Literature DB >> 15072590

Reduced HGF expression in subcutaneous CT26 tumor genetically modified to secrete NK4 and its possible relation with antitumor effects.

Takeshi Kubota1, Hitoshi Fujiwara, Hisashi Amaike, Kazuhiro Takashima, Satoshi Inada, Kiyoto Atsuji, Mamoru Yoshimura, Kunio Matsumoto, Toshikazu Nakamura, Hisakazu Yamagishi.   

Abstract

Tumor-stromal interactions, which are regulated by stromal-derived HGF and tumor-derived HGF inducers, are essential for tumor cell acquisition of such malignant properties as invasion and metastasis. NK4, a proteolytic cleavage product of HGF, has antitumor activities as both an HGF antagonist and an angiogenesis inhibitor. In this study, we examined the in vitro and in vivo behaviors of mouse colon adenocarcinoma C T26 cells modified by gene transfer to secrete NK4, and investigated the influence of NK4 on expression of HGF and HGF inducers associated with tumor-stromal interactions. In vitro cell proliferation rates of NK4 transfectant (C T26-NK4) and mock transfectant (C T26-NEO) were essentially the same, and scattering and invasion were stimulated by HGF in C T26-NEO, but not in C T26-NK4. In syngeneic BALB/c female mice, subcutaneous tumor growth of C T26-NK4 was potently suppressed, and the survival was prolonged significantly. Immunohistochemistry showed significantly decreased microvessels and increased apoptotic cells in C T26-NK4 tumor compared with control. Interestingly, HGF, strongly expressed in C T26-NEO tumor stroma, was reduced in C T26-NK4. In vitro, conditioned medium of C T26-NK4 inhibited fibroblast-derived HGF production, which was increased by that of C T26-NEO. Moreover, although similar constitutive expression levels of PDGF and TGF-alpha (both HGF inducers) were detected in C T26-NK4 and C T26-NEO in semiquantitative RT-PCR analyses, the expression was up-regulated by HGF in C T26-NEO, but not C T26-NK4. These results suggest that NK4 may exert antitumor activities not only by antagonizing HGF, but also by inhibiting HGF amplification via tumor-stromal interactions. Continuous, abundant NK4 production induced at a tumor site by gene transfer should show multiple antitumor activities with potential therapeutic benefit.

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Year:  2004        PMID: 15072590     DOI: 10.1111/j.1349-7006.2004.tb03210.x

Source DB:  PubMed          Journal:  Cancer Sci        ISSN: 1347-9032            Impact factor:   6.716


  6 in total

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Journal:  World J Gastroenterol       Date:  2006-07-07       Impact factor: 5.742

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Journal:  EMBO Rep       Date:  2017-07-27       Impact factor: 8.807

3.  Experimental liver metastasis: standards for local cell implantation to study isolated tumor growth in mice.

Authors:  Otto Kollmar; Martin K Schilling; Michael D Menger
Journal:  Clin Exp Metastasis       Date:  2004       Impact factor: 5.150

4.  NK4, an HGF antagonist, prevents hematogenous pulmonary metastasis by inhibiting adhesion of CT26 cells to endothelial cells.

Authors:  Takeshi Kubota; Hiroaki Taiyoh; Atsushi Matsumura; Yasutoshi Murayama; Daisuke Ichikawa; Kazuma Okamoto; Hitoshi Fujiwara; Hisashi Ikoma; Masayoshi Nakanishi; Shojiro Kikuchi; Chouhei Sakakura; Toshiya Ochiai; Yukihito Kokuba; Hiroki Taniguchi; Teruhisa Sonoyama; Kunio Matsumoto; Toshikazu Nakamura; Eigo Otsuji
Journal:  Clin Exp Metastasis       Date:  2009-02-21       Impact factor: 5.150

5.  Suppression of human colon tumor growth by adenoviral vector-mediated NK4 expression in an athymic mouse model.

Authors:  Jian-Zheng Jie; Jian-Wei Wang; Jian-Guo Qu; Tao Hung
Journal:  World J Gastroenterol       Date:  2007-04-07       Impact factor: 5.742

6.  A Salmonella nanoparticle mimic overcomes multidrug resistance in tumours.

Authors:  Regino Mercado-Lubo; Yuanwei Zhang; Liang Zhao; Kyle Rossi; Xiang Wu; Yekui Zou; Antonio Castillo; Jack Leonard; Rita Bortell; Dale L Greiner; Leonard D Shultz; Gang Han; Beth A McCormick
Journal:  Nat Commun       Date:  2016-07-25       Impact factor: 14.919

  6 in total

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