by Impact Journals LLC
Role for ABCB1 in PDAC chemoresistance. Credit: Oncotarget (2024). DOI: 10.18632/oncotarget.28597
A new editorial paper titled "Targeting ABC transporters in PDAC—past, present, or future?" has been published in Oncotarget.
In this new editorial, Cecilia Bergonzini, Elisa Giovannetti and Erik H.J. Danen from Leiden University discuss targeting ABC transporters in pancreatic ductal carcinoma (PDAC). Despite its lower incidence when compared to more common cancers such as lung or breast carcinomas, PDAC ranks as the third-leading cause of cancer mortality in the US and the sixth worldwide. This is due to the fact that PDAC survival rates are among the lowest for cancer patients, around 13% in the US.
ATP-binding cassette (ABC) transporters represent a family of transmembrane proteins that—using the energy from ATP hydrolysis—extrude molecules from the cytoplasm to the exterior or into vesicles. Some of these transporters have been associated with resistance to a spectrum of structurally diverse chemotherapeutic drugs, earning them the name of multidrug resistance (MDR) pumps.
One of the best-characterized ABC transporters is ABCB1 (MDR1). It is physiologically expressed in tissues such as kidney, liver, pancreas, intestine, the blood-brain barrier, and more, where it exerts a protective role, by extruding xenobiotics and potentially toxic molecules. Moreover, increased ABCB1 expression in tumors has been associated with poor prognosis.
"Paclitaxel is a bona fide substrate for ABCB1 and ABCB1 has been implicated in paclitaxel and nab-paclitaxel resistance in multiple types of cancer. Could ABCB1 represent a therapeutic target in PDAC patients to suppress resistance against GnP? We have recently reported that ABCB1 can indeed play a critical role in paclitaxel resistance in PDAC cells," the researchers write.
More information: Cecilia Bergonzini et al, Targeting ABC transporters in PDAC - past, present, or future?, Oncotarget (2024). DOI: 10.18632/oncotarget.28597
Journal information: Oncotarget
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