ cell numbers at the needle track versus that in WT brains. Targeting DGKα in order to stimulate T-cell function or to combat its tumorigenic effects in cancer is feasible due to the existence of several small-molecule inhibitors. R59949 and R59022 are tool compounds which limit the DGKα conversion of DAG to PA. The compound ritanserin was originally implicated clinically as a serotonin receptor antagonist used for the treatment of schizophrenia and has been used in clinical trial settings with no demonstrated adverse effects. Likely due to ritanserin’s structural similarity to R59949 and R59022, it is also capable of inhibiting DGKα, with the added benefits of safety and being clinically actionable. In the following studies, we have identified several additional and potentially clinically relevant small molecule compounds from a library of ritanserin analogs which are more potent and specific for DGKα than those identified previously. Effective targeting of DGKα has promising therapeutic implications, and our newly identified immune regulatory role of DGKα is further support for the appeal of developing these compounds. Taken together, these studies present a novel immune-regulatory function of DGKα in macrophages with potential implications for wound healing, cancer therapy, and other settings, and the identification of inhibitory compounds to translate these findings therapeutically.

Published

2021

6. Light‐induced uncaging for time‐resolved observations of biochemical reactions by MAS NMR spectroscopy

Author

Clemens Glaubitz, Alexander Heckel, Andreas Jakob, Johanna Becker-Baldus, and Julian de Mos

Subjects

Diacylglycerol Kinase, Magnetic Resonance Spectroscopy, enzymes, Lipid Bilayers, 010402 general chemistry, 01 natural sciences, Catalysis, Cell Physiological Phenomena, DgkA, Enzymes | Very Important Paper, NMR spectroscopy, caged ATP, ddc:570, Escherichia coli, caged diacylglycerol, Phosphorylation, Lipid bilayer, Nuclear Magnetic Resonance, Biomolecular, Integral membrane protein, Diacylglycerol kinase, chemistry.chemical_classification, 010405 organic chemistry, Chemistry, Communication, Biomolecule, Organic Chemistry, fungi, Membrane Proteins, General Chemistry, Nuclear magnetic resonance spectroscopy, Communications, 0104 chemical sciences, Membrane, Membrane protein, Solid-state nuclear magnetic resonance, ddc:540, Biophysics, solid-state NMR, lipids (amino acids, peptides, and proteins)

Abstract

Light‐induced activation of biomolecules by uncaging of photolabile protection groups has found many applications for triggering biochemical reactions with minimal perturbations directly within cells. Such an approach might also offer unique advantages for solid‐state NMR experiments on membrane proteins for initiating reactions within or at the membrane directly within the closed MAS rotor. Herein, we demonstrate that the integral membrane protein E. coli diacylglycerol kinase (DgkA), which catalyzes the phosphorylation of diacylglycerol, can be controlled by light under MAS‐NMR conditions. Uncaging of NPE‐ATP or of lipid substrate NPE‐DOG by in situ illumination triggers its enzymatic activity, which can be monitored by real‐time 31P‐MAS NMR. This proof‐of‐concept illustrates that combining MAS‐NMR with uncaging strategies and illumination methods offers new possibilities for controlling biochemical reactions at or within lipid bilayers., Engineering light control: Light‐induced release of caged substrates to initiate enzymatic activity of the membrane enzyme diacylglycerol kinase. A first demonstration of in situ light control for biomolecular solid‐state NMR, highlighting its potential advantages to initiate reactions in membrane systems (see figure).

Published

2020

7. Lipid cubic phase as a membrane mimetic for integral membrane protein enzymes.

Author

Li, Dianfan and Caffrey, Martin

Subjects

*MEMBRANE proteins, *ENZYMES, *CATALYSTS, *ENZYMOLOGY, *BIOMOLECULES

Abstract

The lipidic cubic mesophase has been used to crystallize important membrane proteins for high-resolution structure determination. To date, however, no integral membrane enzymes have yielded to this method, the in meso. For a crystal structure to be meaningful the target protein must be functional. Using the in meso method with a membrane enzyme requires that the protein is active in the mesophase that grows crystals. Because the cubic phase is sticky and viscous and is bicontinuous topologically, quantitatively assessing enzyme activity in meso is a challenge. Here, we describe a procedure for characterizing the catalytic properties of the integral membrane enzyme, diacylglycerol kinase, reconstituted into the bilayer of the lipidic cubic phase. The kinase activity of this elusive crystallographic target was monitored spectrophotometrically using a coupled assay in a high-throughput, 96-well plate format. In meso, the enzyme exhibits classic Michaelis-Menten kinetics and works with a range of lipid substrates. The fact that the enzyme and its lipid substrate and product remain confined to the porous mesophase while its water-soluble substrate and product are free to partition into the aqueous bathing solution suggests a general and convenient approach for characterizing membrane enzymes that function with lipids in a membrane-like environment. The distinctive rheology of the cubic phase means that a procedural step to physically separate substrate from product is not needed. Because of its open, bicontinuous nature, the cubic phase offers the added benefit that the protein is accessible for assay from both sides of the membrane. [ABSTRACT FROM AUTHOR]

Published

2011

8. Identification of ritanserin analogs that display DGK isoform specificity.

Author

Granade, Mitchell E., Manigat, Laryssa C., Lemke, Michael C., Purow, Benjamin W., and Harris, Thurl E.

Subjects

*SMALL molecules, *IMMUNE checkpoint proteins, *PHOSPHATIDIC acids, *T cells, *GLIOBLASTOMA multiforme, *CELL proliferation, *BRAF genes

Abstract

[Display omitted] The diacylglycerol kinase (DGK) family of lipid enzymes catalyzes the conversion of diacylglycerol (DAG) to phosphatidic acid (PA). Both DAG and PA are lipid signaling molecules that are of notable importance in regulating cell processes such as proliferation, apoptosis, and migration. There are ten mammalian DGK enzymes that appear to have distinct biological functions. DGKα has emerged as a promising therapeutic target in numerous cancers including glioblastoma (GBM) and melanoma as treatment with small molecule DGKα inhibitors results in reduced tumor sizes and prolonged survival. Importantly, DGKα has also been identified as an immune checkpoint due to its promotion of T cell anergy, and its inhibition has been shown to improve T cell activation. There are few small molecule DGKα inhibitors currently available, and the application of existing compounds to clinical settings is hindered by species-dependent variability in potency, as well as concerns regarding isotype specificity particularly amongst other type I DGKs. In order to resolve these issues, we have screened a library of compounds structurally analogous to the DGKα inhibitor, ritanserin, in an effort to identify more potent and specific alternatives. We identified two compounds that more potently and selectively inhibit DGKα, one of which (JNJ-3790339) demonstrates similar cytotoxicity in GBM and melanoma cells as ritanserin. Consistent with its inhibitor profile towards DGKα, JNJ-3790339 also demonstrated improved activation of T cells compared with ritanserin. Together our data support efforts to identify DGK isoform-selective inhibitors as a mechanism to produce pharmacologically relevant cancer therapies. [ABSTRACT FROM AUTHOR]

Published

2022

9. Diacylglycerol Kinase A Is Essential for Polymyxin Resistance Provided by EptA, MCR-1, and Other Lipid A Phosphoethanolamine Transferases.

Author

Purcell, Alexandria B., Voss, Bradley J., and Trent, M. Stephen

Abstract

Gram-negative bacteria utilize glycerophospholipids (GPLs) as phospho-form donors to modify various surface structures. These modifications play important roles in bacterial fitness in diverse environments influencing cell motility, recognition by the host during infection, and antimicrobial resistance. A well-known example is the modification of the lipid A component of lipopolysaccharide by the phosphoethanolamine (pEtN) transferase EptA that utilizes phosphatidyethanoalmine (PE) as the phospho-form donor. Addition of pEtN to lipid A promotes resistance to cationic antimicrobial peptides (CAMPs), including the polymyxin antibiotics like colistin. A consequence of pEtN modification is the production of diacylglycerol (DAG) that must be recycled back into GPL synthesis via the diacylglycerol kinase A (DgkA). DgkA phosphorylates DAG forming phosphatidic acid, the precursor for GPL synthesis. Here we report that deletion of dgkA in polymyxin-resistant E. coli results in a severe reduction of pEtN modification and loss of antibiotic resistance. We demonstrate that inhibition of EptA is regulated posttranscriptionally and is not due to EptA degradation during DAG accumulation. We also show that the inhibition of lipid A modification by DAG is a conserved feature of different Gram-negative pEtN transferases. Altogether, our data suggests that inhibition of EptA activity during DAG accumulation likely prevents disruption of GPL synthesis helping to maintain cell envelope homeostasis. [ABSTRACT FROM AUTHOR]

Published

2022

10. In meso in situ serial X-ray crystallography of soluble and membrane proteins at cryogenic temperatures

Author

Huang, Chiaying, Ma, Pikyee, Olieric, Vincent, Howe, Nicole, Vogeley, Lutz, Liu, Xiangyu, Warshamanage, Rangana, Weinert, Tobias, Panepucci, Ezequiel Horacio, Kobilka, Brian K., Diederichs, Kay, Wang, Meitian, Caffrey, Martin, Huang, Chiaying, Ma, Pikyee, Olieric, Vincent, Howe, Nicole, Vogeley, Lutz, Liu, Xiangyu, Warshamanage, Rangana, Weinert, Tobias, Panepucci, Ezequiel Horacio, Kobilka, Brian K., Diederichs, Kay, Wang, Meitian, and Caffrey, Martin

Abstract

Here, a method for presenting crystals of soluble and membrane proteins growing in the lipid cubic or sponge phase for in situ diffraction data collection at cryogenic temperatures is introduced. The method dispenses with the need for the technically demanding and inefficient crystal-harvesting step that is an integral part of the lipid cubic phase or in meso method of growing crystals. Crystals are dispersed in a bolus of mesophase sandwiched between thin plastic windows. The bolus contains tens to hundreds of crystals, visible with an in-line microscope at macromolecular crystallography synchrotron beamlines and suitably disposed for conventional or serial crystallographic data collection. Wells containing the crystal-laden boluses are removed individually from hermetically sealed glass plates in which crystallization occurs, affixed to pins on goniometer bases and excess precipitant is removed from around the mesophase. The wells are snap-cooled in liquid nitrogen, stored and shipped in Dewars, and manually or robotically mounted on a goniometer in a cryostream for diffraction data collection at 100 K, as is performed routinely with standard, loop-harvested crystals. The method is a variant on the recently introduced in meso in situ serial crystallography (IMISX) method that enables crystallographic measurements at cryogenic temperatures where crystal lifetimes are enormously enhanced whilst reducing protein consumption dramatically. The new approach has been used to generate high-resolution crystal structures of a G-protein-coupled receptor, α-helical and β-barrel transporters and an enzyme as model integral membrane proteins. Insulin and lysozyme were used as test soluble proteins. The quality of the data that can be generated by this method was attested to by performing sulfur and bromine SAD phasing with two of the test proteins., SCOPUS: ar.j, info:eu-repo/semantics/published

Published

2016

11. Light-Induced Uncaging for Time-Resolved Observations of Biochemical Reactions by MAS NMR Spectroscopy.

Author

de Mos J, Jakob A, Becker-Baldus J, Heckel A, and Glaubitz C

Subjects

Catalysis, Cell Physiological Phenomena, Diacylglycerol Kinase chemistry, Escherichia coli chemistry, Membrane Proteins chemistry, Nuclear Magnetic Resonance, Biomolecular methods, Phosphorylation, Diacylglycerol Kinase metabolism, Escherichia coli metabolism, Lipid Bilayers chemistry, Magnetic Resonance Spectroscopy methods, Membrane Proteins metabolism

Abstract

Light-induced activation of biomolecules by uncaging of photolabile protection groups has found many applications for triggering biochemical reactions with minimal perturbations directly within cells. Such an approach might also offer unique advantages for solid-state NMR experiments on membrane proteins for initiating reactions within or at the membrane directly within the closed MAS rotor. Herein, we demonstrate that the integral membrane protein E. coli diacylglycerol kinase (DgkA), which catalyzes the phosphorylation of diacylglycerol, can be controlled by light under MAS-NMR conditions. Uncaging of NPE-ATP or of lipid substrate NPE-DOG by in situ illumination triggers its enzymatic activity, which can be monitored by real-time 31 P-MAS NMR. This proof-of-concept illustrates that combining MAS-NMR with uncaging strategies and illumination methods offers new possibilities for controlling biochemical reactions at or within lipid bilayers., (© 2020 The Authors. Published by Wiley-VCH Verlag GmbH & Co. KGaA.)

Published

2020

12. In meso in situ serial X-ray crystallography of soluble and membrane proteins at cryogenic temperatures.

Author

Huang CY, Olieric V, Ma P, Howe N, Vogeley L, Liu X, Warshamanage R, Weinert T, Panepucci E, Kobilka B, Diederichs K, Wang M, and Caffrey M

Subjects

Animals, Bacteria chemistry, Bacterial Proteins chemistry, Chickens, Cold Temperature, Crystallization methods, Crystallography, X-Ray methods, Models, Molecular, Phase Transition, Solubility, Swine, Insulin chemistry, Membrane Proteins chemistry, Muramidase chemistry

Abstract

Here, a method for presenting crystals of soluble and membrane proteins growing in the lipid cubic or sponge phase for in situ diffraction data collection at cryogenic temperatures is introduced. The method dispenses with the need for the technically demanding and inefficient crystal-harvesting step that is an integral part of the lipid cubic phase or in meso method of growing crystals. Crystals are dispersed in a bolus of mesophase sandwiched between thin plastic windows. The bolus contains tens to hundreds of crystals, visible with an in-line microscope at macromolecular crystallography synchrotron beamlines and suitably disposed for conventional or serial crystallographic data collection. Wells containing the crystal-laden boluses are removed individually from hermetically sealed glass plates in which crystallization occurs, affixed to pins on goniometer bases and excess precipitant is removed from around the mesophase. The wells are snap-cooled in liquid nitrogen, stored and shipped in Dewars, and manually or robotically mounted on a goniometer in a cryostream for diffraction data collection at 100 K, as is performed routinely with standard, loop-harvested crystals. The method is a variant on the recently introduced in meso in situ serial crystallography (IMISX) method that enables crystallographic measurements at cryogenic temperatures where crystal lifetimes are enormously enhanced whilst reducing protein consumption dramatically. The new approach has been used to generate high-resolution crystal structures of a G-protein-coupled receptor, α-helical and β-barrel transporters and an enzyme as model integral membrane proteins. Insulin and lysozyme were used as test soluble proteins. The quality of the data that can be generated by this method was attested to by performing sulfur and bromine SAD phasing with two of the test proteins.

Published

2016

13. Host Lipid and Temperature as Important Screening Variables for Crystallizing Integral Membrane Proteins in Lipidic Mesophases. Trials with Diacylglycerol Kinase.

Author

Li D, Shah ST, and Caffrey M

Abstract

A systematic study of the crystallization of an α-helical, integral membrane enzyme, diacylglycerol kinase, DgkA, using the lipidic cubic mesophase or in meso method is described. These trials have resulted in the production of blocky, rhombohedron-shaped crystals of diffraction quality currently in use for structure determination. Dramatic improvements in crystal quality were obtained when the identity of the lipid used to form the mesophase bilayer into which the protein was reconstituted as a prelude to crystallogenesis was varied. These monoacylglycerol lipids incorporated fatty acyl chains ranging from 14 to 18 carbon atoms long with cis olefinic bonds located toward the middle of the chain. Best crystals were obtained with a lipid that had an acyl chain 15 carbon atoms long with the double bond between carbons 7 and 8. It is speculated that the effectiveness of this lipid derives from hydrophobic mismatch between the target integral membrane protein and the bilayer of the host mesophase. Low temperature (4 °C) worked in concert with the short chain lipid to provide high quality crystals. Recommended screening strategies for crystallizing membrane proteins that include host lipid type and low temperature are made on the basis of this and related in meso crystallization trials.

Published

2013