ABC Transporters and Multidrug Resistance 2009
DOI: 10.1002/9780470495131.ch5
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ABC Proteins and Oncology: Expression, Detection, and Implication of ABC Proteins in Solid Tumors

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Cited by 5 publications
(7 citation statements)
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“…In phase 0, ABCBs would transport toxicants that do not have enzymatic modifications out of the cell. In phase III, ABCC and ABCG transporter subfamilies would transport toxicants that were modified by detoxifying enzymes during phases I and II (e.g., CYP450, GSTs, or UDP-glycosyltransferases) out of the cell 2 3 . Our data appeared to support the role of ABCB transporters early after insecticide treatment.…”
Section: Discussionmentioning
confidence: 99%
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“…In phase 0, ABCBs would transport toxicants that do not have enzymatic modifications out of the cell. In phase III, ABCC and ABCG transporter subfamilies would transport toxicants that were modified by detoxifying enzymes during phases I and II (e.g., CYP450, GSTs, or UDP-glycosyltransferases) out of the cell 2 3 . Our data appeared to support the role of ABCB transporters early after insecticide treatment.…”
Section: Discussionmentioning
confidence: 99%
“…Interestingly, ABCG4 was also overexpressed at early time points after treatment, with the highest value observed at 6 h. This observation indicated that this ABC subfamily could play a role during the initial phase of the detoxification process. Moreover, while studies have shown that the detoxification process can be subdivided into different phases in which different enzymatic complexes act, the time after insecticide treatment at which each single phase starts is unknown 2 3 . Future genome-wide expression studies, carried out at different time points after insecticide treatment, could help to elucidate the interplay among the protein complexes involved in the detoxification process, including phase I and phase II enzymes and ABC transporters.…”
Section: Discussionmentioning
confidence: 99%
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“…Besides their elevated proliferative and invasive capacity, these cells also demonstrate high resistance to anticancer treatments, in particular, to chemotherapy (chemoresistance). One of the mechanisms behind chemoresistance is the overexpression of plasma membrane pumps (ABC transporters) which expel chemotherapeutics from the cell interior [3]. The overall functional characterization of MDR in TICs to date has been provided by a widely used flow cytometric side population assay.…”
Section: Introductionmentioning
confidence: 99%