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Gamma-linolenic acid therapy of human glioma-a review of in vitro, in vivo, and clinical studies

机译:γ-亚麻酸治疗人脑胶质瘤-体外,体内和临床研究综述

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Gamma-linolenic acid (GLA) induced apoptosis of tumor cells without harming normal cells. Both cyclo-oxygenase (COX) and lipoxygenase (LO) inhibitors did not inhibit the selective tumoricidal action of GLA in some, but not all, tumor cells suggesting that GLA by itself is active. In contrast, anti-oxidants such as vitamin E blocked the tumoricidal action of GLA. GLA-treated tumor but not normal cells produced a 2–3-fold increase in free radicals and lipid peroxides. GLA decreased the anti-oxidant content of tumor cells, expression of oncogenes ras, and Bcl-2, enhanced the activity of p53, protected normal cells and tissues from the toxic actions of radiation and anti-cancer drugs, enhanced the cytotoxic action of anti-cancer drugs and reversed tumor cell drug resistance. In the animal glioma model, GLA induced tumor regression and preserved the surrounding normal brain tissue. In three open-label clinical studies, intra-tumoral injection of GLA induced significant reduction of glioma without any significant side effects. The low neurotoxicity of GLA to normal brain neurons and selective activity against tumor cells suggests that it could be an effective anti-glioma molecule.
机译:γ-亚麻酸(GLA)诱导肿瘤细胞凋亡而不损害正常细胞。环氧合酶(COX)和脂氧合酶(LO)抑制剂均不能抑制某些但不是全部肿瘤细胞中GLA的选择性杀伤作用,表明GLA本身具有活性。相反,抗氧化剂例如维生素E阻止了GLA的杀肿瘤作用。用GLA治疗的肿瘤而非正常细胞产生的自由基和脂质过氧化物增加了2-3倍。 GLA降低了肿瘤细胞的抗氧化剂含量,癌基因ras和Bcl-2的表达,增强了p53的活性,保护了正常细胞和组织免受放射线和抗癌药的毒性作用,增强了抗癌药的细胞毒性作用。 -癌症药物和逆转的肿瘤细胞耐药性。在动物神经胶质瘤模型中,GLA导致肿瘤消退并保留了周围的正常脑组织。在三项开放标签的临床研究中,肿瘤内注射GLA可诱导胶质瘤的明显减少,而没有任何明显的副作用。 GLA对正常脑神经元的低神经毒性和对肿瘤细胞的选择性活性表明,它可能是一种有效的抗神经胶质瘤分子。

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