ATR inhibition facilitates targeting of leukemia dependence on convergent nucleotide biosynthetic pathways

Le, Thuc; Poddar, Soumya; Capri, Joseph; Abt, Evan R.; Kim, Woosuk; Liu, Wei; Uong, Nhu T.; Cheng, Chloe; Braas, Daniel; Nikanjam, Mina; Rix, Peter J.; Merkurjev, Daria; Zaretsky, Jesse M.; Kornblum, Harley I.; Ribas, Antoni; Herschman, Harvey R.; Whitelegge, Julian P.; Faull, Kym F.; Donahue, Timothy R.; Czernin, Johannes; Radu, Caius G.

doi:10.1038/s41467-017-00221-3

Cited by 53 publications

(80 citation statements)

References 70 publications

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“…While previous reports have linked ATR signaling to nucleotide metabolism through upregulation of RRM2 protein stability (Le et al, 2017), our model suggests that ATR also modulates nucleotide metabolism through increasing mTORC1 signaling (Fig. 3).…”

Section: Discussionmentioning

confidence: 64%

Suppression of p16 induces mTORC1-mediated nucleotide metabolic reprogramming

Buj

Chen

Dahl

et al. 2018

Preprint

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2 SummaryReprogrammed metabolism and cell cycle dysregulation are two cancer hallmarks. p16 is a cell cycle inhibitor and tumor suppressor that is upregulated during oncogeneinduced senescence (OIS). Loss of p16 allows for uninhibited cell cycle progression, bypass of OIS, and tumorigenesis. Whether p16 loss affects pro-tumorigenic metabolism is unclear. We report that suppression of p16 plays a central role in

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Section: Discussionmentioning

confidence: 64%

Suppression of p16 induces mTORC1-mediated nucleotide metabolic reprogramming

Buj

Chen

Dahl

et al. 2018

Preprint

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“…Furthermore, dCK inactivation has also been associated with resistance to dG-mediated toxicity in PNP-deficient T-lymphoma cells 15 . We found that the lethality of PNP inhibitors be completely prevented by supplementing with a small molecule dCK inhibitor indicating that phosphorylation of dG by dGK does not contribute to the observed lethality at these timepoints ( Figure 2D) 4 .…”

Section: Samhd1-deficient Solid Tumor Models Are Sensitive To Pnp Inhmentioning

confidence: 90%

“…We found that SAMHD1 KO cells exhibited a 200-fold lower thymidine IC50 than SAMHD1 WT controls (Figure 5A). This selectivity was unique to thymidine and did not extend to other RNR inhibitors, including 3-AP, which function by preventing RNR tyrosyl radical regeneration 4 . Similar selectivity was observed using crystal violet proliferation analysis (Figure 5B).…”

Section: Samhd1 Prevents the Anti Proliferative Effects Of Thymidinementioning

confidence: 95%

“…A sufficient supply of deoxyribonucleotide triphosphates (dNTPs) is essential for cell growth, survival and proliferation 1,2 . Thus, the metabolic network that is responsible for the synthesis of dNTPs is tightly regulated by transcriptional, post-translational and allosteric control mechanisms 3,4 . Cancer cells are particularly reliant on dNTP biosynthesis and this non-oncogene addiction has been leveraged clinically by the use of small molecule inhibitors of rate-limiting metabolic enzymes including dihydroorotate dehydrogenase (DHODH), ribonucleotide reductase (RNR), dihydrofolate reductase (DHFR) and thymidylate synthase (TYMS) 5 .…”

Section: Introductionmentioning

confidence: 99%

“…Giblett and colleagues were among the first to identify that inactivating, inherited mutations in the nucleotide catabolic enzymes adenosine deaminase (ADA) and purine nucleoside phosphorylase (PNP) drive the development of SCID 8,9 . ADA and PNP function sequentially in the catabolism of purine deoxyribonucleosides dA and dG and counter their intracellular accumulation mediated by deoxycytidine kinase dCK 4 . For reasons not well understood defective dG catabolism results in remarkably selective T-cell defects, and otherwise normal cellular development, in individuals with PNP-linked SCID 10 .…”

Section: Introductionmentioning

confidence: 99%

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Defective Nucleotide Catabolism Defines a Subset of Cancers Sensitive to Purine Nucleoside Phosphorylase Inhibition

Abt

Lok

et al. 2019

Preprint

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2 Small molecule inhibitors of purine nucleoside phosphorylase (PNP) have been explored as a treatment strategy for leukemia and lymphoma, however, the determinants of response to this class of drugs are incompletely understood. PNP inhibitors impair cell proliferation by preventing catabolism of the nucleoside deoxyguanosine (dG) which induces toxic imbalances amongst intracellular deoxyribonucleotide triphosphate (dNTP) pools following its phosphorylation and trapping by nucleoside kinases. We hypothesized that differential nucleoside uptake or catabolism defines cancer cell lines as either sensitive or resistant to PNP inhibition. Among cancer cell lines we found that T-cell acute lymphoblastic leukemia (T-ALL) cells are uniquely and acutely sensitive to PNP inhibition whereas the B-cell leukemia and solid tumor models are completely resistant. We determined that although the nucleoside scavenging kinase deoxycytidine kinase (dCK) was active in all cells tested, PNP inhibitors only induced dGTP pool increases in sensitive models. By evaluating the expression of key genes involved in nucleotide scavenging, biosynthesis, and phosphohydrolysis in a panel of sensitive and resistant cell lines we found that the dNTP phosphohydrolase SAM histidine aspartate containing protein 1 (SAMHD1) was exclusively expressed in resistant models. Using CRISPR/Cas9 SAMHD1 knockout cell lines, we verified that PNP inhibitor sensitivity is a function of SAMHD1 expression and determined that the pharmacological inhibition of dCK or genetic restoration of SAMHD1 conferred resistance to PNP inhibition. Importantly, we determined that low expression of SAMHD1 is not limited to T-ALL as subset of established and primary solid tumors models are SAMHD1-deficient. These solid tumor models were consistently acutely sensitive to PNP inhibitors which indicates that the utility of PNP inhibitors extends beyond hematological malignancies. Additionally, we found that deoxycytidine (dC) can limit the anti-proliferative effects of PNP inhibitors by competing with dG for phosphorylation by dCK but this effect can be overcome by expression of dC-catabolizing gene cytidine deaminase (CDA). Collectively, these results indicate that SAMHD1, dCK and CDA are critical biomarkers that must be used to stratify patients in clinical trials evaluating pharmacological PNP inhibition.

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Programmable DNA Hydrogel Assisting Microcrystal Formulations for Sustained Locoregional Drug Delivery in Surgical Residual Tumor Lesions and Lymph Node Metastasis

Zhang,

Zhou,

Tong

et al. 2023

Adv Healthcare Materials

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Surgical residual tumor lesions (R1 resection of surgical procedures (e.g., liver cancer infiltrating the diaphragm, surgical residual breast cancer, postoperative residual ovarian cancer) or boundary residual after ablation) and lymph node metastasis that cannot be surgically resected (retroperitoneal lymph nodes) significantly affect postoperative survival of tumor patients. This clinical conundrum poses three challenges for local drug delivery systems: stable and continuous delivery, good biocompatibility, and the ability to package new targeted drugs that can synergize with other treatments. Here, a drug‐laden hydrogel generated from pure DNA strands and highly programmable in adjusting its mesh size is reported. Meanwhile, the DNA hydrogel can assist the microcrystallization of novel radiosensitizing drugs, ataxia telangiectasia and rad3‐related protein (ATR) inhibitor (Elimusertib), further facilitating its long‐term release. When applied to the tumor site, the hydrogel system demonstrates significant antitumor activity, minimized systemic toxicity, and has a modulatory effect on the tumor‐immune cell interface. This drug‐loaded DNA‐hydrogel platform represents a novel modality for adjuvant therapy in patients with surgical residual tumor lesions and lymph node metastasis.

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ATR inhibition facilitates targeting of leukemia dependence on convergent nucleotide biosynthetic pathways

Cited by 53 publications

References 70 publications

Suppression of p16 induces mTORC1-mediated nucleotide metabolic reprogramming

Suppression of p16 induces mTORC1-mediated nucleotide metabolic reprogramming

Defective Nucleotide Catabolism Defines a Subset of Cancers Sensitive to Purine Nucleoside Phosphorylase Inhibition

Programmable DNA Hydrogel Assisting Microcrystal Formulations for Sustained Locoregional Drug Delivery in Surgical Residual Tumor Lesions and Lymph Node Metastasis

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