Hypoxia-Inducible Factor (HIF): Fuel for Cancer Progression

Abstract
Hypoxia is an integral part of the tumor microenvironment, caused primarily due to rapidly multiplying tumor cells and a lack of proper blood supply. Among the major hypoxic pathways, HIF-1 transcription factor activation is one of the widely investigated pathways in the hypoxic tumor microenvironment (TME). HIF-1 is known to activate several adaptive reactions in response to oxygen deficiency in tumor cells. HIF-1 has two subunits, HIF-1 beta (constitutive) and HIF-1 alpha (inducible). The HIF-1 alpha expression is largely regulated via various cytokines (through PI3K-ACT-mTOR signals), which involves the cascading of several growth factors and oncogenic cascades. These events lead to the loss of cellular tumor suppressant activity through changes in the level of oxygen via oxygen-dependent and oxygen-independent pathways. The significant and crucial role of HIF in cancer progression and its underlying mechanisms have gained much attention lately among the translational researchers in the fields of cancer and biological sciences, which have enabled them to correlate these mechanisms with various other disease modalities. In the present review, we have summarized the key findings related to the role of HIF in the progression of tumors.
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Keywords
Hypoxia, normoxia, microenvironment, tumor, HIF, hydroxylation, cancer progression, ARYL-HYDROCARBON RECEPTOR, VHL TUMOR-SUPPRESSOR, PAS DOMAIN PROTEIN-1, FACTOR 1-ALPHA, FACTOR-I, TRANSCRIPTION FACTOR, GENE-EXPRESSION, SIGNAL-TRANSDUCTION, DNA-BINDING, MAP KINASE
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