Your search keyword '"Savvas, N."' showing total 28 results

1. Structures of complete extracellular receptor assemblies mediated by IL-12 and IL-23

Author

Bloch, Yehudi, Felix, Jan, Merceron, Romain, Provost, Mathias, Symakani, Royan Alipour, De Backer, Robin, Lambert, Elisabeth, Mehdipour, Ahmad R., and Savvides, Savvas N.

Abstract

Cell-surface receptor complexes mediated by pro-inflammatory interleukin (IL)-12 and IL-23, both validated therapeutic targets, are incompletely understood due to the lack of structural insights into their complete extracellular assemblies. Furthermore, there is a paucity of structural details describing the IL-12–receptor interaction interfaces, in contrast to IL-23–receptor complexes. Here we report structures of fully assembled mouse IL-12/human IL-23–receptor complexes comprising the complete extracellular segments of the cognate receptors determined by electron cryo-microscopy. The structures reveal key commonalities but also surprisingly diverse features. Most notably, whereas IL-12 and IL-23 both utilize a conspicuously presented aromatic residue on their α-subunit as a hotspot to interact with the N-terminal Ig domain of their high-affinity receptors, only IL-12 juxtaposes receptor domains proximal to the cell membrane. Collectively, our findings will help to complete our understanding of cytokine-mediated assemblies of tall cytokine receptors and will enable a cytokine-specific interrogation of IL-12/IL-23 signaling in physiology and disease.

Published

2024

2. Structural basis of cytokine-mediated activation of ALK family receptors

Author

De Munck, Steven, Provost, Mathias, Kurikawa, Michiko, Omori, Ikuko, Mukohyama, Junko, Felix, Jan, Bloch, Yehudi, Abdel-Wahab, Omar, Bazan, J. Fernando, Yoshimi, Akihide, and Savvides, Savvas N.

Abstract

Anaplastic lymphoma kinase (ALK)1and the related leukocyte tyrosine kinase (LTK)2are recently deorphanized receptor tyrosine kinases3. Together with their activating cytokines, ALKAL1 and ALKAL24–6(also called FAM150A and FAM150B or AUGβ and AUGα, respectively), they are involved in neural development7, cancer7–9and autoimmune diseases10. Furthermore, mammalian ALK recently emerged as a key regulator of energy expenditure and weight gain11, consistent with a metabolic role for DrosophilaALK12. Despite such functional pleiotropy and growing therapeutic relevance13,14, structural insights into ALK and LTK and their complexes with cognate cytokines have remained scarce. Here we show that the cytokine-binding segments of human ALK and LTK comprise a novel architectural chimera of a permuted TNF-like module that braces a glycine-rich subdomain featuring a hexagonal lattice of long polyglycine type II helices. The cognate cytokines ALKAL1 and ALKAL2 are monomeric three-helix bundles, yet their binding to ALK and LTK elicits similar dimeric assemblies with two-fold symmetry, that tent a single cytokine molecule proximal to the cell membrane. We show that the membrane-proximal EGF-like domain dictates the apparent cytokine preference of ALK. Assisted by these diverse structure–function findings, we propose a structural and mechanistic blueprint for complexes of ALK family receptors, and thereby extend the repertoire of ligand-mediated dimerization mechanisms adopted by receptor tyrosine kinases.

Published

2024

3. Pore-forming proteins as drivers of membrane permeabilization in cell death pathways

Author

Vandenabeele, Peter, Bultynck, Geert, and Savvides, Savvas N.

Abstract

Regulated cell death (RCD) relies on activation and recruitment of pore-forming proteins (PFPs) that function as executioners of specific cell death pathways: apoptosis regulator BAX (BAX), BCL-2 homologous antagonist/killer (BAK) and BCL-2-related ovarian killer protein (BOK) for apoptosis, gasdermins (GSDMs) for pyroptosis and mixed lineage kinase domain-like protein (MLKL) for necroptosis. Inactive precursors of PFPs are converted into pore-forming entities through activation, membrane recruitment, membrane insertion and oligomerization. These mechanisms involve protein–protein and protein–lipid interactions, proteolytic processing and phosphorylation. In this Review, we discuss the structural rearrangements incurred by RCD-related PFPs and describe the mechanisms that manifest conversion from autoinhibited to membrane-embedded molecular states. We further discuss the formation and maturation of membrane pores formed by BAX/BAK/BOK, GSDMs and MLKL, leading to diverse pore architectures. Lastly, we highlight commonalities and differences of PFP mechanisms involving BAX/BAK/BOK, GSDMs and MLKL and conclude with a discussion on how, in a population of challenged cells, the coexistence of cell death modalities may have profound physiological and pathophysiological implications.

Published

2023

4. Unexpected complexity of the ammonia monooxygenase in archaea

Author

Hodgskiss, Logan H, Melcher, Michael, Kerou, Melina, Chen, Weiqiang, Ponce-Toledo, Rafael I, Savvides, Savvas N, Wienkoop, Stefanie, Hartl, Markus, and Schleper, Christa

Abstract

Ammonia oxidation, as the first step of nitrification, constitutes a critical process in the global nitrogen cycle. However, fundamental knowledge of its key enzyme, the copper-dependent ammonia monooxygenase, is lacking, in particular for the environmentally abundant ammonia-oxidizing archaea (AOA). Here the structure of the enzyme is investigated by blue-native gel electrophoresis and proteomics from native membrane complexes of two AOA. Besides the known AmoABC subunits and the earlier predicted AmoX, two new protein subunits, AmoY and AmoZ, were identified. They are unique to AOA, highly conserved and co-regulated, and their genes are linked to other AMO subunit genes in streamlined AOA genomes. Modeling and in-gel cross-link approaches support an overall protomer structure similar to the distantly related bacterial particulate methane monooxygenase but also reveals clear differences in extracellular domains of the enzyme. These data open avenues for further structure-function studies of this ecologically important nitrification complex.

Published

2023

5. Mechanism of receptor assembly via the pleiotropic adipokine Leptin

Author

Tsirigotaki, Alexandra, Dansercoer, Ann, Verschueren, Koen H. G., Marković, Iva, Pollmann, Christoph, Hafer, Maximillian, Felix, Jan, Birck, Catherine, Van Putte, Wouter, Catteeuw, Dominiek, Tavernier, Jan, Fernando Bazan, J., Piehler, Jacob, Savvides, Savvas N., and Verstraete, Kenneth

Abstract

The adipokine Leptin activates its receptor LEP-R in the hypothalamus to regulate body weight and exerts additional pleiotropic functions in immunity, fertility and cancer. However, the structure and mechanism of Leptin-mediated LEP-R assemblies has remained unclear. Intriguingly, the signaling-competent isoform of LEP-R is only lowly abundant amid several inactive short LEP-R isoforms contributing to a mechanistic conundrum. Here we show by X-ray crystallography and cryo-EM that, in contrast to long-standing paradigms, Leptin induces type I cytokine receptor assemblies featuring 3:3 stoichiometry and demonstrate such Leptin-induced trimerization of LEP-R on living cells via single-molecule microscopy. In mediating these assemblies, Leptin undergoes drastic restructuring that activates its site III for binding to the Ig domain of an adjacent LEP-R. These interactions are abolished by mutations linked to obesity. Collectively, our study provides the structural and mechanistic framework for how evolutionarily conserved Leptin:LEP-R assemblies with 3:3 stoichiometry can engage distinct LEP-R isoforms to achieve signaling.

Published

2023

6. EGOC inhibits TOROID polymerization by structurally activating TORC1

Author

Prouteau, Manoël, Bourgoint, Clélia, Felix, Jan, Bonadei, Lenny, Sadian, Yashar, Gabus, Caroline, Savvides, Savvas N., Gutsche, Irina, Desfosses, Ambroise, and Loewith, Robbie

Abstract

Target of rapamycin complex 1 (TORC1) is a protein kinase controlling cell homeostasis and growth in response to nutrients and stresses. In Saccharomyces cerevisiae, glucose depletion triggers a redistribution of TORC1 from a dispersed localization over the vacuole surface into a large, inactive condensate called TOROID (TORC1 organized in inhibited domains). However, the mechanisms governing this transition have been unclear. Here, we show that acute depletion and repletion of EGO complex (EGOC) activity is sufficient to control TOROID distribution, independently of other nutrient-signaling pathways. The 3.9-Å-resolution structure of TORC1 from TOROID cryo-EM data together with interrogation of key interactions in vivo provide structural insights into TORC1-TORC1′ and TORC1-EGOC interaction interfaces. These data support a model in which glucose-dependent activation of EGOC triggers binding to TORC1 at an interface required for TOROID assembly, preventing TORC1 polymerization and promoting release of active TORC1.

Published

2023

7. Design of protein-binding proteins from the target structure alone

Author

Cao, Longxing, Coventry, Brian, Goreshnik, Inna, Huang, Buwei, Sheffler, William, Park, Joon Sung, Jude, Kevin M., Marković, Iva, Kadam, Rameshwar U., Verschueren, Koen H. G., Verstraete, Kenneth, Walsh, Scott Thomas Russell, Bennett, Nathaniel, Phal, Ashish, Yang, Aerin, Kozodoy, Lisa, DeWitt, Michelle, Picton, Lora, Miller, Lauren, Strauch, Eva-Maria, DeBouver, Nicholas D., Pires, Allison, Bera, Asim K., Halabiya, Samer, Hammerson, Bradley, Yang, Wei, Bernard, Steffen, Stewart, Lance, Wilson, Ian A., Ruohola-Baker, Hannele, Schlessinger, Joseph, Lee, Sangwon, Savvides, Savvas N., Garcia, K. Christopher, and Baker, David

Abstract

The design of proteins that bind to a specific site on the surface of a target protein using no information other than the three-dimensional structure of the target remains a challenge1–5. Here we describe a general solution to this problem that starts with a broad exploration of the vast space of possible binding modes to a selected region of a protein surface, and then intensifies the search in the vicinity of the most promising binding modes. We demonstrate the broad applicability of this approach through the de novo design of binding proteins to 12 diverse protein targets with different shapes and surface properties. Biophysical characterization shows that the binders, which are all smaller than 65 amino acids, are hyperstable and, following experimental optimization, bind their targets with nanomolar to picomolar affinities. We succeeded in solving crystal structures of five of the binder–target complexes, and all five closely match the corresponding computational design models. Experimental data on nearly half a million computational designs and hundreds of thousands of point mutants provide detailed feedback on the strengths and limitations of the method and of our current understanding of protein–protein interactions, and should guide improvements of both. Our approach enables the targeted design of binders to sites of interest on a wide variety of proteins for therapeutic and diagnostic applications.

Published

2022

8. Hapln1b, a central organizer of the ECM, modulates kit signaling to control developmental hematopoiesis in zebrafish

Author

Mahony, Christopher B., Cacialli, Pietro, Pasche, Corentin, Monteiro, Rui, Savvides, Savvas N., and Bertrand, Julien Y.

Abstract

During early vertebrate development, hematopoietic stem and progenitor cells (HSPCs) are produced in hemogenic endothelium located in the dorsal aorta, before they migrate to a transient niche where they expand to the fetal liver and the caudal hematopoietic tissue, in mammals and zebrafish, respectively. In zebrafish, previous studies have shown that the extracellular matrix (ECM) around the aorta must be degraded to enable HSPCs to leave the aortic floor and reach blood circulation. However, the role of the ECM components in HSPC specification has never been addressed. In this study, hapln1b, a key component of the ECM, was specifically expressed in hematopoietic sites in the zebrafish embryo. Gain- and loss-of-function experiments all resulted in the absence of HSPCs in the early embryo, showing that hapln1b is necessary, at the correct level, to specify HSPCs in the hemogenic endothelium. Furthermore, the expression of hapln1b was necessary to maintain the integrity of the ECM through its link domain. By combining functional analyses and computer modeling, we showed that kitlgb interacts with the ECM to specify HSPCs. The findings show that the ECM is an integral component of the microenvironment and mediates the cytokine signaling that is necessary for HSPC specification.

Published

2021

9. Activating mutations in CSF1Rand additional receptor tyrosine kinases in histiocytic neoplasms

Author

Durham, Benjamin H., Lopez Rodrigo, Estibaliz, Picarsic, Jennifer, Abramson, David, Rotemberg, Veronica, De Munck, Steven, Pannecoucke, Erwin, Lu, Sydney X., Pastore, Alessandro, Yoshimi, Akihide, Mandelker, Diana, Ceyhan-Birsoy, Ozge, Ulaner, Gary A., Walsh, Michael, Yabe, Mariko, Petrova-Drus, Kseniya, Arcila, Maria E., Ladanyi, Marc, Solit, David B., Berger, Michael F., Hyman, David M., Lacouture, Mario E., Erickson, Caroline, Saganty, Ruth, Ki, Michelle, Dunkel, Ira J., Santa-María López, Vicente, Mora, Jaume, Haroche, Julien, Emile, Jean-Francois, Decaux, Olivier, Geissmann, Frederic, Savvides, Savvas N., Drilon, Alexander, Diamond, Eli L., and Abdel-Wahab, Omar

Abstract

Histiocytoses are clonal hematopoietic disorders frequently driven by mutations mapping to the BRAF and MEK1 and MEK2 kinases. Currently, however, the developmental origins of histiocytoses in patients are not well understood, and clinically meaningful therapeutic targets outside of BRAF and MEK are undefined. In this study, we uncovered activating mutations in CSF1Rand rearrangements in RETand ALKthat conferred dramatic responses to selective inhibition of RET (selpercatinib) and crizotinib, respectively, in patients with histiocytosis.

Published

2019

10. Acetyl-CoA is produced by the citrate synthase homology module of ATP-citrate lyase

Author

Verstraete, Kenneth, Verschueren, Koen H. G., Dansercoer, Ann, and Savvides, Savvas N.

Published

2021

11. A Novel Conjugate of Bis[((4-bromophenyl)amino)quinazoline], a EGFR-TK Ligand, with a Fluorescent Ru(II)-Bipyridine Complex Exhibits Specific Subcellular Localization in Mitochondria

Author

Ilmi, Rashid, Tseriotou, Eleni, Stylianou, Panayiota, Christou, Yiota A., Ttofi, Iakovia, Dietis, Nikolas, Pitris, Costas, Odysseos, Andreani D., and Georgiades, Savvas N.

Abstract

The epidermal growth factor receptor (EGFR) is a key target in anticancer research, whose aberrant function in malignancies has been linked to severe irregularities in critical cellular processes, including cell cycle progression, proliferation, differentiation, and survival. EGFR mutant variants, either transmembrane or translocated to the mitochondria and/or the nucleus, often exhibit resistance to EGFR inhibitors. The ability to noninvasively image and quantify EGFR provides novel approaches in the detection, monitoring, and treatment of EGFR-related malignancies. The current study aimed to deliver a new theranostic agent that combines fluorescence imaging properties with EGFR inhibition. This was achieved via conjugation of an in-house-developed ((4-bromophenyl)amino)quinazoline inhibitor of mutant EGFR-TK, selected from a focused aminoquinazoline library, with a [Ru(bipyridine)3]2+fluorophore. A triethyleneglycol-derived diamino linker featuring (+)-ionizable sites was employed to link the two functional moieties, affording two unprecedented Ru conjugates with 1:1 and 2:1 stoichiometry of aminoquinazoline to the Ru complex (mono-quinazoline-Ru-conjugate and bis-quinazoline-Ru-conjugate, respectively). The bis-quinazoline-Ru-conjugate, which retains an essential inhibitory activity, was found by fluorescence imaging to be effectively uptaken by Uppsala 87 malignant glioma (grade IV malignant glioma) cells. The fluorescence imaging study and a time-resolved fluorescence resonance energy transfer study indicated a specific subcellular distribution of the conjugate that coincides with that of a mitochondria-targeted dye, suggesting mitochondrial localization of the conjugate and potential association with mitochondria-translocated forms of EGFR. Mitochondrial localization was further documented by the specific concentration of the bis-quinazoline-Ru-conjugate in a mitochondrial isolation assay.

Published

2019

12. Structure of ATP citrate lyase and the origin of citrate synthase in the Krebs cycle

Author

Verschueren, Koen H. G., Blanchet, Clement, Felix, Jan, Dansercoer, Ann, De Vos, Dirk, Bloch, Yehudi, Van Beeumen, Jozef, Svergun, Dmitri, Gutsche, Irina, Savvides, Savvas N., and Verstraete, Kenneth

Abstract

Across different kingdoms of life, ATP citrate lyase (ACLY, also known as ACL) catalyses the ATP-dependent and coenzyme A (CoA)-dependent conversion of citrate, a metabolic product of the Krebs cycle, to oxaloacetate and the high-energy biosynthetic precursor acetyl-CoA1. The latter fuels pivotal biochemical reactions such as the synthesis of fatty acids, cholesterol and acetylcholine2, and the acetylation of histones and proteins3,4. In autotrophic prokaryotes, ACLY is a hallmark enzyme of the reverse Krebs cycle (also known as the reductive tricarboxylic acid cycle), which fixates two molecules of carbon dioxide in acetyl-CoA5,6. In humans, ACLY links carbohydrate and lipid metabolism and is strongly expressed in liver and adipose tissue1and in cholinergic neurons2,7. The structural basis of the function of ACLY remains unknown. Here we report high-resolution crystal structures of bacterial, archaeal and human ACLY, and use distinct substrate-bound states to link the conformational plasticity of ACLY to its multistep catalytic itinerary. Such detailed insights will provide the framework for targeting human ACLY in cancer8–11and hyperlipidaemia12,13. Our structural studies also unmask a fundamental evolutionary relationship that links citrate synthase, the first enzyme of the oxidative Krebs cycle, to an ancestral tetrameric citryl-CoA lyase module that operates in the reverse Krebs cycle. This molecular transition marked a key step in the evolution of metabolism on Earth.

Published

2019

13. Sensory-Neuropathy-Causing Mutations in ATL3 Cause Aberrant ER Membrane Tethering

Author

Krols, Michiel, Detry, Sammy, Asselbergh, Bob, Almeida-Souza, Leonardo, Kremer, Anna, Lippens, Saskia, De Rycke, Riet, De Winter, Vicky, Müller, Franz-Josef, Kurth, Ingo, McMahon, Harvey T., Savvides, Savvas N., Timmerman, Vincent, and Janssens, Sophie

Abstract

The endoplasmic reticulum (ER) is a complex network of sheets and tubules that is continuously remodeled. The relevance of this membrane dynamics is underscored by the fact that mutations in atlastins (ATLs), the ER fusion proteins in mammals, cause neurodegeneration. How defects in this process disrupt neuronal homeostasis is unclear. Using electron microscopy (EM) volume reconstruction of transfected cells, neurons, and patient fibroblasts, we show that hereditary sensory and autonomic neuropathy (HSAN)-causing ATL3 mutants promote aberrant ER tethering hallmarked by bundles of laterally attached ER tubules. In vitro, these mutants cause excessive liposome tethering, recapitulating the results in cells. Moreover, ATL3 variants retain their dimerization-dependent GTPase activity but are unable to promote membrane fusion, suggesting a defect in an intermediate step of the ATL3 functional cycle. Our data show that the effects of ATL3 mutations on ER network organization go beyond a loss of fusion and shed light on neuropathies caused by atlastin defects.

Published

2018

14. Correction to: Unexpected complexity of the ammonia monooxygenase in archaea

Author

Hodgskiss, Logan H, Melcher, Michael, Kerou, Melina, Chen, Weiqiang, Ponce-Toledo, Rafael I, Savvides, Savvas N, Wienkoop, Stefanie, Hartl, Markus, and Schleper, Christa

Published

2023

15. Transitional B cells commit to marginal zone B cell fate by Taok3-mediated surface expression of ADAM10

Author

Hammad, Hamida, Vanderkerken, Matthias, Pouliot, Philippe, Deswarte, Kim, Toussaint, Wendy, Vergote, Karl, Vandersarren, Lana, Janssens, Sophie, Ramou, Ioanna, Savvides, Savvas N, Haigh, Jody J, Hendriks, Rudi, Kopf, Manfred, Craessaerts, Katleen, de Strooper, Bart, Kearney, John F, Conrad, Daniel H, and Lambrecht, Bart N

Abstract

Notch2 and B cell antigen receptor (BCR) signaling determine whether transitional B cells become marginal zone B (MZB) or follicular B (FoB) cells in the spleen, but it is unknown how these pathways are related. We generated Taok3−/−mice, lacking the serine/threonine kinase Taok3, and found cell-intrinsic defects in the development of MZB but not FoB cells. Type 1 transitional (T1) B cells required Taok3 to rapidly respond to ligation by the Notch ligand Delta-like 1. BCR ligation by endogenous or exogenous ligands induced the surface expression of the metalloproteinase ADAM10 on T1 B cells in a Taok3-dependent manner. T1 B cells expressing surface ADAM10 were committed to becoming MZB cells in vivo, whereas T1 B cells lacking expression of ADAM10 were not. Thus, during positive selection in the spleen, BCR signaling causes immature T1 B cells to become receptive to Notch ligands via Taok3-mediated surface expression of ADAM10.

Published

2017

16. Mechanisms of immunomodulation by mammalian and viral decoy receptors: insights from structures

Author

Felix, Jan and Savvides, Savvas N.

Abstract

Modulation of cellular immune and inflammatory processes — including antiviral defence mechanisms — relies crucially on cytokines, chemokines and their cell surface receptors.Alternative versions of mammalian cytokine and chemokine receptors, widely known as decoy receptors, provide a key extension of immunoregulatory pathways in health and disease.Decoy receptors typically mimic the binding principles that underlie the assembly of canonical complexes between protein effectors and cognate receptors.Structural analyses and comparisons of canonical and decoy receptor complexes have revealed the diverse structural and mechanistic principles that underlie the immunomodulatory potency of decoy receptors.Mechanisms of immune system subversion by viruses often feature virus-encoded decoy receptors that target host cytokines and chemokines.Viral decoy receptors display structural and molecular mimicry of host receptors, but often use other mechanisms in addition to these 'in-built' features, including the use of novel protein scaffolds with functions that are unrelated to host proteins.Structural and mechanistic annotations of mammalian and viral immunomodulatory decoy receptors may enable us to harness the therapeutic potential of such proteins and their complexes.

Published

2017

17. Structural basis of activation and antagonism of receptor signaling mediated by interleukin-27

Author

Składanowska, Katarzyna, Bloch, Yehudi, Strand, Jamie, White, Kerry F., Hua, Jing, Aldridge, Daniel, Welin, Martin, Logan, Derek T., Soete, Arne, Merceron, Romain, Murphy, Casey, Provost, Mathias, Bazan, J. Fernando, Hunter, Christopher A., Hill, Jonathan A., and Savvides, Savvas N.

Abstract

Interleukin-27 (IL-27) uniquely assembles p28 and EBI3 subunits to a heterodimeric cytokine that signals via IL-27Rα and gp130. To provide the structural framework for receptor activation by IL-27 and its emerging therapeutic targeting, we report here crystal structures of mouse IL-27 in complex with IL-27Rα and of human IL-27 in complex with SRF388, a monoclonal antibody undergoing clinical trials with oncology indications. One face of the helical p28 subunit interacts with EBI3, while the opposite face nestles into the interdomain elbow of IL-27Rα to juxtapose IL-27Rα to EBI3. This orients IL-27Rα for paired signaling with gp130, which only uses its immunoglobulin domain to bind to IL-27. Such a signaling complex is distinct from those mediated by IL-12 and IL-23. The SRF388 binding epitope on IL-27 overlaps with the IL-27Rα interaction site explaining its potent antagonistic properties. Collectively, our findings will facilitate the mechanistic interrogation, engineering, and therapeutic targeting of IL-27.

Published

2022

18. A Small Molecule Mimicking a Phosphatidylinositol (4,5)-Bisphosphate Binding Pleckstrin Homology Domain

Author

Mak, Lok Hang, Georgiades, Savvas N., Rosivatz, Evelyn, Whyte, Gillian F., Mirabelli, Marianna, Vilar, Ramon, and Woscholski, Rudiger

Abstract

Inositol phospholipids have emerged as important key players in a wide variety of cellular functions. Among the seven existing inositol phospholipids, phosphatidylinositol (4,5)-bisphosphate (PI(4,5)P2) has attracted much attention in recent years due to its important role in numerous cellular signaling events and regulations, which in turn impact several human diseases. This particular lipid is recognized in the cell by specific lipid binding domains, such as the Pleckstrin-homology (PH) domain, which is also employed as a tool to monitor this important lipid. Here, we describe the synthesis and biological characterization of a small molecule that mimics the PH domain as judged by its ability to bind specifically to only PI(4,5)P2and effectively compete with the PH domain in vitroand in a cellular environment. The binding constant of this small molecule PH domain mimetic (PHDM) was determined to be 17.6 ± 10.1 μM, similar in potency to the PH domain. Using NIH 3T3 mouse fibroblast cells we demonstrated that this compound is cell-permeable and able to modulate PI(4,5)P2-dependent effects in a cellular environment such as the endocytosis of the transferrin receptor, loss of mitochondria, as well as stress fiber formation. This highly PI(4,5)P2-specific chemical mimetic of a PH domain not only is a powerful research tool but might also be a lead compound in future drug developments targeting PI(4,5)P2-dependent diseases such as Lowe syndrome.

Published

2011

19. Structural insights into the extracellular assembly of the hematopoietic Flt3 signaling complex

Author

Verstraete, Kenneth, Vandriessche, Gonzalez, Januar, Mariska, Elegheert, Jonathan, Shkumatov, Alexander V., Desfosses, Ambroise, Van Craenenbroeck, Kathleen, Svergun, Dmitri I., Gutsche, Irina, Vergauwen, Bjorn, and Savvides, Savvas N.

Abstract

The class III receptor tyrosine kinase (RTKIII) Fms-like tyrosine kinase receptor 3 (Flt3) and its cytokine ligand (FL) play central roles in hematopoiesis and the immune system, by establishing signaling cascades crucial for the development and homeostasis of hematopoietic progenitors and antigen-presenting dendritic cells. However, Flt3 is also one of the most frequently mutated receptors in hematologic malignancies and is currently a major prognostic factor and clinical target for acute myeloid leukemia. Here, we report the structural basis for the Flt3 ligand-receptor complex and unveil an unanticipated extracellular assembly unlike any other RTKIII/V complex characterized to date. FL induces dimerization of Flt3 via a remarkably compact binding epitope localized at the tip of extracellular domain 3 of Flt3, and it invokes a ternary complex devoid of homotypic receptor interactions. Comparisons of Flt3 with homologous receptors and available mutagenesis data for FL have allowed us to rationalize the unique features of the Flt3 extracellular assembly. Furthermore, thermodynamic dissection of complex formation points to a pronounced enthalpically driven binding event coupled to an entropic penalty. Together, our data suggest that the high-affinity Flt3:FL complex is driven in part by a single preformed binding epitope on FL reminiscent of a “lock-and-key” binding mode, thereby setting the stage for antagonist design.

Published

2011

20. Wechselwirkung von Metallkomplexen mit G‐Quadruplex‐DNA

Author

Georgiades, Savvas N., Abd Karim, Nurul H., Suntharalingam, Kogularamanan, and Vilar, Ramon

Abstract

Guaninreiche DNA‐Sequenzen können sich zu viersträngigen Aggregaten anordnen, die als G‐Quadruplexe bezeichnet werden. Man nimmt an, dass diese DNA‐Sekundärstrukturen an der Regulation verschiedener biologischer Schlüsselprozesse beteiligt sind. Im menschlichen Genom kommen guaninreiche Sequenzen mit dem Potenzial zur Bildung von G‐Quadruplexen beispielsweise im Telomer sowie in den Promoterregionen bestimmter Onkogene vor. Die Identifizierung dieser Sequenzen als neue Zielstrukturen für Tumortherapeutika hat großes Interesse an der Entwicklung von Verbindungen ausgelöst, die mit Quadruplex‐DNA wechselwirken können. Die meisten bekannten Quadruplex‐DNA‐Bindungssubstanzen beruhen zwar auf rein organischen Templaten, später wurde aber nachgewiesen, dass auch viele Metallkomplexe mit dieser DNA‐Sekundärstruktur effiziente Wechselwirkungen eingehen. Dieser Aufsatz gibt einen Überblick über die wichtigen Funktionen, die Metallkomplexe als Quadruplex‐DNA‐Bindungssubstanzen haben können, und diskutiert die besonderen Eigenschaften von Metallzentren auf diese Verbindungen.

Published

2010

21. Crystal structure of the anticoagulant slow form of thrombin.

Author

Pineda, Agustin O, Savvides, Savvas N, Waksman, Gabriel, and Di Cera, Enrico

Abstract

Using the thrombin mutant R77aA devoid of the site of autoproteolytic degradation at exosite I, we have solved for the first time the structure of thrombin free of any inhibitors and effector molecules and stabilized in the Na(+)-free slow form. The slow form shows subtle differences compared with the currently available structures of the Na(+)-bound fast form that carry inhibitors at the active site or exosite I. The most notable differences are the displacement of Asp-189 in the S1 specificity pocket, a downward shift of the 190-193 strand, a rearrangement of the side chain of Glu-192, and a significant shift in the position of the catalytic Ser-195 that is no longer within H-bonding distance from His-57. The structure of the slow form explains the reduced specificity toward synthetic and natural substrates and suggests a molecular basis for its anticoagulant properties.

Published

2002

22. Crystal Structure of the Antioxidant Enzyme Glutathione Reductase Inactivated by Peroxynitrite*

Author

Savvides, Savvas N., Scheiwein, Michael, Böhme, Catharina C., Arteel, Gavin E., Karplus, P. Andrew, Becker, Katja, and Schirmer, R. Heiner

Abstract

As part of our studies on the nitric oxide-related pathology of cerebral malaria, we show that the antioxidative enzyme glutathione reductase (GR) is inactivated by peroxynitrite, with GR from the malarial parasite Plasmodium falciparumbeing more sensitive than human GR. The crystal structure of modified human GR at 1.9-Å resolution provides the first picture of protein inactivation by peroxynitrite and reveals that this is due to the exclusive nitration of 2 Tyr residues (residues 106 and 114) at the glutathione disulfide-binding site. The selective nitration explains the impairment of binding the peptide substrate and thus the nearly 1000-fold decrease in catalytic efficiency (kcat/Km) of glutathione reductase observed at physiologic pH. By oxidizing the catalytic dithiol to a disulfide, peroxynitrite itself can act as a substrate of unmodified and bisnitrated P. falciparumglutathione reductase.

Published

2002

23. Flt3 ligand structure and unexpected commonalities of helical bundles and cystine knots

Author

Savvides, Savvas N., Boone, Tom, and Andrew Karplus, P.

Abstract

Human Flt3 ligand (Flt3L) stimulates early hematopoiesis by activating a type III tyrosine kinase receptor on primitive bone marrow stem cells. The crystal structure of soluble Flt3L reveals that it is a homodimer of two short chain α-helical bundles. Comparisons of structure-function relationships of Flt3L with the homologous hematopoietic cytokines macrophage colony stimulating factor (MCSF) and stem cell factor (SCF) suggest that they have a common receptor binding mode that is distinct from the paradigm derived from the complex of growth hormone with its receptor. Furthermore, we identify recognition features common to all helical and cystine-knot protein ligands that activate type III tyrosine kinase receptors, and the closely related type V tyrosine kinase receptors.

Published

2000

24. Enzyme inactivation through sulfhydryl oxidation by physiologic NO-carriers

Author

Becker, Katja, Savvides, Savvas N., Keese, Michael, Schirmer, R. Heiner, and Karplus, P. Andrew

Abstract

Nitric oxide (NO) is a pluripotent regulatory molecule, yet the molecular mechanisms by which it exerts its effects are largely unknown. Few physiologic target molecules of NO have been identified, and even for these, the modifications caused by NO remain uncharacterized. Human glutathione reductase (hGR), a central enzyme of cellular antioxidant defense, is inhibited by S-nitrosoglutathione (GSNO) and by diglutathionyl-dinitroso-iron (DNIC-[GSH]2), two in vivo transport forms of NO. Here, crystal structures of hGR inactivated by GSNO and DNIC-[GSH]2at 1.7 Å resolution provide the first picture of enzyme inactivation by NO-carriers: in GSNO-modified hGR, the active site residue Cys 63 is oxidized to an unusually stable cysteine sulfenic acid (R-SOH), whereas modification with DNIC-[GSH]2oxidizes Cys 63 to a cysteine sulfinic acid (R-SO2H). Our results illustrate that various forms of NO can mediate distinct chemistry, and that sulfhydryl oxidation must be considered as a major mechanism of NO action.

Published

1998

25. DNA methylation repels binding of hypoxia-inducible transcription factors to maintain tumor immunotolerance

Author

D’Anna, Flora, Van Dyck, Laurien, Xiong, Jieyi, Zhao, Hui, Berrens, Rebecca V., Qian, Junbin, Bieniasz-Krzywiec, Pawel, Chandra, Vikas, Schoonjans, Luc, Matthews, Jason, De Smedt, Julie, Minnoye, Liesbeth, Amorim, Ricardo, Khorasanizadeh, Sepideh, Yu, Qian, Zhao, Liyun, De Borre, Marie, Savvides, Savvas N., Simon, M. Celeste, Carmeliet, Peter, Reik, Wolf, Rastinejad, Fraydoon, Mazzone, Massimiliano, Thienpont, Bernard, and Lambrechts, Diether

Abstract

Background: Hypoxia is pervasive in cancer and other diseases. Cells sense and adapt to hypoxia by activating hypoxia-inducible transcription factors (HIFs), but it is still an outstanding question why cell types differ in their transcriptional response to hypoxia. Results: We report that HIFs fail to bind CpG dinucleotides that are methylated in their consensus binding sequence, both in in vitro biochemical binding assays and in vivo studies of differentially methylated isogenic cell lines. Based on in silico structural modeling, we show that 5-methylcytosine indeed causes steric hindrance in the HIF binding pocket. A model wherein cell-type-specific methylation landscapes, as laid down by the differential expression and binding of other transcription factors under normoxia, control cell-type-specific hypoxia responses is observed. We also discover ectopic HIF binding sites in repeat regions which are normally methylated. Genetic and pharmacological DNA demethylation, but also cancer-associated DNA hypomethylation, expose these binding sites, inducing HIF-dependent expression of cryptic transcripts. In line with such cryptic transcripts being more prone to cause double-stranded RNA and viral mimicry, we observe low DNA methylation and high cryptic transcript expression in tumors with high immune checkpoint expression, but not in tumors with low immune checkpoint expression, where they would compromise tumor immunotolerance. In a low-immunogenic tumor model, DNA demethylation upregulates cryptic transcript expression in a HIF-dependent manner, causing immune activation and reducing tumor growth. Conclusions: Our data elucidate the mechanism underlying cell-type-specific responses to hypoxia and suggest DNA methylation and hypoxia to underlie tumor immunotolerance.

Published

2020

26. ChemInform Abstract: Interaction of Metal Complexes with G‐Quadruplex DNA

Author

Georgiades, Savvas N., Karim, Nurul H. Abd, Suntharalingam, Kogularamanan, and Vilar, Ramon

Abstract

Review: 105 refs.

Published

2010

27. Total Synthesis of Psammaplysenes A (Ia) and B (Ib), Naturally Occurring Inhibitors of FOXO1a Nuclear Export.

Author

Georgiades, Savvas N. and Clardy, Jon

Published

2006

28. Secretion superfamily ATPases swing big.

Author

Savvides SN

Subjects

Adenosine Triphosphatases genetics, Archaeal Proteins chemistry, Archaeal Proteins genetics, Archaeal Proteins metabolism, Bacterial Proteins chemistry, Bacterial Proteins genetics, Bacterial Proteins metabolism, Adenosine Triphosphatases chemistry, Adenosine Triphosphatases metabolism, Multigene Family

Published

2007