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51. NF546 [4,4′-(Carbonylbis(imino-3,1-phenylene-carbonylimino-3,1-(4-methyl-phenylene)-carbonylimino))-bis(1,3-xylene-α,α′-diphosphonic Acid) Tetrasodium Salt] Is a Non-Nucleotide P2Y11 Agonist and Stimulates Release of Interleukin-8 from Human Monocyte-Derived Dendritic Cells

Author

Michael Wiese, Ralf Hausmann, Günther Schmalzing, Darunee Hongwiset, Didier Communi, Alexandra Hamacher, Jean-Marie Boeynaems, Hans-Dieter Royer, Matthias U. Kassack, Niels Eckstein, Sabine Meis, and Claudia Marzian

Subjects
Purinergic P2 Receptor Agonists, Agonist, medicine.drug_class, Stereochemistry, Cell Culture Techniques, chemistry.chemical_element, Stimulation, Calcium, Ligands, Transfection, Naphthalenesulfonates, Cell Line, Tumor, Cyclic AMP, medicine, Humans, Nucleotide, Interleukin 8, Cloning, Molecular, Binding site, Receptor, Pharmacology, chemistry.chemical_classification, Diphosphonates, Dose-Response Relationship, Drug, Receptors, Purinergic P2, Chemistry, Interleukin-8, Dendritic Cells, Recombinant Proteins, Receptors, Purinergic P2X, Cell culture, Molecular Medicine, Protein Binding
Abstract

The G protein-coupled P2Y(11) receptor is involved in immune system modulation. In-depth physiological evaluation is hampered, however, by a lack of selective and potent ligands. By screening a library of sulfonic and phosphonic acid derivatives at P2Y(11) receptors recombinantly expressed in human 1321N1 astrocytoma cells (calcium and cAMP assays), the selective non-nucleotide P2Y(11) agonist NF546 [4,4'-(carbonylbis(imino-3,1-phenylene-carbonylimino-3,1-(4-methyl-phenylene)carbonylimino))-bis(1,3-xylene-alpha,alpha'-diphosphonic acid) tetrasodium salt] was identified. NF546 had a pEC(50) of 6.27 and is relatively selective for P2Y(11) over P2Y(1), P2Y(2), P2Y(4), P2Y(6), P2Y(12), P2X(1), P2X(2), and P2X(2)-X(3). Adenosine-5'-O-(3-thio)triphosphate (ATPgammaS), a nonhydrolyzable analog of the physiological P2Y(11) agonist ATP, and NF546 use a common binding site as suggested by molecular modeling studies and their competitive behavior toward the nanomolar potency antagonist NF340 [4,4'-(carbonylbis(imino-3,1-(4-methyl-phenylene)carbonylimino))bis(naphthalene-2,6-disulfonic acid) tetrasodium salt] in Schild analysis. The pA(2) of NF340 was 8.02 against ATPgammaS and 8.04 against NF546 (calcium assays). NF546 was further tested for P2Y(11)-mediated effects in monocyte-derived dendritic cells. Similarly to ATPgammaS, NF546 led to thrombospondin-1 secretion and inhibition of lipopolysaccharide-stimulated interleukin-12 release, whereas NF340 inhibited these effects. Further, for the first time, it was shown that ATPgammaS or NF546 stimulation promotes interleukin 8 (IL-8) release from dendritic cells, which could be inhibited by NF340. In conclusion, we have described the first selective, non-nucleotide agonist NF546 for P2Y(11) receptors in both recombinant and physiological expression systems and could show a P2Y(11)-stimulated IL-8 release, further supporting the immunomodulatory role of P2Y(11) receptors.

Published
2009

52. Hyperactivation of the Insulin-like Growth Factor Receptor I Signaling Pathway Is an Essential Event for Cisplatin Resistance of Ovarian Cancer Cells

Author

Sybille Wolf-Kümmeth, Barbara Hildebrandt, Anne Pölitz, Inge Napierski, Carsten Denkert, Manfred Beier, Brigitte Royer-Pokora, Georg von Jonquieres, Alexandra Hamacher, Hans-Dieter Royer, Manfred Dietel, Matthias U. Kassack, Jan Budczies, Niels Eckstein, and Kati Servan

Subjects
Cancer Research, medicine.medical_specialty, endocrine system diseases, medicine.medical_treatment, Gene Expression, Antineoplastic Agents, Biology, Insulin-Like Growth Factor Receptor, Receptor, IGF Type 1, Phosphatidylinositol 3-Kinases, Insulin-like growth factor, Cell Line, Tumor, Internal medicine, Biomarkers, Tumor, medicine, Humans, Insulin-Like Growth Factor I, Autocrine signalling, In Situ Hybridization, Fluorescence, PI3K/AKT/mTOR pathway, Chromosome Aberrations, Ovarian Neoplasms, Cisplatin, Cancer, medicine.disease, female genital diseases and pregnancy complications, Endocrinology, Oncology, Drug Resistance, Neoplasm, Cancer research, Female, Signal transduction, Ovarian cancer, Signal Transduction, medicine.drug
Abstract

Platinum plays a central role in the therapy of ovarian cancer, and the emergence of platinum resistance is a major obstacle for clinical management of the disease. We treated A2780 ovarian cancer cells by weekly cycles of cisplatin over a period of 6 months and unveiled that enhanced insulin-like growth factor I receptor (IGF-IR) expression and autocrine IGF-I are associated with hyperactivation of the IGF-IR and phosphatidylinositol-3-OH kinase (PI3K) pathways in cisplatin-resistant cells. IGF-IR expression levels increased during treatment cycles and correlated with cisplatin resistance. Purified IGF-I induced cisplatin resistance in diverse ovarian cancer cell lines, and small molecule inhibitors proved that IGF-IR and PI3K are essential for cisplatin resistance. Similar results were obtained with BG-1 ovarian cancer cells. Cytogenetic and array comparative genomic hybridization analyses revealed selection and de novo formation of chromosomal alterations during resistance development. An analysis of gene expression profiles of primary ovarian carcinomas identified the regulatory subunit PIK3R2 of PI3-kinase as a significant negative prognosis factor for ovarian cancer. We conclude that targeting the IGF-IR and the PI3K pathways is a promising new strategy to treat cisplatin-resistant ovarian carcinomas. [Cancer Res 2009;69(7):2996–3003]

Published
2009

53. Acquired cisplatin resistance in the head-neck cancer cell line Cal27 is associated with decreased DKK1 expression and can partially be reversed by overexpression of DKK1

Author

Alexandra Hamacher, Hans Dieter Royer, Eva M. Gosepath, Matthias U. Kassack, Hermann Lage, Balazs Gyorffy, Kati Servan, Georg von Jonquieres, and Niels Eckstein

Subjects
musculoskeletal diseases, Cancer Research, Pathology, medicine.medical_specialty, Antineoplastic Agents, Enzyme-Linked Immunosorbent Assay, Biology, Cell Line, Tumor, Gene expression, medicine, Humans, Oligonucleotide Array Sequence Analysis, Cisplatin, Microarray analysis techniques, Wnt signaling pathway, Cancer, medicine.disease, Wnt Proteins, Oncology, DKK1, Drug Resistance, Neoplasm, Head and Neck Neoplasms, Cell culture, Suppression subtractive hybridization, Cancer research, Intercellular Signaling Peptides and Proteins, Signal Transduction, medicine.drug
Abstract

Head and neck cancers are treated by a combination of surgery, radiotherapy and/or chemotherapy. The clinical success of cisplatin-based chemotherapy, mostly in combination with 5-FU or a taxane, is however limited by multifactorial intrinsic or acquired resistance. So far, known genes involved in cisplatin resistance do not sufficiently allow the prediction of cancer chemosensitivity. Thus, the purpose of this study was to search for further genes involved in cisplatin resistance by differential gene expression analysis of the parental tongue cancer cell line Cal27 and its 10-fold more resistant sub-cell line Cal27cis, which was obtained by treating Cal27 with increasing concentrations of cisplatin. As found by the suppression subtractive hybridization, expression of DKK1, an inhibitor of canonical WNT signaling, was decreased in Cal27cis. Microarray analysis, qPCR and ELISA confirmed the approximately 2-fold difference in expression. Cisplatin treatment and serum starvation increased by 2-fold the secretion of DKK1 in Cal27 and Cal27cis, thus rendering DKK1-levels significantly different in both cell lines under basal and stress conditions. Recombinant overexpression of DKK1 in Cal27 and Cal27cis resulted in clonal cell lines, which were both 2.2- to 3-fold more sensitive toward cisplatin in cell viability (MTT) and in proliferation (BrdU) assays. In conclusion, acquired (10-fold) resistance of Cal27 against cisplatin is associated with decreased DKK1 expression and could partially be reversed by DKK1 overexpression, thus suggesting DKK1 and the WNT signaling pathway as a marker and target for cisplatin chemosensitivity.

Published
2008

54. Discovery of Potent and Selective Agonists for the Free Fatty Acid Receptor 1 (FFA1/GPR40), a Potential Target for the Treatment of Type II Diabetes

Author

Andreas Spinrath, Christian Urban, Andrew D. Bond, Elisabeth Christiansen, Evi Kostenis, Matthias U. Kassack, Nicole Merten, Alexandra Hamacher, Trond Ulven, Christel Drewke, Susanne Ullrich, Kasper K. Karlsen, and Kathrin Liebscher

Subjects
Models, Molecular, Agonist, medicine.medical_specialty, Time Factors, medicine.drug_class, Carboxylic acid, medicine.medical_treatment, Type 2 diabetes, Crystallography, X-Ray, Receptors, G-Protein-Coupled, Mice, Structure-Activity Relationship, Free fatty acid receptor 1, Diabetes mellitus, Internal medicine, Insulin Secretion, Drug Discovery, medicine, Animals, Humans, Insulin, G protein-coupled receptor, chemistry.chemical_classification, Dose-Response Relationship, Drug, Molecular Structure, Stereoisomerism, medicine.disease, In vitro, Rats, Glucose, Endocrinology, Diabetes Mellitus, Type 2, chemistry, Cinnamates, Molecular Medicine
Abstract

Udgivelsesdato: 2008-Oct-24 A series of 4-phenethynyldihydrocinnamic acid agonists of the free fatty acid receptor 1 (FFA 1) has been discovered and explored. The preferred compound 20 (TUG-424, EC 50 = 32 nM) significantly increased glucose-stimulated insulin secretion at 100 nM and may serve to explore the role of FFA 1 in metabolic diseases such as diabetes or obesity.

Published
2008

55. Sila-Haloperidol, a Silicon Analogue of the Dopamine (D2) Receptor Antagonist Haloperidol: Synthesis, Pharmacological Properties, and Metabolic Fate

Author

Reinhold Tacke, Friedrich Popp, Matthias U. Kassack, Eric Wellner, Alexandra Hamacher, Dirk Schepmann, Christian Burschka, Barbara Müller, Ulrik Jurva, Bastian Theis, and Bernhard Wünsch

Subjects
medicine.drug_class, Stereochemistry, Biochemistry, Inhibitory Concentration 50, Structure-Activity Relationship, Cytochrome P-450 Enzyme System, Dopamine receptor D2, Drug Discovery, medicine, Haloperidol, Humans, Structure–activity relationship, Organosilicon Compounds, General Pharmacology, Toxicology and Pharmaceutics, Receptor, Pharmacology, Binding Sites, Chemistry, Organic Chemistry, Antagonist, Receptor antagonist, Dopamine D2 Receptor Antagonists, Kinetics, Dopamine receptor, Microsomes, Liver, Microsome, Molecular Medicine, Antipsychotic Agents, medicine.drug
Abstract

Haloperidol (1 a), a dopamine (D(2)) receptor antagonist, is in clinical use as an antipsychotic agent. Carbon/silicon exchange (sila-substitution) at the 4-position of the piperidine ring of 1 a (R(3)COH --> R(3)SiOH) leads to sila-haloperidol (1 b). Sila-haloperidol was synthesized in a new multistep synthesis, starting from tetramethoxysilane and taking advantage of the properties of the 2,4,6-trimethoxyphenyl unit as a unique protecting group for silicon. The pharmacological profiles of the C/Si analogues 1 a and 1 b were studied in competitive receptor binding assays at D(1)-D(5), sigma(1), and sigma(2) receptors. Sila-haloperidol (1 b) exhibits significantly different receptor subtype selectivities from haloperidol (1 a) at both receptor families. The C/Si analogues 1 a and 1 b were also studied for 1) their physicochemical properties (log D, pK(a), solubility in HBSS buffer (pH 7.4)), 2) their permeability in a human Caco-2 model, 3) their pharmacokinetic profiles in human and rat liver microsomes, and 4) their inhibition of the five major cytochrome P450 isoforms. In addition, the major in vitro metabolites of sila-haloperidol (1 b) in human liver microsomes were identified using mass-spectrometric techniques. Due to the special chemical properties of silicon, the metabolic fates of the C/Si analogues 1 a and 1 b are totally different.

Published
2008

56. Stabilizing Alginate Confinement and Polymer Coating of CO-Releasing Molecules Supported on Iron Oxide Nanoparticles To Trigger the CO Release by Magnetic Heating

Author

Christoph Janiak, Matthias U. Kassack, Annette M. Schmidt, Hajo Meyer, Alexandra Hamacher, Peter C. Kunz, and Felix Winkler

Subjects
Calcium alginate, Hot Temperature, Alginates, Phenylalanine, Inorganic chemistry, Kinetics, Nanoparticle, Metal Nanoparticles, Antineoplastic Agents, Ferric Compounds, Ruthenium, Polyethylene Glycols, Inorganic Chemistry, chemistry.chemical_compound, Glucuronic Acid, Coordination Complexes, Cell Line, Tumor, Animals, Humans, Horses, Physical and Theoretical Chemistry, Carbon Monoxide, Myoglobin, Hexuronic Acids, Magnetic Phenomena, Water, Dextrans, Dihydroxyphenylalanine, Quaternary Ammonium Compounds, Membrane, HEK293 Cells, chemistry, Energy Transfer, Solubility, Cisplatin, Polyethylenes, Dispersion (chemistry), Iron oxide nanoparticles, Carbon monoxide, Half-Life
Abstract

Maghemite (Fe2O3) iron oxide nanoparticles (IONPs) were synthesized, modified with covalent surface-bound CO-releasing molecules of a tri(carbonyl)-chlorido-phenylalaninato-ruthenium(II) complex (CORM), and coated with a dextran polymer. The time- and temperature-dependent CO release from this CORM-3 analogue was followed by a myoglobin assay. A new measurement method for the myoglobin assay was developed, based on confining "water-soluble" polymer-coated Dextran500k@CORM@IONP particles in hollow spheres of nontoxic and easily prepared calcium alginate. Dropping a mixture of Dextran500k@CORM@IONP and sodium alginate into a CaCl2 solution leads to stable hollow spheres of Ca(2+) cross-linked alginate which contain the Dextran500k@CORM@IONP particles. This "alginate-method" (i) protects CORM-3 analogues from rapid CO-displacement reactions with a protein, (ii) enables a spatial separation of the CORM from its surrounding myoglobin assay with the alginate acting as a CO-permeable membrane, and (iii) allows the use of substances with high absorptivity (such as iron oxide nanoparticles) in the myoglobin assay without interference in the optical path of the UV cell. Embedding the CORM@IONP nanoparticles in the alginate vessel represents a compartmentation of the reactive component and allows for close contact with, yet facile separation from, the surrounding myoglobin assay. The half-life of the CO release from Dextran500k@CORM@IONP particles surrounded by alginate was determined to be 890 ± 70 min at 20 °C. An acceleration of the CO release occurs at higher temperature with a half-life of 172 ± 27 min at 37 °C and 45 ± 7 min at 50 °C. The CO release can be triggered in an alternating current magnetic field (31.7 kA m(-1), 247 kHz, 39.9 mT) through local magnetic heating of the susceptible iron oxide nanoparticles. With magnetic heating at 20 °C in the bulk solution, the half-life of CO release from Dextran500k@CORM@IONP particles decreased to 155 ± 18 min without a noticeable temperature increase in the dispersion. At 37 and 50 °C, the half-life for the CO release triggered by local magnetic heating was 65 ± 5 min and 30 ± 3 min, respectively. Thus, at a physiological temperature of 37 °C, magnetic heating accelerates the CO release of the IONP-bound CORM by a factor of ∼ 2.6. The activation energy for CO release from a CORM-3 analogue was determined to be EA = 78 kJ/mol.

Published
2015

57. ChemInform Abstract: Absolute Configuration and Antitumor Activity of Torrubiellin B

Author

Wenhan Lin, Georgios Daletos, Peter Proksch, Matthias U. Kassack, Catalina Francis Perez Hemphill, Alexandra Hamacher, Attila Mándi, and Tibor Kurtán

Subjects
Antitumor activity, Chemistry, Stereochemistry, medicine.drug_class, Antibiotics, Absolute configuration, medicine, Torrubiellin B, General Medicine
Published
2015

58. Absolute configuration and anti-tumor activity of torrubiellin B

Author

Attila Mándi, Matthias U. Kassack, Peter Proksch, Catalina Francis Perez Hemphill, Tibor Kurtán, Alexandra Hamacher, Georgios Daletos, and Wenhan Lin

Subjects
Cisplatin, Anthracene, Circular dichroism, biology, Acremonium, Stereochemistry, Organic Chemistry, Absolute configuration, Sonneratia caseolaris, biology.organism_classification, Biochemistry, In vitro, chemistry.chemical_compound, chemistry, Természettudományok, Cell culture, Drug Discovery, medicine, Kémiai tudományok, medicine.drug
Abstract

The dimeric anthracene derivative torrubiellin B ( 1 ) was isolated from the endophytic fungus Acremonium sp. that had been obtained from leaves of the Mangrove plant Sonneratia caseolaris . The absolute configuration of 1 was established as (5′ R ,10′ S ,10a′ R ) for the first time on the basis of its electronic circular dichroism (ECD) spectra aided with TDDFT-ECD calculations. Torrubiellin B ( 1 ) exhibited strong anti-tumor activity when tested in vitro against several solid cancer cell lines including cells that are resistant against the widely used cytostatic drug cisplatin. The IC 50 values of 1 against cisplatin sensitive and cisplatin resistant cells were in the range of 0.2–2.6 μM depending on cell line investigated.

Published
2015

59. Sila-haloperidol: A Silicon Analogue of the Dopamine (D2) Receptor Antagonist Haloperidol

Author

and Alexandra Hamacher, Reinhold Tacke, Christian Burschka, Rüdiger Bertermann, Matthias U. Kassack, and Tilman Heinrich

Subjects
Aqueous solution, Hydrochloride, Stereochemistry, Organic Chemistry, Nuclear magnetic resonance spectroscopy, Disiloxane, Inorganic Chemistry, Silanol, chemistry.chemical_compound, chemistry, Dopamine receptor D2, Piperidine, Physical and Theoretical Chemistry, Conformational isomerism
Abstract

Haloperidol (1a), a dopamine (D2) receptor antagonist, is in clinical use as an antipsychotic agent. Carbon/silicon exchange (sila-substitution) at the 4-position of the piperidine ring of 1a (R3COH → R3SiOH) leads to sila-haloperidol (1b). Sila-haloperidol was synthesized in a multistep synthesis, starting from tetramethoxysilane, and was isolated as the hydrochloride 1b·HCl. ESI-MS studies of aqueous solutions of the silanol 1b and the corresponding disiloxane 10 at different pH values revealed a remarkable stability of 1b. The C/Si analogues 1a·HCl and 1b·HCl were structurally characterized by single-crystal X-ray diffraction and solution ([D6]DMSO) NMR spectroscopy. Analogous chair conformations of the piperidinium (1a·HCl) and 4-silapiperidinium (1b·HCl) skeleton were observed in the crystal, and two analogous chair conformations of the cations were detected in solution, the molar ratios of these two conformers differing substantially (1a·HCl, 13:1; 1b·HCl, 2:1). In radioligand binding studies, the C...

Published
2004

60. Design and Synthesis of Novel Anti-Plasmodial Histone Deacetylase Inhibitors Containing an Alkoxyamide Connecting Unit

Author

Parichat Sureechatchaiyan, Leandro A. Alves Avelar, Katherine T. Andrews, Alexandra Hamacher, Finn K. Hansen, Thomas Kurz, Matthias U. Kassack, Benjamin Mordmüller, Jana Held, and Jessica A. Engel

Subjects
0301 basic medicine, 030106 microbiology, Pharmaceutical Science, Plasmodium falciparum, Biology, biology.organism_classification, 3. Good health, Histone H4, 03 medical and health sciences, 030104 developmental biology, Histone, Biochemistry, Drug Discovery, biology.protein, Structure–activity relationship, Homology modeling, Histone deacetylase, Threonine, IC50
Abstract

Despite recent declines in mortality, malaria remains an important global health problem. New therapies are needed, including new drugs with novel modes of action compared to existing agents. Among new potential therapeutic targets for malaria, inhibition of parasitic histone deacetylases (HDACs) is a promising approach. Homology modeling of PfHDAC1, a known target of some anti-plasmodial HDAC inhibitors, revealed a unique threonine residue at the rim of the active site in close proximity to the location of the cap group of vorinostat-type HDAC inhibitors. Aiming to obtain HDAC inhibitors with potent and preferential anti-plasmodial activity, we synthesized a mini-library of alkoxyamide-based HDAC inhibitors containing hydrogen bond acceptors in the cap group. Using a 5-step synthetic route, 12 new inhibitors were synthesized and assayed against Plasmodium falciparum asexual blood stage parasites (clones 3D7 and Dd2) and human cells (HepG2). The most active compound 6h (Pf3D7 IC50: 0.07 µM; PfDd2 IC50: 0.07 µM) was 25-fold more toxic against the parasite versus human HepG2 cells. Selected compounds were shown to cause hyperacetylation of P. falciparum histone H4, indicating inhibition of one or more PfHDACs.

Published
2017

61. ChemInform Abstract: Absolute Configuration and Antibiotic Activity of Neosartorin (I) from the Endophytic Fungus Aspergillus fumigatiaffinis

Author

Amal H. Aly, Heike Broetz‐Oesterhelt, Attila Mándi, Tibor Kurtán, Ilka Zerfass, Abdessamad Debbab, Antonius R. B. Ola, Matthias U. Kassack, Alexandra Hamacher, and Peter Proksch

Subjects
Broad spectrum, medicine.drug_class, Chemistry, Antibiotics, medicine, Absolute configuration, General Medicine, Aspergillus fumigatiaffinis, Endophytic fungus, Antibacterial activity, Microbiology
Abstract

The title compound (I) exhibits substantial antibacterial activity against a broad spectrum of Gram-positive bacterial species (e.g. staphylococci, streptococci, enterococci, B.

Published
2014

62. Psychrophilin E, a new cyclotripeptide, from co-fermentation of two marine alga-derived fungi of the genus Aspergillus

Author

Bin-Gui Wang, Matthias U. Kassack, Alexandra Hamacher, Thomas Fischer, Eckhard H. Roth, Feng-Yu Du, Yoen Ok Roth, and Sherif S. Ebada

Subjects
Co-fermentation, Stereochemistry, Chemical structure, Oceans and Seas, Antineoplastic Agents, Marine Biology, Plant Science, Biochemistry, Peptides, Cyclic, Hydrolysate, Analytical Chemistry, Polyketide, Alkaloids, Genus, Germany, Botany, Humans, Nuclear Magnetic Resonance, Biomolecular, Mycelium, Aspergillus, biology, Molecular Structure, Organic Chemistry, biology.organism_classification, HCT116 Cells, Drug Resistance, Neoplasm, Fermentation, Female, Cisplatin, Drug Screening Assays, Antitumor, Two-dimensional nuclear magnetic resonance spectroscopy
Abstract

Chemical investigation of the mycelial extract of a mixed culture of two marine alga-derived fungal strains of the genus Aspergillus has yielded one new cyclotripeptide, psychrophilin E (1), the recently reported oxepin-containing alkaloids, protuboxepin A (2) and oxepinamide E (3), together with three other polyketide derivatives (4–6). The chemical structure and relative and absolute configurations of psychrophilin E (1) were unambiguously established based on HRMS, 1D, 2D NMR and chiral-phase HPLC analysis of its hydrolysate. All the isolated compounds were assessed for their anti-proliferative activity against four different human cancer cell lines and some of them revealed selective activities.

Published
2014

63. Absolute configuration and antibiotic activity of neosartorin from the endophytic fungus Aspergillus fumigatiaffinis

Author

Attila Mándi, Heike Brötz-Oesterhelt, Tibor Kurtán, Abdessamad Debbab, Alexandra Hamacher, Amal H. Aly, Matthias U. Kassack, Antonius R. B. Ola, Ilka Zerfass, and Peter Proksch

Subjects
Circular dichroism, biology, medicine.drug_class, Stereochemistry, Chemistry, Organic Chemistry, Antibiotics, Absolute configuration, Bacillus subtilis, Biológiai tudományok, biology.organism_classification, Biochemistry, HeLa, Természettudományok, Drug Discovery, Toxicity, medicine, Chirality (chemistry), Antibacterial activity
Abstract

Neosartorin ( 1 ) was isolated from the endophytic fungus Aspergillus fumigatiaffinis . The absolute configuration of 1 , including both axial and central chirality elements, was established as (a R ,5 S ,10 R ,5′ S ,6′ S ,10′ R ) for the first time on the basis of its electronic circular dichroism (ECD) spectra aided with TDDFT–ECD calculations. Neosartorin ( 1 ) exhibited substantial antibacterial activity against a broad spectrum of Gram-positive bacterial species including staphylococci, streptococci, enterococci, and Bacillus subtilis with minimal inhibitory concentrations in the range of 4–32 μg/mL. When the toxicity of 1 against eukaryotic cells was measured using a panel of different cancer cell lines such as HELA and BALB/3T3, the average IC 50 values exceeded 32 μg/mL.

Published
2014

64. Pro-apoptotic and immunostimulatory tetrahydroxanthone dimers from the endophytic fungus Phomopsis longicolla

Author

Christoph Janiak, Alexandra Hamacher, Richard Sawadogo, Stefanie Scheu, Peter Proksch, Amal H. Aly, Sebastian Wesselborg, Tibor Kurtán, Björn Stork, David Rönsberg, Philip Böhler, Attila Mándi, Matthias U. Kassack, Wenhan Lin, Abdessamad Debbab, Victor Wray, Vera Vasylyeva, Laura H. Engelke, and Marc Diederich

Subjects
Models, Molecular, Circular dichroism, Stereochemistry, T-Lymphocytes, Xanthones, Antineoplastic Agents, Apoptosis, Mice, Structure-Activity Relationship, Immune system, Ascomycota, Cell Line, Tumor, Animals, Humans, Phomopsis longicolla, Cell Proliferation, biology, Dose-Response Relationship, Drug, Molecular Structure, Activator (genetics), Chemistry, Macrophages, Organic Chemistry, biology.organism_classification, Semisynthesis, Killer Cells, Natural, Cell culture, Cancer cell, Leukocytes, Mononuclear, Quantum Theory, Dimerization
Abstract

Four tetrahydroxanthone dimers (1-4) and four biogenetically related monomers (5-8), including the new derivatives 4-6, were isolated from the endophyte Phomopsis longicolla. The absolute configurations of 2-4 were established for the first time by TDDFT electronic circular dichroism calculations, and that of phomoxanthone A (1) was revised by X-ray crystallography. Phomoxanthone A (1) showed the strongest pro-apoptotic activity when tested against a panel of human cancer cell lines, including cisplatin-resistant cells, whereas it was up to 100-fold less active against healthy blood cells. It was also the most potent activator of murine T lymphocytes, NK cells, and macrophages, suggesting an activation of the immune system in parallel to its pro-apoptotic activity. This dual effect in combating cancer cells could help in fighting resistance during chemotherapy. Preliminary structure-activity studies of isolated compounds and derivatives obtained by semisynthesis (9a-11) hinted at the location of the biaryl axis and the presence of acetyl groups as important structural elements for the biological activity of the studied tetrahydroxanthones.

Published
2013

66. In vitro and mouse in vivo characterization of the potent free fatty acid 1 receptor agonist TUG-469

Author

H J Partke, Matthias U. Kassack, Alexandra Hamacher, Holger Gohlke, M Roden, Trond Ulven, Christian Urban, S Schinner, Elisabeth Christiansen, and Maria E Due-Hansen

Subjects
Agonist, TUG-469, Blood Glucose, Male, medicine.medical_specialty, Time Factors, medicine.drug_class, Mice, Obese, Biology, Free fatty acids, Transfection, Receptors, G-Protein-Coupled, Prediabetic State, Methylamines, Mice, In vivo, Internal medicine, Free fatty acid receptor 1, Cell Line, Tumor, Insulin-Secreting Cells, medicine, Cyclic AMP, Animals, Hypoglycemic Agents, Insulin, Calcium Signaling, Receptor, Pharmacology, chemistry.chemical_classification, GPR40, Glucose tolerance test, Aniline Compounds, medicine.diagnostic_test, Dose-Response Relationship, Drug, Phenylpropionates, Diabetes, Rat Insulinoma, GPR120, Fatty acid, General Medicine, FFA1, Recombinant Proteins, Rats, Disease Models, Animal, Endocrinology, chemistry, Propionates, human activities, Biomarkers
Abstract

Activation of the G protein-coupled free fatty acid receptor 1 (FFA1; formerly known as GPR40) leads to an enhancement of glucose-stimulated insulin secretion from pancreatic β-cells. TUG-469 has previously been reported as a potent FFA1 agonist. This study was performed to confirm the higher in vitro potency of TUG-469 compared to the reference FFA1 agonist GW9508 and to prove in vivo activity in a pre-diabetic mouse model. The in vitro pharmacology of TUG-469 was studied using Ca(2+)-, cAMP-, and impedance-based assays at recombinant FFA1 and free fatty acid receptor 4, formerly known as GPR120 (FFA4) expressing 1321N1 cells and the rat insulinoma cell line INS-1. Furthermore, we investigated the systemic effect of TUG-469 on glucose tolerance in pre-diabetic New Zealand obese (NZO) mice performing a glucose tolerance test after intraperitoneal administration of 5 mg/kg TUG-469. In comparison to GW9508, TUG-469 showed a 1.7- to 3.0-times higher potency in vitro at 1321N1 cells recombinantly expressing FFA1. Both compounds increased insulin secretion from rat insulinoma INS-1 cells. TUG-469 is > 200-fold selective for FFA1 over FFA4. Finally, a single dose of 5 mg/kg TUG-469 significantly improved glucose tolerance in pre-diabetic NZO mice. TUG-469 turned out as a promising candidate for further drug development of FFA1 agonists for treatment of type 2 diabetes mellitus.

Published
2013

67. Prenylation at the indole ring leads to a significant increase of cytotoxicity of tryptophan-containing cyclic dipeptides

Author

Matthias U. Kassack, Shu-Ming Li, Lena Ludwig, Xia Yu, Alexandra Hamacher, and Beate Wollinsky

Subjects
Indoles, Magnetic Resonance Spectroscopy, Proline, Stereochemistry, Cell Survival, Clinical Biochemistry, Prenyltransferase, Pharmaceutical Science, Biochemistry, Peptides, Cyclic, Substrate Specificity, Fungal Proteins, Inhibitory Concentration 50, Structure-Activity Relationship, Hemiterpenes, Organophosphorus Compounds, Prenylation, Cell Line, Tumor, Drug Discovery, Moiety, Humans, Cytotoxicity, Molecular Biology, Chromatography, High Pressure Liquid, Indole test, chemistry.chemical_classification, Alanine, Organic Chemistry, Tryptophan, Stereoisomerism, Dipeptides, Dimethylallyltranstransferase, Recombinant Proteins, Amino acid, Enzyme, chemistry, Biocatalysis, Molecular Medicine
Abstract

Fourteen tryptophan-containing cyclic dipeptides 1a–14a, including all four stereoisomers of cyclo-Trp-Pro and cyclo-Trp-Ala, were converted to their C2-regularly prenylated derivatives 1b–14b in the presence of dimethylallyl diphosphate by using the purified recombinant FtmPT1 as catalyst. The enzyme products were isolated on HPLC in preparative scales and their structures were elucidated by NMR and MS analyses. The cytotoxic effects of the prenylated products and their substrates were tested with human leukemia K562 and ovarian cancer A2780 sens and A2780 CisR cell lines. Preliminary results have been clearly shown that prenylation at C2 led to a significant increase of the cytotoxicity of the tested cyclic dipeptides in all the 14 cases. The second amino acid and the stereochemistry of tryptophan moiety of the cyclic dipeptides showed less influence on the cytotoxicity of the tested compounds.

Published
2012

68. Gold(i) complexes of water-soluble diphos-type ligands: Synthesis, anticancer activity, apoptosis and thioredoxin reductase inhibition

Author

Bernhard Spingler, Riccardo Rubbiani, Philip Böhler, Ingo Ott, Peter C. Kunz, Wim Wätjen, Alexandra Hamacher, Corinna Wetzel, Matthias U. Kassack, University of Zurich, and Kunz, P C

Subjects
Models, Molecular, 10120 Department of Chemistry, Thioredoxin-Disulfide Reductase, Stereochemistry, Thioredoxin reductase, Glutathione reductase, Antineoplastic Agents, Apoptosis, Inorganic Chemistry, chemistry.chemical_compound, Cell Line, Tumor, 540 Chemistry, Animals, Humans, Imidazole, Cytotoxic T cell, chemistry.chemical_classification, 1604 Inorganic Chemistry, Imidazoles, Rats, Thiazoles, Enzyme, chemistry, Cell culture, Lipophilicity, Organogold Compounds
Abstract

Gold(I) complexes of imidazole and thiazole-based diphos type ligands were prepared and their potential as chemotherapeutics investigated. Depending on the ligands employed and the reaction conditions complexes [L(AuCl)(2)] and [L(2)Au]X (X = Cl, PF(6)) are obtained. The ligands used are diphosphanes with azoyl substituents R(2)P(CH(2))(2)PR(2) {R = 1-methylimidazol-2-yl (1), 1-methylbenzimidazol-2-yl (4), thiazol-2-yl (5) and benzthiazol-2-yl (6)} as well as the novel ligands RPhP(CH(2))(2)PRPh {R = 1-methylimidazol-2-yl (3)} and R(2)P(CH(2))(3)PR(2) {R = 1-methylimidazol-2-yl (2)}. The cytotoxic activity of the complexes was assessed against three human cancer cell lines and a rat hepatoma cell line and correlated to the lipophilicity of the compounds. The tetrahedral gold complexes [(3)(2)Au]PF(6) and [(5)(2)Au]PF(6) with intermediate lipophilicity (logD(7.4) = 0.21 and 0.25) showed significant cytotoxic activity in different cell lines. Both compounds induce apoptosis and inhibit the enzymes thioredoxin reductase and glutathione reductase.

Published
2011
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69. Fluorescent Polylactides with Rhenium(bisimine) Cores for Tumour Diagnostics (Eur. J. Inorg. Chem. 32/2010)

Author

Nadine E. Brückmann, Matthias U. Kassack, Peter C. Kunz, Alexandra Hamacher, and Susanne Kögel

Subjects
chemistry.chemical_classification, fungi, food and beverages, chemistry.chemical_element, Early detection, Polymer, Rhenium, Fluorescence, Inorganic Chemistry, Membrane, chemistry, Polymer chemistry, Fluorescence microscope, Fluorescent polymer
Abstract

The cover picture shows the structure of a fluorescent polymer consisting of a ligand-functionalised polylactide coordinated to Re(CO)3(phen). This polymer can passively target cancer tissue and transport the fluorescent dye to the cancer cell membranes, where it can be detected by fluorescence microscopy, which enables early detection of cancer. The resulting fluorescence in the membranes of A2780 cells can be seen in the background. Details are discussed in the article by P. C. Kunz et al. on p. 5063 ff.

Published
2010

70. Common variants in P2RY11 are associated with narcolepsy

Author

Marie Dobrovolna, Alex Desautels, Thomas Meitinger, Birgit Frauscher, Jing Li, William T. Longstreth, Yutaka Honda, Sung-Pil Lee, Birgit Högl, Stine Knudsen, Makoto Honda, Fabio Pizza, Pui-Yan Kwok, Neil Risch, Karin Weiner, Elisabeth Ruppert, Mali Einen, Seung-Chul Hong, Sona Nevsimalova, Lawrence Steinman, Birgitte Rahbek Kornum, Ling Lin, Juliette Faraco, Taku Miyagawa, Fang Han, David Kemlink, Joachim Hallmayer, Pablo V. Gejman, Mark N. Kvale, Terry Young, Alexandra Hamacher, Emmanuel Mignot, Matthias U. Kassack, H-Erich Wichmann, Gerald T. Nepom, Robert C. Axtell, Jasmin L Eshragh, Thomas J Rico, Juliane Winkelmann, Jong-Hyun Jeong, Jacques Montplaisir, Minae Kawashima, Christian Gieger, Maurice M. Ohayon, Patrice Bourgin, Giuseppe Plazzi, Xiaosong Dong, Francesca Poli, Hedwich F. Kuipers, Kingman P. Strohl, Simon C. Warby, Paul E. Peppard, Yu-Shu Huang, Stephanie Hesselson, Katsushi Tokunaga, Poul Jennum, Douglas F. Levinson, Thanh G.N. Ton, Guy A. Rouleau, Per Egil Hesla, Kornum B.R., Kawashima M., Faraco J., Lin L., Rico T.J., Hesselson S., Axtell R.C., Kuipers H., Weiner K., Hamacher A., Kassack M.U., Han F., Knudsen S., Li J., Dong X., Winkelmann J., Plazzi G., Nevsimalova S., Hong S.C., Honda Y., Honda M., Hogl B., Ton T.G., Montplaisir J., Bourgin P., Kemlink D., Huang Y.S., Warby S., Einen M., Eshragh J.L., Miyagawa T., Desautels A., Ruppert E., Hesla P.E., Poli F., Pizza F., Frauscher B., Jeong J.H., Lee S.P., Strohl K.P., Longstreth W.T. Jr., Kvale M., Dobrovolna M., Ohayon M.M., Nepom G.T., Wichmann H.E., Rouleau G.A., Gieger C., Levinson D.F., Gejman P.V., Meitinger T., Peppard P., Young T., Jennum P., Steinman L., Tokunaga K., Kwok P.Y., Risch N., Hallmayer J., and Mognot E.

Subjects
Genome-wide association study, Medical and Health Sciences, P2RY11, narcolepsy, narcolepsy with cataplexy, genome-wide association, 0302 clinical medicine, Receptors, Ethnicity, Odds Ratio, 2.1 Biological and endogenous factors, Pandemrix, Aetiology, African Americans, 0303 health sciences, Single Nucleotide, Biological Sciences, Asians, Asian Continental Ancestry Group, European Continental Ancestry Group, Ethnic Groups, Biology, Peripheral blood mononuclear cell, Polymorphism, Single Nucleotide, White People, Article, 03 medical and health sciences, Asian People, Genetics, medicine, Humans, Genetic Predisposition to Disease, Polymorphism, Allele, Alleles, 030304 developmental biology, Narcolepsy, Autoimmune disease, Purinergic P2, Whites, Receptors, Purinergic P2, Human Genome, Case-control study, Genetic Variation, medicine.disease, Brain Disorders, Black or African American, Case-Control Studies, Immunology, 030217 neurology & neurosurgery, CD8, Developmental Biology, Genome-Wide Association Study
Abstract

Growing evidence supports the hypothesis that narcolepsy with cataplexy is an autoimmune disease. We here report genome-wide association analyses for narcolepsy with replication and fine mapping across three ethnic groups (3,406 individuals of European ancestry, 2,414 Asians and 302 African Americans). We identify a SNP in the 3' untranslated region of P2RY11, the purinergic receptor subtype P2Y₁₁ gene, which is associated with narcolepsy (rs2305795, combined P = 6.1 × 10⁻¹⁰, odds ratio = 1.28, 95% CI 1.19-1.39, n = 5689). The disease-associated allele is correlated with reduced expression of P2RY11 in CD8(+) T lymphocytes (339% reduced, P = 0.003) and natural killer (NK) cells (P = 0.031), but not in other peripheral blood mononuclear cell types. The low expression variant is also associated with reduced P2RY11-mediated resistance to ATP-induced cell death in T lymphocytes (P = 0.0007) and natural killer cells (P = 0.001). These results identify P2RY11 as an important regulator of immune-cell survival, with possible implications in narcolepsy and other autoimmune diseases.

Published
2010

71. Structure−Activity Study of Dihydrocinnamic Acids and Discovery of the Potent FFA1 (GPR40) Agonist TUG-469

Author

Sanne Rasmussen, Susanne Ullrich, Alexandra Hamacher, Evi Kostenis, Rasmus Koefoed Petersen, Mette Steensgaard, Michael Pfleiderer, Nicole Merten, Christel Drewke, Kasper K. Karlsen, Matthias U. Kassack, Elisabeth Christiansen, Maria E Due-Hansen, Christian Urban, Johannes Schmidt, Trond Ulven, and Karsten Kristiansen

Subjects
chemistry.chemical_classification, Agonist, Drug discovery, Stereochemistry, medicine.drug_class, business.industry, Organic Chemistry, Fatty acid, Pharmacology, Biochemistry, chemistry, Free fatty acid receptor 1, Drug Discovery, medicine, Potency, Moiety, Receptor, business, Linker
Abstract

The free fatty acid 1 receptor (FFA1 or GPR40), which is highly expressed on pancreatic β-cells and amplifies glucose-stimulated insulin secretion, has emerged as an attractive target for the treatment of type 2 diabetes. Several FFA1 agonists containing the para-substituted dihydrocinnamic acid moiety are known. We here present a structure-activity relationship study of this compound family suggesting that the central methyleneoxy linker is preferable for the smaller compounds, whereas the central methyleneamine linker gives higher potency to the larger compounds. The study resulted in the discovery of the potent and selective full FFA1 agonist TUG-469 (29).

Published
2010

74. Dibenzazecine compounds with a novel dopamine/5HT2A receptor profile and 3D-QSAR analysis

Author

Barbara Hoefgen, Mathias Weigt, Matthias U. Kassack, Jochen Lehmann, Michael Wiese, and Alexandra Hamacher

Subjects
Quantitative structure–activity relationship, Stereochemistry, 5-HT2A receptor, Quantitative Structure-Activity Relationship, CHO Cells, Pharmacology, Biology, Cell Line, Receptors, Dopamine, Dibenzazepines, Dopamine, Cricetinae, Dopamine receptor D2, medicine, Haloperidol, Animals, Humans, Receptor, Serotonin, 5-HT2A, Pharmacology (medical), Receptor, Clozapine, Dose-Response Relationship, Drug, Dopamine Antagonists, Serotonin Antagonists, Pharmacophore, Heterocyclic Compounds, 3-Ring, Research Article, Protein Binding, medicine.drug
Abstract

Background Antipsychotics are divided into typical and atypical compounds based on clinical efficacy and side effects. The purpose of this study was to characterize in vitro a series of novel azecine-type compounds at human dopamine D1-D5 and 5HT2A receptors and to assign them to different classes according to their dopamine/5HT2A receptor profile. Results Regardless of using affinity data (pK i values at D1-D5 and 5HT2A) or selectivity data (15 log (Ki ratios)), principal component analysis with azecine-type compounds, haloperidol, and clozapine revealed three groups of dopamine/5HT2A ligands: 1) haloperidol; 2) clozapine plus four azecine-type compounds; 3) two hydroxylated dibenzazecines. Reducing the number of Ki ratios used for principal component analysis from 15 to two (the D1/D2 and D2/5HT2A Ki ratios) obtained the same three groups of compounds. The most potent dibenzazecine clustering in the same group as clozapine was the non-hydroxylated LE410 which shows a slightly different D2-like receptor profile (D2L > D3 > D4.4) than clozapine (D4.4 > D2L > D3). The monohydroxylated dibenzacezine LE404 clusters in a separate group from clozapine/LE410 and from haloperidol and shows increased D1 selectivity. Conclusion In conclusion, two compounds with a novel dopamine/5HT2A receptor profile, LE404 and LE410, with some differences in their respective D1/D2 receptor affinities including a validated pharmacophore-based 3D-QSAR model for D1 antagonists are presented.

Published
2006

75. Erratum: Common variants in P2RY11 are associated with narcolepsy

Author

Stephanie Hesselson, Juliette Faraco, Fang Han, Terry Young, Emmanuel Mignot, Matthias U. Kassack, Sona Nevsimalova, Joachim Hallmayer, Maurice M. Ohayon, Patrice Bourgin, Jong-Hyun Jeong, Mark N. Kvale, Fabio Pizza, Giuseppe Plazzi, Yutaka Honda, Paul E. Peppard, Yu-Shu Huang, David Kemlink, Thomas J Rico, Jasmin L Eshragh, Minae Kawashima, Francesca Poli, William T. Longstreth, Guy A. Rouleau, H-Erich Wichmann, Birgit Högl, Hedwich F. Kuipers, Poul Jennum, Seung-Chul Hong, Taku Miyagawa, Pablo V. Gejman, Gerald T. Nepom, Thomas Meitinger, Lawrence Steinman, Christian Gieger, Birgit Frauscher, Mali Einen, Karin Weiner, Alex Desautels, Thanh G.N. Ton, Xiaosong Dong, Douglas F. Levinson, Kingman P Strohl, Alexandra Hamacher, Elisabeth Ruppert, Jacques Montplaisir, Sung-Pil Lee, Neil Risch, Marie Dobrovolna, Katsushi Tokunaga, Jing Li, Stine Knudsen, Per Egil Hesla, Makoto Honda, Ling Lin, Simon C. Warby, Birgitte Rahbek Kornum, Robert C. Axtell, Juliane Winkelmann, and Pui-Yan Kwok

Subjects
Genetics, Nat, medicine, Percentage reduction, Biology, medicine.disease, CD8, Narcolepsy
Abstract

Nat. Genet. 43, 66–71 (2011); published online 19 December 2010; corrected after print 22 September 2011 In the version of this article initially published, the percentage reduction of P2RY11 expression in CD8+ T lymphocytes was incorrectly given as 339%, when it should have been 72%. The percentagewas not given for NK cells and should have been 70%.

Published
2011

76. Imidazole-based phosphane gold(I) complexes as potential agents for cancer treatment: Synthesis, structural studies and antitumour activity

Author

Alexandra Hamacher, Matthias U. Kassack, Bernhard Spingler, and Peter C. Kunz

Subjects
Models, Molecular, Tris, Phosphines, Stereochemistry, Molecular Conformation, chemistry.chemical_element, Antineoplastic Agents, Zinc, Inorganic Chemistry, Metal, Inhibitory Concentration 50, chemistry.chemical_compound, Cell Line, Tumor, Animals, Humans, Imidazole, Lewis acids and bases, Bimetallic strip, Ligand, Imidazoles, Water, Gold Compounds, Solubility, chemistry, visual_art, HSAB theory, visual_art.visual_art_medium, Organogold Compounds
Abstract

The reaction of the imidazolyl-4(5)-phosphane ligands 2-isopropylimidazol-4(5)yl-diphenylphosphane (4-MIP(iPr)) and tris(2-isopropylimidazol-4(5)yl)phosphane (4-TIP(iPr)) towards gold(I) has been explored and compared to those of analogous 1-methylimidazol-2-ylphosphane ligands. The structure of [(4-MIP(iPr))AuCl] () shows a linear P-Au-Cl coordination, whereas the 4-TIP(iPr) ligand forms a dinuclear complex [{(4-TIP(iPr))Au}(2)]Cl(2) (). Here, 4-TIP(iPr) bridges two gold(I) atoms in a head-to-tail P,N fashion. Complex forms in the presence of the hard Lewis acid ZnCl(2) the bimetallic complex [AuCl(4-TIP(iPr))ZnCl]Cl (), in which 4-TIP(iPr) bridges the two metal centers. In accordance with the HSAB concept the Au(I) atom is coordinated by the P atom and the zinc(II) by three N atoms in a N,N,N fashion. The solid-state structures of the complexes have been elucidated by single-crystal X-ray analysis. The Au(I)-Au(I) contact in is 2.8821(15) A. The biological activities of all imidazol-2-yl- and imidazol-4(5)-ylphosphane gold(I) complexes towards nine human cancer cell lines including seven ovarian cancer cell lines of different sensitivity towards cisplatin and two leukemia cell lines have been explored.

Published
2009

77. Imidazole-based phosphane gold(I) complexes as potential agents for cancer treatment: Synthesis, structural studies and antitumour activity.

Author

Peter C. Kunz, Matthias U. Kassack, Alexandra Hamacher, and Bernhard Spingler

Subjects
IMIDAZOLES, GOLD compounds, METAL complexes, CANCER treatment, COMPLEX compounds synthesis, ANTINEOPLASTIC agents, PHOSPHORUS compounds, METALS in medicine
Abstract

The reaction of the imidazolyl-4(5)-phosphane ligands 2-isopropylimidazol-4(5)yl-diphenylphosphane (4-MIPiPr) and tris(2-isopropylimidazol-4(5)yl)phosphane (4-TIPiPr) towards gold(I) has been explored and compared to those of analogous 1-methylimidazol-2-ylphosphane ligands. The structure of [(4-MIPiPr)AuCl] (4) shows a linear P–Au–Cl coordination, whereas the 4-TIPiPrligand forms a dinuclear complex [{(4-TIPiPr)Au}2]Cl2(5). Here, 4-TIPiPrbridges two gold(I) atoms in a head-to-tail P,Nfashion. Complex 5forms in the presence of the hard Lewis acid ZnCl2the bimetallic complex [AuCl(4-TIPiPr)ZnCl]Cl (6), in which 4-TIPiPrbridges the two metal centers. In accordance with the HSAB concept the Au(I) atom is coordinated by the P atom and the zinc(II) by three N atoms in a N,N,Nfashion. The solid-state structures of the complexes 4–6have been elucidated by single-crystal X-ray analysis. The Au(I)–Au(I) contact in 5is 2.8821(15) Å. The biological activities of all imidazol-2-yl- and imidazol-4(5)-ylphosphane gold(I) complexes towards nine human cancer cell lines including seven ovarian cancer cell lines of different sensitivity towards cisplatin and two leukemia cell lines have been explored. [ABSTRACT FROM AUTHOR]

Published
2009
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