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In-vivo antitumour effect of daunorubicin–GnRH-III derivative conjugates on colon carcinoma-bearing mice

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2012

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Tóvári, József
Tejeda, Miguel
Schulcz, Ákos
Kapuvári, Bence
Vincze, Borbála
Mező, Gábor

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http://nbn-resolving.de/urn:nbn:de:bsz:352-172342
DOI (zitierfähiger Link)
https://doi.org/10.1097/CAD.0b013e32834bb6b4
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Chemie: Publikationen
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Published

Erschienen in

Anti-Cancer Drugs. 2012, 23(1), pp. 90-97. ISSN 0959-4973. eISSN 1473-5741. Available under: doi: 10.1097/CAD.0b013e32834bb6b4

Zusammenfassung

Targeted cancer chemotherapy is a novel approach developed for the specific delivery of anticancer drugs. Tumour targeting can be achieved by combining a chemotherapeutic agent with a targeting moiety that recognizes tumour-specific or highly expressed receptors on cancer cells. We used the gonadotropin-releasing hormone-III (GnRH-III) as a targeting moiety to which the chemotherapeutic agent daunorubicin (Dau) was attached through an oxime bond either directly or by inserting a GFLG tetrapeptide spacer. The in-vivo toxicity of Dau-GnRH-III derivative conjugates was evaluated on healthy BDF-1 female mice, and their tumour growth inhibitory effect was determined on C26 murine and HT-29 human colon carcinoma-bearing mice. Both oxime bond-containing conjugates were well tolerated and exerted significant antitumour activity on C26 colon carcinoma-bearing mice at a dose of 30 mg Dau content in conjugate/kg body weight. Furthermore, the conjugates inhibited the tumour growth more than the free drug at a dose that was still not toxic. Similar tumour growth inhibitory effects were obtained on HT-29 human colon carcinoma-bearing mice using three treatments with 15 mg Dau content in conjugate/kg. The tumour growth inhibitions according to the tumour volume and the tumour weight were 44/41% and 58/50%, respectively. Considering the results, both of the investigated Dau-GnRH-III derivative conjugates were well tolerated and had significant antitumour effect on colon carcinoma-bearing mice.

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Fachgebiet (DDC)
540 Chemie

Schlagwörter

Colon cancer, Daunorubicin-GnRH-III derivative conjugates, Gonadotropin-releasing hormone-III, In-vivo antitumour activity, In-vivo toxicity, Oxime bond, Targeted cancer chemotherapy

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ISO 690MANEA, Marilena, József TÓVÁRI, Miguel TEJEDA, Ákos SCHULCZ, Bence KAPUVÁRI, Borbála VINCZE, Gábor MEZŐ, 2012. In-vivo antitumour effect of daunorubicin–GnRH-III derivative conjugates on colon carcinoma-bearing mice. In: Anti-Cancer Drugs. 2012, 23(1), pp. 90-97. ISSN 0959-4973. eISSN 1473-5741. Available under: doi: 10.1097/CAD.0b013e32834bb6b4
BibTex
@article{Manea2012-01Inviv-17234,
  year={2012},
  doi={10.1097/CAD.0b013e32834bb6b4},
  title={In-vivo antitumour effect of daunorubicin–GnRH-III derivative conjugates on colon carcinoma-bearing mice},
  number={1},
  volume={23},
  issn={0959-4973},
  journal={Anti-Cancer Drugs},
  pages={90--97},
  author={Manea, Marilena and Tóvári, József and Tejeda, Miguel and Schulcz, Ákos and Kapuvári, Bence and Vincze, Borbála and Mező, Gábor}
}
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