Nucleoside Transport Inhibitors: Structure−Activity Relationships for Pyrimido[5,4-<i>d</i>]pyrimidine Derivatives That Potentiate Pemetrexed Cytotoxicity in the Presence of α<sub>1</sub>-Acid Glycoprotein

Saravanan, Kappusamy; Barlow, HC; Barton, Marion; Calvert, A. H.; Golding, BT; Newell,; Northen, JS; Curtin, Nicola J.; Thomas, HD; Griffin, RJ

doi:10.1021/jm101493z

Cited by 15 publications

(12 citation statements)

References 29 publications

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“…Already in the 1980s and 1990s, the vasodilators dipyridamole and dilazep were identified to inhibit nucleoside transport via targeting hENT1 and, however less potent, hENT2 ( Figure 2 A,D) [ 56 , 57 , 58 ]. Even though targeting nucleoside uptake in combination with other cytotoxic agents was thought to be a promising anti-cancer strategy, clinical phase I studies did not show the desired efficacy, and targeting nucleoside uptake moved out of the focus [ 59 , 60 , 61 , 62 , 63 , 64 ]. Only recently, the potential of dipyridamole to reduce triple-negative breast cancer progression and metastasis in xenograft models was uncovered, which has to be further evaluated in clinical trials [ 65 ].…”

Section: Pyrimidine Salvage As Target In Cancer Therapymentioning

confidence: 99%

“…The failure of dipyridamole in the clinics can be explained by its observed binding to serum protein α 1 -acid glycoprotein (AGP) causing insufficient target engagement and, therefore, the low response rate in vivo as well as in cancer patients [ 63 , 64 ]. To overcome the observed limitations, new chemically optimized hENT1 and hENT2 inhibitors were developed and identified.…”

Section: Pyrimidine Salvage As Target In Cancer Therapymentioning

confidence: 99%

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Re-Discovery of Pyrimidine Salvage as Target in Cancer Therapy

Walter

Herr

2022

Cells

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Nucleotides are synthesized through two distinct pathways: de novo synthesis and nucleoside salvage. Whereas the de novo pathway synthesizes nucleotides from amino acids and glucose, the salvage pathway recovers nucleosides or bases formed during DNA or RNA degradation. In contrast to high proliferating non-malignant cells, which are highly dependent on the de novo synthesis, cancer cells can switch to the nucleoside salvage pathways to maintain efficient DNA replication. Pyrimidine de novo synthesis remains the target of interest in cancer therapy and several inhibitors showed promising results in cancer cells and in vivo models. In the 1980s and 1990s, poor responses were however observed in clinical trials with several of the currently existing pyrimidine synthesis inhibitors. To overcome the observed limitations in clinical trials, targeting pyrimidine salvage alone or in combination with pyrimidine de novo inhibitors was suggested. Even though this approach showed initially promising results, it received fresh attention only recently. Here we discuss the re-discovery of targeting pyrimidine salvage pathways for DNA replication alone or in combination with inhibitors of pyrimidine de novo synthesis to overcome limitations of commonly used antimetabolites in various preclinical cancer models and clinical trials. We also highlight newly emerged targets in pyrimidine synthesis as well as pyrimidine salvage as a promising target in immunotherapy.

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Section: Pyrimidine Salvage As Target In Cancer Therapymentioning

confidence: 99%

Section: Pyrimidine Salvage As Target In Cancer Therapymentioning

confidence: 99%

Re-Discovery of Pyrimidine Salvage as Target in Cancer Therapy

Walter

Herr

2022

Cells

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“…随着人们对该类化合物的深入研究, 发现一些杂环稠合的嘧啶酮衍生物同样具备出色的生物活性, 如吡喃并 [2,3-d]嘧啶酮衍生物可用作降血压药物 [7] 、抗血小板药物 [8] 、抗癌药物 [9] 、抗疟疾药物 [10] 、抗微生物药物 [11] 、神经肽感受器良好的拮抗剂 [12] 等. 因此, 探索合成新颖…”

Section: 嘧啶酮衍生物是一类具有良好生物和药理unclassified

A Convenient Method to Prepare Pyrano[2,3-d]pyrimidine Derivatives

林志兰¹,

张俊民²,

高原³

2016

Chin. J. Org. Chem.

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A series of pyrano [2,3-d]pyrimidine derivatives were synthesized by the reaction of 2-amino-3-cyano-4H-pyrans with acetic anhydride. This method has the advantages of short reaction times (10～15 min), simple operation and convenient post-treatment. All products were fully characterized by IR and 1 H NMR spectra. The molecular structures of 4a and 6a were confirmed using single-crystal X-ray analyses.

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“…Studies suggest that DPM possesses beneficial properties within the endothelium of the vasculature in addition to its anti-platelet effects, including direct and indirect effects such as inhibition of proliferation, antioxidant and anti-inflammatory properties, and downstream effects on cell signaling (13). DPM was previously reported to increase the cytotoxicity of antimetabolites like pemetrexed on human cancer cells (14, 15). Our in vitro study of nucleoside transport inhibitors as chemopreventive agents has found that DPM shows chemopreventive activity in the JB6 cell tumor promotion model (our unpublished results).…”

Section: Introductionmentioning

confidence: 99%

Chemoprevention Activity of Dipyridamole in the MMTV-PyMT Transgenic Mouse Model of Breast Cancer

Wang

Schwab

Fan

et al. 2013

Cancer Prevention Research

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Dipyridamole (DPM) is widely used to prevent strokes and vascular thrombosis. Combination therapy of DPM and antimetabolites has shown synergistic anticancer activity. This study investigated the chemopreventive effects of DPM in the mouse mammary tumor virus promoter driven polyoma middle T oncoprotein (MMTV-PyMT) metastatic breast cancer model. We also investigated the effects of DPM on gene and miRNA expression. Chemopreventive activity was assessed by comparing the time to onset of palpable lesions, primary tumor growth kinetics and the number of lung metastases in transgenic mice treated with DPM or vehicle. Gene expression and microRNA (miRNA) expression profiles of mammary tumor tissues were then analyzed using the Affymetrix GeneChip® or miRNA 2.0 arrays. Real-time quantitative PCR (qPCR) was used to confirm changes in gene expression. Treatment with DPM beginning at the age of four weeks delayed the onset of palpable lesions, delayed tumor progression and suppressed lung metastasis. Microarray gene expression analysis identified 253 genes differentially expressed between DPM-treated and control mammary tumors. miRNA expression analysis revealed that 53 miRNAs were altered by DPM treatment. The results indicate that DPM has chemoprevention activity against breast cancer tumorigenesis and metastasis in mice. The array analyses provide insights into potential mechanisms of DPM’s chemopreventive effects, involving upregulation of several genes and miRNAs known to suppress cancer growth and/or metastasis and downregulation of genes known to promote cancer. Some of these genes have not been previously studied in breast cancer and may serve as novel molecular targets for breast cancer chemoprevention.

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Nucleoside Transport Inhibitors: Structure−Activity Relationships for Pyrimido[5,4-d]pyrimidine Derivatives That Potentiate Pemetrexed Cytotoxicity in the Presence of α₁-Acid Glycoprotein

Cited by 15 publications

References 29 publications

Re-Discovery of Pyrimidine Salvage as Target in Cancer Therapy

Re-Discovery of Pyrimidine Salvage as Target in Cancer Therapy

A Convenient Method to Prepare Pyrano[2,3-d]pyrimidine Derivatives

Chemoprevention Activity of Dipyridamole in the MMTV-PyMT Transgenic Mouse Model of Breast Cancer

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Nucleoside Transport Inhibitors: Structure−Activity Relationships for Pyrimido[5,4-d]pyrimidine Derivatives That Potentiate Pemetrexed Cytotoxicity in the Presence of α1-Acid Glycoprotein

Cited by 15 publications

References 29 publications

Re-Discovery of Pyrimidine Salvage as Target in Cancer Therapy

Re-Discovery of Pyrimidine Salvage as Target in Cancer Therapy

A Convenient Method to Prepare Pyrano[2,3-d]pyrimidine Derivatives

Chemoprevention Activity of Dipyridamole in the MMTV-PyMT Transgenic Mouse Model of Breast Cancer

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Product

Resources

About

Nucleoside Transport Inhibitors: Structure−Activity Relationships for Pyrimido[5,4-d]pyrimidine Derivatives That Potentiate Pemetrexed Cytotoxicity in the Presence of α₁-Acid Glycoprotein