Amino Acid Depletion Therapies: Starving Cancer Cells to Death

Butler, Miriam; Meer, Laurens T. van der; Leeuwen, Frank N. van

doi:10.1016/j.tem.2021.03.003

Cited by 155 publications

(145 citation statements)

References 107 publications

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“…The most common approach targeting amino acid metabolism is the pharmacological suppression of metabolic enzymes that are increased in drug-resistant cancer cells [ 5 , 6 ]. Moreover, the use of modified dietary interventions together with conventional cancer therapy is an approach receiving growing attention owing to its limited toxicity [ 9 , 148 ]. Alteration of the environmental amino acid levels around tumors considerably impacts not only the metabolism of cancer cells but also surrounding cells, including immune and stromal cells, resulting in altered drug sensitivity.…”

Section: Discussionmentioning

confidence: 99%

“…In addition, intercellular or subcellular transportation of amino acids and altered metabolism induced by overexpression of amino acid transporters support cancer cell metabolism overcoming drug-induced stress [ 7 , 8 ]. Growing evidence indicates that suppressing or enhancing amino acid metabolism and depletion or supplementation of amino acid availability is effective in abolishing drug resistance in cancer cells [ 9 , 10 ].…”

Section: Introductionmentioning

confidence: 99%

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Amino Acid Metabolism in Cancer Drug Resistance

Yoo

Han

2022

Cells

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Despite the numerous investigations on resistance mechanisms, drug resistance in cancer therapies still limits favorable outcomes in cancer patients. The complexities of the inherent characteristics of tumors, such as tumor heterogeneity and the complicated interaction within the tumor microenvironment, still hinder efforts to overcome drug resistance in cancer cells, requiring innovative approaches. In this review, we describe recent studies offering evidence for the essential roles of amino acid metabolism in driving drug resistance in cancer cells. Amino acids support cancer cells in counteracting therapies by maintaining redox homeostasis, sustaining biosynthetic processes, regulating epigenetic modification, and providing metabolic intermediates for energy generation. In addition, amino acid metabolism impacts anticancer immune responses, creating an immunosuppressive or immunoeffective microenvironment. A comprehensive understanding of amino acid metabolism as it relates to therapeutic resistance mechanisms will improve anticancer therapeutic strategies.

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Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Amino Acid Metabolism in Cancer Drug Resistance

Yoo

Han

2022

Cells

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“…Consequently, depleting arginine through arginase (ARGase, converting arginine into ornithine and urea) or arginine deiminase (ADI, converting arginine into citrulline and NH 3 ) shows great potential in triggering cell death or reducing tumor growth in various cancer types including nonsmall cell lung cancer, glioblastoma, bladder cancer, pancreatic cancer, liver cancer, leukemia and melanoma (11,(16)(17)(18)(19)(20)(21). However, the anti-cancer effects haven't reached our expectation when using ARGase treatment for cancer patients, possibly due to limited efficacy of ARGase in vivo or compensatory arginine supply from amino acids-related salvage pathways (9). Alternatively, ADI treatment-mediated arginine deprivation exhibits acceptable tolerance and has been brought into clinical trials in several types of cancers (22,23), encouraging persistent dedication to deeply exploring the applications of targeting arginine dependency in cancer treatment.…”

Section: Argininementioning

confidence: 99%

“…Under certain circumstances, like genetic mutations, alterations of metabolic gene expression and limitations of nutrient supply in the tumor environment, tumor cells exhibit relatively high addition to one particular nutrient, which creates nutrient dependency that could be therapeutically targeted in cancer treatment (4)(5)(6). Thus, restricting nutrient availability by various means such as dietary approaches and amino acids degrading enzymes causes growth arrest, cell death and, partly, if not all, tumor suppression, which acts as an anti-cancer strategy and is definitely worth further study (7)(8)(9). In addition, nutrient availability also affects numerous cell types within tumor microenvironment and malignant cells undergo many challenges as well as compensations from other types of cells in the context, which is assumed as heterocellular metabolic interactions that impede our precise understanding of tumor metabolism (10).…”

mentioning

confidence: 99%

“…Interfering with nutrient availability can be secretively lethal to tumor cells, which serves as a cancer-specific Achilles' heel. To date, selective dependencies of tumor cells on amino acids such as asparagine, arginine, methionine, glutamine and cysteine, or the major energy source glucose have been wildly documented, although the underlying mechanisms vary and are highly context dependent (9). How do genetic mutations influence metabolic fluxes?…”

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confidence: 99%

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Targeting Nutrient Dependency in Cancer Treatment

Fan

Li²,

Gao

et al. 2022

Front. Oncol.

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Metabolic reprogramming is one of the hallmarks of tumor. Growing evidence suggests metabolic changes that support oncogenic progression may cause selective vulnerabilities that can be exploited for cancer treatment. Increasing demands for certain nutrients under genetic determination or environmental challenge enhance dependency of tumor cells on specific nutrient, which could be therapeutically developed through targeting such nutrient dependency. Various nutrients including several amino acids and glucose have been found to induce dependency in genetic alteration- or context-dependent manners. In this review, we discuss the extensively studied nutrient dependency and the biological mechanisms behind such vulnerabilities. Besides, existing applications and strategies to target nutrient dependency in different cancer types, accompanied with remaining challenges to further exploit these metabolic vulnerabilities to improve cancer therapies, are reviewed.

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Enzalutamide Sensitizes Castration‐Resistant Prostate Cancer to Copper‐Mediated Cell Death

Gao,

Zhao,

Liu

et al. 2024

Advanced Science

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Despite the initial efficacy of enzalutamide in castration‐resistant prostate cancer (CRPC), inevitable resistance remains a significant challenge. Here, the synergistic induction of copper‐dependent cell death (cuproptosis) in CRPC cells is reported by enzalutamide and copper ionophores (elesclomol/disulfiram). Mechanistically, enzalutamide treatment increases mitochondrial dependence in CRPC cells, rendering them susceptible to cuproptosis, as evidenced by specific reversal with the copper chelator tetrathiomolybdate. This susceptibility is characterized by hallmarks of cuproptosis, including lipoylated protein aggregation and iron‐sulfur cluster protein instability. Interestingly, the mitochondrial matrix reductase, FDX1, specifically correlates with elesclomol sensitivity, suggesting a potential mechanistic divergence between the two copper ionophores. Notably, this synergistic effect extends beyond in vitro models, demonstrating efficacy in 22Rv1 xenografts, mouse Pten p53 knockout organoids. Importantly, enzalutamide significantly enhances copper ionophore‐mediated cytotoxicity in enzalutamide‐resistant cells. Collectively, these findings indicate that enzalutamide and copper ionophores synergistically induce cuproptosis, offering a promising therapeutic avenue for CRPC, potentially including enzalutamide‐resistant cases.

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Amino Acid Depletion Therapies: Starving Cancer Cells to Death

Cited by 155 publications

References 107 publications

Amino Acid Metabolism in Cancer Drug Resistance

Amino Acid Metabolism in Cancer Drug Resistance

Targeting Nutrient Dependency in Cancer Treatment

Enzalutamide Sensitizes Castration‐Resistant Prostate Cancer to Copper‐Mediated Cell Death

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