Mice, men, mustards and methylated xanthines: the potential role of caffeine and related drugs in the sensitization of human tumours to alkylating agents

Byfield, John E.; Murnane, John P.; Ward, John F.; Calabro-Jones, Paula M.; Lynch, Michael J.; Kulhanian, Fimi

doi:10.1038/bjc.1981.98

Cited by 42 publications

(12 citation statements)

References 41 publications

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“…9,11 Increased therapeutic effect has also been achieved under circumstances when viral replication and spreading are not enhanced. 10 Tumor cells encountering 5FU at subtoxic concentrations are altered metabolically by the drug; 34 such cellular changes could potentially affect OV permissiveness. The previous study 22 addressed this question by pretreating cells with 5FU for 24 h, removing the drug at the time of infection and monitoring viral GFP expression.…”

Section: Discussionmentioning

confidence: 99%

“…No change in VSV replication was reported, although a 25% reduction in GFP-positive cells was observed at 12 h and a B7-fold reduction in viral titer at 24 h following infection at 0.1 MOI. We addressed this concern differently by using continuous 5FU treatment at concentrations corresponding to the ED50 over a period of 48 hwhich is necessary to allow 5FU cytotoxicity 34 -and by analyzing the susceptibility of the surviving cells to VSV. Although infection kinetics was slowed at low MOI, VSV was able to infect viable cells, indicating that 5FU did not affect viral infection.…”

Section: Discussionmentioning

confidence: 99%

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Enhancing VSV oncolytic activity with an improved cytosine deaminase suicide gene strategy

Léveillé

Samuel

et al. 2011

Cancer Gene Ther

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Oncolytic viruses (OVs) are promising therapeutic agents for cancer treatment, with recent studies emphasizing the combined use of chemotherapeutic compounds and prodrug suicide gene strategies to improve OV efficacy. In the present study, the synergistic activity of recombinant vesicular stomatitis virus (VSV)-MD51 virus expressing the cytosine deaminase/uracil phosphoribosyltransferase (CD::UPRT) suicide gene and 5-fluorocytosine (5FC) prodrug was investigated in triggering tumor cell oncolysis. In a panel of VSV-sensitive and -resistant cells-prostate PC3, breast MCF7 and TSA, B-lymphoma Karpas and melanoma B16-F10-the combination treatment increased killing of non-infected bystander cells in vitro via the release of 5FC toxic derivatives. In addition, we showed a synergistic effect on cancer cell killing with VSV-MD51 and the active form of the drug 5-fluorouracil. Furthermore, by monitoring VSV replication at the tumor site and maximizing 5FC bioavailability, we optimized the treatment regimen and improved survival of animals bearing TSA mammary adenocarcinoma. Altogether, this study emphasizes the potency of the VSV-CD::UPRT and 5FC combination, and demonstrates the necessity of optimizing each step of a multicomponent therapy to design efficient treatment.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Enhancing VSV oncolytic activity with an improved cytosine deaminase suicide gene strategy

Léveillé

Samuel

et al. 2011

Cancer Gene Ther

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“…Inhibition of this tyrosine kinase might have the effect of inactivating the checkpoint so that damaged cells enter mitosis without delay. The methylated xanthine, caffeine, is also known to inactivate all DNA-damage-responsive checkpoints and induces synergistic lethality in combination with chemotherapeutic drugs (53). Treatment of human fibroblasts with amsacrine and caffeine induced extraordinary chromosome damage as seen in mitotic cells (Fig.…”

Section: Checkpoints Respond To Topoisomerase-induced Dna Damagementioning

confidence: 99%

Human Topoisomerase II Function, Tyrosine Phosphorylation and Cell Cycle Checkpoints

Kaufmann¹

1998

Experimental Biology and Medicine

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Three DNA damage-responsive cell cycle checkpoints can be shown to operate in diploid human fibroblasts. One checkpoint arrests growth in G1, another inhibits replicon initiation in S phase cells, and the third delays progression from G2 into mitosis. Progression from G2 into M is controlled in part by a cyclin-dependent kinase (cyclin B/Cdk1) that is regulated by tyrosine phosphorylation. Phosphorylation of Tyr15 on Cdk1 is inhibitory for kinase activity. Activation of cyclin B/Cdk1 at the onset of mitosis is accomplished by a phosphatase, Cdc25C, that interacts with cyclin B/Cdk1 in an autocatalytic feedback loop to remove the inhibitory phosphate at Tyr15 and activate kinase activity. DNA damage triggers G2 delay by inhibiting formation of the autocatalytic feedback loop so that dephosphorylation of Tyr15 does not occur. This suppression of activation of cyclin B/Cdk1 appears to account for the failure of damaged G2 cells to progress into mitosis. Once the damage to DNA is repaired, cells resume progression into mitosis as the cycle is re-engaged. The isoflavone genistein inhibits tyrosine kinases, including one that phosphorylates Cdk1 on Tyr15. This kinase, p56/p53lyn is rapidly induced by treatments that trigger cell cycle checkpoints (ionizing radiation, cytosine arabinoside), suggesting that this kinase may actively delay the onset of mitosis by phosphorylating Tyr15 on Cdk1. Genistein also inhibits type II DNA topoisomerase to produce a form of DNA damage that triggers all of the DNA damage-responsive cell cycle checkpoints. A brief 10 min incubation with the topoisomerase poison amsacrine was sufficient to trigger the S phase checkpoint response and inhibit replicon initiation. Inhibition of replicon initiation by 1 microM amsacrine was maximal 20-30 min after drug treatment and by 120 min, the checkpoint response had decayed to allow near control rates of replicon initiation. Topoisomerase II poisons also are powerful clastogens inducing lethal and carcinogenic chromosomal aberrations. Type II topoisomerase can break DNA in a region of chromosome 11q23 that contains the ataxia telangiectasia gene (ATM). The ATM gene controls all of the DNA damage-responsive cell cycle checkpoints. Chromosomal aberrations in 11q23 are frequently seen in acute myeloid leukemia that develops as a consequence of etoposide chemotherapy. Thus, topoisomerase poisons such as genistein may trigger chromatid breakage to inactivate AT gene function, disable cell cycle control, and induce genetic instability.

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“…The desirable increase in cell sensitivity to S-phase damage might succeed in increasing the toxicity of sublethal damage. This might be achieved by increasing or prolonging the intracellular level of the active drug or by blocking the capacity of the cell to repair the drug's damage [6].…”

Section: Discussionmentioning

confidence: 99%

A Comparative Study of the Cytogenetic and Antineoplasmatic Effects Induced by Carboplatin in Combination with Niacin in Human Lymphocytes in vitro and in Ehrlich Ascites Tumor Cells in vivo

Mylonaki-Charalambours¹,

Mourelatos²,

Kotsis³

1998

Chemotherapy

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Enhanced sister chromatid exchange (SCE) levels and cell division delays were observed when cultured human lymphocytes treated with carboplatin (cPt) were exposed to niacin. Cytogenetic damage was also observed by cPt when Ehrlich ascites tumor (EAT) cells were exposed in vivo to nontoxic concentrations of niacin. One hour before intraperitoneal injection of 5-bromodeoxyuridine, adsorbed to activated charcoal, EAT-bearing mice treaded intraperitoneally with cPt appeared to have a dose-dependent increase in SCEs and cell division delays. Niacin increased the survival time of the EAT-bearing mice treated with cPt and markedly reduced the ascitic volume. Therefore the in vivo antitumor effect of cPt in conjunction with niacin appears to correlate well with the in vitro or in vivo synergistic effects on cytogenetic damage caused by the combined cPt plus Niacin treatment upon human lymphocytes or EAT cells, respectively.

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Mice, men, mustards and methylated xanthines: the potential role of caffeine and related drugs in the sensitization of human tumours to alkylating agents

Cited by 42 publications

References 41 publications

Enhancing VSV oncolytic activity with an improved cytosine deaminase suicide gene strategy

Enhancing VSV oncolytic activity with an improved cytosine deaminase suicide gene strategy

Human Topoisomerase II Function, Tyrosine Phosphorylation and Cell Cycle Checkpoints

A Comparative Study of the Cytogenetic and Antineoplasmatic Effects Induced by Carboplatin in Combination with Niacin in Human Lymphocytes in vitro and in Ehrlich Ascites Tumor Cells in vivo

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