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糖皮质激素及其他药物对人胶质瘤和非小细胞肺癌的表型修饰

Phenotypic modification of human glioma and non-small cell lung carcinoma by glucocorticoids and other agents.

作者信息

McLean J S, Frame M C, Freshney R I, Vaughan P F, Mackie A E, Singer I

出版信息

Anticancer Res. 1986 Sep-Oct;6(5):1101-6.

PMID:2879508
Abstract

Glucocorticoids are cytostatic for human glioma grown at a high cell density in cell culture. The effect is not cytotoxic, appears to involve a modification of the cell surface, and has been detected with methyl prednisolone, dexamethasone, and beta-methasone. Glucocorticoids were also found to reduce malignancy-associated properties (plasminogen activator and endothelial mitogenesis) and enhance differentiation (glutamyl synthetase activity and high affinity GABA uptake). Cytostasis was also seen at high cell densities in non-small cell lung carcinoma with a concomitant reduction in plasminogen activator activity and endothelial mitogenesis. Preliminary data on surfactant production in A549 cells suggests that the repression of malignancy-associated properties is accompanied by an increase in cell differentiation. Treatment of the WIL adenocarcinoma gown as a xenograft in nude mice caused total cessation of growth and massive central necrosis in the tumor.

摘要

糖皮质激素对细胞培养中高细胞密度生长的人胶质瘤具有细胞生长抑制作用。该作用无细胞毒性,似乎涉及细胞表面的修饰,且已在甲泼尼龙、地塞米松和倍他米松中检测到。还发现糖皮质激素可降低恶性相关特性(纤溶酶原激活剂和内皮细胞有丝分裂)并增强分化(谷氨酰胺合成酶活性和高亲和力γ-氨基丁酸摄取)。在非小细胞肺癌的高细胞密度下也观察到细胞生长抑制,同时纤溶酶原激活剂活性和内皮细胞有丝分裂减少。关于A549细胞表面活性剂产生的初步数据表明,恶性相关特性的抑制伴随着细胞分化的增加。将WIL腺癌作为裸鼠异种移植物进行处理,导致肿瘤生长完全停止并出现大量中央坏死。

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