Your search keyword '"protein kinase CK1"' showing total 19 results

1. Targeting Protein Kinases in Blood Cancer: Focusing on CK1α and CK2

Author

Zaira Spinello, Anna Fregnani, Laura Quotti Tubi, Livio Trentin, Francesco Piazza, and Sabrina Manni

Subjects

protein kinase CK1, protein kinase CK2, blood tumors, survival/stress signaling, non-oncogene addiction, Biology (General), QH301-705.5, Chemistry, QD1-999

Abstract

Disturbance of protein kinase activity may result in dramatic consequences that often lead to cancer development and progression. In tumors of blood origin, both tyrosine kinases and serine/threonine kinases are altered by different types of mutations, critically regulating cancer hallmarks. CK1α and CK2 are highly conserved, ubiquitously expressed and constitutively active pleiotropic kinases, which participate in multiple biological processes. The involvement of these kinases in solid and blood cancers is well documented. CK1α and CK2 are overactive in multiple myeloma, leukemias and lymphomas. Intriguingly, they are not required to the same degree for the viability of normal cells, corroborating the idea of “druggable” kinases. Different to other kinases, mutations on the gene encoding CK1α and CK2 are rare or not reported. Actually, these two kinases are outside the paradigm of oncogene addiction, since cancer cells’ dependency on these proteins resembles the phenomenon of “non-oncogene” addiction. In this review, we will summarize the general features of CK1α and CK2 and the most relevant oncogenic and stress-related signaling nodes, regulated by kinase phosphorylation, that may lead to tumor progression. Finally, we will report the current data, which support the positioning of these two kinases in the therapeutic scene of hematological cancers.

Published

2021

2. Design, Synthesis and Biological Evaluation of Isoxazole-Based CK1 Inhibitors Modified with Chiral Pyrrolidine Scaffolds

Author

Andreas Luxenburger, Dorian Schmidt, Chiara Ianes, Christian Pichlo, Marc Krüger, Thorsten von Drathen, Elena Brunstein, Graeme J. Gainsford, Ulrich Baumann, Uwe Knippschild, and Christian Peifer

Subjects

protein kinase CK1, formerly known as casein kinase 1, chiral kinase inhibitors, iminoribitol, ribose pocket, 3,4-diaryl-isoxazole, Pictet-Spengler cyclization, Organic chemistry, QD241-441

Abstract

In this study, we report on the modification of a 3,4-diaryl-isoxazole-based CK1 inhibitor with chiral pyrrolidine scaffolds to develop potent and selective CK1 inhibitors. The pharmacophore of the lead structure was extended towards the ribose pocket of the adenosine triphosphate (ATP) binding site driven by structure-based drug design. For an upscale compatible multigram synthesis of the functionalized pyrrolidine scaffolds, we used a chiral pool synthetic route starting from methionine. Biological evaluation of key compounds in kinase and cellular assays revealed significant effects of the scaffolds towards activity and selectivity, however, the absolute configuration of the chiral moieties only exhibited a limited effect on inhibitory activity. X-ray crystallographic analysis of ligand-CK1δ complexes confirmed the expected binding mode of the 3,4-diaryl-isoxazole inhibitors. Surprisingly, the original compounds underwent spontaneous Pictet-Spengler cyclization with traces of formaldehyde during the co-crystallization process to form highly potent new ligands. Our data suggests chiral “ribose-like” pyrrolidine scaffolds have interesting potential for modifications of pharmacologically active compounds.

Published

2019

3. Optimized 4,5-Diarylimidazoles as Potent/Selective Inhibitors of Protein Kinase CK1δ and Their Structural Relation to p38α MAPK.

Author

Halekotte, Jakob, Witt, Lydia, Ianes, Chiara, Krüger, Marc, Bührmann, Mike, Rauh, Daniel, Pichlo, Christian, Brunstein, Elena, Luxenburger, Andreas, Baumann, Ulrich, Knippschild, Uwe, Bischof, Joachim, and Peifer, Christian

Subjects

*PROTEIN kinases, *IMIDAZOLES, *MITOGEN-activated protein kinases, *KINASE inhibitors, *ALZHEIMER'S disease, *AMYOTROPHIC lateral sclerosis, *SLEEP disorders, *CANCER

Abstract

The involvement of protein kinase CK1δ in the pathogenesis of severe disorders such as Alzheimer's disease, amyotrophic lateral sclerosis, familial advanced sleep phase syndrome, and cancer has dramatically increased interest in the development of effective small molecule inhibitors for both therapeutic application and basic research. Unfortunately, the design of CK1 isoform-specific compounds has proved to be highly complicated due to the existence of six evolutionarily conserved human CK1 members that possess similar, differenţ or even opposite physiological and pathophysiological implications. Consequently, only few potent and selective CK1δ inhibitors have been reported so far and structurally divergent approaches are urgently needed in order to establish SAR that might enable complete discrimination of CK1 isoforms and related p38α MAPK. In this study we report on design and characterization of optimized 4,5-diarylimidazoles as highly effective ATP-competitive inhibitors of CK1δ with compounds 11b (IC50 CK1δ = 4 nM, IC50 CK1ε = 25 nM), 12a (IC50 CK1δ = 19 nM, IC50 CK1ε = 227 nM), and 16b (IC50 CK1δ = 8 nM, IC50 CK1ε = 81 nM) being among the most potent CK1δ-targeting agents published to date. Inhibitor compound 11b, displaying potential as a pharmacological tool, has further been profiled over a panel of 321 protein kinases exhibiting high selectivity. Cellular efficacy has been evaluated in human pancreatic cancer cell lines Colo357 (EC50 = 3.5 μM) and Panc89 (EC50 = 1.5 μM). SAR is substantiated by X-ray crystallographic analysis of 16b in CK1δ and 11b in p38α. [ABSTRACT FROM AUTHOR]

Published

2017

4. Targeting Protein Kinases in Blood Cancer: Focusing on CK1α and CK2

Author

Livio Trentin, Laura Quotti Tubi, Zaira Spinello, Francesco Piazza, Anna Fregnani, and Sabrina Manni

Subjects

0301 basic medicine, Physiological, survival/stress signaling, Review, Biology, Stress, therapeutic targets, Catalysis, Inorganic Chemistry, lcsh:Chemistry, Blood tumors, Non-oncogene addiction, Protein kinase CK1, Protein kinase CK2, Survival/stress signaling, Animals, Casein Kinase II, Casein Kinase Ialpha, Hematologic Neoplasms, Humans, Molecular Targeted Therapy, Stress, Physiological, 03 medical and health sciences, 0302 clinical medicine, medicine, Physical and Theoretical Chemistry, Protein kinase A, Molecular Biology, lcsh:QH301-705.5, CK1 and CK2 kinases, Spectroscopy, non-oncogene addiction, Kinase, Organic Chemistry, Cancer, General Medicine, medicine.disease, Oncogene Addiction, Computer Science Applications, 030104 developmental biology, lcsh:Biology (General), lcsh:QD1-999, Tumor progression, 030220 oncology & carcinogenesis, blood tumors, Cancer cell, protein kinase CK2, Cancer research, protein kinase CK1, Phosphorylation, CK1 and CK2 kinases, blood tumors, therapeutic targets, Tyrosine kinase

Abstract

Disturbance of protein kinase activity may result in dramatic consequences that often lead to cancer development and progression. In tumors of blood origin, both tyrosine kinases and serine/threonine kinases are altered by different types of mutations, critically regulating cancer hallmarks. CK1α and CK2 are highly conserved, ubiquitously expressed and constitutively active pleiotropic kinases, which participate in multiple biological processes. The involvement of these kinases in solid and blood cancers is well documented. CK1α and CK2 are overactive in multiple myeloma, leukemias and lymphomas. Intriguingly, they are not required to the same degree for the viability of normal cells, corroborating the idea of “druggable” kinases. Different to other kinases, mutations on the gene encoding CK1α and CK2 are rare or not reported. Actually, these two kinases are outside the paradigm of oncogene addiction, since cancer cells’ dependency on these proteins resembles the phenomenon of “non-oncogene” addiction. In this review, we will summarize the general features of CK1α and CK2 and the most relevant oncogenic and stress-related signaling nodes, regulated by kinase phosphorylation, that may lead to tumor progression. Finally, we will report the current data, which support the positioning of these two kinases in the therapeutic scene of hematological cancers.

Published

2021

5. Pyrvinium pamoate does not activate protein kinase CK1, but promotes Akt/PKB down-regulation and GSK3 activation.

Author

VENERANDO, Andrea, GIRARDI, Cristina, RUZZENE, Maria, and PINNA, Lorenzo A.

Subjects

*ANTHELMINTICS, *WNT proteins, *GLYCOGEN synthase kinase-3, *PHOSPHORYLATION kinetics, *CATENINS

Abstract

It has been reported that pyrvinium pamoate (PyrPam), an FDA (U.S. Food and Drug Administration)-approved anthelminthic drug, is a potent inhibitor of Wnt signalling by a mechanism which implies the direct activation of protein kinase CK1α. In the present paper, we provide data ruling out any direct stimulatory effect of PyrPam on CK1, by showing that the catalytic activity of CK1α and those of its isoforms d and ? 1 are not significantly affected by PyrPam when tested with the aid of specific peptide and protein substrates. Accordingly, cell treatment with PyrPam has no significant effect on the phosphorylation of β-catenin Ser45. By contrast, the phosphorylation of β-catenin Thr41 is increased upon cell treatment with PyrPam, through a mechanism that implies the upstream dephosphorylation of Akt/PKB (protein kinase B) and of GSK3 (glycogen synthase kinase 3). It can be concluded from the present study that PyrPam is not a bona fide activator of CK1, its perturbation of cell signalling pathways being mediated by a complex mechanism initiated by a fall in Akt phosphorylation whose down-regulation promotes reduced phosphorylation and activation of GSK3. Consistent with this, lysates of cells treated with PyrPam display enhanced protein phosphorylation which is unaffected by CK1 inhibition, while disappearing upon inhibition of GSK3. Our data are consistent with the observation that PyrPam ultimately inhibits Wnt signalling despite its lack of efficacy on CK1. [ABSTRACT FROM AUTHOR]

Published

2013

6. Multiple phosphorylation sites at the C-terminus regulate nuclear import of HCMV DNA polymerase processivity factor ppUL44

Author

Alvisi, Gualtiero, Marin, Oriano, Pari, Gregory, Mancini, Manuela, Avanzi, Simone, Loregian, Arianna, Jans, David A., and Ripalti, Alessandro

Subjects

*CYTOMEGALOVIRUSES, *DNA polymerases, *PHOSPHORYLATION, *VIRUS diseases, *PHOSPHOPROTEINS, *VIRAL replication, *VIRUS-induced enzymes, *PROTEIN kinases

Abstract

Abstract: The processivity factor of human cytomegalovirus DNA polymerase, phosphoprotein ppUL44, is essential for viral replication. During viral infection ppUL44 is phosphorylated by the viral kinase pUL97, but neither the target residues on ppUL44 nor the effect of phosphorylation on ppUL44''s activity are known. We report here that ppUL44 is phosphorylated when transiently expressed in mammalian cells and coimmunoprecipitates with cellular kinases. Of three potential phosphorylation sites (S413, S415, S418) located upstream of ppUL44''s nuclear localization signal (NLS) and one (T427) within the NLS itself, protein kinase CK2 (CK2) specifically phosphorylates S413, to trigger a cascade of phosphorylation of S418 and S415 by CK1 and CK2, respectively. Negative charge at the CK2/CK1 target serine residues facilitates optimal nuclear accumulation of ppUL44, whereas negative charge on T427, a potential cyclin-dependent 1 phosphorylation site, strongly decreases nuclear accumulation. Thus, nuclear transport of ppUL44 is finely tuned during viral infection through complex phosphorylation events. [Copyright &y& Elsevier]

Published

2011

7. Regulation of protein kinase CK1αLS by dephosphorylation in response to hydrogen peroxide

Author

Bedri, Shahinaz, Cizek, Stephanie M., Rastarhuyeva, Iryna, and Stone, James R.

Subjects

*PROTEIN kinases, *DISINFECTION & disinfectants, *HYDROGEN peroxide, *MILK proteins

Abstract

Abstract: Low levels of hydrogen peroxide (H2O2) are mitogenic to mammalian cells and stimulate the hyperphosphorylation of heterogeneous nuclear ribonucleoprotein C (hnRNP-C) by protein kinase CK1α. However, the mechanisms by which CK1α is regulated have been unclear. Here it is demonstrated that low levels of H2O2 stimulate the rapid dephosphorylation of CK1αLS, a nuclear splice form of CK1α. Furthermore, it is demonstrated that either treatment of endothelial cells with H2O2, or dephosphorylation of CK1αLS in vitro enhances the association of CK1αLS with hnRNP-C. In addition, dephosphorylation of CK1αLS in vitro enhances the kinase’s ability to phosphorylate hnRNP-C. While CK1α appears to be present in all metazoans, analysis of CK1α genomic sequences from several species reveals that the alternatively spliced nuclear localizing L-insert is unique to vertebrates, as is the case for hnRNP-C. These observations indicate that CK1αLS and hnRNP-C represent conserved components of a vertebrate-specific H2O2-responsive nuclear signaling pathway. [Copyright &y& Elsevier]

Published

2007

8. Design, Synthesis and Biological Evaluation of Isoxazole-Based CK1 Inhibitors Modified with Chiral Pyrrolidine Scaffolds

Author

Ulrich Baumann, Marc Krüger, Graeme J. Gainsford, Thorsten von Drathen, Christian Pichlo, Christian Peifer, Dorian Schmidt, Chiara Ianes, Elena Brunstein, Uwe Knippschild, and Andreas Luxenburger

Subjects

Pyrrolidines, Pictet-Spengler cyclization, Pharmaceutical Science, Protein Kinase Ck1, Crystallography, X-Ray, Ligands, 01 natural sciences, Pyrrolidine, Analytical Chemistry, chemistry.chemical_compound, Adenosine Triphosphate, iminoribitol, Drug Discovery, Isoxazole, Enzyme Inhibitors, 0303 health sciences, Absolute configuration, article, ribose pocket, 3,4-Diaryl-isoxazole, 3. Good health, Chemistry (miscellaneous), Casein Kinase Idelta, ddc:540, Molecular Medicine, Iminoribitol, Pharmacophore, Selectivity, 3,4-diaryl-isoxazole, Article, lcsh:QD241-441, 03 medical and health sciences, Structure-Activity Relationship, lcsh:Organic chemistry, Formerly Known As Casein Kinase 1, Ribose Pocket, Ribose, Humans, Physical and Theoretical Chemistry, Binding site, 030304 developmental biology, ddc:5, Binding Sites, 010405 organic chemistry, Organic Chemistry, chiral kinase inhibitors, Isoxazoles, formerly known as casein kinase 1, Combinatorial chemistry, Chiral Kinase Inhibitors, 0104 chemical sciences, chemistry, Drug Design, Multiprotein Complexes, protein kinase CK1, Pictet-spengler Cyclization, Adenosine triphosphate

Abstract

In this study, we report on the modification of a 3,4-diaryl-isoxazole-based CK1 inhibitor with chiral pyrrolidine scaffolds to develop potent and selective CK1 inhibitors. The pharmacophore of the lead structure was extended towards the ribose pocket of the adenosine triphosphate (ATP) binding site driven by structure-based drug design. For an upscale compatible multigram synthesis of the functionalized pyrrolidine scaffolds, we used a chiral pool synthetic route starting from methionine. Biological evaluation of key compounds in kinase and cellular assays revealed significant effects of the scaffolds towards activity and selectivity, however, the absolute configuration of the chiral moieties only exhibited a limited effect on inhibitory activity. X-ray crystallographic analysis of ligand-CK1&delta, complexes confirmed the expected binding mode of the 3,4-diaryl-isoxazole inhibitors. Surprisingly, the original compounds underwent spontaneous Pictet-Spengler cyclization with traces of formaldehyde during the co-crystallization process to form highly potent new ligands. Our data suggests chiral &ldquo, ribose-like&rdquo, pyrrolidine scaffolds have interesting potential for modifications of pharmacologically active compounds.

Published

2018

9. Targeting Protein Kinases in Blood Cancer: Focusing on CK1α and CK2.

Author

Spinello, Zaira, Fregnani, Anna, Quotti Tubi, Laura, Trentin, Livio, Piazza, Francesco, Manni, Sabrina, and Cipak, Lubos

Subjects

*PROTEIN kinases, *SERINE/THREONINE kinases, *BLOOD proteins, *PROTEIN kinase CK2, *KINASES, *HEMATOMA

Abstract

Disturbance of protein kinase activity may result in dramatic consequences that often lead to cancer development and progression. In tumors of blood origin, both tyrosine kinases and serine/threonine kinases are altered by different types of mutations, critically regulating cancer hallmarks. CK1α and CK2 are highly conserved, ubiquitously expressed and constitutively active pleiotropic kinases, which participate in multiple biological processes. The involvement of these kinases in solid and blood cancers is well documented. CK1α and CK2 are overactive in multiple myeloma, leukemias and lymphomas. Intriguingly, they are not required to the same degree for the viability of normal cells, corroborating the idea of "druggable" kinases. Different to other kinases, mutations on the gene encoding CK1α and CK2 are rare or not reported. Actually, these two kinases are outside the paradigm of oncogene addiction, since cancer cells' dependency on these proteins resembles the phenomenon of "non-oncogene" addiction. In this review, we will summarize the general features of CK1α and CK2 and the most relevant oncogenic and stress-related signaling nodes, regulated by kinase phosphorylation, that may lead to tumor progression. Finally, we will report the current data, which support the positioning of these two kinases in the therapeutic scene of hematological cancers. [ABSTRACT FROM AUTHOR]

Published

2021

10. Optimized 4,5-Diarylimidazoles as Potent/Selective Inhibitors of Protein Kinase CK1δ and Their Structural Relation to p38α MAPK

Author

Daniel Rauh, Christian Peifer, Joachim Bischof, Mike Bührmann, Christian Pichlo, Andreas Luxenburger, Marc Krüger, Ulrich Baumann, Chiara Ianes, Jakob Halekotte, Lydia Witt, Uwe Knippschild, and Elena Brunstein

Subjects

0301 basic medicine, Models, Molecular, amyotrophic lateral sclerosis, Pharmaceutical Science, Crystallography, X-Ray, Analytical Chemistry, Pathogenesis, Mitogen-Activated Protein Kinase 14, 0302 clinical medicine, Adenosine Triphosphate, 4,5-diaryl-imidazoles, Drug Discovery, kinase inhibitors, Phylogeny, Kinase, Imidazoles, Alzheimer's disease, Small molecule, Biochemistry, Chemistry (miscellaneous), 030220 oncology & carcinogenesis, Casein Kinase Idelta, Molecular Medicine, Casein kinase 1, Alzheimer’s disease, Gene isoform, familial advanced sleep phase syndrome, Biology, p38 MAPK, Article, 03 medical and health sciences, Inhibitory Concentration 50, Cell Line, Tumor, medicine, Humans, cancer, Physical and Theoretical Chemistry, Protein kinase A, IC50, Protein Kinase Inhibitors, protein kinase CK1, formerly known as casein kinase 1, Organic Chemistry, Cancer, medicine.disease, 030104 developmental biology

Abstract

The involvement of protein kinase CK1δ in the pathogenesis of severe disorders such as Alzheimer’s disease, amyotrophic lateral sclerosis, familial advanced sleep phase syndrome, and cancer has dramatically increased interest in the development of effective small molecule inhibitors for both therapeutic application and basic research. Unfortunately, the design of CK1 isoform-specific compounds has proved to be highly complicated due to the existence of six evolutionarily conserved human CK1 members that possess similar, different, or even opposite physiological and pathophysiological implications. Consequently, only few potent and selective CK1δ inhibitors have been reported so far and structurally divergent approaches are urgently needed in order to establish SAR that might enable complete discrimination of CK1 isoforms and related p38α MAPK. In this study we report on design and characterization of optimized 4,5-diarylimidazoles as highly effective ATP-competitive inhibitors of CK1δ with compounds 11b (IC50 CK1δ = 4 nM, IC50 CK1ε = 25 nM), 12a (IC50 CK1δ = 19 nM, IC50 CK1ε = 227 nM), and 16b (IC50 CK1δ = 8 nM, IC50 CK1ε = 81 nM) being among the most potent CK1δ-targeting agents published to date. Inhibitor compound 11b, displaying potential as a pharmacological tool, has further been profiled over a panel of 321 protein kinases exhibiting high selectivity. Cellular efficacy has been evaluated in human pancreatic cancer cell lines Colo357 (EC50 = 3.5 µM) and Panc89 (EC50 = 1.5 µM). SAR is substantiated by X-ray crystallographic analysis of 16b in CK1δ and 11b in p38α., Molecules;22(4)

Published

2017

11. Design, Synthesis and Biological Evaluation of Isoxazole-Based CK1 Inhibitors Modified with Chiral Pyrrolidine Scaffolds.

Author

Luxenburger, Andreas, Schmidt, Dorian, Ianes, Chiara, Pichlo, Christian, Krüger, Marc, von Drathen, Thorsten, Brunstein, Elena, Gainsford, Graeme J., Baumann, Ulrich, Knippschild, Uwe, Peifer, Christian, and McPhee, Derek J.

Subjects

*PYRROLIDINE, *ADENOSINE triphosphate, *DRUG design, *LIGANDS (Biochemistry), *FORMALDEHYDE, *METHIONINE

Abstract

In this study, we report on the modification of a 3,4-diaryl-isoxazole-based CK1 inhibitor with chiral pyrrolidine scaffolds to develop potent and selective CK1 inhibitors. The pharmacophore of the lead structure was extended towards the ribose pocket of the adenosine triphosphate (ATP) binding site driven by structure-based drug design. For an upscale compatible multigram synthesis of the functionalized pyrrolidine scaffolds, we used a chiral pool synthetic route starting from methionine. Biological evaluation of key compounds in kinase and cellular assays revealed significant effects of the scaffolds towards activity and selectivity, however, the absolute configuration of the chiral moieties only exhibited a limited effect on inhibitory activity. X-ray crystallographic analysis of ligand-CK1δ complexes confirmed the expected binding mode of the 3,4-diaryl-isoxazole inhibitors. Surprisingly, the original compounds underwent spontaneous Pictet-Spengler cyclization with traces of formaldehyde during the co-crystallization process to form highly potent new ligands. Our data suggests chiral "ribose-like" pyrrolidine scaffolds have interesting potential for modifications of pharmacologically active compounds. [ABSTRACT FROM AUTHOR]

Published

2019

12. CK2α/CK1α chimeras are sensitive to regulation by the CK2β subunit

Author

Jedlicki, Ana, Allende, Catherine C., and Allende, Jorge E.

Published

2008

13. Protein Kinase CK1 from Trypanosoma cruzi

Author

Calabokis, Maritza, Kurz, Liliana, Gonzatti, Mary I., and Bubis, José

Published

2003

14. Golgi apparatus mammary gland casein kinase: monitoring by a specific peptide substrate and definition of specificity determinants

Author

Lorenzo A. Pinna, Marina Lasa-Benito, Flavio Meggio, and Oriano Marin

Subjects

animal structures, Molecular Sequence Data, Mammary gland, Biophysics, Protein Serine-Threonine Kinases, Biochemistry, SH3 domain, Substrate Specificity, MAP2K7, Mammary Glands, Animal, Structural Biology, Consensus Sequence, Casein kinase 2, alpha 1, Genetics, Animals, Amino Acid Sequence, Protein kinase CK2, c-Raf, Amino Acids, Phosphorylation, Protein kinase CK1, Casein Kinase II, Molecular Biology, biology, Chemistry, fungi, Cyclin-dependent kinase 2, Caseins, Cell Biology, Rats, Kinetics, Golgi apparatus, biology.protein, Female, Casein kinase 1, Casein kinase 2, Peptides, Casein kinases, Casein Kinases, Protein Kinases, Casein kinase

Abstract

The casein kinase from the Golgi apparatus of lactating mammary gland (GEF-CK) is distinct from ubiquitous ‘casein kinases’ termed protein kinases CK1 and CK2 and appears to define a family of secretory pathways protein kinases that phosphorylate seryl residues followed by an acidic residue at position +2. In this report we show that a new synthetic peptide substrate derived from β-casein (β[28–40]) is suitable for the fast, efficient and selective monitoring of GEF-CK, being unaffected by CK1 and CK2, and we define the consensus sequence of this protein kinase as being Ser-Xaa-Glu/SerP, distinct from that of CK2 (Ser/Thr-X-X-Glu/Asp/SerP/TyrP). In particular, the failure to recognize Asp as crucial specificity determinant prevents the phosphorylation of the specific CK2 peptide substrate RRRADDSDDDD by GEF-CK. Thus, peptide substrates are now available for the fast and specific monitoring of all the three classes of ‘casein kinases’, CK1, CK2 and GEF-CK.

Published

1996

15. Protein kinases - structure and function

Author

Dirk Bossemeyer

Subjects

Models, Molecular, Molecular Sequence Data, Catalytic site, Biophysics, MAP2K2, Biochemistry, SH3 domain, Structure-Activity Relationship, Structural Biology, Genetics, Conserved sequence motif, Amino Acid Sequence, Protein kinase CK1, Protein kinase A, Molecular Biology, cAMP-dependent protein kinase, Binding Sites, Crystallography, biology, Kinase, Crystal structure, Cyclin-dependent kinase 2, Cell Biology, Cyclic AMP-Dependent Protein Kinases, Receptor, Insulin, Protein kinase domain, biology.protein, Casein kinase 1, Casein Kinases, Protein Kinases, Tyrosine kinase, Insulin receptor

Abstract

The solution of crystal structures from half a dozen protein kinases during the last four years in different laboratories has deepened our understanding of the catalysis and regulation of this enzyme class, and given a vigorous impetus to the whole field. Due to the great degree of sequence conservation among protein kinases the informational yield with every new structure is high, as each is a representative of the enzyme family in general and most often of a subclass in particular. This review will focus on the active site structure of cAMP-dependent protein kinase (cAPK) with special regard to two new crystal structures; one of an active protein kinase CK1∗, which may represent an as yet unsolved step in the kinetic pathway, and the other of the insulin receptor kinase domain, the first structure of a tyrosine kinase.

Published

1995

16. Multiple phosphorylation sites at the C-terminus regulate nuclear import of HCMV DNA polymerase processivity factor ppUL44

Author

Simone Avanzi, Gregory S. Pari, Oriano Marin, Arianna Loregian, Manuela Mancini, Gualtiero Alvisi, Alessandro Ripalti, and David A. Jans

Subjects

inorganic chemicals, Active Transport, Cell Nucleus, Large tumor antigen, Replication, Cytomegalovirus, DNA polymerase, Biology, environment and public health, Phosphorylation cascade, Cell Line, 03 medical and health sciences, Viral Proteins, Virology, DNA Polymerase Processivity Factor, Chlorocebus aethiops, Animals, Humans, Protein phosphorylation, Protein kinase CK2, Protein kinase CK1, Phosphorylation, HCMV, 030304 developmental biology, Cell Nucleus, 0303 health sciences, 030302 biochemistry & molecular biology, Processivity, Molecular biology, 3. Good health, DNA-Binding Proteins, enzymes and coenzymes (carbohydrates), Processivity factor, Phosphoprotein, Nuclear transport, Host-Pathogen Interactions, bacteria, Casein kinase 1, Nuclear localization sequence, Regulation

Abstract

The processivity factor of human cytomegalovirus DNA polymerase, phosphoprotein ppUL44, is essential for viral replication. During viral infection ppUL44 is phosphorylated by the viral kinase pUL97, but neither the target residues on ppUL44 nor the effect of phosphorylation on ppUL44's activity are known. We report here that ppUL44 is phosphorylated when transiently expressed in mammalian cells and coimmunoprecipitates with cellular kinases. Of three potential phosphorylation sites (S413, S415, S418) located upstream of ppUL44's nuclear localization signal (NLS) and one (T427) within the NLS itself, protein kinase CK2 (CK2) specifically phosphorylates S413, to trigger a cascade of phosphorylation of S418 and S415 by CK1 and CK2, respectively. Negative charge at the CK2/CK1 target serine residues facilitates optimal nuclear accumulation of ppUL44, whereas negative charge on T427, a potential cyclin-dependent 1 phosphorylation site, strongly decreases nuclear accumulation. Thus, nuclear transport of ppUL44 is finely tuned during viral infection through complex phosphorylation events.

Published

2011

17. Isoform specific phosphorylation of p53 Ser-20 by CK1 is dictated by both a local consensus and a remote docking site

Author

Venerando, Andrea

Subjects

CK1, protein kinase CK1, p53 phosphorylation, adenomatous polyposis coli, CK1 inhibitors, p13 HTLV-1, Settore BIO/10 - Biochimica

Published

2010

18. DESIGN, SYNTHESIS AND BIOCHEMICAL CHARACTERIZATION OF INHIBITORS OF PROTEIN KINASES

Author

Gianoncelli, Alessandra

Subjects

ellagic acid, CK2, Settore BIO/10 - Biochimica, Protein Kinase CK1, Protein Kinase CK1, CK2, ellagic acid, benzimidazole, emodin, benzimidazole, emodin

Published

2010

19. Optimal sequences for non-phosphate-directed phosphorylation by protein kinase CK1 (casein kinase-1)--a re-evaluation

Author

V, Pulgar, O, Marin, F, Meggio, C C, Allende, J E, Allende, and L A, Pinna

Subjects

Binding Sites, Solid-phase synthesis, Synthetic peptides, Blotting, Western, Molecular Sequence Data, Proteins, site specificity, Rats, Substrate Specificity, Kinetics, Protein phosphorylation, Liver, Protein kinase CK1, Consensus sequence, Animals, Amino Acid Sequence, Phosphorylation, Peptides, Casein Kinases, Protein Kinases

Abstract

A variety of synthetic peptides derived from either the inhibitor-2 (I-2) phosphoacceptor sites or the optimal sequences selected in an oriented peptide library have been compared for their susceptibility to phosphorylation by protein kinase CK1 (also termed casein kinase-1). The I-2-derived peptides are by far preferred over the library peptides by both rat liver CK1 (and by the alpha/beta, gamma and delta/epsilon isoforms immunoprecipitated from it) and recombinant Xenopus laevis CK1 alpha. The superiority of the I-2-derived peptides over the library ones is reflected by Vmax values one to two orders of magnitude higher while the Km values are comparable. Individual substitutions of any of the aspartic acids with alanine in the I-2-derived peptide RRKHAAIGDDDDAYSITA is detrimental, producing both a fall in Vmax and an increase in Km which are more pronounced at position n -3, but also quite significant at positions n -4, n -5 and, to a lesser extent, n -6. The unfavourable effect of these substitutions is more evident with rat liver CK1 than with recombinant Xenopus laevis CK1 alpha. The chimeric peptide IGDDDDAY-S-IIIFFA, resulting from the combination of the N-terminal acidic sequence of the I-2 (Ser86) site and the C-terminal hydrophobic cluster selected in the library peptides (MAEFDTG-S-IIIFFAKKK and MAYYDAA-S-IIIFFAKKK) is phosphorylated as efficiently as the I-2-derived peptide in terms of both Km and Vmax. These combined data strongly support the conclusion that, at variance with the optimal sequences selected in the library, optimal non-phosphate-directed phosphorylation of peptide substrates by CK1 critically relies on the presence of a cluster of acidic residues (preferably aspartic acid) upstream from position n -2, while the highly hydrophobic region downstream from serine selected in the library appears to be dispensable. The reason for these discrepancies remains unclear. The possibility that the library data are biased by the invariant elements forming its scaffold (MA-x-x-x-x-x-SI-x-x-x-x-AKKK) would be consistent with the observation that the library-selected peptides, despite their low Km values, fail to compete against the phosphorylation of protein and peptide substrates by CK1, suggesting that they bind to elements partially distinct from those responsible for substrate recognition.

Published

1999