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140 results on '"McKenzie, Grahame"'

1. Target identification for small-molecule discovery in the FOXO3a tumor-suppressor pathway using a biodiverse peptide library

Author

Emery, Amy, Hardwick, Bryn S., Crooks, Alex T., Milech, Nadia, Watt, Paul M., Mithra, Chandan, Kumar, Vikrant, Giridharan, Saranya, Sadasivam, Gayathri, Mathivanan, Subashini, Sudhakar, Sneha, Bairy, Sneha, Bharatham, Kavitha, Hurakadli, Manjunath A., Prasad, Thazhe K., Kamariah, Neelagandan, Muellner, Markus, Coelho, Miguel, Torrance, Christopher J., McKenzie, Grahame J., and Venkitaraman, Ashok R.

Published
2021
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2. A small-molecule inhibitor of the BRCA2-RAD51 interaction modulates RAD51 assembly and potentiates DNA damage-induced cell death

Author

Scott, Duncan E., Francis-Newton, Nicola J., Marsh, May E., Coyne, Anthony G., Fischer, Gerhard, Moschetti, Tommaso, Bayly, Andrew R., Sharpe, Timothy D., Haas, Kalina T., Barber, Lorraine, Valenzano, Chiara R., Srinivasan, Rajavel, Huggins, David J., Lee, Miyoung, Emery, Amy, Hardwick, Bryn, Ehebauer, Matthias, Dagostin, Claudio, Esposito, Alessandro, Pellegrini, Luca, Perrior, Trevor, McKenzie, Grahame, Blundell, Tom L., Hyvönen, Marko, Skidmore, John, Venkitaraman, Ashok R., and Abell, Chris

Published
2021
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4. Selective Aurora A-TPX2 Interaction Inhibitors Have In VivoEfficacy as Targeted Antimitotic Agents

Author

Stockwell, Simon R., Scott, Duncan E., Fischer, Gerhard, Guarino, Estrella, Rooney, Timothy P. C., Feng, Tzu-Shean, Moschetti, Tommaso, Srinivasan, Rajavel, Alza, Esther, Asteian, Alice, Dagostin, Claudio, Alcaide, Anna, Rocaboy, Mathieu, Blaszczyk, Beata, Higueruelo, Alicia, Wang, Xuelu, Rossmann, Maxim, Perrior, Trevor R., Blundell, Tom L., Spring, David R., McKenzie, Grahame, Abell, Chris, Skidmore, John, Venkitaraman, Ashok R., and Hyvönen, Marko

Abstract

Aurora A kinase, a cell division regulator, is frequently overexpressed in various cancers, provoking genome instability and resistance to antimitotic chemotherapy. Localization and enzymatic activity of Aurora A are regulated by its interaction with the spindle assembly factor TPX2. We have used fragment-based, structure-guided lead discovery to develop small molecule inhibitors of the Aurora A-TPX2 protein–protein interaction (PPI). Our lead compound, CAM2602, inhibits Aurora A:TPX2 interaction, binding Aurora A with 19 nM affinity. CAM2602exhibits oral bioavailability, causes pharmacodynamic biomarker modulation, and arrests the growth of tumor xenografts. CAM2602acts by a novel mechanism compared to ATP-competitive inhibitors and is highly specific to Aurora A over Aurora B. Consistent with our finding that Aurora A overexpression drives taxane resistance, these inhibitors synergize with paclitaxel to suppress the outgrowth of pancreatic cancer cells. Our results provide a blueprint for targeting the Aurora A-TPX2 PPI for cancer therapy and suggest a promising clinical utility for this mode of action.

Published
2024
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8. Abstract 454: Validation of GPR35 as a novel cancer target in digestive tract cancers and discovery of potent, selective GPR35 inverse agonists

Author

Westcott, James, primary, Luckhurst, Christopher A., additional, McKenzie, Grahame, additional, Memon, Danish, additional, Lin, Li-Chiung, additional, Knight, Sinead, additional, Blaikley, Elizabeth J., additional, Pearce, Martin, additional, Warren, Hannah R., additional, Parker, Eleanor, additional, Milligan, Graeme, additional, Hughes, Stuart W., additional, and McCarthy, Tom, additional

Published
2023
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9. Selective inhibitors of the Aurora A-TPX2 protein-protein interaction exhibit in vivo efficacy as targeted anti-mitotic agents

Author

Stockwell, Simon R., primary, Scott, Duncan E., additional, Fischer, Gerhard, additional, Guarino, Estrella, additional, Rooney, Timothy P. C., additional, Fang, Tzu-Shean, additional, Moschetti, Tommaso, additional, Srinivasan, Rajavel, additional, Alza, Esther, additional, Asteian, Alice, additional, Dagostin, Claudio, additional, Alcaide, Anna, additional, Rocaboy, Mathieu, additional, Blaszczyk, Beata, additional, Higueruelo, Alicia, additional, Wang, Xuelu, additional, Rossmann, Maxim, additional, Perrior, Trevor R., additional, Blundell, Tom L, additional, Spring, David R., additional, McKenzie, Grahame, additional, Abell, Chris, additional, Skidmore, John, additional, Hyvönen, Marko, additional, and Venkitaraman, Ashok R., additional

Published
2023
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12. A small-molecule inhibitor of the BRCA2-RAD51 interaction modulates RAD51 assembly and potentiates DNA damage-induced cell death

Author

Scott, Duncan E., primary, Francis-Newton, Nicola J., additional, Marsh, May E., additional, Coyne, Anthony G., additional, Fischer, Gerhard, additional, Moschetti, Tommaso, additional, Bayly, Andrew R., additional, Sharpe, Timothy D., additional, Haas, Kalina T., additional, Barber, Lorraine, additional, Valenzano, Chiara R., additional, Srinivasan, Rajavel, additional, Huggins, David J., additional, Ehebauer, Matthias, additional, Esposito, Alessandro, additional, Pellegrini, Luca, additional, Perrior, Trevor, additional, McKenzie, Grahame, additional, Blundell, Tom L., additional, Hyvönen, Marko, additional, Skidmore, John, additional, Venkitaraman, Ashok R., additional, and Abell, Chris, additional

Published
2020
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13. Computationally-guided optimization of small-molecule inhibitors of the Aurora A kinase–TPX2 protein–protein interaction† †Electronic supplementary information (ESI) available: Computational methods and structure files, chemical synthesis, fluorescence polarization assays, crystallographic data. See DOI: 10.1039/c7cc05379g

Author

Cole, Daniel J., Janecek, Matej, Stokes, Jamie E., Rossmann, Maxim, Faver, John C., McKenzie, Grahame J., Venkitaraman, Ashok R., Hyvönen, Marko, Spring, David R., Huggins, David J., and Jorgensen, William L.

Subjects
Models, Molecular, Small Molecule Libraries, Chemistry, Molecular Structure, Humans, Nuclear Proteins, Cell Cycle Proteins, Molecular Dynamics Simulation, Microtubule-Associated Proteins, Protein Kinase Inhibitors, Aurora Kinase A, Protein Binding
Abstract

Computational binding free energy predictions were validated against experiment and used to design new inhibitors of an important protein–protein interaction., Free energy perturbation theory, in combination with enhanced sampling of protein–ligand binding modes, is evaluated in the context of fragment-based drug design, and used to design two new small-molecule inhibitors of the Aurora A kinase–TPX2 protein–protein interaction.

Published
2017

14. Development of a Novel Cell-Permeable Protein-Protein Interaction Inhibitor for the Polo-box Domain of Polo-like Kinase 1

Author

Huggins, David J, Hardwick, Bryn S, Sharma, Pooja, Emery, Amy, Laraia, Luca, Zhang, Fengzhi, Narvaez, Ana J, Roberts-Thomson, Meredith, Crooks, Alex T, Boyle, Robert G, Boyce, Richard, Walker, David W, Mateu, Natalia, McKenzie, Grahame J, Spring, David R, Venkitaraman, Ashok R, Huggins, David J [0000-0003-1579-2496], Apollo - University of Cambridge Repository, Huggins, David [0000-0003-1579-2496], and Spring, David [0000-0001-7355-2824]

Subjects
Orphan Drug, Rare Diseases, 34 Chemical Sciences, 5.1 Pharmaceuticals, 3404 Medicinal and Biomolecular Chemistry, 5 Development of treatments and therapeutic interventions, Cancer
Abstract

Polo-like kinase 1 (PLK1) is a key regulator of mitosis and a recognized drug target for cancer therapy. Inhibiting the polo-box domain of PLK1 offers potential advantages of increased selectivity and subsequently reduced toxicity compared with targeting the kinase domain. However, many if not all existing polo-box domain inhibitors have been shown to be unsuitable for further development. In this paper, we describe a novel compound series, which inhibits the protein-protein interactions of PLK1 via the polo-box domain. We combine high throughput screening with molecular modeling and computer-aided design, synthetic chemistry, and cell biology to address some of the common problems with protein-protein interaction inhibitors, such as solubility and potency. We use molecular modeling to improve the solubility of a hit series with initially poor physicochemical properties, enabling biophysical and biochemical characterization. We isolate and characterize enantiomers to improve potency and demonstrate on-target activity in both cell-free and cell-based assays, entirely consistent with the proposed binding model. The resulting compound series represents a promising starting point for further progression along the drug discovery pipeline and a new tool compound to study kinase-independent PLK functions.

Published
2019
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15. Development of a Novel Cell-Permeable Protein-Protein Interaction Inhibitor for the Polo-box Domain of Polo-like Kinase 1

Author

Huggins, David J., Hardwick, Bryn S., Sharma, Pooja, Emery, Amy, Laraia, Luca, Zhang, Fengzhi, Narvaez, Ana J., Roberts-Thomson, Meredith, Crooks, Alex T., Boyle, Robert G., Boyce, Richard, Walker, David W., Mateu, Natalia, McKenzie, Grahame J., Spring, David R., Venkitaraman, Ashok R., Huggins, David J., Hardwick, Bryn S., Sharma, Pooja, Emery, Amy, Laraia, Luca, Zhang, Fengzhi, Narvaez, Ana J., Roberts-Thomson, Meredith, Crooks, Alex T., Boyle, Robert G., Boyce, Richard, Walker, David W., Mateu, Natalia, McKenzie, Grahame J., Spring, David R., and Venkitaraman, Ashok R.

Abstract

Polo-like kinase 1 (PLK1) is a key regulator of mitosis and a recognized drug target for cancer therapy. Inhibiting the polo-box domain of PLK1 offers potential advantages of increased selectivity and subsequently reduced toxicity compared with targeting the kinase domain. However, many if not all existing polo-box domain inhibitors have been shown to be unsuitable for further development. In this paper, we describe a novel compound series, which inhibits the protein-protein interactions of PLK1 via the polo-box domain. We combine high throughput screening with molecular modeling and computer-aided design, synthetic chemistry, and cell biology to address some of the common problems with protein-protein interaction inhibitors, such as solubility and potency. We use molecular modeling to improve the solubility of a hit series with initially poor physicochemical properties, enabling biophysical and biochemical characterization. We isolate and characterize enantiomers to improve potency and demonstrate on-target activity in both cell-free and cell-based assays, entirely consistent with the proposed binding model. The resulting compound series represents a promising starting point for further progression along the drug discovery pipeline and a new tool compound to study kinase-independent PLK functions.

Published
2020

22. Development of a Novel Cell-Permeable Protein–Protein Interaction Inhibitor for the Polo-box Domain of Polo-like Kinase 1

Author

Huggins, David J., primary, Hardwick, Bryn S., additional, Sharma, Pooja, additional, Emery, Amy, additional, Laraia, Luca, additional, Zhang, Fengzhi, additional, Narvaez, Ana J., additional, Roberts-Thomson, Meredith, additional, Crooks, Alex T., additional, Boyle, Robert G., additional, Boyce, Richard, additional, Walker, David W., additional, Mateu, Natalia, additional, McKenzie, Grahame J., additional, Spring, David R., additional, and Venkitaraman, Ashok R., additional

Published
2019
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24. Cellular Notch responsiveness is defined by phosphoinositide 3-kinase-dependent signals

Author

Lennard Andrew, Papadia Sofia, Briend Emmanuel, Stallwood Yvette, Ward George, Mckenzie Grahame, Turner Martin, Champion Brian, and Hardingham Giles E

Subjects
Cytology, QH573-671
Abstract

Abstract Background Notch plays a wide-ranging role in controlling cell fate, differentiation and development. The PI3K-Akt pathway is a similarly conserved signalling pathway which regulates processes such as differentiation, proliferation and survival. Mice with disrupted Notch and PI3K signalling show phenotypic similarities during haematopoietic cell development, suggesting functional interaction between these pathways. Results We show that cellular responsiveness to Notch signals depends on the activity of the PI3K-Akt pathway in cells as diverse as CHO cells, primary T-cells and hippocampal neurons. Induction of the endogenous PI3K-Akt pathway in CHO cells (by the insulin pathway), in T-cells (via TCR activation) or in neurons (via TrKB activation) potentiates Notch-dependent responses. We propose that the PI3K-Akt pathway exerts its influence on Notch primarily via inhibition of GSK3-beta, a kinase known to phosphorylate and regulate Notch signals. Conclusion The PI3K-Akt pathway acts as a "gain control" for Notch signal responses. Since physiological levels of intracellular Notch are often low, coincidence with PI3K-activation may be crucial for induction of Notch-dependent responses.

Published
2006
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25. Computationally-guided optimization of small-molecule inhibitors of the Aurora A kinase-TPX2 protein-protein interaction

Author

Cole, Daniel J, Janecek, Matej, Stokes, Jamie E, Rossmann, Maxim, Faver, John C, McKenzie, Grahame J, Venkitaraman, Ashok R, Hyvönen, Marko, Spring, David R, Huggins, David J, Jorgensen, William L, Cole, Daniel J [0000-0003-2933-0719], Janecek, Matej [0000-0003-0740-641X], Rossmann, Maxim [0000-0001-8811-3277], Venkitaraman, Ashok R [0000-0002-6876-2672], Hyvönen, Marko [0000-0001-8683-4070], Spring, David R [0000-0001-7355-2824], Huggins, David J [0000-0003-1579-2496], Jorgensen, William L [0000-0002-3993-9520], and Apollo - University of Cambridge Repository

Subjects
Models, Molecular, Small Molecule Libraries, Molecular Structure, Humans, Nuclear Proteins, Cell Cycle Proteins, Molecular Dynamics Simulation, Microtubule-Associated Proteins, Protein Kinase Inhibitors, Aurora Kinase A, Protein Binding
Abstract

Free energy perturbation theory, in combination with enhanced sampling of protein-ligand binding modes, is evaluated in the context of fragment-based drug design, and used to design two new small-molecule inhibitors of the Aurora A kinase-TPX2 protein-protein interaction.

Published
2017

26. Interrogation of the protein-protein interactions between human BRCA2 BRC repeats and RAD51 reveals atomistic determinants of affinity

Author

Kowalczykowski, Stephen Charles, Cole, Daniel J., Rajendra, Eason, Roberts-Thomson, Meredith, Hardwick, Bryn, McKenzie, Grahame J., Payne, Mike C., Venkitaraman, Ashok R., Skylaris, Chris-Kriton, Payne, Michael [0000-0002-5250-8549], and Apollo - University of Cambridge Repository

Subjects
Models, Molecular, Amino Acid Motifs, Plasma protein binding, Molecular Dynamics, medicine.disease_cause, Biochemistry, Biophysics Simulations, 01 natural sciences, chemistry.chemical_compound, Computational Chemistry, Fluorescence Polarization Immunoassay, Protein Interaction Mapping, Recombinase, Biology (General), Biomacromolecule-Ligand Interactions, Peptide sequence, Density Functional Theory, Genetics, 0303 health sciences, Mutation, Ecology, Protein Stability, Physics, Chemistry, Computational Theory and Mathematics, Modeling and Simulation, Interdisciplinary Physics, Thermodynamics, Research Article, Protein Binding, Repetitive Sequences, Amino Acid, QH301-705.5, Molecular Sequence Data, Biophysics, Chemical biology, Sequence alignment, Biology, 010402 general chemistry, Protein–protein interaction, 03 medical and health sciences, Cellular and Molecular Neuroscience, medicine, Humans, Protein Interaction Domains and Motifs, Amino Acid Sequence, Protein Interactions, Molecular Biology, Ecology, Evolution, Behavior and Systematics, Quantum Mechanics, 030304 developmental biology, BRCA2 Protein, Proteins, 0104 chemical sciences, chemistry, Rad51 Recombinase, Sequence Alignment, DNA
Abstract

The breast cancer suppressor BRCA2 controls the recombinase RAD51 in the reactions that mediate homologous DNA recombination, an essential cellular process required for the error-free repair of DNA double-stranded breaks. The primary mode of interaction between BRCA2 and RAD51 is through the BRC repeats, which are ∼35 residue peptide motifs that interact directly with RAD51 in vitro. Human BRCA2, like its mammalian orthologues, contains 8 BRC repeats whose sequence and spacing are evolutionarily conserved. Despite their sequence conservation, there is evidence that the different human BRC repeats have distinct capacities to bind RAD51. A previously published crystal structure reports the structural basis of the interaction between human BRC4 and the catalytic core domain of RAD51. However, no structural information is available regarding the binding of the remaining seven BRC repeats to RAD51, nor is it known why the BRC repeats show marked variation in binding affinity to RAD51 despite only subtle sequence variation. To address these issues, we have performed fluorescence polarisation assays to indirectly measure relative binding affinity, and applied computational simulations to interrogate the behaviour of the eight human BRC-RAD51 complexes, as well as a suite of BRC cancer-associated mutations. Our computational approaches encompass a range of techniques designed to link sequence variation with binding free energy. They include MM-PBSA and thermodynamic integration, which are based on classical force fields, and a recently developed approach to computing binding free energies from large-scale quantum mechanical first principles calculations with the linear-scaling density functional code onetep. Our findings not only reveal how sequence variation in the BRC repeats directly affects affinity with RAD51 and provide significant new insights into the control of RAD51 by human BRCA2, but also exemplify a palette of computational and experimental tools for the analysis of protein-protein interactions for chemical biology and molecular therapeutics., Author Summary The atomic scale interactions that occur at the interfaces between proteins are fundamental to all biological processes. One such critical interface is formed between the proteins, human BRCA2 and RAD51. BRCA2 binds to and delivers RAD51 to sites of DNA damage, where RAD51 mediates the error-free repair of double-stranded DNA breaks. Mutations in BRCA2 have been linked to breast cancer predisposition. Therefore, an accurate picture of the interactions between these two proteins is of great importance. BRCA2 interacts with RAD51 via eight “BRC repeats” that are similar, but not identical, in sequence. Due to lack of experimental structural information regarding the binding of seven of the eight BRC repeats to RAD51, it is unknown how subtle sequence variations in the repeats translate to measurable variations in their binding affinity. We have used a range of computational methods, firstly based on classical force fields, and secondly based on first principles quantum mechanical techniques whose computational cost scales linearly with the number of atoms, allowing us to perform calculations on the entire protein complex. This is the first study comparing all eight BRC repeats at the atomic scale and our results provide critical insights into the control of RAD51 by human BRCA2.

Published
2017
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27. Allosteric modulation of AURKA kinase activity by a small-molecule inhibitor of its protein-protein interaction with TPX2

Author

Janeček, Matej, Rossmann, Maxim, Sharma, Pooja, Emery, Amy, Huggins, David J, Stockwell, Simon R, Stokes, Jamie E, Tan, Yaw S, Almeida, Estrella Guarino, Hardwick, Bryn, Narvaez, Ana J, Hyvönen, Marko, Spring, David R, McKenzie, Grahame J, Venkitaraman, Ashok R, Rossmann, Maxim [0000-0001-8811-3277], Huggins, David [0000-0003-1579-2496], Stockwell, Simon [0000-0002-3345-8945], Spring, David [0000-0001-7355-2824], and Apollo - University of Cambridge Repository

Subjects
Mitosis, Nuclear Proteins, Cell Cycle Proteins, Spindle Apparatus, Phosphoproteins, Neoplasm Proteins, Small Molecule Libraries, Cell Line, Tumor, Humans, Protein Interaction Maps, Microtubule-Associated Proteins, Protein Kinases, Aurora Kinase A, HeLa Cells, Protein Binding
Abstract

The essential mitotic kinase Aurora A (AURKA) is controlled during cell cycle progression via two distinct mechanisms. Following activation loop autophosphorylation early in mitosis when it localizes to centrosomes, AURKA is allosterically activated on the mitotic spindle via binding to the microtubule-associated protein, TPX2. Here, we report the discovery of AurkinA, a novel chemical inhibitor of the AURKA-TPX2 interaction, which acts via an unexpected structural mechanism to inhibit AURKA activity and mitotic localization. In crystal structures, AurkinA binds to a hydrophobic pocket (the 'Y pocket') that normally accommodates a conserved Tyr-Ser-Tyr motif from TPX2, blocking the AURKA-TPX2 interaction. AurkinA binding to the Y- pocket induces structural changes in AURKA that inhibit catalytic activity in vitro and in cells, without affecting ATP binding to the active site, defining a novel mechanism of allosteric inhibition. Consistent with this mechanism, cells exposed to AurkinA mislocalise AURKA from mitotic spindle microtubules. Thus, our findings provide fresh insight into the catalytic mechanism of AURKA, and identify a key structural feature as the target for a new class of dual-mode AURKA inhibitors, with implications for the chemical biology and selective therapeutic targeting of structurally related kinases.

Published
2016

28. Modulating Protein-Protein Interactions of the Mitotic Polo-like Kinases to Target Mutant KRAS

Author

Narvaez, Ana J., primary, Ber, Suzan, additional, Crooks, Alex, additional, Emery, Amy, additional, Hardwick, Bryn, additional, Guarino Almeida, Estrella, additional, Huggins, David J., additional, Perera, David, additional, Roberts-Thomson, Meredith, additional, Azzarelli, Roberta, additional, Hood, Fiona E., additional, Prior, Ian A., additional, Walker, David W., additional, Boyce, Richard, additional, Boyle, Robert G., additional, Barker, Samuel P., additional, Torrance, Christopher J., additional, McKenzie, Grahame J., additional, and Venkitaraman, Ashok R., additional

Published
2017
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29. Allosteric modulation of AURKA kinase activity by a small-molecule inhibitor of its protein-protein interaction with TPX2

Author

Janeček, Matej, primary, Rossmann, Maxim, additional, Sharma, Pooja, additional, Emery, Amy, additional, Huggins, David J., additional, Stockwell, Simon R., additional, Stokes, Jamie E., additional, Tan, Yaw S., additional, Almeida, Estrella Guarino, additional, Hardwick, Bryn, additional, Narvaez, Ana J., additional, Hyvönen, Marko, additional, Spring, David R., additional, McKenzie, Grahame J., additional, and Venkitaraman, Ashok R., additional

Published
2016
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39. Synaptic NMDA receptor activity boosts intrinsic antioxidant defenses

Author

Papadia, Sofia, primary, Soriano, Francesc X, additional, Léveillé, Frédéric, additional, Martel, Marc-Andre, additional, Dakin, Kelly A, additional, Hansen, Henrik H, additional, Kaindl, Angela, additional, Sifringer, Marco, additional, Fowler, Jill, additional, Stefovska, Vanya, additional, Mckenzie, Grahame, additional, Craigon, Marie, additional, Corriveau, Roderick, additional, Ghazal, Peter, additional, Horsburgh, Karen, additional, Yankner, Bruce A, additional, Wyllie, David J A, additional, Ikonomidou, Chrysanthy, additional, and Hardingham, Giles E, additional

Published
2008
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47. Impaired Development of Th2 Cells in IL-13-Deficient Mice

Author

McKenzie, Grahame J, primary, Emson, Claire L, additional, Bell, Sarah E, additional, Anderson, Shannon, additional, Fallon, Padraic, additional, Zurawski, Gerard, additional, Murray, Richard, additional, Grencis, Richard, additional, and McKenzie, Andrew N.J, additional

Published
1998
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49. Nuclear Ca2+ and CaM kinase IV specify hormonal- and Notch-responsiveness.

Author

Mckenzie, Grahame J., Stevenson, Patrick, Ward, George, Papadia, Sofia, Bading, Hilmar, Chawla, Sangeeta, Privalsky, Martin, and Hardingham, Giles E.

Subjects
*PROTEIN kinases, *NEURONS, *CALCIUM, *MITOGENS, *TRANSCRIPTION factors, *HISTONE deacetylase, *NEUROCHEMISTRY
Abstract

Many neuronal processes require gene activation by synaptically evoked Ca2+ transients. Ca2+-dependent signal pathways activate some transcription factors outright, but here we report that such signals also potentiate the activation of nuclear receptors by their cognate hormone, and of CBF1 by Notch, transcription factors hitherto not thought to be Ca2+-responsive. This potentiation is occluded by histone deacetylase inhibition, indicating a mechanism involving inactivation of co-repressors associated with these transcription factors. Synaptic activity, acting via the nuclear Ca2+-dependent activation of CaM kinase IV, triggers the disruption of subnuclear domains containing class II histone deacetylases (HDACs) and silencing mediator of retinoic acid and thyroid hormone receptors (SMRT), a broad-specificity co-repressor which represses nuclear hormone receptors and CBF1. The sequential loss of class II HDACs and SMRT from the subnuclear domains, followed by nuclear export, is associated with disruption of SMRT interaction with its target transcription factors and sensitization of these factors to their activating signal. Counterbalancing these changes, protein phosphatase 1 promotes nuclear localization of SMRT and inactivation of nuclear receptors and CBF1. Thus, the synaptically controlled kinase-phosphatase balance of the neuron determines the efficacy of SMRT-mediated repression and the signal-responsiveness of a variety of transcription factors. [ABSTRACT FROM AUTHOR]

Published
2005
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50. A cryptic hydrophobic pocket in the polo-box domain of the polo-like kinase PLK1 regulates substrate recognition and mitotic chromosome segregation

Author

Sharma, Pooja, Mahen, Robert, Rossmann, Maxim, Stokes, Jamie E, Hardwick, Bryn, Huggins, David J, Emery, Amy, Kunciw, Dominique L, Hyvönen, Marko, Spring, David R, McKenzie, Grahame J, and Venkitaraman, Ashok R

Subjects
Cell Survival, Mitosis, Cell Cycle Proteins, Protein Serine-Threonine Kinases, 3. Good health, Protein Structure, Tertiary, Substrate Specificity, Histones, Protein Domains, Mutagenesis, Chromosome Segregation, Proto-Oncogene Proteins, Humans, RNA Interference, RNA, Small Interfering, Kinetochores, 3' Untranslated Regions, Protein Kinase Inhibitors, HeLa Cells, Protein Binding
Abstract

The human polo-like kinase PLK1 coordinates mitotic chromosome segregation by phosphorylating multiple chromatin- and kinetochore-binding proteins. How PLK1 activity is directed to specific substrates via phosphopeptide recognition by its carboxyl-terminal polo-box domain (PBD) is poorly understood. Here, we combine molecular, structural and chemical biology to identify a determinant for PLK1 substrate recognition that is essential for proper chromosome segregation. We show that mutations ablating an evolutionarily conserved, Tyr-lined pocket in human PLK1 PBD trigger cellular anomalies in mitotic progression and timing. Tyr pocket mutations selectively impair PLK1 binding to the kinetochore phosphoprotein substrate PBIP1, but not to the centrosomal substrate NEDD1. Through a structure-guided approach, we develop a small-molecule inhibitor, Polotyrin, which occupies the Tyr pocket. Polotyrin recapitulates the mitotic defects caused by mutations in the Tyr pocket, further evidencing its essential function, and exemplifying a new approach for selective PLK1 inhibition. Thus, our findings support a model wherein substrate discrimination via the Tyr pocket in the human PLK1 PBD regulates mitotic chromosome segregation to preserve genome integrity.

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