Summary:
Hypoxia results in increased expression of some genes. This can compensate effects of hypoxia on the organism,
and adapt cells and tissues to the environment with low oxygen tension. Mechanisms of cell and tissue responses to
hypoxia have been extensively studied last years. The first identified mediator of cell response to hypoxia was
hypoxia-inducible factor (HIF-1), which is being up regulated during hypoxic conditions. It binds to regulatory
regions of sensitive genes and increases their transcription rate. Other key elements of cell response to hypoxia have
been described recently – von Hippel-Lindau protein and prolyl hydroxylases, that allow degradation of α-subunit
of HIF-1 during normal oxygen tension. This can ensure low level of HIF-1 in cells under physiological oxygen
tension thus the expression of target genes is maintained on basal level. These new findings are starting points for
further research and possible therapeutic use.
Key words:
hypoxia, von Hippel-Lindau, hypoxia inducible factor-1, regulation of gene expression.
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