Your search keyword '"Grütter, Markus G."' showing total 241 results

201. Inhibition of Caspase-2 by a Designed Ankyrin Repeat Protein: Specificity, Structure, and Inhibition Mechanism

Author

Schweizer, Andreas, Roschitzki-Voser, Heidi, Amstutz, Patrick, Briand, Christophe, Gulotti-Georgieva, Maya, Prenosil, Eva, Binz, H. Kaspar, Capitani, Guido, Baici, Antonio, Plückthun, Andreas, and Grütter, Markus G.

Subjects

*APOPTOSIS, *DISSECTION, *CELL death, *SURGERY

Abstract

Summary: Specific and potent caspase inhibitors are indispensable for the dissection of the intricate pathways leading to apoptosis. We selected a designed ankyrin repeat protein (DARPin) from a combinatorial library that inhibits caspase-2 in vitro with a subnanomolar inhibition constant and, in contrast to the peptidic caspase inhibitors, with very high specificity for this particular caspase. The crystal structure of this inhibitor (AR_F8) in complex with caspase-2 reveals the molecular basis for the specificity and, together with kinetic analyses, the allosteric mechanism of inhibition. The structure also shows a conformation of the active site that can be exploited for the design of inhibitory compounds. AR_F8 is a specific inhibitor of an initiator caspase and has the potential to help identify the function of caspase-2 in the complex biological apoptotic signaling network. [Copyright &y& Elsevier]

Published

2007

202. Structural and functional insights into the assembly of type 1 pili from Escherichia coli

Author

Capitani, Guido, Eidam, Oliv, Glockshuber, Rudi, and Grütter, Markus G.

Subjects

*ESCHERICHIA coli, *ENTEROBACTERIACEAE, *ADSORPTION (Chemistry), *TISSUES

Abstract

Abstract: Type 1 pili are filamentous protein complexes that are anchored to the outer membrane of uropathogenic Escherichia coli and mediate bacterial adhesion to the surface of urinary epithelium cells. We review here the current status of structural and functional studies on the assembly of type 1 pili. [Copyright &y& Elsevier]

Published

2006

203. Extended Substrate Recognition in Caspase-3 Revealed by High Resolution X-ray Structure Analysis

Author

Ganesan, Rajkumar, Mittl, Peer R.E., Jelakovic, Stjepan, and Grütter, Markus G.

Subjects

*HYDROGEN, *CELL death, *ORGANIC compounds, *PROTEOLYTIC enzymes

Abstract

Abstract: Caspases are cysteine proteases involved in the signalling cascades of programmed cell death in which caspase-3 plays a central role, since it propagates death signals from intrinsic and extrinsic stimuli to downstream targets. The atomic resolution (1.06 Å) crystal structure of the caspase-3 DEVD-cmk complex reveals the structural basis for substrate selectivity in the S4 pocket. A low-barrier hydrogen bond is observed between the side-chains of the P4 inhibitor aspartic acid and Asp179 of the N-terminal tail of the symmetry related p12 subunit. Site-directed mutagenesis of Asp179 confirmed the significance of this residue in substrate recognition. In the 1.06 Å crystal structure, a radiation damage induced rearrangement of the inhibitor methylketone moiety was observed. The carbon atom that in a substrate would represent the scissile peptide bond carbonyl carbon clearly shows a tetrahedral coordination and resembles the postulated tetrahedral intermediate of the acylation reaction. [Copyright &y& Elsevier]

Published

2006

204. Escherichia coli acid resistance: pH-sensing, activation by chloride and autoinhibition in GadB.

Author

Gut, Heinz, Pennacchietti, Eugenia, John, Robert A, Bossa, Francesco, Capitani, Guido, De Biase, Daniela, and Grütter, Markus G

Subjects

*ESCHERICHIA coli, *ENTEROBACTERIACEAE, *GLUTAMATE decarboxylase, *CHLORIDES, *HYDROGEN-ion concentration, *ACIDITY function

Abstract

Escherichia coli and other enterobacteria exploit the H+-consuming reaction catalysed by glutamate decarboxylase to survive the stomach acidity before reaching the intestine. Here we show that chloride, extremely abundant in gastric secretions, is an allosteric activator producing a 10-fold increase in the decarboxylase activity at pH 5.6. Cooperativity and sensitivity to chloride were lost when the N-terminal 14 residues, involved in the formation of two triple-helix bundles, were deleted by mutagenesis. X-ray structures, obtained in the presence of the substrate analogue acetate, identified halide-binding sites at the base of each N-terminal helix, showed how halide binding is responsible for bundle stability and demonstrated that the interconversion between active and inactive forms of the enzyme is a stepwise process. We also discovered an entirely novel structure of the cofactor pyridoxal 5′-phosphate (aldamine) to be responsible for the reversibly inactivated enzyme. Our results link the entry of chloride ions, via the H+/Cl− exchange activities of ClC-ec1, to the trigger of the acid stress response in the cell when the intracellular proton concentration has not yet reached fatal values. [ABSTRACT FROM AUTHOR]

Published

2006

205. High-resolution Structures of Escherichia coli cDsbD in Different Redox States: A Combined Crystallographic, Biochemical and Computational Study

Author

Stirnimann, Christian U., Rozhkova, Anna, Grauschopf, Ulla, Böckmann, Rainer A., Glockshuber, Rudi, Capitani, Guido, and Grütter, Markus G.

Subjects

*ESCHERICHIA coli, *OXIDATION-reduction reaction, *PROTEINS, *BIOMOLECULES

Abstract

Escherichia coli DsbD transports electrons from cytoplasmic thioredoxin to periplasmic target proteins. DsbD is composed of an N-terminal (nDsbD) and a C-terminal (cDsbD) periplasmic domain, connected by a central transmembrane domain. Each domain possesses two cysteine residues essential for electron transport. The transport proceeds via disulfide exchange reactions from cytoplasmic thioredoxin to the central transmembrane domain and via cDsbD to nDsbD, which then reduces the periplasmic target proteins. We determined four high-resolution structures of cDsbD: oxidized (1.65Å resolution), chemically reduced (1.3Å), photo-reduced (1.1Å) and chemically reduced at pH increased from 4.6 to 7. The latter structure was refined at 0.99Å resolution, the highest achieved so far for a thioredoxin superfamily member. The data reveal unprecedented structural details of cDsbD, demonstrating that the domain is very rigid and undergoes hardly any conformational change upon disulfide reduction or interaction with nDsbD. In full agreement with the crystallographic results, guanidinium chloride-induced unfolding and refolding experiments indicate that oxidized and reduced cDsbD are equally stable. We confirmed the structural rigidity of cDsbD by molecular dynamics simulations. A remarkable feature of cDsbD is the pK a of 9.3 for the active site Cys461: this value, determined using two different experimental methods, surprisingly was around 2.5 units higher than expected on the basis of the redox potential. Additionally, taking advantage of the very high quality of the cDsbD structures, we carried out pK a calculations, which gave results in agreement with the experimental findings. In conclusion, our wide-scope analysis of cDsbD, encompassing atomic-resolution crystallography, computational chemistry and biophysical measurements, highlighted two so far unrecognized key aspects of this domain: its unusual redox properties and extreme rigidity. Both are likely to be correlated to the role of cDsbD as a covalently linked electron shuttle between the membrane domain and the N-terminal periplasmic domain of DsbD. [Copyright &y& Elsevier]

Published

2006

206. Structure of the Mammalian NOS Regulator Dimethylarginine Dimethylaminohydrolase: A Basis for the Design of Specific Inhibitors

Author

Frey, Daniel, Braun, Oliver, Briand, Christophe, Vašák, Milan, and Grütter, Markus G.

Subjects

*ENZYME inhibitors, *ARGININE, *NITRIC oxide, *ENZYME regulation

Abstract

Summary: Dimethylarginine dimethylaminohydrolase (DDAH) is involved in the regulation of nitric oxide synthase (NOS) by metabolizing the free endogenous arginine derivatives Nω -methyl-L-arginine (MMA) and Nω,Nω -dimethyl-L-arginine (ADMA), which are competitive inhibitors of NOS. Here, we present high-resolution crystal structures of DDAH isoform 1 (DDAH-1) isolated from bovine brain in complex with different inhibitors, including S-nitroso-L-homocysteine and Zn2+, a regulator of this mammalian enzyme. The structure of DDAH-1 consists of a propeller-like fold similar to other arginine-modifying enzymes and a flexible loop, which adopts different conformations and acts as a lid at the entrance of the active site. The orientation and interaction mode of inhibitors in the active site give insight into the regulation and the molecular mechanism of the enzyme. The presented structures provide a basis for the structure-based development of specific DDAH-1 inhibitors that might be useful in the therapeutic treatment of NOS dysfunction-related diseases. [Copyright &y& Elsevier]

Published

2006

207. Allosteric Inhibition of Aminoglycoside Phosphotransferase by a Designed Ankyrin Repeat Protein

Author

Kohl, Andreas, Amstutz, Patrick, Parizek, Petra, Binz, H. Kaspar, Briand, Christophe, Capitani, Guido, Forrer, Patrik, Plückthun, Andreas, and Grütter, Markus G.

Subjects

*ENZYME analysis, *PATHOGENIC bacteria, *MEDICAL bacteriology, *FUNGUS-bacterium relationships, *HOMOLOGY (Biology)

Abstract

Summary: Aminoglycoside phosphotransferase (3′)-IIIa (APH) is a bacterial kinase that confers antibiotic resistance to many pathogenic bacteria and shares structural homology with eukaryotic protein kinases. We report here the crystal structure of APH, trapped in an inactive conformation by a tailor-made inhibitory ankyrin repeat (AR) protein, at 2.15 Å resolution. The inhibitor was selected from a combinatorial library of designed AR proteins. The AR protein binds the C-terminal lobe of APH and thereby stabilizes three α helices, which are necessary for substrate binding, in a significantly displaced conformation. BIAcore analysis and kinetic enzyme inhibition experiments are consistent with the proposed allosteric inhibition mechanism. In contrast to most small-molecule kinase inhibitors, the AR proteins are not restricted to active site binding, allowing for higher specificity. Inactive conformations of pharmaceutically relevant enzymes, as can be elucidated with the approach presented here, represent powerful starting points for rational drug design. [Copyright &y& Elsevier]

Published

2005

208. Intracellular Kinase Inhibitors Selected from Combinatorial Libraries of Designed Ankyrin Repeat Proteins.

Author

Amstutz, Patrick, Binz, H. Kaspar, Parizek, Petra, Stumpp, Michael T., Kohl, Andreas, Grütter, Markus G., Forrer, Patrik, and Plückthun, Andreas

Subjects

*PROTEINS, *PHOSPHOTRANSFERASES, *PATHOGENIC bacteria, *ANTIBIOTICS, *ENZYMES

Abstract

The specific intracellular inhibition of protein activity at the protein level allows the determination of protein function in the cellular context. We demonstrate here the use of designed ankyrin repeat proteins as tailor-made intracellular kinase inhibitors. The target was aminoglycoside phosphotransferase (3')-IIIa (APH), which mediates resistance to aminoglycoside antibiotics in pathogenic bacteria and shares structural homology with eukaryotic protein kinases. Combining a selection and screening approach, we isolated 198 potential APH inhibitors from highly diverse combinatorial libraries of designed ankyrin repeat proteins. A detailed analysis of several inhibitors revealed that they bind APH with high specificity and with affinities down to the subnanomolar range. In vitro, the most potent inhibitors showed complete enzyme inhibition, and in vivo, a phenotype comparable with the gene knockout was observed, fully restoring antibiotic sensitivity in resistant bacteria. These results underline the great potential of designed ankyrin repeat proteins for modulation of intracellular protein function. [ABSTRACT FROM AUTHOR]

Published

2005

209. Structural Basis and Kinetics of DsbD-Dependent Cytochrome c Maturation

Author

Stirnimann, Christian U., Rozhkova, Anna, Grauschopf, Ulla, Grütter, Markus G., Glockshuber, Rudi, and Capitani, Guido

Subjects

*ESCHERICHIA, *BIOMOLECULES, *ENTEROBACTERIACEAE, *CATHODE rays

Abstract

Summary: DsbD from Escherichia coli transports two electrons from cytoplasmic thioredoxin to the periplasmic substrate proteins DsbC, DsbG and CcmG. DsbD consists of an N-terminal periplasmic domain (nDsbD), a C-terminal periplasmic domain, and a central transmembrane domain. Each domain possesses two cysteines required for electron transport. Herein, we demonstrate fast (3.9 × 105 M−1s−1) and direct disulfide exchange between nDsbD and CcmG, a highly specific disulfide reductase essential for cytochrome c maturation. We determined the crystal structure of the disulfide-linked complex between nDsbD and the soluble part of CcmG at 1.94 Å resolution. In contrast to the other two known complexes of nDsbD with target proteins, the N-terminal segment of nDsbD contributes to specific recognition of CcmG. This and other features, like the possibility of using an additional interaction surface, constitute the structural basis for the adaptability of nDsbD to different protein substrates. [Copyright &y& Elsevier]

Published

2005

210. Structural basis of chaperone–subunit complex recognition by the type 1 pilus assembly platform FimD.

Author

Nishiyama, Mireille, Horst, Reto, Eidam, Oliv, Herrmann, Torsten, Ignatov, Oleksandr, Vetsch, Michael, Bettendorff, Pascal, Jelesarov, Ilian, Grütter, Markus G., Wüthrich, Kurt, Glockshuber, Rudi, and Capitani, Guido

Subjects

*ESCHERICHIA coli, *BACTERIAL genetics, *CELL membranes, *CHROMOSOMAL translocation, *BIOMOLECULES, *MOLECULAR biology

Abstract

Adhesive type 1 pili from uropathogenic Escherichia coli are filamentous protein complexes that are attached to the assembly platform FimD in the outer membrane. During pilus assembly, FimD binds complexes between the chaperone FimC and type 1 pilus subunits in the periplasm and mediates subunit translocation to the cell surface. Here we report nuclear magnetic resonance and X-ray protein structures of the N-terminal substrate recognition domain of FimD (FimDN) before and after binding of a chaperone–subunit complex. FimDN consists of a flexible N-terminal segment of 24 residues, a structured core with a novel fold, and a C-terminal hinge segment. In the ternary complex, residues 1–24 of FimDN specifically interact with both FimC and the subunit, acting as a sensor for loaded FimC molecules. Together with in vivo complementation studies, we show how this mechanism enables recognition and discrimination of different chaperone–subunit complexes by bacterial pilus assembly platforms. [ABSTRACT FROM AUTHOR]

Published

2005

211. Structural basis and kinetics of inter- and intramolecular disulfide exchange in the redox catalyst DsbD.

Author

Rozhkova, Anna, Stirnimann, Christian U., Frei, Patrick, Grauschopf, Ulla, Brunisholz, René, Grütter, Markus G., Capitani, Guido, and Glockshuber, Rudi

Subjects

*ESCHERICHIA coli, *ELECTRON transport, *THIOREDOXIN, *ISOMERASES, *CATALYSIS, *PROTEINS

Abstract

DsbD from Escherichia coli catalyzes the transport of electrons from cytoplasmic thioredoxin to the periplasmic disulfide isomerase DsbC. DsbD contains two periplasmically oriented domains at the N- and C-terminus (nDsbD and cDsbD) that are connected by a central transmembrane (TM) domain. Each domain contains a pair of cysteines that are essential for catalysis. Here, we show that Cys109 and Cys461 form a transient interdomain disulfide bond between nDsbD and cDsbD in the reaction cycle of DsbD. We solved the crystal structure of this catalytic intermediate at 2.85 Å resolution, which revealed large relative domain movements in DsbD as a consequence of a strong overlap between the surface areas of nDsbD that interact with DsbC and cDsbD. In addition, we have measured the kinetics of all functional and nonfunctional disulfide exchange reactions between redox-active, periplasmic proteins and protein domains from the oxidative DsbA/B and the reductive DsbC/D pathway. We show that both pathways are separated by large kinetic barriers for nonfunctional disulfide exchange between components from different pathways. [ABSTRACT FROM AUTHOR]

Published

2004

212. The critical structural role of a highly conserved histidine residue in group II amino acid decarboxylases

Author

Capitani, Guido, Tramonti, Angela, Bossa, Francesco, Grütter, Markus G., and De Biase, Daniela

Subjects

*GLUTAMATE decarboxylase, *PHOSPHATES, *ENZYMES, *ESCHERICHIA coli

Abstract

Glutamate decarboxylase is a pyridoxal 5′-phosphate (PLP)-dependent enzyme, belonging to the subset of PLP-dependent decarboxylases classified as group II. Site-directed mutagenesis of Escherichia coli glutamate decarboxylase, combined with analysis of the crystal structure, shows that a histidine residue buried in the protein core is critical for correct folding. This histidine is strictly conserved in the PF00282 PFAM family, which includes the group II decarboxylases. A similar role is proposed for residue Ser269, also highly conserved in this group of enzymes, as it provides one of the interactions stabilising His241. [Copyright &y& Elsevier]

Published

2003

213. NMR Structure of the Apoptosis- and Inflammation-Related NALP1 Pyrin Domain

Author

Hiller, Sebastian, Kohl, Andreas, Fiorito, Francesco, Herrmann, Torsten, Wider, Gerhard, Tschopp, Jürg, Grütter, Markus G., and Wüthrich, Kurt

Subjects

*APOPTOSIS, *INFLAMMATION, *PROTEINS, *FAMILIAL Mediterranean fever

Abstract

Signaling in apoptosis and inflammation is often mediated by proteins of the death domain superfamily in the Fas/FADD/Caspase-8 or the Apaf-1/Caspase-9 pathways. This superfamily currently comprises the death domain (DD), death effector domain (DED), caspase recruitment domain (CARD), and pyrin domain (PYD) subfamilies. The PYD subfamily is most abundant, but three-dimensional structures are only available for the subfamilies DD, DED, and CARD, which have an antiparallel arrangement of six α helices as common fold. This paper presents the NMR structure of PYD of NALP1, a protein that is involved in the innate immune response and is a component of the inflammasome. The structure of NALP1 PYD differs from all other known death domain superfamily structures in that the third α helix is replaced by a flexibly disordered loop. This unique feature appears to relate to the molecular basis of familial Mediterranean fever (FMF), a genetic disease caused by single-point mutations. [Copyright &y& Elsevier]

Published

2003

214. Structure-based design of aliskiren, a novel orally effective renin inhibitor

Author

Wood, Jeanette M., Maibaum, Jürgen, Rahuel, Joseph, Grütter, Markus G., Cohen, Nissim-Claude, Rasetti, Vittorio, Rüger, Heinrich, Göschke, Richard, Stutz, Stefan, Fuhrer, Walter, Schilling, Walter, Rigollier, Pascal, Yamaguchi, Yasuchika, Cumin, Frederic, Baum, Hans-Peter, Schnell, Christian R., Herold, Peter, Mah, Robert, Jensen, Chris, and O’Brien, Eoin

Subjects

*HYPERTENSION, *THERAPEUTICS, *CARDIOVASCULAR diseases, *PHARMACOKINETICS

Abstract

Hypertension is a major risk factor for cardiovascular diseases such as stroke, myocardial infarction, and heart failure, the leading causes of death in the Western world. Inhibitors of the renin–angiotensin system (RAS) have proven to be successful treatments for hypertension. As renin specifically catalyses the rate-limiting step of the RAS, it represents the optimal target for RAS inhibition. Several peptide-like renin inhibitors have been synthesized previously, but poor pharmacokinetic properties meant that these compounds were not clinically useful. We employed a combination of molecular modelling and crystallographic structure analysis to design renin inhibitors lacking the extended peptide-like backbone of earlier inhibitors, for improved pharmacokinetic properties. This led to the discovery of aliskiren, a highly potent and selective inhibitor of human renin in vitro, and in vivo; once-daily oral doses of aliskiren inhibit renin and lower blood pressure in sodium-depleted marmosets and hypertensive human patients. Aliskiren represents the first in a novel class of renin inhibitors with the potential for treatment of hypertension and related cardiovascular diseases. [Copyright &y& Elsevier]

Published

2003

215. Structural analysis of mycobacterial and murine hsp60 epitopes in complex with the class I MHC molecule H-2Db

Author

Ciatto, Carlo, Capitani, Guido, Tissot, Alain C., Pecorari, Frédéric, Plückthun, Andreas, and Grütter, Markus G.

Subjects

*PEPTIDES, *T cells

Abstract

The decameric peptide SALQNAASIA from the Mycobacterium bovis heat shock protein (hsp) 60 is recognized by the murine T-cell receptor UZ-3-4 in complex with the murine class I major histocompatibility complex molecule H-2Db. This T-cell receptor cross-reacts with the H-2Db-bound non-homologous decameric peptide KDIGNIISDA from the murine hsp60, but does not recognize the nonameric mycobacterial peptide SALQNAASI. Cross-recognition of the KDIGNIISDA/H-2Db complex induces autoimmune pathology in immunodeficient mice. We solved the X-ray crystal structure of the SALQNAASIA/H-2Db complex at 3.0 A˚ resolution, and we modelled the KDIGNIISDA and SALQNAASI peptides in the H-2Db binding site. The structural analysis of the H-2Db-bound hsp60 epitopes offers insight into T-cell receptor cross-reactivity. [Copyright &y& Elsevier]

Published

2003

216. Structure of 1-aminocyclopropane-1-carboxylate synthase in complex with an amino-oxy analogue of the substrate: implications for substrate binding

Author

Capitani, Guido, Eliot, Andrew C., Gut, Heinz, Khomutov, Radii M., Kirsch, Jack F., and Grütter, Markus G.

Subjects

*METHIONINE, *ENZYMES

Abstract

The crystal structure of 1-aminocyclopropane-1-carboxylate (ACC) synthase in complex with the substrate analogue [2-(amino-oxy)ethyl](5′-deoxyadenosin-5′-yl)(methyl)sulfonium (AMA) was determined at 2.01-A˚ resolution. The crystallographic results show that a covalent adduct (oxime) is formed between AMA (an amino-oxy analogue of the natural substrate S-adenosyl-l-methionine (SAM)) and the pyridoxal 5′-phosphate (PLP) cofactor of ACC synthase. The oxime formation is supported by spectroscopic data. The ACC synthase–AMA structure provides reliable and detailed information on the binding mode of the natural substrate of ACC synthase and complements previous structural and functional work on this enzyme. [Copyright &y& Elsevier]

Published

2003

217. Designed to be stable: Crystal structure of a consensus ankyrin repeat protein.

Author

Kohl, Andreas, Binz, H. Kaspar, Forrer, Patrik, Stumpp, Michael T., Plückthun, Andreas, and Grütter, Markus G.

Subjects

*PROTEINS, *ESCHERICHIA coli

Abstract

Ankyrin repeat (AR) proteins mediate innumerable protein-protein interactions in virtually all phyla. This finding suggested the use of AR proteins as designed binding molecules. Based on sequence and structural analyses, we designed a consensus AR with fixed framework and randomized interacting residues. We generated several combinatorial libraries of AR proteins consisting of defined numbers of this repeat. Randomly chosen library members are expressed in soluble form in the cytoplasm of Escherichia coli constituting up to 30% of total cellular protein and show high thermodynamic stability. We determined the crystal structure of one of those library members to 2.0-Å resolution, providing insight into the consensus AR fold. Besides the highly complementary hydrophobic repeat-repeat interfaces and the absence of structural irregularities in the consensus AR protein, the regular and extended hydrogen bond networks in the β-turn and loop regions are noteworthy. Furthermore, all residues found in the turn region of the Ramachandran plot are glycines. Many of these features also occur in natural AR proteins, but not in this rigorous and standardized fashion. We conclude that the AR domain fold is an intrinsically very stable and well-expressed scaffold, able to display randomized interacting residues. This scaffold represents an excellent basis for the design of novel binding molecules. [ABSTRACT FROM AUTHOR]

Published

2003

218. Insights into the Regulatory Mechanism for Caspase-8 Activation

Author

Donepudi, Mrudula, Sweeney, Aengus Mac, Briand, Christophe, and Grütter, Markus G.

Subjects

*APOPTOSIS, *ENZYME regulation

Abstract

In the death receptor induced apoptotic pathway, caspase-8 autocatalytically cleaves itself at specific cleavage sites. To better understand the regulatory mechanisms behind caspase-8 activation, we compared active wild-type caspase-8 (wtC8) and an uncleavable form of procaspase-8 (uncleavable C8). We demonstrate that wtC8 predominantly exists as a monomer and dimerizes in a concentration and inhibitor binding-dependent fashion. The KD for dimeric wtC8 is ∼50 μM and decreases when inhibitor bound. Uncleavable C8 is mainly monomeric, but a small amount that dimerizes is as active as wtC8. Inhibitor binding does not favor dimerization but induces active site rearrangements in uncleavable C8. Our findings suggest that dimerization is the crucial factor for caspase-8 activation. [Copyright &y& Elsevier]

Published

2003

219. Identification of a basic surface area of the FADD death effector domain critical for apoptotic signaling

Author

Kaufmann, Markus, Bozic, Damir, Briand, Christophe, Bodmer, Jean-Luc, Zerbe, Oliver, Kohl, Andreas, Tschopp, Jürg, and Grütter, Markus G.

Subjects

*SURFACE area, *PROTEINS

Abstract

Death effector domains (DEDs) are protein–protein interaction domains found in the death inducing signaling complex (DISC). Performing a structure-based alignment of all DED sequences we identified a region of high diversity in α-helix 3 and propose a classification of DEDs into class I DEDs typically containing a stretch of basic residues in the α-helix 3 region whereas DEDs of class II do not. Functional assays using mutants of Fas-associated death domain revealed that this basic region influences binding and recruitment of caspase-8 and cellular FLICE inhibitor protein to the DISC. [Copyright &y& Elsevier]

Published

2002

220. Crystal Structure of the Anti-His Tag Antibody 3D5 Single-chain Fragment Complexed to its Antigen

Author

Kaufmann, Markus, Lindner, Peter, Honegger, Annemarie, Blank, Kerstin, Tschopp, Markus, Capitani, Guido, Plückthun, Andreas, and Grütter, Markus G.

Subjects

*CRYSTALS, *IMMUNOGLOBULINS, *EDUCATION

Abstract

The crystal structure of a mutant form of the single-chain fragment (scFv), derived from the monoclonal anti-His tag antibody 3D5, in complex with a hexahistidine peptide has been determined at 2.7 A˚ resolution. The peptide binds to a deep pocket formed at the interface of the variable domains of the light and the heavy chain, mainly through hydrophobic interaction to aromatic residues and hydrogen bonds to acidic residues. The antibody recognizes the C-terminal carboxylate group of the peptide as well as the main chain of the last four residues and the last three imidazole side-chains. The crystals have a solvent content of 77% (v/v) and form 70 A˚-wide channels that would allow the diffusion of peptides or even small proteins. The anti-His scFv crystals could thus act as a framework for the crystallization of His-tagged target proteins. Designed mutations in framework regions of the scFv lead to high-level expression of soluble protein in the periplasm of Escherichia coli. The recombinant anti-His scFv is a convenient detection tool when fused to alkaline phosphatase. When immobilized on a matrix, the antibody can be used for affinity purification of recombinant proteins carrying a very short tag of just three histidine residues, suitable for crystallization. The experimental structure is now the basis for the design of antibodies with even higher stability and affinity. [Copyright &y& Elsevier]

Published

2002

221. The Three-Fold Axis of the HIV-1 Capsid Lattice Is the Species-Specific Binding Interface for TRIM5α

Author

Benjamin Schuler, Damien Morger, Markus G. Grütter, Sara Züger, Jeremy Luban, Maximilian Mittelviefhaus, Franziska Zosel, Martin Bühlmann, University of Zurich, and Grütter, Markus G

Subjects

Models, Molecular, 0301 basic medicine, 1109 Insect Science, binding, Protein Conformation, viruses, Trimer, Crystallography, X-Ray, Antiviral Restriction Factors, Tripartite Motif Proteins, chemistry.chemical_compound, TRIM5α, Sf9 Cells, capsid, TRIM5, 2404 Microbiology, Recombinant Proteins, 3. Good health, Monomer, Capsid, Host-Pathogen Interactions, Cyclophilin A, Protein Binding, CypA, Ubiquitin-Protein Ligases, Immunology, interaction, 610 Medicine & health, Fluorescence correlation spectroscopy, Biology, Microbiology, 03 medical and health sciences, B30.2, Species Specificity, Virology, 10019 Department of Biochemistry, Animals, Humans, Molecule, Protein Interaction Domains and Motifs, 2403 Immunology, Microscale thermophoresis, Structure and Assembly, Proteins, Macaca mulatta, In vitro, 030104 developmental biology, chemistry, Insect Science, Mutation, 2406 Virology, HIV-1, Biophysics, 570 Life sciences, biology, Capsid Proteins, affinity, Carrier Proteins, Cysteine

Abstract

Rhesus TRIM5α (rhTRIM5α) potently restricts replication of human immunodeficiency virus type 1 (HIV-1). Restriction is mediated through direct binding of the C-terminal B30.2 domain of TRIM5α to the assembled HIV-1 capsid core. This host-pathogen interaction involves multiple capsid molecules within the hexagonal HIV-1 capsid lattice. However, the molecular details of this interaction and the precise site at which the B30.2 domain binds remain largely unknown. The human orthologue of TRIM5α (hsTRIM5α) fails to block infection by HIV-1 both in vivo and in vitro . This is thought to be due to differences in binding to the capsid lattice. To map the species-specific binding surface on the HIV-1 capsid lattice, we used microscale thermophoresis and dual-focus fluorescence correlation spectroscopy to measure binding affinity of rhesus and human TRIM5α B30.2 domains to a series of HIV-1 capsid variants that mimic distinct capsid arrangements at each of the symmetry axes of the HIV-1 capsid lattice. These surrogates include previously characterized capsid oligomers, as well as a novel chemically cross-linked capsid trimer that contains cysteine substitutions near the 3-fold axis of symmetry. The results demonstrate that TRIM5α binding involves multiple capsid molecules along the 2-fold and 3-fold interfaces between hexamers and indicate that the binding interface at the 3-fold axis contributes to the well-established differences in restriction potency between TRIM5α orthologues. IMPORTANCE TRIM5α is a cellular protein that fends off infection by retroviruses through binding to the viruses' protein shell surrounding its genetic material. This shell is composed of several hundred capsid proteins arranged in a honeycomb-like hexagonal pattern that is conserved across retroviruses. By binding to the complex lattice formed by multiple capsid proteins, rather than to a single capsid monomer, TRIM5α restriction activity persists despite the high mutation rate in retroviruses such as HIV-1. In rhesus monkeys, but not in humans, TRIM5α confers resistance to HIV-1. By measuring the binding of human and rhesus TRIM5α to a series of engineered HIV-1 capsid mimics of distinct capsid lattice interfaces, we reveal the HIV-1 capsid surface critical for species-specific binding by TRIM5α.

Published

2018

222. Crystal structure of TRIM20 C-terminal coiled-coil/B30.2 fragment: implications for the recognition of higher order oligomers

Author

Damien Morger, Markus G. Grütter, Peer R. E. Mittl, Aleksandra Djekic, Christopher Weinert, University of Zurich, and Grütter, Markus G

Subjects

Models, Molecular, Protein Conformation, Protein domain, Interleukin-1beta, 610 Medicine & health, Plasma protein binding, Biology, Pyrin domain, Article, Protein structure, Capsid, 10019 Department of Biochemistry, Humans, Protein Interaction Domains and Motifs, Coiled coil, 1000 Multidisciplinary, Multidisciplinary, Pyrin, Molecular biology, 3. Good health, Solutions, Cytoskeletal Proteins, Biophysics, HIV-1, 570 Life sciences, biology, Protein Multimerization, Phosphotyrosine-binding domain, TRIM Motif, Linker, Protein Binding

Abstract

Many tripartite motif-containing (TRIM) proteins, comprising RING-finger, B-Box and coiled-coil domains, carry additional B30.2 domains on the C-terminus of the TRIM motif and are considered to be pattern recognition receptors involved in the detection of higher order oligomers (e.g. viral capsid proteins). To investigate the spatial architecture of domains in TRIM proteins we determined the crystal structure of the TRIM20Δ413 fragment at 2.4 Å resolution. This structure comprises the central helical scaffold (CHS) and C-terminal B30.2 domains and reveals an anti-parallel arrangement of CHS domains placing the B-box domains 170 Å apart from each other. Small-angle X-ray scattering confirmed that the linker between CHS and B30.2 domains is flexible in solution. The crystal structure suggests an interaction between the B30.2 domain and an extended stretch in the CHS domain, which involves residues that are mutated in the inherited disease Familial Mediterranean Fever. Dimerization of B30.2 domains by means of the CHS domain is crucial for TRIM20 to bind pro-IL-1β in vitro. To exemplify how TRIM proteins could be involved in binding higher order oligomers we discuss three possible models for the TRIM5α/HIV-1 capsid interaction assuming different conformations of B30.2 domains.

Published

2015

223. Unusual structural features revealed by the solution NMR structure of the NLRC5 caspase recruitment domain

Author

Simon Jurt, Petrus G. M. Gutte, Oliver Zerbe, Markus G. Grütter, University of Zurich, and Grütter, Markus G

Subjects

10120 Department of Chemistry, Protein Folding, 1303 Biochemistry, Subfamily, Death fold, Plasma protein binding, Biochemistry, Protein Structure, Secondary, Domain (software engineering), Cell Line, DEAD-box RNA Helicases, Mice, NLRC5, 540 Chemistry, 10019 Department of Biochemistry, Animals, Humans, Receptors, Immunologic, Gene, Nuclear Magnetic Resonance, Biomolecular, Caspase, biology, Effector, Chemistry, Intracellular Signaling Peptides and Proteins, Cell biology, Protein Structure, Tertiary, biology.protein, 570 Life sciences, DEAD Box Protein 58

Abstract

The cytosolic nucleotide-binding domain and leucine-rich repeat-containing receptors (NLRs) are key sensors for bacterial and viral invaders and endogenous stress signals. NLRs contain a varying N-terminal effector domain that regulates the downstream signaling events upon its activation and determines the subclass to which a NLR member belongs. NLRC5 contains an unclassified N-terminal effector domain that has been reported to interact downstream with the tandem caspase recruitment domain (CARD) of retinoic acid-inducible gene I (RIG-I). Here we report the solution structure of the N-terminal effector domain of NLRC5 and in vitro interaction experiments with the tandem CARD of RIG-I. The N-terminal effector domain of NLRC5 adopts a six α-helix bundle with a general death fold, though it displays specific structural features that are strikingly different from the CARD. Notably, α-helix 3 is replaced by an ordered loop, and α-helix 1 is devoid of the characteristic interruption. Detailed structural alignments between the N-terminal effector domains of NLRC5 with a representative of each death-fold subfamily showed that NLRC5 fits best to the CARD subfamily and can be called an atypical CARD. Due to the specific structural features, the atypical CARD also displays a different electrostatic surface. Because the shape and charge of the surface is crucial for the establishment of a homotypic CARD-CARD interaction, these specific structural features seem to have a significant effect on the interaction between the atypical CARD of NLRC5 and the tandem RIG-I CARD.

Published

2014

224. Combined inhibition of caspase 3 and caspase 7 by two highly selective DARPins slows down cellular demise

Author

Maria Lukarska, Andreas Flütsch, Markus G. Grütter, Thilo Schroeder, Christophe Briand, Georg J. Hausammann, Christopher Weinert, Rafael Ackermann, University of Zurich, and Grütter, Markus G

Subjects

Models, Molecular, 1303 Biochemistry, Caspase 3, Apoptosis, Plasma protein binding, Biochemistry, Caspase 7, 1307 Cell Biology, HeLa, TNF-Related Apoptosis-Inducing Ligand, Peptide Library, 10019 Department of Biochemistry, 1312 Molecular Biology, Humans, Molecular Biology, Caspase, biology, Nuclear Proteins, Cell Biology, biology.organism_classification, Caspase Inhibitors, Recombinant Proteins, Cell biology, Ankyrin Repeat, Molecular Imaging, DARPin, biology.protein, 570 Life sciences, Ankyrin repeat, HeLa Cells, Protein Binding

Abstract

Caspases play important roles during apoptosis, inflammation and proliferation. The high homology among family members makes selective targeting of individual caspases difficult, which is necessary to precisely define the role of these enzymes. We have selected caspase-7-specific binders from a library of DARPins (designed ankyrin repeat proteins). The DARPins D7.18 and D7.43 bind specifically to procaspase 7 and active caspase 7, but not to other members of the family. Binding of the DARPins does not affect the active enzyme, but interferes with its activation by other caspases. The crystal structure of the caspase 7–D7.18 complex elucidates the high selectivity and the mode of inhibition. Combining these caspase-7-specific DARPins with the previously reported caspase-3-inhibitory DARPin D3.4S76R reduces the activity of caspase 3 and 7 in double-transfected HeLa cells during apoptosis. In addition, these cells showed less susceptibility to TRAIL (tumour-necrosis-factor-related apoptosis-inducing ligand)-induced apoptosis in living cell experiments. D7.18 and D7.43 are therefore novel tools for in vitro studies on procaspase 7 activation as well as for clarifying the role of its activation in different cellular processes. If applied in combination with D3.4S76R, they represent an excellent instrument to increase our understanding of these enzymes during various cellular processes.

Published

2014

225. The Structure of Bradyrhizobium japonicum Transcription Factor FixK2 Unveils Sites of DNA Binding and Oxidation*

Author

Mariette Bonnet, Markus G. Grütter, Christophe Briand, Socorro Mesa, Mareike Kurz, Hauke Hennecke, University of Zurich, and Grütter, Markus G

Subjects

DNA, Bacterial, Models, Molecular, 1303 Biochemistry, Nitrogen, Molecular Sequence Data, Biology, Crystallography, X-Ray, Biochemistry, Protein Structure, Secondary, 1307 Cell Biology, 03 medical and health sciences, chemistry.chemical_compound, Bacterial Proteins, Nitrogen Fixation, 10019 Department of Biochemistry, 1312 Molecular Biology, Protein–DNA interaction, Amino Acid Sequence, Bradyrhizobium, Binding site, Molecular Biology, Peptide sequence, Transcription factor, 030304 developmental biology, 0303 health sciences, Binding Sites, General transcription factor, 030306 microbiology, Cell Biology, Gene Expression Regulation, Bacterial, biology.organism_classification, Oxygen, chemistry, cAMP receptor protein, Protein Structure and Folding, biology.protein, 570 Life sciences, biology, Reactive Oxygen Species, Protein Processing, Post-Translational, DNA, Bradyrhizobium japonicum, Plasmids

Abstract

FixK2 is a regulatory protein that activates a large number of genes for the anoxic and microoxic, endosymbiotic, and nitrogen-fixing life styles of the α-proteobacterium Bradyrhizobium japonicum. FixK2 belongs to the cAMP receptor protein (CRP) superfamily. Although most CRP family members are coregulated by effector molecules, the activity of FixK2 is negatively controlled by oxidation of its single cysteine (Cys-183) located next to the DNA-binding domain and possibly also by proteolysis. Here, we report the three-dimensional x-ray structure of FixK2, a representative of the FixK subgroup of the CRP superfamily. Crystallization succeeded only when (i) an oxidation- and protease-insensitive protein variant (FixK2(C183S)-His6) was used in which Cys-183 was replaced with serine and the C terminus was fused with a hexahistidine tag and (ii) this protein was allowed to form a complex with a 30-mer double-stranded target DNA. The structure of the FixK2-DNA complex was solved at a resolution of 1.77 Å, at which the protein formed a homodimer. The precise protein-DNA contacts were identified, which led to an affirmation of the canonical target sequence, the so-called FixK2 box. The C terminus is surface-exposed, which might explain its sensitivity to specific cleavage and degradation. The oxidation-sensitive Cys-183 is also surface-exposed and in close proximity to DNA. Therefore, we propose a mechanism whereby the oxo acids generated after oxidation of the cysteine thiol cause an electrostatic repulsion, thus preventing specific DNA binding.

Published

2013

226. Chimeric hERG channels containing a tetramerization domain are functional and stable

Author

Georg J. Hausammann, Markus G. Grütter, University of Zurich, and Grütter, Markus G

Subjects

congenital, hereditary, and neonatal diseases and abnormalities, Cytoplasm, ERG1 Potassium Channel, 1303 Biochemistry, Recombinant Fusion Proteins, hERG, Xenopus, Gating, Protein Serine-Threonine Kinases, Biochemistry, Membrane Potentials, Xenopus laevis, 10019 Department of Biochemistry, Animals, Humans, Protein Interaction Domains and Motifs, cardiovascular diseases, Cells, Cultured, Scorpion toxin, Binding Sites, biology, Chemistry, Protein Stability, HEK 293 cells, Cell Membrane, biology.organism_classification, Potassium channel, Ether-A-Go-Go Potassium Channels, Peptide Fragments, Cell biology, Protein Transport, HEK293 Cells, Solubility, Cyclic nucleotide-binding domain, biology.protein, Oocytes, 570 Life sciences, Nucleotides, Cyclic, Protein Multimerization

Abstract

Biochemical and detailed structural information of human ether-a-go-go-related gene (hERG) potassium channels are scarce but are a prerequisite to understand the unwanted interactions of hERG with drugs and the effect of mutations that lead to long QT syndrome. Despite the huge interest in hERG, to our knowledge, procedures that provide a purified, functional, and tetrameric hERG channel are not available. Here, we describe hybrid hERG molecules, termed chimeric hERG channels, in which the N-terminal Per-Arnt-Sim (PAS) domain is deleted and the C-terminal C-linker as well as the cyclic nucleotide binding domain (CNBD) portion is replaced by an artificial tetramerization domain. These chimeric hERG channels can be overexpressed in HEK cells, solubilized in detergent, and purified as tetramers. When expressed in Xenopus laevis oocytes, the chimeric channels exhibit efficient trafficking to the cell surface, whereas a hERG construct lacking the PAS and C-linker/CNBD domains is retained in the cytoplasm. The chimeric hERG channels retain essential hERG functions such as voltage-dependent gating and inhibition by astemizole and the scorpion toxin BeKm-1. The chimeric channels are thus powerful tools for helping to understand the contribution of the cytoplasmic hERG domains to the gating process and are suitable for in vitro biochemical and structural studies.

Published

2013

227. New concepts and aids to facilitate crystallization

Author

Markus G. Grütter, Magdalena A Bukowska, University of Zurich, and Grütter, Markus G

Subjects

Computer science, Protein Conformation, Nanotechnology, Intrinsically disordered proteins, Crystallography, X-Ray, Protein Engineering, Antibodies, law.invention, 1315 Structural Biology, Structural Biology, law, 10019 Department of Biochemistry, 1312 Molecular Biology, Humans, Crystallization, Molecular Biology, biology, Proteins, Protein engineering, Membrane protein, Chaperone (protein), biology.protein, 570 Life sciences, Target protein, Molecular Chaperones

Abstract

Novel tools and technologies are required to obtain structural information of difficult to crystallize complex biological systems such as membrane proteins, multiprotein assemblies, transient conformational states and intrinsically disordered proteins. One promising approach is to select a high affinity and specificity-binding partner (crystallization chaperone), form a complex with the protein of interest and crystallize the complex. Often the chaperone reduces the conformational freedom of the target protein and additionally facilitates the formation of well-ordered crystals. This review provides an update on the recent successes in chaperone-assisted crystallography. We also stress the importance of synergistic approaches involving protein engineering, crystallization chaperones and crystallization additives. Recent examples demonstrate that investment in such approaches can be key to success.

Published

2012

228. NLRP3 tyrosine phosphorylation is controlled by protein tyrosine phosphatase PTPN22.

Author

Spalinger MR, Kasper S, Gottier C, Lang S, Atrott K, Vavricka SR, Scharl S, Gutte PM, Grütter MG, Beer HD, Contassot E, Chan AC, Dai X, Rawlings DJ, Mair F, Becher B, Falk W, Fried M, Rogler G, and Scharl M

Published

2023

229. Design, construction, and characterization of a second-generation DARP in library with reduced hydrophobicity.

Author

Seeger MA, Zbinden R, Flütsch A, Gutte PG, Engeler S, Roschitzki-Voser H, and Grütter MG

Subjects

Carrier Proteins chemistry, Caspase 3 chemistry, Caspase 3 metabolism, Caspase 7 chemistry, Caspase 7 metabolism, Entropy, Humans, Models, Molecular, Peptides metabolism, Protein Binding, Surface Properties, Tryptophan chemistry, Tyrosine chemistry, Ankyrin Repeat, Hydrophobic and Hydrophilic Interactions, Peptide Library, Peptides chemical synthesis, Peptides chemistry

Abstract

Designed ankyrin repeat proteins (DARPins) are well-established binding molecules based on a highly stable nonantibody scaffold. Building on 13 crystal structures of DARPin-target complexes and stability measurements of DARPin mutants, we have generated a new DARPin library containing an extended randomized surface. To counteract the enrichment of unspecific hydrophobic binders during selections against difficult targets containing hydrophobic surfaces such as membrane proteins, the frequency of apolar residues at diversified positions was drastically reduced and substituted by an increased number of tyrosines. Ribosome display selections against two human caspases and membrane transporter AcrB yielded highly enriched pools of unique and strong DARPin binders which were mainly monomeric. We noted a prominent enrichment of tryptophan residues during binder selections. A crystal structure of a representative of this library in complex with caspase-7 visualizes the key roles of both tryptophans and tyrosines in providing target contacts. These aromatic and polar side chains thus substitute the apolar residues valine, leucine, isoleucine, methionine, and phenylalanine of the original DARPins. Our work describes biophysical and structural analyses required to extend existing binder scaffolds and simplifies an existing protocol for the assembly of highly diverse synthetic binder libraries., (© 2013 The Protein Society.)

Published

2013

230. New concepts and aids to facilitate crystallization.

Author

Bukowska MA and Grütter MG

Subjects

Antibodies chemistry, Antibodies metabolism, Crystallography, X-Ray, Humans, Molecular Chaperones chemistry, Molecular Chaperones metabolism, Protein Conformation, Proteins metabolism, Crystallization methods, Protein Engineering methods, Proteins chemistry

Abstract

Novel tools and technologies are required to obtain structural information of difficult to crystallize complex biological systems such as membrane proteins, multiprotein assemblies, transient conformational states and intrinsically disordered proteins. One promising approach is to select a high affinity and specificity-binding partner (crystallization chaperone), form a complex with the protein of interest and crystallize the complex. Often the chaperone reduces the conformational freedom of the target protein and additionally facilitates the formation of well-ordered crystals. This review provides an update on the recent successes in chaperone-assisted crystallography. We also stress the importance of synergistic approaches involving protein engineering, crystallization chaperones and crystallization additives. Recent examples demonstrate that investment in such approaches can be key to success., (Copyright © 2013. Published by Elsevier Ltd.)

Published

2013

231. Structure-based optimization of designed Armadillo-repeat proteins.

Author

Madhurantakam C, Varadamsetty G, Grütter MG, Plückthun A, and Mittl PR

Subjects

Amino Acid Sequence, Armadillo Domain Proteins metabolism, Binding Sites, Cloning, Molecular, Crystallography, X-Ray, Gene Expression, Models, Molecular, Molecular Sequence Data, Peptides metabolism, Point Mutation, Protein Engineering, Protein Structure, Secondary, Protein Structure, Tertiary, Saccharomyces cerevisiae metabolism, Saccharomyces cerevisiae Proteins metabolism, Thermodynamics, Armadillo Domain Proteins chemistry, Armadillo Domain Proteins genetics, Saccharomyces cerevisiae chemistry, Saccharomyces cerevisiae genetics, Saccharomyces cerevisiae Proteins chemistry, Saccharomyces cerevisiae Proteins genetics

Abstract

The armadillo domain is a right-handed super-helix of repeating units composed of three α-helices each. Armadillo repeat proteins (ArmRPs) are frequently involved in protein-protein interactions, and because of their modular recognition of extended peptide regions they can serve as templates for the design of artificial peptide binding scaffolds. On the basis of sequential and structural analyses, different consensus-designed ArmRPs were synthesized and show high thermodynamic stabilities, compared to naturally occurring ArmRPs. We determined the crystal structures of four full-consensus ArmRPs with three or four identical internal repeats and two different designs for the N- and C-caps. The crystal structures were refined at resolutions ranging from 1.80 to 2.50 Å for the above mentioned designs. A redesign of our initial caps was required to obtain well diffracting crystals. However, the structures with the redesigned caps caused domain swapping events between the N-caps. To prevent this domain swap, 9 and 6 point mutations were introduced in the N- and C-caps, respectively. Structural and biophysical analysis showed that this subsequent redesign of the N-cap prevented domain swapping and improved the thermodynamic stability of the proteins. We systematically investigated the best cap combinations. We conclude that designed ArmRPs with optimized caps are intrinsically stable and well-expressed monomeric proteins and that the high-resolution structures provide excellent structural templates for the continuation of the design of sequence-specific modular peptide recognition units based on armadillo repeats., (Copyright © 2012 The Protein Society.)

Published

2012

232. TRIM5 structure, HIV-1 capsid recognition, and innate immune signaling.

Author

Grütter MG and Luban J

Subjects

Animals, Antiviral Restriction Factors, Carrier Proteins genetics, Carrier Proteins immunology, HIV Infections genetics, HIV Infections virology, HIV-1 genetics, Humans, Protein Conformation, Signal Transduction, Tripartite Motif Proteins, Ubiquitin-Protein Ligases, Capsid immunology, Carrier Proteins chemistry, HIV Infections immunology, HIV-1 immunology, Immunity, Innate

Abstract

TRIM5 is a restriction factor that blocks retrovirus infection soon after the virion core enters the cell cytoplasm. Restriction activity is targeted to the virion core via recognition of the capsid protein lattice that encases the viral genomic RNA. In common with all of the many TRIM family members, TRIM5 has RING, B-box, and coiled-coil domains. As an E3 ubiquitin ligase TRIM5 cooperates with the heterodimeric E2, UBC13/UEV1A, to activate the TAK1 (MAP3K7) kinase, NF-κB and AP-1 signaling, and the transcription of inflammatory cytokines and chemokines. TAK1, UBC13, and UEV1A all contribute to TRIM5-mediated retrovirus restriction activity. Interaction of the carboxy-terminal PRYSPRY or cyclophilin domains of TRIM5 with the retroviral capsid lattice stimulates the formation of a complementary lattice by TRIM5, with greatly increased TRIM5 E3 activity, and host cell signal transduction. Structural and biochemical studies on TRIM5 have opened a much needed window on how the innate immune system detects the distinct molecular features of HIV-1 and other retroviruses., (Copyright © 2012 Elsevier B.V. All rights reserved.)

Published

2012

233. Chaperone-assisted crystallography with DARPins.

Author

Sennhauser G and Grütter MG

Subjects

Amino Acid Sequence, Antibodies pharmacology, Carrier Proteins chemistry, Carrier Proteins metabolism, Cell Cycle Proteins chemistry, Crystallography, X-Ray methods, Kanamycin Kinase chemistry, Kanamycin Kinase metabolism, Maltose-Binding Proteins, Models, Molecular, Molecular Chaperones chemistry, Molecular Sequence Data, Multiprotein Complexes chemistry, Protein Binding, Protein Serine-Threonine Kinases chemistry, Proto-Oncogene Proteins chemistry, Polo-Like Kinase 1, Ankyrin Repeat physiology, Molecular Chaperones metabolism

Abstract

The structure of proteins that are difficult to crystallize can often be solved by forming a noncovalent complex with a helper protein--a crystallization "chaperone." Although several such applications have been described to date, their handling usually is still very laborious. A valuable addition to the present repertoire of binding proteins is the recently developed designed ankyrin repeat protein (DARPin) technology. DARPins are built based on the natural ankyrin repeat protein fold with randomized surface residue positions allowing specific binding to virtually any target protein. The broad potential of these binding proteins for X-ray crystallography is illustrated by five cocrystal structures that have been determined recently comprising target proteins from distinct families, namely a sugar binding protein, two kinases, a caspase, and a membrane protein. This article reviews the opportunities of this technology for structural biology and the structural aspects of the DARPin-protein complexes.

Published

2008

234. Opportunities for structure-based design of protease-directed drugs.

Author

Mittl PR and Grütter MG

Subjects

Aspartic Acid Endopeptidases chemistry, Aspartic Acid Endopeptidases metabolism, Catalytic Domain, Cysteine Endopeptidases chemistry, Cysteine Endopeptidases metabolism, Metalloproteases chemistry, Metalloproteases metabolism, Models, Molecular, Protein Conformation, Protein Processing, Post-Translational, Serine Endopeptidases chemistry, Serine Endopeptidases metabolism, Drug Design, Peptide Hydrolases chemistry, Peptide Hydrolases metabolism

Abstract

As a result of the recent enormous technological progress, experimental structure determination has become an integral part of the development of drugs against disease-related target proteins. The post-translational modification of proteins is an important regulatory process in living organisms; one such example is lytic processing by peptidases. Many different peptidases represent disease targets and are being used in structure-based drug design approaches. The development of drugs such as aliskiren and tipranavir, which inhibit renin and HIV protease, respectively, testifies to the success of this approach.

Published

2006

235. Structure-activity studies in a family of beta-hairpin protein epitope mimetic inhibitors of the p53-HDM2 protein-protein interaction.

Author

Fasan R, Dias RL, Moehle K, Zerbe O, Obrecht D, Mittl PR, Grütter MG, and Robinson JA

Subjects

Amino Acid Sequence, Crystallization, Models, Molecular, Nuclear Magnetic Resonance, Biomolecular, Protein Binding, Protein Conformation, Structure-Activity Relationship, Epitopes chemistry, Epitopes immunology, Molecular Mimicry, Proto-Oncogene Proteins c-mdm2 chemistry, Tumor Suppressor Protein p53 chemistry

Abstract

Inhibitors of the interaction between the p53 tumor-suppressor protein and its natural human inhibitor HDM2 are attractive as potential anticancer agents. In earlier work we explored designing beta-hairpin peptidomimetics of the alpha-helical epitope on p53 that would bind tightly to the p53-binding site on HDM2. The beta-hairpin is used as a scaffold to display energetically hot residues in an optimal array for interaction with HDM2. The initial lead beta-hairpin mimetic, with a weak inhibitory activity (IC(50)=125 microM), was optimized to afford cyclo-(L-Pro-Phe-Glu-6ClTrp-Leu-Asp-Trp-Glu-Phe-D-Pro) (where 6ClTrp=L-6-chlorotryptophan), which has an affinity almost 1,000 times higher (IC(50)=140 nM). In this work, insights into the origins of this affinity maturation based on structure-activity studies and an X-ray crystal structure of the inhibitor/HDM2(residues 17-125) complex at 1.4 A resolution are described. The crystal structure confirms the beta-hairpin conformation of the bound ligand, and also reveals that a significant component of the affinity increase arises through new aromatic/aromatic stacking interactions between side chains around the hairpin and groups on the surface of HDM2.

Published

2006

236. Fire and death: the pyrin domain joins the death-domain superfamily.

Author

Kohl A and Grütter MG

Subjects

Cytoskeletal Proteins metabolism, Cytoskeletal Proteins physiology, Inflammation metabolism, Multiprotein Complexes, Protein Binding, Pyrin, Apoptosis physiology

Abstract

Apoptosis and inflammation are important cellular processes that are highly regulated through specific protein-protein interactions (PPI). Proteins involved in these signaling cascades often carry PPI domains that belong to the death-domain superfamily. This includes the structurally well-characterized Death Domain (DD), the Death Effector Domain (DED) and the Caspase Recruitment Domain (CARD) subfamilies. Recently, a fourth member of the DD superfamily was identified, the Pyrin Domain (PYD). Based on sequence alignments, homology to other domains occurring in death-signalling pathways, and secondary-structure prediction, the PYD was predicted to have an overall fold similar to other DD superfamily members. Just recently, NMR structures of two PYDs have been determined. The PYD structures not only revealed the DD superfamily fold as previously predicted, but also distinct features that are characteristic exclusively for this subfamily. This review summarizes recent findings and developments regarding structural aspects of the DD superfamily, with a special emphasis on the PPIs of the DD superfamily.

Published

2004

237. The crystal structure of Helicobacter cysteine-rich protein C at 2.0 A resolution: similar peptide-binding sites in TPR and SEL1-like repeat proteins.

Author

Lüthy L, Grütter MG, and Mittl PR

Subjects

Amino Acid Sequence, Binding Sites, Cloning, Molecular, Conserved Sequence, Disulfides chemistry, HSP70 Heat-Shock Proteins chemistry, Models, Molecular, Molecular Sequence Data, Peptides, Protein Binding, Protein C genetics, Protein C isolation & purification, Protein C metabolism, Protein Denaturation, Protein Folding, Protein Structure, Secondary, Recombinant Proteins chemistry, Recombinant Proteins isolation & purification, Recombinant Proteins metabolism, Sequence Homology, Amino Acid, Spectrum Analysis, Raman, Temperature, Thermodynamics, Water chemistry, Crystallography, X-Ray, Cysteine analysis, Helicobacter pylori chemistry, Protein C chemistry

Abstract

Helicobacter pylori is a Gram-negative human pathogen that infects the gastric mucosa and causes an inflammatory process leading to gastritis, ulceration and cancer. Bacterial cell-surface and secreted proteins often play an important role in pathogen-host interactions and are thought to be selective mediators for the pathology of the infection. The Helicobacter cysteine-rich proteins (Hcp) represent a large family of secreted proteins that seem to be specific for microorganisms from the epsilon-subfamily of proteobacteria. Although significantly elevated levels of anti-Hcp antibodies were observed in many patients infected with H.pylori, details on the biological functions of Hcp proteins are sparse. Hcps belong to a large family of Sel1-like multi-repeat proteins. The crystal structure of HcpC was refined at 2.0 A resolution and revealed a super-helical topology composed of seven disulfide bridged alpha/alpha-repeats, an N-terminal capping helix and an extended C-terminal coil consisting of alternating hydrophobic and hydrophilic residues. In the crystal packing, the C-terminal coil interacts with the concave surface of a symmetry-related HcpC super-helix. A hydrophobic pocket and a cluster of negatively charged residues recognize the side-chains of Val290 and Lys287 from the C-terminal coil, respectively. The peptide nitrogen atom of His291 forms a short hydrogen bond with the side-chain of Asn66. The interactions seen in this crystal contact are strikingly similar to the peptide-binding modes of the Hsp70/Hsp90 organizing protein and the PEX5 receptor. The conservation of the peptide-binding mode suggests that HcpC might recognize its binding partner in a similar way.

Published

2004

238. Crystal structure and functional analysis of Escherichia coli glutamate decarboxylase.

Author

Capitani G, De Biase D, Aurizi C, Gut H, Bossa F, and Grütter MG

Subjects

Binding Sites, Crystallography, X-Ray, Dimerization, Escherichia coli genetics, Escherichia coli growth & development, Glutamate Decarboxylase genetics, Hydrogen-Ion Concentration, Models, Molecular, Molecular Weight, Mutagenesis, Site-Directed, Point Mutation, Protein Conformation, Protein Structure, Secondary, Protein Structure, Tertiary, Repetitive Sequences, Amino Acid, Sodium Acetate metabolism, Escherichia coli enzymology, Glutamate Decarboxylase chemistry, Glutamate Decarboxylase metabolism

Abstract

Glutamate decarboxylase is a vitamin B6-dependent enzyme, which catalyses the decarboxylation of glutamate to gamma-aminobutyrate. In Escherichia coli, expression of glutamate decarboxylase (GadB), a 330 kDa hexamer, is induced to maintain the physiological pH under acidic conditions, like those of the passage through the stomach en route to the intestine. GadB, together with the antiporter GadC, constitutes the gad acid resistance system, which confers the ability for bacterial survival for at least 2 h in a strongly acidic environment. GadB undergoes a pH-dependent conformational change and exhibits an activity optimum at low pH. We determined the crystal structures of GadB at acidic and neutral pH. They reveal the molecular details of the conformational change and the structural basis for the acidic pH optimum. We demonstrate that the enzyme is localized exclusively in the cytoplasm at neutral pH, but is recruited to the membrane when the pH falls. We show by structure-based site-directed mutagenesis that the triple helix bundle formed by the N-termini of the protein at acidic pH is the major determinant for this behaviour.

Published

2003

239. Apple 1-aminocyclopropane-1-carboxylate synthase in complex with the inhibitor L-aminoethoxyvinylglycine. Evidence for a ketimine intermediate.

Author

Capitani G, McCarthy DL, Gut H, Grütter MG, and Kirsch JF

Subjects

Biochemical Phenomena, Biochemistry, Crystallography, X-Ray, Electrons, Kinetics, Models, Chemical, Models, Molecular, Recombinant Proteins chemistry, Spectrophotometry, Time Factors, Amines chemistry, Glycine analogs & derivatives, Glycine chemistry, Ketones chemistry, Lyases chemistry, Malus enzymology

Abstract

The 1.6-A crystal structure of the covalent ketimine complex of apple 1-aminocyclopropane-1-carboxylate (ACC) synthase with the potent inhibitor l-aminoethoxyvinylglycine (AVG) is described. ACC synthase catalyzes the committed step in the biosynthesis of ethylene, a plant hormone that is responsible for the initiation of fruit ripening and for regulating many other developmental processes. AVG is widely used in plant physiology studies to inhibit the activity of ACC synthase. The structural assignment is supported by the fact that the complex absorbs maximally at 341 nm. These results are not in accord with the recently reported crystal structure of the tomato ACC synthase AVG complex, which claims that the inhibitor only associates noncovalently. The rate constant for the association of AVG with apple ACC synthase was determined by stopped-flow spectrophotometry (2.1 x 10(5) m(-1) s(-1)) and by the rate of loss of enzyme activity (1.1 x 10(5) m(-1) s(-1)). The dissociation rate constant determined by activity recovery is 2.4 x 10(-6) s(-1). Thus, the calculated K(d) value is 10-20 pm.

Published

2002

240. Structure and zymogen activation of caspases.

Author

Donepudi M and Grütter MG

Subjects

Caspases chemistry, Enzyme Activation, Models, Molecular, Protein Conformation, Substrate Specificity, Caspases metabolism, Enzyme Precursors metabolism

Abstract

Apoptosis is primarily executed by active caspases, which are derived from the inactive zymogens. Structural and biochemical studies of caspases-1, -3, -7, -8 and -9 have greatly enhanced our understanding of the structure, function, and specificity of the active form of these enzymes. Only recently, the structures of procaspase-7 and biochemical studies of procaspase-9 and -8 have provided insight into the process of procaspase activation. The mechanism of zymogen activation requires limited proteolysis as for many other proteases. In addition, self-activation through oligomerization has been demonstrated for the initiator caspases-8, -9 and -10. These studies provide a structural mechanism for caspase activation, substrate/inhibitor binding, and contribute to the understanding of the biological role of caspases in the processes of apoptosis., (Copyright 2002 Elsevier Science B.V.)

Published

2002

241. The long form of FLIP is an activator of caspase-8 at the Fas death-inducing signaling complex.

Author

Micheau O, Thome M, Schneider P, Holler N, Tschopp J, Nicholson DW, Briand C, and Grütter MG

Subjects

Amino Acid Sequence, Binding Sites, CASP8 and FADD-Like Apoptosis Regulating Protein, Carrier Proteins chemistry, Carrier Proteins genetics, Caspase 3, Caspase 8, Caspase 9, Caspase Inhibitors, Caspases chemistry, Cell Line, Cell Size, Dimerization, Enzyme Activation, Enzyme Inhibitors chemistry, Fas Ligand Protein, Humans, Ligands, Macromolecular Substances, Membrane Glycoproteins genetics, Membrane Glycoproteins metabolism, Models, Molecular, Molecular Sequence Data, Protein Structure, Tertiary, Sequence Alignment, Apoptosis physiology, Carrier Proteins metabolism, Caspases metabolism, Enzyme Inhibitors metabolism, Intracellular Signaling Peptides and Proteins, Signal Transduction physiology, fas Receptor metabolism

Abstract

Death receptors, such as Fas and tumor necrosis factor-related apoptosis-inducing ligand receptors, recruit Fas-associated death domain and pro-caspase-8 homodimers, which are then autoproteolytically activated. Active caspase-8 is released into the cytoplasm, where it cleaves various proteins including pro-caspase-3, resulting in apoptosis. The cellular Fas-associated death domain-like interleukin-1-beta-converting enzyme-inhibitory protein long form (FLIP(L)), a structural homologue of caspase-8 lacking caspase activity because of several mutations in the active site, is a potent inhibitor of death receptor-induced apoptosis. FLIP(L) is proposed to block caspase-8 activity by forming a proteolytically inactive heterodimer with caspase-8. In contrast, we propose that FLIP(L)-bound caspase-8 is an active protease. Upon heterocomplex formation, a limited caspase-8 autoprocessing occurs resulting in the generation of the p43/41 and the p12 subunits. This partially processed form but also the non-cleaved FLIP(L)-caspase-8 heterocomplex are proteolytically active because they both bind synthetic substrates efficiently. Moreover, FLIP(L) expression favors receptor-interacting kinase (RIP) processing within the Fas-signaling complex. We propose that FLIP(L) inhibits caspase-8 release-dependent pro-apoptotic signals, whereas the single, membrane-restricted active site of the FLIP(L)-caspase-8 heterocomplex is proteolytically active and acts on local substrates such as RIP.

Published

2002