TAS-102: A Novel Antimetabolite for the 21st Century

Uboha, Nataliya Volodymyrivna; Hochster, Howard S.

doi:10.2217/fon.15.276

Cited by 20 publications

(15 citation statements)

References 55 publications

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“…Our data demonstrate that fluorinated and ethynyl-deoxyuridine analogues selectively induced DNA damage in p53mt cancer cells. Fluorinated uridine antimetabolites (FdUrd and 5FU) have been in clinical practice for several decades and their pharmacology is well studied 54 , 55 . The main mechanism of action for these analogues involves inhibition of thymidylate synthase (TS) by a common metabolite FdUMP, leading to a reduction of dTTP levels and promoting the incorporation of dUTP and FdUTP into the genome 46 , 55 .…”

Section: Discussionmentioning

confidence: 99%

Selective therapeutic strategy for p53-deficient cancer by targeting dysregulation in DNA repair

et al. 2021

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Breast carcinomas commonly carry mutations in the tumor suppressor p53, although therapeutic efforts to target mutant p53 have previously been unfruitful. Here we report a selective combination therapy strategy for treatment of p53 mutant cancers. Genomic data revealed that p53 mutant cancers exhibit high replication activity and express high levels of the Base-Excision Repair (BER) pathway, whereas experimental testing showed substantial dysregulation in BER. This defect rendered accumulation of DNA damage in p53 mutant cells upon treatment with deoxyuridine analogues. Notably, inhibition of poly (ADP-ribose) polymerase (PARP) greatly enhanced this response, whereas normal cells responded with activation of the p53-p21 axis and cell cycle arrest. Inactivation of either p53 or p21/CDKN1A conferred the p53 mutant phenotype. Preclinical animal studies demonstrated a greater anti-neoplastic efficacy of the drug combination (deoxyuridine analogue and PARP inhibitor) than either drug alone. This work illustrates a selective combination therapy strategy for p53 mutant cancers that will improve survival rates and outcomes for thousands of breast cancer patients.

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Section: Discussionmentioning

confidence: 99%

Selective therapeutic strategy for p53-deficient cancer by targeting dysregulation in DNA repair

et al. 2021

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“…Furthermore, defluorination can be directly connected to the mode of action of TFT. Although DNA incorporation of tri-phosphorylated TFT is considered the main mechanism by which it exerts anticancer properties, 39 , 40 mono-phosphorylated TFT also covalently binds to and inhibits thymidylate synthase (TS). 41 Several reports have determined that this covalent linkage results in a stepwise loss of the three fluorine substituents of TFT, 42 – 44 which in the case of [ 18 F]TFT, would result in bone uptake of free [ 18 F]fluoride in the PET scans.…”

Section: Resultsmentioning

confidence: 99%

Radiosynthesis of the anticancer nucleoside analogue Trifluridine using an automated ¹⁸F-trifluoromethylation procedure

et al. 2018

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“…Inhibits de novo purine synthesis Produces genotoxic thioguanine nucleotides that inhibit DNA and RNA synthesis and alter their subsequent metabolism [7,9] Thymidine phophorylase inhibitor Tipiracil Hydrochloride (TAS-102) Induces cell cycle arrest at G2 phase and DNA double-strand breaks with enhanced drug potency. [135,136] Antifolate Methotrexate, Pemetrexed…”

Section: Discussionmentioning

confidence: 99%

Getting Lost in the Cell–Lysosomal Entrapment of Chemotherapeutics

Zhai

Hiani

2020

Cancers

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Despite extensive research, resistance to chemotherapy still poses a major obstacle in clinical oncology. An exciting strategy to circumvent chemoresistance involves the identification and subsequent disruption of cellular processes that are aberrantly altered in oncogenic states. Upon chemotherapeutic challenges, lysosomes are deemed to be essential mediators that enable cellular adaptation to stress conditions. Therefore, lysosomes potentially hold the key to disarming the fundamental mechanisms of chemoresistance. This review explores modes of action of classical chemotherapeutic agents, adaptive response of the lysosomes to cell stress, and presents physiological and pharmacological insights pertaining to drug compartmentalization, sequestration, and extracellular clearance through the lens of lysosomes.

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TAS-102: A Novel Antimetabolite for the 21st Century

Cited by 20 publications

References 55 publications

Selective therapeutic strategy for p53-deficient cancer by targeting dysregulation in DNA repair

Selective therapeutic strategy for p53-deficient cancer by targeting dysregulation in DNA repair

Radiosynthesis of the anticancer nucleoside analogue Trifluridine using an automated ¹⁸F-trifluoromethylation procedure

Getting Lost in the Cell–Lysosomal Entrapment of Chemotherapeutics

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TAS-102: A Novel Antimetabolite for the 21st Century

Cited by 20 publications

References 55 publications

Selective therapeutic strategy for p53-deficient cancer by targeting dysregulation in DNA repair

Selective therapeutic strategy for p53-deficient cancer by targeting dysregulation in DNA repair

Radiosynthesis of the anticancer nucleoside analogue Trifluridine using an automated 18F-trifluoromethylation procedure

Getting Lost in the Cell–Lysosomal Entrapment of Chemotherapeutics

Contact Info

Product

Resources

About

Radiosynthesis of the anticancer nucleoside analogue Trifluridine using an automated ¹⁸F-trifluoromethylation procedure