Your search keyword '"Robert Waibel"' showing total 61 results

1. High-Yield Production of Recombinant Antibody Fragments in HEK-293 Cells Using Sodium Butyrate

Author

Jürgen Grünberg, Karin Knogler, Robert Waibel, and Ilse Novak-Hofer

Subjects

Biology (General), QH301-705.5

Abstract

To develop new recombinant monoclonal antibody fragments for therapy and imaging, it is indispensable to have a simple and easy procedure to handle the eukaryotic expression system for production of proteins in high amounts. Gene amplification techniques such as the dehydrofolate reductase (DHFR) system in Chinese hamster ovary cells or the glutamine synthase system in myeloma cells have a couple of disadvantages. The selection procedure is complex, time-consuming, and not fruitful in all cases. The toxic drug methotrexate (for the DHFR system) can increase the production rate but decreases the specific growth rate of the cells. The production rate is not always stable over a long-term cultivation period. To overcome these problems, we are using stably transfected human embryonic kidney (HEK-293) cells in combination with an efficient screening method. Sodium butyrate can increase the expression of recombinant antibody fragments in the transfectomas up to 500 μg/4.2 × 107 cells/24 h corresponding to 175 μg/mL culture medium. This strategy allows a rapid development of new recombinant monoclonal antibody fragments and allows one to proceed rapidly to in vivo testing.

Published

2003

2. Comparison of recombinant human haptocorrin expressed in human embryonic kidney cells and native haptocorrin.

Author

Evelyne Furger, Sergey N Fedosov, Dorte Launholt Lildballe, Robert Waibel, Roger Schibli, Ebba Nexo, and Eliane Fischer

Subjects

Medicine, Science

Abstract

Haptocorrin (HC) is a circulating corrinoid binding protein with unclear function. In contrast to transcobalamin, the other transport protein in blood, HC is heavily glycosylated and binds a variety of cobalamin (Cbl) analogues. HC is present not only in blood but also in various secretions like milk, tears and saliva. No recombinant form of HC has been described so far. We report the expression of recombinant human HC (rhHC) in human embryonic kidney cells. We purified the protein with a yield of 6 mg (90 nmol) per litre of cell culture supernatant. The isolated rhHC behaved as native HC concerning its spectral properties and ability to recognize both Cbl and its baseless analogue cobinamide. Similar to native HC isolated from blood, rhHC bound to the asialoglycoprotein receptor only after removal of terminal sialic acid residues by treatment with neuraminidase. Interestingly, rhHC, that compared to native HC contains four excessive amino acids (…LVPR) at the C-terminus, showed subtle changes in the binding kinetics of Cbl, cobinamide and the fluorescent Cbl conjugate CBC. The recombinant protein has properties very similar to native HC and although showing slightly different ligand binding kinetics, rhHC is valuable for further biochemical and structural studies.

Published

2012

3. Radiopharmaceuticals: From Molecular Imaging to Targeted Radionuclide Therapy

Author

P. August Schubiger, Jürgen Grünberg, Simon Mensah Ametamey, Michael Honer, Elisa Garcia-Garayoa, Peter Bläuenstein, Robert Waibel, Ilse Novak-Hofer, and Roger Schibli

Subjects

Molecular imaging, Pet-tracer, Radioimmunotherapy, Radionuclide therapy, Radiopharmaceuticals, Chemistry, QD1-999

Abstract

The research and development of smart radiodrugs is the goal of the Center of Radiopharmaceutical Science of ETH, PSI, and USZ. Positron Emission Tomography (PET) allows the non-invasive visualization of biochemical processes within the body. Radiolabeled PET-tracers allow the study of neurophysiological diseases like Alzheimer, Parkinson's disease or the imaging of metastatic tumors. PET-techniques are nowadays an important part of routine nuclear medicine diagnosis. Tumor-cell targeting biomolecules (e.g. antibodies or peptides) coupled to therapeutic radionuclides can sterilize the malignant cells while sparing healthy tissue. This so-called targeted radionuclide therapy has made tremendous progress in the recent years and the first approved radiotherapeutics are available for clinical use.

Published

2004

4. Radiopharmaceuticals for Targeted Tumor Diagnosis and Therapy

Author

Robert Waibel, Matthias Brühlmeier, Alain Blanc, Olga Gasser, Raimo Pellikka, Kurt Zimmermann, Rolf Schwarzbach, Elisa Garcia-Garayoa, Peter Bläuenstein, Roger Schibli, Ilse Novak-Hofer, and P. August Schubiger

Subjects

Nuclide therapy, Pharmaceutical chemistry, Radioimmunotherapy, Radiopharmaceuticals, 99mtc, Tumor imaging, Chemistry, QD1-999

Abstract

Radiopharmaceutical research and development is carried out by the Center for Radiopharmaceutical Science as part of the PSI Life Science Department, the Department of Applied BioSciences at the Swiss Federal Institute of Technology Zürich and the University Hospital Zürich. The common theme is the search for radioactive-labeled tracer molecules, which bind to specific targets in the body. Such radiopharmaceuticals are applied either systemically into the blood stream or locally to patients. Due to their specific molecular binding properties combined with the emitted radiation, they can be used for non-invasive imaging of tumors and the destruction of tumor cells. In this first of two articles, we will present exemplified topics from the research activities of the groups involved with tumor targeting.

Published

2000

5. Supplementary Table 1 from New Derivatives of Vitamin B12 Show Preferential Targeting of Tumors

Author

Pius August Schubiger, Roger Schibli, Holger Moch, Alexander Knuth, Jakob Nüesch, Roger Alberto, Martin Küenzi, Susanne Kunze, Stefan Mundwiler, Dave R. van Staveren, Niklaus G. Schaefer, Hansjörg Treichler, and Robert Waibel

Abstract

Supplementary Table 1 from New Derivatives of Vitamin B12 Show Preferential Targeting of Tumors

Published

2023

6. Supplementary Table 2 from New Derivatives of Vitamin B12 Show Preferential Targeting of Tumors

Author

Pius August Schubiger, Roger Schibli, Holger Moch, Alexander Knuth, Jakob Nüesch, Roger Alberto, Martin Küenzi, Susanne Kunze, Stefan Mundwiler, Dave R. van Staveren, Niklaus G. Schaefer, Hansjörg Treichler, and Robert Waibel

Abstract

Supplementary Table 2 from New Derivatives of Vitamin B12 Show Preferential Targeting of Tumors

Published

2023

7. Supplementary Materials, Table 1-6, Figures 1-10 from Efficient Tumor Targeting with High-Affinity Designed Ankyrin Repeat Proteins: Effects of Affinity and Molecular Size

Author

Andreas Plückthun, Robert Waibel, H. Kaspar Binz, Roger Schibli, Birgit Dreier, Gabriela Nagy-Davidescu, Rastislav Tamaskovic, Christine de Pasquale, Michael T. Stumpp, Martin Kawe, and Christian Zahnd

Abstract

Supplementary Materials, Table 1-6, Figures 1-10 from Efficient Tumor Targeting with High-Affinity Designed Ankyrin Repeat Proteins: Effects of Affinity and Molecular Size

Published

2023

8. Evaluation of a Novel Tc-99m Labelled Vitamin B12 Derivative for Targeting Escherichia coli and Staphylococcus aureus In Vitro and in an Experimental Foreign-Body Infection Model

Author

Daniela Baldoni, Andrej Trampuz, Filippo Galli, Violetta Iodice, Alberto Signore, Peter Bläuenstein, Roger Schibli, and Robert Waibel

Subjects

Staphylococcus aureus, Cancer Research, Biodistribution, Colony Count, Microbial, In Vitro Techniques, Biology, medicine.disease_cause, Infection imaging, Microbiology, Mice, Drug Delivery Systems, In vivo, hemic and lymphatic diseases, Escherichia coli, medicine, scintigraphy, Animals, Radiology, Nuclear Medicine and imaging, Cyanocobalamin, Vitamin B12, 99mTc, Medicine(all), Foreign-Body Reaction, fungi, Technetium, tc-99m, biology.organism_classification, infection, In vitro, 3. Good health, Mice, Inbred C57BL, Vitamin B 12, Oncology, vitamin b12, escherichia coli, staphylococcus aureus, infection imaging, Bacteria, Research Article

Abstract

Purpose: Vitamin B12 (cyanocobalamin, Cbl) is accumulated by rapidly replicating prokaryotic and eukaryotic cells. We investigated the potential of a Tc-99m labelled Cbl derivative ([99mTc]PAMA(4)-Cbl) for targeting infections caused by Escherichia coli and Staphylococcus aureus. In vitro binding assays were followed by biodistribution studies in a mouse model of foreign body infection. Procedures: E. coli (ATCC 25922) and S. aureus (ATCC 43335) were used as test strains. [57Co]Cbl, [67Ga]citrate and [99mTc]DTPA served as reference compounds. The in vitro competitive binding of [57Co]Cbl or [99mTc]PAMA(4)-Cbl, and unlabeled Cbl, to viable or killed bacteria, was evaluated at 37 and 4 °C. A cage mouse model of infection was used for biodistribution of intravenous [57Co]Cbl and [99mTc]PAMA(4)-Cbl in cage and dissected tissues of infected and non-infected mice. Results: Maximum binding (mean ± SD) of [57Co]Cbl to viable E. coli was 81.7 ± 2.6 % and to S. aureus 34.0 ± 6.7 %, at 37 °C; no binding occurred to heat-killed bacteria. Binding to both test strains was displaced by 100- to 1000-fold excess of unlabeled Cbl. The in vitro binding of [99mTc]PAMA(4)-Cbl was 100-fold and 3-fold lower than the one of [57Co]Cbl for E. coli and S. aureus, respectively. In vivo, [99mTc]PAMA(4)-Cbl showed peak percentage of injected dose (% ID) values between 1.33 and 2.3, at 30 min post-injection (p.i.). Significantly higher retention occurred in cage fluids infected with S. aureus at 4 h and with E. coli at 8 h p.i. than in non-infected animals. Accumulation into infected cages was also higher than the one of [99mTc]DTPA, which showed similar biodistribution in infected and sterile mice. [57Co]Cbl gradually accumulated in cages with peaks % ID between 3.58 and 4.83 % achieved from 24 to 48 h. Discrimination for infection occurred only in E. coli-infected mice, at 72 h p.i. [67Ga]citrate, which showed a gradual accumulation into cage fluids during 12 h, was discriminative for infection from 48 to 72 h p.i. (P, Molecular Imaging and Biology, 17 (6), ISSN:1860-2002, ISSN:1536-1632

Published

2015

9. Expression of alternatively spliced forms of the CD44 extracellular-matrix receptor on human lung carcinomas

Author

David A. Jackson, John I. Bell, Robert Waibel, Rolf A. Stahel, and Thomas Schenker

Subjects

Cancer Research, Pathology, medicine.medical_specialty, Lung Neoplasms, Molecular Sequence Data, Receptors, Lymphocyte Homing, Gene Expression, Receptors, Cell Surface, Polymerase Chain Reaction, Cell Line, Metastasis, Exon, Cell surface receptor, Gene expression, Tumor Cells, Cultured, medicine, Humans, RNA, Messenger, Carcinoma, Small Cell, Cloning, Molecular, DNA Primers, Base Sequence, biology, Alternative splicing, CD44, Flow Cytometry, medicine.disease, Hyaluronan-mediated motility receptor, Clone Cells, Alternative Splicing, Hyaluronan Receptors, Oncology, Carcinoma, Squamous Cell, biology.protein, Cancer research, Adenocarcinoma, Carrier Proteins, Oligonucleotide Probes

Abstract

Expression of isoforms of the CD44 hyaluronan receptor/lymph-node endothelial receptor by human tumour cells is thought to play a role in tumour growth and metastasis. These isoforms which vary in the length of the extracellular domain are generated by differential RNA splicing that involves the 10 alternative exons (v1 to v10) encoding the membrane proximal region of the molecule. Several tumours have been shown to over-express CD44 containing the v6 exon, and this, together with other evidence, has led to the suggestion that v6 may play a causative role in tumour metastasis. In this report we have compared the expression of CD44 isoforms between different lung tumour lines, including SCLC, squamous-cell carcinoma, adenocarcinoma and mesothelioma, using both RT-PCR and fluorescent antibody staining with a panel of CD44 exon-specific monoclonal antibodies (MAbs). Our results show large differences in vCD44 expression between individual tumour lines. Little or no vCD44 containing the metastasis-associated v6 exon was detected in most tumours, including the highly metastatic SCLC lines. Indeed, the SCLC lines and some squamous-cell carcinomas contained only very low levels of either vCD44 or CD44H, indicating that CD44 expression may not always correlate with tumour development or dissemination. One of the squamous-cell carcinomas studied (HOTZ) was found to express a complex mixture of CD44 splice variants similar to the immortalized normal bronchial epithelial line BEAS-2B. Cloning and sequencing of vCD44 from the HOTZ cell line yielded several splice variants that have also been identified on leukaemic cells, normal keratinocytes and activated peripheral-blood lymphocytes.

Published

2016

10. Radiolabeling of rituximab with 188Re and 99mTc using the tricarbonyl technology

Author

Christine de Pasquale, Cristina Müller, Carla Roberta Dias, Roger Schibli, Robert Waibel, Joao A. Osso, Alexander Hohn, and Simone Jeger

Subjects

Cancer Research, Biodistribution, Radioimmunoconjugate, Stereochemistry, Antibodies, Monoclonal, Murine-Derived, Mice, Drug Stability, In vivo, Cell Line, Tumor, Animals, Humans, Histidine, Radiology, Nuclear Medicine and imaging, Cysteine, Radioisotopes, CD20, biology, Chemistry, Lymphoma, Non-Hodgkin, Biological activity, Organotechnetium Compounds, Antigens, CD20, Molecular biology, In vitro, Raji cell, Rhenium, Isotope Labeling, biology.protein, Autoradiography, Molecular Medicine, Female, Antibody, Rituximab

Abstract

Introduction The most successful clinical studies of immunotherapy in patients with non-Hodgkin's lymphoma (NHL) use the antibody rituximab (RTX) targeting CD20 + B-cell tumors. Rituximab radiolabeled with β − emitters could potentiate the therapeutic efficacy of the antibody by virtue of the particle radiation. Here, we report on a direct radiolabeling approach of rituximab with the 99m Tc- and 188 Re-tricarbonyl core (IsoLink technology). Methods The native format of the antibody (RTX wt ) as well as a reduced form (RTX red ) was labeled with 99m Tc/ 188 Re(CO) 3 . The partial reduction of the disulfide bonds to produce free sulfhydryl groups (–SH) was achieved with 2-mercaptoethanol. Radiolabeling efficiency, in vitro human plasma stability as well as transchelation toward cysteine and histidine was investigated. The immunoreactivity and binding affinity were determined on Ramos and/or Raji cells expressing CD20. Biodistribution was performed in mice bearing subcutaneous Ramos lymphoma xenografts. Results The radiolabeling efficiency and kinetics of RTX red were superior to that of RTX wt ( 99m Tc: 98% after 3 h for RTX red vs. 70% after 24 h for RTX wt ). 99m Tc(CO) 3 -RTX red was used without purification for in vitro and in vivo studies whereas 188 Re(CO) 3 -RTX red was purified to eliminate free 188 Re-precursor. Both radioimmunoconjugates were stable in human plasma for 24 h at 37°C. In contrast, displacement experiments with excess cysteine/histidine showed significant transchelation in the case of 99m Tc(CO) 3 -RTX red but not with pre-purified 188 Re(CO) 3 -RTX red . Both conjugates revealed high binding affinity to the CD20 antigen ( K d =5–6 nM). Tumor uptake of 188 Re(CO) 3 -RTX red was 2.5 %ID/g and 0.8 %ID/g for 99m Tc(CO) 3 -RTX red 48 h after injection. The values for other organs and tissues were similar for both compounds, for example the tumor-to-blood and tumor-to-liver ratios were 0.4 and 0.3 for 99m Tc(CO) 3 -RTX red and for 188 Re(CO) 3 -RTX red 0.5 and 0.5 (24 h pi). Conclusion Rituximab could be directly and stably labeled with the matched pair 99m Tc/ 188 Re using the IsoLink technology under retention of the biological activity. Labeling kinetics and yields need further improvement for potential routine application in radioimmunodiagnosis and therapy.

Published

2011

11. In-Line Radiolabeling: A Novel Continuous-Flow System for Commercial-Scale Protein Labeling

Author

Debra A. Harris, Missag H. Parseghian, P. August Schubiger, Peter Blaeuenstein, Steven W. King, Olga Gasser, Robert Waibel, and Raimo Pellikka

Subjects

Radioisotopes, Commercial scale, Chromatography, Chemistry, Continuous flow, Drug Compounding, Commerce, Antibodies, Monoclonal, Structural integrity, Nanotechnology, Equipment Design, Protein labeling, medicine.disease, Online Systems, Equipment Failure Analysis, Reaction rate, Isotope Labeling, Flow Injection Analysis, medicine, Radiology, Nuclear Medicine and imaging, Radiopharmaceuticals, Reaction tube, Glioblastoma

Abstract

A key limitation in developing radiotherapeutic proteins is the expense of manufacturing the drug in small batches using traditional reaction vessels. Removing limitations on the quantity of protein labeled at any one time significantly decreases the cost of production, and nowhere is the need for cost-effective radiotherapeutics more acute than in the treatment of cancer. Methods: We describe a novel method that can rapidly radiolabel, theoretically, unlimited amounts of protein, without causing significant damage to binding potency or structural integrity. Our process controls the reaction rate for the isotope and reactants as they simultaneously flow through a reaction tube. Results: We have demonstrated proof of principle by labelingnearlyagramofantibodywith481GBq(13Ci)of 131 Iduring a single 30-min reaction run. Conclusion: Simple to construct, our system is already used to manufacture a radiolabeled antibody, both in the United States and in India, as part of clinical trials to treat glioblastoma multiforme. Modified, this system may be also applicable for nonradioactive labeling.

Published

2009

12. PEGylation and Multimerization of the Anti-p185HER-2 Single Chain Fv Fragment 4D5

Author

Ela Balic, Uwe Zangemeister-Wittke, Susanne Kubetzko, Robert Waibel, and Andreas Plückthun

Subjects

chemistry.chemical_classification, biology, C-terminus, Miniantibody, Cell Biology, Biochemistry, Molecular biology, Divalent, chemistry, PEG ratio, PEGylation, biology.protein, Moiety, Avidity, Antibody, Molecular Biology

Abstract

A major goal in antibody design for cancer therapy is to tailor the pharmacokinetic properties of the molecule according to specific treatment requirements. Key parameters determining the pharmacokinetics of therapeutic antibodies are target specificity, affinity, stability, and size. Using the p185HER-2 (HER-2)-specific scFv 4D5 as model system, we analyzed how changes in molecular weight and valency independently affect antigen binding and tumor localization. By employing multimerization and PEGylation, four different antibody formats were generated and compared with the scFv 4D5. First, dimeric and tetrameric miniantibodies were constructed by fusion of self-associating, disulfide-linked peptides to the scFv 4D5. Second, we attached a 20-kDa PEG moiety to the monovalent scFv and to the divalent miniantibody at the respective C terminus. In all formats, serum stability and full binding reactivity of the scFv 4D5 were retained. Functional affinity, however, did change. An avidity increase was achieved by multimerization, whereas PEGylation resulted in a 5-fold decreased affinity. Nevertheless, the PEGylated monomer showed an 8.5-fold, and the PEGylated dimer even a 14.5-fold higher tumor accumulation than the corresponding scFv, 48 h post-injection, because of a significantly longer serum half-life. In comparison, the non-PEGylated bivalent and tetravalent miniantibodies showed only a moderate increase in tumor localization compared with the scFv, which correlated with the degree of multimerization. However, these non-PEGylated formats resulted in higher tumor-to-blood ratios. Both multimerization and PEGylation represent thus useful strategies to tailor the pharmacokinetic properties of therapeutic antibodies and their combined use can additively improve tumor targeting.

Published

2006

13. Picolylamine-methylphosphonic acid esters as tridentate ligands for the labeling of alcohols with the fac-[M(CO)3]+ core (M=99mTc, Re): synthesis and biodistribution of model compounds and of a 99mTc-labeled cobinamide

Author

Roger Alberto, Robert Waibel, Susanne Kunze, Stefan Mundwiler, Bernhard Spingler, University of Zurich, and Alberto, R

Subjects

10120 Department of Chemistry, Cancer Research, Biodistribution, Magnetic Resonance Spectroscopy, Haptocorrin, Stereochemistry, chemistry.chemical_element, Ligands, Mice, chemistry.chemical_compound, Organophosphorus Compounds, Transcobalamin, 540 Chemistry, Organometallic Compounds, 2741 Radiology, Nuclear Medicine and Imaging, Animals, Molecule, 1306 Cancer Research, Tissue Distribution, Radiology, Nuclear Medicine and imaging, Chelation, Methylphosphonic acid, Mice, Inbred BALB C, Ligand, Technetium, Organotechnetium Compounds, Rhenium, chemistry, 1313 Molecular Medicine, Alcohols, Molecular Medicine, Female, Cobamides, Radiopharmaceuticals

Abstract

[(Methyl-pyridin-2-ylmethyl-amino)-methyl]-phosphonic acid is a new bifunctional chelator for the fac-[(99m)Tc(CO(3))](+) core which can be linked to biomolecules via formation of phosphonic acid esters. Its synthesis and the coupling to model alcohols and to a bioactive molecule (cobinamide) are described. The rhenium complexes [Re(CO)(3)L] of the esters have been prepared and characterized, one of them by X-ray crystallography. The model esters could be labeled with [(99m)Tc(OH(2))(3)(CO)(3)](+) under mild conditions and relatively low ligand concentration with >97% yield and only one isomer formed. The (99m)Tc-labeled cobinamide analog was a mixture of four isomers. It bound strongly to transcobalamin I (TC I, haptocorrin) but only slightly to transcobalamin II (TC II) and intrinsic factor (IF), reflecting the binding abilities of cobinamide. Biodistribution studies in mice with B(16) melanoma exhibited fast clearance with no specific tissue binding.

Published

2005

14. S-Functionalized Cysteine: Powerful Ligands for the Labelling of Bioactive Molecules with Triaquatricarbonyltechnetium-99m(1+) ([99mTc(OH2)3(CO)3]+)

Author

Jae-Kyoung Pak, Paul Benny, Roger Alberto, Robert Waibel, Dave R. van Staveren, and Philipp Kurz

Subjects

chemistry.chemical_classification, Stereochemistry, Organic Chemistry, Peptide, Alkylation, Conjugated system, Biochemistry, Catalysis, Inorganic Chemistry, Nucleophile, chemistry, Drug Discovery, Moiety, Chelation, Amine gas treating, Physical and Theoretical Chemistry, Cysteine

Abstract

S-Alkylated cysteines are used as efficient tridentate N,O,S-donor-atom ligands for the fac-[M(CO)3]+ moiety (M=99mTc or Re). Reaction of (Et4N)2[ReBr3(CO)3] (3) with the model S-benzyl-L-cysteine (2) leads to the formation of [Re(2′)(CO)3] (4) as the exclusive product (2′=C-terminal anion of 2). The tridentate nature of the alkylated cysteine in 4 was established by X-ray crystallography. Compound 2 reacts with [99mTc(OH2)3(CO)3]+ under mild conditions (10−4M, 50°, 30 min) to afford [99mTc(2′)(CO)3] (5) and represents, therefore, an efficient chelator for the labelling of biomolecules. L-Cysteine, S-alkylated with a 3-aminopropyl group (7), was conjugated via a peptide coupling sequence with Coα-[α-(5,6-dimethyl-1H-benzimidazolyl)]-Coβ-cyanocobamic b-acid (6), the b-acid of cyanocob(III)alamin (vitamin B12) (Scheme 3). More convenient was a one-pot procedure with a derivative of vitamin B12 comprising a free amine group at the b-position. This amine 15 was treated with NHS (N-hydroxysuccinimide)-activated 1-iodoacetic acid 14 to introduce an I-substituent in vitamin B12. Subsequent addition of unprotected L-cysteine resulted in nucleophilic displacement of the I-atom by the S-substituent, affording the vitamin B12 alkylated cysteine fragment 17 (Scheme 4). The procedure was quantitative and did not require purification of intermediates. Both cobalamin–cysteine conjugates could be efficiently labelled with [99mTc(OH2)3(CO)3]+ (1) under conditions identical to those of the model complex 5. Biodistribution studies of the cobalamin conjugates in mice bearing B10-F16 melanoma tumors showed a tumor uptake of 8.1±0.6% and 4.4±0.5% injected dose per gram of tumor tissue after 4 h and 24 h, respectively (Table 1).

Published

2005

15. Conjugates of vitamin B12 with Nε-functionalized histidine for labeling with [99mTc(OH2)3(CO)3]+: synthesis and biodistribution studies in tumor bearing mice

Author

Dave R. van Staveren, Stefan Mundwiler, P. August Schubiger, Roger Alberto, and Robert Waibel

Subjects

Biodistribution, Stereochemistry, Organic Chemistry, Substituent, Biochemistry, Inorganic Chemistry, chemistry.chemical_compound, Acetic acid, chemistry, Amide, Materials Chemistry, Moiety, Amine gas treating, Physical and Theoretical Chemistry, Histidine, Conjugate

Abstract

In this work, histidine derivatives bearing an acetic acid or a propyl amine substituent on the N e -atom are conjugated to the b -acid, c -acid and d -acid moiety of cyanocobalamin (vitamin B12) via amide formation. Four different derivatives were prepared with different sites of conjugation ( b -, c - or d -acid) and different spacer lengths between histidine and the acid moiety. These conjugates can be efficiently labeled with [ 99m Tc(OH 2 ) 3 (CO) 3 ] + at yields higher than 95% under mild conditions (50 °C, 30 min, 10 −4 M). The biodistribution of the 99m Tc(CO) 3 labeled conjugates is determined in mice bearing B16-F10 melanoma tumors. The organ distribution varies significantly for each of the derivatives with the percentage injected dose per gram of tumor tissue ranging from 4.4 ± 0.9 to 9.2 ± 2.0.

Published

2004

16. Versatile synthetic approach to new bifunctional chelating agents tailor made for labeling with the fac-[M(CO)3]+ core (M = Tc, 99mTc, Re): synthesis, in vitro, and in vivo behavior of the model complex [M(APPA)(CO)3] (appa = [(5-amino-pentyl)-pyridin-2-yl-methyl-amino]-acetic acid)

Author

Albert Stichelberger, Roger Schibli, P.A Schubiger, Robert Waibel, and Cécile Dumas

Subjects

Cancer Research, Metabolic Clearance Rate, Stereochemistry, Carboxylic acid, Whole-Body Counting, Mice, chemistry.chemical_compound, Acetic acid, Drug Stability, Pyridine, Animals, Peptide bond, Tissue Distribution, Radiology, Nuclear Medicine and imaging, Chelation, Bifunctional, Radioisotopes, chemistry.chemical_classification, Mice, Inbred BALB C, Ligand, Organotechnetium Compounds, Cross-Linking Reagents, Rhenium, chemistry, Organ Specificity, Isotope Labeling, Molecular Medicine, Female, Amine gas treating, Radiopharmaceuticals

Abstract

A general synthetic approach for potent tridentate, bifunctional chelating agent (BFCA) for the [M(CO)(3)](+) fragment (M = (99g)Tc, (99m)Tc, and Re) has been elaborated. The strategy allows the facile preparation of BFCA with a pendent amino or carboxylic acid functionality for coupling to peptides and proteins via formation of an amide bond. [(5-amino-pentyl)-pyridin-2-yl-methyl-amino]-acetic acid (APPA) and [pyridin-2-yl-methyl-amino]-diacetic acid (PADA) were synthesized according to this protocol. The BFCA were labeled with the [M(CO)(3)](+) fragment, which resulted in formation of uniform products with a ligand to metal ratio of 1:1. The complexes have been fully characterized by means of mass spectrometry, IR, and NMR ((1)H, (13)C, (99)Tc) spectroscopy. Coordination of the tricarbonyl core with APPA and PADA was exclusively tridentate (via the acid function, the ternary amine, and the pyridine nitrogen). On the n.c.a. level the complexes were almost quantitatively formed (yield90%) at ligand concentrations of 10+/-2 microM (PADA) or 50+/-4 microM (APPA) after 30 min at 70 degrees C. Chromatographic behavior of the (99m)Tc complexes is similar to that of the corresponding (99)Tc/Re complexes suggesting the identical chemical structure. Pharmacokinetic experiments with the (99m)Tc-APPA complex were performed in BALB/c mice and compared with previously published results of the (99m)Tc-PADA complex. The (99m)Tc-APPA complex revealed good clearance from the blood pool (0.29 +/- 0.03% ID after 24h p.i.) and a low uptake in the liver (2.41 +/- 0.14% ID/g), in the kidneys (2.81 +/- 0.12% ID/g) and other tissue and organs.

Published

2003

17. Human scFv antibody fragments specific for the epithelial tumour marker MUC-1, selected by phage display on living cells

Author

Jean-Pierre Mach, Cindy Wong, Robert Waibel, R. Finnern, Michael D. Sheets, and Publica

Subjects

Cancer Research, Phage display, Molecular Sequence Data, Immunology, Biology, Epitope, Mice, Antigen, Tandem repeat, Peptide Library, Tumor Cells, Cultured, Animals, Humans, Immunology and Allergy, Amino Acid Sequence, Immunoglobulin Fragments, Binding selectivity, tumour, Mucin-1, Mucin, Molecular biology, In vitro, mucin MUC-1, Oncology, cell surface selection, Cell culture, Female, immunotherapy, phage display, human scFv, Epitope Mapping

Abstract

New anti-cancer agents are being developed that specifically recognise tumour cells. Recognition is dependent upon the enhanced expression of antigenic determinants on the surface of tumour cells. The tumour exposure and the extracellular accessibility of the mucin MUC-1 make this marker a suitable target for tumour diagnosis and therapy. We isolated and characterised six human scFv antibody fragments that bound to the MUC-1 core protein, by selecting a large naive human phage display library directly on a MUC-1-expressing breast carcinoma cell line. Their binding characteristics have been studied by ELISA, FACS and indirect immunofluorescence. The human scFv antibody fragments were specific for the tandem repeat region of MUC-1 and their binding is inhibited by soluble antigen. Four human scFv antibody fragments (M2, M3, M8, M12) recognised the hydrophilic PDTRP region of the MUC-1 core protein, which is thought to be an immunodominant region. The human scFv antibody fragments were stable in human serum at 37 degrees C and retained their binding specificity. For imaging or targeting to tumours over-expressing MUC-1, it might be feasible to use these human scFv, or multivalent derivatives, as vehicles to deliver anti-cancer agents.

Published

2001

18. Anti-neuroblastoma antibody chCE7 binds to an isoform of L1-CAM present in renal carcinoma cells

Author

F. Carrel, Pius A. Schubiger, Holger Moch, Hanspeter Amstutz, R Jaussi, M L Meli, N Crompton, Ilse Novak-Hofer, and Robert Waibel

Subjects

Cancer Research, Pathology, medicine.medical_specialty, Kidney, medicine.drug_class, Cell adhesion molecule, Biology, Monoclonal antibody, medicine.disease, Molecular biology, medicine.anatomical_structure, Oncology, Cell culture, Neuroblastoma, medicine, Carcinoma, biology.protein, Northern blot, Antibody

Abstract

Immunoprecipitation after cell surface labeling of human neuroblastoma cells showed that the anti-neuroblastoma monoclonal antibody (mAb) chCE7 binds to a 200,000 M(r) cell surface protein. The protein was partially purified by immuno-affinity chromatography from a human renal carcinoma and a human neuroblastoma cell line, which both showed high levels of binding of MAb chCE7. NH(2)-terminal sequences of 18 and 15 amino acid residues were determined. Both sequences isolated from the renal carcinoma and the neuroblastoma cells showed strong homology to human cell adhesion molecule L1 (L1-CAM), and both were characterized by the NH(2)-terminal deletion of 5 amino acids, comprising exon 2 of L1-CAM. Reverse trancription-polymerase chain reaction (RT-PCR) analysis of the regions spanning exon 2 and exon 27 of L1-CAM indicated that in neuroblastoma cells both transcripts for the full-length and exon-deleted forms are present, whereas in the renal carcinoma cell lines only the exon-deleted L1-CAM isoform were detected. Western blot analysis showed that 6 of 7 tested renal carcinoma cell lines and 5 of 15 renal carcinoma tissues expressed L1-CAM. In normal adult kidney tissue, very low levels of protein expression were found. Northern blot analysis confirmed that in renal carcinoma and neuroblastoma cell lines L1-CAM mRNA levels are correlated with protein expression.

Published

1999

19. Basic aqueous chemistry of [M(OH2)3(CO)3]+ (M=Re, Tc) directed towards radiopharmaceutical application

Author

August P. Schubiger, Robert Waibel, Roger Alberto, Roger Schibli, and Ulrich Abram

Subjects

chemistry.chemical_classification, Aqueous solution, Lability, Chemistry, Stereochemistry, Bioorganometallic chemistry, Medicinal chemistry, Coordination complex, Inorganic Chemistry, chemistry.chemical_compound, Materials Chemistry, Molecule, Imidazole, Moiety, Titration, Physical and Theoretical Chemistry

Abstract

A review on the synthesis and properties of the organometallic aqua-ion [M(OH2)3(CO)3]+ (M=Re, 99Tc, 99mTc), as relevant for radiopharmaceutical application, is presented. These important starting compounds can be prepared quantitatively, (a) on the no carrier added (n.c.a.) level (99mTc) in water, or (b) in organic solvents (Re, 99Tc) at atmospheric pressure in a short time and from [MO4]−. The main characteristics of these carbonyl complexes are the high substitution stability of the three CO ligands and the substitution lability of the coordinated water molecules. [M(OH2)3(CO)3]+ can be considered as a ‘semi aquo–ion’. On the macroscopic level, upon titration with OH−, hydroxo-bridged oligomers have been isolated and characterized. The formation of hydroxo-bridged complexes is a consequence of the considerable Bronstedt acidity of [M(OH2)3(CO)3]+, whereas on the n.c.a. level no such behavior was observed. Conditions and products of the water exchange by imidazole (im) and derivatives thereof (histamine, histidine) will be presented. The different mononuclear complexes with these ligands are of extraordinary inertness, which is the basis for potential applications in biology and nuclear medicine. Finally, as a basis for bioorganometallic chemistry, the adoption of the results from basic coordination chemistry to the labeling of biomolecules with an organometallic moiety will be exemplified with a selected penta-peptide and a recombinant single chain fragment.

Published

1999

20. Tumor Imaging in Patients with Advanced Tumors Using a New 99mTc-Radiolabeled Vitamin B12 Derivative

Author

Irene A. Burger, Ebba Nexo, Pius A. Schubiger, Peter Bläuenstein, Niklaus Schaefer, Lotta von Boehmer, Jan Soyka, Stefan K. Haerle, Anass Johayem, Roger Schibli, Alexander Knuth, Ennio Müller, Robert Waibel, Eliane Fischer, Bert-Ram Sah, University of Zurich, and Burger, Irene A

Subjects

Male, cancer, cobalamin, haptocorrin, transcobalamin receptors, vitamin B12, medicine.medical_specialty, Time Factors, Haptocorrin, Biopsy, Urology, 610 Medicine & health, Breast Adenocarcinoma, Scintigraphy, Cobalamin, Multimodal Imaging, Sensitivity and Specificity, chemistry.chemical_compound, Transcobalamin, Neoplasms, medicine, polycyclic compounds, Humans, 2741 Radiology, Nuclear Medicine and Imaging, Radiology, Nuclear Medicine and imaging, Tissue Distribution, Whole Body Imaging, Vitamin B12, Prospective Studies, Neoplasm Metastasis, Radionuclide Imaging, Aged, Aged, 80 and over, Tomography, Emission-Computed, Single-Photon, medicine.diagnostic_test, business.industry, Cancer, Technetium, Organotechnetium Compounds, 10181 Clinic for Nuclear Medicine, Middle Aged, medicine.disease, Vitamin B 12, chemistry, Cancer cell, Female, Radiopharmaceuticals, business, Tomography, X-Ray Computed

Abstract

Targeting cancer cells with vitamin B12 (cobalamin) is hampered by unwanted physiologic tissue uptake mediated by transcobalamin. Adhering to good manufacturing practice, we have developed a new (99m)Tc-cobalamin derivative ((99m)Tc(CO)3-[(4-amido-butyl)-pyridin-2-yl-methyl-amino-acetato] cobalamin, (99m)Tc-PAMA-cobalamin). The derivative shows no binding to transcobalamin but is recognized by haptocorrin, a protein present in the circulation and notably expressed in many tumor cells. In this prospective study, we investigated cancer-specific uptake of (99m)Tc-PAMA-cobalamin in 10 patients with various metastatic tumors. METHODS: Ten patients with biopsy-proven metastatic cancer were included. Dynamic imaging was started immediately after injection of 300-500 MBq of (99m)Tc-PAMA-cobalamin, and whole-body scintigrams were obtained at 10, 30, 60, 120, and 240 min and after 24 h. The relative tumor activity using SPECT/CT over the tumor region after 4 h was measured in comparison to disease-free lung parenchyma. Patients 3-10 received between 20 and 1,000 μg of cobalamin intravenously before injection of (99m)Tc-PAMA-cobalamin. The study population comprised 4 patients with adenocarcinomas of the lung, 3 with squamous cell carcinomas of the hypopharyngeal region, 1 with prostate adenocarcinoma, 1 with breast, and 1 with colon adenocarcinoma. RESULTS: The median age of the study group was 61 ± 11 y. Six of 10 patients showed positive tumor uptake on (99m)Tc-PAMA-cobalamin whole-body scintigraphy. The scan was positive in 1 patient with colon adenocarcinoma, in 3 of 4 lung adenocarcinomas, in 1 of 3 hypopharyngeal squamous cell carcinomas, and in 1 breast adenocarcinoma. Renal uptake was between 1% and 3% for the left kidney. Predosing with cobalamin increased the tumor uptake and improved blood-pool clearance. The best image quality was achieved with a predose of 20-100 ug of cold cobalamin. The mean patient dose was 2.7 ± 0.9 mSv/patient. CONCLUSION: To our knowledge, we report for the first time on (99m)Tc-PAMA-cobalamin imaging in patients with metastatic cancer disease and show that tumor targeting is feasible. Targeting cancer cells with vitamin B12 (cobalamin) is hampered by unwanted physiologic tissue uptake mediated by transcobalamin. Adhering to good manufacturing practice, we have developed a new (99m)Tc-cobalamin derivative ((99m)Tc(CO)3-[(4-amido-butyl)-pyridin-2-yl-methyl-amino-acetato] cobalamin, (99m)Tc-PAMA-cobalamin). The derivative shows no binding to transcobalamin but is recognized by haptocorrin, a protein present in the circulation and notably expressed in many tumor cells. In this prospective study, we investigated cancer-specific uptake of (99m)Tc-PAMA-cobalamin in 10 patients with various metastatic tumors.

Published

2014

21. Differential inhibitory effect of L-lysine on renal accumulation of67Cu-labelled F(ab′)2 fragments in mice

Author

Alan Smith, P. August Schubiger, Richard A.D. Rutherford, and Robert Waibel

Subjects

chemistry.chemical_classification, Cancer Research, Kidney, biology, Ratón, Renal cortex, Lysine, Diuresis, Molecular biology, Amino acid, medicine.anatomical_structure, Oncology, chemistry, Biochemistry, Pharmacokinetics, medicine, biology.protein, Antibody

Abstract

The basic amino acid L-lysine was administered to mice in an attempt to circumvent unwanted renal accumulation of 67Cu-labelled F(ab')2 fragments derived from the anti-NCAM IgG1, SEN7 and anti-CEA IgG1 monoclonal antibody (MAb)35. In control experiments, significant renal uptake of both 67Cu-labelled F(ab')2 fragments was observed, radiolabel being primarily localised to proximal tubules in the renal cortex. Following optimised L-lysine dosing protocols, renal uptake of 67Cu-MAb35 F(ab')2 was inhibited by up to 42%. Surprisingly, little inhibition (< 10%) of 67Cu-SEN7 F(ab')2 uptake was observed. Experiments to investigate this differential inhibition indicated that inhibition of MAb35 F(ab')2 uptake was relatively short-lived (approx. 6 hr), whilst no apparent differences were found in blood clearance rates between either 67Cu-F(ab')2 fragment. L-lysine administration caused a significant diuresis with high levels of intact 67Cu-labelled SEN7 and MAb35 F(ab')2 appearing in the urine, possibly due to blockade of renal uptake and lysine-induced increases in glomerular membrane permeability. Iso-electric focusing studies failed to identify any charge differences between the 67Cu-labelled F(ab')2 fragments, although a cathodal migration of all 67Cu-labelled samples, presumably due to the net positive charge conferred by addition of 67Cu2+ ions, was observed. Our results demonstrate that in addition to net charge, other unidentified characteristics may influence renal accumulation of radiometal-labelled F(ab')2 fragments and their inhibition by L-lysine.

Published

1997

22. A comparison of67Cu- and131I-labelled forms of monoclonal antibodies SEN7 and SWA20 directed against small-cell lung cancer

Author

Rolf A. Stahel, P. August Schubiger, Robert Waibel, Uwe Zangemeister-Wittke, Thomas Schenker, and Alan Smith

Subjects

Cancer Research, Pathology, medicine.medical_specialty, Lung Neoplasms, Time Factors, medicine.drug_class, Transplantation, Heterologous, Mice, Nude, Heterologous, Spleen, Monoclonal antibody, Iodine Radioisotopes, Immunoglobulin Fab Fragments, Mice, In vivo, medicine, Animals, Humans, Tissue Distribution, Carcinoma, Small Cell, biology, Antibodies, Monoclonal, Biological activity, Molecular biology, In vitro, Transplantation, medicine.anatomical_structure, Copper Radioisotopes, Radioimmunodetection, Oncology, Immunoglobulin G, biology.protein, Female, Indicators and Reagents, Antibody

Abstract

The intact anti-SCLC monoclonal antibody (MAb) SEN7 and its F(ab')2 were labelled with the beta-emitting isotope 67Cu. Both materials retained their biological activity in vitro as determined by the Lindmo assay. In a direct comparison of in vivo distribution in a xenograph model, 131I- and 67Cu-labelled intact SEN7 showed similar absolute tumour accumulation. Blood levels were markedly lower in the case of the 67Cu-labelled antibody, resulting in improved tumour:blood ratios which reached a maximum of 13:1 compared with only 4.5:1 for 131I-SEN7. In the case of the 67Cu-labelled F(ab')2, very high accumulation of the nuclide was observed in the kidney. Levels of radio copper in liver and spleen were also found to be significantly raised when compared with radio iodine. SWA20, a MAb which had previously failed to show any selective in vivo accumulation in tumour xenografts when labelled with radio iodine showed higher and more stable tumour accumulation when labelled with 67Cu.

Published

1994

23. Immunotoxins recognising a new epitope on the neural cell adhesion molecule have potent cytotoxic effects against small cell lung cancer

Author

Uwe Zangemeister-Wittke, A. R. Collinson, Robert Waibel, B. Frösch, T. Schenker, and Rolf A. Stahel

Subjects

Cancer Research, Lung Neoplasms, Virulence Factors, Cell Adhesion Molecules, Neuronal, Bacterial Toxins, Exotoxins, Ricin, Biology, Epitope, Epitopes, Antibody Specificity, Immunotoxin, Culture Techniques, Tumor Cells, Cultured, Humans, Cytotoxic T cell, Pseudomonas exotoxin, Carcinoma, Small Cell, Clonogenic assay, ADP Ribose Transferases, Cell adhesion molecule, Immunotoxins, Antibodies, Monoclonal, Drug Synergism, Virology, Molecular biology, Neoplasm Proteins, Kinetics, Oncology, Cell culture, Neural cell adhesion molecule, Research Article

Abstract

The present study describes a comparison of two potent immunotoxins which utilise an identical targeting component, a monoclonal antibody (SEN7) specific for small cell lung cancer (SCLC), conjugated to two different effector components, blocked ricin (bR) and Pseudomonas exotoxin A (PE). SEN7 recognises a novel epitope on the neural cell adhesion molecule (NCAM) which is highly associated with SCLC. The immunotoxins SEN7-PE and SEN7-bR were selectively and potently active against a number of SCLC cell lines, of both classic and variant morphologies, inhibiting the incorporation of [3H]leucine with IC50 values ranging between 22 pM and 85 pM and between 7 pM and 62 pM for SEN7-PE and SEN7-bR respectively. Intoxication by both immunotoxins proceeded rapidly following short 2 h lag phases; the initial rates of protein synthesis inhibition occurred with t50 values of 6.5 h for SEN7-PE and 5.5 h for SEN7-bR. Monensin drastically enhanced the cytotoxic activity of the weakly active SEN7-ricin A-chain by 2,100-fold and of SEN7-bR by 80-fold but had no effect on SEN7-PE. In limiting dilution assays, four and more than 4.5 logs of clonogenic SW2 tumour cells were selectively eliminated from the cultures during continuous exposure to the immunotoxins SEN7-PE and SEN7-bR respectively, while antigen-negative cells required up to 1,000-fold more drug for a similar cell kill. SW2 cells surviving SEN7-bR treatment in the cultures did not express NCAM and consequently were not selectively killed by SEN7 immunotoxins. SW2 cells surviving continuous exposure to SEN7-PE showed no alteration in NCAM expression but were more resistant to intoxication mediated by PE. These cells were still sensitive to SEN7-bR. Images Figure 1

Published

1994

24. Anti-tumor activity of a blocked ricin immunotoxin with specificity against the cluster-5A antigen associated with human small-cell lung cancer

Author

Rolf A. Stahel, Robert Waibel, Uwe Zangemeister-Wittke, Robert M. L. Jones, Albert R. Collinson, Igor Fisch, and Hans-Peter Lehman

Subjects

Cancer Research, Lung Neoplasms, medicine.drug_class, Mice, Nude, Ricin, Biology, Monoclonal antibody, Mice, chemistry.chemical_compound, Antigen, Antigens, Neoplasm, Immunotoxin, Galactose binding, Tumor Cells, Cultured, medicine, Animals, Humans, Carcinoma, Small Cell, Cytotoxicity, Mice, Inbred ICR, Immunotoxins, Antibodies, Monoclonal, Virology, Molecular biology, Oncology, chemistry, Cell culture, biology.protein, Female, Antibody

Abstract

The monoclonal antibody (MAb) SEN3I, a mouse IgG1 which recognizes the cluster-5a antigen on small-cell lung cancer (SCLC) cells, was used to prepare a selective and potent blocked ricin immunotoxin. In a series of experiments in vitro and in a SCLC xenograft model in nude mice, the tumor localization potential of the radiolabeled antibody SEN31 and the anti-tumor activity of the immunotoxin SEN31-bR, the non-specific binding activity of which had been greatly reduced by blocking of the galactose binding domains of the B-chain, was determined. Radiolabeling of SEN31 was performed by linking a 67Ga-labeled desferrioxamine moiety to the oligosaccharide side chains of the antibody in order to preserve the specific cell-binding activity. 67Ga-SEN31 bound to the antigenic sites on cells of the SW2 SCLC cell line, with a dissociation constant of 3.5 nM and, when injected i.v., selectively localized at the site of s.c.-growing SW2 tumor xenografts in nude mice, with a tumor-to-blood ratio of 3.5. The immunotoxin SEN31 -bR was potently and selectively active against SCLC cell lines both of classic and of variant morphologies. At a concentration of 300 pM the immunotoxin selectively eliminated 4.5 logs of clono-genic tumor cells. In nude mice, SEN31 -bR was cleared from the blood with biphasic kinetics following i.v. injection and maintained a stable serum level during continuous i.p. infusion. The growth of s.c. SW2 solid-tumor xenografts was delayed following a single i.v. injection or a continuous i.p. infusion, each at a non-toxic dose.

Published

1993

25. Action of a cd24-specific deglycosylated ricin-a-chain immunotoxin in conventional and novel models of small-cell-lung-cancer xenograft

Author

Edward J. Wawrzynczak, Rolf A. Stahel, Uwe Zangemeister-Wittke, Robert Waibel, and Hans-Peter Lehmann

Subjects

Cancer Research, Pathology, medicine.medical_specialty, Glycosylation, Lung Neoplasms, Cell Survival, Metabolic Clearance Rate, Population, Mice, Nude, Ricin, In Vitro Techniques, Biology, Mice, Tissue culture, Antigen, Antigens, CD, In vivo, Immunotoxin, Tumor Cells, Cultured, medicine, Animals, Humans, Carcinoma, Small Cell, education, Cytotoxicity, Clonogenic assay, education.field_of_study, Membrane Glycoproteins, Immunotoxins, CD24 Antigen, Flow Cytometry, Oncology, Cell culture, Cancer research, Female, Neoplasm Transplantation

Abstract

The therapeutic efficacy of an immunotoxin, SWAII-SPDB-dg.ricin A chain, recognizing the leukocyte-differentiation antigen CD24, was evaluated against SCLC cell lines in tissue culture and in 2 nude-mouse models. The first model used conventional s.c. solid-tumor xenografts. The second used small tumor-cell deposits established in s.c. implanted sponge matrices and allowed us to directly estimate the killing efficiency of the immunotoxin under experimentally defined conditions in vivo. It also mimics the clinical setting of disseminated tumor cells which form the basis of residual disease in SCLC. The cytotoxic potency of SWAII-SPDB-dg.ricin A chain was demonstrated in tissue culture by the inhibition of 3H-leucine incorporation and by the selective elimination of CD24-positive tumor cells in clonogenic assays. In nude mice, SWAII-SPDB-dg.ricin A chain was cleared from the blood circulation with biphasic kinetics: an initial alpha phase of 1 hr and a second beta phase of 20.5 hr. Following i.v. injection of a dose equivalent to 30% of the LD50, the immunotoxin delayed the growth of SW2 solid-tumor xenografts by 16 days. The therapeutic efficacy of SWAII-SPDB-dg.ricin A chain was further demonstrated by the selective elimination of clonogenic SW2 cells from small tumor-cell deposits established in sponge matrices. Regrowth of the solid tumors after the initial response and the clonogenic activity in the sponge-derived cell population were mediated by CD24-positive cells, excluding the selection of CD24-negative mutants during immunotoxin therapy.

Published

1993

26. A preliminary comparison of methods for production of 188Re-C595 antibody for radioimmunotherapy of bladder cancer

Author

Alan C. Perkins, Robert Waibel, D. P. Scholfield, R. M. Vincent, I. Novak, Roger Schibli, and Andrea Murray

Subjects

Bladder cancer, biology, Chemistry, Stereochemistry, medicine.drug_class, medicine.medical_treatment, Organic Chemistry, medicine.disease, Monoclonal antibody, Biochemistry, Analytical Chemistry, Radioimmunotherapy, Labelling, Drug Discovery, medicine, Cancer research, biology.protein, Radiology, Nuclear Medicine and imaging, Antibody, Spectroscopy, Ex vivo, Conjugate

Abstract

Two different methods (reduction mediated and carbonyl labelling) for conjugating 188Re to an anti-tumour monoclonal antibody are described. The radioimmunoconjugates produced were analysed for stability, immunoreactivity, specificity and homogeneity. This indicated that although the two conjugates were comparable in terms of specificity and homogeneity, the carbonyl labelled preparation was more stable. Tumour localisation of both conjugates was confirmed in an ex vivo model of bladder cancer. It is concluded that although both radioimmunoconjugates have potential for intravesical therapy of bladder cancer, carbonyl labelling may offer a method with increased stability.

Published

2001

27. Chemical modifications of 99mTc tricarbonyl labeled single chain antibody fragments for improved in vivo behavior in tumor targeting

Author

Robert Waibel, K. Chester, A. Stichelberger, Pius A. Schubiger, Ilse Novak-Hofer, and H. Jager

Subjects

Tumor targeting, biology, Organic Chemistry, Kinetics, Succinic anhydride, Single chain, Biochemistry, Molecular biology, Antibody fragments, Analytical Chemistry, chemistry.chemical_compound, chemistry, In vivo, Drug Discovery, biology.protein, Radiology, Nuclear Medicine and imaging, Antibody, Spectroscopy, Renal uptake

Abstract

One of the major limitations of using intact immunoglobulins for targeting tumors is the poor penetration into tissues. Although small single chain Fv (scFv) antibody fragments have been used because of their improved kinetics, some exhibit high renal accumulation. In this study we show a significant reduction of renal accumulation of His-tagged scFv's directly labelled with 99mTc-tricarbonyl by use of succinic anhydride. Further decrease of renal uptake will make this approach hopefully suitable for therapeutic application, using 188/186Re(I)-tricarbonyl.

Published

2001

28. 99mTc-labeled cobalamin and cobinamide

Author

Susanne Kunze, Kirstin Ortner, Stefan Mundwiler, Roger Alberto, and Robert Waibel

Subjects

chemistry.chemical_compound, Biochemistry, Chemistry, Organic Chemistry, Drug Discovery, Radiology, Nuclear Medicine and imaging, Cobalamin, Spectroscopy, Analytical Chemistry

Published

2001

29. Efficient tumor targeting with high-affinity designed ankyrin repeat proteins: effects of affinity and molecular size

Author

Robert Waibel, Christian Zahnd, Martin Kawe, H. Kaspar Binz, Christine de Pasquale, Andreas Plückthun, Roger Schibli, Gabriela Nagy-Davidescu, Rastislav Tamaskovic, Michael T. Stumpp, Birgit Dreier, University of Zurich, and Plückthun, A

Subjects

Cancer Research, medicine.drug_class, Antibody Affinity, Mice, Nude, Antineoplastic Agents, Monoclonal antibody, Protein Engineering, Substrate Specificity, Mice, Nude mouse, Drug Delivery Systems, Neoplasms, medicine, Tumor Cells, Cultured, 10019 Department of Biochemistry, Animals, Humans, 1306 Cancer Research, biology, Molecular mass, Chemistry, Immunoglobulin Fc Fragments, Proteins, Protein engineering, biology.organism_classification, Molecular biology, Xenograft Model Antitumor Assays, Ankyrin Repeat, Molecular Weight, Treatment Outcome, Oncology, DARPin, Drug Design, Immunology, PEGylation, 570 Life sciences, Ankyrin repeat, Female, 2730 Oncology

Abstract

Slow-clearing, tumor-targeting proteins such as monoclonal antibodies typically exhibit high tumor accumulation but low tissue contrast, whereas intermediate-sized proteins such as scFvs show faster clearance but only moderate tumor accumulation. For both, tumor targeting does not seem to improve further above an optimal affinity. We show here that with very small high-affinity proteins such as designed ankyrin repeat proteins (DARPins), these limits can be overcome. We have systematically investigated the influence of molecular mass and affinity on tumor accumulation with DARPins with specificity for HER2 in SK-OV-3.ip nude mouse xenografts. DARPins with a mass of 14.5 kDa and affinities between 270 nmol/L and 90 pmol/L showed a strong correlation of tumor accumulation with affinity to HER2, with the highest affinity DARPin reaching 8% ID/g after 24 hours and 6.5% ID/g after 48 hours (tumor-to-blood ratio >60). Tumor autoradiographs showed good penetration throughout the tumor mass. Genetic fusion of two DARPins (30 kDa) resulted in significantly lower tumor accumulation, similar to values observed for scFvs, whereas valency had no influence on accumulation. PEGylation of the DARPins increased the circulation half-life, leading to higher tumor accumulation (13.4% ID/g after 24 hours) but lower tumor-to-blood ratios. Affinity was less important for tumor uptake of the PEGylated constructs. We conclude that two regimes exist for delivering high levels of drug to a tumor: small proteins with very high affinity, such as unmodified DARPins, and large proteins with extended half-life, such as PEGylated DARPins, in which the importance of affinity is less pronounced. Cancer Res; 70(4); 1595–605

Published

2010

30. Molecular and biological properties of an abrin A chain immunotoxin designed for therapy of human small cell lung cancer

Author

Uwe Zangemeister-Wittke, G. D. Parnell, Robert Waibel, A. J. Cumber, Rolf A. Stahel, M. Jones, E. J. Wawrzynczak, and R. V. Henry

Subjects

Male, Cancer Research, Lung Neoplasms, Cell Survival, Macromolecular Substances, Transplantation, Heterologous, Mice, Nude, Butyrate, Biology, Cell Line, chemistry.chemical_compound, Mice, Affinity chromatography, Antigen, Immunotoxin, Animals, Humans, Carcinoma, Small Cell, Cytotoxicity, Immunotoxins, Antibodies, Monoclonal, Kinetics, Oncology, chemistry, Biochemistry, Cell culture, Drug Design, biology.protein, Abrin, Antibody, Ribosomes, Neoplasm Transplantation, Research Article

Abstract

An immunotoxin (IT) comprising abrin A chain attached to the mouse monoclonal antibody SWA11, recognising a cell surface antigen highly associated with human small cell lung cancer (SCLC), was synthesised using a hindered disulphide crosslinker, N-succinimidyl 3-(2-pyridyldithio) butyrate (SPDB), and purified by Blue Sepharose CL-6B affinity chromatography. The IT preparation contained monomeric conjugate, composed of one abrin A chain molecule linked to one SWA11 molecule, and was free from unconjugated A chain or antibody. The IT fully retained the cell-binding capacity of the antibody component and the ribosome-inactivating activity of the A chain. In cytotoxicity assays using the SW2 SCLC cell line in tissue culture, SWA11-SPDB-abrin A chain inhibited the incorporation of 3H-leucine by 50% at a concentration of 10 pM and by 99% at a concentration of 1 nM. The anti-tumour efficacy of the IT was tested in nude mice bearing established s.c. solid SW2 tumour xenografts. A single i.v. injection of SWA11-SPDB-abrin A chain at a non-toxic dose induced a significant 7 to 10 day growth delay that could not be matched by administration of equivalent doses of either unconjugated SWA11 or abrin A chain alone. The results of this study indicate that the antigen recognised by SWA11 is an effective target for therapy of SCLC with A chain ITs in vivo. Images Figure 1

Published

1992

31. Selective immunotherapy of small cell cancer xenografts using 131I-labelled SWA11 antibody

Author

Robert Waibel, Rolf A. Stahel, and A Smith

Subjects

Cancer Research, Pathology, medicine.medical_specialty, Necrosis, Lung Neoplasms, medicine.medical_treatment, Transplantation, Heterologous, Mice, Nude, Iodine Radioisotopes, Mice, Nude mouse, medicine, Carcinoma, Animals, Humans, Carcinoma, Small Cell, biology, Antibodies, Monoclonal, Immunotherapy, biology.organism_classification, medicine.disease, Transplantation, Regimen, Oncology, Radioimmunotherapy, biology.protein, Antibody, medicine.symptom, Neoplasm Transplantation, Research Article

Abstract

Intact SWA11 antibody was evaluated as a potential radioimmunotherapeutic agent against small cell lung cancer xenografts in a nude mouse model system. 131I-labelled SWA11 was given either in a single injection regimen (1 x 300 microCi) or as a multiple injection regimen achieving a total of 900 microCi (3 x 300 microCi with a 2 week interval between injections). Treatment of both small (mean volume approximately 0.2 cm3) and large (mean volume approximately 1.0 cm3) established xenografts resulted in significant anti-tumour effects and, in the case of the fractionated protocol, the failure of the xenografts to regrow within the period of observation (84 days). Xenograft histology following radioimmunotherapy showed large areas of necrosis, fibrosis and very few residual cells of SCLC origin. Images Figure 5

Published

1991

32. New derivatives of vitamin B12 show preferential targeting of tumors

Author

Susanne Kunze, Stefan Mundwiler, Holger Moch, Jakob Nuesch, Martin Küenzi, Pius A. Schubiger, Alexander Knuth, Hansjörg Treichler, Niklaus Schaefer, Roger Alberto, Roger Schibli, Dave R. van Staveren, Robert Waibel, University of Zurich, and Waibel, R

Subjects

Vitamin, 10120 Department of Chemistry, Cancer Research, Antineoplastic Agents, 610 Medicine & health, chemistry.chemical_compound, Transcobalamin, Cell Line, Tumor, 10049 Institute of Pathology and Molecular Pathology, 540 Chemistry, medicine, Humans, Distribution (pharmacology), 1306 Cancer Research, Vitamin B12, Receptor, Melanoma, Transcobalamins, Carcinoma, Cancer, Biological Transport, 10181 Clinic for Nuclear Medicine, medicine.disease, Kidney Neoplasms, Transport protein, Vitamin B 12, Urinary Bladder Neoplasms, Oncology, Biochemistry, chemistry, Cell culture, 10032 Clinic for Oncology and Hematology, Cancer research, 2730 Oncology

Abstract

Rapidly growing cells show an increased demand for nutrients and vitamins. The objective of our work is to exploit the supply route of vitamin B12 to deliver new derivatives of this vital vitamin to hyperproliferative cells. To date, radiolabeled (57Co and 111In) vitamin B12 derivatives showed labeling of tumor tissue but also undesired high accumulation of radioactivity in normal tissue. By abolishing the interaction of a tailored vitamin B12 derivative to its transport protein transcobalamin II and therefore interrupting transcobalamin II receptor and megalin mediated uptake in normal tissue, preferential accumulation of a radiolabeled vitamin in cancer tissue could be accomplished. We identified transcobalamin I on tumors as a possible new receptor for this preferential accumulation of vitamin-mediated targeting. The low systemic distribution of radioactivity and the high tumor to blood ratio opens the possibility of a more successful clinical application of vitamin B12 for imaging or therapy. [Cancer Res 2008;68(8):2904–11]

Published

2008

33. Selective cytotoxic effects of a ricin A chain immunotoxin made with the monoclonal antibody SWA11 recognising a human small cell lung cancer antigen

Author

G. D. Parnell, E. J. Derbyshire, A Smith, Rolf A. Stahel, Robert Waibel, E. J. Wawrzynczak, and R. V. Henry

Subjects

Cancer Research, Lung Neoplasms, medicine.drug_class, Enzyme-Linked Immunosorbent Assay, Ricin, In Vitro Techniques, Biology, Monoclonal antibody, chemistry.chemical_compound, Antigen, Antigens, Neoplasm, Immunotoxin, medicine, Humans, Cytotoxic T cell, Carcinoma, Small Cell, Cytotoxicity, Cells, Cultured, Dose-Response Relationship, Drug, Immunotoxins, Antibodies, Monoclonal, Virology, Molecular biology, Oncology, chemistry, Cell culture, biology.protein, Antibody, Research Article

Abstract

The potential of mouse monoclonal antibodies for recognising different antigens associated with human small cell lung cancer (SCLC) to form active immunotoxins was assessed by an indirect in vitro screening assay. The screening agent used was a conjugate made by linking ricin A chain to a sheep anti-mouse IgG Fab' fragment via a disulphide bond. The monoclonal antibodies SWA11 and SWA20 both mediated the toxic effects of ricin A chain against the HC12 classic SCLC cell line in dose-dependent fashion. The SWA11 antibody was the more effective; in combination with the screening agent at a concentration of 1 x 10(-7) M, it inhibited the incorporation of [3H] leucine into HC12 cells by 94% compared with only 44% inhibition in the case of SWA20. An immunotoxin made by the direct chemical conjugation of ricin A chain to SWA11 exhibited selective toxic effects upon HC12 cells in tissue culture inhibiting the incorporation of [3H] leucine by 50% at a concentration (IC50) of 6.2 x 10(-10) M and by 98% at 1 x 10(-7) M. SWA11-ricin A chain had an IC50 of 4.4 x 10(-10) M against the NCI-H69 classic SCLC cell line but showed no cytotoxic activity against the human lung adenocarcinoma cell line NCI-H23 at a concentration of 1 x 10(-8) M.

Published

1990

34. PEGylation and multimerization of the anti-p185HER-2 single chain Fv fragment 4D5: effects on tumor targeting

Author

Susanne, Kubetzko, Ela, Balic, Robert, Waibel, Uwe, Zangemeister-Wittke, and Andreas, Plückthun

Subjects

Models, Molecular, Ovarian Neoplasms, Receptor, ErbB-2, Antibody Affinity, Immunoglobulin Variable Region, Mice, Nude, Antibodies, Polyethylene Glycols, Kinetics, Mice, Protein Transport, Structure-Activity Relationship, Antibody Specificity, Cell Line, Tumor, Animals, Humans, Female, Immunoglobulin Fragments, Protein Binding

Abstract

A major goal in antibody design for cancer therapy is to tailor the pharmacokinetic properties of the molecule according to specific treatment requirements. Key parameters determining the pharmacokinetics of therapeutic antibodies are target specificity, affinity, stability, and size. Using the p185HER-2 (HER-2)-specific scFv 4D5 as model system, we analyzed how changes in molecular weight and valency independently affect antigen binding and tumor localization. By employing multimerization and PEGylation, four different antibody formats were generated and compared with the scFv 4D5. First, dimeric and tetrameric miniantibodies were constructed by fusion of self-associating, disulfide-linked peptides to the scFv 4D5. Second, we attached a 20-kDa PEG moiety to the monovalent scFv and to the divalent miniantibody at the respective C terminus. In all formats, serum stability and full binding reactivity of the scFv 4D5 were retained. Functional affinity, however, did change. An avidity increase was achieved by multimerization, whereas PEGylation resulted in a 5-fold decreased affinity. Nevertheless, the PEGylated monomer showed an 8.5-fold, and the PEGylated dimer even a 14.5-fold higher tumor accumulation than the corresponding scFv, 48 h post-injection, because of a significantly longer serum half-life. In comparison, the non-PEGylated bivalent and tetravalent miniantibodies showed only a moderate increase in tumor localization compared with the scFv, which correlated with the degree of multimerization. However, these non-PEGylated formats resulted in higher tumor-to-blood ratios. Both multimerization and PEGylation represent thus useful strategies to tailor the pharmacokinetic properties of therapeutic antibodies and their combined use can additively improve tumor targeting.

Published

2006

35. Immunoscintigraphy of patients with head and neck carcinomas, with an anti-angiogenetic antibody fragment

Author

Daniel M. Schmid, Stephen Schmid, Christina Thuerl, Gerrhard W. Goerres, Dario Neri, August P. Schubiger, Robert Waibel, Sandro J. Stoeckli, and Manfred Birchler

Subjects

Male, Pathology, medicine.medical_specialty, Angiogenesis, Cell, Antibodies, Immunoscintigraphy, 03 medical and health sciences, 0302 clinical medicine, Medicine, Humans, 030223 otorhinolaryngology, Radionuclide Imaging, biology, medicine.diagnostic_test, Neovascularization, Pathologic, business.industry, medicine.disease, Primary tumor, Fibronectins, Fibronectin, medicine.anatomical_structure, Otorhinolaryngology, Positron emission tomography, Head and Neck Neoplasms, 030220 oncology & carcinogenesis, biology.protein, Carcinoma, Squamous Cell, Surgery, Tomography, Antibody, business, Nuclear medicine

Abstract

Objective In a phase I/II clinical study, we investigated tumor targeting in patients with head and neck squamous cell carcinomas (SCC), using an antibody directed against the extra-domain-B of fibronectin (EDB), a marker of angiogenesis and tissue remodeling. Study Design and Setting Five patients with SCC were injected with the 123-iodine-radiolabeled L19(scFv)2 antibody and underwent scintigraphic detection with single photon emission tomography with computerized tomography (SPECT/CT). In addition, 18F-fluorodeoxyglucose (18FDG) positron emission tomography with computerized tomography (PET/CT) was performed. Results Successful targeting of the primary tumor could be achieved in 4 of 5 patients and was comparable to PET imaging. No side effects were observed. Conclusions Tumor targeting with the L19(scFv)2 antibody is also feasible for head and neck SCC. Significance These results may serve as a base for future therapeutical applications in human beings, with modified versions of the L19(scFv)2 antibody, designed to selectively deliver bioactive molecules into malignant tumors.

Published

2006

36. Radiometal labeling of antibodies and antibody fragments for imaging and therapy

Author

Ilse, Novak-Hofer, Robert, Waibel, Kurt, Zimmermann, Roger, Schibli, Jürgen, Grünberg, Kerry A, Chester, Andrea, Murray, Benny K C, Lo, Alan C, Perkins, and P August, Schubiger

Subjects

Radioisotopes, Metals, Immunoglobulin Fragments, Antibodies, Chromatography, High Pressure Liquid

Published

2004

37. Radiometal Labeling of Antibodies and Antibody Fragments for Imaging and Therapy

Author

Ilse Novak-Hofer, Robert Waibel, Kurt Zimmermann, Roger Schibli, Jürgen Grünberg, Kerry A. Chester, Andrea Murray, Benny K.C. Lo, Alan C. Perkins, and P. August Schubiger

Subjects

Text mining, biology, business.industry, Chemistry, biology.protein, Antibody, business, Molecular biology, Antibody fragments

Published

2004

38. A recombinant immunotoxin derived from a humanized epithelial cell adhesion molecule-specific single-chain antibody fragment has potent and selective antitumor activity

Author

Claudio, Di Paolo, Jörg, Willuda, Susanne, Kubetzko, Ikar, Lauffer, Dominique, Tschudi, Robert, Waibel, Andreas, Plückthun, Rolf A, Stahel, and Uwe, Zangemeister-Wittke

Subjects

Models, Molecular, Time Factors, Virulence Factors, Bacterial Toxins, Genetic Vectors, Exotoxins, Mice, Nude, Antineoplastic Agents, Inhibitory Concentration 50, Mice, Cell Line, Tumor, Animals, Humans, Immunoglobulin Fragments, ADP Ribose Transferases, Dose-Response Relationship, Drug, Immunotoxins, Epithelial Cells, Flow Cytometry, Recombinant Proteins, Protein Structure, Tertiary, Mice, Inbred C57BL, Chromatography, Gel, Female, Cell Adhesion Molecules, Cell Division, Neoplasm Transplantation

Abstract

Epithelial cell adhesion molecule (Ep-CAM) is a tumor-associated antigen overexpressed in many solid tumors but shows limited expression in normal epithelial tissues. To exploit this favorable expression pattern for targeted cancer therapy, an Ep-CAM-specific recombinant immunotoxin was developed and its antitumor activity investigated.The immunotoxin 4D5MOCB-ETA was developed by genetically fusing a truncated form of Pseudomonas aeruginosa exotoxin A (ETA) (ETA(252-608)KDEL) to the highly stable humanized single-chain antibody fragment (scFv) 4D5MOCB. Cytotoxicity of 4D5MOCB-ETA was measured in cell growth and leucine incorporation assays in vitro. Tumor localization and antitumor activity were assessed in athymic mice bearing established human tumor xenografts.Fusion of the toxin moiety to the scFv did neither affect its thermal stability nor its antigen-binding affinity. In vitro, 4D5MOCB-ETA potently and specifically inhibited protein synthesis and reduced the viability of Ep-CAM-positive carcinoma cells of diverse histological origins with IC(50)s ranging from 0.005 to 0.2 pM. Upon systemic administration in mice, 4D5MOCB-ETA showed similar organ distribution as the scFv 4D5MOCB and preferentially localized to Ep-CAM-positive tumor xenografts with a tumor:blood ratio of 5.4. The potent antitumor activity of 4D5MOCB-ETA was demonstrated by its ability to strongly inhibit the growth and induce regression of relatively large tumor xenografts derived from lung, colon, or squamous cell carcinomas.We describe for the first time the development of a fully recombinant Ep-CAM-specific immunotoxin and demonstrate its potent activity against solid tumors of various histological origins. 4D5MOCB-ETA is currently being evaluated in a Phase I study in patients with refractory squamous cell carcinoma of the head and neck.

Published

2003

39. Tumor targeting of mono-, di-, and tetravalent anti-p185(HER-2) miniantibodies multimerized by self-associating peptides

Author

P. August Schubiger, Susanne Kubetzko, Jörg Willuda, Uwe Zangemeister-Wittke, Andreas Plückthun, and Robert Waibel

Subjects

Time Factors, Receptor, ErbB-2, Dimer, Radioimmunoassay, Plasma protein binding, Biochemistry, Antibodies, law.invention, chemistry.chemical_compound, Mice, Antigen, Tetramer, law, Escherichia coli, Tumor Cells, Cultured, Animals, Humans, Avidity, Tissue Distribution, Surface plasmon resonance, Cloning, Molecular, Molecular Biology, Mice, Inbred BALB C, biology, Dose-Response Relationship, Drug, Models, Genetic, Chemistry, Temperature, Technetium, Cell Biology, Molecular biology, Recombinant Proteins, Protein Structure, Tertiary, Kinetics, Periplasm, Recombinant DNA, biology.protein, Chromatography, Gel, Electrophoresis, Polyacrylamide Gel, Female, Antibody, Peptides, Dimerization, Protein Binding

Abstract

Multimerization of antibody fragments increases the valency and the molecular weight, both identified as key features in the design of the optimal targeting molecule. Here, we report the construction of mono-, di-, and tetrameric variants of the anti-tumor p185(HER-2) single chain Fv fragment 4D5 by fusion of self-associating peptides to the carboxyl terminus. Dimeric miniantibodies with a synthetic helix-turn-helix domain and tetrameric ones with the multimerization domain of the human p53 protein were produced in functional form in the periplasm of Escherichia coli. We have directly compared these molecules and the single-chain Fv fragment in the targeting of SK-OV-3 xenografts. Tetramerization of the 4D5 antibody fragment resulted in increased serum persistence, significantly reduced off-rate, due to the avidity effect, both in surface plasmon resonance measurements on purified p185(HER-2) and on SK-OV-3 cells. The (99m)technetium-tricarbonyl-labeled tetrameric 4D5-p53 miniantibody localized with the highest dose at the tumor and remained stably bound for at least 72 h. The highest total dose was 4.3% injected dose/g after 24 h, whereas the highest tumor-to-blood ratio was found to be 13.5:1 after 48 h, with a total dose of 3.2% injected dose/g. The tetramer shows no higher avidity than the dimer, presumably since the simultaneous binding to more than two antigen molecules on the surface of cells is not possible, and the improvement in performance over the dimer must at least be due in part to the molecular weight. These results demonstrate that multimerization by self-associating peptides can be used for the development of more effective targeting molecules for medical diagnostics and therapy.

Published

2001

40. Association of CD24 with the kinase c-fgr in a small cell lung cancer cell line and with the kinase lyn in an erythroleukemia cell line

Author

Jürg A. Zarn, Maria K. Pass, Sandra M. Zimmermann, Robert Waibel, and Rolf A. Stahel

Subjects

Biophysics, Biology, Biochemistry, LYN, Antigens, CD, hemic and lymphatic diseases, Proto-Oncogene Proteins, Tumor Cells, Cultured, Humans, Carcinoma, Small Cell, skin and connective tissue diseases, Molecular Biology, Membrane Glycoproteins, CD24, Kinase, CD24 Antigen, Cell Biology, Molecular biology, Precipitin Tests, Blot, src-Family Kinases, Cell culture, Leukemia, Erythroblastic, Acute, Signal transduction, Tyrosine kinase, K562 cells, Signal Transduction

Abstract

Human CD24 is a highly glycosylated glycosylphosphatidylinositol-linked (GPI-linked) cell surface protein. GPI-linked proteins are involved in signal transduction mediated by members of the protein tyrosine kinase (PTK) family. Therefore we studied associated molecules providing the signaling capacity of CD24. Lysates of SW2 and K562 cells were analysed for expression of PTK of the c-src family by Western blotting. We identified c-fgr in SW2 lysates and c-fgr and also lyn in K562 lysates. To study a putative association of these PTK with CD24 we performed immunoprecipitations with the mAb SWA11 directed against CD24. Western analysis of the precipitates showed an association of c-fgr with CD24 in SW2 cells and lyn in K562 cells. We conclude that either c-fgr or lyn is physically associated with CD24 in a cell-type depending manner. An involvement of these complexes in signaling phenomenons of CD24 in small cell lung cancer and in leukaemias is discussed.

Published

1996

41. Radiation studies on B cell differentiation marker CD24/SCLC Cluster-4 antigen expressing and non-expressing lung cancer cell lines and mouse fibroblasts

Author

P. Huguenin, Mack Mabry, Robert Waibel, H. Resch, Jürg A. Zarn, Rolf A. Stahel, Erich Weber, and Doris Schmitter

Subjects

Cell type, Pathology, medicine.medical_specialty, Cell Survival, Biology, In Vitro Techniques, Transfection, Radiation Tolerance, Mice, Radiation sensitivity, Antigens, CD, Radioresistance, medicine, Tumor Cells, Cultured, Animals, Humans, Radiology, Nuclear Medicine and imaging, Radiosensitivity, Carcinoma, Small Cell, skin and connective tissue diseases, B cell, Membrane Glycoproteins, Radiological and Ultrasound Technology, Oncogene, CD24, CD24 Antigen, Dose-Response Relationship, Radiation, 3T3 Cells, medicine.anatomical_structure, Cell culture, Cancer research

Abstract

A correlation between CD24 expression and higher intrinsic radiation sensitivity has been described in B-lineage acute lymphoblastic leukaemia (B-ALL). We recently identified the SCLC surface antigen Cluster-4 (CL-4) to be identical to the B cell differentiation marker CD24, except for one amino acid residue. The CD24/CL-4 antigen is highly expressed on SCLC, but rarely on NSCLC cells. In order to investigate the influence of the expression of CD24/CL-4 on the radiation sensitivity in a non-leukaemic cell system, sublines of the human SCLC H249 cell line transfected with mutated ras oncogene, and differing in their CD24/CL-4 expression, were studied. In addition, we stably transfected the NSCLC A125 cell line and the mouse fibroblast NIH3T3 cell line with the CL-4 cDNA. The differential expression of CD24/CL-4 on the cells had no influence on morphology, proliferation and cloning efficiency. Radiation studies were done with cells in exponential growth phase. In the highly resistant NSCLC A125 cells no difference in radioresponsiveness was observed between CD24/CL-4 expressing and non-expressing cells. In the rather radiosensitive cells, similar responses to radiation were observed between CD24/CL-4 expressing and non-expressing SCLC H249-ras cells, whereas the CL-4 transfected NIH3T3 mouse fibroblasts showed a substantially higher radioresistance than the CD24/CL-4 non-expressing control cells. In conclusion, the correlation between CD24/CL-4 expression and radiation sensitivity is controversial and depends on the cell type.

Published

1995

42. Antibodies to the protein core of the small cell lung cancer workshop antigen cluster-w4 and to the leucocyte workshop antigen CD24 recognize the same short protein sequence leucine-alanine-proline

Author

and Annette G. Beck-Sickinger, H P Lehmann, E. J. Wawrzynczak, Robert Waibel, Gerd Folkers, Rolf A. Stahel, and Erich Weber

Subjects

Glycosylation, Lung Neoplasms, Antibodies, Neoplasm, Immunology, Molecular Sequence Data, Peptide, Peptide binding, Biology, Epitope, chemistry.chemical_compound, Epitopes, Antigen, Antigens, CD, Antigens, Neoplasm, Immunology and Allergy, Humans, Amino Acid Sequence, Carcinoma, Small Cell, skin and connective tissue diseases, Peptide sequence, chemistry.chemical_classification, Membrane Glycoproteins, Antibodies, Monoclonal, CD24 Antigen, Molecular biology, Antigens, Differentiation, Peptide Fragments, Epitope mapping, chemistry, biology.protein, Antibody, Research Article

Abstract

SUMMARY We recently described the identity of the small cell lung cancer (SCLC) cluster-w4 antigen and the human B cell differentiation marker CD24, a glycosylphosphatidylinositol (GPI)-anchored, highly glycosylated surface molecule of only 31–35 amino acids [15]. The specificities of three anti-cluster-w4 and of eleven anti-CD24 MoAbs have been investigated with respect to their binding capacity to the protein core of cluster-w4/CD24 antigen. Four overlapping peptides spanning this protein core were synthesized. MoAbs shown to bind to two overlapping peptides by antibody binding inhibition using the clustcr-w4/CD24-positive SCLC cell line SW2 and by direct peptide binding detected in an ELISA were investigated in more detail. To determine the exact epitopes recognized by these MoAbs, an epitope mapping assay using peptides synthesized onto polyethylene pins was established. The three anti-cluster-w4 MoAbs SWA11, SWA21 and SWA22 and the anli-CD24 MoAbs OKB2 and ALB9 recognized the same short leucine-alanine-proline (LAP) sequence in an area without potential glycosylation sites close to the GPI anchor of the protein core of the cluster-w4/CD24 antigen.

Published

1993

43. An autocrine mitogenic activity produced by a pleural human mesothelioma cell line

Author

Robert Waibel, Béatrice Lauber, Rolf A. Stahel, Josefina Cano‐Santos, Margrit Leuthold, and Doris Schmitter

Subjects

Adult, DNA Replication, Male, Mesothelioma, Cancer Research, medicine.medical_specialty, Cell division, Transplantation, Heterologous, Mice, Nude, Biology, Adenocarcinoma, Cell Line, Mice, Internal medicine, medicine, Tumor Cells, Cultured, Animals, Humans, Autocrine signalling, Lung, DNA synthesis, Cell biology, Chromosome Banding, Culture Media, Transplantation, Pleural Effusion, Chemically defined medium, Endocrinology, Oncology, Cell culture, Karyotyping, biology.protein, Carcinoma, Squamous Cell, Mitogens, Mesothelial Cell, Platelet-derived growth factor receptor, Cell Division, Neoplasm Transplantation

Abstract

The pleural human mesothelioma cell line ZL5 established in our laboratory exhibits an unusual phenotype with adherent and floating cells. ZL5 cells grow in a chemically defined medium (ACL3*) and can be maintained over 3 weeks in protein-free basal medium alone (RPMI). Basal medium conditioned by ZL5 cells possesses a mitogenic activity with an autocrine effect, as measured by cell counting and by a 3H-thymidine incorporation assay. Moreover, the conditioned medium affects the DNA synthesis of a variety of other lung-derived cells. The active principle of medium conditioned by ZL5 cells is not identical to the defined growth-factors EGF, PDGF, and TGF-beta, known to stimulate the growth of normal human mesothelial cells: treatment with these factors does not mimic the effect of conditioned medium on ZL5 cells. Our observations suggest that the mesothelioma cell line ZL5 produces an unknown autocrine mitogen.

Published

1992

44. Tumor-antigen-specific humoral immune response of animals to anti-idiotypic antibodies and comparative serological analysis of patients with small-cell lung carcinoma

Author

Rolf A. Stahel, Hans-Peter Lehmann, Caroline Zwicky, and Robert Waibel

Subjects

Cancer Research, Lung Neoplasms, Antibodies, Neoplasm, Sialoglycoproteins, Active immunotherapy, Biology, Binding, Competitive, Serology, Mice, Immune system, Antigen, Immunity, Antibody Specificity, Antigens, Neoplasm, Biomarkers, Tumor, Animals, Humans, Carcinoma, Small Cell, Antibodies, Monoclonal, Tumor antigen, respiratory tract diseases, Antibodies, Anti-Idiotypic, Oncology, Monoclonal, Immunology, biology.protein, Rabbits, Antibody

Abstract

We have previously developed 3 monoclonal anti-idiotypic antibodies (Ab2) of LOU rat origin directed against the binding site of the murine monoclonal IgM LAM8, which recognizes the small-cell lung carcinoma (SCLC)-associated sialoglycoprotein antigen sGP 90-135. The aim of this study was to compare the efficiencies of these 3 Ab2, designated LY8-229, LX8-531 and LX8-632, to induce antigen-specific immunity in different animal species without prior exposure of the recipients to the nominal antigen, and thereby possibly select an Ab2 candidate for active immunotherapy against SCLC in patients. The feasibility of this approach was further evaluated by a serological analysis of patients with SCLC compared with healthy individuals, in whom the spontaneous antibody reactivities against SCLC cell lines and Ab2 were tested. LY8-229 was shown to be the most effective Ab2 in inducing antigen-specific antibodies in BALB/c mice, CBA/J/Zur mice and one NZW rabbit. Furthermore, LY8-229 was the only Ab2 against which significantly elevated idiotype-specific antibody reactivities existed in sera of patients with SCLC. These reactivities correlated positively with binding to antigen-positive tumor cells. Our findings suggest that LY8-229 represents in its reactivity pattern the nominal SCLC antigen in humans also, and therefore may be of diagnostic and possibly therapeutic relevance for patients with SCLC.

Published

1992

45. Cytotoxicity and therapeutic potential of immunotoxins recognizing different antigens of small cell lung cancer

Author

Rolf A. Stahel, E. J. Wawrzynczak, Robert Waibel, A. R. Collinson, Uwe Zangemeister-Wittke, and H.P. Lehman

Subjects

Pulmonary and Respiratory Medicine, Cancer Research, Oncology, Antigen, Immunotoxin, business.industry, Immunology, Medicine, Non small cell, Cytotoxicity, business

Published

1991

46. Immunolocalisation and imaging of small cell cancer xenografts by the IgG2a monoclonal antibody SWA11

Author

A T Zimmerman, Robert Waibel, A Martin, A Smith, Rolf A. Stahel, and G Westera

Subjects

Cancer Research, Pathology, medicine.medical_specialty, Lung Neoplasms, medicine.drug_class, medicine.medical_treatment, Transplantation, Heterologous, Cell, Mice, Inbred Strains, Monoclonal antibody, Immunoglobulin G, Cell Line, Iodine Radioisotopes, Mice, Antigen, medicine, Animals, Carcinoma, Small Cell, Radionuclide Imaging, biology, Antibodies, Monoclonal, Molecular biology, medicine.anatomical_structure, Oncology, Cell culture, Radioimmunotherapy, Monoclonal, biology.protein, Female, Antibody, Neoplasm Transplantation, Research Article

Abstract

We describe here a murine monoclonal antibody of the IgG2a isotype which was generated against the SW2 human small cell carcinoma cell line. The antibody, SWA11, was shown to bind to a partially defined antigen preferentially expressed on cell lines of small cell carcinoma origin. In vitro binding studies revealed 6.1 x 10(5) antigenic sites on the SW2 cell line and the Ka to be 1.2 x 10(9)M-1. Following injection into mice bearing 1-2 cm3 SW2 xenografts, SWA11 showed strong selective accumulation in the small cell heterotransplants with a tumour to blood ratio of 7.5:1 at day 4. Other tumour to organ ratios were similarly high at 19:1, 22:1 and 12:1 for liver, kidney and spleen respectively. The absolute amount of SWA11 which localised was 10.5% of total injected material per gram tumour at day 2 and this level did not markedly decrease by day 4. The high ability of SWA11 to localise to SCC xenografts was confirmed by external gamma scintigraphy. The potential application of SWA11 as a model system for in vivo radioimmunotherapy is discussed. Images Figure 4

Published

1989

47. Cytochemical detection of hyaluronidase activity in single human and mouse sperm by an improved substrate-film technique

Author

Leonard C. Ginsberg, Robert Waibel, and Gyula Ficsor

Subjects

Male, Infertility, chemistry.chemical_classification, Time Factors, Histology, Ratón, Hyaluronidase activity, Hyaluronoglucosaminidase, Substrate (chemistry), Semen, Biology, medicine.disease, Spermatozoa, Molecular biology, Sperm, Mice, Enzyme, chemistry, Hyaluronidase, Methods, medicine, Animals, Humans, Anatomy, medicine.drug

Abstract

A substrate-film method is described that allows the detection of hyaluronidase activity in nearly 100% of single human and mouse sperm. The level of hyaluronidase activity as determined by halo diameters was greater in mouse than in human sperm. This simple method may have use as a screening method for identifying compounds that cause developmental or genetic defects in male germ cells, or for the diagnosis of infertility due to decreased hyaluronidase activity.

Published

1984

48. Effect of galactose content on the solution and interaction properties of guar and carob galactomannans

Author

Renato Amadò, Barry V. McCleary, Hans Neukom, and Robert Waibel

Subjects

chemistry.chemical_classification, Chromatography, Organic Chemistry, Guar, General Medicine, bacterial infections and mycoses, Biochemistry, Analytical Chemistry, carbohydrates (lipids), Sepharose, chemistry.chemical_compound, Viscosity, Galactomannan, Enzyme, chemistry, Affinity chromatography, Galactose, skin and connective tissue diseases, Mannan

Abstract

Guar galactomannan has been modified by treatment with an α- d -galactosidase A preparation from lucerne seeds. This enzyme was purified by affinity chromatography on N -ϵ-aminocaproyl-α- d -galactopyranosylamine linked to Sepharose 4B, had a high activity towards galactomannans, and was completely devoid of β- d -mannanase. On incubation for 2 h, this enzyme removed ⪢ 75% of the galactose from guar galactomannan with no concurrent decrease in viscosity. Eventual decrease in viscosity was associated with the formation of insoluble, mannan-type precipitates. This phenomenon, although directly related to the galactose content of the galactomannan, was also time-dependent. The limiting viscosity numbers calculated for the “mannan backbones” of α- D -galactosidase-treated, guar galactomannan having galactose-mannose ratios of 38:62 to 15:85 were the same. Modified, guar galactomannan (at 0.4% w/v) having a galactose-mannose ratio of 20:80, or less, forms a gel on storage at 4° over several weeks. Also, gel particles form when solutions of these galactomannans are passed through a freeze-thaw cycle. Samples containing ⪡ 10% of galactose rapidly precipitate from solution even at 30°. The interaction of guar galactomannan with xanthan is greatly increased by removal of galactose residues. Samples having galactose-mannose ratios of ~19:81 interact with xanthan to essentially the same degree as carob galactomannan (Gal/Man = 23:77).

Published

1981

49. Mouse Sperm Antigens that Participate in Fertilization. III. Passive Immunization with a Single Monoclonal Antisperm Antibody Inhibits Pregnancy and Fertilization in Vivo1

Author

Patricia M. Saling and Robert Waibel

Subjects

endocrine system, biology, medicine.drug_class, Cell Biology, General Medicine, Monoclonal antibody, Oocyte, Sperm, Molecular biology, Human chorionic gonadotropin, Andrology, medicine.anatomical_structure, Human fertilization, Reproductive Medicine, Antigen, In vivo, biology.protein, medicine, Antibody

Abstract

Passive immunization was used to study the effect of antimouse sperm monoclonal antibodies on fertilization in vivo. The effects of two antibodies were compared in this investigation. One of them, M29, has been shown previously to localize to the equatorial segment of the sperm head and to inhibit mouse fertilization in vitro in a concentration-dependent manner. The second antibody, M2, binds to the same area of the sperm head, and also belongs to the M immunoglobulin class (IgM), but does not affect fertilization in vitro. Superovulated female mice received two antibody injections intraperitoneally (at the times of the pregnant mare's serum gonadotropin and human chorionic gonadotropin injections) at concentrations of 0.5-4.0 mg of IgM or control IgG; animals were mated within 6-12 h of the hCG injection. Fertilization and concomitant establishment of pregnancy were reduced significantly, in a dose-dependent manner, only in those animals immunized with M29 IgM (e.g., 4 mg M29 IgM: 12.6% of 304 eggs fertilized; 4 mg M2 IgM: 96% of 192 eggs fertilized). Intraperitoneal administration of the antibodies did not depress superovulation levels nor oocyte viability. 125I-labeled M29 IgM was used to determine the amount of antibody present in the oviductal ampulla at the time of fertilization in passively immunized mice. Luminal M29 IgM was found to be a linear function of the intraperitoneal dose: 0.002-0.003% of the injected dose was present in the oviductal lumen 14-16 h post-hCG.(ABSTRACT TRUNCATED AT 250 WORDS)

Published

1985

50. Chapter 30 Characterisation of small cell carcinoma surface membrane antigens by indirect immunofluorescence. Solid phase radioimmunoassay and immunoblotting

Author

Carl O'Hara, Rolf A. Stahel, and Robert Waibel

Subjects

Pulmonary and Respiratory Medicine, Cancer Research, Indirect immunofluorescence, Radioimmunoassay, Biology, medicine.disease, Molecular biology, Small-cell carcinoma, Surface membrane, Oncology, Antigen, Cell culture, medicine, biology.protein, Small Cell Lung Carcinoma, Antibody

Abstract

Five antibodies to surface membrane antigens of small cell lung carcinoma (SCLC), were selected by indirect immunofluorescence (IF). Their characteristics were compared to antibody LAM8. Antibody reactivity on a panel of lung tumour cell lines was determined by IF and by indirect solid phase radioimmunoassays (RIA). Biochemical characterisation of the antigens was done by RIA and immunoblotting. By IF antibodies SWA4, SWA20, SWA23, and LAM8 reacted selectively with 4/8 SCLC cell lines. By RIA this selectivity was lost for antibodies SWA4 and SWA23. Antibodies SWA21 and SWA22 reacted with all SCLC, weakly with one non-SCLC cell line and also stained leukocytes. RIA and immunoblotting experiments suggested antigens recognised by antibodies SWA4, SWA23 are identical to sGP90-135 identified by antibody LAM8 and suggest similarities of the antigens recognised by antibodies SWA21 and SWA22. In contrast, antibody SWA20 appeared to recognise a different membrane antigen. These results demonstrate that antibodies which recognise the same membrane antigen can differ considerably in their pattern of reactivity with cell lines depending on the method employed, and that the same pattern of cell line reactivity, even when examined over a large number of cell lines by different methods, does not necessarily establish the similarities of antigens.

Published

1988