Spreafico Adriano, Schenone Silvia, Serchi Tommaso, Orlandini Maurizio, Angelucci Adriano, Magrini David, Bernardini Giulia, Collodel Giulia, Di Stefano Anna, Tintori Cristina, Bologna Mauro, Manetti Fabrizio, Botta Maurizio, Santucci Annalisa
Università degli Studi di Siena, Dipartimento di Biologia Molecolare, via Fiorentina 1, 53100 Siena, Italy.
FASEB J. 2008 May;22(5):1560-71. doi: 10.1096/fj.07-9873com. Epub 2008 Jan 2.
Osteosarcoma is the most frequent primitive malignant tumor of the skeletal system, characterized by an extremely aggressive clinical course that still lacks an effective treatment. Src kinase seems to be involved in the osteosarcoma malignant phenotype. We show that the treatment of human osteosarcoma cell lines with a new pyrazolo[3,4-d]pyrimidine derivative Src inhibitor, namely SI-83, impaired cell viability, with a half-maximal inhibitory concentration of 12 microM in nonstarved cells and a kinetic different from that known for the Src inhibitor PP2. Analysis by terminal deoxynucleotidyl transferase-mediated nick end labeling, Hoechst, and flow cytometric assay showed that SI-83 induced apoptosis in SaOS-2 cells. Moreover, SI-83, by inhibiting Src phosphorylation, decreased in vivo osteosarcoma tumor mass in a mouse model. Finally, SI-83 showed selectivity for osteosarcoma, since it had a far lower effect in primary human osteoblasts. These results show that human osteosarcoma had Src-dependent proliferation and that modulation of Src activity may be a therapeutic target of this new compound with low toxicity for nonneoplastic cells.
骨肉瘤是骨骼系统中最常见的原发性恶性肿瘤,其临床病程极具侵袭性,目前仍缺乏有效的治疗方法。Src激酶似乎与骨肉瘤的恶性表型有关。我们发现,用一种新型吡唑并[3,4-d]嘧啶衍生物Src抑制剂SI-83处理人骨肉瘤细胞系,会损害细胞活力,在未饥饿细胞中的半数最大抑制浓度为12微摩尔,其动力学与已知的Src抑制剂PP2不同。通过末端脱氧核苷酸转移酶介导的缺口末端标记、Hoechst染色和流式细胞术分析表明,SI-83可诱导SaOS-2细胞凋亡。此外,SI-83通过抑制Src磷酸化,在小鼠模型中减少了体内骨肉瘤肿瘤块。最后,SI-83对骨肉瘤具有选择性,因为它对原代人成骨细胞的作用要小得多。这些结果表明,人骨肉瘤具有Src依赖性增殖,调节Src活性可能是这种对非肿瘤细胞毒性低的新化合物的治疗靶点。
