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Understanding hypoxia signalling in cells--a new therapeutic opportunity?

机译:了解细胞中的缺氧信号-新的治疗机会吗?

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The possibility that cells possess specific interfaces with molecular oxygen that have a prime function in biological control has long interested biologists. Specific 'oxygen-sensing' mechanisms have been defined in bacteria and yeast, but, until recently, have remained elusive in higher organisms. Studies of hypoxia pathways have now, however, revealed the existence of a series of non-haem Fe(ll) and 2-oxoglutarate-dependent dioxygenases that catalyse oxygen-regulated hydroxylation of specific amino acids in a key transcription factor termed hypoxia-inducible factors (HIFs). These post-translational hydroxylations govern both the proteolytic stability and activity of HIF and therefore the transcription of many hundreds of human genes whose expression changes in accordance with cellular oxygen availability. This paper will review these developments and consider the biological and potential therapeutic implications.
机译:细胞与分子氧具有特定界面的可能性在生物学控制中起主要作用,这一直引起生物学家的兴趣。在细菌和酵母菌中已经定义了特定的“氧感应”机制,但是直到最近,在高等生物中仍然难以捉摸。现在,对缺氧途径的研究表明,存在一系列非血红素Fe(II)和2-氧戊二酸依赖性双加氧酶,这些酶在称为低氧诱导因子的关键转录因子中催化特定氨基酸的氧调节羟基化。 (HIF)。这些翻译后羟基化控制着HIF的蛋白水解稳定性和活性,并因此控制了数百个人类基因的转录,其表达随细胞氧的利用而变化。本文将回顾这些进展,并考虑其生物学和潜在的治疗意义。

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