Doxorubicin prodrug for cytoplasmic and nuclear delivery in breast cancer cells

Animikh Ray, K. Cholkar, Ravinder Earla, A. Mitra
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引用次数: 3

Abstract

Purpose: The objective of this study was to develop a novel peptide prodrug of doxorubicin which can evade over-expressed efflux pumps in breast cancer cells. This approach may lead to increased uptake and higher drug accumulation in nuclei of cancer cells. Materials and Methods: L-val-L-val doxorubicin prodrug was synthesized following standard f-moc chemistry. The prodrug was analyzed for stability, cellular and nuclear uptake and interaction with efflux and peptide transporters. Breast cancer cells (T47D) were grown on polystyrene 12-well plates. Result: The prodrug Val-Val-doxorubicin was found to be very stable in breast cancer cell homogenate. It was able to evade efflux pumps. The prodrug penetrated cytoplasm and nucleus of cancer cells by interacting with peptide transporters.These transporters (pepT1 and pepT2) are expressed both on plasma and nuclear membrane of breast cancer cells. Uptake of prodrug was found to be 10 times more than parent drug. Conclusion: Peptide prodrug derivatization of doxorubicin has potential to evade efflux pumps and increase availability and nuclear accumulation of doxorubcin in breast cancer cells.
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阿霉素前药在乳腺癌细胞的细胞质和核传递
目的:本研究的目的是开发一种新的多肽前药阿霉素,它可以逃避乳腺癌细胞中过表达的外排泵。这种方法可能导致增加摄取和更高的药物积累在细胞核的癌细胞。材料与方法:采用标准f-moc化学方法合成左旋-左旋阿霉素前药。分析了前药的稳定性、细胞和核摄取以及与外排和肽转运体的相互作用。乳腺癌细胞(T47D)在聚苯乙烯12孔板上生长。结果:发现前药val - val -阿霉素在乳腺癌细胞匀浆中非常稳定。它能够避开外排泵。前药通过与肽转运体相互作用穿透细胞质和细胞核。这些转运蛋白(pepT1和pepT2)在乳腺癌细胞的血浆和核膜上均有表达。发现前药的摄取是母体药物的10倍。结论:多柔比星的肽前药物衍生化有可能逃避外排泵,增加多柔比星在乳腺癌细胞中的可用性和核积累。
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