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Improvement of potential therapeutic value of tumor necrosis-α (TNF-α) by charge modulation in the tip region
1 National Institute of Chemistry, Hajdrihova 19, SI-1000, Ljubljana, Slovenia
2 Lek Pharmaceuticals d.d., Verovškova 57, Ljubljana, Slovenia
3 National Institute for Biological Standards and Control (NIBSC), United Kingdom
* Corresponding Author: Viktor Menart,
European Cytokine Network 2005, 16(1), 17-26.
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Analysis of published data reveals that the introduction of more basic amino acid residues in the flexible N-terminal region of the human tumour necrosis factor alpha (TNF) molecule indicates a weak but consistent trend towards increased in vitro cytotoxicity, especially when the effect of N-terminal length is taken into account. In our laboratory, a series of TNF analogues with a charge modification in the tip region of the molecule was prepared, and cytotoxicity measured. Similar trends in cytotoxicity with increasing basicity of the TNF analogue were found in this study for two mouse cell lines, L929 and WEHI-164 clone 13-1, as well as for the human line KYM-1D4. For the series of analogues as a whole, a general increase in in vitro cytotoxicity with increasing pI values was not apparent, but some analogues with charge reversal in the tip region, for example, the LK-805 analogue (E107K), exhibited significantly increased cytotoxicity in comparison to native TNF in a range of cell lines, including L929, KYM-1D4-K, WEHI-164 clone 13-1, HEPA 1-6 and EAhy926 cell lines. Experiments with heparinase-pre-treated cells demonstrated that the increased in vitro cytotoxicity of LK-805 is most probably due to interactions with cell surface heparan sulphates that effectively concentrate it before binding to TNF receptors occurs. Examination of structural models of TNF bound to soluble TNF receptor 1 (TNFR1) indicates that simple mutations in the tip region most probably cannot interact with receptor binding sites, and therefore do not directly modulate cytotoxicity.Keywords
TNF, basic analogues, isoelectric point, heparan sulphate, L929, KYM-1D4
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APA Style
Fonda, I., Pernuš, M., Gaberc-Porekar, V., Kenig, M., Štalc, A. et al. (2005). Improvement of potential therapeutic value of tumor necrosis-α (TNF-α) by charge modulation in the tip region. European Cytokine Network, 16(1), 17–26.
Vancouver Style
Fonda I, Pernuš M, Gaberc-Porekar V, Kenig M, Štalc A, Meager A, et al. Improvement of potential therapeutic value of tumor necrosis-α (TNF-α) by charge modulation in the tip region. Eur Cytokine Network. 2005;16(1):17–26.
IEEE Style
I. Fonda et al., “Improvement of potential therapeutic value of tumor necrosis-α (TNF-α) by charge modulation in the tip region,” Eur. Cytokine Network, vol. 16, no. 1, pp. 17–26, 2005.
Copyright © 2005 The Author(s). Published by Tech Science Press.This work is licensed under a Creative Commons Attribution 4.0 International License , which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
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