Your search keyword '"Sauer DB"' showing total 27 results

1. Transport and inhibition of the sphingosine-1-phosphate exporter SPNS2.

Author

Li HZ, Pike ACW, Chang YN, Prakaash D, Gelova Z, Stanka J, Moreau C, Scott HC, Wunder F, Wolf G, Scacioc A, McKinley G, Batoulis H, Mukhopadhyay S, Garofoli A, Pinto-Fernández A, Kessler BM, Burgess-Brown NA, Štefanić S, Wiedmer T, Dürr KL, Puetter V, Ehrmann A, Khalid S, Ingles-Prieto A, Superti-Furga G, and Sauer DB

Subjects

Humans, Animals, Fingolimod Hydrochloride pharmacology, Fingolimod Hydrochloride metabolism, Anion Transport Proteins metabolism, Anion Transport Proteins genetics, Anion Transport Proteins chemistry, Biological Transport, Mice, Mutation, HEK293 Cells, Hearing Loss metabolism, Hearing Loss genetics, Sphingosine metabolism, Sphingosine analogs & derivatives, Lysophospholipids metabolism, Cryoelectron Microscopy, Molecular Dynamics Simulation

Abstract

Sphingosine-1-phosphate (S1P) is a signaling lysolipid critical to heart development, immunity, and hearing. Accordingly, mutations in the S1P transporter SPNS2 are associated with reduced white cell count and hearing defects. SPNS2 also exports the S1P-mimicking FTY720-P (Fingolimod) and thereby is central to the pharmacokinetics of this drug when treating multiple sclerosis. Here, we use a combination of cryo-electron microscopy, immunofluorescence, in vitro binding and in vivo S1P export assays, and molecular dynamics simulations to probe SPNS2's substrate binding and transport. These results reveal the transporter's binding mode to its native substrate S1P, the therapeutic FTY720-P, and the reported SPNS2-targeting inhibitor 33p. Further capturing an inward-facing apo state, our structures illuminate the protein's mechanism for exchange between inward-facing and outward-facing conformations. Finally, using these structural, localization, and S1P transport results, we identify how pathogenic mutations ablate the protein's export activity and thereby lead to hearing loss., Competing Interests: Competing interests: J.S., F.W., H.B., and A.E. are employees of Bayer AG. Y.N.C. and V.P. are employees of Nuvisan ICB GmbH. G.S.F is co-founder and owns shares of Solgate GmbH, and SLC-focused company. The remaining authors declare no competing interests., (© 2025. The Author(s).)

Published

2025

2. Structural basis of the mechanism and inhibition of a human ceramide synthase.

Author

Pascoa TC, Pike ACW, Tautermann CS, Chi G, Traub M, Quigley A, Chalk R, Štefanić S, Thamm S, Pautsch A, Carpenter EP, Schnapp G, and Sauer DB

Abstract

Ceramides are bioactive sphingolipids crucial for regulating cellular metabolism. Ceramides and dihydroceramides are synthesized by six ceramide synthase (CerS) enzymes, each with specificity for different acyl-CoA substrates. Ceramide with a 16-carbon acyl chain (C16 ceramide) has been implicated in obesity, insulin resistance and liver disease and the C16 ceramide-synthesizing CerS6 is regarded as an attractive drug target for obesity-associated disease. Despite their importance, the molecular mechanism underlying ceramide synthesis by CerS enzymes remains poorly understood. Here we report cryo-electron microscopy structures of human CerS6, capturing covalent intermediate and product-bound states. These structures, along with biochemical characterization, reveal that CerS catalysis proceeds through a ping-pong reaction mechanism involving a covalent acyl-enzyme intermediate. Notably, the product-bound structure was obtained upon reaction with the mycotoxin fumonisin B1, yielding insights into its inhibition of CerS. These results provide a framework for understanding CerS function, selectivity and inhibition and open routes for future drug discovery., Competing Interests: Competing interests C.S.T., M.T., S.T., A.P. and G.S. are employees of Boehringer Ingelheim Pharma, GmbH & Co. KG. The other authors declare no competing interests., (© 2024. The Author(s).)

Published

2024

3. Protein Binder Toolbox for Studies of Solute Carrier Transporters.

Author

Gelová Z, Ingles-Prieto A, Bohstedt T, Frommelt F, Chi G, Chang YN, Garcia J, Wolf G, Azzollini L, Tremolada S, Scacioc A, Hansen JS, Serrano I, Droce A, Bernal JC, Burgess-Brown NA, Carpenter EP, Dürr KL, Kristensen P, Geertsma ER, Štefanić S, Scarabottolo L, Wiedmer T, Puetter V, Sauer DB, and Superti-Furga G

Subjects

Humans, Membrane Transport Proteins metabolism, Membrane Transport Proteins genetics, Membrane Transport Proteins chemistry, HEK293 Cells, Solute Carrier Proteins metabolism, Protein Binding

Abstract

Transporters of the solute carrier superfamily (SLCs) are responsible for the transmembrane traffic of the majority of chemical substances in cells and tissues and are therefore of fundamental biological importance. As is often the case with membrane proteins that can be heavily glycosylated, a lack of reliable high-affinity binders hinders their functional analysis. Purifying and reconstituting transmembrane proteins in their lipidic environments remains challenging and standard approaches to generate binders for multi-transmembrane proteins, such as SLCs, channels or G protein-coupled receptors (GPCRs) are lacking. While generating protein binders to 27 SLCs, we produced full length protein or cell lines as input material for binder generation by selected binder generation platforms. As a result, we obtained 525 binders for 22 SLCs. We validated the binders with a cell-based validation workflow using immunofluorescent and immunoprecipitation methods to process all obtained binders. Finally, we demonstrated the potential applications of the binders that passed our validation pipeline in structural, biochemical, and biological applications using the exemplary protein SLC12A6, an ion transporter relevant in human disease. With this work, we were able to generate easily renewable and highly specific binders against SLCs, which will greatly facilitate the study of this neglected protein family. We hope that the process will serve as blueprint for the generation of binders against the entire superfamily of SLC transporters., Competing Interests: Declaration of competing interest The authors declare the following financial interests/personal relationships which may be considered as potential competing interests: “L.S., L.A. and S.T. are employees of Axxam S.p.A. Y.-N.C. and V.P. are employees of Nuvisan GmbH. G.S.-F. is scientific founder and shareholder of Proxygen and Solgate. The rest of authors declare no competing interests”., (Copyright © 2024. Published by Elsevier Ltd.)

Published

2024

4. Pho pictures provide powerful perspectives of phosphate importing proteins.

Author

Speedman D and Sauer DB

Subjects

Cryoelectron Microscopy, Sodium metabolism, Saccharomyces cerevisiae metabolism, Saccharomyces cerevisiae Proteins metabolism, Saccharomyces cerevisiae Proteins chemistry, Phosphates metabolism, Phosphates chemistry

Abstract

In this issue of Structure, Schneider et al. 1 report multiple structures of the low-affinity inorganic-phosphate transporter Pho90 from Saccharomyces cerevisiae. With remarkable resolution of the Divalent Anion Sodium Symporter family member, their cryo-EM studies of this fungal protein reveal new modes of sodium, substrate, and lipid binding., Competing Interests: Declaration of interests The author declares no competing interests., (Copyright © 2024 Elsevier Inc. All rights reserved.)

Published

2024

5. Advancing drug discovery through assay development: a survey of tool compounds within the human solute carrier superfamily.

Author

Digles D, Ingles-Prieto A, Dvorak V, Mocking TAM, Goldmann U, Garofoli A, Homan EJ, Di Silvio A, Azzollini L, Sassone F, Fogazza M, Bärenz F, Pommereau A, Zuschlag Y, Ooms JF, Tranberg-Jensen J, Hansen JS, Stanka J, Sijben HJ, Batoulis H, Bender E, Martini R, IJzerman AP, Sauer DB, Heitman LH, Manolova V, Reinhardt J, Ehrmann A, Leippe P, Ecker GF, Huber KVM, Licher T, Scarabottolo L, Wiedmer T, and Superti-Furga G

Abstract

With over 450 genes, solute carriers (SLCs) constitute the largest transporter superfamily responsible for the uptake and efflux of nutrients, metabolites, and xenobiotics in human cells. SLCs are associated with a wide variety of human diseases, including cancer, diabetes, and metabolic and neurological disorders. They represent an important therapeutic target class that remains only partly exploited as therapeutics that target SLCs are scarce. Additionally, many small molecules reported in the literature to target SLCs are poorly characterized. Both features may be due to the difficulty of developing SLC transport assays that fulfill the quality criteria for high-throughput screening. Here, we report one of the main limitations hampering assay development within the RESOLUTE consortium: the lack of a resource providing high-quality information on SLC tool compounds. To address this, we provide a systematic annotation of tool compounds targeting SLCs. We first provide an overview on RESOLUTE assays. Next, we present a list of SLC-targeting compounds collected from the literature and public databases; we found that most data sources lacked specificity data. Finally, we report on experimental tests of 19 selected compounds against a panel of 13 SLCs from seven different families. Except for a few inhibitors, which were active on unrelated SLCs, the tested inhibitors demonstrated high selectivity for their reported targets. To make this knowledge easily accessible to the scientific community, we created an interactive dashboard displaying the collected data in the RESOLUTE web portal (https://re-solute.eu). We anticipate that our open-access resources on assays and compounds will support the development of future drug discovery campaigns for SLCs., Competing Interests: AS, LA, FS, MF, and LS are employees of Axxam SpA. JS, HB, EB, and AE are employees of Bayer Pharmaceuticals. VM is an employee of CSL Vifor. JR is an employee of Novartis Pharma AG. GS-F is co-founder and own shares of Solgate GmbH, and SLC-focused company. FB, AP, YZ, and TL are employees of Sanofi. The remaining authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2024 Digles, Ingles-Prieto, Dvorak, Mocking, Goldmann, Garofoli, Homan, Di Silvio, Azzollini, Sassone, Fogazza, Bärenz, Pommereau, Zuschlag, Ooms, Tranberg-Jensen, Hansen, Stanka, Sijben, Batoulis, Bender, Martini, IJzerman, Sauer, Heitman, Manolova, Reinhardt, Ehrmann, Leippe, Ecker, Huber, Licher, Scarabottolo, Wiedmer and Superti-Furga.)

Published

2024

6. Structure and function of the SIT1 proline transporter in complex with the COVID-19 receptor ACE2.

Author

Li HZ, Pike ACW, Lotsaris I, Chi G, Hansen JS, Lee SC, Rödström KEJ, Bushell SR, Speedman D, Evans A, Wang D, He D, Shrestha L, Nasrallah C, Burgess-Brown NA, Vandenberg RJ, Dafforn TR, Carpenter EP, and Sauer DB

Subjects

Humans, COVID-19 virology, COVID-19 metabolism, Amino Acid Transport Systems, Neutral metabolism, Amino Acid Transport Systems, Neutral genetics, Amino Acid Transport Systems, Neutral chemistry, Models, Molecular, Angiotensin-Converting Enzyme 2 metabolism, Angiotensin-Converting Enzyme 2 chemistry, Angiotensin-Converting Enzyme 2 genetics, Cryoelectron Microscopy, Proline metabolism, SARS-CoV-2 metabolism, SARS-CoV-2 genetics

Abstract

Proline is widely known as the only proteogenic amino acid with a secondary amine. In addition to its crucial role in protein structure, the secondary amino acid modulates neurotransmission and regulates the kinetics of signaling proteins. To understand the structural basis of proline import, we solved the structure of the proline transporter SIT1 in complex with the COVID-19 viral receptor ACE2 by cryo-electron microscopy. The structure of pipecolate-bound SIT1 reveals the specific sequence requirements for proline transport in the SLC6 family and how this protein excludes amino acids with extended side chains. By comparing apo and substrate-bound SIT1 states, we also identify the structural changes that link substrate release and opening of the cytoplasmic gate and provide an explanation for how a missense mutation in the transporter causes iminoglycinuria., (© 2024. The Author(s).)

Published

2024

7. Still in Search for an EAAT Activator: GT949 Does Not Activate EAAT2, nor EAAT3 in Impedance and Radioligand Uptake Assays.

Author

van Veggel L, Mocking TAM, Sijben HJ, Liu R, Gorostiola González M, Dilweg MA, Royakkers J, Li A, Kumar V, Dong YY, Bullock A, Sauer DB, Diliën H, van Westen GJP, Schreiber R, Heitman LH, and Vanmierlo T

Subjects

Electric Impedance, Biological Transport, Excitatory Amino Acid Transporter 3 metabolism, Excitatory Amino Acid Transporter 2 metabolism, Glutamic Acid metabolism

Abstract

Excitatory amino acid transporters (EAATs) are important regulators of amino acid transport and in particular glutamate. Recently, more interest has arisen in these transporters in the context of neurodegenerative diseases. This calls for ways to modulate these targets to drive glutamate transport, EAAT2 and EAAT3 in particular. Several inhibitors (competitive and noncompetitive) exist to block glutamate transport; however, activators remain scarce. Recently, GT949 was proposed as a selective activator of EAAT2, as tested in a radioligand uptake assay. In the presented research, we aimed to validate the use of GT949 to activate EAAT2-driven glutamate transport by applying an innovative, impedance-based, whole-cell assay (xCELLigence). A broad range of GT949 concentrations in a variety of cellular environments were tested in this assay. As expected, no activation of EAAT3 could be detected. Yet, surprisingly, no biological activation of GT949 on EAAT2 could be observed in this assay either. To validate whether the impedance-based assay was not suited to pick up increased glutamate uptake or if the compound might not induce activation in this setup, we performed radioligand uptake assays. Two setups were utilized; a novel method compared to previously published research, and in a reproducible fashion copying the methods used in the existing literature. Nonetheless, activation of neither EAAT2 nor EAAT3 could be observed in these assays. Furthermore, no evidence of GT949 binding or stabilization of purified EAAT2 could be observed in a thermal shift assay. To conclude, based on experimental evidence in the present study GT949 requires specific assay conditions, which are difficult to reproduce, and the compound cannot simply be classified as an activator of EAAT2 based on the presented evidence. Hence, further research is required to develop the tools needed to identify new EAAT modulators and use their potential as a therapeutic target.

Published

2024

8. The binding and mechanism of a positive allosteric modulator of Kv3 channels.

Author

Liang Q, Chi G, Cirqueira L, Zhi L, Marasco A, Pilati N, Gunthorpe MJ, Alvaro G, Large CH, Sauer DB, Treptow W, and Covarrubias M

Subjects

Binding Sites, Shaw Potassium Channels metabolism

Abstract

Small-molecule modulators of diverse voltage-gated K + (Kv) channels may help treat a wide range of neurological disorders. However, developing effective modulators requires understanding of their mechanism of action. We apply an orthogonal approach to elucidate the mechanism of action of an imidazolidinedione derivative (AUT5), a highly selective positive allosteric modulator of Kv3.1 and Kv3.2 channels. AUT5 modulation involves positive cooperativity and preferential stabilization of the open state. The cryo-EM structure of the Kv3.1/AUT5 complex at a resolution of 2.5 Å reveals four equivalent AUT5 binding sites at the extracellular inter-subunit interface between the voltage-sensing and pore domains of the channel's tetrameric assembly. Furthermore, we show that the unique extracellular turret regions of Kv3.1 and Kv3.2 essentially govern the selective positive modulation by AUT5. High-resolution apo and bound structures of Kv3.1 demonstrate how AUT5 binding promotes turret rearrangements and interactions with the voltage-sensing domain to favor the open conformation., (© 2024. The Author(s).)

Published

2024

9. High-Throughput Expression and Purification of Human Solute Carriers for Structural and Biochemical Studies.

Author

Raturi S, Li H, Chang YN, Scacioc A, Bohstedt T, Fernandez-Cid A, Evans A, Abrusci P, Balakrishnan A, Pascoa TC, He D, Chi G, Kaur Singh N, Ye M, Li A, Shrestha L, Wang D, Williams EP, Burgess-Brown NA, Dürr KL, Puetter V, Ingles-Prieto A, and Sauer DB

Subjects

Humans, Drug Discovery methods, High-Throughput Screening Assays, Membrane Proteins metabolism, Pharmaceutical Preparations, Membrane Transport Proteins genetics, Membrane Transport Proteins metabolism, Solute Carrier Proteins chemistry, Solute Carrier Proteins metabolism

Abstract

Solute carriers (SLCs) are membrane transporters that import and export a range of endogenous and exogenous substrates, including ions, nutrients, metabolites, neurotransmitters, and pharmaceuticals. Despite having emerged as attractive therapeutic targets and markers of disease, this group of proteins is still relatively underdrugged by current pharmaceuticals. Drug discovery projects for these transporters are impeded by limited structural, functional, and physiological knowledge, ultimately due to the difficulties in the expression and purification of this class of membrane-embedded proteins. Here, we demonstrate methods to obtain high-purity, milligram quantities of human SLC transporter proteins using codon-optimized gene sequences. In conjunction with a systematic exploration of construct design and high-throughput expression, these protocols ensure the preservation of the structural integrity and biochemical activity of the target proteins. We also highlight critical steps in the eukaryotic cell expression, affinity purification, and size-exclusion chromatography of these proteins. Ultimately, this workflow yields pure, functionally active, and stable protein preparations suitable for high-resolution structure determination, transport studies, small-molecule engagement assays, and high-throughput in vitro screening.

Published

2023

10. The solute carrier SPNS2 recruits PI(4,5)P 2 to synergistically regulate transport of sphingosine-1-phosphate.

Author

Tang H, Li H, Prakaash D, Pedebos C, Qiu X, Sauer DB, Khalid S, Duerr K, and Robinson CV

Subjects

Humans, Anion Transport Proteins genetics, Anion Transport Proteins metabolism, Lysophospholipids, Sphingosine

Abstract

Solute carrier spinster homolog 2 (SPNS2), one of only four known major facilitator superfamily (MFS) lysolipid transporters in humans, exports sphingosine-1-phosphate (S1P) across cell membranes. Here, we explore the synergistic effects of lipid binding and conformational dynamics on SPNS2's transport mechanism. Using mass spectrometry, we discovered that SPNS2 interacts preferentially with PI(4,5)P 2 . Together with functional studies and molecular dynamics (MD) simulations, we identified potential PI(4,5)P 2 binding sites. Mutagenesis of proposed lipid binding sites and inhibition of PI(4,5)P 2 synthesis reduce S1P transport, whereas the absence of the N terminus renders the transporter essentially inactive. Probing the conformational dynamics of SPNS2, we show how synergistic binding of PI(4,5)P 2 and S1P facilitates transport, increases dynamics of the extracellular gate, and stabilizes the intracellular gate. Given that SPNS2 transports a key signaling lipid, our results have implications for therapeutic targeting and also illustrate a regulatory mechanism for MFS transporters., Competing Interests: Declaration of interests C.V.R. is a co-founder and consultant and K.D. is an employee of OMass Therapeutics., (Copyright © 2023 The Author(s). Published by Elsevier Inc. All rights reserved.)

Published

2023

11. Structural basis for inhibition of the drug efflux pump NorA from Staphylococcus aureus.

Author

Brawley DN, Sauer DB, Li J, Zheng X, Koide A, Jedhe GS, Suwatthee T, Song J, Liu Z, Arora PS, Koide S, Torres VJ, Wang DN, and Traaseth NJ

Subjects

Anti-Bacterial Agents chemistry, Bacterial Proteins metabolism, Cryoelectron Microscopy, Humans, Microbial Sensitivity Tests, Multidrug Resistance-Associated Proteins chemistry, Multidrug Resistance-Associated Proteins metabolism, Multidrug Resistance-Associated Proteins pharmacology, Staphylococcus aureus metabolism, Methicillin-Resistant Staphylococcus aureus, Staphylococcal Infections

Abstract

Membrane protein efflux pumps confer antibiotic resistance by extruding structurally distinct compounds and lowering their intracellular concentration. Yet, there are no clinically approved drugs to inhibit efflux pumps, which would potentiate the efficacy of existing antibiotics rendered ineffective by drug efflux. Here we identified synthetic antigen-binding fragments (Fabs) that inhibit the quinolone transporter NorA from methicillin-resistant Staphylococcus aureus (MRSA). Structures of two NorA-Fab complexes determined using cryo-electron microscopy reveal a Fab loop deeply inserted in the substrate-binding pocket of NorA. An arginine residue on this loop interacts with two neighboring aspartate and glutamate residues essential for NorA-mediated antibiotic resistance in MRSA. Peptide mimics of the Fab loop inhibit NorA with submicromolar potency and ablate MRSA growth in combination with the antibiotic norfloxacin. These findings establish a class of peptide inhibitors that block antibiotic efflux in MRSA by targeting indispensable residues in NorA without the need for membrane permeability., (© 2022. The Author(s), under exclusive licence to Springer Nature America, Inc.)

Published

2022

12. Structural basis of ion - substrate coupling in the Na + -dependent dicarboxylate transporter VcINDY.

Author

Sauer DB, Marden JJ, Sudar JC, Song J, Mulligan C, and Wang DN

Subjects

Binding Sites, Sodium metabolism, Succinic Acid metabolism, Dicarboxylic Acid Transporters chemistry, Dicarboxylic Acid Transporters genetics, Dicarboxylic Acid Transporters metabolism, Vibrio cholerae metabolism

Abstract

The Na + -dependent dicarboxylate transporter from Vibrio cholerae (VcINDY) is a prototype for the divalent anion sodium symporter (DASS) family. While the utilization of an electrochemical Na + gradient to power substrate transport is well established for VcINDY, the structural basis of this coupling between sodium and substrate binding is not currently understood. Here, using a combination of cryo-EM structure determination, succinate binding and site-directed cysteine alkylation assays, we demonstrate that the VcINDY protein couples sodium- and substrate-binding via a previously unseen cooperative mechanism by conformational selection. In the absence of sodium, substrate binding is abolished, with the succinate binding regions exhibiting increased flexibility, including HP in b, TM10b and the substrate clamshell motifs. Upon sodium binding, these regions become structurally ordered and create a proper binding site for the substrate. Taken together, these results provide strong evidence that VcINDY's conformational selection mechanism is a result of the sodium-dependent formation of the substrate binding site., (© 2022. The Author(s).)

Published

2022

13. The ups and downs of elevator-type di-/tricarboxylate membrane transporters.

Author

Sauer DB, Wang B, Sudar JC, Song J, Marden J, Rice WJ, and Wang DN

Subjects

Anions metabolism, Dicarboxylic Acid Transporters genetics, Dicarboxylic Acid Transporters metabolism, Humans, Sodium metabolism, Membrane Transport Proteins genetics, Symporters metabolism

Abstract

The divalent anion sodium symporter (DASS) family contains both sodium-driven anion cotransporters and anion/anion exchangers. The family belongs to a broader ion transporter superfamily (ITS), which comprises 24 families of transporters, including those of AbgT antibiotic efflux transporters. The human proteins in the DASS family play major physiological roles and are drug targets. We recently determined multiple structures of the human sodium-dependent citrate transporter (NaCT) and the succinate/dicarboxylate transporter from Lactobacillus acidophilus (LaINDY). Structures of both proteins show high degrees of structural similarity to the previously determined VcINDY fold. Conservation between these DASS protein structures and those from the AbgT family indicates that the VcINDY fold represents the overall protein structure for the entire ITS. The new structures of NaCT and LaINDY are captured in the inward- or outward-facing conformations, respectively. The domain arrangements in these structures agree with a rigid body elevator-type transport mechanism for substrate translocation across the membrane. Two separate NaCT structures in complex with a substrate or an inhibitor allowed us to explain the inhibition mechanism and propose a detailed classification scheme for grouping disease-causing mutations in the human protein. Structural understanding of multiple kinetic states of DASS proteins is a first step toward the detailed characterization of their entire transport cycle., (© 2021 Federation of European Biochemical Societies.)

Published

2022

14. Structure and inhibition mechanism of the human citrate transporter NaCT.

Author

Sauer DB, Song J, Wang B, Hilton JK, Karpowich NK, Mindell JA, Rice WJ, and Wang DN

Subjects

Binding Sites, Brain metabolism, Carrier Proteins genetics, Carrier Proteins ultrastructure, Citric Acid chemistry, Dicarboxylic Acid Transporters chemistry, Dicarboxylic Acid Transporters metabolism, Epilepsy genetics, Epilepsy metabolism, Humans, Malates chemistry, Models, Molecular, Mutation, Phenylbutyrates chemistry, Protein Multimerization, Sodium metabolism, Substrate Specificity drug effects, Substrate Specificity genetics, Symporters genetics, Symporters ultrastructure, Carrier Proteins antagonists & inhibitors, Carrier Proteins chemistry, Citric Acid metabolism, Cryoelectron Microscopy, Malates pharmacology, Phenylbutyrates pharmacology, Symporters antagonists & inhibitors, Symporters chemistry

Abstract

Citrate is best known as an intermediate in the tricarboxylic acid cycle of the cell. In addition to this essential role in energy metabolism, the tricarboxylate anion also acts as both a precursor and a regulator of fatty acid synthesis 1-3 . Thus, the rate of fatty acid synthesis correlates directly with the cytosolic concentration of citrate 4,5 . Liver cells import citrate through the sodium-dependent citrate transporter NaCT (encoded by SLC13A5) and, as a consequence, this protein is a potential target for anti-obesity drugs. Here, to understand the structural basis of its inhibition mechanism, we determined cryo-electron microscopy structures of human NaCT in complexes with citrate or a small-molecule inhibitor. These structures reveal how the inhibitor-which binds to the same site as citrate-arrests the transport cycle of NaCT. The NaCT-inhibitor structure also explains why the compound selectively inhibits NaCT over two homologous human dicarboxylate transporters, and suggests ways to further improve the affinity and selectivity. Finally, the NaCT structures provide a framework for understanding how various mutations abolish the transport activity of NaCT in the brain and thereby cause epilepsy associated with mutations in SLC13A5 in newborns (which is known as SLC13A5-epilepsy) 6-8 .

Published

2021

15. Structural basis for the reaction cycle of DASS dicarboxylate transporters.

Author

Sauer DB, Trebesch N, Marden JJ, Cocco N, Song J, Koide A, Koide S, Tajkhorshid E, and Wang DN

Subjects

Cryoelectron Microscopy, Crystallography, X-Ray, Lactobacillus acidophilus metabolism, Molecular Dynamics Simulation, Dicarboxylic Acid Transporters metabolism, Escherichia coli metabolism, Escherichia coli Proteins metabolism

Abstract

Citrate, α-ketoglutarate and succinate are TCA cycle intermediates that also play essential roles in metabolic signaling and cellular regulation. These di- and tricarboxylates are imported into the cell by the divalent anion sodium symporter (DASS) family of plasma membrane transporters, which contains both cotransporters and exchangers. While DASS proteins transport substrates via an elevator mechanism, to date structures are only available for a single DASS cotransporter protein in a substrate-bound, inward-facing state. We report multiple cryo-EM and X-ray structures in four different states, including three hitherto unseen states, along with molecular dynamics simulations, of both a cotransporter and an exchanger. Comparison of these outward- and inward-facing structures reveal how the transport domain translates and rotates within the framework of the scaffold domain through the transport cycle. Additionally, we propose that DASS transporters ensure substrate coupling by a charge-compensation mechanism, and by structural changes upon substrate release., Competing Interests: DS, NT, JM, NC, JS, AK, SK, ET, DW No competing interests declared, (© 2020, Sauer et al.)

Published

2020

16. Predicting the optimal growth temperatures of prokaryotes using only genome derived features.

Author

Sauer DB and Wang DN

Subjects

Genomics, High-Throughput Nucleotide Sequencing, Sequence Analysis, DNA, Software, Temperature

Abstract

Motivation: Optimal growth temperature is a fundamental characteristic of all living organisms. Knowledge of this temperature is central to the study of a prokaryote, the thermal stability and temperature dependent activity of its genes, and the bioprospecting of its genome for thermally adapted proteins. While high throughput sequencing methods have dramatically increased the availability of genomic information, the growth temperatures of the source organisms are often unknown. This limits the study and technological application of these species and their genomes. Here, we present a novel method for the prediction of growth temperatures of prokaryotes using only genomic sequences., Results: By applying the reverse ecology principle that an organism's genome includes identifiable adaptations to its native environment, we can predict a species' optimal growth temperature with an accuracy of 5.17°C root-mean-square error and a coefficient of determination of 0.835. The accuracy can be further improved for specific taxonomic clades or by excluding psychrophiles. This method provides a valuable tool for the rapid calculation of organism growth temperature when only the genome sequence is known., Availability and Implementation: Source code, genomes analyzed and features calculated are available at: https://github.com/DavidBSauer/OGT_prediction., Supplementary Information: Supplementary data are available at Bioinformatics online., (© The Author(s) 2019. Published by Oxford University Press. All rights reserved. For permissions, please e-mail: journals.permissions@oup.com.)

Published

2019

17. Rapid Bioinformatic Identification of Thermostabilizing Mutations.

Author

Sauer DB, Karpowich NK, Song JM, and Wang DN

Subjects

Amino Acids chemistry, Amino Acids genetics, Anti-Bacterial Agents pharmacology, Antiporters chemistry, Antiporters genetics, Bacillus subtilis, Bacterial Proteins chemistry, Bacterial Proteins genetics, Escherichia coli, Green Fluorescent Proteins genetics, Green Fluorescent Proteins metabolism, Tetracycline pharmacology, Transfection, Computational Biology methods, Mutation, Protein Stability, Temperature

Abstract

Ex vivo stability is a valuable protein characteristic but is laborious to improve experimentally. In addition to biopharmaceutical and industrial applications, stable protein is important for biochemical and structural studies. Taking advantage of the large number of available genomic sequences and growth temperature data, we present two bioinformatic methods to identify a limited set of amino acids or positions that likely underlie thermostability. Because these methods allow thousands of homologs to be examined in silico, they have the advantage of providing both speed and statistical power. Using these methods, we introduced, via mutation, amino acids from thermoadapted homologs into an exemplar mesophilic membrane protein, and demonstrated significantly increased thermostability while preserving protein activity., (Copyright © 2015 Biophysical Society. Published by Elsevier Inc. All rights reserved.)

Published

2015

18. The conserved potassium channel filter can have distinct ion binding profiles: structural analysis of rubidium, cesium, and barium binding in NaK2K.

Author

Lam YL, Zeng W, Sauer DB, and Jiang Y

Subjects

Barium pharmacology, Cesium pharmacology, Humans, Models, Molecular, Patch-Clamp Techniques, Potassium metabolism, Potassium Channel Blockers pharmacology, Potassium Channels drug effects, Protein Binding, Protein Structure, Tertiary, Recombinant Proteins metabolism, Rubidium pharmacology, Barium metabolism, Cesium metabolism, Ions metabolism, Potassium Channels metabolism, Rubidium metabolism

Abstract

Potassium channels are highly selective for K(+) over the smaller Na(+). Intriguingly, they are permeable to larger monovalent cations such as Rb(+) and Cs(+) but are specifically blocked by the similarly sized Ba(2+). In this study, we used structural analysis to determine the binding profiles for these permeant and blocking ions in the selectivity filter of the potassium-selective NaK channel mutant NaK2K and also performed permeation experiments using single-channel recordings. Our data revealed that some ion binding properties of NaK2K are distinct from those of the canonical K(+) channels KcsA and MthK. Rb(+) bound at sites 1, 3, and 4 in NaK2K, as it does in KcsA. Cs(+), however, bound predominantly at sites 1 and 3 in NaK2K, whereas it binds at sites 1, 3, and 4 in KcsA. Moreover, Ba(2+) binding in NaK2K was distinct from that which has been observed in KcsA and MthK, even though all of these channels show similar Ba(2+) block. In the presence of K(+), Ba(2+) bound to the NaK2K channel at site 3 in conjunction with a K(+) at site 1; this led to a prolonged block of the channel (the external K(+)-dependent Ba(2+) lock-in state). In the absence of K(+), however, Ba(2+) acts as a permeating blocker. We found that, under these conditions, Ba(2+) bound at sites 1 or 0 as well as site 3, allowing it to enter the filter from the intracellular side and exit from the extracellular side. The difference in the Ba(2+) binding profile in the presence and absence of K(+) thus provides a structural explanation for the short and prolonged Ba(2+) block observed in NaK2K., (© 2014 Lam et al.)

Published

2014

19. Sodium and potassium competition in potassium-selective and non-selective channels.

Author

Sauer DB, Zeng W, Canty J, Lam Y, and Jiang Y

Subjects

Bacillus cereus metabolism, Bacillus subtilis metabolism, Bacterial Proteins metabolism, Binding Sites, Binding, Competitive, Crystallography, X-Ray, Electrophysiology, Escherichia coli metabolism, Liposomes metabolism, Mutation, Protein Conformation, Ion Channel Gating, Potassium metabolism, Potassium Channels metabolism, Sodium metabolism

Abstract

Potassium channels selectively conduct K(+), primarily to the exclusion of Na(+), despite the fact that both ions can bind within the selectivity filter. Here we perform crystallographic titration and single-channel electrophysiology to examine the competition of Na(+) and K(+) binding within the filter of two NaK channel mutants; one is the potassium-selective NaK2K mutant and the other is the non-selective NaK2CNG, a CNG channel pore mimic. With high-resolution structures of these engineered NaK channel constructs, we explicitly describe the changes in K(+) occupancy within the filter upon Na(+) competition by anomalous diffraction. Our results demonstrate that the non-selective NaK2CNG still retains a K(+)-selective site at equilibrium, whereas the NaK2K channel filter maintains two high-affinity K(+) sites. A double-barrier mechanism is proposed to explain K(+) channel selectivity at low K(+) concentrations.

Published

2013

20. Distinct gating mechanisms revealed by the structures of a multi-ligand gated K(+) channel.

Author

Kong C, Zeng W, Ye S, Chen L, Sauer DB, Lam Y, Derebe MG, and Jiang Y

Subjects

Adenosine Diphosphate, Allosteric Regulation, Amino Acid Sequence, Bacterial Proteins genetics, Bacterial Proteins metabolism, Calcium metabolism, Crystallography, X-Ray, Escherichia coli genetics, Escherichia coli metabolism, Gene Expression, Geobacter metabolism, Ion Channel Gating, Ligand-Gated Ion Channels genetics, Ligand-Gated Ion Channels metabolism, Ligands, Models, Molecular, Molecular Sequence Data, NAD chemistry, NAD metabolism, Potassium Channels genetics, Potassium Channels metabolism, Protein Structure, Secondary, Protein Structure, Tertiary, Recombinant Proteins chemistry, Recombinant Proteins genetics, Recombinant Proteins metabolism, Sequence Alignment, Bacterial Proteins chemistry, Calcium chemistry, Geobacter chemistry, Ligand-Gated Ion Channels chemistry, Potassium Channels chemistry

Abstract

The gating ring-forming RCK domain regulates channel gating in response to various cellular chemical stimuli in eukaryotic Slo channel families and the majority of ligand-gated prokaryotic K(+) channels and transporters. Here we present structural and functional studies of a dual RCK-containing, multi-ligand gated K(+) channel from Geobacter sulfurreducens, named GsuK. We demonstrate that ADP and NAD(+) activate the GsuK channel, whereas Ca(2+) serves as an allosteric inhibitor. Multiple crystal structures elucidate the structural basis of multi-ligand gating in GsuK, and also reveal a unique ion conduction pore with segmented inner helices. Structural comparison leads us to propose a novel pore opening mechanics that is distinct from other K(+) channels.DOI:http://dx.doi.org/10.7554/eLife.00184.001.

Published

2012

21. Structural insight into the ion-exchange mechanism of the sodium/calcium exchanger.

Author

Liao J, Li H, Zeng W, Sauer DB, Belmares R, and Jiang Y

Subjects

Amino Acid Sequence, Archaeal Proteins metabolism, Binding Sites, Crystallization, Crystallography, X-Ray, Ion Transport, Ligands, Models, Molecular, Molecular Sequence Data, Protein Conformation, Protein Structure, Secondary, Archaeal Proteins chemistry, Calcium metabolism, Methanococcales chemistry, Methanococcales metabolism, Sodium metabolism, Sodium-Calcium Exchanger chemistry, Sodium-Calcium Exchanger metabolism

Abstract

Sodium/calcium (Na(+)/Ca(2+)) exchangers (NCX) are membrane transporters that play an essential role in maintaining the homeostasis of cytosolic Ca(2+) for cell signaling. We demonstrated the Na(+)/Ca(2+)-exchange function of an NCX from Methanococcus jannaschii (NCX_Mj) and report its 1.9 angstrom crystal structure in an outward-facing conformation. Containing 10 transmembrane helices, the two halves of NCX_Mj share a similar structure with opposite orientation. Four ion-binding sites cluster at the center of the protein: one specific for Ca(2+) and three that likely bind Na(+). Two passageways allow for Na(+) and Ca(2+) access to the central ion-binding sites from the extracellular side. Based on the symmetry of NCX_Mj and its ability to catalyze bidirectional ion-exchange reactions, we propose a structure model for the inward-facing NCX_Mj.

Published

2012

22. Protein interactions central to stabilizing the K+ channel selectivity filter in a four-sited configuration for selective K+ permeation.

Author

Sauer DB, Zeng W, Raghunathan S, and Jiang Y

Subjects

Amino Acid Motifs, Crystallography, Electrophysiology, Sodium-Potassium-Exchanging ATPase genetics, Models, Molecular, Potassium chemistry, Protein Conformation, Sodium-Potassium-Exchanging ATPase metabolism

Abstract

The structural and functional conversion of the nonselective NaK channel to a K(+) selective channel (NaK2K) allows us to identify two key residues, Tyr and Asp in the filter sequence of TVGYGD, that participate in interactions central to stabilizing the K(+) channel selectivity filter. By using protein crystallography and channel electrophysiology, we demonstrate that the K(+) channel filter exists as an energetically strained structure and requires these key protein interactions working in concert to hold the filter in the precisely defined four-sited configuration that is essential for selective K(+) permeation. Disruption of either interaction, as tested on both the NaK2K and eukaryotic K(v)1.6 channels, can reduce or completely abolish K(+) selectivity and in some cases may also lead to channel inactivation due to conformational changes at the filter. Additionally, on the scaffold of NaK we recapitulate the protein interactions found in the filter of the Kir channel family, which uses a distinct interaction network to achieve similar stabilization of the filter.

Published

2011

23. Tuning the ion selectivity of tetrameric cation channels by changing the number of ion binding sites.

Author

Derebe MG, Sauer DB, Zeng W, Alam A, Shi N, and Jiang Y

Subjects

Bacillus subtilis metabolism, Binding Sites, Carbon chemistry, Crystallography, X-Ray methods, Electrophysiology methods, Ligands, Mutation, Oxygen chemistry, Potassium chemistry, Potassium Channels chemistry, Protein Binding, Protein Conformation, Sodium chemistry, Ions chemistry

Abstract

Selective ion conduction across ion channel pores is central to cellular physiology. To understand the underlying principles of ion selectivity in tetrameric cation channels, we engineered a set of cation channel pores based on the nonselective NaK channel and determined their structures to high resolution. These structures showcase an ensemble of selectivity filters with a various number of contiguous ion binding sites ranging from 2 to 4, with each individual site maintaining a geometry and ligand environment virtually identical to that of equivalent sites in K(+) channel selectivity filters. Combined with single channel electrophysiology, we show that only the channel with four ion binding sites is K(+) selective, whereas those with two or three are nonselective and permeate Na(+) and K(+) equally well. These observations strongly suggest that the number of contiguous ion binding sites in a single file is the key determinant of the channel's selectivity properties and the presence of four sites in K(+) channels is essential for highly selective and efficient permeation of K(+) ions.

Published

2011

24. Metabolites of Alternaria in grain sorghum. Compounds which could be mistaken for zearalenone and aflatoxin.

Author

Seitz LM, Sauer DB, Monr HE, Burroughs R, and Paukstelis JV

Subjects

Chromatography, Thin Layer, Spectrometry, Fluorescence, Zearalenone, Aflatoxins, Alternaria metabolism, Edible Grain, Mitosporic Fungi metabolism

Published

1975

25. Toxicity of Alternaria metabolites found in weathered sorghum grain at harvest.

Author

Sauer DB, Seitz LM, Burroughs R, Mohr HE, West JL, Milleret RJ, and Anthony HD

Subjects

Animal Feed, Animals, Chickens, Edible Grain, Rats, Time Factors, Alternaria metabolism, Mitosporic Fungi metabolism, Mycotoxins toxicity

Published

1978

26. Effect of substrate on metabolite production of Alternaria alternata.

Author

Burroughs R, Seitz LM, Sauer DB, and Mohr HE

Subjects

Culture Media, Oryza metabolism, Triticum metabolism, Zea mays metabolism, Alternaria metabolism, Biphenyl Compounds metabolism, Edible Grain metabolism, Food Microbiology, Mitosporic Fungi metabolism

Abstract

Alternariol and alternariol monomethyl ether are commonly associated with weathered grain sorghum. Production of these metabolites and altenuene by isolates of Alternaria alternata was evaluated on various sterile grain substrates. At 35% moisture content and 25 C, metabolite yields were highest on rice, intermediate on sorghums, and lowest on wheat and yellow corn. Fourteen-to 21-day cultures on milled rice were best in terms of ease of metabolite recovery, even though yields were higher on 28-day cultures of rough and brown rice. Metabolite production was reduced when rice was supplemented with yeast extract or yeast extract plus Czapek-Dox broth.

Published

1976

27. Effects of fungal deterioration on grain: nutritional value, toxicity, germination.

Author

Sauer DB

Subjects

Fungi growth & development, Humidity, Temperature, Edible Grain microbiology, Food Microbiology, Food Preservation, Fungi metabolism, Nutritive Value

Abstract

Moulds or fungi that grow in grains and seeds during storage and transport cause germination decrease, visible mouldiness, discoloration, musty or sour odours, caking, chemical and nutritional changes, reduction in processing quality, and form of mycotoxins. These deteriorative changes affect the grade and price of grain and contribute to customer dissatisfaction when the grain is marketed. The respiration of grain and fungi results in a loss in dry matter as well as the production of heat and moisture which contribute to further spoilage. Net changes in nutritional value and the risk of mycotoxin contamination are difficult to predict because they depend on a complex interaction of factors such as temperature, moisture, storage time, fungal species composition, kind of grain, and previous storage history. Moisture is the most important variable determining the rate of deterioration caused by fungi, with temperature being the second major factor. Problems with deterioration of grain in export shipments are not a recent development. They are related primarily to grain moisture at loading, and also to the extent of previous mould invasion.

Published

1988