ZIB

11

Digitale Medien

Genetic analysis of the molecular basis for β-adrenergic receptor subtype specificity (1989)

Dixon, Richard A. F. ; Hill, Wendy S. ; Candelore, Mari R. ; [weitere]

New York, NY : Wiley-Blackwell

Proteins: Structure, Function, and Genetics 6 (1989), S. 267-274

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ISSN: 0887-3585

Schlagwort(e): β-adrenergic recepor ; chimeric proteins ; receptor subtypes ; ligand binding ; protein structure-function ; Chemistry ; Biochemistry and Biotechnology

Quelle: Wiley InterScience Backfile Collection 1832-2000

Thema: Medizin

Notizen: Pharmacological analysis of ligand binding to the β-adrenergic receptor (βAR) has revealed the existence of two distinct receptor subtypes (β1 and β2) which are the products of different genes. The predicted amino acid sequence of the β1 and β2 receptors differ by 48%. To identify the regions of the proteins responsible for determining receptor subtype, chimeras were constructed from domains of the human β1 and hamster β2 receptors. Analyses of the ligand-binding characteristics of these hybrid receptors revealed that residues in the middle portion of the βAR sequence, particularly around transmembrane regions 4 and 5, contribute to the subtype specific binding of agonists. Smaller molecular replacement of regions of the hamster β2AR with the analogous regions from the avian β1AR, however, failed to identify any single residue substitution capable of altering the subtype specificity of the receptor. These data indicate that, whereas sequences around transmembrane regions 4 and 5 may contribute to conformations which influence the ligand-binding properties of the receptor, the subtype-specific differences in amine-substituted agonist binding cannot be attributed to a single molecular interaction between the ligand and any amino acid residue which is divergent between the β1 and β2 receptors.

Zusätzliches Material: 4 Ill.

Materialart: Digitale Medien

URL: http://dx.doi.org/10.1002/prot.340060309

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12

Digitale Medien

Constructing amino acid residue substitution classes maximally indicative of local protein structure (1996)

Thompson, Michael J. ; Goldstein, Richard A.

New York, NY : Wiley-Blackwell

Proteins: Structure, Function, and Genetics 25 (1996), S. 28-37

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ISSN: 0887-3585

Schlagwort(e): protein evolution ; structure prediction ; information theory ; amino acid substitution ; multiple sequence alignment ; Chemistry ; Biochemistry and Biotechnology

Quelle: Wiley InterScience Backfile Collection 1832-2000

Thema: Medizin

Notizen: Using an information theoretic formalism, we optimize classes of amino acid substitution to be maximally indicative of local protein structure. Our statistically-derived classes are loosely identifiable with the heuristic constructions found in previously published work. However, while these other methods provide a more rigid idealization of physicochemically constrained residue substitution, our classes provide substantially more structural information with many fewer parameters. Moreover, these substitution classes are consistent with the paradigmatic view of the sequence-to-structure relationship in globular proteins which holds that the three-dimensional architecture is predominantly determined by the arrangement of hydrophobic and polar side chains with weak constraints on the actual amino acid identities. More specific constraints are imposed on the placement of prolines, glycines, and the charged residues. These substitution classes have been used in highly accurate predictions of residue solvent accessibility. They could also be used in the identification of homologous proteins, the construction and refinement of multiple sequence alignments, and as a means of condensing and codifying the information in multiple sequence alignments for secondary structure prediction and tertiary fold recognition. © 1996 Wiley-Liss, Inc.

Zusätzliches Material: 3 Ill.

Materialart: Digitale Medien

URL: http://dx.doi.org/10.1002/prot.3

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13

Digitale Medien

Mutation matrices and physical-chemical properties: Correlations and implications (1997)

Koshi, Jeffrey M. ; Goldstein, Richard A.

New York, NY : Wiley-Blackwell

Proteins: Structure, Function, and Genetics 27 (1997), S. 336-344

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ISSN: 0887-3585

Schlagwort(e): hydrophobicity ; molecular evolution ; local propensities ; reverse hydrophobic effect ; protein stability ; Chemistry ; Biochemistry and Biotechnology

Quelle: Wiley InterScience Backfile Collection 1832-2000

Thema: Medizin

Notizen: To investigate how the properties of individual amino acids result in proteins with particular structures and functions, we have examined the correlations between previously derived structure-dependent mutation rates and changes in various physical-chemical properties of the amino acids such as volume, charge, α-helical and β-sheet propensity, and hydrophobicity. In most cases we found the ΔG of transfer from octanol to water to be the best model for evolutionary constraints, in contrast to the much weaker correlation with the ΔG of transfer from cyclohexane to water, a property found to be highly correlated to changes in stability in site-directed mutagenesis studies. This suggests that natural evolution may follow different rules than those suggested by results obtained in the laboratory. A high degree of conservation of a surface residue's relative hydrophobicity was also observed, a fact that cannot be explained by constraints on protein stability but that may reflect the consequences of the reverse-hydrophobic effect. Local propensity, especially α-helical propensity, is rather poorly conserved during evolution, indicating that non-local interactions dominate protein structure formation. We found that changes in volume were important in specific cases, most significantly in transitions among the hydrophobic residues in buried locations. To demonstrate how these techniques could be used to understand particular protein families, we derived and analyzed mutation matrices for the hypervariable and framework regions of antibody light chain V regions. We found a surprisingly high conservation of hydrophobicity in the hypervariable region, possibly indicating an important role for hydrophobicity in antigen recognition. Proteins 27:336-344, 1997. © 1997 Wiley-Liss, Inc.

Zusätzliches Material: 1 Ill.

Materialart: Digitale Medien

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14

Digitale Medien

Rapid identification of drug metabolites with tandem mass spectrometry (1988)

Lee, Mike S. ; Yost, Richard A.

Chichester : Wiley-Blackwell

Biological Mass Spectrometry 15 (1988), S. 193-204

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ISSN: 0887-6134

Schlagwort(e): Chemistry ; Analytical Chemistry and Spectroscopy

Quelle: Wiley InterScience Backfile Collection 1832-2000

Thema: Chemie und Pharmazie

Notizen: A method which involves the use of tandem mass spectrometry (MS/MS) for the identification of drug metabolites has been demonstrated with a triple quadrupole mass spectrometer. The method is based on the fact that metabolites usually retain various substructures of the original drug molecule. MS/MS is capable of rapidly identifying molecules with characteristic substructures without prior separation. It is shown that this method makes it possible to postulate possible drug metabolite structures rapidly and systematically without the use of standards. The MS/MS method, as it was applied to the identification of the metabolites of a new antiepileptic drug, zonisamide, is discussed. In this case it was possible to identify isomeric metabolites due to their differences in vaporization times off the probe and their different daughter spectra. The complementary uses of the neutral loss and parent scans for the determination of the site of metabolism is demonstrated. A new figure of merit, the limit of identification, is introduced. The amount of the epoxide metabolite of carbamazepine necessary for its reliable identification in urine was shown to be 0.4 ng/μl. The application of various techniques to confirm preliminary findings with this MS/MS method are described.

Zusätzliches Material: 12 Ill.

Materialart: Digitale Medien

URL: http://dx.doi.org/10.1002/bms.1200150403

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15

Digitale Medien

Evolution of model proteins on a foldability landscape (1997)

Govindarajan, Sridhar ; Goldstein, Richard A.

New York, NY : Wiley-Blackwell

Proteins: Structure, Function, and Genetics 29 (1997), S. 461-466

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ISSN: 0887-3585

Schlagwort(e): protein folding ; molecular evolution ; lattice models ; fitness landscapes ; neutral networks ; spin-glass theory ; Chemistry ; Biochemistry and Biotechnology

Quelle: Wiley InterScience Backfile Collection 1832-2000

Thema: Medizin

Notizen: We model the evolution of simple lattice proteins as a random walk in a fitness landscape, where the fitness represents the ability of the protein to fold. At higher selective pressure, the evolutionary trajectories are confined to neutral networks where the native structure is conserved and the dynamics are non self-averaging and nonexponential. The optimizability of the corresponding native structure has a strong effect on the size of these neutral networks and thus on the nature of the evolutionary process. Proteins 29:461-466, 1997. © 1997 Wiley-Liss, Inc.

Zusätzliches Material: 4 Ill.

Materialart: Digitale Medien

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16

Digitale Medien

Poly(p-Phenylenebenzobisoxazole) fiber with polyphenylene sulfide pendent groups (1995)

So, Ying-Hung ; Bell, Bruce ; Heeschen, Jerry P. ; [weitere]

Bognor Regis [u.a.] : Wiley-Blackwell

Journal of Polymer Science Part A: Polymer Chemistry 33 (1995), S. 159-164

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ISSN: 0887-624X

Schlagwort(e): poly(p-phenylenebenzobisoxazole) ; polyphenylene sulfide ; pendent group ; crosslinking ; heat treatment ; compressive strength ; Chemistry ; Polymer and Materials Science

Quelle: Wiley InterScience Backfile Collection 1832-2000

Thema: Chemie und Pharmazie

Notizen: Poly(p-phenylenebenzobisoxazole) (PBO) fiber with polyphenylene sulfide (PPS) pendent groups was made to improve PBO fiber compressive strength by crosslinking. PPS moieties allowed the polymeric network to crosslink at heat-treatment temperatures at which PBO does not thermally degrade. PBO-PPS fiber heat-treated for 30 s at 600°C did not dissolve or break up in methanesulfonic acid. Compressive strength of crosslinked fiber was about 20% better than that of unmodified PBO fiber. In another experiment, 10 mol % of 2,5-diphenylsulfideterephthalic acid was incorporated into PBO fiber. The side chain of one phenyl sulfide unit was too short to enhance crosslinking, and the fiber had about the same compressive strength as unmodified PBO fiber. © 1995 John Wiley & Sons, Inc.

Zusätzliches Material: 3 Ill.

Materialart: Digitale Medien

URL: http://dx.doi.org/10.1002/pola.1995.080330118

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17

Digitale Medien

Retardation of dibenzo polyether-formaldehyde resin formation by alkali-metal cations (1995)

Zhao, Qiang ; Bartsch, Richard A.

Bognor Regis [u.a.] : Wiley-Blackwell

Journal of Polymer Science Part A: Polymer Chemistry 33 (1995), S. 2267-2274

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ISSN: 0887-624X

Schlagwort(e): dibenzo polyether ; formaldehyde condensation polymerization ; alkali-metal cation sorption ; template polymerization ; Chemistry ; Polymer and Materials Science

Quelle: Wiley InterScience Backfile Collection 1832-2000

Thema: Chemie und Pharmazie

Notizen: Macrocyclic polyethers are well-known complexing agents for alkali-metal and alkaline earth-metal cations. The influence of alkali-metal cations upon the polycondensation rate of acyclic and cyclic dibenzo polyethers with formaldehyde in formic acid and alkali-metal cation sorption by some of the resultant resins have been investigated. For certain dibenzo polyether and alkali-metal cation combinations, polymer formation is markedly reduced. The alkali-metal cation that provides the best fit for the macrocyclic polyether cavity produces the greatest retardation of polymer formation. It is proposed that metal ion complexation renders the dibenzo polyether monomer inert to polymerization under the reaction conditions. No template effect for alkali-metal cation sorption by dibenzo polyether carboxylic acid resins was observed. © 1995 John Wiley & Sons, Inc.

Zusätzliches Material: 6 Ill.

Materialart: Digitale Medien

URL: http://dx.doi.org/10.1002/pola.1995.080331321

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18

Digitale Medien

The high-resolution crystal structure of a 24-kDa gyrase B fragment from E. coli complexed with one of the most potent coumarin inhibitors, clorobiocin (1997)

Tsai, Francis T.F. ; Singh, Onkar M.P. ; Skarzynski, Tadeusz ; [weitere]

New York, NY : Wiley-Blackwell

Proteins: Structure, Function, and Genetics 28 (1997), S. 41-52

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ISSN: 0887-3585

Schlagwort(e): type II topoisomerase ; gyrase ; coumarin inhibitor ; clorobiocin ; Chemistry ; Biochemistry and Biotechnology

Quelle: Wiley InterScience Backfile Collection 1832-2000

Thema: Medizin

Notizen: Coumarin antibiotics, such as clorobiocin, novobiocin, and coumermycin A1, inhibit the supercoiling activity of gyrase by binding to the gyrase B (GyrB) subunit. Previous crystallographic studies of a 24-kDa N-terminal domain of GyrB from E. coli complexed with novobiocin and a cyclothialidine analogue have shown that both ligands act by binding at the ATP-binding site. Clorobiocin is a natural antibiotic isolated from several Streptomyces strains and differs from novobiocin in that the methyl group at the 8 position in the coumarin ring of novobiocin is replaced by a chlorine atom, and the carbamoyl at the 3′ position of the noviose sugar is substituted by a 5-methyl-2-pyrrolylcarbonyl group. To understand the difference in affinity, in order that this information might be exploited in rational drug design, the crystal structure of the 24-kDa GyrB fragment in complex with clorobiocin was determined to high resolution. This structure was determined independently in two laboratories, which allowed the validation of equivalent interpretations. The clorobiocin complex structure is compared with the crystal structures of gyrase complexes with novobiocin and 5′-adenylyl-β,γ-imidodiphosphate, and with information on the bound conformation of novobiocin in the p24-novobiocin complex obtained by heteronuclear isotope-filtered NMR experiments in solution. Moreover, to understand the differences in energetics of binding of clorobiocin and novobiocin to the protein, the results from isothermal titration calorimetry are also presented. © 1997 Wiley-Liss Inc.

Zusätzliches Material: 8 Ill.

Materialart: Digitale Medien

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19

Digitale Medien

Excited states of CF4 plasma for polymerization of TMPTA monomer (1992)

Bretagne, J. ; Epaillard, F. ; Richard, A.

Bognor Regis [u.a.] : Wiley-Blackwell

Journal of Polymer Science Part A: Polymer Chemistry 30 (1992), S. 323-328

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ISSN: 0887-624X

Schlagwort(e): CF4 plasma ; trimethylolpropane triacrylate ; excited states ; plasma induced polymerization ; Chemistry ; Polymer and Materials Science

Quelle: Wiley InterScience Backfile Collection 1832-2000

Thema: Chemie und Pharmazie

Notizen: The F and CF2-CF2+ excited states have been detected by emission spectroscopy in CF4RF plasmas used for TMPTA polymerization. These excited states are related through electron collision to F and CF2 ground states. The temporal variation of the F and CF2-CF2+ radiative states near the substrate reveals that the F atoms disappear first by incorporation in the monomer during the polymerization phase and, then, by a third body recombination process enhanced by the polymer surface. The CF2-CF2+ radiative states are varying as the inverse of the F states indicating a strong destruction mechanism of CF2 radicals by F atoms.

Zusätzliches Material: 6 Ill.

Materialart: Digitale Medien

URL: http://dx.doi.org/10.1002/pola.1992.080300217

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20

Digitale Medien

Size determination of multienzyme complexes using two-dimensional agarose gel electrophoresis (1989)

Easom, Richard A. ; Debuysere, Michael S. ; Olson, Merle S. ; [weitere]

New York, NY : Wiley-Blackwell

Proteins: Structure, Function, and Genetics 5 (1989), S. 224-232

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ISSN: 0887-3585

Schlagwort(e): effective pore's radius ; α-ketoglutarate dehydrogenase complex ; branched chain α-keto acid dehydrogenase complex ; electron microscopy ; multienzyme complex ; two-dimensional ; electrophoresis ; multienzyme complex ; aggregation of Pyruvate dehydrogenase complex ; Chemistry ; Biochemistry and Biotechnology

Quelle: Wiley InterScience Backfile Collection 1832-2000

Thema: Medizin

Notizen: In the studies of the size and structure of multienzyme complexes, a procedure complementary to electron microscopy for determining the molecular dimensions of hydrated multisubunit complexes is needed. For some applications this procedure must be capable of detecting aggregation of complexes and must be applicable to impure preparations. In the present study, a procedure of two-dimensional agarose gel electrophoresis (2d-AGE) (Serwer, P. et al. Anal. Biochem. 152: 339-345, 1986) was modified and employed to provide accurate sizemeasurements of several classical multienzyme complexes. To improve band clarity and to achieve required gel pore sizes, a hydroxyethylated agarose was used. The effective pore's radius (PE) as a function of gel concentration was determined for this agarose inthe range of PE value needed for multienzyme complexes (effective radius, R = 10-30 nm). Appropriate conditions wereestablished to measure R value ± 1% of the pyruvate (PDC), α-ketoglutarate (α-KGDC), and the branched chain α-keto acid (BCDC) dehydrogenase multienzyme complexes; the accuracy of R was limited by the accuracy of the determinations of the R value for the sizestandards. The PDC from bovine heart was found to have an R = 22.4 ± 0.2 nm following cross-linking with glutaraldehyde that was necessary for stabilization of the complex. Dimers and trimers of PDC, present in the preparations used, were separated from monomeric PDCduring 2d-AGE. All R values for the enzyme complexes studied were agreement with, though more accurate than, R valuesobtained by use of electron microscopy. In contrast to this statement, the internal dihydrolipoyl transacetylase core of PDC (E2) had an R of 18.8 ± 0.2 nm using 2d-AGE, but 10.5 nm by electron microscopy. This observation confirms the proposal that the core of the PDC has externally projecting fibrous domains invisibleto electron microscopy.

Zusätzliches Material: 7 Ill.

Materialart: Digitale Medien

URL: http://dx.doi.org/10.1002/prot.340050306

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