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Anti-tumour activity of tachykinin NK1receptor antagonists on human glioma U373 MG xenograft

机译:速激肽NK1受体拮抗剂对人神经胶质瘤U373 MG异种移植物的抗肿瘤活性

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摘要

Astrocytes harbour functional receptors to many neurotransmitters, including substance P (SP), an undecapeptide belonging to the tachykinin family of peptide transmitters. SP activates malignant glial cells to induce cytokine release and proliferation, both responses being relevant for tumour progression. In tumours developed in nude mice transplanted subcutaneously (s.c.) to U373 MG human glioma cells, the presence of SP was observed at immunohistochemistry. Although the administration of exogenous SP did not significantly affect the size or development of U373 MG xenograft, a role of SP in supporting glioma progression in vivo was highlighted by the tumour growth inhibition induced by highly specific and selective human tachykinin NK1receptor antagonists (MEN 11467 and MEN 11149). The anti-tumour activity of MEN 11467 was observed both with s.c. or intravenous treatments and was partially reverted by the concomitant administration of exogenous SP. Doxorubicin did not show any activity in controlling U373 MG growth in this in vivo model. A novel therapeutic approach to treat malignant gliomas with tachykinin NK1receptor antagonists is suggested by these findings. © 2000 Cancer Research Campaign
机译:星形胶质细胞对许多神经递质具有功能性受体,包括物质P(SP),一种属于肽激肽释放素速激肽家族的十一肽。 SP激活恶性神经胶质细胞以诱导细胞因子的释放和增殖,这两种反应都与肿瘤的进展有关。在皮下(s.c.)移植到U373 MG人脑胶质瘤细胞的裸鼠体内形成的肿瘤中,在免疫组织化学中观察到SP的存在。尽管外源性SP的施用并未显着影响U373 MG异种移植物的大小或发育,但高度特异性和选择性的人类速激肽NK1受体拮抗剂诱导的肿瘤生长抑制突显了SP在体内支持神经胶质瘤进展的作用(MEN 11467和男士11149)。皮下注射均观察到MEN 11467的抗肿瘤活性。或静脉内治疗,并同时给予外源性SP可部分恢复。在该体内模型中,阿霉素在控制U373 MG生长方面未显示任何活性。这些发现提出了一种用速激肽NK1受体拮抗剂治疗恶性神经胶质瘤的新颖治疗方法。 ©2000癌症研究运动

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