Your search keyword '"Ethylmaleimide metabolism"' showing total 134 results

1. Apicoplast biogenesis mediated by ATG8 requires the ATG12-ATG5-ATG16L and SNAP29 complexes in Toxoplasma gondii .

Author

Fu J, Zhao L, Pang Y, Chen H, Yamamoto H, Chen Y, Li Z, Mizushima N, and Jia H

Subjects

Animals, Humans, Ethylmaleimide metabolism, Autophagy, Ubiquitins metabolism, Protozoan Proteins genetics, Autophagy-Related Protein 12 metabolism, Qb-SNARE Proteins metabolism, Qc-SNARE Proteins, Autophagy-Related Protein 5 metabolism, Toxoplasma genetics, Toxoplasma metabolism, Apicoplasts genetics, Apicoplasts metabolism, Parasites

Abstract

In apicomplexan parasites, the macroautophagy/autophagy machinery is repurposed to maintain the plastid-like organelle apicoplast. Previously, we showed that in Toxoplasma and Plasmodium , ATG12 interacts with ATG5 in a non-covalent manner, in contrast to the covalent interaction in most organisms. However, it remained unknown whether apicomplexan parasites have functional orthologs of ATG16L1, a protein that is essential for the function of the covalent ATG12-ATG5 complex in vivo in other organisms. Furthermore, the mechanism used by the autophagy machinery to maintain the apicoplast is unclear. We report that the ATG12-ATG5-ATG16L complex exists in Toxoplasma gondii (Tg). This complex is localized on isolated structures at the periphery of the apicoplast dependent on TgATG16L. Inducible depletion of TgATG12, TgATG5, or TgATG16L caused loss of the apicoplast and affected parasite growth. We found that a putative soluble N-ethylmaleimide sensitive factor attachment protein receptor (SNARE) protein, synaptosomal-associated protein 29 (TgSNAP29, Qbc SNARE), is required to maintain the apicoplast in T. gondii . TgSNAP29 depletion disrupted TgATG8 localization at the apicoplast. Additionally, we identified a putative ubiquitin-interacting motif-docking site (UDS) of TgATG8. Mutation of the UDS site abolished TgATG8 localization on the apicoplast but not lipidation. These findings suggest that the TgATG12-TgATG5-TgATG16L complex is required for biogenesis of the apicoplast, in which TgATG8 is translocated to the apicoplast via vesicles in a SNARE -dependent manner in T. gondii . Abbreviations : AID: auxin-inducible degron; CCD: coiled-coil domain; HFF: human foreskin fibroblast; IAA: indole-3-acetic acid; LAP: LC3-associated phagocytosis; NAA: 1-naphthaleneacetic acid; PtdIns3P: phosphatidylinositol-3-phosphate; SNARE: soluble N-ethylmaleimide sensitive factor attachment protein receptor; UDS: ubiquitin-interacting motif-docking site; UIM: ubiquitin-interacting motif.

Published

2023

2. Lamp1 mediates lipid transport, but is dispensable for autophagy in Drosophila .

Author

Chaudhry N, Sica M, Surabhi S, Hernandez DS, Mesquita A, Selimovic A, Riaz A, Lescat L, Bai H, MacIntosh GC, and Jenny A

Subjects

Amino Acids metabolism, Animals, Biocompatible Materials metabolism, Biocompatible Materials pharmacology, Calnexin metabolism, Drosophila metabolism, Drosophila Proteins, Endosomal Sorting Complexes Required for Transport metabolism, Ethylmaleimide metabolism, Ethylmaleimide pharmacology, Fibroblasts metabolism, Hepatocyte Growth Factor metabolism, Humans, Lipoproteins, HDL metabolism, Lipoproteins, HDL pharmacology, Lipoproteins, LDL metabolism, Lysosomal Membrane Proteins genetics, Lysosomal Membrane Proteins metabolism, Lysosomes metabolism, Mammals metabolism, Mice, Protein-Tyrosine Kinases metabolism, SNARE Proteins metabolism, Sirolimus pharmacology, Sterols metabolism, Sterols pharmacology, Triglycerides metabolism, Tubulin metabolism, Untranslated Regions, Autophagy genetics, Diglycerides metabolism, Diglycerides pharmacology

Abstract

The endolysosomal system not only is an integral part of the cellular catabolic machinery that processes and recycles nutrients for synthesis of biomaterials, but also acts as signaling hub to sense and coordinate the energy state of cells with growth and differentiation. Lysosomal dysfunction adversely influences vesicular transport-dependent macromolecular degradation and thus causes serious problems for human health. In mammalian cells, loss of the lysosome associated membrane proteins LAMP1 and LAMP2 strongly affects autophagy and cholesterol trafficking. Here we show that the previously uncharacterized Drosophila Lamp1 is a bona fide ortholog of vertebrate LAMP1 and LAMP2. Surprisingly and in contrast to lamp1 lamp2 double-mutant mice, Drosophila Lamp1 is not required for viability or autophagy, suggesting that fly and vertebrate LAMP proteins acquired distinct functions, or that autophagy defects in lamp1 lamp2 mutants may have indirect causes. However, Lamp1 deficiency results in an increase in the number of acidic organelles in flies. Furthermore, we find that Lamp1 mutant larvae have defects in lipid metabolism as they show elevated levels of sterols and diacylglycerols (DAGs). Because DAGs are the main lipid species used for transport through the hemolymph (blood) in insects, our results indicate broader functions of Lamp1 in lipid transport. Our findings make Drosophila an ideal model to study the role of LAMP proteins in lipid assimilation without the confounding effects of their storage and without interfering with autophagic processes. Abbreviations : aa: amino acid; AL: autolysosome; AP: autophagosome; APGL: autophagolysosome; AV: autophagic vacuole (i.e. AP and APGL/AL); AVi: early/initial autophagic vacuoles; AVd: late/degradative autophagic vacuoles; Atg : autophagy-related; CMA: chaperone-mediated autophagy; Cnx99A: Calnexin 99A; DAG: diacylglycerol; eMI: endosomal microautophagy; ESCRT: endosomal sorting complexes required for transport; FB: fat body; HDL: high-density lipoprotein; Hrs: Hepatocyte growth factor regulated tyrosine kinase substrate; LAMP: lysosomal associated membrane protein; LD: lipid droplet; LDL: low-density lipoprotein; Lpp: lipophorin; LTP: Lipid transfer particle; LTR: LysoTracker Red; MA: macroautophagy; MCC: Manders colocalization coefficient; MEF: mouse embryonic fibroblast MTORC: mechanistic target of rapamycin kinase complex; PV: parasitophorous vacuole; SNARE: soluble N-ethylmaleimide sensitive factor attachment protein receptor; Snap: Synaptosomal-associated protein; st: starved; TAG: triacylglycerol; TEM: transmission electron microscopy; TFEB/Mitf: transcription factor EB; TM: transmembrane domain; tub: tubulin; UTR: untranslated region.

Published

2022

3. A small-molecule competitive inhibitor of phosphatidic acid binding by the AAA+ protein NSF/Sec18 blocks the SNARE-priming stage of vacuole fusion.

Author

Sparks RP, Arango AS, Starr ML, Aboff ZL, Hurst LR, Rivera-Kohr DA, Zhang C, Harnden KA, Jenkins JL, Guida WC, Tajkhorshid E, and Fratti RA

Subjects

ATPases Associated with Diverse Cellular Activities chemistry, ATPases Associated with Diverse Cellular Activities genetics, Adenosine Triphosphatases chemistry, Membrane Fusion drug effects, Membrane Fusion genetics, Membrane Lipids chemistry, Membrane Lipids genetics, Membrane Transport Proteins chemistry, Membrane Transport Proteins genetics, Molecular Dynamics Simulation, N-Ethylmaleimide-Sensitive Proteins chemistry, N-Ethylmaleimide-Sensitive Proteins genetics, Phosphatidic Acids antagonists & inhibitors, SNARE Proteins chemistry, SNARE Proteins genetics, Saccharomyces cerevisiae chemistry, Saccharomyces cerevisiae genetics, Saccharomyces cerevisiae Proteins chemistry, Small Molecule Libraries pharmacology, Soluble N-Ethylmaleimide-Sensitive Factor Attachment Proteins chemistry, Soluble N-Ethylmaleimide-Sensitive Factor Attachment Proteins genetics, Vacuoles genetics, Vesicular Transport Proteins chemistry, Adenosine Triphosphatases genetics, Ethylmaleimide metabolism, Phosphatidic Acids chemistry, Saccharomyces cerevisiae Proteins genetics, Small Molecule Libraries chemistry, Vesicular Transport Proteins genetics

Abstract

The homeostasis of most organelles requires membrane fusion mediated by s oluble N -ethylmaleimide-sensitive factor (NSF) a ttachment protein re ceptors (SNAREs). SNAREs undergo cycles of activation and deactivation as membranes move through the fusion cycle. At the top of the cycle, inactive cis -SNARE complexes on a single membrane are activated, or primed, by the hexameric ATPase associated with the diverse cellular activities (AAA+) protein, N -ethylmaleimide-sensitive factor (NSF/Sec18), and its co-chaperone α-SNAP/Sec17. Sec18-mediated ATP hydrolysis drives the mechanical disassembly of SNAREs into individual coils, permitting a new cycle of fusion. Previously, we found that Sec18 monomers are sequestered away from SNAREs by binding phosphatidic acid (PA). Sec18 is released from the membrane when PA is hydrolyzed to diacylglycerol by the PA phosphatase Pah1. Although PA can inhibit SNARE priming, it binds other proteins and thus cannot be used as a specific tool to further probe Sec18 activity. Here, we report the discovery of a small-molecule compound, we call IPA (inhibitor of priming activity), that binds Sec18 with high affinity and blocks SNARE activation. We observed that IPA blocks SNARE priming and competes for PA binding to Sec18. Molecular dynamics simulations revealed that IPA induces a more rigid NSF/Sec18 conformation, which potentially disables the flexibility required for Sec18 to bind to PA or to activate SNAREs. We also show that IPA more potently and specifically inhibits NSF/Sec18 activity than does N- ethylmaleimide, requiring the administration of only low micromolar concentrations of IPA, demonstrating that this compound could help to further elucidate SNARE-priming dynamics., (© 2019 Sparks et al.)

Published

2019

4. Role of SNAREs in Atopic Dermatitis-Related Cytokine Secretion and Skin-Nerve Communication.

Author

Meng J, Wang J, Buddenkotte J, Buhl T, and Steinhoff M

Subjects

Animals, Cells, Cultured, Cytokines metabolism, Disease Models, Animal, Endothelin-1 metabolism, Ethylmaleimide metabolism, Gene Knockdown Techniques, Humans, Immunity, Innate, Mice, Mice, Inbred C57BL, Organ Culture Techniques, SNARE Proteins metabolism, Vesicle-Associated Membrane Protein 3 genetics, Dermatitis, Atopic metabolism, Epidermis metabolism, Keratinocytes physiology, Sensory Receptor Cells physiology, Vesicle-Associated Membrane Protein 3 metabolism

Abstract

The role of soluble N-ethylmaleimide-sensitive factor attachment protein receptors in atopic dermatitis (AD) is unknown. This study identifies the function of soluble N-ethylmaleimide sensitive factor attachment protein receptor in AD-related cytokine secretion and epidermis-nerve communication. Herein, we report that various cytokines were simultaneously upregulated and coreleased in innate immunity-activated primary human keratinocytes. AD-related cytokines thymic stromal lymphopoietin, endothelin-1, and inflammatory tumor necrosis factor-α activated distinct but overlapping sensory neurons. Tumor necrosis factor-α potentiated thymic stromal lymphopoietin-induced Ca 2+ -influx, whereas endothelin-1 caused itch-selective B-type natriuretic peptide release. In primary human keratinocytes, B-type natriuretic peptide upregulated genes promoting dermatological and neuroinflammatory diseases and conditions. VAMP3, SNAP-29, and syntaxin 4 proved important in driving cytokine release from primary human keratinocytes. Depletion of VAMP3 inhibited nearly all the cytokine release including thymic stromal lymphopoietin and endothelin-1. Accordingly, VAMP3 co-occurred with endothelin-1 in the skins of patients with AD. Our study pinpoints the pivotal role of soluble N-ethylmaleimide sensitive factor attachment protein receptors in mediating cytokine secretion related to AD. VAMP3 is identified as a suitable target for developing broad-spectrum anticytokine therapeutics for controlling itch and atopic skin inflammation., (Copyright © 2019 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2019

5. Phosphoregulation of the intracellular termini of K + -Cl - cotransporter 2 (KCC2) enables flexible control of its activity.

Author

Cordshagen A, Busch W, Winklhofer M, Nothwang HG, and Hartmann AM

Subjects

Amino Acid Motifs, Amino Acid Substitution, Ethylmaleimide metabolism, HEK293 Cells, Humans, Mutation, Phosphorylation, Staurosporine metabolism, Symporters genetics, Symporters chemistry, Symporters metabolism

Abstract

The pivotal role of K + -Cl - cotransporter 2 (KCC2) in inhibitory neurotransmission and severe human diseases fosters interest in understanding posttranslational regulatory mechanisms such as (de)phosphorylation. Here, the regulatory role of the five bona fide phosphosites Ser 31 , Thr 34 , Ser 932 , Thr 999 , and Thr 1008 was investigated by the use of alanine and aspartate mutants. Tl + -based flux analyses in HEK-293 cells demonstrated increased transport activity for S932D (mimicking phosphorylation) and T1008A (mimicking dephosphorylation), albeit to a different extent. Increased activity was due to changes in intrinsic activity, as it was not caused by increased cell-surface abundance. Substitutions of Ser 31 , Thr 34 , or Thr 999 had no effect. Additionally, we show that the indirect actions of the known KCC2 activators staurosporine and N -ethylmaleimide (NEM) involved multiple phosphosites. S31D, T34A, S932A/D, T999A, or T1008A/D abrogated staurosporine mediated stimulation, and S31A, T34D, or S932D abolished NEM-mediated stimulation. This demonstrates for the first time differential effects of staurosporine and NEM on KCC2. In addition, the staurosporine-mediated effects involved both KCC2 phosphorylation and dephosphorylation with Ser 932 and Thr 1008 being bona fide target sites. In summary, our data reveal a complex phosphoregulation of KCC2 that provides the transporter with a toolbox for graded activity and integration of different signaling pathways., (© 2018 Cordshagen et al.)

Published

2018

6. N -Ethylmaleimide increases KCC2 cotransporter activity by modulating transporter phosphorylation.

Author

Conway LC, Cardarelli RA, Moore YE, Jones K, McWilliams LJ, Baker DJ, Burnham MP, Bürli RW, Wang Q, Brandon NJ, Moss SJ, and Deeb TZ

Subjects

Animals, Cell Membrane metabolism, Embryo, Mammalian, Humans, Membrane Transport Modulators metabolism, Neurons metabolism, Phosphorylation physiology, Rats, Rats, Sprague-Dawley, Receptors, GABA metabolism, Symporters physiology, K Cl- Cotransporters, Ethylmaleimide metabolism, Symporters metabolism

Abstract

K + /Cl - cotransporter 2 (KCC2) is selectively expressed in the adult nervous system and allows neurons to maintain low intracellular Cl - levels. Thus, KCC2 activity is an essential prerequisite for fast hyperpolarizing synaptic inhibition mediated by type A γ-aminobutyric acid (GABA A ) receptors, which are Cl - -permeable, ligand-gated ion channels. Consistent with this, deficits in the activity of KCC2 lead to epilepsy and are also implicated in neurodevelopmental disorders, neuropathic pain, and schizophrenia. Accordingly, there is significant interest in developing activators of KCC2 as therapeutic agents. To provide insights into the cellular processes that determine KCC2 activity, we have investigated the mechanism by which N -ethylmaleimide (NEM) enhances transporter activity using a combination of biochemical and electrophysiological approaches. Our results revealed that, within 15 min, NEM increased cell surface levels of KCC2 and modulated the phosphorylation of key regulatory residues within the large cytoplasmic domain of KCC2 in neurons. More specifically, NEM increased the phosphorylation of serine 940 (Ser-940), whereas it decreased phosphorylation of threonine 1007 (Thr-1007). NEM also reduced with no lysine (WNK) kinase phosphorylation of Ste20-related proline/alanine-rich kinase (SPAK), a kinase that directly phosphorylates KCC2 at residue Thr-1007. Mutational analysis revealed that Thr-1007 dephosphorylation mediated the effects of NEM on KCC2 activity. Collectively, our results suggest that compounds that either increase the surface stability of KCC2 or reduce Thr-1007 phosphorylation may be of use as enhancers of KCC2 activity., (© 2017 by The American Society for Biochemistry and Molecular Biology, Inc.)

Published

2017

7. Calcium Channel Opening Rather than the Release of ATP Causes the Apoptosis of Osteoblasts Induced by Overloaded Mechanical Stimulation.

Author

Liu L, Li H, Cui Y, Li R, Meng F, Ye Z, and Zhang X

Subjects

Adenosine Triphosphate metabolism, Alkaline Phosphatase genetics, Alkaline Phosphatase metabolism, Apoptosis genetics, Athletes, Calcium metabolism, Cell Proliferation genetics, Ethylmaleimide metabolism, Fractures, Stress pathology, Humans, Osteoblasts metabolism, Osteoblasts pathology, Polyesters pharmacology, Calcium Channels metabolism, Cell Differentiation genetics, Fractures, Stress genetics, Stress, Mechanical

Abstract

Background: Stress fracture is one of the most common overuse injuries in athletes. Overloaded mechanical stimulation is an important factor affecting stress fractures, but the mechanism is unclear., Methods: MC3T3-E1 cells and a polycaprolactone (PCL) scaffold were co-cultured, and finite element analysis (FEA) was used to analyze the load-carrying capability. Cell proliferation was investigated with CCK-8 assays. An alkaline phosphatase (AKP) activity assay was used to evaluate cell differentiation. Cell apoptosis was analyzed using Hoechst/ PI double-labeling, Caspase-3 activity and lactate dehydrogenase (LDH) activity assays. Realtime PCR and Western blotting were used to examine the gene and protein expression, respectively, of Caspase-3 and Caspase-9. Assays of the intracellular calcium with fluorescent probe technique and extracellular ATP with fluorometric assay kit were used to analyze the changes in the intracellular calcium concentration induced by calcium channel opening and the release of ATP, respectively, at different operation times., Results: When the apparent strain reached 10000 µε, the strain scope of fber at levels greater than 4000 µε was 60%. Overloading for 4 days and operation times of 0.5 h and 2 h increased the cell number and AKP secretion. However, apoptosis genes were activated at the same time, and the operation time of 2 h had a significantly greater effect than 0.5 h. At 8 days, the cell numbers were greater for the operation time of 0.5 h than for 2 h, and the 2-h groups had the fastest apoptosis rate. Overloading for 1 day increased intracellular calcium levels and ATP release. The increase in intracellular calcium could be blocked by the addition of N-ethylmaleimide (NEM) or Hank's medium. Overloading for 8 days increased intracellular calcium levels but decreased extracellular ATP, and verapamil blocked the increase in intracellular calcium., Conclusion: We found that a simultaneous 'double effect' on osteoblasts was induced by overloading, which promoted cell proliferation, differentiation and apoptosis. Short-term overloading could open the cell membrane calcium channels and release calcium stores to elevate intracellular calcium levels, thereby promoting the proliferation and differentiation of cells to a greater extent than the effect of apoptosis. For long-term overloading, calcium channel opening in the membrane could lead to overloading of intracellular calcium levels, inducing an apoptosis effect that is greater than the effect on proliferation and differentiation., (© 2017 The Author(s). Published by S. Karger AG, Basel.)

Published

2017

8. LRRK2 phosphorylates pre-synaptic N-ethylmaleimide sensitive fusion (NSF) protein enhancing its ATPase activity and SNARE complex disassembling rate.

Author

Belluzzi E, Gonnelli A, Cirnaru MD, Marte A, Plotegher N, Russo I, Civiero L, Cogo S, Carrion MP, Franchin C, Arrigoni G, Beltramini M, Bubacco L, Onofri F, Piccoli G, and Greggio E

Subjects

Animals, Carrier Proteins metabolism, Ethylmaleimide metabolism, Leucine-Rich Repeat Serine-Threonine Protein Kinase-2, Mice, Mice, Transgenic, Phosphorylation, Protein Serine-Threonine Kinases genetics, Vesicular Transport Proteins genetics, Vesicular Transport Proteins metabolism, Adenosine Triphosphatases metabolism, Mutation genetics, N-Ethylmaleimide-Sensitive Proteins metabolism, Protein Serine-Threonine Kinases metabolism, SNARE Proteins metabolism

Abstract

Background: Lrrk2, a gene linked to Parkinson's disease, encodes a large scaffolding protein with kinase and GTPase activities implicated in vesicle and cytoskeletal-related processes. At the presynaptic site, LRRK2 associates with synaptic vesicles through interaction with a panel of presynaptic proteins., Results: Here, we show that LRRK2 kinase activity influences the dynamics of synaptic vesicle fusion. We therefore investigated whether LRRK2 phosphorylates component(s) of the exo/endocytosis machinery. We have previously observed that LRRK2 interacts with NSF, a hexameric AAA+ ATPase that couples ATP hydrolysis to the disassembling of SNARE proteins allowing them to enter another fusion cycle during synaptic exocytosis. Here, we demonstrate that NSF is a substrate of LRRK2 kinase activity. LRRK2 phosphorylates full-length NSF at threonine 645 in the ATP binding pocket of D2 domain. Functionally, NSF phosphorylated by LRRK2 displays enhanced ATPase activity and increased rate of SNARE complex disassembling. Substitution of threonine 645 with alanine abrogates LRRK2-mediated increased ATPase activity., Conclusions: Given that the most common Parkinson's disease LRRK2 G2019S mutation displays increased kinase activity, our results suggest that mutant LRRK2 may impair synaptic vesicle dynamics via aberrant phosphorylation of NSF.

Published

2016

9. Thiol-blocking electrophiles interfere with labeling and detection of protein sulfenic acids.

Author

Reisz JA, Bechtold E, King SB, Poole LB, and Furdui CM

Subjects

Ascorbic Acid chemistry, Ascorbic Acid metabolism, Cyclohexanones chemistry, Cyclohexanones metabolism, Cysteine metabolism, Dithiothreitol metabolism, Ethylmaleimide chemistry, Ethylmaleimide metabolism, Iodoacetamide chemistry, Iodoacetamide metabolism, Methyl Methanesulfonate analogs & derivatives, Methyl Methanesulfonate chemistry, Methyl Methanesulfonate metabolism, Oxidation-Reduction, Proteins metabolism, Reactive Oxygen Species metabolism, Spectrometry, Mass, Electrospray Ionization, Sulfenic Acids metabolism, Sulfhydryl Compounds metabolism, Cysteine chemistry, Dithiothreitol chemistry, Proteins chemistry, Sulfenic Acids chemistry, Sulfhydryl Compounds chemistry

Abstract

Cellular exposure to reactive oxygen species induces rapid oxidation of DNA, proteins, lipids and other biomolecules. At the proteome level, cysteine thiol oxidation is a prominent post-translational process that is implicated in normal physiology and numerous pathologies. Methods for investigating protein oxidation include direct labeling with selective chemical probes and indirect tag-switch techniques. Common to both approaches is chemical blocking of free thiols using reactive electrophiles to prevent post-lysis oxidation or other thiol-mediated cross-reactions. These reagents are used in large excess, and their reactivity with cysteine sulfenic acid, a critical oxoform in numerous proteins, has not been investigated. Here we report the reactivity of three thiol-blocking electrophiles, iodoacetamide, N-ethylmaleimide and methyl methanethiosulfonate, with protein sulfenic acid and dimedone, the structural core of many sulfenic acid probes. We demonstrate that covalent cysteine -SOR (product) species are partially or fully susceptible to reduction by dithiothreitol, tris(2-carboxyethyl)phosphine and ascorbate, regenerating protein thiols, or, in the case of ascorbate, more highly oxidized species. The implications of this reactivity on detection methods for protein sulfenic acids and S-nitrosothiols are discussed., (© 2013 FEBS.)

Published

2013

10. Pathways of cadmium fluxes in the root of the halophyte Suaeda salsa.

Author

Li L, Liu X, Peijnenburg WJ, Zhao J, Chen X, Yu J, and Wu H

Subjects

Biodegradation, Environmental, Cadmium toxicity, Chenopodiaceae physiology, Ethylmaleimide metabolism, Plant Roots metabolism, Rhizosphere, Salt-Tolerant Plants metabolism, Salt-Tolerant Plants physiology, Sodium Chloride metabolism, Soil chemistry, Soil Pollutants toxicity, Cadmium metabolism, Chenopodiaceae metabolism, Soil Pollutants metabolism

Abstract

Halophyte plants offer a greater potential for phytoremediation research for reducing the levels of toxic metals from saline soils than salt sensitive plants. Using the scanning ion-selective electrode technique, we analyzed the pattern and rate of Cd(2+) fluxes at different regions of the root apex of Suaeda salsa. The Cd(2+) influx in the rhizosphere was greatest near the root tip (within 150μm of the tip). The results indicated that Cd(2+) influx into roots was significantly suppressed by the pre-treatment or in the presence of two kinds of Ca(2+) channel blockers; LaCl(3) and verapamil. The Cd(2+) influx was also reduced by N-ethylmaleimide, a thiol blocker. Cd content determination and labeling of Cd using fluorescent dye support our conclusion. The results of this study provide a more stable theoretical basis for the phytoremediation of Cd contamination in saline soils of coastal zones., (Copyright © 2011 Elsevier Inc. All rights reserved.)

Published

2012

11. A yeast metabolite extraction protocol optimised for time-series analyses.

Author

Sasidharan K, Soga T, Tomita M, and Murray DB

Subjects

Calibration, Electrophoresis, Capillary, Ethylmaleimide metabolism, Sulfhydryl Compounds metabolism, Time Factors, Metabolome, Metabolomics methods, Saccharomyces cerevisiae metabolism

Abstract

There is an increasing call for the absolute quantification of time-resolved metabolite data. However, a number of technical issues exist, such as metabolites being modified/degraded either chemically or enzymatically during the extraction process. Additionally, capillary electrophoresis mass spectrometry (CE-MS) is incompatible with high salt concentrations often used in extraction protocols. In microbial systems, metabolite yield is influenced by the extraction protocol used and the cell disruption rate. Here we present a method that rapidly quenches metabolism using dry-ice ethanol bath and methanol N-ethylmaleimide solution (thus stabilising thiols), disrupts cells efficiently using bead-beating and avoids artefacts created by live-cell pelleting. Rapid sample processing minimised metabolite leaching. Cell weight, number and size distribution was used to calculate metabolites to an attomol/cell level. We apply this method to samples obtained from the respiratory oscillation that occurs when yeast are grown continuously.

Published

2012

12. Disulfide bond formation contributes to herpes simplex virus capsid stability and retention of pentons.

Author

Szczepaniak R, Nellissery J, Jadwin JA, Makhov AM, Kosinski A, Conway JF, and Weller SK

Subjects

Animals, Chlorocebus aethiops, Dithiothreitol metabolism, Ethylmaleimide metabolism, Herpesvirus 1, Human drug effects, Models, Molecular, Reducing Agents metabolism, Vero Cells, Virion ultrastructure, Capsid Proteins chemistry, Capsid Proteins metabolism, Disulfides metabolism, Herpesvirus 1, Human chemistry, Herpesvirus 1, Human metabolism

Abstract

Disulfide bonds reportedly stabilize the capsids of several viruses, including papillomavirus, polyomavirus, and simian virus 40, and have been detected in herpes simplex virus (HSV) capsids. In this study, we show that in mature HSV-1 virions, capsid proteins VP5, VP23, VP19C, UL17, and UL25 participate in covalent cross-links, and that these are susceptible to dithiothreitol (DTT). In addition, several tegument proteins were found in high-molecular-weight complexes, including VP22, UL36, and UL37. Cross-linked capsid complexes can be detected in virions isolated in the presence and absence of N-ethylmaleimide (NEM), a chemical that reacts irreversibly with free cysteines to block disulfide formation. Intracellular capsids isolated in the absence of NEM contain disulfide cross-linked species; however, intracellular capsids isolated from cells pretreated with NEM did not. Thus, the free cysteines in intracellular capsids appear to be positioned such that disulfide bond formation can occur readily if they are exposed to an oxidizing environment. These results indicate that disulfide cross-links are normally present in extracellular virions but not in intracellular capsids. Interestingly, intracellular capsids isolated in the presence of NEM are unstable; B and C capsids are converted to a novel form that resembles A capsids, indicating that scaffold and DNA are lost. Furthermore, these capsids also have lost pentons and peripentonal triplexes as visualized by cryoelectron microscopy. These data indicate that capsid stability, and especially the retention of pentons, is regulated by the formation of disulfide bonds in the capsid.

Published

2011

13. Inactivation of hantaviruses by N-ethylmaleimide preserves virion integrity.

Author

Strandin T, Hepojoki J, Wang H, Vaheri A, and Lankinen H

Subjects

Animals, Antigens, Viral immunology, Cell Line, Dithionitrobenzoic Acid metabolism, Orthohantavirus immunology, Virus Attachment, Disinfectants metabolism, Ethylmaleimide metabolism, Orthohantavirus drug effects, Preservatives, Pharmaceutical metabolism, Virion drug effects, Virus Inactivation

Abstract

Thiol groups of cysteine residues are crucial for the infectivity of various enveloped viruses, but their role in the infectivity of viruses of the family Bunyaviridae has thus far not been studied. This report shows that thiol groups are essential to the infectivity of hantaviruses. Alkylation of the thiol functional groups using the membrane-permeable compound N-ethylmaleimide (NEM) and membrane-impermeable compound 5,5'-dithio-bis-(2-nitrobenzoic acid) (DTNB) showed NEM to be a highly effective inactivator of Puumala and Tula hantaviruses. The NEM-inactivated hantavirus maintained the buoyant density of the wild-type virus. Furthermore, the antigenicity of glycoproteins and the cell attachment capacity of virions were retained at NEM concentrations that totally abolished virus infectivity. These results signified preservation of virion integrity following inactivation with NEM, making chemically inactivated virions valuable research antigens. It was demonstrated with biotin-conjugated maleimide, a mechanistic analogue of NEM, that all the structural proteins of hantavirus were sensitive towards thiol alkylation. In contrast to hantaviruses, NEM did not abolish Uukuniemi phlebovirus infectivity to the same extent. This indicates differences in the use of free thiols in virus entry among members of the family Bunyaviridae.

Published

2011

14. Interaction between N-ethylmaleimide-sensitive factor and GluR2 is essential for fear memory formation in lateral amygdala.

Author

Joels G and Lamprecht R

Subjects

Amino Acid Sequence, Animals, Ethylmaleimide metabolism, Male, Molecular Sequence Data, N-Ethylmaleimide-Sensitive Proteins genetics, Protein Binding physiology, Rats, Rats, Sprague-Dawley, Receptors, AMPA genetics, Amygdala physiology, Fear physiology, Memory physiology, N-Ethylmaleimide-Sensitive Proteins metabolism, Receptors, AMPA metabolism

Abstract

Long-term memory formation is believed to involve alterations of synaptic efficacy. It has been shown that GluR1-containing AMPA receptors are inserted into synapses following stimuli leading to plasticity and that GluR2/GluR3-containing receptors replace existing synaptic AMPA receptors continuously and may act to maintain synaptic efficacy. Maintaining GluR2/GluR3 receptors level in synapse requires interactions of N-ethylmaleimide-sensitive factor (NSF) with GluR2. To assess possible roles of NSF-GluR2 interaction in rat lateral amygdala (LA) in fear memory formation we used a specific GluR2-NSF interaction inhibitory peptide (pep-R845A). This inhibitory peptide, composed of a modified NSF binding site of GluR2, was previously shown to interact specifically with NSF and to affect AMPA-mediated synaptic efficacy. The inhibitory peptide was linked to a TAT peptide (TAT-pep-R845A) to facilitate internalization into LA cells. Infusion of the TAT-pep-R845A inhibitory peptide into LA 30 min before fear conditioning led to a significant impairment of long-term fear memory formation. In contrast, the control TAT peptide alone had no effect on fear memory. Injection of TAT-pep-R845A peptide into LA had no effect on short-term fear memory. In addition, the inhibitory peptide had no effect on memory retrieval when injected into LA 30 min before fear memory test. Furthermore, maintenance of memory was not impaired when the peptide was injected 24 h after fear conditioning and fear memory was tested 48 h afterward. These results show that GluR2-NSF interaction in LA is necessary for fear memory consolidation but not retrieval or persistence.

Published

2010

15. Legionella pneumophila promotes functional interactions between plasma membrane syntaxins and Sec22b.

Author

Arasaki K and Roy CR

Subjects

Calnexin metabolism, Cell Membrane metabolism, Endoplasmic Reticulum metabolism, Ethylmaleimide metabolism, Legionella pneumophila metabolism, Microsomes metabolism, N-Ethylmaleimide-Sensitive Proteins metabolism, Organelles metabolism, Phagosomes metabolism, Phagosomes microbiology, Protein Transport, SNARE Proteins metabolism, Secretory Vesicles metabolism, Soluble N-Ethylmaleimide-Sensitive Factor Attachment Proteins metabolism, Membrane Proteins metabolism, Qa-SNARE Proteins metabolism, Vacuoles metabolism, Vacuoles microbiology

Abstract

Biogenesis of a specialized organelle that supports intracellular replication of Legionella pneumophila involves the fusion of secretory vesicles exiting the endoplasmic reticulum (ER) with phagosomes containing this bacterial pathogen. Here, we investigated host plasma membrane SNARE proteins to determine whether they play a role in trafficking of vacuoles containing L. pneumophila. Depletion of plasma membrane syntaxins by RNA interference resulted in delayed acquisition of the resident ER protein calnexin and enhanced retention of Rab1 on phagosomes containing virulent L. pneumophila, suggesting that these SNARE proteins are involved in vacuole biogenesis. Plasma membrane-localized SNARE proteins syntaxin 2, syntaxin 3, syntaxin 4 and SNAP23 localized to vacuoles containing L. pneumophila. The ER-localized SNARE protein Sec22b was found to interact with plasma membrane SNAREs on vacuoles containing virulent L. pneumophila, but not on vacuoles containing avirulent mutants of L. pneumophila. The addition of alpha-SNAP and N-ethylmaleimide-sensitive factor (NSF) to the plasma membrane SNARE complexes formed by virulent L. pneumophila resulted in the dissociation of Sec22b, indicating functional pairing between these SNAREs. Thus, L. pneumophila stimulates the non-canonical pairing of plasma membrane t-SNAREs with the v-SNARE Sec22b to promote fusion of the phagosome with ER-derived vesicles. The mechanism by which L. pneumophila promotes pairing of plasma membrane syntaxins and Sec22b could provide unique insight into how the secretory vesicles could provide an additional membrane reserve subverted during phagosome maturation.

Published

2010

16. Anti-ulcerogenic effect of a whey protein isolate and collagen hydrolysates against ethanol ulcerative lesions on oral administration to rats.

Author

Castro GA, Carvalho JE, Tinti SV, Possenti A, and Sgarbieri VC

Subjects

Alkylation, Animals, Anti-Ulcer Agents pharmacology, Carbenoxolone therapeutic use, Cattle, Collagen metabolism, Collagen pharmacology, Disease Models, Animal, Drug Synergism, Drug Therapy, Combination, Ethanol, Ethylmaleimide metabolism, Gastric Mucosa pathology, Gastrins blood, Hydrolysis, Male, Milk Proteins pharmacology, Mucus metabolism, Rats, Rats, Wistar, Stomach pathology, Stomach Ulcer metabolism, Stomach Ulcer pathology, Sulfhydryl Compounds metabolism, Swine, Whey Proteins, Anti-Ulcer Agents therapeutic use, Collagen therapeutic use, Gastric Mucosa drug effects, Milk Proteins therapeutic use, Stomach drug effects, Stomach Ulcer drug therapy

Abstract

The effect of the administration of a whey protein isolate (WPI) and collagen hydrolysates on ethanol-induced ulcerative lesions was studied in rats. WPI and bovine or porcine collagen hydrolysate (BCH and PCH, respectively) were given to rats by gavage. In acute experiments, (single-dose) physiological saline (10 mL/kg of body weight) was used as the negative control, and carbenoxolone (200 mg/kg of body weight) was used as a positive control. Ethanol (1 mL per 250-g rat) was also given by gavage. These treatments reduced the ulcerative lesion index (ULI) in a range of 40-77%, depending on the dosage. Some mixtures of WPI with either PCH or BCH provided results that suggested synergisms between WPI and the collagen hydrolysates. For example, WPI/BCH (in the proportion of 375:375 mg/kg of body weight) decreased ULI by 64%. The mechanism for mucosal protection involved a decrease in plasma gastrin (approximately 40%), a significant increase (50-267%) in mucus production, and a reduction in ULI (percentage) when intragastric administrations were performed after in vivo alkylation by N-ethylmaleimide. Results suggest that gastrin, sulfhydryl substances, and some mechanisms related to mucus production are all involved in gastric ulcer protection against ethanol. The collagen hydrolysates (both PCH and BCH) presented a stronger effect on mucus production; on the other hand, the effect of WPI was also dependent on sulfhydryl compounds, resulting in a more protective effect when the two proteins were administered together.

Published

2010

17. Some cardiomyopathy-causing troponin I mutations stabilize a functional intermediate actin state.

Author

Mathur MC, Kobayashi T, and Chalovich JM

Subjects

Actomyosin metabolism, Adenosine Triphosphatases metabolism, Animals, Calcium metabolism, Cattle, Ethylmaleimide metabolism, Mice, Muscle, Skeletal metabolism, Mutation, Myosins metabolism, Rabbits, Actins metabolism, Cardiomyopathies genetics, Troponin I genetics, Troponin I metabolism

Abstract

We examined four cardiomyopathy-causing mutations of troponin I that appear to disturb function by altering the distribution of thin filament states. The R193H (mouse) troponin I mutant had greater than normal actin-activated myosin-S1 ATPase activity in both the presence and absence of calcium. The rate of ATPase activity was the same as that of the wild-type at near-saturating concentrations of the activator, N-ethylmaleimide-S1. This mutant appeared to function by stabilizing the active state of thin filaments. Mutations D191H, R146G, and R146W had lower ATPase activities in the presence of calcium, but higher activities in the absence of calcium. These effects were most pronounced with mutations at position 146. For all three mutants the rates were similar to those of the wild-type at near-saturating concentrations of N-ethylmaleimide-S1. These results, combined with previous results, show that any alteration in the normal distribution of actomyosin states is capable of producing cardiomyopathy. The results of the D191H, R146G, and R146W mutations are most readily explained if the intermediate state of regulated actin has a unique function. The intermediate state appears to have an ability to accelerate the rate of ATP hydrolysis by myosin that exceeds that of the inactive state.

Published

2009

18. Analysis of the interaction between the UL11 and UL16 tegument proteins of herpes simplex virus.

Author

Yeh PC, Meckes DG Jr, and Wills JW

Subjects

Amino Acid Motifs, Amino Acid Substitution, Animals, Binding Sites, Cell Line, Chlorocebus aethiops, Cloning, Molecular, Conserved Sequence, Cysteine genetics, Ethylmaleimide metabolism, Gene Expression, Humans, Mutagenesis, Site-Directed, Protein Binding, Protein Interaction Domains and Motifs, Recombinant Proteins isolation & purification, Recombinant Proteins metabolism, Sequence Deletion, Serine genetics, Viral Structural Proteins genetics, Viral Structural Proteins isolation & purification, Herpesvirus 1, Human physiology, Protein Interaction Mapping, Viral Structural Proteins metabolism

Abstract

The UL11 and UL16 tegument proteins of herpes simplex virus are conserved throughout the herpesvirus family. Previous studies have shown that these proteins interact, perhaps to link UL16-bound nucleocapsids to UL11, which resides on the cytoplasmic face of the trans-Golgi network, where maturation budding occurs. Little is known about the interaction except that it requires the leucine-isoleucine (LI) and acidic cluster motifs in UL11 and that no other viral proteins are involved. In particular, the important question of whether these two proteins bind to each other directly has not been addressed. Accordingly, UL11 and UL16 were expressed in bacteria, and the purified proteins were found to retain the ability to interact in a manner that was dependent upon the LI and acidic cluster. In an attempt to map the UL11-binding site contained in UL16, a large number of deletion mutants were constructed. The first 40 (nonconserved) amino acids were found to be dispensable, but all the other constructs failed to bind UL11 or had poor expression in transfected cells, suggesting that UL16 is very sensitive to alterations and probably lacks a multidomain structure. As an alternative strategy for identifying residues that are important for the interaction, the cysteines of UL16 were investigated, because many of these are highly conserved. Approximately half of the 20 cysteines in UL16 have been shown to be covalently modified by N-ethylmaleimide, and this treatment was found to block the interaction with UL11. Moreover, individual serine replacements of six of the most conserved cysteine residues were made, and four of these disrupted the interaction with UL11 without affecting protein stability. However, the UL11-UL16 interaction does not involve the formation of interspecies disulfide bonds, because binding occurred even when all the cysteines in UL11 were eliminated. Thus, UL16 directly interacts with UL11 and does so in a manner that requires free cysteines.

Published

2008

19. Thematic review series: glycerolipids. Mammalian glycerol-3-phosphate acyltransferases: new genes for an old activity.

Author

Gimeno RE and Cao J

Subjects

Amino Acid Motifs, Amino Acid Sequence, Animals, Ethylmaleimide metabolism, Glycerol-3-Phosphate O-Acyltransferase chemistry, Humans, Isoenzymes chemistry, Isoenzymes genetics, Isoenzymes metabolism, Microsomes enzymology, Microsomes metabolism, Glycerol-3-Phosphate O-Acyltransferase genetics, Glycerol-3-Phosphate O-Acyltransferase metabolism

Abstract

Glycerol-3-phosphate acyltransferases (GPATs; EC2.3.1.15) catalyze the first step in the de novo synthesis of neutral lipids (triglycerides) and glycerophospholipids. The existence of multiple enzyme isoforms with GPAT activity was predicted many years ago when GPAT activities with distinct kinetic profiles and sensitivity to inhibitors were characterized in two subcellular compartments, mitochondria and microsomes. We now know that mammals have at least four GPAT isoforms with distinct tissue distribution and function. GPAT1 is the major mitochondrial GPAT isoform and is characterized by its resistance to sulfhydryl-modifying reagents, such as N-ethylmaleimide (NEM). GPAT2 is a minor NEM-sensitive mitochondrial isoform. The activity referred to as microsomal GPAT is encoded by two closely related genes, GPAT3 and GPAT4. GPAT isoforms are important regulators of cellular triglyceride and phospholipid content, and may channel fatty acids toward particular metabolic fates. Overexpression and knock-out studies suggest that GPAT isoforms can play important roles in the development of hepatic steatosis, insulin resistance, and obesity; GPAT isoforms are also important for lactation. This review summarizes the current state of knowledge on mammalian GPAT isoforms.

Published

2008

20. The uncharacterized transcription factor YdhM is the regulator of the nemA gene, encoding N-ethylmaleimide reductase.

Author

Umezawa Y, Shimada T, Kori A, Yamada K, and Ishihama A

Subjects

Base Sequence, Binding Sites, Blotting, Northern, DNA Footprinting, Electrophoretic Mobility Shift Assay, Escherichia coli Proteins genetics, Escherichia coli Proteins physiology, Ethylmaleimide metabolism, Immunoblotting, Models, Genetic, Molecular Sequence Data, Operon genetics, Oxidoreductases genetics, Promoter Regions, Genetic genetics, Protein Binding, Recombinant Proteins metabolism, Transcription Factors genetics, Transcription Factors physiology, Escherichia coli Proteins metabolism, Gene Expression Regulation, Bacterial, Oxidoreductases metabolism, Oxidoreductases physiology, Transcription Factors metabolism

Abstract

N-ethylmaleimide (NEM) has been used as a specific reagent of Cys modification in proteins and thus is toxic for cell growth. On the Escherichia coli genome, the nemA gene coding for NEM reductase is located downstream of the gene encoding an as-yet-uncharacterized transcription factor, YdhM. Disruption of the ydhM gene results in reduction of nemA expression even in the induced state, indicating that the two genes form a single operon. After in vitro genomic SELEX screening, one of the target recognition sequences for YdhM was identified within the promoter region for this ydhM-nemA operon. Both YdhM binding in vitro to the ydhM promoter region and transcription repression in vivo of the ydhM-nemA operon by YdhM were markedly reduced by the addition of NEM. Taken together, we propose that YdhM is the repressor for the nemA gene, thus hereafter designated NemR. The repressor function of NemR was inactivated by the addition of not only NEM but also other Cys modification reagents, implying that Cys modification of NemR renders it inactive. This is an addition to the mode of controlling activity of transcription factors by alkylation with chemical agents.

Published

2008

21. Subunit a facilitates aqueous access to a membrane-embedded region of subunit c in Escherichia coli F1F0 ATP synthase.

Author

Steed PR and Fillingame RH

Subjects

Adenosine Triphosphate pharmacology, Amino Acid Substitution, Binding Sites, Carbon Radioisotopes, Cell Membrane drug effects, Cysteine genetics, Escherichia coli drug effects, Ethylmaleimide metabolism, Mesylates metabolism, Models, Molecular, Mutant Proteins metabolism, Proton Pumps metabolism, Silver metabolism, Staining and Labeling, Sulfhydryl Reagents pharmacology, Cell Membrane enzymology, Escherichia coli enzymology, Mitochondrial Proton-Translocating ATPases metabolism, Protein Subunits metabolism

Abstract

Rotary catalysis in F(1)F(0) ATP synthase is powered by proton translocation through the membrane-embedded F(0) sector. Proton binding and release occurs in the middle of the membrane at Asp-61 on transmembrane helix 2 of subunit c. Previously, the reactivity of cysteines substituted into F(0) subunit a revealed two regions of aqueous access, one extending from the periplasm to the middle of the membrane and a second extending from the middle of the membrane to the cytoplasm. To further characterize aqueous accessibility at the subunit a-c interface, we have substituted Cys for residues on the cytoplasmic side of transmembrane helix 2 of subunit c and probed the accessibility to these substituted positions using thiolate-reactive reagents. The Cys substitutions tested were uniformly inhibited by Ag(+) treatment, which suggested widespread aqueous access to this generally hydrophobic region. Sensitivity to N-ethylmaleimide (NEM) and methanethiosulfonate reagents was localized to a membrane-embedded pocket surrounding Asp-61. The cG58C substitution was profoundly inhibited by all the reagents tested, including membrane impermeant methanethiosulfonate reagents. Further studies of the highly reactive cG58C substitution revealed that NEM modification of a single c subunit in the oligomeric c-ring was sufficient to cause complete inhibition. In addition, NEM modification of subunit c was dependent upon the presence of subunit a. The results described here provide further evidence for an aqueous-accessible region at the interface of subunits a and c extending from the middle of the membrane to the cytoplasm.

Published

2008

22. Negative charges at protein kinase C sites of troponin I stabilize the inactive state of actin.

Author

Mathur MC, Kobayashi T, and Chalovich JM

Subjects

Adenosine Diphosphate metabolism, Adenosine Triphosphatases antagonists & inhibitors, Animals, Cattle, Crystallography, X-Ray, Enzyme Activation, Ethylmaleimide metabolism, Humans, Mice, Models, Biological, Muscle, Skeletal metabolism, Mutant Proteins metabolism, Mutation genetics, Myosins metabolism, Protein Binding, Rabbits, Thermodynamics, Troponin C chemistry, Troponin C metabolism, Troponin I chemistry, Actins metabolism, Protein Kinase C metabolism, Troponin I metabolism

Abstract

Alterations in the troponin complex can lead to increases or decreases in contractile activity. Most mutations of troponin that cause hypertrophic cardiomyopathy increase the activity of cardiac muscle fibers. In at least some cases these mutants stabilize the active state of regulated actin. In contrast, phosphorylation of troponin I at residues 43, 45, and 144 inhibits muscle contractility. To determine if alterations of troponin I that reduce activity do stabilize the inactive state of actin, we introduced negative charges at residues 43, 45, and 144 of troponin I to mimic a constitutively phosphorylated state. At saturating calcium, all mutants decreased ATPase rates relative to wild-type actin-tropomyosin-troponin. Reduced activation of ATPase activity was seen with a single mutation at S45E and was not further altered by mutating the other two sites. In the presence of low concentrations of NEM-S1, wild-type troponin was more active than the mutants. At high NEM-S1, the rates of wild-type and mutants approached the same limiting value. Changes in Ca(2+) affinity also support the idea that the equilibrium between states of actin-tropomyosin-troponin was shifted to the inactive state by mutations that mimic troponin I phosphorylation.

Published

2008

23. Formation of N-ethylmaleimide (NEM)-glutathione conjugate and N-ethylmaleamic acid revealed by mass spectral characterization of intracellular and extracellular microbial metabolites of NEM.

Author

Mojica ER, Kim S, and Aga DS

Subjects

Biotransformation, Chromatography, Liquid, Mass Spectrometry, Sewage microbiology, Culture Media chemistry, Cytosol chemistry, Ethylmaleimide metabolism, Maleates metabolism, Maleimides metabolism

Abstract

The extracellular and intracellular metabolites formed upon exposure of activated sludge microorganisms to a sublethal concentration of N-ethylmaleimide were monitored by liquid chromatography with ion trap mass spectrometry. The metabolite N-ethylsuccinimido-S-glutathione (m/z 433) was converted rapidly to N-(2-oxoethyl)-2,2-(propionylamino)propanamide (m/z 187) and N-ethylmaleamic acid (m/z 144).

Published

2008

24. COG-7-deficient Human Fibroblasts Exhibit Altered Recycling of Golgi Proteins.

Author

Steet R and Kornfeld S

Subjects

Adaptor Proteins, Vesicular Transport genetics, Brefeldin A pharmacology, Endoplasmic Reticulum metabolism, Ethylmaleimide metabolism, Fibroblasts chemistry, Fibroblasts drug effects, Fibroblasts metabolism, Glycosylation, Humans, Mannose-Binding Lectins analysis, Membrane Proteins analysis, Metabolic Diseases metabolism, Microtubules chemistry, Microtubules metabolism, Protein Transport, Qb-SNARE Proteins analysis, Qc-SNARE Proteins analysis, Adaptor Proteins, Vesicular Transport metabolism, Golgi Apparatus metabolism, Mannose-Binding Lectins metabolism, Membrane Proteins metabolism, Metabolic Diseases genetics, Qb-SNARE Proteins metabolism, Qc-SNARE Proteins metabolism

Abstract

Recently, we reported that two siblings presenting with the clinical syndrome congenital disorders of glycosylation (CDG) have mutations in the gene encoding Cog7p, a member of the conserved oligomeric Golgi (COG) complex. In this study, we analyzed the localization and trafficking of multiple Golgi proteins in patient fibroblasts under a variety of conditions. Although the immunofluorescent staining pattern of several Golgi proteins was indistinguishable from normal, the staining of endoplasmic reticulum (ER)-Golgi intermediate compartment (ERGIC)-53 and the vesicular-soluble N-ethylmaleimide-sensitive factor attachment protein receptors GS15 and GS28 was abnormal, and the steady-state level of GS15 was greatly decreased. Retrograde transport of multiple Golgi proteins to the ER in patient fibroblasts via brefeldin A-induced tubules was significantly slower than occurs in normal fibroblasts, whereas anterograde protein trafficking was much less affected. After prolonged treatment with brefeldin A, several Golgi proteins were detected in clusters that colocalize with the microtubule-organizing center in patient cells. All of these abnormalities were normalized in COG7-corrected patient fibroblasts. These results serve to better define the role of the COG complex in facilitating protein trafficking between the Golgi and ER and provide a diagnostic framework for the identification of CDG defects involving trafficking proteins.

Published

2006

25. NADPH dependent activation of microsomal glutathione transferase 1.

Author

Rinaldi R, Aniya Y, Svensson R, Eliasson E, Swedmark S, Shimoji M, and Morgenstern R

Subjects

Animals, Dithiothreitol pharmacology, Enzyme Activation drug effects, Enzyme Inhibitors pharmacology, Ethylmaleimide metabolism, Glutathione pharmacology, Hydrogen Peroxide pharmacology, Male, Microsomes, Liver drug effects, Rats, Rats, Sprague-Dawley, Superoxides pharmacology, Glutathione Transferase biosynthesis, Microsomes, Liver enzymology, NADP metabolism

Abstract

Microsomal glutathione transferase 1 (MGST1) can become activated up to 30-fold by several mechanisms in vitro (e.g. covalent modification by reactive electrophiles such as N-ethylmaleimide (NEM)). Activation has also been observed in vivo during oxidative stress. It has been noted that an NADPH generating system (g.s.) can activate MGST1 (up to 2-fold) in microsomal incubations, but the mechanism was unclear. We show here that NADPH g.s treatment impaired N-ethylmaleimide activation, indicating a shared target (identified as cysteine-49 in the latter case). Furthermore, NADPH activation was prevented by sulfhydryl compounds (glutathione and dithiothreitol). A well established candidate for activation would be oxidative stress, however we could exclude that oxidation mediated by cytochrome P450 2E1 (or flavine monooxygenase) was responsible for activation under a defined set of experimental conditions since superoxide or hydrogen peroxide alone did not activate the enzyme (in microsomes prepared by our routine procedure). Actually, the ability of MGST1 to become activated by hydrogen peroxide is critically dependent on the microsome preparation method (which influences hydrogen peroxide decomposition rate as shown here), explaining variable results in the literature. NADPH g.s. dependent activation of MGST1 could instead be explained, at least partly, by a direct effect observed also with purified enzyme (up to 1.4-fold activation). This activation was inhibited by sulfhydryl compounds and thus displays the same characteristics as that of the microsomal system. Whereas NADPH, and also ATP, activated purified MGST1, several nucleotide analogues did not, demonstrating specificity. It is thus an intriguing possibility that MGST1 function could be modulated by ligands (as well as reactive oxygen species) during oxidative stress when sulfhydryls are depleted.

Published

2004

26. Mycobacterium tuberculosis phagosome maturation arrest: mycobacterial phosphatidylinositol analog phosphatidylinositol mannoside stimulates early endosomal fusion.

Author

Vergne I, Fratti RA, Hill PJ, Chua J, Belisle J, and Deretic V

Subjects

Adenosine Triphosphate metabolism, Androstadienes pharmacology, Animals, Cells, Cultured, Endosomes drug effects, Enzyme Inhibitors pharmacology, Ethylmaleimide metabolism, Macrophages drug effects, Membrane Proteins metabolism, Mice, Phosphatidylinositol 3-Kinases metabolism, Phosphoinositide-3 Kinase Inhibitors, Qa-SNARE Proteins, Transport Vesicles drug effects, Transport Vesicles metabolism, Wortmannin, Endosomes metabolism, Macrophages metabolism, Mycobacterium tuberculosis metabolism, Phosphatidylinositols pharmacology, rab GTP-Binding Proteins metabolism

Abstract

Mycobacterium tuberculosis is a facultative intracellular pathogen that parasitizes macrophages by modulating properties of the Mycobacterium-containing phagosome. Mycobacterial phagosomes do not fuse with late endosomal/lysosomal organelles but retain access to early endosomal contents by an unknown mechanism. We have previously reported that mycobacterial phosphatidylinositol analog lipoarabinomannan (LAM) blocks a trans-Golgi network-to-phagosome phosphatidylinositol 3-kinase-dependent pathway. In this work, we extend our investigations of the effects of mycobacterial phosphoinositides on host membrane trafficking. We present data demonstrating that phosphatidylinositol mannoside (PIM) specifically stimulated homotypic fusion of early endosomes in an ATP-, cytosol-, and N-ethylmaleimide sensitive factor-dependent manner. The fusion showed absolute requirement for small Rab GTPases, and the stimulatory effect of PIM increased upon partial depletion of membrane Rabs with RabGDI. We found that stimulation of early endosomal fusion by PIM was higher when phosphatidylinositol 3-kinase was inhibited by wortmannin. PIM also stimulated in vitro fusion between model phagosomes and early endosomes. Finally, PIM displayed in vivo effects in macrophages by increasing accumulation of plasma membrane-endosomal syntaxin 4 and transferrin receptor on PIM-coated latex bead phagosomes. In addition, inhibition of phagosomal acidification was detected with PIM-coated beads. The effects of PIM, along with the previously reported action of LAM, suggest that M. tuberculosis has evolved a two-prong strategy to modify its intracellular niche: its products block acquisition of late endosomal/lysosomal constituents, while facilitating fusion with early endosomal compartments.

Published

2004

27. Labeling and quantifying sites of protein palmitoylation.

Author

Drisdel RC and Green WN

Subjects

Animals, Binding Sites, Biotinylation, Blotting, Western methods, Cell Line, Chickens, Ethylmaleimide metabolism, Genetic Vectors, Humans, Membrane Proteins metabolism, Mice, Nerve Tissue Proteins metabolism, Palmitates analysis, Protein Binding, Proteins analysis, Synaptosomal-Associated Protein 25, Transfection, Tritium metabolism, Palmitates metabolism, Proteins metabolism, Staining and Labeling methods

Abstract

As a reversible posttranslational modification, protein palmitoylation has the potential to regulate the trafficking and function of a variety of proteins. However, the extent, function, and dynamic nature of palmitoylation are poorly resolved because of limitations in assay methods. Here, we introduce methods where hydroxylamine-mediated cleavage of the palmitoyl-thioester bond generates a free sulfhydryl, which can then be specifically labeled with sulfhydryl-reactive reagents. This methodology is more sensitive and allows for quantitative estimates of palmitoylation. Unlike other techniques used to assay posttranslational modifications, the techniques we have developed can label all sites of modification with a variety of probes, radiolabeled or nonradioactive, and can be used to assay the palmitoylation of proteins expressed in vivo in brain or other tissues.

Published

2004

28. Membrane topology of ABC-type macrolide antibiotic exporter MacB in Escherichia coli.

Author

Kobayashi N, Nishino K, Hirata T, and Yamaguchi A

Subjects

ATP-Binding Cassette Transporters genetics, ATP-Binding Cassette Transporters metabolism, Amino Acid Sequence, Carbon Radioisotopes, Cell Membrane chemistry, Escherichia coli genetics, Ethylmaleimide metabolism, Molecular Sequence Data, Radioligand Assay, ATP-Binding Cassette Transporters chemistry, Escherichia coli chemistry, Escherichia coli Proteins

Abstract

MacB is an ABC-type membrane protein that exports only macrolide compounds containing 14- and 15-membered lactones, cooperating with a membrane fusion protein, MacA, and a multifunctional outer membrane channel, TolC. We determined the membrane topology of MacB by means of site-specific competitive chemical modification of single cysteine mutants. As a result, it was revealed that MacB is composed of four transmembrane (TM) segments with a cytoplasmic N-terminal nucleotide binding domain of about 270 amino acid residues and a periplasmic large hydrophilic polypeptide between TM segments 1 and 2 of about 200 amino acid residues.

Published

2003

29. Transport of L-arginine and nitric oxide formation in human platelets.

Author

Signorello MG, Pascale R, and Leoncini G

Subjects

Anti-Bacterial Agents pharmacology, Biological Transport, Blood Platelets drug effects, Cyclic GMP metabolism, Enzyme Inhibitors metabolism, Ethylmaleimide metabolism, Gramicidin pharmacology, Humans, Ionophores pharmacology, Leucine metabolism, Quaternary Ammonium Compounds pharmacology, Sodium metabolism, Valinomycin pharmacology, Arginine metabolism, Blood Platelets metabolism, Membrane Transport Proteins metabolism, Nitric Oxide metabolism

Abstract

The results of the present study show that human platelets take up l-arginine by two transport systems which are compatible with the systems y+ and y+L. These Na+independent transporters have been distinguished by treating platelets with N-ethylmaleimide that blocks selectively system y+. System y+, that accounts for 30-40% of the total transport, is characterized by low affinity for l-arginine, is unaffected by l-leucine, is sensitive to changes of membrane potential and to trans-stimulation. The other component of l-arginine transport identified with the system y+L (approximately 60-70% of the total flux) shows high affinity for l-arginine, is insensitive to N-ethylmaleimide treatment, unaffected by changes in membrane potential, sensitive to trans-stimulation and inhibited by l-leucine in the presence of Na+. Moreover a strict correlation between l-arginine transport and nitric oxide (NO) production in whole cells was found. N-ethylmaleimide and l-leucine decreased NO production as well as cGMP elevation, and the effect on NO and cGMP were closely related. It is likely that the l-arginine transport systems y+ and y+L are both involved in supplying substrate for NO production and regulation in human platelets.

Published

2003

30. Characterization of AtCDC48. Evidence for multiple membrane fusion mechanisms at the plane of cell division in plants.

Author

Rancour DM, Dickey CE, Park S, and Bednarek SY

Subjects

Adenosine Triphosphatases metabolism, Adenosine Triphosphate metabolism, Arabidopsis cytology, Arabidopsis genetics, Arabidopsis Proteins genetics, Arabidopsis Proteins metabolism, Carrier Proteins genetics, Carrier Proteins metabolism, Cell Cycle Proteins genetics, Cell Division physiology, Ethylmaleimide metabolism, Immunohistochemistry, Membrane Proteins genetics, Membrane Proteins metabolism, Microscopy, Fluorescence, N-Ethylmaleimide-Sensitive Proteins, Nuclear Proteins metabolism, Protein Isoforms, Qa-SNARE Proteins, SNARE Proteins, Soluble N-Ethylmaleimide-Sensitive Factor Attachment Proteins, Valosin Containing Protein, Arabidopsis physiology, Cell Cycle Proteins metabolism, Membrane Fusion physiology, Vesicular Transport Proteins

Abstract

The components of the cellular machinery that accomplish the various complex and dynamic membrane fusion events that occur at the division plane during plant cytokinesis, including assembly of the cell plate, are not fully understood. The most well-characterized component, KNOLLE, a cell plate-specific soluble N-ethylmaleimide-sensitive fusion protein (NSF)-attachment protein receptor (SNARE), is a membrane fusion machine component required for plant cytokinesis. Here, we show the plant ortholog of Cdc48p/p97, AtCDC48, colocalizes at the division plane in dividing Arabidopsis cells with KNOLLE and another SNARE, the plant ortholog of syntaxin 5, SYP31. In contrast to KNOLLE, SYP31 resides in defined punctate membrane structures during interphase and is targeted during cytokinesis to the division plane. In vitro-binding studies demonstrate that AtCDC48 specifically interacts in an ATP-dependent manner with SYP31 but not with KNOLLE. In contrast, we show that KNOLLE assembles in vitro into a large approximately 20S complex in an Sec18p/NSF-dependent manner. These results suggest that there are at least two distinct membrane fusion pathways involving Cdc48p/p97 and Sec18p/NSF that operate at the division plane to mediate plant cytokinesis. Models for the role of AtCDC48 and SYP31 at the division plane will be discussed.

Published

2002

31. Binding of the beta2 adrenergic receptor to N-ethylmaleimide-sensitive factor regulates receptor recycling.

Author

Cong M, Perry SJ, Hu LA, Hanson PI, Claing A, and Lefkowitz RJ

Subjects

Animals, Binding Sites, Blotting, Western, COS Cells, Carrier Proteins chemistry, Cell Line, Glutathione Transferase metabolism, Green Fluorescent Proteins, Humans, Immunoblotting, Isoproterenol pharmacology, Luminescent Proteins metabolism, Mutation, N-Ethylmaleimide-Sensitive Proteins, Precipitin Tests, Propranolol pharmacology, Protein Binding, Protein Structure, Tertiary, Receptors, Adrenergic, beta-2 chemistry, Recombinant Fusion Proteins metabolism, Spectrometry, Fluorescence, Time Factors, Two-Hybrid System Techniques, Carrier Proteins metabolism, Ethylmaleimide metabolism, Receptors, Adrenergic, beta-2 metabolism, Vesicular Transport Proteins

Abstract

Following agonist stimulation, most G protein-coupled receptors become desensitized and are internalized, either to be degraded or recycled back to the cell surface. What determines the fate of a specific receptor type after it is internalized is poorly understood. Here we show that the rapidly recycling beta2 adrenergic receptor (beta2AR) binds via a determinant including the last three amino acids in its carboxyl-terminal tail to the membrane fusion regulatory protein, N-ethylmaleimide-sensitive factor (NSF). This is documented by in vitro overlay assays and by cellular coimmunoprecipitations. Receptors bearing mutations in any of the last three residues fail to interact with NSF. After stimulation with the agonist isoproterenol, a green fluorescent protein fusion of NSF colocalizes with the wild type beta2AR but not with a tail-mutated beta2AR. The beta2AR-NSF interaction is required for efficient internalization of the receptors and for their recycling to the cell surface. Mutations in the beta2AR tail that ablate NSF binding reduce the efficiency of receptor internalization upon agonist stimulation. Upon subsequent treatment of cells with the antagonist propranolol, wild type receptors return to the cell surface, while tail-mutated receptors remain sequestered. Thus, the direct binding of the beta2AR to NSF demonstrates how, after internalization, the fate of a receptor is reliant on a specific interaction with a component of the cellular membrane-trafficking machinery.

Published

2001

32. Complete cysteine-scanning mutagenesis and site-directed chemical modification of the Tn10-encoded metal-tetracycline/H+ antiporter.

Author

Tamura N, Konishi S, Iwaki S, Kimura-Someya T, Nada S, and Yamaguchi A

Subjects

Amino Acid Sequence, Antiporters chemistry, Antiporters metabolism, Bacterial Proteins chemistry, Bacterial Proteins metabolism, Ethylmaleimide chemistry, Ethylmaleimide metabolism, Molecular Sequence Data, Mutagenesis, Site-Directed, Antiporters genetics, Bacterial Proteins genetics, Cysteine genetics, DNA Transposable Elements

Abstract

Bacterial Tn10-encoded metal-tetracycline/H(+) antiporter was the first found drug exporter and has been studied as a paradigm of antiporter-type major facilitator superfamily transporters. Here the 400 amino acid residues of this protein were individually replaced by cysteine except for the initial methionine. As a result, we could obtain a complete map of the functionally or structurally important residues. In addition, we could determine the precise boundaries of all the transmembrane segments on the basis of the reactivity with N-ethylmaleimide (NEM). The NEM binding results indicated the presence of a transmembrane water-filled channel in the transporter. The twelve transmembrane segments can be divided into three groups; four are totally embedded in the hydrophobic interior, four face a putative water-filled channel along their full length, and the remaining four face the channel for half their length, the other halves being embedded in the hydrophobic interior. These three types of transmembrane segments are mutually arranged with a 4-fold symmetry. The competitive binding of membrane-permeable and -impermeable SH reagents in intact cells indicates that the transmembrane water-filled channel has a thin barrier against hydrophilic molecules in the middle of the transmembrane region. Inhibition and stimulation of NEM binding in the presence of tetracycline reflects the substrate-induced protection or conformational change of the Tn10-encoded metal-tetracycline/H(+) antiporter. The mutations protected from NEM binding by tetracycline were mainly located around the permeability barrier in the N-terminal half, suggesting the location of the substrate binding site.

Published

2001

33. Mapping of contact sites in complex formation between transducin and light-activated rhodopsin by covalent crosslinking: use of a photoactivatable reagent.

Author

Cai K, Itoh Y, and Khorana HG

Subjects

Amino Acid Sequence, Animals, Azides chemistry, Azides metabolism, Binding Sites, COS Cells, Cattle, Cross-Linking Reagents chemistry, Cysteine genetics, Cysteine metabolism, Disulfides chemistry, Disulfides metabolism, Dithiothreitol metabolism, Ethylmaleimide metabolism, Guanosine Diphosphate metabolism, Light, Lysine analogs & derivatives, Lysine chemistry, Lysine metabolism, Maleimides chemistry, Maleimides metabolism, Models, Molecular, Molecular Sequence Data, Mutation genetics, Protein Binding, Protein Structure, Secondary, Pyridines chemistry, Pyridines metabolism, Rhodopsin chemistry, Rhodopsin genetics, Sepharose metabolism, Spectrometry, Mass, Matrix-Assisted Laser Desorption-Ionization, Transducin chemistry, Trypsin metabolism, Ultraviolet Rays, Cross-Linking Reagents metabolism, Photolysis radiation effects, Rhodopsin metabolism, Transducin metabolism

Abstract

Interaction of light-activated rhodopsin with transducin (T) is the first event in visual signal transduction. We use covalent crosslinking approaches to map the contact sites in interaction between the two proteins. Here we use a photoactivatable reagent, N-[(2-pyridyldithio)-ethyl], 4-azido salicylamide. The reagent is attached to the SH group of cytoplasmic monocysteine rhodopsin mutants by a disulfide-exchange reaction with the pyridylthio group, and the derivatized rhodopsin then is complexed with T by illumination at lambda >495 nm. Subsequent irradiation of the complex at lambda310 nm generates covalent crosslinks between the two proteins. Crosslinking was demonstrated between T and a number of single cysteine rhodopsin mutants. However, sites of crosslinks were investigated in detail only between T and the rhodopsin mutant S240C (cytoplasmic loop V-VI). Crosslinking occurred predominantly with T(alpha). For identification of the sites of crosslinks in T(alpha), the strategy used involved: (i) derivatization of all of the free cysteines in the crosslinked proteins with N-ethylmaleimide; (ii) reduction of the disulfide bond linking the two proteins and isolation of all of the T(alpha) species carrying the crosslinked moiety with a free SH group; (iii) adduct formation of the latter with the N-maleimide moiety of the reagent, maleimido-butyryl-biocytin, containing a biotinyl group; (iv) trypsin degradation of the resulting T(alpha) derivatives and isolation of T(alpha) peptides carrying maleimido-butyryl-biocytin by avidin-agarose chromatography; and (v) identification of the isolated peptides by matrix-assisted laser desorption/ionization time-of-flight mass spectrometry. We found that crosslinking occurred mainly to two C-terminal peptides in T(alpha) containing the amino acid sequences 310-313 and 342-345.

Published

2001

34. Endothelial transcytotic machinery involves supramolecular protein-lipid complexes.

Author

Predescu SA, Predescu DN, and Palade GE

Subjects

Animals, Biological Transport, Caveolin 1, Caveolins metabolism, Cells, Cultured, Cross-Linking Reagents metabolism, Endothelium, Vascular cytology, Humans, Macromolecular Substances, Membrane Proteins metabolism, Microscopy, Electron, N-Ethylmaleimide-Sensitive Proteins, Qa-SNARE Proteins, Rats, Rats, Sprague-Dawley, Recombinant Fusion Proteins metabolism, Staining and Labeling, Succinimides metabolism, Vesicle-Associated Membrane Protein 3, Carrier Proteins metabolism, Cytosol metabolism, Endothelium, Vascular metabolism, Ethylmaleimide metabolism, Lipid Metabolism, Proteins metabolism, Vesicular Transport Proteins

Abstract

We have demonstrated that the plasmalemmal vesicles (caveolae) of the continuous microvascular endothelium function as transcytotic vesicular carriers for protein molecules > 20 A and that transcytosis is an N-ethylmaleimide-sensitive factor (NSF)-dependent, N-ethylmaleimide-sensitive process. We have further investigated NSF interactions with endothelial proteins to find out 1) whether a complete set of fusion and targeting proteins is present in the endothelium; 2) whether they are organized in multimolecular complexes as in neurons; and 3) whether the endothelial multimolecular complexes differ from their neuronal counterparts, because of their specialized role in transcytosis. To generate the complexes, we have used myc-NSF, cultured pulmonary endothelial cells, and rat lung cytosol and membrane preparations; to detect them we have applied coimmunoprecipitation with myc antibodies; and to characterize them we have used velocity sedimentation and cross-linking procedures. We have found that both cytosolic and membrane fractions contain complexes that comprise beside soluble NSF attachment proteins and SNAREs (soluble NSF attachment protein receptor), rab 5, dynamin, caveolin, and lipids. By immunogold labeling and negative staining we have detected in these complexes, myc-NSF, syntaxin, dynamin, caveolin, and endogenous NSF. Similar complexes are formed by endogenous NSF. The results indicate that complexes with a distinct protein-lipid composition exist and suggest that they participate in targeting, fusion, and fission of caveolae with the endothelial plasmalemma.

Published

2001

35. Cysteine residues in the D-galactose-H+ symport protein of Escherichia coli: effects of mutagenesis on transport, reaction with N-ethylmaleimide and antibiotic binding.

Author

McDonald TP and Henderson PJ

Subjects

Amino Acid Sequence, Base Sequence, Biological Transport, Colforsin metabolism, Cytochalasin B metabolism, DNA Primers, Eosine Yellowish-(YS) analogs & derivatives, Eosine Yellowish-(YS) metabolism, Galactose metabolism, Molecular Sequence Data, Monosaccharide Transport Proteins chemistry, Monosaccharide Transport Proteins genetics, Mutagenesis, Site-Directed, Protein Binding, Anti-Bacterial Agents metabolism, Calcium-Binding Proteins, Cysteine genetics, Ethylmaleimide metabolism, Monosaccharide Transport Proteins metabolism, Periplasmic Binding Proteins

Abstract

The galactose-H(+) membrane-transport protein, GalP, of Escherichia coli is similar in substrate specificity and susceptibility to cytochalasin B and forskolin, to the human GLUT1 sugar-transport protein; furthermore, they are about 30% identical in amino acid sequence. Transport activities of both GalP and GLUT1 are inhibited by the thiol-group-specific reagent, N-ethylmaleimide. GalP contains only three cysteine residues at positions 19, 374 and 389, each of which we have mutated, singly and in combination, to serine. Each single change of Cys-->Ser has only a minor effect on transport activity, whereas alteration of all three simultaneously profoundly diminishes V(max) for transport. The high level of expression of the GalP protein facilitates measurements of the reactivity of each mutant with N-ethylmaleimide or eosin 5-maleimide, which conclusively demonstrate that Cys(374) is the site of covalent modification by the reagents. By comparing the reactivity of Cys(374) in right-side-out and inside-out vesicles it appears that Cys(374) is located on the cytoplasmic face of the GalP protein. Although impaired in transport activity, the 'Cys-free' mutant, with all three cysteine residues mutated into serine, binds cytochalasin B and forskolin with wild-type affinities. All these results are interpreted in terms of a 12-helix model of the folding of the protein, in which the relative orientations of helix 10, containing the reactive Cys(374) residue, and helix 11, containing the unreactive Cys(389) residue, can now be defined.

Published

2001

36. Reaction of S-nitrosoglutathione with the heme group of deoxyhemoglobin.

Author

Spencer NY, Zeng H, Patel RP, and Hogg N

Subjects

Cell Line, Chromatography, High Pressure Liquid, Electron Spin Resonance Spectroscopy, Ethylmaleimide metabolism, Glutathione metabolism, Humans, Luminescent Measurements, Nitric Oxide metabolism, Pentetic Acid metabolism, S-Nitrosoglutathione, Ultrafiltration, Glutathione analogs & derivatives, Heme metabolism, Hemoglobins metabolism, Nitroso Compounds metabolism

Abstract

The mechanism of interaction between S-nitrosoglutathione (GSNO) and hemoglobin is a crucial component of hypotheses concerning the role played by S-nitrosohemoglobin in vivo. We previously demonstrated (Patel, R. P., Hogg, N., Spencer, N. Y., Kalyanaraman, B., Matalon, S., and Darley-Usmar, V. M. (1999) J. Biol. Chem. 274, 15487-15492) that transnitrosation between oxygenated hemoglobin and GSNO is a slow, reversible process, and that the reaction between GSNO and deoxygenated hemoglobin (deoxyHb) did not conform to second order reversible kinetics. In this study we have reinvestigated this reaction and show that GSNO reacts with deoxyHb to form glutathione, nitric oxide, and ferric hemoglobin. Nitric oxide formed from this reaction is immediately autocaptured to form nitrosylated hemoglobin. GSNO reduction by deoxyHb is essentially irreversible. The kinetics of this reaction depended upon the conformation of the protein, with more rapid kinetics occurring in the high oxygen affinity state (i.e. modification of the Cysbeta-93) than in the low oxygen affinity state (i.e. treatment with inositol hexaphosphate). A more rapid reaction occurred when deoxymyoglobin was used, further supporting the observation that the kinetics of reduction are directly proportional to oxygen affinity. This observation provides a mechanism for how deoxygenation of hemoglobin/myoglobin could facilitate nitric oxide release from S-nitrosothiols and represents a potential physiological mechanism of S-nitrosothiol metabolism.

Published

2000

37. Low N-ethylmaleimide concentrations activate ryanodine receptors by a reversible interaction, not an alkylation of critical thiols.

Author

Menshikova EV, Cheong E, and Salama G

Subjects

Alkylation, Animals, Calcium metabolism, Muscle, Skeletal metabolism, Nitric Oxide metabolism, Rabbits, Ruthenium Red metabolism, Ryanodine metabolism, Sarcoplasmic Reticulum metabolism, Ethylmaleimide metabolism, Ryanodine Receptor Calcium Release Channel metabolism, Sulfhydryl Compounds metabolism

Abstract

Previous studies proposed that N-ethylmaleimide (NEM) alkylates 3 classes of thiols on skeletal muscle ryanodine receptors (RyRs) producing 3 phases of channel modification, as function of time and concentration. NEM (5 mm) decreased, increased, and then decreased the open probability (P(o)) of the channel by thiol alkylation, a reaction not reversed by reducing agents. We now show that low NEM concentrations (20-200 microm) elicit Ca(2+) release from sarcoplasmic reticulum (SR) vesicles, but contrary to expectations, the effect was fully reversed by reducing agents or by washing SR vesicles. In bilayers, NEM (0.2 mm) increased P(o) of RyRs within seconds when added to the cis (not trans) side, and dithiothreitol (DTT; 1 mm) decreased P(o) in seconds. High (5 mm) NEM concentrations elicited SR Ca(2+) release that was not reversed by DTT, as expected for an alkylation reaction. A non-sulfhydryl reagent structurally related to NEM, N-ethylsuccinimide (0.1-0.5 mm), also elicited SR Ca(2+) release that was not reversed by DTT (1 mm). Other alkylating agents elicited SR Ca(2+) release, which was fully (N-methylmaleimide) or partially (iodoacetic acid) reversed by DTT and inhibited by ruthenium red. Nitric oxide (NO) donors at concentrations that did not activate RyRs inhibited NEM-induced Ca(2+) release, most likely by an interaction of NO with NEM rather than an inactivation of RyRs by NO. Thus, at low concentrations, NEM does not act as a selective thiol reagent and activates RyRs without alkylating critical thiols indicating that the multiple phases of ryanodine binding are unrelated to RyR activity or to NEM alkylation of RyRs.

Published

2000

38. Identification of a cysteine residue in the active site of nitroalkane oxidase by modification with N-ethylmaleimide.

Author

Gadda G, Banerjee A, Dangott LJ, and Fitzpatrick PF

Subjects

Amino Acid Sequence, Binding Sites drug effects, Chromatography, High Pressure Liquid, Cysteine chemistry, Flavin-Adenine Dinucleotide metabolism, Flavoproteins chemistry, Flavoproteins metabolism, Half-Life, Kinetics, Mass Spectrometry, Molecular Sequence Data, Oxygenases antagonists & inhibitors, Peptide Fragments chemistry, Peptide Fragments metabolism, Peptide Mapping, Sequence Analysis, Protein, Trypsin metabolism, Valerates pharmacology, Cysteine metabolism, Dioxygenases, Ethylmaleimide metabolism, Fusarium enzymology, Oxygenases chemistry, Oxygenases metabolism

Abstract

The flavoprotein nitroalkane oxidase catalyzes the oxidative denitrification of primary or secondary nitroalkanes to the corresponding aldehydes or ketones with production of hydrogen peroxide and nitrite. The enzyme is irreversibly inactivated by treatment with N-ethylmaleimide at pH 7. The inactivation is time-dependent and shows first-order kinetics for three half-lives. The second-order rate constant for inactivation is 3.4 +/- 0.06 m(-)(1) min(-)(1). The competitive inhibitor valerate protects the enzyme from inactivation, indicating an active site-directed modification. Comparison of tryptic maps of enzyme treated with N-[ethyl-1-(14)C]maleimide in the absence and presence of valerate shows a single radioactive peptide differentially labeled in the unprotected enzyme. The sequence of this peptide was determined to be LLNEVMCYPLFDGGNIGLR using Edman degradation and matrix-assisted laser desorption/ionization time-of-flight mass spectrometry. The cysteine residue was identified as the site of alkylation by ion trap mass spectrometry.

Published

2000

39. Cysteine-scanning mutagenesis of transmembrane segments 4 and 5 of the Tn10-encoded metal-tetracycline/H+ antiporter reveals a permeability barrier in the middle of a transmembrane water-filled channel.

Author

Iwaki S, Tamura N, Kimura-Someya T, Nada S, and Yamaguchi A

Subjects

Amino Acid Sequence, Antiporters chemistry, Antiporters metabolism, Bacterial Proteins chemistry, Bacterial Proteins metabolism, Binding Sites, Biological Transport, Ethylmaleimide metabolism, Molecular Sequence Data, Mutagenesis, Site-Directed, Protein Conformation, Sequence Homology, Amino Acid, Stilbenes metabolism, Sulfonic Acids metabolism, Tetracycline metabolism, Antiporters genetics, Bacterial Proteins genetics, DNA Transposable Elements

Abstract

Cysteine-scanning mutants as to putative transmembrane segments 4 and 5 and the flanking regions of Tn10-encoded metal-tetracycline/H(+) antiporter (TetA(B)) were constructed. All mutants were normally expressed. Among the 57 mutants (L99C to I155C), nine conserved arginine-, aspartate-, and glycine-replaced ones exhibited greatly reduced tetracycline resistance and almost no transport activity, and five conserved glycine- and proline-replaced mutants exhibited greatly reduced tetracycline transport activity in inverted membrane vesicles despite their high or moderate drug resistance. All other cysteine-scanning mutants retained normal drug resistance and normal tetracycline transport activity except for the L142C and I143C mutants. The transmembrane (TM) regions TM4 and TM5 were determined to comprise 20 amino acid residues, Leu-99 to Ile-118, and 17 amino acid residues, Ala-136 to Ala-152, respectively, on the basis of N-[(14)C]ethylmaleimide ([(14)C]NEM) reactivity. The NEM reactivity patterns of the TM4 and TM5 mutants were quite different from each other. TM4 could be divided into two halves, that is, a NEM nonreactive periplasmic half and a periodically reactive cytoplasmic half, indicating that TM4 is tilted toward a water-filled transmembrane channel and that only its cytoplasmic half faces the channel. On the other hand, NEM-reactive mutations were observed periodically (every two residues) along the whole length of TM5. A permeability barrier for a membrane-impermeable sulfhydryl reagent, 4-acetamido-4'-maleimidylstilbene-2,2'-disulfonic acid, was present in the middle of TM5 between Leu-142 and Gly-145, whereas all the NEM-reactive mutants as to TM4 were not accessible to 4-acetamido-4'-maleimidylstilbene-2,2'-disulfonic acid, indicating that the channel-facing side of TM4 is located inside the permeability barrier. Tetracycline protected the G141C mutant from the NEM binding, whereas the other mutants in TM4 and TM5 were not protected by tetracycline.

Published

2000

40. SNAREs in mammalian sperm: possible implications for fertilization.

Author

Ramalho-Santos J, Moreno RD, Sutovsky P, Chan AW, Hewitson L, Wessel GM, Simerly CR, and Schatten G

Subjects

Acrosome Reaction, Animals, Blotting, Western, Cattle, Cricetinae, Electrophoresis, Polyacrylamide Gel, Fertilization in Vitro, Humans, Immunohistochemistry, Macaca mulatta, Male, Membrane Fusion, Membrane Glycoproteins biosynthesis, Membrane Proteins biosynthesis, Mice, Microscopy, Electron, Nerve Tissue Proteins biosynthesis, R-SNARE Proteins, Sperm Injections, Intracytoplasmic, Spermatozoa cytology, Synaptotagmin I, Synaptotagmins, Calcium-Binding Proteins, Ethylmaleimide metabolism, Fertilization genetics, Fertilization physiology, Spermatozoa metabolism

Abstract

Soluble N-ethylmalameide-sensitive factor attachment protein receptor (SNARE) proteins are present in mammalian sperm and could be involved in critical membrane fusion events during fertilization, namely the acrosome reaction. Vesicle-associated membrane protein/synaptobrevin, a SNARE on the membrane of a vesicular carrier, and syntaxin 1, a SNARE on the target membrane, as well as the calcium sensor synaptotagmin I, are present in the acrosome of mammalian sperm (human, rhesus monkey, bull, hamster, mouse). Sperm SNAREs are sloughed off during the acrosome reaction, paralleling the release of sperm membrane vesicles and acrosomal contents, and SNARE antibodies inhibit both the acrosome reaction and fertilization, without inhibiting sperm-egg binding. In addition, sperm SNAREs may be responsible, together with other sperm components, for the asynchronous male DNA decondensation that occurs following intracytoplasmic sperm injection, an assisted reproduction technique that bypasses normal sperm-egg surface interactions. The results suggest the participation of sperm SNAREs during membrane fusion events at fertilization in mammals., (Copyright 2000 Academic Press.)

Published

2000

41. Cysteine-scanning mutagenesis around transmembrane segments 1 and 11 and their flanking loop regions of Tn10-encoded metal-Tetracycline/H+ antiporter.

Author

Kimura-Someya T, Iwaki S, Konishi S, Tamura N, Kubo Y, and Yamaguchi A

Subjects

Amino Acid Sequence, Carbon Radioisotopes, Disulfides metabolism, Ethylmaleimide metabolism, Molecular Sequence Data, Mutagenesis, Site-Directed, Antiporters genetics, Bacterial Proteins genetics, Cysteine genetics, DNA Transposable Elements, Membrane Proteins genetics

Abstract

Putative transmembrane helices (TM) 1 and 11 in the metal-tetracycline/H(+) antiporter are predicted to be close to each other on the basis of disulfide cross-linking experiments of the double-cysteine mutants in the periplasmic loop regions (Kubo, Y., Konishi, S., Kawabe, T., Nada, S., and Yamaguchi, A. (2000) J. Biol. Chem. 275, 5270-5274). In this study, each amino acid from Asn-2 to Gly-44 in the putative TM1 and loop1-2 regions or that from Ser-328 to Gly-366 in TM11 and its flanking regions was individually replaced with cysteine. With respect to the TM1 region, 10 mutants, from T5C to L14C, were all not reactive with N-ethylmaleimide (NEM), and from D15C to I22C, NEM-reactive and non-reactive mutations periodically appeared every two residues. Three mutants, M23C to V25C, were all NEM-reactive, but the degree of the latter two mutants was very low. Seven mutants, from L26C to E32C, were all highly reactive with NEM. Therefore, the region of TM1 is composed of the 21 amino acid residues from Thr-5 to Val-25. It is a partially amphiphilic helix, that is, the N-terminal (cytoplasmic) half is embedded in the hydrophobic interior, and the C-terminal (periplasmic) half faces a water-filled channel. With respect to TM11, nine mutants, from S328C to G336C, and six mutants, from L361C to G366C, were all reactive with NEM. On the other hand, out of the 24 mutants, from L337C to S360C, 17 were not reactive with NEM, and the 7 NEM-reactive mutants were scattered, indicating that this region is a transmembrane segment. The 7 residues from Val-347 to Phe-353 including Pro-350 formed a central hydrophobic core, and the 7 NEM-reactive mutations were periodically distributed in its flanking regions, indicating that both ends of TM11 face a water-filled channel. Ala-354 is located at about 1/3 of the length from the periplasmic end of TM11. Disulfide cross-linking experiments on double-cysteine mutants having the combination of A354C and a cysteine-scanning mutation in the loop1-2 region indicated that loop1-2 is very flexible and close to the periplasmic end of TM11. Tetracycline prevented the cross-linking formation between the periplasmic ends of TM1 and TM11; however, it did not affect the cross-linking between loop1-2 and TM11, indicating that the substrate-induced conformational change involves a shift in the relative locations of TM1 and TM11.

Published

2000

42. Glutathione-dependent conversion of N-ethylmaleimide to the maleamic acid by Escherichia coli: an intracellular detoxification process.

Author

McLaggan D, Rufino H, Jaspars M, and Booth IR

Subjects

Escherichia coli growth & development, Glutathione analogs & derivatives, Magnetic Resonance Spectroscopy, Maleimides metabolism, NAD metabolism, Succinimides metabolism, Escherichia coli metabolism, Ethylmaleimide metabolism, Glutathione metabolism, Maleates metabolism

Abstract

The electrophile N-ethylmaleimide (NEM) elicits rapid K(+) efflux from Escherichia coli cells consequent upon reaction with cytoplasmic glutathione to form an adduct, N-ethylsuccinimido-S-glutathione (ESG) that is a strong activator of the KefB and KefC glutathione-gated K(+) efflux systems. The fate of the ESG has not previously been investigated. In this report we demonstrate that NEM and N-phenylmaleimide (NPM) are rapidly detoxified by E. coli. The detoxification occurs through the formation of the glutathione adduct of NEM or NPM, followed by the hydrolysis of the imide bond after which N-substituted maleamic acids are released. N-ethylmaleamic acid is not toxic to E. coli cells even at high concentrations. The glutathione adducts are not released from cells, and this allows glutathione to be recycled in the cytoplasm. The detoxification is independent of new protein synthesis and NAD(+)-dependent dehydrogenase activity and entirely dependent upon glutathione. The time course of the detoxification of low concentrations of NEM parallels the transient activation of the KefB and KefC glutathione-gated K(+) efflux systems.

Published

2000

43. Assignment of a single disulfide bridge in rat liver methionine adenosyltransferase.

Author

Martínez-Chantar ML and Pajares MA

Subjects

Amino Acid Sequence, Animals, Cellulase metabolism, Cysteine metabolism, Dimerization, Dithiothreitol metabolism, Ethylmaleimide metabolism, Molecular Sequence Data, Nitric Oxide Donors metabolism, Peptide Fragments chemistry, Peptide Fragments metabolism, Peptide Mapping, Protein Denaturation drug effects, Protein Structure, Quaternary drug effects, Rats, Sequence Analysis, Protein, Trypsin metabolism, Urea pharmacology, Disulfides metabolism, Liver enzymology, Methionine Adenosyltransferase chemistry, Methionine Adenosyltransferase metabolism

Abstract

Rat liver methionine adenosyltransferase incorporated 8 mol of N-ethylmaleimide per mol of subunit upon denaturation in the presence of 8 M urea, whereas 10 such groups were labelled when dithiothreitol was also included. This observation prompted a re-examination of the state of the thiol groups, which was carried out using peptide mapping, amino acid analysis and N-terminal sequencing. The results obtained revealed a disulfide bridge between Cys35 and Cys61. This disulfide did not appear to be conserved because cysteines homologous to residue 61 do not exist in methionine adenosyltransferases of other origins, therefore suggesting its importance for the differential aspects of the liver-specific enzyme.

Published

2000

44. Kinase-dependent change in the conformation of the leukocyte NADPH oxidase subunit p47phox.

Author

Park JW, Park HS, and Chang YM

Subjects

Cyclic AMP-Dependent Protein Kinases metabolism, Enzyme Activation, Ethylmaleimide metabolism, Humans, Mitogen-Activated Protein Kinases metabolism, Mutation, Neutrophil Activation, Phosphoproteins genetics, Phosphorylation, Protein Kinase C metabolism, Recombinant Proteins chemistry, Spectrometry, Fluorescence, Tryptophan chemistry, NADPH Oxidases chemistry, Neutrophils enzymology, Phosphoproteins chemistry, Protein Conformation

Abstract

The leukocyte NADPH oxidase of neutrophils is a membrane-bound enzyme that catalyzes the production of O2- from oxygen using NADPH as the electron donor. Dormant in resting neutrophils, the enzyme acquires catalytic activity when the cells are exposed to appropriate stimuli. During activation, the cytosolic oxidase components p47phox and p67phox migrate to the plasma membrane, where they associate with cytochrome b558, a membrane-integrated flavohemoprotein, to assemble the active oxidase. In whole cells and under certain circumstances in the cell-free system, the phosphorylation of p47phox mediates the activation process. It has been proposed that conformational changes in the protein structure of cytosolic factor p47phox may be an important part of the activation mechanism. The total protein steady-state intrinsic fluorescence (an emission maximum of 338 nm) exhibited by the tryptophan residues of p47phox was substantially decreased, reflecting on the conformational change that occurs when p47phox was phosphorylated with protein kinase C. We show here that the phosphorylation of p47phox by protein kinase A or mitogen-activated protein kinase, however, had little effect on the intrinsic fluorescence of p47phox. In addition, the present experiments indicate that in the mutant p47phoxS379A, only the single S-->A mutation appears to be a major importance for the function of p47phox, which is able to undergo the change in conformation that takes place when p47phox is phosphorylated by protein kinase C.

Published

1999

45. A role for cysteine 3635 of RYR1 in redox modulation and calmodulin binding.

Author

Porter Moore C, Zhang JZ, and Hamilton SL

Subjects

Alkylation, Amino Acid Sequence, Animals, Cysteine, Ethylmaleimide metabolism, Molecular Sequence Data, Oxidation-Reduction, Rabbits, Ryanodine Receptor Calcium Release Channel chemistry, Structure-Activity Relationship, Calmodulin metabolism, Ryanodine Receptor Calcium Release Channel metabolism

Abstract

Oxidation of the skeletal muscle Ca(2+) release channel (RYR1) increases its activity, produces intersubunit disulfide bonds, and blocks its interaction with calmodulin. Conversely, bound calmodulin protects RYR1 from the effects of oxidants (Zhang, J.-Z., Wu, Y., Williams, B. Y., Rodney, G., Mandel, F., Strasburg, G. M., and Hamilton, S. L. (1999) Am. J. Physiol. 276, Cell Physiol. C46-C53). In addition, calmodulin protects RYR1 from trypsin cleavage at amino acids 3630 and 3637 (Moore, C. P., Rodney, G., Zhang, J.-Z., Santacruz-Toloza, L., Strasburg, G. M., and Hamilton, S. L. (1999) Biochemistry 38, 8532-8537). The sequence between these two tryptic sites is AVVACFR. Alkylation of RYR1 with N-ethylmaleimide (NEM) blocks both (35)S-apocalmodulin binding and oxidation-induced intersubunit cross-linking. In the current work, we demonstrate that both cysteines needed for the oxidation-induced intersubunit cross-link are protected from alkylation with N-ethylmaleimide by bound calmodulin. We also show, using N-terminal amino acid sequencing together with analysis of the distribution of [(3)H]NEM labeling with each sequencing cycle, that cysteine 3635 of RYR1 is rapidly labeled by NEM and that this labeling is blocked by bound calmodulin. We propose that cysteine 3635 is located at an intersubunit contact site that is close to or within a calmodulin binding site. These findings suggest that calmodulin and oxidation modulate RYR1 activity by regulating intersubunit interactions in a mutually exclusive manner and that these interactions involve cysteine 3635.

Published

1999

46. Cysteine-scanning mutagenesis around transmembrane segment VI of Tn10-encoded metal-tetracycline/H(+) antiporter.

Author

Konishi S, Iwaki S, Kimura-Someya T, and Yamaguchi A

Subjects

Amino Acid Sequence, Cell Membrane chemistry, Chemical Phenomena, Chemistry, Physical, Cysteine chemistry, Escherichia coli drug effects, Ethylmaleimide metabolism, Models, Molecular, Molecular Sequence Data, Mutagenesis, Site-Directed, Protein Conformation, Sulfhydryl Compounds metabolism, Tetracycline Resistance genetics, Protein Structure, Secondary

Abstract

Each amino acid in putative transmembrane helix VI and its flanking regions, from Ser-156 to Thr-185, of a Cys-free mutant of the Tn10-encoded metal-tetracycline/H(+) antiporter (TetA(B)) was individually replaced by Cys. All of the cysteine-scanning mutants showed a normal level of tetracycline resistance except for the S156C mutant, which showed moderate resistance, indicating that there is no essential residue located in this region. All 20 mutants from S159C to W178C showed no reactivity with N-ethylmaleimide (NEM), whereas the mutants of the flanking regions from S156C to H158C and F179C to T185C were highly or moderately reactive with NEM. These results indicate that like transmembrane helices III and IX, the transmembrane helix VI comprising residues Ser-159-Trp-178 is totally embedded in the hydrophobic environment.

Published

1999

47. Assignment of muscarinic receptor subtypes mediating G-protein modulation of Ca(2+) channels by using knockout mice.

Author

Shapiro MS, Loose MD, Hamilton SE, Nathanson NM, Gomeza J, Wess J, and Hille B

Subjects

Animals, Ethylmaleimide metabolism, Mice, Mice, Inbred C57BL, Mice, Knockout, Models, Biological, Oxotremorine metabolism, Patch-Clamp Techniques, Time Factors, Virulence Factors, Bordetella metabolism, Calcium Channels metabolism, GTP-Binding Proteins metabolism, Receptors, Muscarinic classification

Abstract

There are five known subtypes of muscarinic receptors (M(1)-M(5)). We have used knockout mice lacking the M(1), M(2), or M(4) receptors to determine which subtypes mediate modulation of voltage-gated Ca(2+) channels in mouse sympathetic neurons. Muscarinic agonists modulate N- and L-type Ca(2+) channels in these neurons through two distinct G-protein-mediated mechanisms. One pathway is fast and membrane-delimited and inhibits N- and P/Q-type channels by shifting their activation to more depolarized potentials. The other is slow and voltage-independent and uses a diffusible cytoplasmic messenger to inhibit both Ca(2+) channel types. Using patch-clamp methods on acutely dissociated sympathetic neurons, we isolated each pathway by pharmacological and kinetic means and found that each one is nearly absent in a particular knockout mouse. The fast and voltage-dependent pathway is lacking in the M(2) receptor knockout mice; the slow and voltage-independent pathway is absent from the M(1) receptor knockout mice; and neither pathway is affected in the M(4) receptor knockout mice. The knockout effects are clean and are apparently not accompanied by compensatory changes in other muscarinic receptors.

Published

1999

48. Scanning cysteine accessibility of EmrE, an H+-coupled multidrug transporter from Escherichia coli, reveals a hydrophobic pathway for solutes.

Author

Mordoch SS, Granot D, Lebendiker M, and Schuldiner S

Subjects

Acriflavine pharmacology, Amino Acid Sequence, Escherichia coli, Escherichia coli Proteins, Ethidium pharmacology, Ethylmaleimide metabolism, Molecular Sequence Data, Phenotype, Protein Structure, Secondary, Solutions, ATP Binding Cassette Transporter, Subfamily B, Member 1 metabolism, Antiporters, Bacterial Proteins metabolism, Carrier Proteins metabolism, Cysteine metabolism, Membrane Proteins metabolism

Abstract

EmrE is a 12-kDa Escherichia coli multidrug transporter that confers resistance to a wide variety of toxic reagents by actively removing them in exchange for hydrogen ions. The three native Cys residues in EmrE are inaccessible to N-ethylmaleimide (NEM) and a series of other sulfhydryls. In addition, each of the three residues can be replaced with Ser without significant loss of activity. A protein without all the three Cys residues (Cys-less) has been generated and shown to be functional. Using this Cys-less protein, we have now generated a series of 48 single Cys replacements throughout the protein. The majority of them (43) show transport activity as judged from the ability of the mutant proteins to confer resistance against toxic compounds and from in vitro analysis of their activity in proteoliposomes. Here we describe the use of these mutants to study the accessibility to NEM, a membrane permeant sulfhydryl reagent. The study has been done systematically so that in one transmembrane segment (TMS2) each single residue was replaced. In each of the other three transmembrane segments, at least four residues covering one turn of the helix were replaced. The results show that although the residues in putative hydrophilic loops readily react with NEM, none of the residues in putative transmembrane domains are accessible to the reagent. The results imply very tight packing of the protein without any continuous aqueous domain. Based on the findings described in this work, we conclude that in EmrE the substrates are translocated through a hydrophobic pathway.

Published

1999

49. Identification of the amine-polyamine-choline transporter superfamily 'consensus amphipathic region' as the target for inactivation of the Escherichia coli GABA transporter GabP by thiol modification reagents. Role of Cys-300 in restoring thiol sensitivity to Gabp lacking Cys.

Author

Hu LA and King SC

Subjects

4-Chloromercuribenzenesulfonate metabolism, 4-Chloromercuribenzenesulfonate pharmacology, Amines metabolism, Amino Acid Substitution, Biological Transport drug effects, Cell Membrane Permeability, Choline metabolism, Cysteine genetics, Escherichia coli Proteins, Ethylmaleimide metabolism, Ethylmaleimide pharmacology, GABA Plasma Membrane Transport Proteins, Kinetics, Membrane Proteins antagonists & inhibitors, Membrane Proteins chemistry, Membrane Proteins genetics, Membrane Proteins metabolism, Membrane Transport Modulators, Membrane Transport Proteins chemistry, Membrane Transport Proteins genetics, Mesylates metabolism, Mesylates pharmacology, Models, Biological, Polyamines metabolism, Protein Conformation, Substrate Specificity, Sulfhydryl Reagents chemistry, Sulfhydryl Reagents metabolism, gamma-Aminobutyric Acid metabolism, Consensus Sequence genetics, Cysteine metabolism, Escherichia coli enzymology, Membrane Transport Proteins metabolism, Organic Anion Transporters, Sulfhydryl Compounds metabolism, Sulfhydryl Reagents pharmacology

Abstract

The Escherichia coli gamma-aminobutyric acid transporter GabP (gab permease) contains a functionally significant cysteine residue (Cys-300) within its consensus amphipathic region (CAR), a putative channel-forming structure that extends out of transmembrane helix 8 and into the adjoining cytoplasmic loop 8-9 of transporters from the amine-polyamine-choline (APC) superfamily. Here we show that of the five cysteine residues (positions 158, 251, 291, 300 and 443) in the E. coli GabP, Cys-300 is the one that renders the transport activity sensitive to inhibition by thiol modification reagents: whereas substituting Ala for Cys-300 mimics the inhibitory effect of thiol modification, substituting Ala at position 158, 251, 291 or 443 preserves robust transport activity and confers no resistance to thiol inactivation; and whereas the robustly active Cys-300 single-Cys mutant is fully sensitive to thiol modification, other single-Cys mutants (Cys at 158, 251, 291 or 443) exhibit kinetically compromised transport activities that resist further chemical inactivation by thiol reagents. The present study reveals additionally that Cys-300 exhibits (1) sensitivity to hydrophobic thiol reagents, (2) general resistance to bulky (fluorescein 5-maleimide) and/or charged {2-sulphonatoethyl methanethiosulphonate or [2-(trimethylammonium)ethyl] methanethiosulphonate} thiol reagents and (3) a peculiar sensitivity to p-chloromercuribenzenesulphonate (PCMBS). The accessibility of PCMBS to Cys-300 (located midway through the lipid bilayer) might be related to the structural similarity that it shares with guvacine (1, 2,3,6-tetrahydro-3-pyridinecarboxylic acid), a transported GabP substrate. These structural requirements for thiol sensitivity provide the first chemical evidence consistent with channel-like access to the polar surface of the CAR, a physical configuration that might provide a basis for understanding how this region impacts the function of APC transporters generally [Closs, Lyons, Kelly and Cunningham (1993) J. Biol. Chem. 268, 20796-20800] and the gab permease particularly [Hu and King (1998) Biochem. J. 300, 771-776].

Published

1999

50. Nitric oxide-induced S-glutathionylation and inactivation of glyceraldehyde-3-phosphate dehydrogenase.

Author

Mohr S, Hallak H, de Boitte A, Lapetina EG, and Brüne B

Subjects

Animals, Borates pharmacology, Cattle, Endothelium, Vascular metabolism, Ethylmaleimide metabolism, Glutathione analogs & derivatives, Glutathione pharmacology, Nitroso Compounds pharmacology, S-Nitrosoglutathione, Sulfhydryl Compounds metabolism, Glutathione metabolism, Glyceraldehyde-3-Phosphate Dehydrogenases metabolism, Nitric Oxide pharmacology

Abstract

S-Nitrosylation of protein thiol groups by nitric oxide (NO) is a widely recognized protein modification. In this study we show that nitrosonium tetrafluoroborate (BF4NO), a NO+ donor, modified the thiol groups of glyceraldehyde-3-phosphate dehydrogenase (GAPDH) by S-nitrosylation and caused enzyme inhibition. The resultant protein-S-nitrosothiol was found to be unstable and to decompose spontaneously, thereby restoring enzyme activity. In contrast, the NO-releasing compound S-nitrosoglutathione (GSNO) promoted S-glutathionylation of a thiol group of GAPDH both in vitro and under cellular conditions. The GSH-mixed protein disulfide formed led to a permanent enzyme inhibition, but upon dithiothreitol addition a functional active GAPDH was recovered. This S-glutathionylation is specific for GSNO because GSH itself was unable to produce protein-mixed disulfides. During cellular nitrosative stress, the production of intracellular GSNO might channel signaling responses to form protein-mixed disulfide that can regulate intracellular function.

Published

1999