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氧自由基代谢与肿瘤生长控制

Oxy-radical metabolism and control of tumour growth.

作者信息

Galeotti T, Masotti L, Borrello S, Casali E

机构信息

Institute of General Pathology, Catholic University, Rome, Italy.

出版信息

Xenobiotica. 1991 Aug;21(8):1041-51. doi: 10.3109/00498259109039544.

Abstract
  1. The content of oxy-radical scavenging enzymes is decreased in Morris hepatomas in a fashion which is inversely related with the growth rate of the tumour. 2. Hepatoma microsomal membranes are more resistant than normal rat liver membranes to lipid peroxidation induced in vitro by organic hydroperoxides or superoxide radicals. 3. In tumour membranes the most relevant rate-limiting factor of peroxidation is the low availability of polyunsaturated fatty acids (PUFA). Besides lipids, some proteins (particularly cytochrome P-450) act as controlling factors of peroxidation. 4. Tumour microsomes are more ordered and less fluid than liver microsomes. The latter, exposed to superoxide radical attack, exhibit chemical (fatty acid composition) and physical (molecular order) properties that are similar to those of transformed cell membranes. 5. These data indicate an aberration in the oxy-radical metabolism of cancer cells, and a sequence of events is hypothesized that could drive the transformed cell towards uncontrolled proliferation.
摘要
  1. 莫里斯肝癌中氧自由基清除酶的含量以与肿瘤生长速率呈负相关的方式降低。2. 肝癌微粒体膜比正常大鼠肝膜对有机氢过氧化物或超氧自由基在体外诱导的脂质过氧化更具抗性。3. 在肿瘤膜中,过氧化最相关的限速因素是多不饱和脂肪酸(PUFA)的低可用性。除了脂质外,一些蛋白质(特别是细胞色素P-450)作为过氧化的控制因素。4. 肿瘤微粒体比肝微粒体更有序且流动性更低。后者暴露于超氧自由基攻击下,表现出与转化细胞膜相似的化学(脂肪酸组成)和物理(分子有序性)特性。5. 这些数据表明癌细胞的氧自由基代谢存在异常,并推测了一系列可能驱使转化细胞走向不受控制的增殖的事件。

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