Attacking the supply wagons to starve cancer cells to death

Selwan, Elizabeth; Finicle, Brendan T.; Kim, Seong M.; Edinger, Aimee L.

doi:10.1002/1873-3468.12121

Cited by 67 publications

(64 citation statements)

References 231 publications

(309 reference statements)

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“…Our results showed that SRPK2 inhibition with lipid deprivation inhibits cancer cell proliferation (Figure 7). Therefore, combination therapies using specific SRPK2 inhibitors and lipid uptake blockers such as CD36 antibodies (Pascual et al, 2016; Selwan et al, 2016) would also be a promising regimen for treatment of cancers with high dependency on mTORC1 signaling and lipid metabolism.…”

Section: Discussionmentioning

confidence: 99%

Post-transcriptional Regulation of De Novo Lipogenesis by mTORC1-S6K1-SRPK2 Signaling

Lee

Zheng

Cho

et al. 2017

Cell

171

156

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Summary mTORC1 is a signal integrator and master regulator of cellular anabolic processes linked to cell growth and survival. Here we demonstrate that mTORC1 promotes lipid biogenesis via SRPK2, a key regulator of RNA-binding SR proteins. mTORC1-activated S6K1 phosphorylates SRPK2 at Ser494, which primes Ser497 phosphorylation by CK1. These phosphorylation events promote SRPK2 nuclear translocation and phosphorylation of SR proteins. Genome-wide transcriptome analysis reveals that lipid biosynthetic enzymes are among the downstream targets of mTORC1-SRPK2 signaling. Mechanistically, SRPK2 promotes SR protein binding to U1-70k to induce splicing of lipogenic pre-mRNAs. Inhibition of this signaling pathway leads to intron retention of lipogenic genes which triggers nonsense-mediated mRNA decay. Genetic or pharmacological inhibition of SRPK2 blunts de novo lipid synthesis, thereby suppressing cell growth. These results thus reveal a novel role of mTORC1-SRPK2 signaling in post-transcriptional regulation of lipid metabolism and demonstrate that SRPK2 is a potential therapeutic target for mTORC1-driven metabolic disorders.

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Section: Discussionmentioning

confidence: 99%

Post-transcriptional Regulation of De Novo Lipogenesis by mTORC1-S6K1-SRPK2 Signaling

Lee

Zheng

Cho

et al. 2017

Cell

171

156

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“…How SH-BC-893 administration affects whole-body metabolism and cytokine levels merits further investigation. As a single agent, SH-BC-893 acts like a combination therapy by targeting the multiple nutrient acquisition pathways that fuel cancer anabolism (17). It will be important to test whether pairing SH-BC-893 with drugs that target oncogenic signal transduction pathways will increase efficacy.…”

Section: Discussionmentioning

confidence: 99%

“…The following antibodies were used: murine 4F2HC (catalog 128208; eBioscience) and LAMP1 (catalog 53-1079-42; eBioscience); human 4F2HC (catalog 556077; BD Biosciences); human GLUT1 (catalog NB300-666; Novus Biologicals); LC3 (catalog 4108; Cell Signaling Technology); PIKfyve (catalog 4082; Tocris); VAC14 (catalog SAB4200074; Sigma-Aldrich); and WIPI2 (catalog LS-C154557-100; LifeSpan Biosciences). Colocalization was determined using the JACoP plugin in ImageJ software (NIH (17). The development of resistance limits the effectiveness of targeted therapies.…”

Section: Discussionmentioning

confidence: 99%

“…Cells adapt to nutrient stress by increasing autophagic flux (17). However, autophagosome-lysosome fusion reactions depend upon Ca 2+ released through TRPML1 channels that are activated or SH-BC-893-treated cells.…”

Section: 9mentioning

confidence: 99%

“…The identification of compounds with good pharmacological properties that restrict access to multiple nutrients presents a significant challenge (17). Sphingolipids offer a promising alternative to competitive inhibitors of individual nutrient uptake pathways.…”

Section: Introductionmentioning

confidence: 99%

See 2 more Smart Citations

Targeting cancer metabolism by simultaneously disrupting parallel nutrient access pathways

Kim

Roy

Chen

et al. 2016

Journal of Clinical Investigation

Self Cite

138

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Porous Pt Nanospheres Incorporated with GOx to Enable Synergistic Oxygen‐Inductive Starvation/Electrodynamic Tumor Therapy

et al. 2020

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Glucose‐oxidase (GOx)‐mediated starvation by consuming intracellular glucose has aroused extensive exploration as an advanced approach for tumor treatment. However, this reaction of catalytic oxidation by GOx is highly dependent on the on‐site oxygen content, and thus starvation therapy often suffers unexpected anticancer outcomes due to the intrinsic tumorous hypoxia. Herein, porous platinum nanospheres (pPts), incorporated with GOx molecules (PtGs), are synthesized to enable synergistic cancer therapy. In this system, GOx can effectively catalyze the oxidation of glucose to generate H2O2, while pPt triggers the decomposition of both endogenous and exogenous H2O2 to produce considerable content of O2 to facilitate the glucose consumption by GOx. Meanwhile, pPt induces remarkable content of intracellular reactive oxygen species (ROS) under an alternating electric field, leading to cellular oxidative stress injury and promotes apoptosis following the mechanism of electrodynamic therapy (EDT). In consequence, the PtG nanocomposite exhibits significant anticancer effect both in vitro and in vivo. This study has therefore demonstrated a fascinating therapeutic platform enabling oxygen‐inductive starvation/EDT synergistic strategy for effective tumor treatment.

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Attacking the supply wagons to starve cancer cells to death

Cited by 67 publications

References 231 publications

Post-transcriptional Regulation of De Novo Lipogenesis by mTORC1-S6K1-SRPK2 Signaling

Post-transcriptional Regulation of De Novo Lipogenesis by mTORC1-S6K1-SRPK2 Signaling

Targeting cancer metabolism by simultaneously disrupting parallel nutrient access pathways

Porous Pt Nanospheres Incorporated with GOx to Enable Synergistic Oxygen‐Inductive Starvation/Electrodynamic Tumor Therapy

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