Abstract
Multidrug resistance (MDR) to chemotherapeutic drugs remains one of the major impediments to the treatment of cancer. Discovery and development of drugs that can prevent and reverse the acquisition of multidrug resistance constitute a foremost challenge in cancer therapeutics. In this work, we screened a library of 1,127 compounds with known targets for their ability to overcome Pgp-mediated multidrug resistance in cancer cell lines. We identified four compounds (CHIR-124, Elesclomol, Tyrphostin-9 and Brefeldin A) that inhibited the growth of two pairs of parental and Pgp-overexpressing multidrug-resistant cell lines with similar potency irrespective of their Pgp status. Mechanistically, CHIR-124 (a potent inhibitor of Chk1 kinase) inhibited Pgp activity in both multidrug-resistant cell lines (KB-V1 and A2780-Pac-Res) as determined through cell-based Pgp-efflux assays. Other three inhibitors on the contrary, were effective in Pgp-overexpressing resistant cells without increasing the cellular accumulation of a Pgp substrate, indicating that they overcome resistance by avoiding efflux through Pgp. None of these compounds modulated the expression of Pgp in resistant cell lines. PIK-75, a PI3 Kinase inhibitor, was also determined to inhibit Pgp activity, despite being equally potent in only one of the two pairs of resistant and parental cell lines. Strong binding of both CHIR-124 and PIK-75 to Pgp was predicted through docking studies and both compounds inhibited Pgp in a biochemical assay. The inhibition of Pgp causes accumulation of these compounds in the cells where they can modulate the function of their target proteins and thereby inhibit cell proliferation. In conclusion, we have identified compounds with various cellular targets that overcome multidrug resistance in Pgp-overexpressing cell lines through mechanisms that include Pgp inhibition and efflux evasion. These compounds, therefore, can avoid challenges associated with the co-administration of Pgp inhibitors with chemotherapeutic or targeted drugs such as additive toxicities and differing pharmacokinetic properties.
Highlights
Chemotherapy is one of the most common and successful treatments for cancers
We screened a library of 1,127 inhibitors with known targets in a pair of parental and multidrug-resistant cell lines for their ability to overcome Permeability glycoprotein (Pgp)-mediated multidrug resistance in a 3-day proliferation assay
Identification of compounds that can overcome multidrug resistance (MDR) through highthroughput screening In order to identify compounds with the ability to overcome Pgp-mediated MDR, we screened a library of 1,127 inhibitors (Selleckchem inhibitor library) in KB-3-1 cell line, and its multidrugresistant (Pgp overexpressing) derivative cell line, KB-V1 (Fig 1A)
Summary
The success of chemotherapy, can be limited by several factors including toxicity and the development of multidrug resistance (MDR), where cancer cells become resistant to structurally and functionally unrelated drugs[1]. Among various mechanisms that contribute to the development of multidrug resistance, overexpression of ABC (ATP binding cassette) transporters is the most prevalent. Forty-eight ABC transporters from seven different families (ABCA-ABCG) have been identified in the human genome, and nearly twenty of them act as drug efflux pumps. These include Permeability glycoprotein (Pgp), MDR-associated protein 1 (MRP1) and breast cancer resistant protein (BCRP), among others[3]. MDR1 overexpression can result from gene amplification or transcriptional activation[5, 6]
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