Your search keyword '"Goldsmith EJ"' showing total 103 results

1. Identification of a Class of WNK Isoform-Specific Inhibitors Through High-Throughput Screening

Author

Chlebowicz J, Akella R, Humphreys JM, He H, Kannangara AR, Wei S, Posner B, and Goldsmith EJ

Subjects

wnk, inhibition screen, kinase inhibitor, wnk3-specific, structure activity relationship, crystallography, Therapeutics. Pharmacology, RM1-950

Abstract

Julita Chlebowicz,1 Radha Akella,1 John M Humphreys,1 Haixia He,1 Ashari R Kannangara,1 Shuguang Wei,2 Bruce Posner,2 Elizabeth J Goldsmith1 1Department of Biophysics, The University of Texas Southwestern Medical Center, Dallas, TX, USA; 2Department of Biochemistry, The University of Texas Southwestern Medical Center, Dallas, TX, USACorrespondence: Elizabeth J Goldsmith, Department of Biophysics, The University of Texas Southwestern Medical Center, 5323 Harry Hines Boulevard, Dallas, TX, 75390-8816, USA, Tel +1 214 645 6376, Email Elizabeth.goldsmith@utsouthwestern.eduIntroduction: WNK [with no lysine (K)] kinases are serine/threonine kinases associated with familial hyperkalemic hypertension (FHHt). WNKs are therapeutic targets for blood pressure regulation, stroke and several cancers including triple negative breast cancer and glioblastoma. Here, we searched for and characterized novel WNK kinase inhibitors.Methods: We used a ~210,000-compound library in a high-throughput screen, re-acquisition and assay, commercial specificity screens and crystallography to identify WNK-isoform-selective inhibitors.Results: We identified five classes of compounds that inhibit the kinase activity of WNK1: quinoline compounds, halo-sulfones, cyclopropane-containing thiazoles, piperazine-containing compounds, and nitrophenol-derived compounds. The compounds are strongly pan-WNK selective, inhibiting all four WNK isoforms. A class of quinoline compounds was identified that further shows selectivity among the WNK isoforms, being more potent toward WNK3 than WNK1. The crystal structure of the quinoline-derived SW120619 bound to the kinase domain of WNK3 reveals active site binding, and comparison to the WNK1 structure reveals the potential origin of isoform specificity.Discussion: The newly discovered classes of compounds may be starting points for generating pharmacological tools and potential drugs treating hypertension and cancer.Graphical Abstract: Keywords: WNK, inhibition screen, kinase inhibitor, WNK3-specific, structure–activity relationship, crystallography

Published

2023

2. Serpins: the uncut version

Author

Goldsmith, EJ, primary and Mottonen, J, additional

Published

1994

3. Water and chloride as allosteric inhibitors in WNK kinase osmosensing.

Author

Teixeira LR, Akella R, Humphreys JM, He H, and Goldsmith EJ

Subjects

Phosphorylation, Humans, Allosteric Regulation, Crystallography, X-Ray, Osmoregulation, Water chemistry, Water metabolism, Protein Serine-Threonine Kinases metabolism, Protein Serine-Threonine Kinases chemistry, Protein Serine-Threonine Kinases genetics, Chlorides metabolism, WNK Lysine-Deficient Protein Kinase 1 metabolism, WNK Lysine-Deficient Protein Kinase 1 genetics, WNK Lysine-Deficient Protein Kinase 1 chemistry

Abstract

Osmotic stress and chloride regulate the autophosphorylation and activity of the WNK1 and WNK3 kinase domains. The kinase domain of unphosphorylated WNK1 (uWNK1) is an asymmetric dimer possessing water molecules conserved in multiple uWNK1 crystal structures. Conserved waters are present in two networks, referred to here as conserved water networks 1 and 2 (CWN1 and CWN2). Here, we show that PEG400 applied to crystals of dimeric uWNK1 induces de-dimerization. Both the WNK1 the water networks and the chloride-binding site are disrupted by PEG400. CWN1 is surrounded by a cluster of pan-WNK-conserved charged residues. Here, we mutagenized these charges in WNK3, a highly active WNK isoform kinase domain, and WNK1, the isoform best studied crystallographically. Mutation of E314 in the Activation Loop of WNK3 (WNK3/E314Q and WNK3/E314A, and the homologous WNK1/E388A) enhanced the rate of autophosphorylation, and reduced chloride sensitivity. Other WNK3 mutants reduced the rate of autophosphorylation activity coupled with greater chloride sensitivity than wild-type. The water and chloride regulation thus appear linked. The lower activity of some mutants may reflect effects on catalysis. Crystallography showed that activating mutants introduced conformational changes in similar parts of the structure to those induced by PEG400. WNK activating mutations and crystallography support a role for CWN1 in WNK inhibition consistent with water functioning as an allosteric ligand., Competing Interests: LT, RA, JH, HH, EG No competing interests declared, (© 2023, Teixeira et al.)

Published

2024

4. Hydrostatic Pressure Sensing by WNK kinases.

Author

Humphreys JM, Teixeira LR, Akella R, He H, Kannangara AR, Sekulski K, Pleinis J, Liwocha J, Jiou J, Servage KA, Orth K, Joachimiak L, Rizo J, Cobb MH, Brautigam CA, Rodan AR, and Goldsmith EJ

Subjects

Animals, Hydrostatic Pressure, Phosphorylation, Protein Serine-Threonine Kinases metabolism

Abstract

Previous study has demonstrated that the WNK kinases 1 and 3 are direct osmosensors consistent with their established role in cell-volume control. WNK kinases may also be regulated by hydrostatic pressure. Hydrostatic pressure applied to cells in culture with N 2 gas or to Drosophila Malpighian tubules by centrifugation induces phosphorylation of downstream effectors of endogenous WNKs. In vitro, the autophosphorylation and activity of the unphosphorylated kinase domain of WNK3 (uWNK3) is enhanced to a lesser extent than in cells by 190 kPa applied with N 2 gas. Hydrostatic pressure measurably alters the structure of uWNK3. Data from size exclusion chromatography in line with multi-angle light scattering (SEC-MALS), SEC alone at different back pressures, analytical ultracentrifugation (AUC), NMR, and chemical crosslinking indicate a change in oligomeric structure in the presence of hydrostatic pressure from a WNK3 dimer to a monomer. The effects on the structure are related to those seen with osmolytes. Potential mechanisms of hydrostatic pressure activation of uWNK3 and the relationships of pressure activation to WNK osmosensing are discussed.

Published

2023

5. Intracellular Ion Control of WNK Signaling.

Author

Goldsmith EJ and Rodan AR

Subjects

Humans, Signal Transduction physiology, Kidney metabolism, Protein Serine-Threonine Kinases chemistry, Protein Serine-Threonine Kinases metabolism, Chlorides

Abstract

The with no lysine (K) (WNK) kinases are an evolutionarily ancient group of kinases with atypical placement of the catalytic lysine and diverse physiological roles. Recent studies have shown that WNKs are directly regulated by chloride, potassium, and osmotic pressure. Here, we review the discovery of WNKs as chloride-sensitive kinases and discuss physiological contexts in which chloride regulation of WNKs has been demonstrated. These include the kidney, pancreatic duct, neurons, and inflammatory cells. We discuss the interdependent relationship of osmotic pressure and intracellular chloride in cell volume regulation. We review the recent demonstration of potassium regulation of WNKs and speculate on possible physiological roles. Finally, structural and mechanistic aspects of intracellular ion and osmotic pressure regulation of WNKs are discussed.

Published

2023

6. Synthesis and Structural Characterization of Novel Trihalo-sulfone Inhibitors of WNK1.

Author

Rodriguez M, Kannangara A, Chlebowicz J, Akella R, He H, Tambar UK, and Goldsmith EJ

Abstract

With No lysine (K) [WNK] kinases are structurally unique serine/threonine protein kinases that have therapeutic potential for blood pressure regulation and cancer. A novel class of trihalo-sulfone compounds was identified by high-throughput screening. Trihalo-sulfone 1 emerged as an effective inhibitor of WNK1 with an IC 50 value of 1.6 μM. Herein, we define chemical features necessary for inhibition of WNK1 using chemical synthesis and X-ray crystallography. Analogues that probed the role of specific functional groups to the inhibitory activity were synthesized. X-ray structures of trihalo-sulfone 1 and a second trihalo-sulfone 23 bound to WNK1 revealed active site binding to two of the three previously defined canonical inhibitor binding pockets as well as a novel binding site for the trihalo-sulfone moiety. The elucidation of these novel interaction sites may allow for the strategic design of even more selective and potent WNK inhibitors., Competing Interests: The authors declare no competing financial interest., (© 2022 American Chemical Society.)

Published

2022

7. WNK1 collaborates with TGF-β in endothelial cell junction turnover and angiogenesis.

Author

Jaykumar AB, Plumber S, Barry DM, Binns D, Wichaidit C, Grzemska M, Earnest S, Goldsmith EJ, Cleaver O, and Cobb MH

Subjects

Animals, Mice, Proteolysis, Proto-Oncogene Proteins metabolism, Receptor Protein-Tyrosine Kinases metabolism, Axl Receptor Tyrosine Kinase, Endothelial Cells metabolism, Intercellular Junctions metabolism, Neovascularization, Physiologic genetics, Neovascularization, Physiologic physiology, Transforming Growth Factor beta metabolism, WNK Lysine-Deficient Protein Kinase 1 genetics, WNK Lysine-Deficient Protein Kinase 1 metabolism

Abstract

Angiogenesis is essential for growth of new blood vessels, remodeling existing vessels, and repair of damaged vessels, and these require reorganization of endothelial cell-cell junctions through a partial endothelial-mesenchymal transition. Homozygous disruption of the gene encoding the protein kinase WNK1 results in lethality in mice near embryonic day (E) 12 due to impaired angiogenesis. This angiogenesis defect can be rescued by endothelial-specific expression of an activated form of the WNK1 substrate kinase OSR1. We show that inhibition of WNK1 kinase activity not only prevents sprouting of endothelial cells from aortic slices but also vessel extension in inhibitor-treated embryos ex vivo. Mutations affecting TGF-β signaling also result in abnormal vascular development beginning by E10 and, ultimately, embryonic lethality. Previously, we demonstrated cross-talk of WNK1 with TGF-β-regulated SMAD signaling, and OSR1 was identified as a component of the TGF-β interactome. However, molecular events jointly regulated by TGF-β and WNK1/OSR1 have not been delineated. Here, we show that inhibition of WNK1 promotes TGF-β-dependent degradation of the tyrosine kinase receptor AXL, which is involved in TGF-β-mediated cell migration and angiogenesis. We also show that interaction between OSR1 and occludin, a protein associated with endothelial tight junctions, is an essential step to enable tight junction turnover. Furthermore, we show that these phenomena are WNK1 dependent, and sensitive to TGF-β. These findings demonstrate intimate connections between WNK1/OSR1 and multiple TGF-β-sensitive molecules controlling angiogenesis and suggest that WNK1 may modulate many TGF-β-regulated functions.

Published

2022

8. Nuclear speckle integrity and function require TAO2 kinase.

Author

Gao S, Esparza M, Dehghan I, Aksenova V, Zhang K, Batten K, Ferretti MB, Begg BE, Cagatay T, Shay JW, García-Sastre A, Goldsmith EJ, Chen ZJ, Dasso M, Lynch KW, Cobb MH, and Fontoura BMA

Subjects

Active Transport, Cell Nucleus, HeLa Cells, Humans, RNA metabolism, RNA, Messenger metabolism, Serine-Arginine Splicing Factors genetics, Cell Nucleus enzymology, Nuclear Speckles, Protein Kinases metabolism, RNA Splicing

Abstract

Nuclear speckles are non-membrane-bound organelles known as storage sites for messenger RNA (mRNA) processing and splicing factors. More recently, nuclear speckles have also been implicated in splicing and export of a subset of mRNAs, including the influenza virus M mRNA that encodes proteins required for viral entry, trafficking, and budding. However, little is known about how nuclear speckles are assembled or regulated. Here, we uncovered a role for the cellular protein kinase TAO2 as a constituent of nuclear speckles and as a factor required for the integrity of these nuclear bodies and for their functions in pre-mRNA splicing and trafficking. We found that a nuclear pool of TAO2 is localized at nuclear speckles and interacts with nuclear speckle factors involved in RNA splicing and nuclear export, including SRSF1 and Aly/Ref. Depletion of TAO2 or inhibition of its kinase activity disrupts nuclear speckle structure, decreasing the levels of several proteins involved in nuclear speckle assembly and splicing, including SC35 and SON. Consequently, splicing and nuclear export of influenza virus M mRNA were severely compromised and caused a disruption in the virus life cycle. In fact, low levels of TAO2 led to a decrease in viral protein levels and inhibited viral replication. Additionally, depletion or inhibition of TAO2 resulted in abnormal expression of a subset of mRNAs with key roles in viral replication and immunity. Together, these findings uncovered a function of TAO2 in nuclear speckle formation and function and revealed host requirements and vulnerabilities for influenza infection.

Published

2022

9. WNK1 Enhances Migration and Invasion in Breast Cancer Models.

Author

Jaykumar AB, Jung JU, Parida PK, Dang TT, Wichaidit C, Kannangara AR, Earnest S, Goldsmith EJ, Pearson GW, Malladi S, and Cobb MH

Subjects

Animals, Apoptosis, Biomarkers, Tumor genetics, Breast Neoplasms drug therapy, Breast Neoplasms genetics, Breast Neoplasms metabolism, Cell Movement, Cell Proliferation, Female, Humans, Imidazoles pharmacology, Mice, Mice, Inbred NOD, Mice, SCID, Neoplasm Invasiveness, Pyrrolidines pharmacology, Tumor Cells, Cultured, WNK Lysine-Deficient Protein Kinase 1 antagonists & inhibitors, WNK Lysine-Deficient Protein Kinase 1 genetics, Xenograft Model Antitumor Assays, Biomarkers, Tumor metabolism, Breast Neoplasms pathology, Gene Expression Regulation, Neoplastic, WNK Lysine-Deficient Protein Kinase 1 metabolism

Abstract

Metastasis is the major cause of mortality in patients with breast cancer. Many signaling pathways have been linked to cancer invasiveness, but blockade of few protein components has succeeded in reducing metastasis. Thus, identification of proteins contributing to invasion that are manipulable by small molecules may be valuable in inhibiting spread of the disease. The protein kinase with no lysine (K) 1 (WNK1) has been suggested to induce migration of cells representing a range of cancer types. Analyses of mouse models and patient data have implicated WNK1 as one of a handful of genes uniquely linked to invasive breast cancer. Here, we present evidence that inhibition of WNK1 slows breast cancer metastasis. We show that depletion or inhibition of WNK1 reduces migration of several breast cancer cell lines in wound healing assays and decreases invasion in collagen matrices. Furthermore, WNK1 depletion suppresses expression of AXL, a tyrosine kinase implicated in metastasis. Finally, we demonstrate that WNK inhibition in mice attenuates tumor progression and metastatic burden. These data showing reduced migration, invasion, and metastasis upon WNK1 depletion in multiple breast cancer models suggest that WNK1 contributes to the metastatic phenotype, and that WNK1 inhibition may offer a therapeutic avenue for attenuating progression of invasive breast cancers., (©2021 American Association for Cancer Research.)

Published

2021

10. Osmosensing by WNK Kinases.

Author

Akella R, Humphreys JM, Sekulski K, He H, Durbacz M, Chakravarthy S, Liwocha J, Mohammed ZJ, Brautigam CA, and Goldsmith EJ

Subjects

Autoradiography, Chromatography, Gel, Ethylene Glycol chemistry, Osmotic Pressure physiology, Phosphorylation, Polyethylene Glycols chemistry, Protein Conformation, Protein Multimerization, Scattering, Small Angle, Water chemistry, X-Ray Diffraction, Protein Kinases chemistry, Protein Kinases metabolism, WNK Lysine-Deficient Protein Kinase 1 chemistry, WNK Lysine-Deficient Protein Kinase 1 metabolism

Abstract

With No Lysine (K) WNK kinases regulate electro-neutral cotransporters that are controlled by osmotic stress and chloride. We showed previously that autophosphorylation of WNK1 is inhibited by chloride, raising the possibility that WNKs are activated by osmotic stress. Here we demonstrate that unphosphorylated WNK isoforms 3 and 1 autophosphorylate in response to osmotic pressure in vitro, applied with the crowding agent polyethylene glycol (PEG)400 or osmolyte ethylene glycol (EG), and that this activation is opposed by chloride. Small angle x-ray scattering of WNK3 in the presence and absence of PEG400, static light scattering in EG, and crystallography of WNK1 were used to understand the mechanism. Osmosensing in WNK3 and WNK1 appears to occur through a conformational equilibrium between an inactive, unphosphorylated, chloride-binding dimer and an autophosphorylation-competent monomer. An improved structure of the inactive kinase domain of WNK1, and a comparison with the structure of a monophosphorylated form of WNK1, suggests that large cavities, greater hydration, and specific bound water may participate in the osmosensing mechanism. Our prior work showed that osmolytes have effects on the structure of phosphorylated WNK1, suggestive of multiple stages of osmotic regulation in WNKs.

Published

2021

11. LRRC8A reduces intracellular chloride to permit WNK activation in response to hypertonic stress.

Author

Goldsmith EJ and Huang CL

Subjects

Osmotic Pressure, Carrier Proteins, Chlorides metabolism

Abstract

Competing Interests: The authors declare no competing interest.

Published

2021

12. WNKs are potassium-sensitive kinases.

Author

Pleinis JM, Norrell L, Akella R, Humphreys JM, He H, Sun Q, Zhang F, Sosa-Pagan J, Morrison DE, Schellinger JN, Jackson LK, Goldsmith EJ, and Rodan AR

Subjects

Animals, Animals, Genetically Modified, Binding Sites, Cell Line, Chlorides metabolism, Drosophila Proteins genetics, Drosophila melanogaster genetics, Hydrogen-Ion Concentration, Mutation, Phosphorylation, Protein Serine-Threonine Kinases genetics, Protein Stability, Substrate Specificity, Drosophila Proteins metabolism, Drosophila melanogaster enzymology, Malpighian Tubules enzymology, Potassium metabolism, Protein Serine-Threonine Kinases metabolism

Abstract

With no lysine (K) (WNK) kinases regulate epithelial ion transport in the kidney to maintain homeostasis of electrolyte concentrations and blood pressure. Chloride ion directly binds WNK kinases to inhibit autophosphorylation and activation. Changes in extracellular potassium are thought to regulate WNKs through changes in intracellular chloride. Prior studies demonstrate that in some distal nephron epithelial cells, intracellular potassium changes with chronic low- or high-potassium diet. We, therefore, investigated whether potassium regulates WNK activity independent of chloride. We found decreased activity of Drosophila WNK and mammalian WNK3 and WNK4 in fly Malpighian (renal) tubules bathed in high extracellular potassium, even when intracellular chloride was kept constant at either ∼13 mM or 26 mM. High extracellular potassium also inhibited chloride-insensitive mutants of WNK3 and WNK4. High extracellular rubidium was also inhibitory and increased tubule rubidium. The Na + /K + -ATPase inhibitor, ouabain, which is expected to lower intracellular potassium, increased tubule Drosophila WNK activity. In vitro, potassium increased the melting temperature of Drosophila WNK, WNK1, and WNK3 kinase domains, indicating ion binding to the kinase. Potassium inhibited in vitro autophosphorylation of Drosophila WNK and WNK3, and also inhibited WNK3 and WNK4 phosphorylation of their substrate, Ste20-related proline/alanine-rich kinase (SPAK). The greatest sensitivity of WNK4 to potassium occurred in the range of 80-180 mM, encompassing physiological intracellular potassium concentrations. Together, these data indicate chloride-independent potassium inhibition of Drosophila and mammalian WNK kinases through direct effects of potassium ion on the kinase.

Published

2021

13. A Phosphorylated Intermediate in the Activation of WNK Kinases.

Author

Akella R, Drozdz MA, Humphreys JM, Jiou J, Durbacz MZ, Mohammed ZJ, He H, Liwocha J, Sekulski K, and Goldsmith EJ

Subjects

Animals, Crystallography, X-Ray, Humans, Models, Molecular, Phosphorylation, Protein Serine-Threonine Kinases chemistry, Rats, WNK Lysine-Deficient Protein Kinase 1 chemistry, Protein Serine-Threonine Kinases metabolism, WNK Lysine-Deficient Protein Kinase 1 metabolism

Abstract

WNK kinases autoactivate by autophosphorylation. Crystallography of the kinase domain of WNK1 phosphorylated on the primary activating site (pWNK1) in the presence of AMP-PNP reveals a well-ordered but inactive configuration. This new pWNK1 structure features specific and unique interactions of the phosphoserine, less hydration, and smaller cavities compared with those of unphosphorylated WNK1 (uWNK1). Because WNKs are activated by osmotic stress in cells, we addressed whether the structure was influenced directly by osmotic pressure. pWNK1 crystals formed in PEG3350 were soaked in the osmolyte sucrose. Suc-WNK1 crystals maintained X-ray diffraction, but the lattice constants and pWNK1 structure changed. Differences were found in the activation loop and helix C, common switch loci in kinase activation. On the basis of these structural changes, we tested for effects on in vitro activity of two WNKs, pWNK1 and pWNK3. The osmolyte PEG400 enhanced ATPase activity. Our data suggest multistage activation of WNKs.

Published

2020

14. Functional divergence caused by mutations in an energetic hotspot in ERK2.

Author

Taylor CA 4th, Cormier KW, Keenan SE, Earnest S, Stippec S, Wichaidit C, Juang YC, Wang J, Shvartsman SY, Goldsmith EJ, and Cobb MH

Subjects

Animals, Animals, Genetically Modified, Crystallography, X-Ray, Drosophila Proteins chemistry, Drosophila Proteins metabolism, Enzyme Activation, Enzyme Stability, Extracellular Signal-Regulated MAP Kinases chemistry, Extracellular Signal-Regulated MAP Kinases metabolism, Humans, Models, Molecular, Mutant Proteins metabolism, Drosophila Proteins genetics, Drosophila melanogaster enzymology, Drosophila melanogaster genetics, Extracellular Signal-Regulated MAP Kinases genetics, Mutation genetics

Abstract

The most frequent extracellular signal-regulated kinase 2 (ERK2) mutation occurring in cancers is E322K (E-K). ERK2 E-K reverses a buried charge in the ERK2 common docking (CD) site, a region that binds activators, inhibitors, and substrates. Little is known about the cellular consequences associated with this mutation, other than apparent increases in tumor resistance to pathway inhibitors. ERK2 E-K, like the mutation of the preceding aspartate (ERK2 D321N [D-N]) known as the sevenmaker mutation, causes increased activity in cells and evades inactivation by dual-specificity phosphatases. As opposed to findings in cancer cells, in developmental assays in Drosophila , only ERK2 D-N displays a significant gain of function, revealing mutation-specific phenotypes. The crystal structure of ERK2 D-N is indistinguishable from that of wild-type protein, yet this mutant displays increased thermal stability. In contrast, the crystal structure of ERK2 E-K reveals profound structural changes, including disorder in the CD site and exposure of the activation loop phosphorylation sites, which likely account for the decreased thermal stability of the protein. These contiguous mutations in the CD site of ERK2 are both required for docking interactions but lead to unpredictably different functional outcomes. Our results suggest that the CD site is in an energetically strained configuration, and this helps drive conformational changes at distal sites on ERK2 during docking interactions., Competing Interests: The authors declare no conflict of interest.

Published

2019

15. Intracellular Chloride and Scaffold Protein Mo25 Cooperatively Regulate Transepithelial Ion Transport through WNK Signaling in the Malpighian Tubule.

Author

Sun Q, Wu Y, Jonusaite S, Pleinis JM, Humphreys JM, He H, Schellinger JN, Akella R, Stenesen D, Krämer H, Goldsmith EJ, and Rodan AR

Subjects

Animals, Animals, Genetically Modified, Calcium-Binding Proteins genetics, Drosophila Proteins genetics, Drosophila melanogaster, Epithelium physiology, Female, Gene Knockdown Techniques, Ion Transport genetics, Phosphorylation, Signal Transduction, Calcium-Binding Proteins metabolism, Chlorides metabolism, Drosophila Proteins metabolism, Malpighian Tubules metabolism, Protein Serine-Threonine Kinases metabolism

Abstract

Background With No Lysine kinase (WNK) signaling regulates mammalian renal epithelial ion transport to maintain electrolyte and BP homeostasis. Our previous studies showed a conserved role for WNK in the regulation of transepithelial ion transport in the Drosophila Malpighian tubule. Methods Using in vitro assays and transgenic Drosophila lines, we examined two potential WNK regulators, chloride ion and the scaffold protein mouse protein 25 (Mo25), in the stimulation of transepithelial ion flux. Results In vitro , autophosphorylation of purified Drosophila WNK decreased as chloride concentration increased. In conditions in which tubule intracellular chloride concentration decreased from 30 to 15 mM as measured using a transgenic sensor, Drosophila WNK activity acutely increased. Drosophila WNK activity in tubules also increased or decreased when bath potassium concentration decreased or increased, respectively. However, a mutation that reduces chloride sensitivity of Drosophila WNK failed to alter transepithelial ion transport in 30 mM chloride. We, therefore, examined a role for Mo25. In in vitro kinase assays, Drosophila Mo25 enhanced the activity of the Drosophila WNK downstream kinase Fray, the fly homolog of mammalian Ste20-related proline/alanine-rich kinase (SPAK), and oxidative stress-responsive 1 protein (OSR1). Knockdown of Drosophila Mo25 in the Malpighian tubule decreased transepithelial ion flux under stimulated but not basal conditions. Finally, whereas overexpression of wild-type Drosophila WNK , with or without Drosophila Mo25 , did not affect transepithelial ion transport, Drosophila Mo25 overexpressed with chloride-insensitive Drosophila WNK increased ion flux. Conclusions Cooperative interactions between chloride and Mo25 regulate WNK signaling in a transporting renal epithelium., (Copyright © 2018 by the American Society of Nephrology.)

Published

2018

16. How activating mutations affect MEK1 regulation and function.

Author

Jindal GA, Goyal Y, Humphreys JM, Yeung E, Tian K, Patterson VL, He H, Burdine RD, Goldsmith EJ, and Shvartsman SY

Subjects

Animals, Crystallography, X-Ray, Enzyme Activation, Humans, MAP Kinase Kinase 1 chemistry, Mitogen-Activated Protein Kinase 1 metabolism, Models, Molecular, Neoplasms genetics, Neoplasms metabolism, Phosphorylation, Protein Conformation, Zebrafish, raf Kinases metabolism, MAP Kinase Kinase 1 genetics, MAP Kinase Kinase 1 metabolism, Point Mutation

Abstract

The MEK1 kinase directly phosphorylates ERK2, after the activation loop of MEK1 is itself phosphorylated by Raf. Studies over the past decade have revealed a large number of disease-related mutations in the MEK1 gene that lead to tumorigenesis and abnormal development. Several of these mutations result in MEK1 constitutive activity, but how they affect MEK1 regulation and function remains largely unknown. Here, we address these questions focusing on two pathogenic variants of the Phe-53 residue, which maps to the well-characterized negative regulatory region of MEK1. We found that these variants are phosphorylated by Raf faster than the wild-type enzyme, and this phosphorylation further increases their enzymatic activity. However, the maximal activities of fully phosphorylated wild-type and mutant enzymes are indistinguishable. On the basis of available structural information, we propose that the activating substitutions destabilize the inactive conformation of MEK1, resulting in its constitutive activity and making it more prone to Raf-mediated phosphorylation. Experiments in zebrafish revealed that the effects of activating variants on embryonic development reflect the joint control of the negative regulatory region and activating phosphorylation. Our results underscore the complexity of the effects of activating mutations on signaling systems, even at the level of a single protein., (© 2017 by The American Society for Biochemistry and Molecular Biology, Inc.)

Published

2017

17. Discovery of novel TAOK2 inhibitor scaffolds from high-throughput screening.

Author

Piala AT, Akella R, Potts MB, Dudics-Giagnocavo SA, He H, Wei S, White MA, Posner BA, and Goldsmith EJ

Subjects

Autophagy drug effects, Cell Line, Tumor, Drug Evaluation, Preclinical, High-Throughput Screening Assays, Humans, Protein Binding, Protein Kinase Inhibitors metabolism, Protein Kinase Inhibitors toxicity, Protein Serine-Threonine Kinases metabolism, Small Molecule Libraries metabolism, Small Molecule Libraries toxicity, Structure-Activity Relationship, Transition Temperature, p38 Mitogen-Activated Protein Kinases chemistry, p38 Mitogen-Activated Protein Kinases metabolism, Protein Kinase Inhibitors chemistry, Protein Serine-Threonine Kinases antagonists & inhibitors, Small Molecule Libraries chemistry

Abstract

The MAP3K (Mitogen Activated Protein Kinase Kinase Kinase) TAOK2 (Thousand-And-One Kinase 2) is an activator of p38 MAP kinase cascade that is up-regulated in response to environmental stresses. A synthetic lethal screen performed using a NSCLC (non-small cell lung cancer) cell line, and a second screen identifying potential modulators of autophagy have implicated TAOK2 as a potential cancer therapeutic target. Using a 200,000 compound high throughput screen, we identified three specific small molecule compounds that inhibit the kinase activity of TAOK2. These compounds also showed inhibition of autophagy. Based on SAR (structure-activity relationship) studies, we have predicted the modifications on the reactive groups for the three compounds., (Copyright © 2016 Elsevier Ltd. All rights reserved.)

Published

2016

18. Domain-Swapping Switch Point in Ste20 Protein Kinase SPAK.

Author

Taylor CA 4th, Juang YC, Earnest S, Sengupta S, Goldsmith EJ, and Cobb MH

Subjects

Amino Acid Sequence, Amino Acid Substitution, Animals, Crystallography, X-Ray, Enzyme Activation, Mice, Models, Molecular, Molecular Sequence Data, Mutagenesis, Site-Directed, Peptide Fragments chemistry, Peptide Fragments genetics, Peptide Fragments metabolism, Phosphorylation, Protein Conformation, Protein Interaction Domains and Motifs, Protein Serine-Threonine Kinases genetics, Recombinant Proteins chemistry, Recombinant Proteins genetics, Recombinant Proteins metabolism, Sequence Homology, Amino Acid, Protein Serine-Threonine Kinases chemistry, Protein Serine-Threonine Kinases metabolism

Abstract

The related protein kinases SPAK and OSR1 regulate ion homeostasis in part by phosphorylating cation cotransporter family members. The structure of the kinase domain of OSR1 was determined in the unphosphorylated inactive form and, like some other Ste20 kinases, exhibited a domain-swapped activation loop. To further probe the role of domain swapping in SPAK and OSR1, we have determined the crystal structures of SPAK 63-403 at 3.1 Å and SPAK 63-390 T243D at 2.5 Å resolution. These structures encompass the kinase domain and different portions of the C-terminal tail, the longer without and the shorter with an activating T243D point mutation. The structure of the T243D protein reveals significant conformational differences relative to unphosphorylated SPAK and OSR1 but also has some features of an inactive kinase. Both structures are domain-swapped dimers. Sequences involved in domain swapping were identified and mutated to create a SPAK monomeric mutant with kinase activity, indicating that monomeric forms are active. The monomeric mutant is activated by WNK1 but has reduced activity toward its substrate NKCC2, suggesting regulatory roles for domain swapping. The structure of partially active SPAK T243D is consistent with a multistage activation process in which phosphorylation induces a SPAK conformation that requires further remodeling to build the active structure.

Published

2015

19. MAP kinase modules: the excursion model and the steps that count.

Author

Piala AT, Humphreys JM, and Goldsmith EJ

Subjects

Animals, Humans, Mitogen-Activated Protein Kinases genetics, Phosphorylation, Mitogen-Activated Protein Kinases metabolism

Abstract

MAP kinase modules propagate diverse extracellular signals to downstream effectors. The two dual phosphorylation reactions catalyzed by the modules are thought to control the switch behavior of the pathway. Here we review recent approaches to understand these pathways through signal-to-response studies in cells and in vitro. These data are reconciled with physical models as well as predictions made on mathematical and theoretical grounds. Biochemical analysis has shown recently that the dual phosphorylation reactions catalyzed by MAP kinase modules are sequential at both levels of the cascade. The observed order of phosphorylation events suggests an excursion from the Ser/Thr kinase activity of the MAP3K into Tyr kinase activity of the central dual specificity MAP2K. How the order of events might be encoded in the structures and interactions is discussed. The ordered mechanism confirms predictions that reactions should be sequential to generate the steep signal-to-response curves and delayed responses observed in cells.

Published

2014

20. Chloride sensing by WNK1 involves inhibition of autophosphorylation.

Author

Piala AT, Moon TM, Akella R, He H, Cobb MH, and Goldsmith EJ

Subjects

Catalytic Domain, Crystallography, X-Ray, Humans, Intracellular Signaling Peptides and Proteins chemistry, Minor Histocompatibility Antigens, Models, Molecular, Phosphorylation, Protein Serine-Threonine Kinases chemistry, WNK Lysine-Deficient Protein Kinase 1, Chlorides analysis, Intracellular Signaling Peptides and Proteins metabolism, Protein Serine-Threonine Kinases metabolism

Abstract

WNK1 [with no lysine (K)] is a serine-threonine kinase associated with a form of familial hypertension. WNK1 is at the top of a kinase cascade, leading to phosphorylation of several cotransporters, in particular those transporting sodium, potassium, and chloride (NKCC), sodium and chloride (NCC), and potassium and chloride (KCC). The responsiveness of NKCC, NCC, and KCC to changes in extracellular chloride parallels their phosphorylation state, provoking the proposal that these transporters are controlled by a chloride-sensitive protein kinase. We found that chloride stabilizes the inactive conformation of WNK1, preventing kinase autophosphorylation and activation. Crystallographic studies of inactive WNK1 in the presence of chloride revealed that chloride binds directly to the catalytic site, providing a basis for the unique position of the catalytic lysine. Mutagenesis of the chloride-binding site rendered the kinase less sensitive to inhibition of autophosphorylation by chloride, validating the binding site. Thus, these data suggest that WNK1 functions as a chloride sensor through direct binding of a regulatory chloride ion to the active site, which inhibits autophosphorylation.

Published

2014

21. Precisely ordered phosphorylation reactions in the p38 mitogen-activated protein (MAP) kinase cascade.

Author

Humphreys JM, Piala AT, Akella R, He H, and Goldsmith EJ

Subjects

Activating Transcription Factor 2 chemistry, Activating Transcription Factor 2 genetics, Activating Transcription Factor 2 metabolism, Animals, Humans, MAP Kinase Kinase 6 genetics, MAP Kinase Kinase 6 metabolism, MAP Kinase Kinase Kinase 5 genetics, MAP Kinase Kinase Kinase 5 metabolism, MAP Kinase Kinase Kinases genetics, MAP Kinase Kinase Kinases metabolism, MAP Kinase Signaling System physiology, Mitogen-Activated Protein Kinase 14 genetics, Mitogen-Activated Protein Kinase 14 metabolism, Models, Biological, Phosphorylation physiology, Protein Kinases genetics, Protein Kinases metabolism, Protein Serine-Threonine Kinases, Rats, MAP Kinase Kinase 6 chemistry, MAP Kinase Kinase Kinase 5 chemistry, MAP Kinase Kinase Kinases chemistry, Mitogen-Activated Protein Kinase 14 chemistry, Models, Chemical, Protein Kinases chemistry

Abstract

The MAP kinase cascades, composed of a MAP3K, a MAP2K, and a MAPK, control switch responses to extracellular stimuli and stress in eukaryotes. The most important feature of these modules is thought to be the two double phosphorylation reactions catalyzed by MAP3Ks and MAP2Ks. We addressed whether the reactions are sequential or random in the p38 MAP kinase module. Mass spectrometry was used to track the phosphorylation of the MAP2K MEK6 by two MAP3Ks, TAO2 and ASK1, and the subsequent phosphorylation of p38α by MEK6/S*T* (where S (Ser) and T (Thr) are the two phosphorylation sites and * denotes phosphorylation). Both double phosphorylation reactions are precisely ordered. MEK6 is phosphorylated first on Thr-211 and then on Ser-207 by both MAP3Ks. This is the first demonstration of a precise reaction order for a MAP2K. p38α is phosphorylated first on Tyr-182 and then on Thr-180, the same reaction order observed previously in ERK2. Thus, intermediates were MEK6/ST* and p38α/TY*. Similarly, the phosphorylation of the p38α transcription factor substrate ATF2 occurs in a precise sequence. Progress curves for the appearance of intermediates were fit to kinetic models. The models confirmed the reaction order, revealed processivity in the phosphorylation of MEK6 by ASK1, and suggested that the order of phosphorylation is dictated by both binding and catalysis rates.

Published

2013

22. Solution structure of the WNK1 autoinhibitory domain, a WNK-specific PF2 domain.

Author

Moon TM, Correa F, Kinch LN, Piala AT, Gardner KH, and Goldsmith EJ

Subjects

Amino Acid Sequence, Magnetic Resonance Spectroscopy, Minor Histocompatibility Antigens, Models, Molecular, Protein Binding, Protein Conformation, Sequence Homology, Amino Acid, WNK Lysine-Deficient Protein Kinase 1, Protein Serine-Threonine Kinases chemistry

Abstract

WNK1 [with no lysine (K)-1] is a 250-kDa serine/threonine protein kinase involved in the maintenance of cellular salt levels and is directly linked to a hereditary form of hypertension. Here, we report the solution NMR structure of the autoinhibitory domain of WNK1 (WNK1-AI), a small regulatory subunit that lies immediately C-terminal of the kinase domain. We show that this domain is a homolog of the RFXV-binding PASK/FRAY homology 2 (PF2) domain found in OSR (oxidative stress responsive) and SPAK (serine/threonine proline-alanine-rich) kinases, which are substrates of WNK1. The WNK1-AI has a circularly permuted topology relative to the OSR1-PF2 domain. Nevertheless, like PF2 domains, WNK1-AI binds peptides that contain an RFXV motif with micromolar affinities as assessed by changes in (1)H,(15)N heteronuclear single quantum coherence spectra. Mutations to the WNK1-AI and binding peptides confirm a similar binding mode., (Copyright © 2013. Published by Elsevier Ltd.)

Published

2013

23. Cell-free formation of RNA granules: low complexity sequence domains form dynamic fibers within hydrogels.

Author

Kato M, Han TW, Xie S, Shi K, Du X, Wu LC, Mirzaei H, Goldsmith EJ, Longgood J, Pei J, Grishin NV, Frantz DE, Schneider JW, Chen S, Li L, Sawaya MR, Eisenberg D, Tycko R, and McKnight SL

Subjects

Animals, Brain cytology, Brain metabolism, Caenorhabditis elegans cytology, Caenorhabditis elegans metabolism, Cell-Free System, Cytoplasmic Granules chemistry, Embryonic Stem Cells metabolism, Male, Mice, Models, Molecular, NIH 3T3 Cells, RNA-Binding Proteins chemistry, RNA-Binding Proteins metabolism, Testis cytology, Testis metabolism, X-Ray Diffraction, Cytoplasmic Granules metabolism, Hydrogel, Polyethylene Glycol Dimethacrylate metabolism, RNA metabolism, RNA-Binding Proteins analysis

Abstract

Eukaryotic cells contain assemblies of RNAs and proteins termed RNA granules. Many proteins within these bodies contain KH or RRM RNA-binding domains as well as low complexity (LC) sequences of unknown function. We discovered that exposure of cell or tissue lysates to a biotinylated isoxazole (b-isox) chemical precipitated hundreds of RNA-binding proteins with significant overlap to the constituents of RNA granules. The LC sequences within these proteins are both necessary and sufficient for b-isox-mediated aggregation, and these domains can undergo a concentration-dependent phase transition to a hydrogel-like state in the absence of the chemical. X-ray diffraction and EM studies revealed the hydrogels to be composed of uniformly polymerized amyloid-like fibers. Unlike pathogenic fibers, the LC sequence-based polymers described here are dynamic and accommodate heterotypic polymerization. These observations offer a framework for understanding the function of LC sequences as well as an organizing principle for cellular structures that are not membrane bound., (Copyright © 2012 Elsevier Inc. All rights reserved.)

Published

2012

24. Three-dimensional docking in the MAPK p38α.

Author

Goldsmith EJ

Subjects

Amino Acid Motifs, Animals, Dual-Specificity Phosphatases chemistry, Dual-Specificity Phosphatases metabolism, Humans, MAP Kinase Signaling System physiology, Mitogen-Activated Protein Kinase 14 metabolism, Mitogen-Activated Protein Kinase Phosphatases chemistry, Mitogen-Activated Protein Kinase Phosphatases metabolism, Protein Structure, Tertiary, Mitogen-Activated Protein Kinase 14 chemistry, Models, Molecular

Abstract

Mitogen-activated protein kinases (MAPKs) are central players in eukaryotic signaling circuitry and interact with numerous other proteins. The structure of a MAPK with a kinase-binding domain (KBD) from a MAPK phosphatase, MKP5, reveals that the contacts with the MAPK are made with the folded three-dimensional KBD, although the KBD occupies the same binding site on the kinase as canonical linear docking motifs found in substrates and MAPK kinases. This structure offers insights into the action of MKP5 and other MKPs.

Published

2011

25. Map2k4 functions as a tumor suppressor in lung adenocarcinoma and inhibits tumor cell invasion by decreasing peroxisome proliferator-activated receptor γ2 expression.

Author

Ahn YH, Yang Y, Gibbons DL, Creighton CJ, Yang F, Wistuba II, Lin W, Thilaganathan N, Alvarez CA, Roybal J, Goldsmith EJ, Tournier C, and Kurie JM

Subjects

Adenocarcinoma genetics, Adenocarcinoma pathology, Amino Acid Sequence, Animals, Base Sequence, Cell Line, Tumor, DNA Primers genetics, Enzyme Stability, Humans, Lung Neoplasms genetics, Lung Neoplasms pathology, MAP Kinase Kinase 4 chemistry, MAP Kinase Kinase 4 genetics, Mice, Models, Molecular, Molecular Sequence Data, Mutant Proteins chemistry, Mutant Proteins genetics, Mutant Proteins metabolism, Neoplasm Invasiveness, Sequence Homology, Amino Acid, Tumor Suppressor Proteins chemistry, Tumor Suppressor Proteins genetics, Tumor Suppressor Proteins metabolism, Adenocarcinoma metabolism, Lung Neoplasms metabolism, MAP Kinase Kinase 4 metabolism, PPAR gamma metabolism

Abstract

MAP2K4 encodes a dual-specificity kinase (mitogen-activated protein kinase kinase 4, or MKK4) that is mutated in a variety of human malignancies, but the biochemical properties of the mutant kinases and their roles in tumorigenesis have not been fully elucidated. Here we showed that 8 out of 11 cancer-associated MAP2K4 mutations reduce MKK4 protein stability or impair its kinase activity. On the basis of findings from bioinformatic studies on human cancer cell lines with homozygous MAP2K4 loss, we posited that MKK4 functions as a tumor suppressor in lung adenocarcinomas that develop in mice owing to expression of mutant Kras and Tp53. Conditional Map2k4 inactivation in the bronchial epithelium of mice had no discernible effect alone but increased the multiplicity and accelerated the growth of incipient lung neoplasias induced by oncogenic Kras. MKK4 suppressed the invasion and metastasis of Kras-Tp53-mutant lung adenocarcinoma cells. MKK4 deficiency increased peroxisomal proliferator-activated receptor γ2 (PPARγ2) expression through noncanonical MKK4 substrates, and PPARγ2 enhanced tumor cell invasion. We conclude that Map2k4 functions as a tumor suppressor in lung adenocarcinoma and inhibits tumor cell invasion by decreasing PPARγ2 levels.

Published

2011

26. Structure-guided lead optimization of triazolopyrimidine-ring substituents identifies potent Plasmodium falciparum dihydroorotate dehydrogenase inhibitors with clinical candidate potential.

Author

Coteron JM, Marco M, Esquivias J, Deng X, White KL, White J, Koltun M, El Mazouni F, Kokkonda S, Katneni K, Bhamidipati R, Shackleford DM, Angulo-Barturen I, Ferrer SB, Jiménez-Díaz MB, Gamo FJ, Goldsmith EJ, Charman WN, Bathurst I, Floyd D, Matthews D, Burrows JN, Rathod PK, Charman SA, and Phillips MA

Subjects

Animals, Antimalarials chemical synthesis, Antimalarials pharmacology, Chemical Phenomena, Crystallography, X-Ray, Dihydroorotate Dehydrogenase, Drug Resistance, Humans, Mice, Plasmodium falciparum enzymology, Pyrimidines chemical synthesis, Pyrimidines pharmacokinetics, Pyrimidines pharmacology, Rats, Structure-Activity Relationship, Triazoles chemical synthesis, Triazoles pharmacokinetics, Triazoles pharmacology, Oxidoreductases Acting on CH-CH Group Donors antagonists & inhibitors, Pyrimidines chemistry, Triazoles chemistry

Abstract

Drug therapy is the mainstay of antimalarial therapy, yet current drugs are threatened by the development of resistance. In an effort to identify new potential antimalarials, we have undertaken a lead optimization program around our previously identified triazolopyrimidine-based series of Plasmodium falciparum dihydroorotate dehydrogenase (PfDHODH) inhibitors. The X-ray structure of PfDHODH was used to inform the medicinal chemistry program allowing the identification of a potent and selective inhibitor (DSM265) that acts through DHODH inhibition to kill both sensitive and drug resistant strains of the parasite. This compound has similar potency to chloroquine in the humanized SCID mouse P. falciparum model, can be synthesized by a simple route, and rodent pharmacokinetic studies demonstrated it has excellent oral bioavailability, a long half-life and low clearance. These studies have identified the first candidate in the triazolopyrimidine series to meet previously established progression criteria for efficacy and ADME properties, justifying further development of this compound toward clinical candidate status.

Published

2011

27. The third conformation of p38α MAP kinase observed in phosphorylated p38α and in solution.

Author

Akella R, Min X, Wu Q, Gardner KH, and Goldsmith EJ

Subjects

Amino Acid Sequence, Animals, Binding Sites, Crystallography, X-Ray, Mice, Mitogen-Activated Protein Kinase 14 isolation & purification, Models, Biological, Models, Molecular, Molecular Sequence Data, Nuclear Magnetic Resonance, Biomolecular, Phosphorylation physiology, Protein Binding, Protein Interaction Domains and Motifs physiology, Protein Structure, Secondary, Protein Structure, Tertiary, Solutions, Mitogen-Activated Protein Kinase 14 chemistry, Mitogen-Activated Protein Kinase 14 metabolism, Mitogen-Activated Protein Kinase Kinases metabolism

Abstract

MAPKs engage substrates, MAP2Ks, and phosphatases via a docking groove in the C-terminal domain of the kinase. Prior crystallographic studies on the unphosphorylated MAPKs p38α and ERK2 defined the docking groove and revealed long-range conformational changes affecting the activation loop and active site of the kinase induced by peptide. Solution NMR data presented here for unphosphorylated p38α with a MEK3b-derived peptide (p38α/pepMEK3b) validate these findings. Crystallograhic data from doubly phosphorylated active p38α (p38α/T∗GY∗/pepMEK3b) reveal a structure similar to unphosphorylated p38α/MEK3b, and distinct from phosphorylated p38γ (p38γ/T∗GY∗) and ERK2 (ERK2/T∗EY∗). The structure supports the idea that MAP kinases adopt three distinct conformations: unphosphorylated, phosphorylated, and a docking peptide-induced form., (Copyright © 2010 Elsevier Ltd. All rights reserved.)

Published

2010

28. Novel inhibitors of Plasmodium falciparum dihydroorotate dehydrogenase with anti-malarial activity in the mouse model.

Author

Booker ML, Bastos CM, Kramer ML, Barker RH Jr, Skerlj R, Sidhu AB, Deng X, Celatka C, Cortese JF, Guerrero Bravo JE, Crespo Llado KN, Serrano AE, Angulo-Barturen I, Jiménez-Díaz MB, Viera S, Garuti H, Wittlin S, Papastogiannidis P, Lin JW, Janse CJ, Khan SM, Duraisingh M, Coleman B, Goldsmith EJ, Phillips MA, Munoz B, Wirth DF, Klinger JD, Wiegand R, and Sybertz E

Subjects

Animals, Cell Line, Dihydroorotate Dehydrogenase, Disease Models, Animal, Drug Evaluation, Preclinical, Humans, Imidazoles pharmacology, Mice, Mice, Inbred NOD, Mice, SCID, Plasmodium berghei enzymology, Plasmodium vivax enzymology, Rats, Antimalarials pharmacology, Enzyme Inhibitors pharmacology, Malaria, Falciparum drug therapy, Malaria, Falciparum enzymology, Oxidoreductases Acting on CH-CH Group Donors antagonists & inhibitors, Plasmodium falciparum enzymology, Protozoan Proteins antagonists & inhibitors

Abstract

Plasmodium falciparum, the causative agent of the most deadly form of human malaria, is unable to salvage pyrimidines and must rely on de novo biosynthesis for survival. Dihydroorotate dehydrogenase (DHODH) catalyzes the rate-limiting step in the pyrimidine biosynthetic pathway and represents a potential target for anti-malarial therapy. A high throughput screen and subsequent medicinal chemistry program identified a series of N-alkyl-5-(1H-benzimidazol-1-yl)thiophene-2-carboxamides with low nanomolar in vitro potency against DHODH from P. falciparum, P. vivax, and P. berghei. The compounds were selective for the parasite enzymes over human DHODH, and x-ray structural data on the analog Genz-667348, demonstrated that species selectivity could be attributed to amino acid differences in the inhibitor-binding site. Compounds from this series demonstrated in vitro potency against the 3D7 and Dd2 strains of P. falciparum, good tolerability and oral exposure in the mouse, and ED(50) values in the 4-day murine P. berghei efficacy model of 13-21 mg/kg/day with oral twice-daily dosing. In particular, treatment with Genz-667348 at 100 mg/kg/day resulted in sterile cure. Two recent analogs of Genz-667348 are currently undergoing pilot toxicity testing to determine suitability as clinical development candidates.

Published

2010

29. Evolution of substrate specificity within a diverse family of beta/alpha-barrel-fold basic amino acid decarboxylases: X-ray structure determination of enzymes with specificity for L-arginine and carboxynorspermidine.

Author

Deng X, Lee J, Michael AJ, Tomchick DR, Goldsmith EJ, and Phillips MA

Subjects

Amino Acid Sequence, Amino Acids, Basic metabolism, Bacterial Proteins chemistry, Bacterial Proteins metabolism, Kinetics, Molecular Sequence Data, Protein Structure, Secondary, Sequence Homology, Amino Acid, Substrate Specificity, Carboxy-Lyases chemistry, Carboxy-Lyases metabolism, Crystallography, X-Ray methods, Evolution, Molecular

Abstract

Pyridoxal 5'-phosphate (PLP)-dependent basic amino acid decarboxylases from the beta/alpha-barrel-fold class (group IV) exist in most organisms and catalyze the decarboxylation of diverse substrates, essential for polyamine and lysine biosynthesis. Herein we describe the first x-ray structure determination of bacterial biosynthetic arginine decarboxylase (ADC) and carboxynorspermidine decarboxylase (CANSDC) to 2.3- and 2.0-A resolution, solved as product complexes with agmatine and norspermidine. Despite low overall sequence identity, the monomeric and dimeric structures are similar to other enzymes in the family, with the active sites formed between the beta/alpha-barrel domain of one subunit and the beta-barrel of the other. ADC contains both a unique interdomain insertion (4-helical bundle) and a C-terminal extension (3-helical bundle) and it packs as a tetramer in the asymmetric unit with the insertions forming part of the dimer and tetramer interfaces. Analytical ultracentrifugation studies confirmed that the ADC solution structure is a tetramer. Specificity for different basic amino acids appears to arise primarily from changes in the position of, and amino acid replacements in, a helix in the beta-barrel domain we refer to as the "specificity helix." Additionally, in CANSDC a key acidic residue that interacts with the distal amino group of other substrates is replaced by Leu(314), which interacts with the aliphatic portion of norspermidine. Neither product, agmatine in ADC nor norspermidine in CANSDC, form a Schiff base to pyridoxal 5'-phosphate, suggesting that the product complexes may promote product release by slowing the back reaction. These studies provide insight into the structural basis for the evolution of novel function within a common structural-fold.

Published

2010

30. Structural studies of MAP Kinase cascade components.

Author

Goldsmith EJ, Min X, He H, and Zhou T

Subjects

Animals, Cell Line, Crystallization, Escherichia coli genetics, Humans, MAP Kinase Kinase 6 genetics, MAP Kinase Kinase 6 isolation & purification, MAP Kinase Kinase Kinases genetics, MAP Kinase Kinase Kinases isolation & purification, Mice, Phosphorylation, Rats, Selenomethionine metabolism, MAP Kinase Kinase 6 chemistry, MAP Kinase Kinase 6 metabolism, MAP Kinase Kinase Kinases chemistry, MAP Kinase Kinase Kinases metabolism, MAP Kinase Signaling System

Abstract

MAPK cascade components have been the subject of structural analysis, advancing our understanding of how these enzymes are activated and how they interact. A surprising finding has been that unique inactive conformers are adopted by many of these kinases. These inactive conformers are interesting and often require experimental phases to determine their crystal structures because molecular replacement techniques are not successful. Here, we describe the preparation of MAP2K MEK6 and MAP3K TAO2 substituted with selenomethionine (SeMet) for de novo phasing. TAO2 and SeMet TAO2 were expressed in insect cells.

Published

2010

31. Structural plasticity of malaria dihydroorotate dehydrogenase allows selective binding of diverse chemical scaffolds.

Author

Deng X, Gujjar R, El Mazouni F, Kaminsky W, Malmquist NA, Goldsmith EJ, Rathod PK, and Phillips MA

Subjects

Amino Acid Sequence, Animals, Antimalarials chemistry, Antimalarials metabolism, Antimalarials pharmacology, Binding Sites, Crystallography, X-Ray, Dihydroorotate Dehydrogenase, Humans, Hydrogen Bonding, Malaria, Falciparum parasitology, Malaria, Falciparum prevention & control, Models, Molecular, Molecular Sequence Data, Molecular Structure, Oxidoreductases Acting on CH-CH Group Donors antagonists & inhibitors, Oxidoreductases Acting on CH-CH Group Donors chemistry, Plasmodium falciparum drug effects, Plasmodium falciparum genetics, Protein Binding, Protein Structure, Secondary, Protein Structure, Tertiary, Protozoan Proteins antagonists & inhibitors, Protozoan Proteins chemistry, Pyrimidines chemistry, Pyrimidines metabolism, Pyrimidines pharmacology, Sequence Homology, Amino Acid, Structure-Activity Relationship, Triazoles chemistry, Triazoles metabolism, Triazoles pharmacology, Oxidoreductases Acting on CH-CH Group Donors metabolism, Plasmodium falciparum enzymology, Protozoan Proteins metabolism

Abstract

Malaria remains a major global health burden and current drug therapies are compromised by resistance. Plasmodium falciparum dihydroorotate dehydrogenase (PfDHODH) was validated as a new drug target through the identification of potent and selective triazolopyrimidine-based DHODH inhibitors with anti-malarial activity in vivo. Here we report x-ray structure determination of PfDHODH bound to three inhibitors from this series, representing the first of the enzyme bound to malaria specific inhibitors. We demonstrate that conformational flexibility results in an unexpected binding mode identifying a new hydrophobic pocket on the enzyme. Importantly this plasticity allows PfDHODH to bind inhibitors from different chemical classes and to accommodate inhibitor modifications during lead optimization, increasing the value of PfDHODH as a drug target. A second discovery, based on small molecule crystallography, is that the triazolopyrimidines populate a resonance form that promotes charge separation. These intrinsic dipoles allow formation of energetically favorable H-bond interactions with the enzyme. The importance of delocalization to binding affinity was supported by site-directed mutagenesis and the demonstration that triazolopyrimidine analogs that lack this intrinsic dipole are inactive. Finally, the PfDHODH-triazolopyrimidine bound structures provide considerable new insight into species-selective inhibitor binding in this enzyme family. Together, these studies will directly impact efforts to exploit PfDHODH for the development of anti-malarial chemotherapy.

Published

2009

32. Natural language query in the biochemistry and molecular biology domains based on cognition search™.

Author

Goldsmith EJ, Mendiratta S, Akella R, and Dahlgren K

Abstract

Motivation: With the increasing volume of scientific papers and heterogeneous nomenclature in the biomedical literature, it is apparent that an improvement over standard pattern matching available in existing search engines is required. Cognition Search Information Retrieval (CSIR) is a natural language processing (NLP) technology that possesses a large dictionary (lexicon) and large semantic databases, such that search can be based on meaning. Encoded synonymy, ontological relationships, phrases, and seeds for word sense disambiguation offer significant improvement over pattern matching. Thus, the CSIR has the right architecture to form the basis for a scientific search engine., Result: Here we have augmented CSIR to improve access to the MEDLINE database of scientific abstracts. New biochemical, molecular biological and medical language and acronyms were introduced from curated web-based sources. The resulting system was used to interpret MEDLINE abstracts. Meaning-based search of MEDLINE abstracts yields high precision (estimated at >90%), and high recall (estimated at >90%), where synonym, ontology, phrases and sense seeds have been encoded. The present implementation can be found at http://MEDLINE.cognition.com., Contact: Elizabeth.goldsmith@UTsouthwestern.edu Kathleen.dahlgren@cognition.com.

Published

2009

33. Crystal structure of domain-swapped STE20 OSR1 kinase domain.

Author

Lee SJ, Cobb MH, and Goldsmith EJ

Subjects

Catalytic Domain, Conserved Sequence, Crystallography, X-Ray, Humans, Models, Molecular, Protein Binding, Protein Interaction Domains and Motifs, Protein Kinases chemistry, Protein Kinases genetics, Protein Kinases metabolism, Protein Multimerization, Protein Serine-Threonine Kinases genetics, Protein Serine-Threonine Kinases metabolism, Sequence Alignment, Protein Serine-Threonine Kinases chemistry, Protein Structure, Tertiary

Abstract

OSR1 (oxidative stress-responsive-1) and SPAK (Ste20/Sps1-related proline/alanine-rich kinase) belong to the GCK-VI subfamily of Ste20 group kinases. OSR1 and SPAK are key regulators of NKCCs (Na(+)/K(+)/2Cl(-) cotransporters) and activated by WNK family members (with-no-lysine kinase), mutations of which are known to cause Gordon syndrome, an autosomal dominant form of inherited hypertension. The crystal structure of OSR1 kinase domain has been solved at 2.25 A. OSR1 forms a domain-swapped dimer in an inactive conformation, in which P+1 loop and alphaEF helix are swapped between dimer-related monomers. Structural alignment with nonswapped Ste20 TAO2 kinase indicates that the integrity of chemical interactions in the kinase domain is well preserved in the domain-swapped interfaces. The OSR1 kinase domain has now been added to a growing list of domain-swapped protein kinases recently reported, suggesting that the domain-swapping event provides an additional layer of complexity in regulating protein kinase activity.

Published

2009

34. The structure of the MAP2K MEK6 reveals an autoinhibitory dimer.

Author

Min X, Akella R, He H, Humphreys JM, Tsutakawa SE, Lee SJ, Tainer JA, Cobb MH, and Goldsmith EJ

Subjects

Amino Acid Sequence, Animals, Crystallography, X-Ray, Dimerization, Enzyme Activation, Humans, MAP Kinase Kinase 1 antagonists & inhibitors, MAP Kinase Kinase 1 metabolism, MAP Kinase Kinase 6 antagonists & inhibitors, MAP Kinase Kinase 6 metabolism, Mice, Models, Molecular, Molecular Mimicry, Molecular Sequence Data, Phosphorylation, Protein Conformation, Rats, Scattering, Radiation, Sequence Homology, Amino Acid, Substrate Specificity, MAP Kinase Kinase 1 chemistry, MAP Kinase Kinase 6 chemistry

Abstract

MAP2Ks are dual-specificity protein kinases functioning at the center of three-tiered MAP kinase modules. The structure of the kinase domain of the MAP2K MEK6 with phosphorylation site mimetic aspartic acid mutations (MEK6/DeltaN/DD) has been solved at 2.3 angstroms resolution. The structure reveals an autoinhibited elongated ellipsoidal dimer. The enzyme adopts an inactive conformation, based upon structural queues, despite the phosphomimetic mutations. Gel filtration and small-angle X-ray scattering analysis confirm that the crystallographically observed ellipsoidal dimer is a feature of MEK6/DeltaN/DD and full-length unphosphorylated wild-type MEK6 in solution. The interface includes the phosphate binding ribbon of each subunit, part of the activation loop, and a rare "arginine stack" between symmetry-related arginine residues in the N-terminal lobe. The autoinhibited structure likely confers specificity on active MAP2Ks. The dimer may also serve the function in unphosphorylated MEK6 of preventing activation loop phosphorylation by inappropriate kinases.

Published

2009

35. Unique MAP Kinase binding sites.

Author

Akella R, Moon TM, and Goldsmith EJ

Subjects

Amino Acid Motifs, Animals, Antineoplastic Agents metabolism, Binding Sites, Crystallography, X-Ray, Flavonoids metabolism, Humans, Mitogen-Activated Protein Kinase 1 chemistry, Mitogen-Activated Protein Kinase 1 metabolism, Protein Binding, Protein Conformation, Protein Kinase Inhibitors metabolism, Sulindac analogs & derivatives, Sulindac metabolism, p38 Mitogen-Activated Protein Kinases chemistry, p38 Mitogen-Activated Protein Kinases metabolism, Mitogen-Activated Protein Kinases chemistry, Mitogen-Activated Protein Kinases metabolism

Abstract

Map kinases are drug targets for autoimmune disease, cancer, and apoptosis-related diseases. Drug discovery efforts have developed MAP kinase inhibitors directed toward the ATP binding site and neighboring "DFG-out" site, both of which are targets for inhibitors of other protein kinases. On the other hand, MAP kinases have unique substrate and small molecule binding sites that could serve as inhibition sites. The substrate and processing enzyme D-motif binding site is present in all MAP kinases, and has many features of a good small molecule binding site. Further, the MAP kinase p38alpha has a binding site near its C-terminus discovered in crystallographic studies. Finally, the MAP kinases ERK2 and p38alpha have a second substrate binding site, the FXFP binding site that is exposed in active ERK2 and the D-motif peptide induced conformation of MAP kinases. Crystallographic evidence of these latter two binding sites is presented.

Published

2008

36. Substrate and docking interactions in serine/threonine protein kinases.

Author

Goldsmith EJ, Akella R, Min X, Zhou T, and Humphreys JM

Subjects

Fungi enzymology, Models, Molecular, Protein Conformation, Substrate Specificity, Protein Serine-Threonine Kinases chemistry, Protein Serine-Threonine Kinases metabolism

Published

2007

37. Mutations in ERK2 binding sites affect nuclear entry.

Author

Yazicioglu MN, Goad DL, Ranganathan A, Whitehurst AW, Goldsmith EJ, and Cobb MH

Subjects

Active Transport, Cell Nucleus physiology, Amino Acid Motifs genetics, Animals, Binding Sites genetics, Carrier Proteins genetics, Carrier Proteins metabolism, Cell Nucleus genetics, HeLa Cells, Humans, Mitogen-Activated Protein Kinase 1 genetics, Nuclear Pore Complex Proteins genetics, Rats, Recombinant Proteins genetics, Recombinant Proteins metabolism, Amino Acid Substitution, Cell Nucleus enzymology, Mitogen-Activated Protein Kinase 1 metabolism, Mutation, Missense, Nuclear Pore Complex Proteins metabolism

Abstract

The MAPK ERK2 can enter and exit the nucleus by an energy-independent process that is facilitated by direct interactions with nuclear pore proteins. Several studies also suggest that the localization of ERK2 can be influenced by carrier proteins. Using import reconstitution assays, we examined a group of ERK2 mutants defective in known protein interactions to determine structural properties of ERK2 that contribute to its nuclear entry. ERK2 mutants defective in binding to substrates near the active site or to basic/hydrophobic docking (D) motifs were imported normally. Several ERK2 mutants defective in interactions with FXF motifs displayed slowed rates of nuclear import. The import-impaired mutants also showed reduced binding to a recombinant C-terminal fragment of nucleoporin 153 that is rich in FXF motifs. Despite the deficit revealed in some mutants via reconstitution assays, all but one of the ERK2 mutants accumulated in nuclei of stimulated cells in a manner comparable with the wild type protein; the mutant most defective in import remained in the cytoplasm. These results further support the idea that direct interactions with nucleoporins are involved in ERK2 nuclear entry and that multiple events contribute to the ligand-dependent relocalization of these protein kinases.

Published

2007

38. Phylogenetic diversity and the structural basis of substrate specificity in the beta/alpha-barrel fold basic amino acid decarboxylases.

Author

Lee J, Michael AJ, Martynowski D, Goldsmith EJ, and Phillips MA

Subjects

Amino Acid Sequence, Bacteria classification, Eflornithine pharmacology, Molecular Sequence Data, Ornithine Decarboxylase metabolism, Ornithine Decarboxylase Inhibitors, Phylogeny, Substrate Specificity, Bacteria enzymology, Ornithine Decarboxylase chemistry, Protein Folding

Abstract

The beta/alpha-barrel fold type basic amino acid decarboxylases include eukaryotic ornithine decarboxylases (ODC) and bacterial and plant enzymes with activity on L-arginine and meso-diaminopimelate. These enzymes catalyze essential steps in polyamine and lysine biosynthesis. Phylogenetic analysis suggests that diverse bacterial species also contain ODC-like enzymes from this fold type. However, in comparison with the eukaryotic ODCs, amino acid differences were identified in the sequence of the 3(10)-helix that forms a key specificity element in the active site, suggesting they might function on novel substrates. Putative decarboxylases from a phylogenetically diverse range of bacteria were characterized to determine their substrate preference. Enzymes from species within Methanosarcina, Pseudomonas, Bartonella, Nitrosomonas, Thermotoga, and Aquifex showed a strong preference for L-ornithine, whereas the enzyme from Vibrio vulnificus (VvL/ODC) had dual specificity functioning well on both L-ornithine and L-lysine. The x-ray structure of VvL/ODC was solved in the presence of the reaction products putrescine and cadaverine to 1.7 and 2.15A, respectively. The overall structure is similar to eukaryotic ODC; however, reorientation of the 3(10)-helix enlarging the substrate binding pocket allows L-lysine to be accommodated. The structure of the putrescine-bound enzyme suggests that a bridging water molecule between the shorter L-ornithine and key active site residues provides the structural basis for VvL/ODC to also function on this substrate. Our data demonstrate that there is greater structural and functional diversity in bacterial polyamine biosynthetic decarboxylases than previously suspected.

Published

2007

39. X-ray structure of Paramecium bursaria Chlorella virus arginine decarboxylase: insight into the structural basis for substrate specificity.

Author

Shah R, Akella R, Goldsmith EJ, and Phillips MA

Subjects

Agmatine chemistry, Amino Acid Sequence, Animals, Crystallography, X-Ray, Models, Molecular, Molecular Sequence Data, Protein Conformation, Substrate Specificity, Carboxy-Lyases chemistry, Chlorella virology, Paramecium virology

Abstract

The group IV pyridoxal-5'-phosphate (PLP)-dependent decarboxylases belong to the beta/alpha barrel structural family, and include enzymes with substrate specificity for a range of basic amino acids. A unique homolog of this family, the Paramecium bursaria Chlorella virus arginine decarboxylase (cvADC), shares about 40% amino acid sequence identity with the eukaryotic ornithine decarboxylases (ODCs). The X-ray structure of cvADC has been solved to 1.95 and 1.8 A resolution for the free and agmatine (product)-bound enzymes. The global structural differences between cvADC and eukaryotic ODC are minimal (rmsd of 1.2-1.4 A); however, the active site has significant structural rearrangements. The key "specificity element," is identified as the 310-helix that contains and positions substrate-binding residues such as E296 cvADC (D332 in T. brucei ODC). In comparison to the ODC structures, the 310-helix in cvADC is shifted over 2 A away from the PLP cofactor, thus accommodating the larger arginine substrate. Within the context of this conserved fold, the protein is designed to be flexible in the positioning and amino acid sequence of the 310-helix, providing a mechanism to evolve different substrate preferences within the family without large structural rearrangements. Also, in the structure, the "K148-loop" (homologous to the "K169-loop" of ODC) is observed in a closed, substrate-bound conformation for the first time. Apparently the K148 loop is a mobile loop, analogous to those observed in triose phosphate isomerase and tryptophan synthetase. In conjunction with prior structural studies these data predict that this loop adopts different conformations throughout the catalytic cycle, and that loop movement may be kinetically linked to the rate-limiting step of product release.

Published

2007

40. Characterization of mitogen-activated protein kinase (MAPK) dimers.

Author

Wilsbacher JL, Juang YC, Khokhlatchev AV, Gallagher E, Binns D, Goldsmith EJ, and Cobb MH

Subjects

Amino Acid Sequence, Chromatography, Gel, Dimerization, Electrophoresis, Polyacrylamide Gel, Mitogen-Activated Protein Kinases chemistry, Models, Molecular, Molecular Sequence Data, Protein Conformation, Sequence Homology, Amino Acid, Mitogen-Activated Protein Kinases metabolism

Abstract

Phosphorylated ERK2 has an increased capacity to form homodimers relative to unphosphorylated ERK2. We have characterized the nature of the ERK2 dimer and have mutated residues in the crystal dimer interface to examine the impact of dimerization on ERK2 activity. Analysis of the mutants by gel filtration indicates that at least five residues must be mutated simultaneously to produce an ERK2 mutant that is predominantly monomeric. Mutants, whether monomers or dimers, have specific protein kinase activities under fixed assay conditions that are roughly equivalent to wild-type ERK2. The ratio of dimers to monomers is increased as the salt concentration increases, consistent with a strong hydrophobic contribution to the energy of dimer formation. ERK2 dimerization also requires divalent cations. Sedimentation analysis indicates that the related c-Jun N-terminal kinase SAPKalphaI/JNK2 also forms dimers, but dimerization displays no dependence on phosphorylation; the unphosphorylated and phosphorylated forms of the kinase behave similarly, with low micromolar dimer dissociation constants.

Published

2006

41. Crystallization of MAP kinases.

Author

Lee SJ, Zhou T, and Goldsmith EJ

Subjects

Animals, Bacteria genetics, Baculoviridae genetics, Enzyme Inhibitors chemistry, Enzyme Inhibitors metabolism, Insecta cytology, Mitogen-Activated Protein Kinases antagonists & inhibitors, Mitogen-Activated Protein Kinases genetics, Mitogen-Activated Protein Kinases metabolism, Mutagenesis, Phosphorylation, Protein Engineering methods, Recombinant Proteins genetics, Recombinant Proteins isolation & purification, Recombinant Proteins metabolism, Crystallization methods, Mitogen-Activated Protein Kinases chemistry

Abstract

X-ray structural studies of MAP kinases and MAP kinase module components are elucidating how kinase activity is regulated and how specificity of signaling is conferred. In the past decade, MAP kinases have been crystallized in their active, phosphorylated forms or low-activity, unphosphorylated forms, as well as in the presence of binding partners such as docking peptides and inhibitors. Crystallization has been achieved via diverse strategies including control of phosphorylation, coding sequence modification, incorporation of tags for purification, and use of a variety of cell-types for protein expression. Recently, interest has been focused on use of crystallography for lead optimization in the development for pharmacological inhibitors on MAP kinases. Further, some success has been gained in crystallizing the MAP kinase activators MAP2Ks and MAP3K kinase domains. This review describes the key methods that have been utilized to crystallize MAP kinases and MAP kinase pathway components.

Published

2006

42. Crystal structure of the MAP3K TAO2 kinase domain bound by an inhibitor staurosporine.

Author

Zhou TJ, Sun LG, Gao Y, and Goldsmith EJ

Subjects

Animals, Baculoviridae, Crystallography, X-Ray, Enzyme Inhibitors pharmacology, Inhibitory Concentration 50, Insecta, MAP Kinase Signaling System, Models, Molecular, Protein Conformation, Protein Serine-Threonine Kinases, Protein Structure, Tertiary, Rats, MAP Kinase Kinase Kinases chemistry, Staurosporine pharmacology

Abstract

Mitogen-activated protein kinase (MAPK) signal transduction pathways are ubiquitous in eukaryotic cells, which transfer signals from the cell surface to the nucleus, controlling multiple cellular programs. MAPKs are activated by MAPK kinases [MAP2Ks or MAP/extracellular signal-regulated kinase (ERK) kinases (MEK)], which in turn are activated by MAPK kinase kinases (MAP3Ks). TAO2 is a MAP3K level kinase that activates the MAP2Ks MEK3 and MEK6 to activate p38 MAPKs. Because p38 MAPKs are key regulators of expression of inflammatory cytokines, they appear to be involved in human diseases such as asthma and autoimmunity. As an upstream activator of p38s, TAO2 represents a potential drug target. Here we report the crystal structure of active TAO2 kinase domain in complex with staurosporine, a broad-range protein kinase inhibitor that inhibits TAO2 with an IC50 of 3 mM. The structure reveals that staurosporine occupies the position where the adenosine of ATP binds in TAO2, and the binding of the inhibitor mimics many features of ATP binding. Both polar and nonpolar interactions contribute to the enzyme-inhibitor recognition. Staurosporine induces conformational changes in TAO2 residues that surround the inhibitor molecule, but causes very limited global changes in the kinase. The structure provides atomic details for TAO2-staurosporine interactions, and explains the relatively low potency of staurosporine against TAO2. The structure presented here should aid in the design of inhibitors specific to TAO2 and related kinases.

Published

2006

43. Docking interactions induce exposure of activation loop in the MAP kinase ERK2.

Author

Zhou T, Sun L, Humphreys J, and Goldsmith EJ

Subjects

Amino Acid Motifs, Amino Acid Sequence, Animals, Enzyme Activation, Intracellular Signaling Peptides and Proteins chemistry, Mitogen-Activated Protein Kinase 1 metabolism, Molecular Sequence Data, Protein Conformation, Protein Interaction Mapping, Protein Tyrosine Phosphatase, Non-Receptor Type 6, Protein Tyrosine Phosphatases chemistry, Mitogen-Activated Protein Kinase 1 chemistry

Abstract

MAP kinases bind activating kinases, phosphatases, and substrates through docking interactions. Here, we report a 1.9 A crystallographic analysis of inactive ERK2 bound to a "D motif" docking peptide (pepHePTP) derived from hematopoietic tyrosine phosphatase, a negative regulator of ERK2. In this complex, the complete D motif interaction defined by mutagenic analysis is observed, including extensive electrostatic interactions with the "CD" site of the kinase. Large conformational changes occur in the activation loop where the dual phosphorylation sites, which are buried in the inactive form of ERK2, become exposed to solvent in the complex. Similar conformational changes occur in a complex between ERK2 and a MEK2 (MAP/ERK kinase-2)-derived D motif peptide (pepMEK2). D motif peptides are known to bind homologous loci in the MAP kinases p38alpha and JNK1, also inducing conformational changes in these enzymes. However, the binding interactions and conformational changes are unique to each, thus contributing to specificity among MAP kinases.

Published

2006

44. Yersinia YopJ acetylates and inhibits kinase activation by blocking phosphorylation.

Author

Mukherjee S, Keitany G, Li Y, Wang Y, Ball HL, Goldsmith EJ, and Orth K

Subjects

Acetyl Coenzyme A metabolism, Acetylation, Acetyltransferases metabolism, Catalytic Domain, Cell Line, Cell-Free System, Electrophoresis, Polyacrylamide Gel, Enzyme Activation, Extracellular Signal-Regulated MAP Kinases metabolism, Humans, MAP Kinase Kinase 6 chemistry, MAP Kinase Signaling System, NF-kappa B metabolism, Phosphorylation, Recombinant Proteins metabolism, Serine metabolism, Signal Transduction, Threonine metabolism, Yersinia pathogenicity, Bacterial Proteins metabolism, I-kappa B Kinase metabolism, MAP Kinase Kinase 6 metabolism, Yersinia metabolism

Abstract

Yersinia species use a variety of type III effector proteins to target eukaryotic signaling systems. The effector YopJ inhibits mitogen-activated protein kinase (MAPK) and the nuclear factor kappaB (NFkappaB) signaling pathways used in innate immune response by preventing activation of the family of MAPK kinases (MAPKK). We show that YopJ acted as an acetyltransferase, using acetyl-coenzyme A (CoA) to modify the critical serine and threonine residues in the activation loop of MAPKK6 and thereby blocking phosphorylation. The acetylation on MAPKK6 directly competed with phosphorylation, preventing activation of the modified protein. This covalent modification may be used as a general regulatory mechanism in biological signaling.

Published

2006

45. Determinants that control the specific interactions between TAB1 and p38alpha.

Author

Zhou H, Zheng M, Chen J, Xie C, Kolatkar AR, Zarubin T, Ye Z, Akella R, Lin S, Goldsmith EJ, and Han J

Subjects

Adaptor Proteins, Signal Transducing chemistry, Alanine metabolism, Amino Acid Motifs, Amino Acid Sequence, Amino Acid Substitution, Binding Sites, Blotting, Western, Cell Culture Techniques, Cell Line, Circular Dichroism, DNA Mutational Analysis, Enzyme Activation, Escherichia coli genetics, Gene Deletion, Genes, Reporter, Humans, Luciferases metabolism, Mass Spectrometry, Mitogen-Activated Protein Kinase 14 analysis, Mitogen-Activated Protein Kinase 14 chemistry, Models, Molecular, Molecular Sequence Data, Point Mutation, Precipitin Tests, Protein Binding, Protein Conformation, Protein Structure, Tertiary, Recombinant Fusion Proteins analysis, Sequence Homology, Amino Acid, Spectrum Analysis, Threonine chemistry, Transfection, beta-Galactosidase metabolism, Adaptor Proteins, Signal Transducing genetics, Adaptor Proteins, Signal Transducing metabolism, Mitogen-Activated Protein Kinase 14 genetics, Mitogen-Activated Protein Kinase 14 metabolism

Abstract

Previous studies have revealed that transforming growth factor-beta-activated protein kinase 1 (TAB1) interacts with p38alpha and induces p38alpha autophosphorylation. Here, we examine the sequence requirements in TAB1 and p38alpha that drive their interaction. Deletion and point mutations in TAB1 reveal that a proline residue in the C terminus of TAB1 (Pro412) is necessary for its interaction with p38alpha. Furthermore, a cryptic D-domain-like docking site was identified adjacent to the N terminus of Pro412, putting Pro412 in the phi(B)+3 position of the docking site. Through mutational analysis, we found that the previously identified hydrophobic docking groove in p38alpha is involved in this interaction, whereas the CD domain and ED domain are not. Furthermore, chimeric analysis with p38beta (which does not bind to TAB1) revealed a previously unidentified locus of p38alpha comprising Thr218 and Ile275 that is essential for specific binding of p38alpha to TAB1. Converting either of these residues to the corresponding amino acid of p38beta abolishes p38alpha interaction with TAB1. These p38alpha mutants still can be fully activated by p38alpha upstream activating kinase mitogen-activated protein kinase kinase 6, but their basal activity and activation in response to some extracellular stimuli are reduced. Adjacent to Thr218 and Ile275 is a site where large conformational changes occur in the presence of docking-site peptides derived from p38alpha substrates and activators. This suggests that TAB1-induced autophosphorylation of p38alpha results from conformational changes that are similar but unique to those seen in p38alpha interactions with its substrates and activating kinases.

Published

2006

46. Properties of WNK1 and implications for other family members.

Author

Lenertz LY, Lee BH, Min X, Xu BE, Wedin K, Earnest S, Goldsmith EJ, and Cobb MH

Subjects

Animals, Cell Line, Cell Line, Tumor, Epithelial Cells pathology, Humans, Hypertension etiology, Hypotonic Solutions pharmacology, Intracellular Signaling Peptides and Proteins, Minor Histocompatibility Antigens, Phosphorylation, Protein Serine-Threonine Kinases chemistry, Protein Serine-Threonine Kinases metabolism, Protein Structure, Tertiary, Stress, Physiological metabolism, WNK Lysine-Deficient Protein Kinase 1, Protein Serine-Threonine Kinases physiology

Abstract

WNKs are large serine/threonine protein kinases structurally distinct from all other members of the protein kinase superfamily. Of the four human WNK family members, WNK1 and WNK4 have been linked to a hereditary form of hypertension, pseudohypoaldosteronism type II. We characterized the biochemical properties and regulation of WNK1 that may contribute to its physiological activities and abnormal function in disease. We showed that WNK1 is activated by hypertonic stress in kidney epithelial cells and in breast and colon cancer cell lines. In addition, hypotonic stress also led to a modest increase in WNK1 activity. Gel filtration suggested that WNK1 exists as a tetramer, and yeast two-hybrid data showed that the N terminus of WNK1 (residues 1-222) interacts with residues 481-660, which includes the WNK1 autoinhibitory domain and a C-terminal coiled-coil domain. Although cell biological studies have suggested a functional interaction between WNK1 and WNK4, we found no evidence of stable interactions between these kinases. However, WNK1 phosphorylated both WNK4 and WNK2. In addition, the WNK1 autoinhibitory domain inhibited the catalytic activity of these WNKs. These findings suggest potential mechanisms for interconnected regulation of WNK family members.

Published

2005

47. WNK1: analysis of protein kinase structure, downstream targets, and potential roles in hypertension.

Author

Xu BE, Lee BH, Min X, Lenertz L, Heise CJ, Stippec S, Goldsmith EJ, and Cobb MH

Subjects

Animals, Brain metabolism, COS Cells, Calcium-Binding Proteins metabolism, Cell Line, Tumor, Cell Membrane metabolism, Crystallography, X-Ray, DNA, Complementary metabolism, Electrolytes, Enzyme Activation, Gene Deletion, Gene Library, Humans, Intracellular Signaling Peptides and Proteins, Ligands, MAP Kinase Signaling System, Membrane Glycoproteins metabolism, Minor Histocompatibility Antigens, Mitogen-Activated Protein Kinase 7 metabolism, Models, Biological, Nerve Tissue Proteins metabolism, Protein Conformation, Protein Serine-Threonine Kinases genetics, Protein Structure, Tertiary, Pseudohypoaldosteronism genetics, RNA Interference, Synaptotagmins, Two-Hybrid System Techniques, WNK Lysine-Deficient Protein Kinase 1, Protein Serine-Threonine Kinases chemistry, Protein Serine-Threonine Kinases physiology

Abstract

The WNK kinases are a recently discovered family of serine-threonine kinases that have been shown to play an essential role in the regulation of electrolyte homeostasis. Intronic deletions in the WNK1 gene result in its overexpression and lead to pseudohypoaldosteronism type II, a disease with salt-sensitive hypertension and hyperkalemia. This review focuses on the recent evidence elucidating the structure of the kinase domain of WNK1 and functions of these kinases in normal and disease physiology. Their functions have implications for understanding the biochemical mechanism that could lead to the retention or insertion of proteins in the plasma membrane. The WNK kinases may be able to influence ion homeostasis through its effects on synaptotagmin function.

Published

2005

48. Multiple active site conformations revealed by distant site mutation in ornithine decarboxylase.

Author

Jackson LK, Baldwin J, Akella R, Goldsmith EJ, and Phillips MA

Subjects

Alanine genetics, Animals, Binding Sites genetics, Crystallization, Crystallography, X-Ray, Diamines chemistry, Dimerization, Kinetics, Lysine genetics, Ornithine chemistry, Protein Conformation, Putrescine chemistry, Pyridoxal Phosphate chemistry, Spectrophotometry, Ultraviolet, Trypanosoma brucei brucei enzymology, Trypanosoma brucei brucei genetics, Mutagenesis, Site-Directed, Ornithine Decarboxylase chemistry, Ornithine Decarboxylase genetics

Abstract

Ornithine decarboxylase (ODC) is an obligate homodimer that catalyzes the pyridoxal 5'-phosphate-dependent decarboxylation of l-ornithine to putrescine, a vital step in polyamine biosynthesis. A previous mutagenic analysis of the ODC dimer interface identified several residues that were distant from the active site yet had a greater impact on catalytic activity than on dimer stability [Myers, D. P., et al. (2001) Biochemistry 40, 13230-13236]. To better understand the basis of this phenomenon, the structure of the Trypanosoma brucei ODC mutant K294A was determined to 2.15 A resolution in complex with the substrate analogue d-ornithine. This residue is distant from the reactive center (>10 A from the PLP Schiff base), and its mutation reduced catalytic efficiency by 3 kcal/mol. The X-ray structure demonstrates that the mutation increases the disorder of residues Leu-166-Ala-172 (Lys-169 loop), which normally form interactions with Lys-294 across the dimer interface. In turn, the Lys-169 loop forms interactions with the active site, suggesting that the reduced catalytic efficiency is mediated by the decreased stability of this loop. The extent of disorder varies in the four Lys-169 loops in the asymmetric unit, suggesting that the mutation has led to an increase in the population of inactive conformations. The structure also reveals that the mutation has affected the nature of the ligand-bound species. Each of the four active sites contains unusual ligands. The electron density suggests one active site contains a gem-diamine intermediate with d-ornithine; the second has density consistent with a tetrahedral adduct with glycine, and the remaining two contain tetrahedral adducts of PLP, Lys-69, and water (or hydroxide). These data also suggest that the structure is less constrained in the mutant enzyme. The observation of a gem-diamine intermediate provides insight into the conformational changes that occur during the ODC catalytic cycle.

Published

2004

49. Crystal structure of the TAO2 kinase domain: activation and specificity of a Ste20p MAP3K.

Author

Zhou T, Raman M, Gao Y, Earnest S, Chen Z, Machius M, Cobb MH, and Goldsmith EJ

Subjects

Adenosine Triphosphate metabolism, Amino Acid Sequence, Animals, Cloning, Molecular, Crystallography, Crystallography, X-Ray, Enzyme Activation, MAP Kinase Kinase 6 metabolism, MAP Kinase Kinase Kinases genetics, MAP Kinase Kinase Kinases metabolism, Molecular Sequence Data, Mutation genetics, Phosphorylation, Protein Serine-Threonine Kinases genetics, Protein Serine-Threonine Kinases metabolism, Protein Structure, Tertiary genetics, Rats, Structural Homology, Protein, Substrate Specificity, MAP Kinase Kinase Kinases chemistry

Abstract

TAO2 is a mitogen-activated protein kinase kinase kinase (MAP3K) that doubly phosphorylates and activates the MAP kinase kinases (MAP2Ks) MEK3 and MEK6. The structure of the kinase domain of TAO2 (1-320) has been solved in its phosphorylated active conformation. The structure, together with structure-based mutagenic analysis, reveals that positively charged residues in the substrate binding groove mediate the first step in the dual phosphorylation of MEK6, on the threonine residue in the motif DS*VAKT*I (*denotes phosphorylation site) of MEK6. TAO2 is a Ste20p homolog, and the structure of active TAO2, in comparison with that of low-activity p21-activated protein kinase (PAK1), a Ste20p-related MAP4K, reveals how this group of kinases is activated by phosphorylation. Finally, active TAO2 displays unusual interactions with ATP, involving, in part, a subgroup-specific C-terminal extension of TAO2. The observed interactions may be useful in making specific inhibitors of TAO kinases., (Copyright 2004 Elsevier Ltd.)

Published

2004

50. WNK1 phosphorylates synaptotagmin 2 and modulates its membrane binding.

Author

Lee BH, Min X, Heise CJ, Xu BE, Chen S, Shu H, Luby-Phelps K, Goldsmith EJ, and Cobb MH

Subjects

Animals, Binding Sites physiology, Calcium Signaling genetics, Calcium-Binding Proteins metabolism, Cell Line, Humans, Intracellular Signaling Peptides and Proteins, Minor Histocompatibility Antigens, Mutation genetics, Phosphorylation, Protein Serine-Threonine Kinases genetics, Protein Structure, Tertiary physiology, Secretory Vesicles metabolism, Synaptotagmin II, Threonine metabolism, Two-Hybrid System Techniques, WNK Lysine-Deficient Protein Kinase 1, Water-Electrolyte Balance, Cell Membrane metabolism, Nerve Tissue Proteins metabolism, Protein Binding physiology, Protein Serine-Threonine Kinases metabolism

Abstract

WNK (with no lysine [K]) protein kinases were named for their unique active site organization. Mutations in WNK1 and WNK4 cause a familial form of hypertension by undefined mechanisms. Here, we report that WNK1 selectively binds to and phosphorylates synaptotagmin 2 (Syt2) within its calcium binding C2 domains. Endogenous WNK1 and Syt2 coimmunoprecipitate and colocalize on a subset of secretory granules in INS-1 cells. Phosphorylation by WNK1 increases the amount of Ca2+ required for Syt2 binding to phospholipid vesicles; mutation of threonine 202, a WNK1 phosphorylation site, partially prevents this change. These findings suggest that phosphorylation of Syts by WNK1 can regulate Ca2+ sensing and the subsequent Ca2+-dependent interactions mediated by Syt C2 domains. These findings provide a biochemical mechanism that could lead to the retention or insertion of proteins in the plasma membrane. Interruption of this regulatory pathway may disturb membrane events that regulate ion balance., (Copyright 2004 Cell Press)

Published

2004