Publication | Closed Access
Limitations of the reporter green fluorescent protein under simulated tumor conditions.
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Citations
28
References
2001
Year
Oncologic ImagingMolecular BiologyCellular Gfp FluorescenceCancer BiologyTumor BiologyOxidative StressRedox RegulatorCancer Cell BiologyMolecular ImagingCancer ResearchSimulated Tumor ConditionsMedicineHypoxia (Medicine)Tumor TargetingGene ExpressionCell BiologyTumor MicroenvironmentReporter Gene AssayNatural SciencesGfp FluorescenceTissue OxygenationFluorescence Recovery
This paper reports a detailed analysis of the effect of low oxygen conditions (hypoxia) on the reporter green fluorescent protein (GFP). It questions the feasibility of using GFP for gene expression studies under tumor conditions. Hypoxia is a characteristic of both experimental and clinical tumors. Several important factors are pointed out which need to be considered when using GFP as reporter gene. GFP fluorescence is the final product of a long and complex pathway involving transcription, translation, and posttranslational modifications. All of these steps may be affected by the availability of oxygen. We show specifically that cellular GFP fluorescence decreased with reduced oxygenation, anoxia virtually eliminated fluorescence and protein levels, and fluorescence recovery after anoxia required 5-10 h of reoxygenation. In conclusion, GFP appears to be a good marker gene to study location or movement of proteins or cells but should be used with great caution as a reporter of gene expression under tumor conditions.
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