par Camby, Isabelle 
;Salmon, Isabelle ;Bourdel, E;Nagy, Nathalie ;Danguy, André ;Brotchi, Jacques ;Pasteels, Jean Lambert ;Martinez, Jean;Kiss, Robert
Référence Neuropeptides, 30, 2, page (133-139)
Publication Publié, 1996-04
;Salmon, Isabelle ;Bourdel, E;Nagy, Nathalie ;Danguy, André ;Brotchi, Jacques ;Pasteels, Jean Lambert ;Martinez, Jean;Kiss, Robert Référence Neuropeptides, 30, 2, page (133-139)
Publication Publié, 1996-04
Article révisé par les pairs
| Résumé : | Neurotensin (NT) and neurotensin receptors (NTRs) are widely found in the brain, NT may be considered as a mitogen factor in some tissues. However, no NT-mediated effects on glioma cell proliferation have been reported so far. In our present study we investigated the influence of NT on the proliferation of astrocytic tumor cell lines. To this end we used a synthetic NT agonist (JMV-449), a protease inhibitor which blocks the natural degradation of NT (JMV-531), and NT. The in vitro biological models used in the present study included the low grade SW1088, and the high grade U87, U373 and A172 astrocytic tumor cell lines. The peptide-induced influence on astrocytic tumor cell proliferation was investigated by means of the colorimetric MTT assay. Our results show that the NT and the NT agonist significantly stimulated the proliferation in 2/4 and 3/4 of the astrocytic cell lines respectively. Similarly, compound JMV-531 also induced an increase in the proliferation of 2/4 of the astrocytic cell lines. This marked influence of the NT and NT agonists, or the enzyme-endogenous prevention of its degradation on the regulation of astrocytic tumor growth therefore suggests that NT antagonists might be used to treat certain patients with high grade astrocytic tumors that do not respond to chemotherapy and/or radiotherapy. |
