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Dive into the research topics where Börje Karlsson is active.

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Featured researches published by Börje Karlsson.


Nuclear Medicine and Biology | 2001

High-efficiency astatination of antibodies using N-iodosuccinimide as the oxidising agent in labelling of N-succinimidyl 3-(trimethylstannyl)benzoate

Sture Lindegren; Håkan Andersson; Bäck T; Lars Jacobsson; Börje Karlsson; Gunnar Skarnemark

Monoclonal antibodies C215, reactive with colorectal carcinomas, and MOv18, reactive with most of the ovarian carcinomas, were radiohalogenated with [211At]astatine. The radiohalogen was conjugate coupled to antibodies via the intermediate labelling reagent N-succinimidyl-3-(trimethylstannyl)benzoate (m-MeATE) in a two-step, single-pot reaction. Optimisation of the labelling of the reagent was achieved using N-iodosuccinimide, NIS, as the oxidising agent. The yields ranged from 69-95% in the labelling of 0.1-1.0 nmole of the m-MeATE precursor. Subsequent conjugation to antibodies resulted in yields of 58+/-7%. In vitro binding to tumour cells showed that the immunoreactivity of both antibodies was retained after astatine labelling.


Nuclear Medicine and Biology | 1998

Chloramine-T in high-specific-activity radioiodination of antibodies using N-succinimidyl-3-(trimethylstannyl)benzoate as an intermediate.

Sture Lindegren; Gunnar Skarnemark; Lars Jacobsson; Börje Karlsson

Monoclonal antibodies C215 and MOv18 have been radiohalogenated, using a single-batch method employing N-succinimidyl-3-(trimethylstannyl)benzoate, m-MeATE. Labelling to the stannyl ester was optimized using chloramine-T as oxidizing agent. The results show that the stannyl ester is effectively labelled with short reaction times giving reproducible yields from 85% to 95%. Subsequent antibody conjugation, 10 to 80 microg MAb, resulted in biologically active, labelled antibodies with overall radiochemical yields of 50% to 80%, with corresponding specific activities of 490-50 kBq(125I)/microg.


Nuclear Medicine and Biology | 1993

Therapy with 125I-labelled internalized and non-internalized monoclonal antibodies in nude mice with human colon carcinoma xenografts

Eva Forssell Aronsson; Jakobína Grétarsdóttir; Lars Jacobsson; Tom Bäck; Sven Hertzman; Sture Lindegren; Börje Karlsson; Leif Lindholm; Stig Holmberg; Larsolof Hafström; Sören Mattsson

The therapeutic effects of 125I-labelled (18-97 MBq) monoclonal antibodies (MAb) C-242, C-215 and S-S.1 were studied in nude mice with human colorectal adenocarcinoma tumours. The antibodies were administered 2 or 10-16 days after implantation of the tumour cells. The monoclonal antibody C-242 was internalized into the tumour cells, C-215 was internalized to a lower degree while S-S.1 (unspecific MAb) was not internalized at all. No enhanced therapeutic effect of 125I-C-242 was observed, as a result of Auger electrons, compared with 125I-C-215 and 125I-S-S.1.


Acta Oncologica | 1991

Comparison of Seven Iodine-Labelled Monoclonal Antibodies in Nude Mice with Human Colon Carcinoma Xenografts

E. Forssell Aronsson; Jakobína Grétarsdóttir; Lars Jacobsson; Sören Mattsson; Stig Holmberg; L.-O. Hafström; Börje Karlsson; Leif Lindholm

The biokinetics of seven 131I-labelled monoclonal antibodies (MAbs), directed against human colon carcinoma and one 125I-labelled unspecific MAb have been examined. The study in nude mice, carrying human colon carcinoma, was intended to be a step in the selection of the most suitable antibody for clinical scintigraphy. The biological half-life in blood was found to be between 1.3 and 7.4 days for the different MAbs. Chromatography of plasma samples showed that the radioiodine was mainly bound to IgG-sized molecules. The (normal tissue)/blood ratios were similar for all the MAbs. The tumour/blood ratio was 0.41 for the unspecific MAb and 0.49-1.1 for the specific MAbs, and the tumour/muscle ratio was between 3.2 and 6.8 for the specific MAbs 6 days after injection. For one MAb tumour/blood and tumour/muscle ratios were 3.9 and 9.8 respectively 9 days after injection. Localization indices were at their highest 2.6 6 days after injection. For at least two of the monoclonal antibodies the tumour/blood and tumour/muscle ratios found are high enough to justify clinical trials regarding their usefulness for scintigraphy of colon cancer in man.


International Journal of Radiation Applications and Instrumentation. Part B. Nuclear Medicine and Biology | 1992

Comparison of the biodistribution of 75Se- and 131I-labelled monoclonal antibodies in nude mice

Jakobína Grétarsdóttir; Eva Forssell Aronsson; Lars Jacobsson; Ólöf Hafsteinsdóttir; Stig Holmberg; Larsolof Hafström; Sture Lindegren; Börje Karlsson; Leif Lindholm; Sören Mattsson

A monoclonal antibody, C-215, against colon cancer, was internally labelled with [75Se]methionine. The biodistribution was studied in tumour-bearing nude mice and compared with the biodistribution of [131I]C-215. The tissue uptake was divided into three parts: antibody bound to the antigen, antibody in the extracellular space and uptake of the released radionuclide. [75Se]C-215 showed a greater amount of antigen-bound antibody in the tumour, but also a greater unspecific uptake both in tumour and normal tissue.


Nuclear Medicine and Biology | 1994

125I-labelling of an internally 75Se-labelled monoclonal antibody—Biodistribution in tumour-bearing nude mice

Jakobína Grétarsdóttir; Eva Forssell Aronsson; Lars Jacobsson; Ólöf Hafsteinsdóttir; Stig Holmberg; Larsolof Hafström; Sture Lindegren; Börje Karlsson; Leif Lindholm; Sören Mattsson

A monoclonal antibody, C215, was first internally labelled with 75Se-methionine and then labelled with 125I. The biodistribution of the dual-labelled [125I][75Se]C215 was studied in tumour-bearing nude mice killed 3 days after injection. The biodistribution of the dual-labelled [125I][75Se]C215 was compared with the biodistribution of single-labelled [131I]C215 and [75Se]C215. Iodine-labelled antibodies seem to be damaged during iodination, affecting the disappearance rate and tumour uptake. There were no signs of dehalogenation of circulating antibodies or antibodies taken up in the tumour.


The Journal of Nuclear Medicine | 2005

Therapeutic Efficacy and Tumor Dose Estimations in Radioimmunotherapy of Intraperitoneally Growing OVCAR-3 Cells in Nude Mice with 211At-Labeled Monoclonal Antibody MX35

Jörgen Elgqvist; Håkan Andersson; Tom Bäck; Ragnar Hultborn; Holger Jensen; Börje Karlsson; Sture Lindegren; Stig Palm; Elisabet Warnhammar; Lars Jacobsson


Clinical Cancer Research | 2003

Astatine-211-labeled antibodies for treatment of disseminated ovarian cancer: an overview of results in an ovarian tumor model.

Håkan Andersson; Jörgen Elgqvist; György Horvath; Ragnar Hultborn; Lars Jacobsson; Holger Jensen; Börje Karlsson; Sture Lindegren; Stig Palm


The Journal of Nuclear Medicine | 2005

Myelotoxicity and RBE of 211At-Conjugated Monoclonal Antibodies Compared with 99mTc-Conjugated Monoclonal Antibodies and 60Co Irradiation in Nude Mice

Jörgen Elgqvist; Peter Bernhardt; Ragnar Hultborn; Holger Jensen; Börje Karlsson; Sture Lindegren; Elisabet Warnhammar; Lars Jacobsson


Bioconjugate Chemistry | 2002

Synthesis and biodistribution of 211At-labeled, biotinylated, and charge-modified poly-L-lysine: evaluation for use as an effector molecule in pretargeted intraperitoneal tumor therapy.

Sture Lindegren; Håkan Andersson; Lars Jacobsson; Tom Bäck; Gunnar Skarnemark; Börje Karlsson

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Lars Jacobsson

University of Gothenburg

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Sture Lindegren

Sahlgrenska University Hospital

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Håkan Andersson

Sahlgrenska University Hospital

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Gunnar Skarnemark

Chalmers University of Technology

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Stig Holmberg

Sahlgrenska University Hospital

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Holger Jensen

Copenhagen University Hospital

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