115 results on '"Hansen, Paul Robert"'
Search Results
2. Recent advances in the development of antimicrobial peptides against ESKAPE pathogens
- Author
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Roque-Borda, Cesar Augusto, Primo, Laura Maria Duran Gleriani, Franzyk, Henrik, Hansen, Paul Robert, and Pavan, Fernando Rogério
- Published
- 2024
- Full Text
- View/download PDF
3. Antimicrobial peptides grafted onto the surface of N-acetylcysteine-chitosan nanoparticles can revitalize drugs against clinical isolates of Mycobacterium tuberculosis
- Author
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Primo, Laura Maria Duran Gleriani, Roque-Borda, Cesar Augusto, Carnero Canales, Christian Shleider, Caruso, Icaro Putinhon, de Lourenço, Isabella Ottenio, Colturato, Vitória Maria Medalha, Sábio, Rafael Miguel, de Melo, Fernando Alves, Vicente, Eduardo Festozo, Chorilli, Marlus, da Silva Barud, Hernane, Barbugli, Paula Aboud, Franzyk, Henrik, Hansen, Paul Robert, and Pavan, Fernando Rogério
- Published
- 2024
- Full Text
- View/download PDF
4. Cyclic N-locked indolicidin analogues with antimicrobial activity: Effect of ring size and fatty acid acylation
- Author
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Lone, Abdullah, Nielsen, Josefine Eilsø, Thulstrup, Peter W., Lund, Reidar, Hansen, Paul Robert, and Jenssen, Håvard
- Published
- 2022
- Full Text
- View/download PDF
5. Halogenation as a tool to tune antimicrobial activity of peptoids
- Author
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Molchanova, Natalia, Nielsen, Josefine Eilsø, Sørensen, Kristian B., Prabhala, Bala Krishna, Hansen, Paul Robert, Lund, Reidar, Barron, Annelise E., and Jenssen, Håvard
- Published
- 2020
- Full Text
- View/download PDF
6. Rifampicin-loaded N-acetylcysteine-chitosan nanoparticles surface-grafted with a peptide exhibit potent activity against multidrug-resistant Mycobacterium tuberculosis
- Author
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Roque-Borda, Cesar Augusto, Primo, Laura Maria Duran Gleriani, Vicente, Eduardo Festozo, Barbugli, Paula Aboud, Franzyk, Henrik, Hansen, Paul Robert, and Pavan, Fernando Rogério
- Published
- 2023
7. Identification of continuous epitopes of HuD antibodies related to paraneoplastic diseases/small cell lung cancer
- Author
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Trier, Nicole Hartwig, Hansen, Paul Robert, Vedeler, Christian A., Somnier, Finn Engeborg, and Houen, Gunnar
- Published
- 2012
- Full Text
- View/download PDF
8. Antigenic Profiling of a Chlamydia trachomatis Gene-Expression Library
- Author
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Follmann, Frank, Olsen, Anja Weinreich, Jensen, Klaus Thorleif, Hansen, Paul Robert, Andersen, Peter, and Theisen, Michael
- Published
- 2008
- Full Text
- View/download PDF
9. Antibodies with specificity for native and denatured forms of ovalbumin differ in reactivity between enzyme-linked immunosorbent assays
- Author
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Holm, Bettina Eide, Bergmann, Ann Christina, Hansen, Paul Robert, Koch, Claus, Houen, Gunnar, and Trier, Nicole Hartwig
- Published
- 2015
- Full Text
- View/download PDF
10. Specificity of Anti-Citrullinated Protein Antibodies to Citrullinated α-Enolase Peptides as a Function of Epitope Structure and Composition
- Author
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Fanelli, Ilaria, Rovero, Paolo, Hansen, Paul Robert, Frederiksen, Jette, Houen, Gunnar, and Trier, Nicole Hartwig
- Subjects
anti-citrullinated protein antibodies ,citrullinated peptides ,epitopes ,rheumatoid arthritis - Published
- 2021
11. Production and Characterization of Peptide Antibodies to the C-Terminal of Frameshifted Calreticulin Associated with Myeloproliferative Diseases.
- Author
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Mughal, Farah Perveen, Bergmann, Ann Christina, Huynh, Ha Uyen Buu, Jørgensen, Sarah Hyllekvist, Mansha, Inaam, Kesmez, Meliha, Schürch, Patrick Mark, Theocharides, Alexandre Pierre André, Hansen, Paul Robert, Friis, Tina, Holmström, Morten Orebo, Ciplys, Evaldas, Slibinskas, Rimantas, Højrup, Peter, Houen, Gunnar, and Trier, Nicole Hartwig
- Subjects
CALRETICULIN ,BONE marrow cells ,PEPTIDES ,WESTERN immunoblotting ,ENZYME-linked immunosorbent assay ,IMMUNOGLOBULINS ,ERYTHROCYTES - Abstract
Myeloproliferative Neoplasms (MPNs) constitute a group of rare blood cancers that are characterized by mutations in bone marrow stem cells leading to the overproduction of erythrocytes, leukocytes, and thrombocytes. Mutations in calreticulin (CRT) genes may initiate MPNs, causing a novel variable polybasic stretch terminating in a common C-terminal sequence in the frameshifted CRT (CRTfs) proteins. Peptide antibodies to the mutated C-terminal are important reagents for research in the molecular mechanisms of MPNs and for the development of new diagnostic assays and therapies. In this study, eight peptide antibodies targeting the C-terminal of CRTfs were produced and characterised by modified enzyme-linked immunosorbent assays using resin-bound peptides. The antibodies reacted to two epitopes: CREACLQGWTE for SSI-HYB 385-01, 385-02, 385-03, 385-04, 385-07, 385-08, and 385-09 and CLQGWT for SSI-HYB 385-06. For the majority of antibodies, the residues Cys
1 , Trp9 , and Glu11 were essential for reactivity. SSI-HYB 385-06, with the highest affinity, recognised recombinant CRTfs produced in yeast and the MARIMO cell line expressing CRTfs when examined in Western immunoblotting. Moreover, SSI-HYB 385-06 occasionally reacted to CRTfs from MPN patients when analysed by flow cytometry. The characterized antibodies may be used to understand the role of CRTfs in the pathogenesis of MPNs and to design and develop new diagnostic assays and therapeutic targets. [ABSTRACT FROM AUTHOR]- Published
- 2022
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12. Fluorescent analogues of Human α-Calcitonin Gene-Related Peptide with vasodilator potency
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Zhu, Jing, Pedersen, Mahdieh Dagina, Ahmed, L. Sabbah, Abdolalizadeh, Bahareh, Grell, Anne-Sofie, Berg, Jais Oliver, Thulstrup, Peter Waaben, Franzyk, Henrik, Edvinsson, Lars, Sams, Anette, Sheykhzade, Majid, and Hansen, Paul Robert
- Abstract
Human α-calcitonin gene-related peptide (h-α-CGRP) is a highly potent vasodilator peptide that belongs to the family of calcitonin peptides. There are two forms of CGRP receptors in humans and rodents: α-CGRP receptor predominately found in the cardiovascular system and β-CGRP receptor predominating in the gastrointestinal tract. The CGRP receptors are primarily localized to C and Aδ sensory fibers, where they are involved in nociceptive transmission and migraine pathophysiology. These fibers are found both peripherally and centrally, with extensive perivascular location. The CGRP receptors belong to the class B G-protein-coupled receptors, and they are primarily associated to signaling via Gα proteins. The objectives of the present work were: (i) synthesis of three single-labelled fluorescent analogues of h-α-CGRP by 9-fluorenylmethyloxycarbonyl (Fmoc)-based solid-phase peptide synthesis, and (ii) testing of their biological activity in isolated human, mouse, and rat arteries by using a small-vessel myograph setup. The three analogues were labelled with 5(6)-carboxyfluorescein via the spacer 6-aminohexanoic acid at the chain of Lys24 or Lys35. Circular dichroism (CD) experiments were performed to obtain information on the secondary structure of these fluorescently labelled peptides. The CD spectra indicated that the folding of all three analogues was similar to that of native α-CGRP. The three fluorescent analogues of α-CGRP were successfully prepared with a purity of >95%. In comparison to α-CGRP, the three analogues exhibited similar efficacy, but different potency in producing a vasodilator effect. The analogue labelled at the N-terminus proved to be the most readily synthesized, but it was found to possess the lowest vasodilator potency. The analogues labelled at Lys35 or Lys24 exhibited an acceptable reduction in potency (i.e., 3-5 times and 5-10 times less potent, respectively), and thus they have potential for use in further investigations of receptor internalization and neuronal reuptake.
- Published
- 2020
13. Cross-reactivity of a human IgG1 anticitrullinated fibrinogen monoclonal antibody to a citrullinated profilaggrin peptide
- Author
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Trier, Nicole Hartwig, Leth, Maria Louise, Hansen, Paul Robert, and Houen, Gunnar
- Published
- 2012
- Full Text
- View/download PDF
14. Peptide Antibody Reactivity to Homologous Regions in Glutamate Decarboxylase Isoforms and Coxsackievirus B4 P2C.
- Author
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Trier, Nicole Hartwig, Valdarnini, Niccolo, Fanelli, Ilaria, Rovero, Paolo, Hansen, Paul Robert, Schafer-Nielsen, Claus, Ciplys, Evaldas, Slibinskas, Rimantas, Pociot, Flemming, Friis, Tina, and Houen, Gunnar
- Subjects
GLUTAMATE decarboxylase ,PEPTIDES ,MONOCLONAL antibodies ,STIFF-person syndrome ,TYPE 1 diabetes ,MOLECULAR mimicry - Abstract
Two isoforms of the glutamate decarboxylase (GAD) enzyme exist, GAD65 and GAD67, which are associated with type 1 diabetes (T1D) and stiff-person syndrome (SPS), respectively. Interestingly, it has been reported that T1D patients seldom develop SPS, whereas patients with SPS occasionally develop T1D. In addition, coxsackievirus B4 (CVB4) has previously been proposed to be involved in the onset of T1D through molecular mimicry. On this basis, we aimed to examine antibody cross-reactivity between a specific region of GAD65 and GAD67, which has high sequence homology to the nonstructural P2C protein of CVB4 to determine potential correlations at antibody level. Monoclonal peptide antibodies generated in mice specific for a region with high similarity in all three proteins were screened for reactivity along with human sera in immunoassays. In total, six antibodies were generated. Two of the antibodies reacted to both GAD isoforms. However, none of the antibodies were cross-reactive to CVB, suggesting that antibody cross-reactivity between GAD65 and CVB, and GAD67 and CVB may not contribute to the onset of T1D and SPS, respectively. [ABSTRACT FROM AUTHOR]
- Published
- 2022
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15. Identification of Amino Acid Residues in PEPHC1 Important for Binding to the Tumor-Specific Receptor EGFRvIII
- Author
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Hansen, Charlotte Lund, Hansen, Paul Robert, Pedersen, Nina, Poulsen, Hans Skovgaard, Gillings, Nic, and Kjær, Andreas
- Published
- 2008
16. [(64) Cu]-labelled trastuzumab:optimisation of labelling by DOTA and NODAGA conjugation and initial evaluation in mice
- Author
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Schjoeth-Eskesen, Christina, Nielsen, Carsten Haagen, Heissel, Søren, Højrup, Peter, Hansen, Paul Robert, Gillings, Nic, and Kjaer, Andreas
- Subjects
trastuzumab ,PET ,DOTA ,NODAGA ,skin and connective tissue diseases ,neoplasms - Abstract
The human epidermal growth factor receptor-2 (HER2) is overexpressed in 20-30% of all breast cancer cases, leading to increased cell proliferation, growth and migration. The monoclonal antibody, trastuzumab, binds to HER2 and is used for treatment of HER2-positive breast cancer. Trastuzumab has previously been labelled with copper-64 by conjugation of a 1,4,7,10-tetraazacyclododecane-1,4,7,10-tetraacetic acid (DOTA) chelator. The aim of this study was to optimise the (64) Cu-labelling of DOTA-trastuzumab and as the first to produce and compare with its 1,4,7-triazacyclononane, 1-glutaric acid-5,7 acetic acid (NODAGA) analogue in a preliminary HER2 tumour mouse model. The chelators were conjugated to trastuzumab using the activated esters DOTA mono-N-hydroxysuccinimide (NHS) and NODAGA-NHS. (64) Cu-labelling of DOTA-trastuzumab was studied by varying the amount of DOTA-trastuzumab used, reaction temperature and time. Full (64) Cu incorporation could be achieved using a minimum of 10-µg DOTA-trastuzumab, but the fastest labelling was obtained after 15 min at room temperature using 25 µg of DOTA-trastuzumab. In comparison, 80% incorporation was achieved for (64) Cu-labelling of NODAGA-trastuzumab. Both [(64) Cu]DOTA-trastuzumab and [(64) Cu]NODAGA-trastuzumab were produced after purification with radiochemical purities of >97%. The tracers were injected into mice with HER2 expressing tumours. The mice were imaged by positron emission tomography and showed high tumour uptake of 3-9% ID/g for both tracers.
- Published
- 2015
17. Synthetic analogs of anoplin show improved antimicrobial activities
- Author
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Munk, Jens, Uggerhøj, Lars Erik, Poulsen, Tanja Juul, Frimodt-Møller, Niels, Wimmer, Reinhard, Nyberg, Nils, and Hansen, Paul Robert
- Published
- 2013
18. Contribution of Peptide Backbone to Anti-Citrullinated Peptide Antibody Reactivity.
- Author
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Trier, Nicole Hartwig, Dam, Catharina Essendrup, Olsen, Dorthe Tange, Hansen, Paul Robert, and Houen, Gunnar
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RHEUMATOID arthritis treatment ,PEPTIDE analysis ,IMMUNOGLOBULINS ,AUTOIMMUNE diseases ,IMMUNOASSAY - Abstract
Rheumatoid arthritis (RA) is one of the most common autoimmune diseases, affecting approximately 1–2% of the world population. One of the characteristic features of RA is the presence of autoantibodies. Especially the highly specific anti-citrullinated peptide antibodies (ACPAs), which have been found in up to 70% of RA patients’ sera, have received much attention. Several citrullinated proteins are associated with RA, suggesting that ACPAs may react with different sequence patterns, separating them from traditional antibodies, whose reactivity usually is specific towards a single target. As ACPAs have been suggested to be involved in the development of RA, knowledge about these antibodies may be crucial. In this study, we examined the influence of peptide backbone for ACPA reactivity in immunoassays. The antibodies were found to be reactive with a central Cit-Gly motif being essential for ACPA reactivity and to be cross-reactive between the selected citrullinated peptides. The remaining amino acids within the citrullinated peptides were found to be of less importance for antibody reactivity. Moreover, these findings indicated that the Cit-Gly motif in combination with peptide backbone is essential for antibody reactivity. Based on these findings it was speculated that any amino acid sequence, which brings the peptide into a properly folded structure for antibody recognition is sufficient for antibody reactivity. These findings are in accordance with the current hypothesis that structural homology rather than sequence homology are favored between citrullinated epitopes. These findings are important in relation to clarifying the etiology of RA and to determine the nature of ACPAs, e.g. why some Cit-Gly-containing sequences are not targeted by ACPAs. [ABSTRACT FROM AUTHOR]
- Published
- 2015
- Full Text
- View/download PDF
19. [64Cu]-labelled trastuzumab: optimisation of labelling by DOTA and NODAGA conjugation and initial evaluation in mice.
- Author
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Schjoeth ‐ Eskesen, Christina, Nielsen, Carsten Haagen, Heissel, Søren, Højrup, Peter, Hansen, Paul Robert, Gillings, Nic, and Kjaer, Andreas
- Subjects
EPIDERMAL growth factor receptors ,BREAST cancer research ,CELL proliferation ,CELL migration ,TRASTUZUMAB ,TRIAZACYCLONONANE ,GLUTARIC acid ,THERAPEUTICS - Abstract
The human epidermal growth factor receptor-2 (HER2) is overexpressed in 20-30% of all breast cancer cases, leading to increased cell proliferation, growth and migration. The monoclonal antibody, trastuzumab, binds to HER2 and is used for treatment of HER2-positive breast cancer. Trastuzumab has previously been labelled with copper-64 by conjugation of a 1,4,7,10-tetraazacyclododecane-1,4,7,10-tetraacetic acid (DOTA) chelator. The aim of this study was to optimise the
64 Cu-labelling of DOTA-trastuzumab and as the first to produce and compare with its 1,4,7-triazacyclononane, 1-glutaric acid-5,7 acetic acid (NODAGA) analogue in a preliminary HER2 tumour mouse model. The chelators were conjugated to trastuzumab using the activated esters DOTA mono- N-hydroxysuccinimide (NHS) and NODAGA-NHS.64 Cu-labelling of DOTA-trastuzumab was studied by varying the amount of DOTA-trastuzumab used, reaction temperature and time. Full64 Cu incorporation could be achieved using a minimum of 10-µg DOTA-trastuzumab, but the fastest labelling was obtained after 15 min at room temperature using 25 µg of DOTA-trastuzumab. In comparison, 80% incorporation was achieved for64 Cu-labelling of NODAGA-trastuzumab. Both [64 Cu]DOTA-trastuzumab and [64 Cu]NODAGA-trastuzumab were produced after purification with radiochemical purities of >97%. The tracers were injected into mice with HER2 expressing tumours. The mice were imaged by positron emission tomography and showed high tumour uptake of 3-9% ID/g for both tracers. [ABSTRACT FROM AUTHOR]- Published
- 2015
- Full Text
- View/download PDF
20. Efficient Regioselective Ring Opening of Activated Aziridine-2-Carboxylates with [18F]Fluoride.
- Author
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Schjoeth-Eskesen, Christina, Hansen, Paul Robert, Kjaer, Andreas, and Gillings, Nic
- Subjects
- *
AZIRIDINATION , *NUCLEOPHILES , *STEREOCHEMISTRY , *ALANINE aminotransferase , *CHEMICAL synthesis , *CARBOXYLATES - Abstract
Aziridines can undergo a range of ring-opening reactions with nucleophiles. The regio- and stereochemistry of the products depend on the substituents on the aziridine. Aziridine ringopening reactions have rarely been used in radiosynthesis. Herein we report the ring opening of activated aziridine-2-carboxylates with [18F]fluoride. The aziridine was activated for nucleophilic attack by substitution of various groups on the aziridine nitrogen atom. Fluorine-18 radiolabelling was followed by ester hydrolysis and removal of the activation group. Totally regioselective ring opening and subsequent deprotection was achieved with tert-butyloxycarbonyl- and carboxybenzyl-activated aziridines to give α-[18F]fluoro-β-alanine in good radiochemical yield. [ABSTRACT FROM AUTHOR]
- Published
- 2015
- Full Text
- View/download PDF
21. Rational Design of Alpha-Helical Antimicrobial Peptides: Do's and Don'ts.
- Author
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Uggerhøj, Lars Erik, Poulsen, Tanja Juul, Munk, Jens Kristian, Fredborg, Marlene, Sondergaard, Teis Esben, Frimodt‐Moller, Niels, Hansen, Paul Robert, and Wimmer, Reinhard
- Published
- 2015
- Full Text
- View/download PDF
22. Reactivity of Rheumatoid Arthritis-Associated Citrulline-Dependent Antibodies to Epstein-Barr Virus Nuclear Antigen1-3.
- Author
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Fanelli, Ilaria, Rovero, Paolo, Hansen, Paul Robert, Frederiksen, Jette Lautrup, Houen, Gunnar, and Trier, Nicole Hartwig
- Subjects
VIRAL antibodies ,EPSTEIN-Barr virus ,MYELIN basic protein ,RHEUMATOID factor ,PEPTIDES - Abstract
Rheumatoid arthritis (RA) is a chronic disease which causes joint inflammation and, ultimately, erosion of the underlying bone. Diagnosis of RA is based on the presence of biomarkers, such as anti-citrullinated protein antibodies (ACPA) and rheumatoid factors, along with clinical symptoms. Much evidence points to a link between the Epstein-Barr virus and RA. In this study, we analyzed ACPA reactivity to citrullinated peptides originating from Epstein-Barr nuclear antigens (EBNA1, EBNA2, and EBNA3) in order to elaborate the diagnostic potential of citrullinated EBNA peptides. Moreover, ACPA cross-reactivity to citrullinated peptides from myelin basic protein (MBP) was analyzed, as citrullinated MBP recently was described to be associated with multiple sclerosis, and some degree of sequence homology between MBP and citrullinated EBNA exists. A peptide from EBNA2, (EBNA2-A, GQGRGRWRG-Cit-GSKGRGRMH) reacted with approximately 70% of all RA sera, whereas only limited reactivity was detected to EBNA1 and EBNA3 peptides. Moreover, screening of ACPA reactivity to hybrid peptides of EBNA3-A (EPDSRDQQS-Cit-GQRRGDENRG) and EBNA2-A and peptides containing citrulline close to the N-terminal confirmed that ACPA sera contain different populations of ACPAs. No notable ACPA reactivity to MBP peptides was found, confirming that ACPAs are specific for RA, and that other factors than the presence of a central Cit-Gly motif are crucial for antibody binding. Collectively, these findings illustrate that citrullinated EBNA2 is an optimal candidate for ACPA detection, supporting current evidence that EBV is linked to RA onset. [ABSTRACT FROM AUTHOR]
- Published
- 2022
- Full Text
- View/download PDF
23. Correlation between centromere protein-F autoantibodies and cancer analyzed by enzyme-linked immunosorbent assay.
- Author
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Welner, Simon, Trier, Nicole Hartwig, Frisch, Morten, Locht, Henning, Hansen, Paul Robert, and Houen, Gunnar
- Subjects
IMMUNOGLOBULINS ,CANCER patients ,AUTOANTIBODIES ,ENZYME-linked immunosorbent assay ,AUTOIMMUNITY - Abstract
Background: Centromere protein-F (CENP-F) is a large nuclear protein of 367 kDa, which is involved in multiple mitosis-related events such as proper assembly of the kinetochores, stabilization of heterochromatin, chromosome alignment and mitotic checkpoint signaling. Several studies have shown a correlation between CENP-F and cancer, e.g. the expression of CENP-F has been described to be upregulated in cancer cells. Furthermore, several studies have described a significant correlation between the expression of autoantibodies to CENP-F and cancer. Methods: Autoantibodies to CENP-F were detected in a small number of samples during routine indirect immunofluorescence (IIF) analysis for anti-nuclear antibodies (ANA) using HEp-2 cells as substrate. Using overlapping synthetic peptides covering a predicted structural maintenance of chromosomes (SMC) domain, we developed an enzyme-linked immunosorbent assay (ELISA) for detection of CENP-F antibodies. Results: Analyzing the reactivity of the sera positive in IIF for CENP-F antibodies to overlapping CENP-F peptides, we showed that autoantibodies to several peptides correlate with the presence of antibodies to CENP-F and a diagnosis of cancer, as increased CENP-F antibody expression specific for malignant cancer patients to five peptides was found (A9, A12, A14, A16, A27). These antibodies to CENP-F in clinical samples submitted for ANA analysis were found to have a positive predictive value for cancer of 50%. Furthermore, the expression of cancer-correlated CENP-F antibodies seemed to increase as a function of time from diagnosis. Conclusion: These results conform to previous findings that approximately 50% of those patients clinically tested for ANA analyses who express CENP-F antibodies are diagnosed with cancer, confirming that these antibodies may function as circulating tumor markers. Thus, a peptide-based CENP-F ELISA focused on the SMC domain may aid in identifying individuals with a potential cancer. [ABSTRACT FROM AUTHOR]
- Published
- 2013
- Full Text
- View/download PDF
24. Cyclic Peptide Inhibitors of the β-Sliding Clamp in Staphylococcus aureus.
- Author
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Kjelstrup, Susanne, Hansen, Paula Melo Paulon, Thomsen, Line E., Hansen, Paul Robert, and Løbner-Olesen, Anders
- Subjects
CYCLIC peptides ,STAPHYLOCOCCUS aureus ,REPLICATION protein A ,ESCHERICHIA coli ,BACTERIAL cell walls ,CELL death ,DNA replication - Abstract
Interaction between pairs of Staphylococcus aureus replication proteins was detected in an Escherichia coli based two-hybrid analysis. A reverse two-hybrid system was constructed for selection of compounds that hindered interaction between interacting protein pairs. A number of cyclic peptides, from a library generated by the split intein-mediated circular ligation of peptides and proteins technology, were found to interfere with dimerization of the β-sliding clamp of the replisome. Two 8-mer peptides were analyzed in more detail. Both inhibited DNA replication, led to SOS induction, altered cell morphology and cell death. The peptides were active when added to bacterial cultures indicating that they could traverse the bacterial membrane to find their intracellular target. Peptide specificity was confirmed by overproduction of the putative target (DnaN) which resulted in resistance. The minimum inhibitory concentration was ∼50 μg/ml for S. aureus cells. These compounds may serve as lead candidates for future development into novel classes of antibiotics as well as provide information on the function of the S. aureus replication process. [ABSTRACT FROM AUTHOR]
- Published
- 2013
- Full Text
- View/download PDF
25. Cross-reactivity of a human IgG1 anticitrullinated fibrinogen monoclonal antibody to a citrullinated profilaggrin peptide.
- Author
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Trier, Nicole Hartwig, Leth, Maria Louise, Hansen, Paul Robert, and Houen, Gunnar
- Abstract
Rheumatoid arthritis (RA) is the most common autoimmune rheumatic disease. It is characterized by persistent joint inflammation, resulting in loss of joint function, morbidity and premature mortality. The presence of antibodies against citrullinated proteins is a characteristic feature of RA and up to 70% of RA patients are anticitrullinated protein antibody (ACPA) positive. ACPA responses have been widely studied and are suggested to be heterogeneous, favoring antibody cross-reactivity to citrullinated proteins. In this study, we examined factors that may influence cross-reactivity between a commercial human anticitrullinated fibrinogen monoclonal antibody and a citrullinated peptide. Using a citrullinated profilaggrin sequence (HQCHQEST- Cit-GRSRGRCGRSGS) as template, cyclic and linear truncated peptide versions were tested for reactivity to the monoclonal antibody. Factors such as structure, peptide length and flanking amino acids were found to have a notable impact on antibody cross-reactivity. The results achieved contribute to the understanding of the interactions between citrullinated peptides and ACPA, which may aid in the development of improved diagnostics of ACPA. [ABSTRACT FROM AUTHOR]
- Published
- 2012
- Full Text
- View/download PDF
26. Fine mapping of a monoclonal antibody to the N-Methyl D-aspartate receptor reveals a short linear epitope.
- Author
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Amrutkar, Surekha Dipak, Trier, Nicole Hartwig, Hansen, Paul Robert, and Houen, Gunnar
- Abstract
Anti-N-Methyl D-aspartate receptor encephalitis is an autoimmune disease in which autoantibodies are produced against extracellular regions of the N-Methyl D-aspartate receptor (NMDAR). In this study, we used resin-bound peptides equipped with a base labile linker to map the epitope of a monoclonal NMDAR antibody against the NMDAR NR1 subunit. The antigenicity of the synthesized resin-bound peptides was determined by enzyme-linked immunosorbent assay. Distinct reactivity was found to two extracellular overlapping peptides (amino acids, 658-687). Using N- and C-terminally truncated resin-bound peptides, the minimum functional epitope was identified as the NPSDK sequence. The peptide sequence RNPSDK (amino acids, 673-678) was identified as the complete epitope, which was found to be located in the extracellular S2 domain of the NR1 subunit. Especially, the N-terminal arginine residue was found to be essential for reactivity, whereas the remaining amino acids could be replaced with amino acids of similar side-chain functionality, indicating the importance of backbone interaction in antibody reactivity. © 2012 Wiley Periodicals, Inc. Biopolymers (Pept Sci) 98: 567-575, 2012. [ABSTRACT FROM AUTHOR]
- Published
- 2012
- Full Text
- View/download PDF
27. Fast and efficient characterization of an anti-gliadin monoclonal antibody epitope related to celiac disease using resin-bound peptides
- Author
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Petersen, Nicole Hartwig, Hansen, Paul Robert, and Houen, Gunnar
- Subjects
- *
MONOCLONAL antibodies , *EPITOPES , *CELIAC disease , *PEPTIDES , *ACETIC acid , *ALKALINE phosphatase , *SERUM albumin , *ENZYME-linked immunosorbent assay - Abstract
Abstract: Celiac disease is a permanent intolerance to gluten. A strong indication for celiac disease is the presence of antibodies specific for gliadin, a main component of gluten. Using a deamidated immunogenic gliadin fragment, corresponding to amino acid residues 58–73 (LQPFPQPQLPYPQPQ) of gliadin a monoclonal anti-gliadin antibody has previously been generated. In this study we present an alternative approach for fast and efficient epitope mapping of the monoclonal anti-gliadin antibody, using gliadin peptide (Lys57)-Glu65-[gliadin 58–73] as template. This approach involves generation of a number of N-terminally truncated peptide analogues in one synthesis, and the use of these resin-bound peptides for rapid screening, in order to identify the minimal peptide length required for antibody recognition. The peptides were assembled on a TentaGel resin equipped with an acid-stable HMBA linker, which allows cleavage of the side-chain protecting groups but leaves the peptide attached to the resin. If required, the peptides may be cleaved from the support under mild basic conditions. Using this approach and competitive inhibition assays we identified the immunodominant epitope as the PELPYPQPQ sequence, which was located in the C-terminal end of the gliadin peptide. Our results show that the N-terminal proline residue and the C-terminal glutamine residues are essential for antibody recognition in addition to the deamidated glutamine residue. [Copyright &y& Elsevier]
- Published
- 2011
- Full Text
- View/download PDF
28. Identification of novel peptide ligands for the cancer-specific receptor mutation EFGRvIII using a mixture-based synthetic combinatorial library.
- Author
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Denholt, Charlotte Lund, Hansen, Paul Robert, Pedersen, Nina, Poulsen, Hans Skovgaard, Gillings, Nic, and Kjær, Andreas
- Published
- 2009
- Full Text
- View/download PDF
29. Efficient protection against Mycobacterium tuberculosis by vaccination with a single subdominant epitope from the ESAT-6 antigen.
- Author
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Weinreich Olsen, Anja, Hansen, Paul Robert, Holm, Arne, and Andersen, Peter
- Published
- 2000
- Full Text
- View/download PDF
30. Solid-phase peptide synthesis on proteins.
- Author
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HANSEN, PAUL ROBERT, HOLM, ARNE, and HOUEN, GUNNAR
- Published
- 1993
- Full Text
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31. A quantitative assay to measure the interaction between immunogenic peptides and purified class I major histocompatibility complex molecules.
- Author
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Olsen, Anna Catharina, Pedersen, Lars ØStergaard, Hansen, Anette Stryhn, Buus, Søren, Nissen, Mogens Holst, Olsen, Marianne, Hansen, Paul Robert, and Holm, Arne
- Published
- 1994
- Full Text
- View/download PDF
32. Development of Antimicrobial Stapled Peptides Based on Magainin 2 Sequence.
- Author
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Hirano, Motoharu, Saito, Chihiro, Yokoo, Hidetomo, Goto, Chihiro, Kawano, Ryuji, Misawa, Takashi, Demizu, Yosuke, Hansen, Paul Robert, and Franzyk, Henrik
- Subjects
ANTIMICROBIAL peptides ,AMINO acid residues ,XENOPUS ,HELICAL structure ,GRAM-positive bacteria ,ANTIMICROBIAL polymers ,PEPTIDE antibiotics - Abstract
Magainin 2 (Mag2), which was isolated from the skin of the African clawed frog, is a representative antimicrobial peptide (AMP) that exerts antimicrobial activity via microbial membrane disruption. It has been reported that the helicity and amphipathicity of Mag2 play important roles in its antimicrobial activity. We investigated and recently reported that 17 amino acid residues of Mag2 are required for its antimicrobial activity, and accordingly developed antimicrobial foldamers containing α,α-disubstituted amino acid residues. In this study, we further designed and synthesized a set of Mag2 derivatives bearing the hydrocarbon stapling side chain for helix stabilization. The preferred secondary structures, antimicrobial activities, and cell-membrane disruption activities of the synthesized peptides were evaluated. Our analyses revealed that hydrocarbon stapling strongly stabilized the helical structure of the peptides and enhanced their antimicrobial activity. Moreover, peptide 2 stapling between the first and fifth position from the N-terminus showed higher antimicrobial activity than that of Mag2 against both gram-positive and gram-negative bacteria without exerting significant hemolytic activity. To investigate the modes of action of tested peptides 2 and 8 in antimicrobial and hemolytic activity, electrophysiological measurements were performed. [ABSTRACT FROM AUTHOR]
- Published
- 2021
- Full Text
- View/download PDF
33. Covalently Immobilized Battacin Lipopeptide Gels with Activity against Bacterial Biofilms.
- Author
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De Zoysa, Gayan Heruka, Wang, Kelvin, Lu, Jun, Hemar, Yacine, Sarojini, Vijayalekshmi, and Hansen, Paul Robert
- Subjects
GELATION ,ERYTHROCYTES ,BIOFILMS ,CLICK chemistry ,SKIN infections ,POLYETHYLENE glycol ,PHARMACEUTICAL gels - Abstract
Novel antibiotic treatments are in increasing demand to tackle life-threatening infections from bacterial pathogens. In this study, we report the use of a potent battacin lipopeptide as an antimicrobial gel to inhibit planktonic and mature biofilms of S. aureus and P. aeruginosa. The antimicrobial gels were made by covalently linking the N-terminal cysteine containing lipopeptide (GZ3.163) onto the polyethylene glycol polymer matrix and initiating gelation using thiol-ene click chemistry. The gels were prepared both in methanol and in water and were characterised using rheology, Fourier transform infrared (FT-IR) spectroscopy and scanning electron microscopy (SEM). Antibacterial and antibiofilm analyses revealed that the gels prepared in methanol have better antibacterial and antibiofilm activity. Additionally, a minimum peptide content of 0.5 wt% (relative to polymer content) is required to successfully inhibit the planktonic bacterial growth and disperse mature biofilms of P. aeruginosa and S. aureus. The antibacterial activity of these lipopeptide gels is mediated by a contact kill mechanism of action. The gels are non-haemolytic against mouse red blood cells and are non-cytotoxic against human dermal fibroblasts. Findings from this study show that battacin lipopeptide gels have the potential to be developed as novel topical antibacterial agents to combat skin infections, particularly caused by S. aureus. [ABSTRACT FROM AUTHOR]
- Published
- 2020
- Full Text
- View/download PDF
34. Lactoferrin and Its Derived Peptides: An Alternative for Combating Virulence Mechanisms Developed by Pathogens.
- Author
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Zarzosa-Moreno, Daniela, Avalos-Gómez, Christian, Ramírez-Texcalco, Luisa Sofía, Torres-López, Erick, Ramírez-Mondragón, Ricardo, Hernández-Ramírez, Juan Omar, Serrano-Luna, Jesús, de la Garza, Mireya, Hansen, Paul Robert, and Franzyk, Henrik
- Subjects
LACTOFERRIN ,CELL receptors ,PEPTIDES ,EXOCRINE secretions ,PEPTIDOMIMETICS ,PATHOGENIC bacteria - Abstract
Due to the emergence of multidrug-resistant pathogens, it is necessary to develop options to fight infections caused by these agents. Lactoferrin (Lf) is a cationic nonheme multifunctional glycoprotein of the innate immune system of mammals that provides numerous benefits. Lf is bacteriostatic and/or bactericidal, can stimulate cell proliferation and differentiation, facilitate iron absorption, improve neural development and cognition, promote bone growth, prevent cancer and exert anti-inflammatory and immunoregulatory effects. Lactoferrin is present in colostrum and milk and is also produced by the secondary granules of polymorphonuclear leukocytes, which store this glycoprotein and release it at sites of infection. Lf is also present in many fluids and exocrine secretions, on the surfaces of the digestive, respiratory and reproductive systems that are commonly exposed to pathogens. Apo-Lf (an iron-free molecule) can be microbiostatic due to its ability to capture ferric iron, blocking the availability of host iron to pathogens. However, apo-Lf is mostly microbicidal via its interaction with the microbial surface, causing membrane damage and altering its permeability function. Lf can inhibit viral entry by binding to cell receptors or viral particles. Lf is also able to counter different important mechanisms evolved by microbial pathogens to infect and invade the host, such as adherence, colonization, invasion, production of biofilms and production of virulence factors such as proteases and toxins. Lf can also cause mitochondrial and caspase-dependent regulated cell death and apoptosis-like in pathogenic yeasts. All of these mechanisms are important targets for treatment with Lf. Holo-Lf (the iron-saturated molecule) can contain up to two ferric ions and can also be microbicidal against some pathogens. On the other hand, lactoferricins (Lfcins) are peptides derived from the N-terminus of Lf that are produced by proteolysis with pepsin under acidic conditions, and they cause similar effects on pathogens to those caused by the parental Lf. Synthetic analog peptides comprising the N-terminus Lf region similarly exhibit potent antimicrobial properties. Importantly, there are no reported pathogens that are resistant to Lf and Lfcins; in addition, Lf and Lfcins have shown a synergistic effect with antimicrobial and antiviral drugs. Due to the Lf properties being microbiostatic, microbicidal, anti-inflammatory and an immune modulator, it represents an excellent natural alternative either alone or as adjuvant in the combat to antibiotic multidrug-resistant bacteria and other pathogens. This review aimed to evaluate the data that appeared in the literature about the effects of Lf and its derived peptides on pathogenic bacteria, protozoa, fungi and viruses and how Lf and Lfcins inhibit the mechanisms developed by these pathogens to cause disease. [ABSTRACT FROM AUTHOR]
- Published
- 2020
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- View/download PDF
35. Synergistic Effect of Propidium Iodide and Small Molecule Antibiotics with the Antimicrobial Peptide Dendrimer G3KL against Gram-Negative Bacteria.
- Author
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Gan, Bee-Ha, Cai, Xingguang, Javor, Sacha, Köhler, Thilo, Reymond, Jean-Louis, and Hansen, Paul Robert
- Subjects
SMALL molecules ,GRAM-negative bacteria ,PROPIDIUM iodide ,ANTIMICROBIAL peptides ,KLEBSIELLA pneumoniae ,PEPTIDE antibiotics ,FLUOROPOLYMERS - Abstract
There is an urgent need to develop new antibiotics against multidrug-resistant bacteria. Many antimicrobial peptides (AMPs) are active against such bacteria and often act by destabilizing membranes, a mechanism that can also be used to permeabilize bacteria to other antibiotics, resulting in synergistic effects. We recently showed that G3KL, an AMP with a multibranched dendritic topology of the peptide chain, permeabilizes the inner and outer membranes of Gram-negative bacteria including multidrug-resistant strains, leading to efficient bacterial killing. Here, we show that permeabilization of the outer and inner membranes of Pseudomonas aeruginosa by G3KL, initially detected using the DNA-binding fluorogenic dye propidium iodide (PI), also leads to a synergistic effect between G3KL and PI in this bacterium. We also identify a synergistic effect between G3KL and six different antibiotics against the Gram-negative Klebsiella pneumoniae, against which G3KL is inactive. [ABSTRACT FROM AUTHOR]
- Published
- 2020
- Full Text
- View/download PDF
36. The Spectrum of Design Solutions for Improving the Activity-Selectivity Product of Peptide Antibiotics against Multidrug-Resistant Bacteria and Prostate Cancer PC-3 Cells.
- Author
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Juretić, Davor, Golemac, Anja, Strand, Denise E., Chung, Keshi, Ilić, Nada, Goić-Barišić, Ivana, Pellay, François-Xavier, and Hansen, Paul Robert
- Subjects
CELL-penetrating peptides ,CANCER cells ,PROSTATE cancer ,PEPTIDE antibiotics ,PRODUCT improvement ,DESIGN templates - Abstract
The link between the antimicrobial and anticancer activity of peptides has long been studied, and the number of peptides identified with both activities has recently increased considerably. In this work, we hypothesized that designed peptides with a wide spectrum of selective antimicrobial activity will also have anticancer activity, and tested this hypothesis with newly designed peptides. The spectrum of peptides, used as partial or full design templates, ranged from cell-penetrating peptides and putative bacteriocin to those from the simplest animals (placozoans) and the Chordata phylum (anurans). We applied custom computational tools to predict amino acid substitutions, conferring the increased product of bacteriostatic activity and selectivity. Experiments confirmed that better overall performance was achieved with respect to that of initial templates. Nine of our synthesized helical peptides had excellent bactericidal activity against both standard and multidrug-resistant bacteria. These peptides were then compared to a known anticancer peptide polybia-MP1, for their ability to kill prostate cancer cells and dermal primary fibroblasts. The therapeutic index was higher for seven of our peptides, and anticancer activity stronger for all of them. In conclusion, the peptides that we designed for selective antimicrobial activity also have promising potential for anticancer applications. [ABSTRACT FROM AUTHOR]
- Published
- 2020
- Full Text
- View/download PDF
37. Structure Elucidation of Prenyl- and Geranyl-Substituted Coumarins in Gerbera piloselloides by NMR Spectroscopy, Electronic Circular Dichroism Calculations, and Single Crystal X-ray Crystallography.
- Author
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Li, Tuo, Ma, Xue, Fedotov, Daniil, Kjaerulff, Louise, Frydenvang, Karla, Coriani, Sonia, Hansen, Paul Robert, Kongstad, Kenneth T., and Staerk, Dan
- Subjects
CIRCULAR dichroism ,NUCLEAR magnetic resonance spectroscopy ,SINGLE crystals ,GERBERA ,COUMARINS ,ETHYL acetate ,X-ray crystallography ,PROTEIN-tyrosine phosphatase - Abstract
Crude ethyl acetate extract of Gerbera piloselloides (L.) Cass. was investigated by dual high-resolution PTP1B/α-glucosidase inhibition profiling and LC-PDA-HRMS. This indicated the presence of a series of unprecedented prenyl- and geranyl-substituted coumarin derivatives correlated with both α-glucosidase and PTP1B inhibitory activity. Repeated chromatographic separation targeting these compounds led to the isolation of 13 new compounds, of which ten could be isolated as both enantiomers after chiral separation. The structures of all isolated compounds were characterized by HRMS and extensive 1D and 2D NMR analysis. The absolute configurations of the isolated compounds were determined by comparison of experimental and calculated electronic circular dichroism spectra. Compound 6 features a rare furan-oxepane 5/7 ring system, possibly formed through addition of a geranyl unit to C-3 of 5-methylcoumarin, representing a new type of geranyl-substituted coumarin skeleton. Compounds 19 and 24 are the first examples of dimeric natural products consisting of both coumarin and chromone moieties. [ABSTRACT FROM AUTHOR]
- Published
- 2020
- Full Text
- View/download PDF
38. Fluorescent Analogues of Human α-Calcitonin Gene-Related Peptide with Potent Vasodilator Activity.
- Author
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Zhu, Jing, Pedersen, Mahdieh Dagina, Ahmed, Laraib Sabbah, Abdolalizadeh, Bahareh, Grell, Anne-Sofie, Berg, Jais Oliver, Thulstrup, Peter Waaben, Franzyk, Henrik, Edvinsson, Lars, Sams, Anette, Sheykhzade, Majid, and Hansen, Paul Robert
- Subjects
SOLID-phase synthesis ,CALCITONIN ,CARDIOVASCULAR system ,PEPTIDE synthesis ,GASTROINTESTINAL system ,CIRCULAR dichroism - Abstract
Human α-calcitonin gene-related peptide (h-α-CGRP) is a highly potent vasodilator peptide that belongs to the family of calcitonin peptides. There are two forms of CGRP receptors in humans and rodents: α-CGRP receptor predominately found in the cardiovascular system and β-CGRP receptor predominating in the gastrointestinal tract. The CGRP receptors are primarily localized to C and Aδ sensory fibers, where they are involved in nociceptive transmission and migraine pathophysiology. These fibers are found both peripherally and centrally, with extensive perivascular location. The CGRP receptors belong to the class B G-protein-coupled receptors, and they are primarily associated to signaling via Gα proteins. The objectives of the present work were: (i) synthesis of three single-labelled fluorescent analogues of h-α-CGRP by 9-fluorenylmethyloxycarbonyl (Fmoc)-based solid-phase peptide synthesis, and (ii) testing of their biological activity in isolated human, mouse, and rat arteries by using a small-vessel myograph setup. The three analogues were labelled with 5(6)-carboxyfluorescein via the spacer 6-aminohexanoic acid at the chain of Lys
24 or Lys35 . Circular dichroism (CD) experiments were performed to obtain information on the secondary structure of these fluorescently labelled peptides. The CD spectra indicated that the folding of all three analogues was similar to that of native α-CGRP. The three fluorescent analogues of α-CGRP were successfully prepared with a purity of >95%. In comparison to α-CGRP, the three analogues exhibited similar efficacy, but different potency in producing a vasodilator effect. The analogue labelled at the N-terminus proved to be the most readily synthesized, but it was found to possess the lowest vasodilator potency. The analogues labelled at Lys35 or Lys24 exhibited an acceptable reduction in potency (i.e., 3–5 times and 5–10 times less potent, respectively), and thus they have potential for use in further investigations of receptor internalization and neuronal reuptake. [ABSTRACT FROM AUTHOR]- Published
- 2020
- Full Text
- View/download PDF
39. Review on Abyssomicins: Inhibitors of the Chorismate Pathway and Folate Biosynthesis.
- Author
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Sadaka, Carmen, Ellsworth, Edmund, Hansen, Paul Robert, Ewin, Richard, Damborg, Peter, and Watts, Jeffrey L.
- Subjects
CHORISMATE synthase ,VITAMIN B complex ,ANTI-infective agents ,EUKARYOTES ,AMINOBENZOIC acids - Abstract
Antifolates targeting folate biosynthesis within the shikimate-chorismate-folate metabolic pathway are ideal and selective antimicrobials, since higher eukaryotes lack this pathway and rely on an exogenous source of folate. Resistance to the available antifolates, inhibiting the folate pathway, underlines the need for novel antibiotic scaffolds and molecular targets. While para-aminobenzoic acid synthesis within the chorismate pathway constitutes a novel molecular target for antifolates, abyssomicins are its first known natural inhibitors. This review describes the abyssomicin family, a novel spirotetronate polyketide Class I antimicrobial. It summarizes synthetic and biological studies, structural, biosynthetic, and biological properties of the abyssomicin family members. This paper aims to explain their molecular target, mechanism of action, structure–activity relationship, and to explore their biological and pharmacological potential. Thirty-two natural abyssomicins and numerous synthetic analogues have been reported. The biological activity of abyssomicins includes their antimicrobial activity against Gram-positive bacteria and mycobacteria, antitumor properties, latent human immunodeficiency virus (HIV) reactivator, anti-HIV and HIV replication inducer properties. Their antimalarial properties have not been explored yet. Future analoging programs using the structure–activity relationship data and synthetic approaches may provide a novel abyssomicin structure that is active and devoid of cytotoxicity. Abyssomicin J and atrop-
o -benzyl-desmethylabyssomicin C constitute promising candidates for such programs. [ABSTRACT FROM AUTHOR]- Published
- 2018
- Full Text
- View/download PDF
40. Physiological response in E. coli to YdgR overexpression depends on whether the protein has an intact function.
- Author
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Sajid, Salvia, Salas, Lilia Hernandez, Rafiq, Maria, Lund, Torben, Jørgensen, Mikkel Girke, Honoré, Bent, Christensen, Lars Porskjær, Hansen, Paul Robert, Franzyk, Henrik, Mirza, Osman, and Prabhala, Bala Krishna
- Subjects
- *
ESCHERICHIA coli , *MEMBRANE transport proteins , *CARRIER proteins , *AMINO acid metabolism , *MEMBRANE proteins , *PROTEOMICS , *HOMEOSTASIS - Abstract
Membrane transport proteins are essential for the transport of a wide variety of molecules across the cell membrane to maintain cellular homeostasis. Generally, these transport proteins can be overexpressed in a suitable host (bacteria, yeast, or mammalian cells), and it is well documented that overexpression of membrane proteins alters the global metabolomic and proteomic profiles of the host cells. In the present study, we investigated the physiological consequences of overexpression of a membrane transport protein YdgR that belongs to the POT/PTR family from E. coli by using the lab strain BL21 (DE3)pLysS in its functional and attenuated mutant YdgR-E33Q. We found significant differences between the omics (metabolomics and proteomics) profiles of the cells expressing functional YdgR as compared to cells expressing attenuated YdgR, e.g., upregulation of several uncharacterized y-proteins and enzymes involved in the metabolism of peptides and amino acids. Furthermore, molecular network analysis suggested a relatively higher presence of proline-containing tripeptides in cells expressing functional YdgR. We envisage that an in-depth investigation of physiological alterations due to protein over-expression may be used for the deorphanization of the y-gene transportome. • Physiological response to membrane protein overexpression depends upon functionality. • Protein functionality tunes the expression of uncharacterized proteins. • Changes in cell shape as a consequence of membrane protein overexpression. [ABSTRACT FROM AUTHOR]
- Published
- 2023
- Full Text
- View/download PDF
41. A biophysical study of the interactions between the antimicrobial peptide indolicidin and lipid model systems.
- Author
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Nielsen, Josefine Eilsø, Lind, Tania Kjellerup, Lone, Abdullah, Gerelli, Yuri, Hansen, Paul Robert, Jenssen, Håvard, Cárdenas, Marité, and Lund, Reidar
- Subjects
- *
BILAYER lipid membranes , *QUARTZ crystal microbalances , *SMALL-angle X-ray scattering , *LIPIDS , *ATOMIC force microscopy , *CELL membranes - Abstract
The naturally occurring peptide indolicidin from bovine neutrophils exhibits strong biological activity against a broad spectrum of microorganisms. This is believed to arise from selective interactions with the negatively charged cytoplasmic lipid membrane found in bacteria. We have investigated the peptide interaction with supported lipid model membranes using a combination of complementary surface sensitive techniques: neutron reflectometry (NR), atomic force microscopy (AFM), and quartz crystal microbalance with dissipation monitoring (QCM-D). The data are compared with small-angle X-ray scattering (SAXS) results obtained with lipid vesicle/peptide solutions. The peptide membrane interaction is shown to be significantly concentration dependent. At low concentrations, the peptide inserts at the outer leaflet in the interface between the headgroup and tail core. Insertion of the peptide results in a slight decrease in the lipid packing order of the bilayer, although not sufficient to cause membrane thinning. By increasing the indolicidin concentration well above the physiologically relevant conditions, a deeper penetration of the peptide into the bilayer and subsequent lipid removal take place, resulting in a slight membrane thinning. The results suggest that indolicidin induces lipid removal and that mixed indolicidin-lipid patches form on top of the supported lipid bilayers. Based on the work presented using model membranes, indolicidin seems to act through the interfacial activity model rather than through the formation of stable pores. Unlabelled Image • The lipid interaction of antimicrobial peptides is studied by neutrons and X-rays. • The interaction of indolicidin on model lipid membranes is concentration dependent. • At low concentrations indolicidin does not penetrate through the membrane. • Indolicidin induce significant lipid removal at higher concentrations. • Indolicidin seems to disrupt the membranes in a disordered fashion. [ABSTRACT FROM AUTHOR]
- Published
- 2019
- Full Text
- View/download PDF
42. Biopolymer nanogels improve antibacterial activity and safety profile of a novel lysine-based α-peptide/β-peptoid peptidomimetic.
- Author
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Kłodzińska, Sylvia Natalie, Molchanova, Natalia, Franzyk, Henrik, Hansen, Paul Robert, Damborg, Peter, and Nielsen, Hanne Mørck
- Subjects
- *
PSEUDOMONAS aeruginosa , *BIOPOLYMERS , *NANOGELS , *ANTIBACTERIAL agents , *LYSINE , *PEPTIDOMIMETICS , *AMPHIPHILES - Abstract
Infections caused by Pseudomonas aeruginosa are associated with high morbidity and mortality, especially in immunocompromised patients. These bacteria frequently grow within a biofilm matrix, rendering therapy with conventional antibiotics inefficient; a fact that emphasizes the need for new treatment strategies. Antimicrobial peptidomimetics constitute potential alternatives to traditional antimicrobial agents. However, their application remains limited due to the lack of efficient delivery to their target site in vivo and the risk of high systemic toxicity. Nanogels composed of cross-linked networks of amphiphilic polymers with a therapeutic drug molecule embedded constitute attractive drug delivery systems, as they have been shown to display unique properties such as biocompatibility and biodegrability, as well as confer improved drug stability and reduced drug-mediated cytotoxicity. Here, we report on the first formulation of biopolymer nanogels incorporating a potent antibacterial peptidomimetic. A lysine-based α-peptide/β-peptoid hybrid with potent activity against P. aeruginosa was designed and formulated into a nanogel together with octenyl succinic anhydride-modified hyaluronic acid in order to improve its cell selectivity. Twelve nanogel formulations were prepared by using a design of experiments setup in order to identify the parameters yielding the highest drug loading and the smallest particle size. Encapsulation of the peptidomimetic into nanogels significantly decreased the cytotoxicity of the peptidomimetic to eukaryotes. The most promising formulation with high encapsulation efficiency (88%) of the peptidomimetic demonstrated a three-fold reduction in cytotoxicity towards hepatocytes along with improved bacterial killing kinetics. [ABSTRACT FROM AUTHOR]
- Published
- 2018
- Full Text
- View/download PDF
43. Cyclic Peptide Inhibitors of the β-Sliding Clamp in Staphylococcus aureus.
- Author
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Kjelstrup, Susanne, Hansen, Paula Melo Paulon, Thomsen, Line E., Hansen, Paul Robert, and Løbner-Olesen, Anders
- Subjects
- *
CYCLIC peptides , *STAPHYLOCOCCUS aureus , *REPLICATION protein A , *ESCHERICHIA coli , *BACTERIAL cell walls , *CELL death , *DNA replication - Abstract
Interaction between pairs of Staphylococcus aureus replication proteins was detected in an Escherichia coli based two-hybrid analysis. A reverse two-hybrid system was constructed for selection of compounds that hindered interaction between interacting protein pairs. A number of cyclic peptides, from a library generated by the split intein-mediated circular ligation of peptides and proteins technology, were found to interfere with dimerization of the β-sliding clamp of the replisome. Two 8-mer peptides were analyzed in more detail. Both inhibited DNA replication, led to SOS induction, altered cell morphology and cell death. The peptides were active when added to bacterial cultures indicating that they could traverse the bacterial membrane to find their intracellular target. Peptide specificity was confirmed by overproduction of the putative target (DnaN) which resulted in resistance. The minimum inhibitory concentration was ∼50 μg/ml for S. aureus cells. These compounds may serve as lead candidates for future development into novel classes of antibiotics as well as provide information on the function of the S. aureus replication process. [ABSTRACT FROM AUTHOR]
- Published
- 2013
- Full Text
- View/download PDF
44. Evaluation of 4-[18F]fluorobenzoyl-FALGEA-NH2 as a positron emission tomography tracer for epidermal growth factor receptor mutation variant III imaging in cancer
- Author
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Denholt, Charlotte Lund, Binderup, Tina, Stockhausen, Marie-Thérése, Poulsen, Hans Skovgaard, Spang-Thomsen, Mogens, Hansen, Paul Robert, Gillings, Nic, and Kjær, Andreas
- Subjects
- *
POSITRON emission tomography , *RADIOACTIVE tracers , *EPIDERMAL growth factor , *MEDICAL imaging systems , *CANCER treatment , *RADIOLIGAND assay , *BLOOD plasma , *LABORATORY mice - Abstract
Abstract: Introduction: This study describes the radiosynthesis, in vitro and in vivo evaluation of the novel small peptide radioligand, 4-[18F]fluorobenzoyl-Phe-Ala-Leu-Gly-Glu-Ala-NH2, ([18F]FBA-FALGEA-NH2) as a positron emission tomography (PET) tracer for imaging of the cancer specific epidermal growth factor receptor (EGFR) variant III mutation, EGFRvIII. Methods: For affinity, stability and PET measurements, H-FALGEA-NH2 was radiolabelled using 4-[18F]fluorobenzoic acid ([18F]FBA). The binding affinity of ([18F]FBA)-FALGEA-NH2 was measured on EGFRvIII expressing cells, NR6M. Stability studies in vitro and in vivo were carried out in blood plasma from nude mice. PET investigations of [18F]FBA-FALGEA-NH2 were performed on a MicroPET scanner, using seven nude mice xenografted subcutaneously with human glioblastoma multiforme (GBM) tumours, expressing the EGFRvIII in its native form, and five nude mice xenografted subcutaneously with GBM tumours lacking EGFRvIII expression. Images of [18F]FDG were also obtained for comparison. The mice were injected with 5–10 MBq of the radiolabelled peptide or [18F]FDG. Furthermore, the gene expression of EGFRvIII in the tumours was determined using quantitative real-time PCR. Results: Radiolabelling and purification was achieved within 180 min, with overall radiochemical yields of 2.6–9.8% (decay-corrected) and an average specific radioactivity of 6.4 GBq/μmol. The binding affinity (K d) of [18F]FBA-FALGEA-NH2 to EGFRvIII expressing cells was determined to be 23 nM. The radiolabelled peptide was moderately stable in the plasma from nude mice where 53% of the peptide was intact after 60 min of incubation in plasma but rapidly degraded in vivo, where no intact peptide was observed in plasma 5 min post-injection. The PET imaging showed that [18F]FBA-FALGEA-NH2 accumulated preferentially in the human GBM xenografts which expressed high amounts of the mutated receptor. The average tumour-to-muscle ratio (T/M) in the EGFRvIII tumours was 7.8 at 60 min post-injection, compared with 4.6 in the wild-type EGFR tumours. Furthermore, there was a strong correlation (R=0.86, P=.007) between the expression of EGFRvIII in the tumours and the tracer uptake expressed as T/M. Conclusion: Our results indicate that, despite its rapid metabolism, [18F]FBA-FALGEA-NH2 binds preferentially to EGFRvIII in the tumours in vivo and is a promising lead for further development of EGFRvIII specific peptide radiopharmaceuticals. [Copyright &y& Elsevier]
- Published
- 2011
- Full Text
- View/download PDF
45. Complex metabolism of aromatic glucosinolates in Pieris rapae caterpillars involving nitrile formation, hydroxylation, demethylation, sulfation, and host plant dependent carboxylic acid formation
- Author
-
Agerbirk, Niels, Olsen, Carl Erik, Poulsen, Eva, Jacobsen, Niels, and Hansen, Paul Robert
- Subjects
- *
GLUCOSINOLATES , *CARBOHYDRATE metabolism , *PIERIS rapae , *CATERPILLARS , *NITRILES , *HYDROXYLATION , *CARBOXYLIC acids , *METABOLITES - Abstract
Abstract: We investigated the metabolism of two chain elongated phenolic glucosinolates and the corresponding O-methyl derivatives upon ingestion by caterpillars of the butterfly Pieris rapae (L.). The glucosinolates (GSLs) were 4-hydroxyphenethylGSL, (R)-2-hydroxy-2-(4-hydroxyphenyl)ethylGSL, 4-methoxyphenethylGSL, and (R)-2-hydroxy-2-(4-methoxyphenyl)ethylGSL, variously occurring in foliage of two Arabis species: Arabis hirsuta (L.) Scop. and Arabis soyeri Reut. & Huet subsp. subcoriacea (Gren. ex Nyman) Breitstr. (Brassicaceae). Frass from caterpillars reared on each Arabis species contained two sulfated nitriles (4-sulfates of 3-(4-hydroxyphenyl)propanenitrile and 3-hydroxy-3-(4-hydroxyphenyl)propanenitrile) as apparent GSL metabolites. Comparison of glucosinolate levels in foliage and levels of sulfated nitriles in frass, and experiments with isolated GSLs spiked to crucifer foliage and ingested by P. rapae, demonstrated that phenolic GSLs and the corresponding O-methyl derivatives were metabolised to sulfated nitriles, and that metabolites lacking a β-hydroxy group were partially hydroxylated in this position during metabolism in P. rapae. In contrast, an induction experiment did not show increased levels of β-hydroxylated GSLs in A. soyeri plants upon caterpillar feeding. Frass contents of other putative GSL metabolites from the interaction with the two Arabis species differed significantly; caterpillars reared on A. hirsuta excreted significant amounts of four carboxylic acids (3-(4-hydroxyphenyl)propanoic acid, 3-hydroxy-3-(4-hydroxyphenyl)propanoic acid, and the corresponding 4-sulfates), which were low or absent when the caterpillars were reared on A. soyeri. The excreted carboxylic acids could be formed by hydrolysis of nitriles to carboxylic acids in caterpillar guts by an ingested nitrilase enzyme from A. hirsuta foliage; this hypothesis was supported by demonstration of 3-(4-hydroxyphenyl)propanenitrile hydrolysing nitrilase activity (E.C. 3.5.5.x) in a crude A. hirsuta extract. Some hypothetic metabolites, glycine conjugates of phenolic carboxylic acids, were not detected. Conditions for group separation and HPLC isolation of intact GSLs and sulfated metabolites were optimised, NMR spectroscopic data of the compounds are reported, and evolutionary and ecological implications are discussed. [Copyright &y& Elsevier]
- Published
- 2010
- Full Text
- View/download PDF
46. Use of peptide antibodies to probe for the mitoxantrone resistance-associated protein MXR/BCRP/ABCP/ABCG2
- Author
-
Litman, Thomas, Jensen, Ulla, Hansen, Alastair, Covitz, Kuang-Ming, Zhan, Zhirong, Fetsch, Patricia, Abati, Andrea, Hansen, Paul Robert, Horn, Thomas, Skovsgaard, Torben, and Bates, Susan E.
- Subjects
- *
CANCER cells , *MITOXANTRONE hydrochloride - Abstract
Recent studies have characterized the ABC half-transporter associated with mitoxantrone resistance in human cancer cell lines. Encoded by the ABCG2 gene, overexpression confers resistance to camptothecins, as well as to mitoxantrone. We developed four polyclonal antibodies against peptides corresponding to four different epitopes on the mitoxantrone resistance-associated protein, ABCG2. Three epitopes localized on the cytoplasmic region of ABCG2 gave rise to high-affinity antibodies, which were demonstrated to be specific for ABCG2. Western blot analysis of cells with high levels of ABCG2 showed a single major band of the expected 72-kDa molecular size of ABCG2 under denaturing conditions. Immunoblot analysis performed under non-reducing conditions and after treatment with cross-linking reagents demonstrated a molecular weight shift from 72 kDa to several bands of 180 kDa and higher molecular weight, suggesting detection of dimerization products of ABCG2. Evidence of N-linked glycosylation was also obtained using tunicamycin and N-glycosidase F. Finally, both by light, fluorescence and electron microscopic immunohistochemical staining, we demonstrate cytoplasmic and predominantly plasma membrane localization of ABCG2 in cell lines with high levels of expression. Plasma membrane staining was observed on the surface of the chorionic villi in placenta. These results support the hypothesis that ABCG2 is an ABC half-transporter that forms dimers in the plasma membrane, functioning as an ATP-dependent outward pump for substrate transport. [Copyright &y& Elsevier]
- Published
- 2002
- Full Text
- View/download PDF
47. Analogues of the antimicrobial peptide BP214
- Author
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Coelho, Catarina Rainho, Hansen, Paul Robert, and Lopes, Francisca
- Subjects
Mestrado Integrado - 2017 ,Ciências da Saúde ,Hydrophobicity ,Hemolytic activity ,Antimicrobial peptides ,Antimicrobial activity - Abstract
Trabalho Final de Mestrado Integrado, Ciências Farmacêuticas, Universidade de Lisboa, Faculdade de Farmácia, 2017 Submitted by Repositório FFUL (repositorio@ff.ul.pt) on 2018-12-18T15:41:13Z No. of bitstreams: 1 MICF_Catarina_Rainho_Coelho.pdf: 5179141 bytes, checksum: d5e178c54b2805b10a859e8f9bb4b0f1 (MD5) Made available in DSpace on 2018-12-18T20:36:15Z (GMT). No. of bitstreams: 1 MICF_Catarina_Rainho_Coelho.pdf: 5179141 bytes, checksum: d5e178c54b2805b10a859e8f9bb4b0f1 (MD5) Previous issue date: 2017-12-07
- Published
- 2017
48. Analogues of the antimicrobial peptide BP214
- Author
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Freire, Catarina Maria Boto, Rocha, Maria de Jesus Perry, and Hansen, Paul Robert
- Subjects
Mestrado Integrado - 2017 ,Ciências da Saúde ,Hydrophobicity ,Hemolytic activity ,Antimicrobial peptides ,Gram-negative infections ,Antimicrobial activity - Abstract
Trabalho Final de Mestrado Integrado, Ciências Farmacêuticas, Universidade de Lisboa, Faculdade de Farmácia, 2017 Submitted by Repositório FFUL (repositorio@ff.ul.pt) on 2018-12-18T15:28:30Z No. of bitstreams: 1 MICF_Catarina_Freire.pdf: 2718495 bytes, checksum: 654c353b08c3554ee8d49fa463fbb0b9 (MD5) Made available in DSpace on 2018-12-18T20:35:53Z (GMT). No. of bitstreams: 1 MICF_Catarina_Freire.pdf: 2718495 bytes, checksum: 654c353b08c3554ee8d49fa463fbb0b9 (MD5) Previous issue date: 2017-12-07
- Published
- 2017
49. Fmoc Solid-Phase Peptide Synthesis.
- Author
-
Hansen PR and Oddo A
- Subjects
- Amino Acids chemistry, Solid-Phase Synthesis Techniques methods, Peptides chemical synthesis, Peptides chemistry, Fluorenes chemistry
- Abstract
Synthetic peptides are important as drugs and in research. Currently, the method of choice for producing these compounds is solid-phase peptide synthesis. Here, we describe the scope and limitations of Fmoc solid-phase peptide synthesis. Furthermore, we provide a detailed protocol for Fmoc peptide synthesis., (© 2024. The Author(s), under exclusive license to Springer Science+Business Media, LLC, part of Springer Nature.)
- Published
- 2024
- Full Text
- View/download PDF
50. Peptide-Carrier Conjugation.
- Author
-
Hansen PR
- Subjects
- Animals, Cattle, Peptides chemistry, Serum Albumin, Bovine chemistry, Cysteine chemistry
- Abstract
To produce antibodies against synthetic peptides, it is necessary to couple them to a protein carrier. This chapter provides a nonspecialist overview of peptide-carrier conjugation. Furthermore, a protocol for coupling cysteine-containing peptides to bovine serum albumin is outlined., (© 2024. The Author(s), under exclusive license to Springer Science+Business Media, LLC, part of Springer Nature.)
- Published
- 2024
- Full Text
- View/download PDF
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