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Publication Date:
June 2010
ISSN:
1437-4315
DOI:
10.1515/bc.2010.109

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Biological Chemistry

Editor-in-Chief: Brüne, Bernhard

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Nuclear cysteine cathepsin variants in thyroid carcinoma cells

Sofia Tedelind1 / Kseniia Poliakova1 / Amanda Valeta1 / Ruth Hunegnaw1 / Eyoel Lemma Yemanaberhan1 / Nils-Erik Heldin2 / Junichi Kurebayashi3 / Ekkehard Weber4 / Nataša Kopitar-Jerala5 / Boris Turk5 / Matthew Bogyo6 / Klaudia Brix1

1School of Engineering and Science, Research Center of Molecular Life Science, Jacobs University Bremen, Campus Ring 1, D-28759 Bremen, Germany

2Department of Genetics and Pathology, Uppsala University, S-75185 Uppsala, Sweden

3Department of Breast and Thyroid Surgery, Kawasaki Medical School, 701-0192 Okayama, Japan

4Institute of Physiological Chemistry, Martin Luther University, D-06097 Halle-Wittenberg, Germany

5Department of Biochemistry, Molecular and Structural Biology, Jožef Stefan Institute, SI-1000 Ljubljana, Slovenia

6Departments of Pathology and Microbiology and Immunology, Stanford University School of Medicine, 300 Pasteur Dr., Stanford, CA 94305-5324, USA

Corresponding author

Citation Information: Biological Chemistry. Volume 391, Issue 8, Pages 923–935, ISSN (Online) 1437-4315, ISSN (Print) 1431-6730, DOI: 10.1515/bc.2010.109, June 2010

Publication History:
Received:
2010-02-08
Accepted:
2010-05-20
Published Online:
2010-06-11

Abstract

The cysteine peptidase cathepsin B is important in thyroid physiology by being involved in thyroid prohormone processing initiated in the follicular lumen and completed in endo-lysosomal compartments. However, cathepsin B has also been localized to the extrafollicular space and is therefore suggested to promote invasiveness and metastasis in thyroid carcinomas through, e.g., ECM degradation. In this study, immunofluorescence and biochemical data from subcellular fractionation revealed that cathepsin B, in its single- and two-chain forms, is localized to endo-lysosomes in the papillary thyroid carcinoma cell line KTC-1 and in the anaplastic thyroid carcinoma cell lines HTh7 and HTh74. This distribution is not affected by thyroid stimulating hormone (TSH) incubation of HTh74, the only cell line that expresses a functional TSH-receptor. Immunofluorescence data disclosed an additional nuclear localization of cathepsin B immunoreactivity. This was supported by biochemical data showing a proteolytically active variant slightly smaller than the cathepsin B proform in nuclear fractions. We also demonstrate that immunoreactions specific for cathepsin V, but not cathepsin L, are localized to the nucleus in HTh74 in peri-nucleolar patterns. As deduced from co-localization studies and in vitro degradation assays, we suggest that nuclear variants of cathepsins are involved in the development of thyroid malignancies through modification of DNA-associated proteins.

Keywords: cysteine peptidases; HTh7; HTh74; KTC-1; nuclear proteases

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