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Revisiting strategies to target ABC transporter-mediated drug resistance in CNS cancer

摘要A significant number of anticancer drugs fail to treat primary and metastatic brain tumors primarily because of the complex blood-brain barrier(BBB)and overexpression of ATP-binding cassette(ABC)transporters,which decrease drug penetration into the central nervous system and ultimately into tumors.It is noteworthy that the ABC transporters,ABCB1[known as P-glycoprotein(P-gp)]and ABCG2[known as breast cancer resistance protein(BCRP)],are overexpressed in brain tumors,including common gliomas.The co-presence of these transporters may negate the inhibition of either transporter,particularly if both transport the same anticancer drug.The cellular export of drugs by ABC transporters has been implicated in mediating resistance to anticancer drugs.However,the clinical relevance as a therapeutic target in human tumors remains a matter of contention.Although effective and clinically approved ABC transporter inhibitors could potentially overcome drug resistance,none are currently approved.Furthermore,the ABC transporter inhibitors in clinical trials produced low or no clinical efficacy,significant toxicities,and unsuitable pharmacokinetic profiles.Therefore,innovative approaches are needed to efficaciously and simultaneously inhibit these transporters to surmount anticancer drug resistance.This review emphasizes the clinical significance of ABC transporters in diminishing the efficacy of brain tumor treatments.The molecular alterations in BBB following brain tumor development,which are linked to various cancer therapies,are discussed.The overexpression of ABCB1 and ABCG2 at the BBB is discussed,potential strategies to decrease the export of chemotherapeutics by these transporters and the associated challenges and failures are discussed,and the implementation of novel approaches is considered.

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作者 Haneen Amawi [1] Alaa M.Hammad [2] F.Scott Hall [3] Noor Hussein [4] Aseel O.Rataan [1] Abeer Mrayyan [5] Taqwa Al-kofahi [5] Ali Hmedat [6] Charles R.Ashby Jr. [7] Amit K.Tiwari [8] 学术成果认领
作者单位 Department of Clinical Pharmacy and Pharmacy Practice,College of Pharmacy,Yarmouk University,Irbid 21163,Jordan [1] Department of Pharmacy,College of Pharmacy,Al-Zaytoonah University of Jordan,Amman 11733,Jordan [2] Department of Pharmacology and Experimental Therapeutics,College of Pharmacy and Pharmaceutical Sciences,University of Toledo,Toledo,OH 43614,USA [3] Department of Pediatrics,School of Medicine,Stanford University,Stanford,CA 94305,USA [4] Department of Biological Sciences,Faculty of Science,Yarmouk University,Irbid 21163,Jordan [5] Department of Pharmaceutics and Pharmaceutical Technology,Faculty of Pharmacy,Yarmouk University,Irbid 21163,Jordan [6] Department of Pharmaceutical Sciences,College of Pharmacy,St.John's University,Queens,NY 11439,USA [7] Department of Pharmaceutical Sciences,College of Pharmacy,University of Arkansas for Medical Sciences,Little Rock,AR 72205,USA [8]
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DOI 10.20892/j.issn.2095-3941.2025.0060
发布时间 2025-10-30(万方平台首次上网日期,不代表论文的发表时间)
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癌症生物学与医学(英文版)

癌症生物学与医学(英文版)

2025年22卷10期

1158-1180页

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