Your search keyword '"Leitao, Charles Dahlsson"' showing total 5 results

1. Bacterial Cell Display for Selection of Affibody Molecules

Author

Leitao, Charles Dahlsson, Ståhl, Stefan, Löfblom, John, Leitao, Charles Dahlsson, Ståhl, Stefan, and Löfblom, John

Abstract

This review describes the principles for generation of affibody molecules using bacterial display on the Gram-negative Escherichia coli and the Gram-positive Staphylococcus carnosus, respectively. Affibody molecules are small and robust alternative scaffold proteins that have been explored for therapeutic, diagnostic, and biotechnological applications. They typically exhibit high-stability, affinity, and specificity with high modularity of functional domains. Due to the small size of the scaffold, affibody molecules are rapidly excreted through renal filtration and can efficiently extravasate from blood and penetrate tissues. Preclinical and clinical studies have demonstrated that affibody molecules are promising and safe complements to antibodies for in vivo diagnostic imaging and therapy. Sorting of affibody libraries displayed on bacteria using fluorescence-activated cell sorting is an effective and straightforward methodology and has been used successfully to generate novel affibody molecules with high affinity for a diverse range of molecular targets., Part of book ISBN 978-1-0716-3278-9 978-1-0716-3279-6 978-1-0716-3281-9QC 20230816

Published

2023

2. Comparison Of Affibody- And Antibody Fragments-based Caix Imaging Probes In Mice Bearing Renal Cell Carcinoma Xenografts

Author

Garousi, J., Huizing, F., Vorobyeva, A., Mitran, B., Andersson, Ken G., Leitao, Charles Dahlsson, Frejd, F., Löfblom, John, Bussink, J., Orlova, A., Heskamp, S., Tolmachev, V., Garousi, J., Huizing, F., Vorobyeva, A., Mitran, B., Andersson, Ken G., Leitao, Charles Dahlsson, Frejd, F., Löfblom, John, Bussink, J., Orlova, A., Heskamp, S., and Tolmachev, V.

Abstract

QC 20191202

Published

2019

3. Improved contrast of affibody-mediated imaging of HER3 expression in mouse xenograft model through co-injection of a trivalent affibody for in vivo blocking of hepatic uptake

Author

Rosestedt, Maria, Andersson, Ken G., Rinne, Sara S., Leitao, Charles Dahlsson, Mitran, Bogdan, Vorobyeva, Anzhelika, Ståhl, Stefan, Löfblom, John, Tolmachev, Vladimir, Orlova, Anna, Rosestedt, Maria, Andersson, Ken G., Rinne, Sara S., Leitao, Charles Dahlsson, Mitran, Bogdan, Vorobyeva, Anzhelika, Ståhl, Stefan, Löfblom, John, Tolmachev, Vladimir, and Orlova, Anna

Abstract

Human epidermal growth factor receptor type 3 (HER3) plays a crucial role in the progression of many cancer types. In vivo radionuclide imaging could be a reliable method for repetitive detection of HER3-expression in tumors. The main challenge of HER3-imaging is the low expression in tumors together with endogenous receptor expression in normal tissues, particularly the liver. A HER3-targeting affibody molecule labeled with radiocobalt via a NOTA chelator [Co-57]Co-NOTA-Z(08699) has demonstrated the most favorable biodistribution profile with the lowest unspecific hepatic uptake and high activity uptake in tumors. We hypothesized that specific uptake of labeled affibody monomer might be selectively blocked in the liver but not in tumors by a co-injection of non-labeled corresponding trivalent affibody (Z(08699))(3). Biodistribution of [Co-57]Co-NOTA-Z(08699) and [In-111]ln-DOTA-(Z(08699))(3) was studied in BxPC-3 xenografted mice. [Co-57]Co-NOTA-Z(08699) was co-injected with unlabeled trivalent affibody DOTA-(Z(08699))(3) at different monomer:trimer molar ratios. HER3-expression in xenografts was imaged using [Co-57]Co-NOTA-Z(08699) and [Co-57]Co-NOTA-Z(08699): DOTA-(Z(08699))(3). Hepatic activity uptake of [Co-57] Co-NOTA-Z(08699): DOTA-(Z(08699))(3) decreased with increasing monomer:trimer molar ratio. The tumor activity uptake and tumor-to-liver ratios were the highest for the 1:3 ratio. SPECT/CT images confirmed the biodistribution data. Imaging of HER3 expression can be improved by co-injection of a radiolabeled monomeric affi body-based imaging probe together with a trivalent affibody., QC 20200325

Published

2019

4. Optimization of molecular design of Ga-68-labeled affibody molecule for PET imaging of HER3 expression

Author

Rinne, S., Mitran, B., Vorobyeva, A., Leitao, Charles Dahlsson, Andersson, Ken G., Löfblom, John, Tolmachev, V., Orlova, A., Rinne, S., Mitran, B., Vorobyeva, A., Leitao, Charles Dahlsson, Andersson, Ken G., Löfblom, John, Tolmachev, V., and Orlova, A.

Abstract

QC 20221006

Published

2018

5. Optimization of HER3 expression imaging using affibody molecules: Influence of chelator for labeling with indium-111.

Author

Rinne, Sara S., Leitao, Charles Dahlsson, Mitran, Bogdan, Bass, Tarek Z., Andersson, Ken G., Tolmachev, Vladimir, Ståhl, Stefan, Löfblom, John, and Orlova, Anna

Abstract

Radionuclide molecular imaging of human epidermal growth factor receptor 3 (HER3) expression using affibody molecules could be used for patient stratification for HER3-targeted cancer therapeutics. We hypothesized that the properties of HER3-targeting affibody molecules might be improved through modification of the radiometal-chelator complex. Macrocyclic chelators NOTA (1,4,7-triazacyclononane-N,N′,N′′-triacetic acid), NODAGA (1-(1,3-carboxypropyl)-4,7-carboxymethyl-1,4,7-triazacyclononane), DOTA (1,4,7,10-tetraazacyclododecane-1,4,7,10-tetraacetic acid), and DOTAGA (1,4,7,10-tetraazacyclododececane,1-(glutaric acid)−4,7,10-triacetic acid) were conjugated to the C-terminus of anti-HER3 affibody molecule Z08698 and conjugates were labeled with indium-111. All conjugates bound specifically and with picomolar affinity to HER3 in vitro. In mice bearing HER3-expressing xenografts, no significant difference in tumor uptake between the conjugates was observed. Presence of the negatively charged 111In-DOTAGA-complex resulted in the lowest hepatic uptake and the highest tumor-to-liver ratio. In conclusion, the choice of chelator influences the biodistribution of indium-111 labeled anti-HER3 affibody molecules. Hepatic uptake of anti-HER3 affibody molecules could be reduced by the increase of negative charge of the radiometal-chelator complex on the C-terminus without significantly influencing the tumor uptake. [ABSTRACT FROM AUTHOR]

Published

2019