2015
DOI: 10.1016/j.nucmedbio.2015.07.004
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PET-CT imaging with [18F]-gefitinib to measure Abcb1a/1b (P-gp) and Abcg2 (Bcrp1) mediated drug–drug interactions at the murine blood–brain barrier

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Cited by 23 publications
(18 citation statements)
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“…Inadequate brain delivery of TKIs is probably the most important reason why clinical trials to treat CNS malignancies with TKIs have largely remained without success, even though growth of a considerable percentage of brain tumors may be dependent on activated tyrosine kinases . Several radiolabeled versions of these drugs ([ 11 C]imatinib, [ 11 C]erlotinib, [ 11 C]gefitinib, [ 18 F]gefitinib, [ 11 C]sorafenib, [ 11 C]lapatinib, and [ 18 F]afatinib) have been synthesized, and it was shown that some of these tracers allow studying of the functional interplay of P‐gp and BCRP at the BBB . Transporter‐mediated DDIs resulting in increases in brain distribution of dual P‐gp/BCRP substrates, such as TKIs, would require perpetrator drugs that inhibit both transporters simultaneously at clinically relevant plasma concentrations.…”
Section: Transporter‐mediated Ddis Assessed With Petmentioning
confidence: 99%
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“…Inadequate brain delivery of TKIs is probably the most important reason why clinical trials to treat CNS malignancies with TKIs have largely remained without success, even though growth of a considerable percentage of brain tumors may be dependent on activated tyrosine kinases . Several radiolabeled versions of these drugs ([ 11 C]imatinib, [ 11 C]erlotinib, [ 11 C]gefitinib, [ 18 F]gefitinib, [ 11 C]sorafenib, [ 11 C]lapatinib, and [ 18 F]afatinib) have been synthesized, and it was shown that some of these tracers allow studying of the functional interplay of P‐gp and BCRP at the BBB . Transporter‐mediated DDIs resulting in increases in brain distribution of dual P‐gp/BCRP substrates, such as TKIs, would require perpetrator drugs that inhibit both transporters simultaneously at clinically relevant plasma concentrations.…”
Section: Transporter‐mediated Ddis Assessed With Petmentioning
confidence: 99%
“…Such compounds are expected to be very rare. It was shown that pretreatment of wild‐type mice with elacridar, the most potent experimental dual P‐gp/BCRP inhibitor known to date, increased brain exposure of [ 11 C]gefitinib, [ 18 F]gefitinib, or [ 11 C]erlotinib to comparable levels as in Mdr1a/b (‐/‐) Bcrp1 (‐/‐) mice, suggesting that elacridar can completely inhibit P‐gp and BCRP at the mouse BBB . Human PET studies using elacridar as P‐gp/BCRP inhibitor have not so far been reported.…”
Section: Transporter‐mediated Ddis Assessed With Petmentioning
confidence: 99%
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“…Overall, those results indicated that gefitinib is a substrate of both human and murine efflux transporters, albeit with potential species specific differences in their affinities for the drug [61]. …”
Section: Introductionmentioning
confidence: 99%