Your search keyword '"Köhn M"' showing total 145 results

101. Non-coding RNAs, the cutting edge of histone messages.

Author

Köhn M and Hüttelmaier S

Subjects

RNA Precursors genetics, RNA Processing, Post-Transcriptional, RNA, Untranslated genetics, RNA, Untranslated metabolism, Histones metabolism, RNA, Untranslated physiology

Abstract

In metazoan the 3'-end processing of histone mRNAs is a conserved process involving the concerted action of many protein factors and the non-coding U7 snRNA. Recently, we identified that the processing of histone pre-mRNAs is promoted by an additional ncRNA, the Y3-derived Y3** RNA. U7 modulates the association of the U7 snRNP whereas Y3** promotes recruitment of CPSF (cleavage and polyadenylation specific factor) proteins to nascent histone transcripts at histone locus bodies (HLBs) in mammals. This enhances the 3'-end cleavage of nascent histone pre-mRNAs and modulates HLB assembly. Here we discuss new insights in the role of ncRNAs in the spatiotemporal control of histone synthesis. We propose that ncRNAs scaffold the formation of functional protein-RNA complexes and their sequential deposition on nascent histone pre-mRNAs at HLBs. These findings add to the multiple roles of ncRNAs in controlling gene expression and may provide new avenues for targeting histone synthesis in cancer.

Published

2016

102. The Y3** ncRNA promotes the 3' end processing of histone mRNAs.

Author

Köhn M, Ihling C, Sinz A, Krohn K, and Hüttelmaier S

Subjects

ATP-Binding Cassette Transporters genetics, ATP-Binding Cassette Transporters metabolism, HEK293 Cells, Humans, RNA Precursors genetics, RNA, Long Noncoding metabolism, RNA, Untranslated genetics, Histones genetics, RNA 3' End Processing genetics, RNA Precursors metabolism, RNA, Long Noncoding genetics, RNA, Untranslated metabolism

Abstract

We demonstrate that the Y3/Y3** noncoding RNAs (ncRNAs) bind to the CPSF (cleavage and polyadenylation specificity factor) and that Y3** associates with the 3' untranslated region (UTR) of histone pre-mRNAs. The depletion of Y3** impairs the 3' end processing of histone pre-mRNAs as well as the formation and protein dynamics of histone locus bodies (HLBs), the site of histone mRNA synthesis and processing. HLB morphology is also disturbed by knockdown of the CPSF but not the U7-snRNP components. In conclusion, we propose that the Y3** ncRNA promotes the 3' end processing of histone pre-mRNAs by enhancing the recruitment of the CPSF to histone pre-mRNAs at HLBs., (© 2015 Köhn et al.; Published by Cold Spring Harbor Laboratory Press.)

Published

2015

103. Procyanidins Negatively Affect the Activity of the Phosphatases of Regenerating Liver.

Author

Stadlbauer S, Rios P, Ohmori K, Suzuki K, and Köhn M

Subjects

Catechin pharmacology, Cell Cycle Proteins antagonists & inhibitors, Flow Cytometry, HEK293 Cells drug effects, Humans, Membrane Proteins antagonists & inhibitors, Neoplasm Proteins antagonists & inhibitors, Protein Tyrosine Phosphatases antagonists & inhibitors, Wound Healing drug effects, Liver Regeneration drug effects, Phosphoprotein Phosphatases antagonists & inhibitors, Proanthocyanidins pharmacology

Abstract

Natural polyphenols like oligomeric catechins (procyanidins) derived from green tea and herbal medicines are interesting compounds for pharmaceutical research due to their ability to protect against carcinogenesis in animal models. It is nevertheless still unclear how intracellular pathways are modulated by polyphenols. Monomeric polyphenols were shown to affect the activity of some protein phosphatases (PPs). The three phosphatases of regenerating liver (PRLs) are close relatives and promising therapeutic targets in cancer. In the present study we show that several procyanidins inhibit the activity of all three members of the PRL family in the low micromolar range, whereas monomeric epicatechins show weak inhibitory activity. Increasing the number of catechin units in procyanidins to more than three does not further enhance the potency. Remarkably, the tested procyanidins showed selectivity in vitro when compared to other PPs, and over 10-fold selectivity toward PRL-1 over PRL-2 and PRL-3. As PRL overexpression induces cell migration compared to control cells, the effect of procyanidins on this phenotype was studied. Treatment with procyanidin C2 led to a decrease in cell migration of PRL-1- and PRL-3-overexpressing cells, suggesting the compound-dependent inhibition of PRL-promoted cell migration. Treatment with procyanidin B3 led to selective suppression of PRL-1 overexpressing cells, thereby corroborating the selectivity toward PRL-1- over PRL-3 in vitro. Together, our results show that procyanidins negatively affect PRL activity, suggesting that PRLs could be targets in the polypharmacology of natural polyphenols. Furthermore, they are interesting candidates for the development of PRL-1 inhibitors due to their low cellular toxicity and the selectivity within the PRL family.

Published

2015

104. Chemistry and biology of protein and inositol phosphorylation.

Author

Köhn M

Subjects

Animals, Drug Discovery, Humans, Inositol Phosphates metabolism, Phosphoric Monoester Hydrolases metabolism, Phosphorylation, Protein Kinases metabolism, Inositol metabolism, Proteins metabolism

Published

2015

105. Azide-alkyne cycloaddition-mediated cyclization of phosphonopeptides and their evaluation as PTP1B binders and enrichment tools.

Author

Meyer C, Hoeger B, Chatterjee J, and Köhn M

Subjects

Alkynes chemistry, Azides chemistry, Cycloaddition Reaction, Humans, Peptides, Cyclic chemical synthesis, Protein Tyrosine Phosphatase, Non-Receptor Type 1 metabolism, Protein Tyrosine Phosphatase, Non-Receptor Type 2 antagonists & inhibitors, Protein Tyrosine Phosphatase, Non-Receptor Type 2 metabolism, Peptides, Cyclic chemistry, Peptides, Cyclic pharmacology, Protein Tyrosine Phosphatase, Non-Receptor Type 1 antagonists & inhibitors

Abstract

Protein tyrosine phosphatases (PTPs) are important enzymes in health and disease, and chemical tools are crucial to understand and modulate their biological roles. PTP1B is involved in diabetes, obesity and cancer. One of the main challenges for the design of chemical tools for PTP1B is the homology to TCPTP, making tool selectivity a highly challenging task. Here, we aimed to study if azide-alkyne cycloaddition-mediated cyclization of a peptide inhibitor could increase its selectivity toward PTP1B over TCPTP, and if cyclic and linear peptide binders can be applied as enrichment tools of endogenous PTP1B. While the cyclization of the peptide binders did not improve the selectivity toward PTP1B over TCPTP, it enhanced strongly the efficiency to co-precipitate endogenous PTP1B out of cell lysates. Our results show that fine-tuning the molecular structure of peptidic pull-down baits can greatly enhance their efficiency compared to the parental peptide sequences., (Copyright © 2015 Elsevier Ltd. All rights reserved.)

Published

2015

106. Synthesis of hydrolysis-resistant pyridoxal 5'-phosphate analogs and their biochemical and X-ray crystallographic characterization with the pyridoxal phosphatase chronophin.

Author

Knobloch G, Jabari N, Stadlbauer S, Schindelin H, Köhn M, and Gohla A

Subjects

Animals, Crystallography, X-Ray, Enzyme Inhibitors chemical synthesis, Hydrolysis, Mice, Molecular Docking Simulation, Phosphoprotein Phosphatases, Phosphoric Monoester Hydrolases chemistry, Pyridoxal Phosphate chemical synthesis, Enzyme Inhibitors chemistry, Enzyme Inhibitors pharmacology, Phosphoric Monoester Hydrolases antagonists & inhibitors, Phosphoric Monoester Hydrolases metabolism, Pyridoxal Phosphate analogs & derivatives, Pyridoxal Phosphate pharmacology

Abstract

A set of phosphonic acid derivatives (1-4) of pyridoxal 5'-phosphate (PLP) was synthesized and characterized biochemically using purified murine pyridoxal phosphatase (PDXP), also known as chronophin. The most promising compound 1 displayed primarily competitive PDXP inhibitory activity with an IC50 value of 79μM, which was in the range of the Km of the physiological substrate PLP. We also report the X-ray crystal structure of PDXP bound to compound 3, which we solved to 2.75Å resolution (PDB code 5AES). The co-crystal structure proves that compound 3 binds in the same orientation as PLP, and confirms the mode of inhibition to be competitive. Thus, we identify compound 1 as a PDXP phosphatase inhibitor. Our results suggest a strategy to design new, potent and selective PDXP inhibitors, which may be useful to increase the sensitivity of tumor cells to treatment with cytotoxic agents., (Copyright © 2015 Elsevier Ltd. All rights reserved.)

Published

2015

107. VHR/DUSP3 phosphatase: structure, function and regulation.

Author

Pavic K, Duan G, and Köhn M

Subjects

Animals, Humans, Mitogen-Activated Protein Kinases metabolism, Neoplasms enzymology, Neoplasms metabolism, Signal Transduction physiology, Dual Specificity Phosphatase 3 metabolism

Abstract

Vaccinia H1-related (VHR) phosphatase, also known as dual-specificity phosphatase (DUSP) 3, is a small member of the DUSP (also called DSP) family of phosphatases. VHR has a preference for phospho-tyrosine substrates, and has important roles in cellular signaling ranging from cell-cycle regulation and the DNA damage response to MAPK signaling, platelet activation and angiogenesis. VHR/DUSP3 has been implicated in several human cancers, where its tumor-suppressing and -promoting properties have been described. We give a detailed overview of VHR/DUSP3 phosphatase and compare it with its most closely related phosphatases DUSP13B, DUSP26 and DUSP27., (© 2015 The Authors. FEBS Journal published by John Wiley & Sons Ltd on behalf of FEBS.)

Published

2015

108. The human DEPhOsphorylation database DEPOD: a 2015 update.

Author

Duan G, Li X, and Köhn M

Subjects

Humans, Internet, Phosphoprotein Phosphatases metabolism, Phosphoric Monoester Hydrolases chemistry, Phosphoric Monoester Hydrolases classification, Protein Processing, Post-Translational, Databases, Protein, Phosphoric Monoester Hydrolases metabolism

Abstract

Phosphatases are crucial enzymes in health and disease, but the knowledge of their biological roles is still limited. Identifying substrates continues to be a great challenge. To support the research on phosphatase-kinase-substrate networks we present here an update on the human DEPhOsphorylation Database: DEPOD (http://www.depod.org or http://www.koehn.embl.de/depod). DEPOD is a manually curated open access database providing human phosphatases, their protein and non-protein substrates, dephosphorylation sites, pathway involvements and external links to kinases and small molecule modulators. All internal data are fully searchable including a BLAST application. Since the first release, more human phosphatases and substrates, their associated signaling pathways (also from new sources), and interacting proteins for all phosphatases and protein substrates have been added into DEPOD. The user interface has been further optimized; for example, the interactive human phosphatase-substrate network contains now a 'highlight node' function for phosphatases, which includes the visualization of neighbors in the network., (© The Author(s) 2014. Published by Oxford University Press on behalf of Nucleic Acids Research.)

Published

2015

109. Biochemical evaluation of virtual screening methods reveals a cell-active inhibitor of the cancer-promoting phosphatases of regenerating liver.

Author

Hoeger B, Diether M, Ballester PJ, and Köhn M

Subjects

Cell Movement drug effects, Cell Proliferation drug effects, Cell Survival drug effects, Cells, Cultured, Dose-Response Relationship, Drug, Enzyme Inhibitors chemistry, HEK293 Cells, Humans, Molecular Docking Simulation, Molecular Structure, Phosphoric Monoester Hydrolases metabolism, Small Molecule Libraries chemistry, Structure-Activity Relationship, Enzyme Inhibitors pharmacology, High-Throughput Screening Assays, Liver enzymology, Liver Regeneration, Neoplasms enzymology, Neoplasms pathology, Phosphoric Monoester Hydrolases antagonists & inhibitors, Small Molecule Libraries pharmacology

Abstract

Computationally supported development of small molecule inhibitors has successfully been applied to protein tyrosine phosphatases in the past, revealing a number of cell-active compounds. Similar approaches have also been used to screen for small molecule inhibitors for the cancer-related phosphatases of regenerating liver (PRL) family. Still, selective and cell-active compounds are of limited availability. Since especially PRL-3 remains an attractive drug target due to its clear role in cancer metastasis, such compounds are highly demanded. In this study, we investigated various virtual screening approaches for their applicability to identify novel small molecule entities for PRL-3 as target. Biochemical evaluation of purchasable compounds revealed ligand-based approaches as well suited for this target, compared to docking-based techniques that did not perform well in this context. The best hit of this study, a 2-cyano-2-ene-ester and hence a novel chemotype targeting the PRLs, was further optimized by a structure-activity-relationship (SAR) study, leading to a low micromolar PRL inhibitor with acceptable selectivity over other protein tyrosine phosphatases. The compound is active in cells, as shown by its ability to specifically revert PRL-3 induced cell migration, and exhibits similar effects on PRL-1 and PRL-2. It is furthermore suitable for fluorescence microscopy applications, and it is commercially available. These features make it the only purchasable, cell-active and acceptably selective PRL inhibitor to date that can be used in various cellular applications., (Copyright © 2014 The Authors. Published by Elsevier Masson SAS.. All rights reserved.)

Published

2014

110. Building up a chemical proteomics network in Europe and beyond.

Author

Köhn M, Meijler MM, and Kaiser M

Subjects

Europe, Proteomics

Published

2014

111. Unnatural amino acid mutagenesis reveals dimerization as a negative regulatory mechanism of VHR's phosphatase activity.

Author

Pavic K, Rios P, Dzeyk K, Koehler C, Lemke EA, and Köhn M

Subjects

Animals, Benzophenones chemistry, COS Cells, Catalytic Domain, Chlorocebus aethiops, Cross-Linking Reagents chemistry, Dual Specificity Phosphatase 3 chemistry, Dual Specificity Phosphatase 3 genetics, Enzyme Activation, Humans, Models, Molecular, Mutagenesis, Mutation, Phenylalanine chemistry, Phenylalanine genetics, Phenylalanine metabolism, Photochemical Processes, Benzophenones metabolism, Dual Specificity Phosphatase 3 metabolism, Phenylalanine analogs & derivatives, Protein Multimerization

Abstract

Vaccinia H1-related (VHR) phosphatase is a dual specificity phosphatase that is required for cell-cycle progression and plays a role in cell growth of certain cancers. Therefore, it represents a potential drug target. VHR is structurally and biochemically well characterized, yet its regulatory principles are still poorly understood. Understanding its regulation is important, not only to comprehend VHR's biological mechanisms and roles but also to determine its potential and druggability as a target in cancer. Here, we investigated the functional role of the unique "variable insert" region in VHR by selectively introducing the photo-cross-linkable amino acid para-benzoylphenylalanine (pBPA) using the amber suppression method. This approach led to the discovery of VHR dimerization, which was further confirmed using traditional chemical cross-linkers. Phe68 in VHR was discovered as a residue involved in the dimerization. We demonstrate that VHR can dimerize inside cells, and that VHR catalytic activity is reduced upon dimerization. Our results suggest that dimerization could occlude the active site of VHR, thereby blocking its accessibility to substrates. These findings indicate that the previously unknown transient self-association of VHR acts as a means for the negative regulation of its catalytic activity.

Published

2014

112. Dual-specificity phosphatases as molecular targets for inhibition in human disease.

Author

Ríos P, Nunes-Xavier CE, Tabernero L, Köhn M, and Pulido R

Subjects

Amino Acid Sequence, Dual-Specificity Phosphatases genetics, Dual-Specificity Phosphatases metabolism, Enzyme Inhibitors chemistry, Enzyme Inhibitors therapeutic use, Humans, Molecular Structure, Neoplasms metabolism, Sequence Alignment, Structure-Activity Relationship, Dual-Specificity Phosphatases antagonists & inhibitors, Enzyme Inhibitors pharmacology, Molecular Targeted Therapy, Neoplasms drug therapy, Neoplasms enzymology

Abstract

Significance: The dual-specificity phosphatases (DUSPs) constitute a heterogeneous group of cysteine-based protein tyrosine phosphatases, whose members exert a pivotal role in cell physiology by dephosphorylation of phosphoserine, phosphothreonine, and phosphotyrosine residues from proteins, as well as other non-proteinaceous substrates., Recent Advances: A picture is emerging in which a selected group of DUSP enzymes display overexpression or hyperactivity that is associated with human disease, especially human cancer, making feasible targeted therapy approaches based on their inhibition. A panoply of molecular and functional studies on DUSPs have been performed in the previous years, and drug-discovery efforts are ongoing to develop specific and efficient DUSP enzyme inhibitors. This review summarizes the current status on inhibitory compounds targeting DUSPs that belong to the MAP kinase phosphatases-, small-sized atypical-, and phosphatases of regenerating liver subfamilies, whose inhibition could be beneficial for the prevention or mitigation of human disease., Critical Issues: Achieving specificity, potency, and bioavailability are the major challenges in the discovery of DUSP inhibitors for the clinics. Clinical validation of compounds or alternative inhibitory strategies of DUSP inhibition has yet to come., Future Directions: Further work is required to understand the dual role of many DUSPs in human cancer, their function-structure properties, and to identify their physiologic substrates. This will help in the implementation of therapies based on DUSPs inhibition.

Published

2014

113. Development of accessible peptidic tool compounds to study the phosphatase PTP1B in intact cells.

Author

Meyer C, Hoeger B, Temmerman K, Tatarek-Nossol M, Pogenberg V, Bernhagen J, Wilmanns M, Kapurniotu A, and Köhn M

Subjects

Amino Acid Sequence, Binding Sites, CSK Tyrosine-Protein Kinase, Cell Line, Tumor, Cell Proliferation drug effects, Cell-Penetrating Peptides chemistry, Cell-Penetrating Peptides toxicity, Crystallography, X-Ray, Enzyme Inhibitors toxicity, Fluorescence Polarization, Humans, Models, Molecular, Molecular Sequence Data, Peptides toxicity, Protein Binding, Protein Tyrosine Phosphatase, Non-Receptor Type 1 chemistry, Substrate Specificity, src-Family Kinases antagonists & inhibitors, src-Family Kinases chemistry, Computational Biology methods, Enzyme Inhibitors chemistry, Peptides chemistry, Protein Tyrosine Phosphatase, Non-Receptor Type 1 antagonists & inhibitors

Abstract

Protein tyrosine phosphatases (PTPs) play crucial roles in health and disease. Chemical modulators of their activity are vital tools to study their function. An important aspect is the accessibility of these tools, which is usually limited or not existent due to the required, often complex synthesis of the molecules. We describe here a strategy for the development of cellular active inhibitors and in-cell detection tools for PTP1B as a model PTP, which plays important roles in diabetes, obesity, and cancer. The tool compounds are based on a peptide sequence from PTP1B's substrate Src, and the resulting compounds are commercially accessible through standard peptide synthesis. The peptide inhibitor is remarkably selective against a panel of PTPs. We provide the co-crystal structure of PTP1B with the sequence from Src and the optimized peptide inhibitor, showing the molecular basis of the interaction of PTP1B with part of its natural substrate and explaining the crucial interactions to enhance binding affinity, which are made possible by simple optimization of the sequence. Our approach enables the broad accessibility of PTP1B tools to researchers and has the potential for the systematic development of accessible PTP modulators to enable the study of PTPs.

Published

2014

114. Medical yoga: another way of being in the world-a phenomenological study from the perspective of persons suffering from stress-related symptoms.

Author

Anderzén-Carlsson A, Persson Lundholm U, Köhn M, and Westerdahl E

Subjects

Adult, Female, Humans, Interviews as Topic methods, Male, Middle Aged, Quality of Life psychology, Self Concept, Sweden, Treatment Outcome, Stress, Psychological psychology, Stress, Psychological therapy, Yoga psychology

Abstract

The prevalence of stress-related illness has grown in recent years. Many of these patients seek help in primary health care. Yoga can reduce stress and thus complements pharmacological therapy in medical practice. To our knowledge, no studies have investigated patients' experiences of yoga treatment in a primary health care setting or, specifically, the experiences of yoga when suffering from stress-related illness. Thus, the aim of the present study was to explore the meaning of participating in medical yoga as a complementary treatment for stress-related symptoms and diagnosis in a primary health care setting. This study has a descriptive phenomenological design and took place at a primary health care centre in Sweden during 2011. Five women and one man (43-51 years) participated. They were recruited from the intervention group (n=18) in a randomized control trial, in which they had participated in a medical yoga group in addition to standard care for 12 weeks. Data were collected by means of qualitative interviews, and a phenomenological data analysis was conducted. The essential meaning of the medical yoga experience was that the medical yoga was not an endpoint of recovery but the start of a process towards an increased sense of wholeness. It was described as a way of alleviating suffering, and it provided the participants with a tool for dealing with their stress and current situation on a practical level. It led to greater self-awareness and self-esteem, which in turn had an implicit impact on their lifeworld. In phenomenological terms, this can be summarized as Another way of being in the world, encompassing a perception of deepened identity. From a philosophical perspective, due to using the body in a new way (yoga), the participants had learnt to see things differently, which enriched and recast their perception of themselves and their lives.

Published

2014

115. Chemical activators of protein phosphatase-1 induce calcium release inside intact cells.

Author

Reither G, Chatterjee J, Beullens M, Bollen M, Schultz C, and Köhn M

Subjects

Amino Acid Sequence, Calcineurin chemistry, Calcineurin metabolism, HeLa Cells, Humans, Molecular Sequence Data, Peptides chemical synthesis, Peptides chemistry, Peptides metabolism, Protein Binding, Protein Phosphatase 1 chemistry, Protein Phosphatase 2 chemistry, Protein Phosphatase 2 metabolism, Calcium metabolism, Protein Phosphatase 1 metabolism

Abstract

Protein phosphatase-1 (PP1) is a major Ser/Thr phosphatase that is involved in numerous cellular processes. PP1-disrupting peptides (PDPs) are selective chemical tools used to study PP1. They generate catalytically active PP1 inside cells but do not bind to the closely related PP2A. Here, we show that PDPs also do not act directly on PP2B, thus demonstrating the selectivity of PDPs toward PP1. We present PDPs with different properties, enabling reversible versus permanent activation of PP1. We also show that Ca(2+) spiking is an acute effect caused by PDP-induced activation of PP1. The Ca(2+) is released from internal stores. Our data show that PDPs can be used as selective chemical genetics tools to study acute and long-term effects of PP1 activation in intact cells, and PDPs will therefore be valuable tools to study PP1 biology., (Copyright © 2013 Elsevier Ltd. All rights reserved.)

Published

2013

116. Insulin-like growth factor 2 mRNA-binding proteins (IGF2BPs): post-transcriptional drivers of cancer progression?

Author

Bell JL, Wächter K, Mühleck B, Pazaitis N, Köhn M, Lederer M, and Hüttelmaier S

Subjects

Cell Movement physiology, Cell Polarity physiology, Cytoplasmic Granules metabolism, Humans, Multigene Family genetics, Neoplasms metabolism, Neurons physiology, Proto-Oncogene Proteins c-myc metabolism, RNA-Binding Proteins genetics, Ribonucleoproteins metabolism, beta Catenin metabolism, Embryonic Development physiology, Gene Expression Regulation, Neoplastic physiology, Models, Biological, Neoplasms physiopathology, RNA, Messenger metabolism, RNA-Binding Proteins metabolism

Abstract

The insulin-like growth factor-2 mRNA-binding proteins 1, 2, and 3 (IGF2BP1, IGF2BP2, IGF2BP3) belong to a conserved family of RNA-binding, oncofetal proteins. Several studies have shown that these proteins act in various important aspects of cell function, such as cell polarization, migration, morphology, metabolism, proliferation and differentiation. In this review, we discuss the IGF2BP family's role in cancer biology and how this correlates with their proposed functions during embryogenesis. IGF2BPs are mainly expressed in the embryo, in contrast with comparatively lower or negotiable levels in adult tissues. IGF2BP1 and IGF2BP3 have been found to be re-expressed in several aggressive cancer types. Control of IGF2BPs' expression is not well understood; however, let-7 microRNAs, β-catenin (CTNNB1) and MYC have been proposed to be involved in their regulation. In contrast to many other RNA-binding proteins, IGF2BPs are almost exclusively observed in the cytoplasm where they associate with target mRNAs in cytoplasmic ribonucleoprotein complexes (mRNPs). During development, IGF2BPs are required for proper nerve cell migration and morphological development, presumably involving the control of cytoskeletal remodeling and dynamics, respectively. Likewise, IGF2BPs modulate cell polarization, adhesion and migration in tumor-derived cells. Moreover, they are highly associated with cancer metastasis and the expression of oncogenic factors (KRAS, MYC and MDR1). However, a pro-metastatic role of IGF2BPs remains controversial due to the lack of 'classical' in vivo studies. Nonetheless, IGF2BPs could provide valuable targets in cancer treatment with many of their in vivo roles to be fully elucidated.

Published

2013

117. Subcellular localization and RNP formation of IGF2BPs (IGF2 mRNA-binding proteins) is modulated by distinct RNA-binding domains.

Author

Wächter K, Köhn M, Stöhr N, and Hüttelmaier S

Subjects

Animals, Cell Line, Chickens, Humans, Mutation, Protein Structure, Tertiary, RNA-Binding Proteins genetics, Insulin-Like Growth Factor II metabolism, RNA, Messenger metabolism, RNA-Binding Proteins analysis, RNA-Binding Proteins metabolism, Ribonucleoproteins metabolism

Abstract

The IGF2 mRNA-binding protein family (IGF2BPs) directs the cytoplasmic fate of various target mRNAs and controls essential cellular functions. The three IGF2BP paralogues expressed in mammals comprise two RNA-recognition motifs (RRM) as well as four KH domains. How these domains direct IGF2BP paralogue-dependent protein function remains largely elusive. In this study, we analyze the role of KH domains in IGF2BPs by the mutational GXXG-GEEG conversion of single KH domain loops in the context of full-length polypeptides. These analyses reveal that all four KH domains of IGF2BP1 and IGF2BP2 are essentially involved in RNA-binding in vitro and the cellular association with RNA-binding proteins (RBPs). Moreover the KH domains prevent the nuclear accumulation of these two paralogues and facilitate their recruitment to stress granules. The role of KH domains appears less pronounced in IGF2BP3, because GxxG-GEEG conversion in all four KH domains only modestly affects RNA-binding, subcellular localization and RNA-dependent protein association of this paralogue. These findings indicate paralogue-dependent RNA-binding properties of IGF2BPs which likely direct distinct cellular functions. Our findings suggest that IGF2BPs contact target RNAs via all four KH domains. This implies significant structural constraints, which presumably allow the formation of exceedingly stable protein-RNA complexes.

Published

2013

118. Targeting the untargetable: recent advances in the selective chemical modulation of protein phosphatase-1 activity.

Author

Chatterjee J and Köhn M

Subjects

Enzyme Activation drug effects, Enzyme Inhibitors pharmacology, Protein Phosphatase 1 antagonists & inhibitors, Protein Phosphatase 1 chemistry, Drug Discovery methods, Protein Phosphatase 1 metabolism

Abstract

Protein phosphatase-1 (PP1) has long been neglected as a potential drug target owing to its misinterpreted unselective nature. However, growing evidence demonstrates that PP1 is highly selective in complex with regulatory proteins at the holoenzyme level, each of which is involved in different essential cellular signaling events. Here we summarize promising approaches to specifically activate or inhibit PP1 activity, and discuss remaining challenges and potential solutions. The summarized chemical tools pave the way for a better understanding of PP1's role in signaling networks, and the effects resulting from their application suggest their potential as future therapeutic candidates., (Copyright © 2013 Elsevier Ltd. All rights reserved.)

Published

2013

119. Elucidating human phosphatase-substrate networks.

Author

Li X, Wilmanns M, Thornton J, and Köhn M

Subjects

Databases, Protein, Humans, Phosphorylation physiology, Sequence Analysis, Protein, Models, Biological, Phosphoric Monoester Hydrolases metabolism, Systems Biology

Abstract

Phosphatases are crucially involved in cellular processes by dephosphorylating cellular components. We describe a structure-based classification scheme for all active human phosphatases that reveals previously unrecognized relationships between them. By collating protein and nonprotein substrates and integrating colocalization and coexpression data, we generated a human phosphatase-substrate network. Analysis of the protein sequences surrounding sites of dephosphorylation suggested that common recognition mechanisms may apply to both kinases and a subset of phosphatases. Analysis of three-dimensional substrate recognition by protein phosphatases revealed preferred domains in the substrates. We identified phosphatases with highly specific substrates and those with less specificity by examining the relationship between phosphatases, kinases, and their shared substrates and showed how this analysis can be used to generate testable hypotheses about phosphatase biological function. DEPOD (human DEPhOsphorylation Database, version 1.0, http://www.DEPOD.org) is an online resource with information about active human phosphatases, their substrates, and the pathways in which they function. The database includes links to kinases and chemical modulators of phosphatase activity and contains a sequence similarity search function for identifying related proteins in other species.

Published

2013

120. Why YRNAs? About Versatile RNAs and Their Functions.

Author

Köhn M, Pazaitis N, and Hüttelmaier S

Abstract

Y RNAs constitute a family of highly conserved small noncoding RNAs (in humans: 83-112 nt; Y1, Y3, Y4 and Y5). They are transcribed from individual genes by RNA-polymerase III and fold into conserved stem-loop-structures. Although discovered 30 years ago, insights into the cellular and physiological role of Y RNAs remains incomplete. In this review, we will discuss knowledge on the structural properties, associated proteins and discuss proposed functions of Y RNAs. We suggest Y RNAs to be an integral part of ribonucleoprotein networks within cells and could therefore have substantial influence on many different cellular processes. Putative functions of Y RNAs include small RNA quality control, DNA replication, regulation of the cellular stress response and proliferation. This suggests Y RNAs as essential regulators of cell fate and indicates future avenues of research, which will provide novel insights into the role of small noncoding RNAs in gene expression.

Published

2013

121. Challenges and opportunities in the development of protein phosphatase-directed therapeutics.

Author

De Munter S, Köhn M, and Bollen M

Subjects

Humans, Phosphoprotein Phosphatases chemistry, Phosphoprotein Phosphatases metabolism, Small Molecule Libraries chemistry, Small Molecule Libraries pharmacology, Drug Delivery Systems trends, Phosphoprotein Phosphatases antagonists & inhibitors

Abstract

Protein phosphatases have both protective and promoting roles in the etiology of diseases. A prominent example is the existence of oncogenic as well as tumor-suppressing protein phosphatases. A few protein phosphatase activity modulators are already applied in therapies. These were however not developed in target-directed approaches, and the recent discovery of phosphatase involvement followed their application in therapy. Nevertheless, these examples demonstrate that small molecules can be generated that modulate the activity of protein phosphatases and are beneficial for the treatment of protein phosphorylation diseases. We describe here strategies for the development of activators and inhibitors of protein phosphatases and clarify some long-standing misconceptions concerning the druggability of these enzymes. Recent developments suggest that it is feasible to design potent and selective protein phosphatase modulators with a therapeutic potential.

Published

2013

122. Medical yoga for patients with stress-related symptoms and diagnoses in primary health care: a randomized controlled trial.

Author

Köhn M, Persson Lundholm U, Bryngelsson IL, Anderzén-Carlsson A, and Westerdahl E

Abstract

An increasing number of patients are suffering from stress-related symptoms and diagnoses. The purpose of this study was to evaluate the medical yoga treatment in patients with stress-related symptoms and diagnoses in primary health care. A randomized controlled study was performed at a primary health care centre in Sweden from March to June, 2011. Patients were randomly allocated to a control group receiving standard care or a yoga group treated with medical yoga for 1 hour, once a week, over a 12-week period in addition to the standard care. A total of 37 men and women, mean age of 53 ± 12 years were included. General stress level (measured using Perceived Stress Scale (PSS)), burnout (Shirom-Melamed Burnout Questionnaire (SMBQ)), anxiety and depression (Hospital Anxiety and Depression Scale (HADS)), insomnia severity (Insomnia Severity Index (ISI)), pain (visual analogue scale (VAS)), and overall health status (Euro Quality of Life VAS (EQ-VAS)) were measured before and after 12 weeks. Patients assigned to the Yoga group showed significantly greater improvements on measures of general stress level (P < 0.000), anxiety (P < 0.019), and overall health status (P < 0.018) compared to controls. Treatment with medical yoga is effective in reducing levels of stress and anxiety in patients with stress-related symptoms in primary health care.

Published

2013

123. Molecular mechanisms of the PRL phosphatases.

Author

Rios P, Li X, and Köhn M

Subjects

Amino Acid Sequence, Cell Cycle Proteins chemistry, Cell Cycle Proteins genetics, Humans, Membrane Proteins chemistry, Membrane Proteins genetics, Models, Molecular, Molecular Sequence Data, Neoplasm Proteins chemistry, Neoplasm Proteins genetics, Protein Structure, Tertiary, Protein Tyrosine Phosphatases chemistry, Protein Tyrosine Phosphatases genetics, Sequence Homology, Amino Acid, Cell Cycle Proteins metabolism, Membrane Proteins metabolism, Neoplasm Proteins metabolism, Protein Tyrosine Phosphatases metabolism, Signal Transduction

Abstract

The phosphatases of regenerating liver (PRLs) are an intriguing family of dual specificity phosphatases due to their oncogenicity. The three members are small, single domain enzymes. We provide an overview of the phosphatases of regenerating liver, compare them to related phosphatases, and review recent reports about each phosphatase. Finally, we discuss similarities and differences between the phosphatases of regenerating liver, focusing on their molecular mechanisms and signalling pathways., (© 2012 The Authors Journal compilation © 2012 FEBS.)

Published

2013

124. Development of a peptide that selectively activates protein phosphatase-1 in living cells.

Author

Chatterjee J, Beullens M, Sukackaite R, Qian J, Lesage B, Hart DJ, Bollen M, and Köhn M

Subjects

Amino Acid Sequence, Cell Line, Tumor, Cell Membrane Permeability, Enzyme Activators pharmacology, Humans, Microscopy, Confocal, Models, Molecular, Molecular Sequence Data, Drug Design, Osteosarcoma drug therapy, Peptides pharmacology, Protein Phosphatase 1 metabolism

Published

2012

125. A molecular tête-à-tête arranged by a designed adaptor protein.

Author

Meyer C and Köhn M

Subjects

Membrane Proteins chemical synthesis, Membrane Proteins chemistry, Protein Binding, Signal Transduction, Membrane Proteins metabolism

Published

2012

126. Chemical biology techniques unlock the secrets of casein kinase 2 regulation by phosphorylation and glycosylation.

Author

Pavic K and Köhn M

Subjects

Casein Kinase II chemistry, Glycosylation, Humans, Phosphorylation, Biology methods, Casein Kinase II metabolism, Chemistry methods

Abstract

The key to understanding: The application of expressed protein ligation and protein microarrays enabled an unparalleled insight into the complex interaction of phosphorylation and glycosylation on casein kinase 2 and its biological outcome., (Copyright © 2012 WILEY-VCH Verlag GmbH & Co. KGaA, Weinheim.)

Published

2012

127. Omics and chemical biology--a powerful synergism.

Author

Köhn M

Subjects

Proteins chemistry, Proteins genetics, Proteins metabolism, Genomics methods, Periodicals as Topic

Published

2012

128. IGF2BP1 promotes cell migration by regulating MK5 and PTEN signaling.

Author

Stöhr N, Köhn M, Lederer M, Glass M, Reinke C, Singer RH, and Hüttelmaier S

Subjects

Actins metabolism, Cell Line, Tumor, Cell Movement, Cell Polarity physiology, Enzyme Activation, Extracellular Signal-Regulated MAP Kinases metabolism, HSP27 Heat-Shock Proteins metabolism, Heat-Shock Proteins, Humans, Molecular Chaperones, Phosphorylation, RNA, Messenger metabolism, Intracellular Signaling Peptides and Proteins metabolism, PTEN Phosphohydrolase metabolism, Protein Serine-Threonine Kinases metabolism, Signal Transduction

Abstract

In primary neurons, the oncofetal RNA-binding protein IGF2BP1 (IGF2 mRNA-binding protein 1) controls spatially restricted β-actin (ACTB) mRNA translation and modulates growth cone guidance. In cultured tumor-derived cells, IGF2BP1 was shown to regulate the formation of lamellipodia and invadopodia. However, how and via which target mRNAs IGF2BP1 controls the motility of tumor-derived cells has remained elusive. In this study, we reveal that IGF2BP1 promotes the velocity and directionality of tumor-derived cell migration by determining the cytoplasmic fate of two novel target mRNAs: MAPK4 and PTEN. Inhibition of MAPK4 mRNA translation by IGF2BP1 antagonizes MK5 activation and prevents phosphorylation of HSP27, which sequesters actin monomers available for F-actin polymerization. Consequently, HSP27-ACTB association is reduced, mobilizing cellular G-actin for polymerization in order to promote the velocity of cell migration. At the same time, stabilization of the PTEN mRNA by IGF2BP1 enhances PTEN expression and antagonizes PIP(3)-directed signaling. This enforces the directionality of cell migration in a RAC1-dependent manner by preventing additional lamellipodia from forming and sustaining cell polarization intrinsically. IGF2BP1 thus promotes the velocity and persistence of tumor cell migration by controlling the expression of signaling proteins. This fine-tunes and connects intracellular signaling networks in order to enhance actin dynamics and cell polarization.

Published

2012

129. The metastasis-promoting phosphatase PRL-3 shows activity toward phosphoinositides.

Author

McParland V, Varsano G, Li X, Thornton J, Baby J, Aravind A, Meyer C, Pavic K, Rios P, and Köhn M

Subjects

Amino Acid Sequence, Catalysis, Cysteine genetics, Enzyme Activation genetics, Genetic Variation, HEK293 Cells, Humans, Molecular Sequence Data, Mutation genetics, Neoplasm Invasiveness genetics, Neoplasm Invasiveness pathology, Neoplasm Proteins genetics, Phosphatidylinositols chemistry, Protein Tyrosine Phosphatases genetics, Recombinant Proteins chemistry, Recombinant Proteins genetics, Serine genetics, Substrate Specificity genetics, Cell Movement genetics, Neoplasm Proteins chemistry, Neoplasm Proteins physiology, Phosphatidylinositols metabolism, Protein Tyrosine Phosphatases chemistry, Protein Tyrosine Phosphatases physiology

Abstract

Phosphatase of regenerating liver 3 (PRL-3) is suggested as a biomarker and therapeutic target in several cancers. It has a well-established causative role in cancer metastasis. However, little is known about its natural substrates, pathways, and biological functions, and only a few protein substrates have been suggested so far. To improve our understanding of the substrate specificity and molecular determinants of PRL-3 activity, the wild-type (WT) protein, two supposedly catalytically inactive mutants D72A and C104S, and the reported hyperactive mutant A111S were tested in vitro for substrate specificity and activity toward phosphopeptides and phosphoinositides (PIPs), their structural stability, and their ability to promote cell migration using stable HEK293 cell lines. We discovered that WT PRL-3 does not dephosphorylate the tested phosphopeptides in vitro. However, as shown by two complementary biochemical assays, PRL-3 is active toward the phosphoinositide PI(4,5)P(2). Our experimental results substantiated by molecular docking studies suggest that PRL-3 is a phosphatidylinositol 5-phosphatase. The C104S variant was shown to be not only catalytically inactive but also structurally destabilized and unable to promote cell migration, whereas WT PRL-3 promotes cell migration. The D72A mutant is structurally stable and does not dephosphorylate the unnatural substrate 3-O-methylfluorescein phosphate (OMFP). However, we observed residual in vitro activity of D72A against PI(4,5)P(2), and in accordance with this, it exhibits the same cellular phenotype as WT PRL-3. Our analysis of the A111S variant shows that the hyperactivity toward the unnatural OMFP substrate is not apparent in dephosphorylation assays with phosphoinositides: the mutant is completely inactive against PIPs. We observed significant structural destabilization of this variant. The cellular phenotype of this mutant equals that of the catalytically inactive C104S mutant. These results provide a possible explanation for the absence of the conserved Ser of the PTP catalytic motif in the PRL family. The correlation of the phosphatase activity toward PI(4,5)P(2) with the observed phenotypes for WT PRL-3 and the mutants suggests a link between the PI(4,5)P(2) dephosphorylation by PRL-3 and its role in cell migration.

Published

2011

130. Near-infrared (NIR) dye-labeled RNAs identify binding of ZBP1 to the noncoding Y3-RNA.

Author

Köhn M, Lederer M, Wächter K, and Hüttelmaier S

Subjects

Animals, Avian Proteins isolation & purification, Cell Line, Chickens, Electrophoretic Mobility Shift Assay, Humans, Immunoprecipitation, Protein Binding genetics, RNA-Binding Proteins isolation & purification, Avian Proteins metabolism, RNA, Small Cytoplasmic metabolism, RNA-Binding Proteins metabolism

Abstract

The analysis of protein-RNA association in vitro commonly involves radiolabeled in vitro transcribed RNAs. Nucleotides labeled with near-infrared (NIR) dyes provide promising alternatives for studying protein-RNA binding in vitro. However, it remained elusive whether random labeling of RNA probes by NIR dyes interferes with protein binding. Here, we demonstrate that infrared scanning allows the detection of randomly NIR-labeled RNA probes in the low femtomole range. The analyses of eight distinct protein-RNA complexes by electrophoretic mobility shift assay, filter binding, or UV crosslinking revealed that protein binding specificity remains unaffected by random NIR labeling. Accordingly, NIR probes allowed the rapid identification of the short noncoding Y3-RNA as a novel RNA target of ZBP1 (zipcode binding protein). Whereas binding of ZBP1 to the ACTB-zipcode and Y3 was exclusive, the protein formed a trimeric complex with the La protein and Y3. This was dissociated in the presence of Y5 RNA, resulting in the formation of ZBP1/Y3 and La/Y5 complexes. Hence, ZBP1 apparently resides in at least two distinct cellular RNPs: mRNA-containing mRNPs or Y3-containing yRNPs. In conclusion, our findings indicate that randomly labeled NIR probes provide a powerful tool for the rapid and sensitive analysis of protein-RNA binding in vitro. In contrast to radiolabeled RNAs, NIR probes remain stable for months, do not pose any safety considerations, and enable the significantly expedited analysis of experimental data due to fast read technologies available. The most prominent advantage of probes labeled by NIR dyes is the option to color-code distinct transcripts, allowing the unbiased identification of distinct protein-RNA complexes in one sample.

Published

2010

131. Preparation of biomolecule microstructures and microarrays by thiol-ene photoimmobilization.

Author

Weinrich D, Köhn M, Jonkheijm P, Westerlind U, Dehmelt L, Engelkamp H, Christianen PC, Kuhlmann J, Maan JC, Nüsse D, Schröder H, Wacker R, Voges E, Breinbauer R, Kunz H, Niemeyer CM, and Waldmann H

Subjects

Animals, Antibodies immunology, Antibodies metabolism, Glycopeptides chemistry, Glycopeptides metabolism, Immobilized Proteins chemistry, Immobilized Proteins metabolism, Light, Mice, Mucin-1 metabolism, Photochemical Processes, Ultraviolet Rays, Biotin chemistry, Microarray Analysis, Mucin-1 chemistry, Oligonucleotides chemistry, Sulfhydryl Compounds chemistry

Abstract

A mild, fast and flexible method for photoimmobilization of biomolecules based on the light-initiated thiol-ene reaction has been developed. After investigation and optimization of various surface materials, surface chemistries and reaction parameters, microstructures and microarrays of biotin, oligonucleotides, peptides, and MUC1 tandem repeat glycopeptides were prepared with this photoimmobilization method. Furthermore, MUC1 tandem repeat glycopeptide microarrays were successfully used to probe antibodies in mouse serum obtained from vaccinated mice. Dimensions of biomolecule microstructures were shown to be freely controllable through photolithographic techniques, and features down to 5 microm in size covering an area of up to 75x25 mm were created. Use of a confocal laser microscope with a UV laser as UV-light source enabled further reduction of biotin feature size opening access to nanostructured biochips.

Published

2010

132. Structure-activity analysis of semisynthetic nucleosomes: mechanistic insights into the stimulation of Dot1L by ubiquitylated histone H2B.

Author

McGinty RK, Köhn M, Chatterjee C, Chiang KP, Pratt MR, and Muir TW

Subjects

Animals, Histone-Lysine N-Methyltransferase, Histones chemistry, Histones genetics, Humans, Kinetics, Methylation, Methyltransferases genetics, Models, Molecular, Mutation, Protein Structure, Quaternary, Protein Structure, Tertiary, Histones metabolism, Methyltransferases metabolism, Nucleosomes metabolism, Ubiquitinated Proteins metabolism, Xenopus metabolism

Abstract

Post-translational modification of histones plays an integral role in regulation of genomic expression through modulation of chromatin structure and function. Chemical preparations of histones bearing these modifications allows for comprehensive in vitro mechanistic investigation into their action to deconvolute observations from genome-wide studies in vivo. Previously, we reported the semisynthesis of ubiquitylated histone H2B (uH2B) using two orthogonal expressed protein ligation reactions. Semisynthetic uH2B, when incorporated into nucleosomes, directly stimulates methylation of histone H3 lysine 79 (K79) by the methyltransferase, disruptor of telomeric silencing-like (Dot1L). Although recruitment of Dot1L to the nucleosomal surface by uH2B could be excluded, comprehensive mechanistic analysis was precluded by systematic limitations in the ability to generate uH2B in large scale. Here we report a highly optimized synthesis of ubiquitylated H2B bearing a G76A point mutation u(G76A)H2B, yielding tens of milligrams of ubiquitylated protein. u(G76A)H2B is indistinguishable from the native uH2B by Dot1L, allowing for detailed studies of the resultant trans-histone crosstalk. Kinetic and structure-activity relationship analyses using u(G76A)H2B suggest a noncanonical role for ubiquitin in the enhancement of the chemical step of H3K79 methylation. Furthermore, titration of the level of uH2B within the nucleosome revealed a 1:1 stoichiometry of Dot1L activation.

Published

2009

133. Immobilization strategies for small molecule, peptide and protein microarrays.

Author

Köhn M

Subjects

Models, Theoretical, Peptides chemistry, Proteins chemistry, Substrate Specificity, Microarray Analysis methods, Peptides analysis, Protein Array Analysis methods, Proteins analysis

Abstract

Protein, peptide and small molecule microarrays are valuable tools in biological research. In the last decade, substantial progress has been achieved to make these powerful technologies more reliable and available for researchers. This review describes chemical preparation methods for these microarrays with focus on site-selective and bioorthogonal immobilization reactions, particularly the Staudinger ligation and the thiol-ene reaction. In addition, the application of peptide microarrays, which were prepared by Staudinger ligation, to substrate specificity mapping is illustrated.

Published

2009

134. Chemical biologists gather in Heidelberg.

Author

Köhn M and Schultz C

Subjects

Drug Design, Germany, Peptides chemistry, Protein Engineering, Biochemistry

Abstract

Chemical biology is well defined at its core--chemistry helping to answer biological questions--yet the boundaries are rather fuzzy. What are the differences between chemical biology and pharmacology? Is intracellular imaging a branch of chemical biology, and what about screening libraries? At Chemical Biology 2008, held in Heidelberg in October, participants heard presentations covering all these topics and more.

Published

2009

135. Control of c-myc mRNA stability by IGF2BP1-associated cytoplasmic RNPs.

Author

Weidensdorfer D, Stöhr N, Baude A, Lederer M, Köhn M, Schierhorn A, Buchmeier S, Wahle E, and Hüttelmaier S

Subjects

Binding Sites, Cell Line, Tumor, Cells, Cultured, DNA-Binding Proteins genetics, DNA-Binding Proteins metabolism, Fluorescent Antibody Technique, Heterogeneous-Nuclear Ribonucleoproteins genetics, Heterogeneous-Nuclear Ribonucleoproteins metabolism, Humans, Nuclear Proteins genetics, Nuclear Proteins metabolism, Proto-Oncogene Proteins c-myc metabolism, RNA Stability, RNA, Messenger genetics, RNA-Binding Proteins genetics, Transfection, Y-Box-Binding Protein 1, Cytoplasm metabolism, Proto-Oncogene Proteins c-myc genetics, RNA, Messenger metabolism, RNA-Binding Proteins metabolism, Ribonucleoproteins metabolism

Abstract

The RNA-binding protein IGF2BP1 (IGF-II mRNA binding protein 1) stabilizes the c-myc RNA by associating with the Coding Region instability Determinant (CRD). If and how other proteins cooperate with IGF2BP1 in promoting stabilization of the c-myc mRNA via the CRD remained elusive. Here, we identify various RNA-binding proteins that associate with IGF2BP1 in an RNA-dependent fashion. Four of these proteins (HNRNPU, SYNCRIP, YBX1, and DHX9) were essential to ensure stabilization of the c-myc mRNA via the CRD. These factors associate with IGF2BP1 in a CRD-dependent manner, co-distribute with IGF2BP1 in non-polysomal fractions comprising c-myc mRNA, and colocalize with IGF2BP1 in the cytoplasm. A selective shift of relative c-myc mRNA levels to the polysomal fraction is observed upon IGF2BP1 knockdown. These findings suggest that IGF2BP1 in complex with at least four proteins promotes CRD-mediated mRNA stabilization. Complex formation at the CRD presumably limits the transfer of c-myc mRNA to the polysomal fraction and subsequent translation-coupled decay.

Published

2009

136. Simultaneous protein tagging in two colors.

Author

Schultz C and Köhn M

Subjects

Alkyl and Aryl Transferases chemistry, Alkyl and Aryl Transferases metabolism, Fluorescent Dyes analysis, Models, Molecular, Protein Structure, Tertiary, Proteins chemistry, Color, Proteins metabolism, Staining and Labeling methods

Abstract

The fluorescent tagging of proteins in the natural environment of the cell is an emerging technique in cell biology. In this issue of Chemistry & Biology, Gautier et al. introduce a fluorescent labeling procedure orthogonal to existing ones, enabling tagging of two different proteins in living cells.

Published

2008

137. Photochemical surface patterning by the thiol-ene reaction.

Author

Jonkheijm P, Weinrich D, Köhn M, Engelkamp H, Christianen PC, Kuhlmann J, Maan JC, Nüsse D, Schroeder H, Wacker R, Breinbauer R, Niemeyer CM, and Waldmann H

Subjects

Surface Properties, Alkenes chemistry, Photochemistry methods, Proteins chemistry, Sulfhydryl Compounds chemistry

Published

2008

138. A microarray strategy for mapping the substrate specificity of protein tyrosine phosphatase.

Author

Köhn M, Gutierrez-Rodriguez M, Jonkheijm P, Wetzel S, Wacker R, Schroeder H, Prinz H, Niemeyer CM, Breinbauer R, Szedlacsek SE, and Waldmann H

Subjects

Amino Acids chemistry, Binding Sites, Color, Models, Molecular, Molecular Structure, Peptides chemistry, Phosphotyrosine chemistry, Substrate Specificity, Protein Array Analysis methods, Protein Tyrosine Phosphatases chemistry, Protein Tyrosine Phosphatases metabolism

Published

2007

139. A generic building block for C- and N-terminal protein-labeling and protein-immobilization.

Author

Watzke A, Gutierrez-Rodriguez M, Köhn M, Wacker R, Schroeder H, Breinbauer R, Kuhlmann J, Alexandrov K, Niemeyer CM, Goody RS, and Waldmann H

Subjects

Azides chemistry, Binding Sites, Fluorescent Dyes chemical synthesis, Maleimides chemical synthesis, Molecular Structure, Protein Conformation, Structure-Activity Relationship, ras Proteins chemistry, Fluorescent Dyes chemistry, GTP-Binding Proteins chemistry, Maleimides chemistry, Protein Engineering methods, Proteins chemistry

Abstract

Expressed protein ligation (EPL) and bioconjugation based on the maleimide group (MIC-conjugation) provide powerful tools for protein modification. In the light of the importance of site-selectively modified proteins for the study of protein function, a flexible method for the introduction of tags and reporter groups into the C-terminus of proteins employing EPL and MIC-conjugation was developed. We describe the solid-phase synthesis of a generic building block, equipped with fluorescence markers or different functional groups. This generic building block allows for a flexible incorporation of different tags into proteins and was used for the introduction of fluorescence markers into the C-terminus of Rab and Ras GTPases by EPL or MIC-conjugation techniques. In addition, a building block appropriately modified for the incorporation of an azide into proteins was synthesized. Azide-functionalized Ras protein was immobilized on a phosphane-modified surface by means of Staudinger ligation providing a highly chemoselective ligation method for the immobilization of proteins.

Published

2006

140. Site-selective protein immobilization by Staudinger ligation.

Author

Watzke A, Köhn M, Gutierrez-Rodriguez M, Wacker R, Schröder H, Breinbauer R, Kuhlmann J, Alexandrov K, Niemeyer CM, Goody RS, and Waldmann H

Subjects

Azides chemical synthesis, Binding Sites, Glass chemistry, Ligands, Molecular Conformation, Stereoisomerism, Surface Properties, Azides chemistry, Proteins chemistry

Published

2006

141. Diels-Alder ligation and surface immobilization of proteins.

Author

de Araújo AD, Palomo JM, Cramer J, Köhn M, Schröder H, Wacker R, Niemeyer C, Alexandrov K, and Waldmann H

Subjects

Models, Molecular, Molecular Conformation, Spectrometry, Mass, Matrix-Assisted Laser Desorption-Ionization, Proteins chemistry

Published

2005

142. The Staudinger ligation-a gift to chemical biology.

Author

Köhn M and Breinbauer R

Subjects

Genetic Engineering, History, 20th Century, Ligands, Peptides chemical synthesis, Azides chemistry, Chemistry, Organic history, Chemistry, Organic trends, Phosphines chemistry

Abstract

Although the reaction between an azide and a phosphane to form an aza-ylide was discovered by Hermann Staudinger more than 80 years ago and has found widespread application in organic synthesis, its potential as a highly chemoselective ligation method for the preparation of bioconjugates has been recognized only recently. As the two reaction partners are bioorthogonal to almost all functionalities that exist in biological systems and react at room temperature in an aqueous environment, the Staudinger ligation has even found application in the complex environment of living cells. Herein we describe the current state of knowledge on this reaction and its application both for the preparation of bioconjugates and as a ligation method in chemical biology.

Published

2004

143. Functional evaluation of carbohydrate-centred glycoclusters by enzyme-linked lectin assay: ligands for concanavalin A.

Author

Köhn M, Benito JM, Ortiz Mellet C, Lindhorst TK, and García Fernández JM

Subjects

Binding Sites, Carbohydrate Conformation, Carbohydrate Sequence, Carbohydrates chemistry, Glucose chemistry, Glucose metabolism, Lectins chemistry, Ligands, Mannose chemistry, Stereoisomerism, Thiourea chemistry, Carbohydrate Metabolism, Concanavalin A metabolism, Glycosides chemistry, Lectins metabolism, Mannose metabolism

Abstract

The affinities of the mannose-specific lectin concanavalin A (Con A) towards D-glucose-centred mannosyl clusters differing in the anomeric configuration of the monosaccharide core, nature of the bridging functional groups and valency, have been measured by a competitive enzyme-linked lectin assay. Pentavalent thioether-linked ligands (5 and 7) were prepared by radical addition of 2,3,4,6-tetra-O-acetyl-1-thio-alpha-D-mannopyranose to the corresponding penta-O-allyl-alpha- or -beta-D-glucopyranose, followed by deacetylation. The distinct reactivity of the anomeric position in the D-glucose scaffold was exploited in the preparation of a tetravalent cluster (10) that keeps a reactive aglyconic group for further manipulation, including incorporation of a reporter group or attachment to a solid support. Hydroboration of the double bonds in the penta-O-allyl-alpha-D-glucopyranose derivative and replacement of the hydroxy groups with amine moieties gave a suitable precursor for the preparation of pentavalent and 15-valent mannosides through the thiourea-bridging reaction (17 and 20, respectively). The diastereomeric 1-thiomannose-coated clusters 5 and 7 were demonstrated to be potent ligands for Con A, with IC(50) values for the inhibition of the Con A-yeast mannan association indicative of 6.4- and 5.5-fold increases in binding affinity (valency-corrected values), respectively, relative to the value for methyl alpha-D-mannopyranoside. The tetravalent cluster 10 exhibited a valency-corrected relative lectin-binding potency virtually identical to that of the homologous pentavalent mannoside 7. In sharp contrast, replacement of the 1-thiomannose wedges of 5 with alpha-D-mannopyranosylthioureido units (17) virtually abolished any multivalent or statistic effects, with a dramatic decrease of binding affinity. The 15-valent ligand 20, possessing classical O-glycosidic linkages, exhibited a twofold increase in lectin affinity relative to the penta-O-(thioglycoside) 5; it is less efficient based on the number of mannose units. The results illustrate the potential of carbohydrates as polyfunctional platforms for glycocluster construction and underline the importance of careful design of the overall architecture in optimising glycocluster recognition by specific lectins.

Published

2004

144. Azide-alkyne coupling: a powerful reaction for bioconjugate chemistry.

Author

Breinbauer R and Köhn M

Subjects

Animals, Catalysis, Molecular Structure, Alkynes chemistry, Azides chemistry, Cholinesterase Inhibitors chemistry

Published

2003

145. Staudinger ligation: a new immobilization strategy for the preparation of small-molecule arrays.

Author

Köhn M, Wacker R, Peters C, Schröder H, Soulère L, Breinbauer R, Niemeyer CM, and Waldmann H

Subjects

Biotin chemistry, Carbocyanines, Concanavalin A chemistry, Haptens chemistry, Immunoglobulin G chemistry, Molecular Structure, Molecular Weight, Streptavidin chemistry, Molecular Probe Techniques instrumentation

Published

2003