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缺氧诱导因子-1:一种氧和金属反应性转录因子。

HIF-1: an oxygen and metal responsive transcription factor.

作者信息

Maxwell Patrick, Salnikow Konstantin

机构信息

Imperial College, London, UK.

出版信息

Cancer Biol Ther. 2004 Jan;3(1):29-35. doi: 10.4161/cbt.3.1.547. Epub 2004 Jan 10.

Abstract

Normal development and function of metazoan organisms depend on oxygen availability. The level of oxygen can be sensed by individual cells, which respond to reduced oxygenation (hypoxia) largely through activation of hypoxia-inducible factor-1 (HIF-1). At the organism level the response to hypoxia involves an increase in red blood cell production. Within tissues, HIF activation increases the blood supply and blood vessel growth. At the individual cell level it is manifested as an increase in anaerobic metabolism in order to sustain basic cellular functions. Iron is central to the oxygen sensing mechanism, and sensitivity to other metals, namely cobalt and nickel, is a distinctive feature of the HIF system; in fact, this is often used as an initial way of implicating HIF-1 in a biological response. Historically, the fact that nickel or cobalt mimicked hypoxia provided an important clue as to the nature of the oxygen sensing mechanism. It also raises the possibility that nickel or cobalt exposure may have important toxic and pathological effects mediated by HIF activation. Here we review the implications of the metal sensitivity of the HIF-1 system, and examine the hypothesis that HIF-1 activation may play an important role in metal induced carcinogenesis.

摘要

后生动物的正常发育和功能依赖于氧气供应。单个细胞能够感知氧气水平,这些细胞主要通过激活缺氧诱导因子-1(HIF-1)来对氧合减少(缺氧)做出反应。在机体水平上,对缺氧的反应包括红细胞生成增加。在组织内,HIF激活会增加血液供应和血管生长。在单个细胞水平上,它表现为无氧代谢增加,以维持基本的细胞功能。铁是氧感应机制的核心,对其他金属(即钴和镍)的敏感性是HIF系统的一个显著特征;事实上,这通常被用作将HIF-1与生物反应联系起来的一种初步方法。从历史上看,镍或钴模拟缺氧这一事实为氧感应机制的本质提供了重要线索。这也增加了镍或钴暴露可能通过HIF激活产生重要毒性和病理效应的可能性。在这里,我们回顾了HIF-1系统金属敏感性的影响,并探讨了HIF-1激活可能在金属诱导的致癌作用中发挥重要作用这一假说。

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