2008
DOI: 10.1158/0008-5472.can-07-5472
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Chronic Hypoxia Decreases Synthesis of Homologous Recombination Proteins to Offset Chemoresistance and Radioresistance

Abstract: Hypoxic and/or anoxic tumor cells can have increased rates of mutagenesis and altered DNA repair protein expression. Yet very little is known regarding the functional consequences of any hypoxia-induced changes in the expression of proteins involved in DNA double-strand break repair. We have developed a unique hypoxic model system using H1299 cells expressing an integrated direct repeat green fluorescent protein (DR-GFP) homologous recombination (HR) reporter system to study HR under prolonged chronic hypoxia … Show more

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Cited by 278 publications
(308 citation statements)
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References 48 publications
(73 reference statements)
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“…The residual 8-oxo-dG accumulated under hypoxic conditions is therefore probably a result of impaired BER and MMR pathways. It has previously been documented that hypoxiapretreated cells have increased radiosensitivity and at the time this was attributed to a hypoxia-mediated defect in HR (23). However, in light of these findings, decreased BER may also play a role.…”
Section: Discussionmentioning
confidence: 94%
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“…The residual 8-oxo-dG accumulated under hypoxic conditions is therefore probably a result of impaired BER and MMR pathways. It has previously been documented that hypoxiapretreated cells have increased radiosensitivity and at the time this was attributed to a hypoxia-mediated defect in HR (23). However, in light of these findings, decreased BER may also play a role.…”
Section: Discussionmentioning
confidence: 94%
“…Logarithmically growing cells were exposed to 0.2% O 2 with 5% CO 2 and balance N 2 using an Invivo2 400 Hypoxic Workstation (Ruskinn). The chronic hypoxic gassing condition (72 hours with 0.2% O 2 ) was based on previous studies in which the translation of DNA repair genes was downregulated by hypoxia (23,45). This gassing condition for RKO and HCT116 cells was optimal for (i) minimizing toxicity (e.g., 35%-50% cell kill based on clonogenic survival assays); (ii) no effect on S-phase fraction or cell proliferation; and (iii) maintaining the inhibitory effect of hypoxia on protein translation (see Supplementary Fig.…”
Section: Cell Culture and Hypoxic Treatmentsmentioning
confidence: 99%
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