Statins: a repurposed drug to fight cancer

Jiang, Wen Qi; Hu, Jin Wei; He, Xu; Jin, Wei; He, Xin

doi:10.1186/s13046-021-02041-2

Cited by 200 publications

(185 citation statements)

References 313 publications

(269 reference statements)

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“…Co-targeting of Wee1 and the DNA damage response kinase ATM was shown to downregulate PD-L1 expression in pancreatic cancer ( 15 ). Wee1 inhibition was found to sensitize cancer cells to immunotherapy via PD-1 checkpoint blockade in oral cavity carcinoma, melanoma and colon adenocarcinoma with variable Tp53 mutations, which provide a pre-clinical rationale for the combination of agents that target cell cycle checkpoints and activate anti-tumor immunity and simultaneously support the clinical trials of Wee1 inhibitor in combination with immunotherapy ( 16 ). The effect of the combination of Wee1 inhibitor ZN-c3 with PD1 inhibitor Pembrolizumab will also be studied in patients with solid tumors with advanced or metastatic disease at the clinical trial NCT04158336.…”

Section: Wee1 Inhibitorsmentioning

confidence: 97%

“…It was later determined that knockout of mevalonate kinase (MVK) has the same effect as reducing mevalonate 5-phosphate, suggesting that the disruption of mutp53 functions may be brought about through targeting and manipulating different parts of the mevalonate pathway ( 18 ). In addition to its effects on mevalonate 5-phosphate, statins inhibit HMG-CoA (HMGCR) reductase activity, which mediates the synthesis of cholesterol and the inhibition of the biosynthesis of selenoproteins (such as GPX4) and CoQ10, and thus enhance ferroptosis ( 11 , 16 , 17 ). Several groups have reported that Hsp90, Hsp40, CHIP and MDM2 play critical roles to stabilize mutant p53 via the HSP chaperone system, which suggests a possible synergism between HSP chaperone system inhibitors and statins in tandem ( 22 , 24 , 25 , 30 ).…”

Section: Mutant P53 and Mevalonate Pathwaymentioning

confidence: 99%

“…Mevalonate-5-phosphate (MVP) promotes mutp53 stabilization by increasing the interaction between mutp53 and KSP40/DNAJA1 and inhibiting CHIP-mediated ubiquitination and proteasomal degradation of mutp53 ( 11 ). The mevalonate pathway inhibition can also sensitize cancer cells to ferroptosis by depleting CoQ10 and the biosynthesis of GPX4 by inhibiting tRNA isopentenylation via TRIT1 ( 12 – 16 ). In cancers with GOF Mutp53, statins can inhibit tumor growth by inducing mutp53 degradation, inhibiting prenylation of oncogenes and cholesterol synthesis, as well as inducing ferroptosis by inhibiting the biosynthesis of GPX4 and CoQ10 ( 16 – 18 ).…”

Section: Introductionmentioning

confidence: 99%

“…The mevalonate pathway inhibition can also sensitize cancer cells to ferroptosis by depleting CoQ10 and the biosynthesis of GPX4 by inhibiting tRNA isopentenylation via TRIT1 ( 12 – 16 ). In cancers with GOF Mutp53, statins can inhibit tumor growth by inducing mutp53 degradation, inhibiting prenylation of oncogenes and cholesterol synthesis, as well as inducing ferroptosis by inhibiting the biosynthesis of GPX4 and CoQ10 ( 16 – 18 ). The function of Wee1, as well as the progress of Wee1 inhibitors, statins and effect on immunotherapy in cancer with p53 mutations, will thus be discussed.…”

Section: Introductionmentioning

confidence: 99%

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Recent Advances of WEE1 Inhibitors and Statins in Cancers With p53 Mutations

et al. 2021

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p53 is among the most frequently mutated tumor suppressor genes given its prevalence in >50% of all human cancers. One critical tumor suppression function of p53 is to regulate transcription of downstream genes and maintain genomic stability by inducing the G1/S checkpoint in response to DNA damage. Tumor cells lacking functional p53 are defective in the G1/S checkpoint and become highly dependent on the G2/M checkpoint to maintain genomic stability and are consequently vulnerable to Wee1 inhibitors, which override the cell cycle G2/M checkpoint and induce cell death through mitotic catastrophe. In addition to the lost tumor suppression function, many mutated p53 (Mutp53) proteins acquire gain-of-function (GOF) activities as oncogenes to promote cancer progression, which manifest through aberrant expression of p53. In cancer cells with GOF Mutp53, statins can induce CHIP-mediated degradation of Mutp53 within the mevalonate pathway by blocking the interaction between mutp53 and DNAJA1. Therefore, targeting critical downstream pathways of Mutp53 provides an alternative strategy for treating cancers expressing Mutp53. In this review, we summarize recent advances with Wee1 inhibitors, statins, and mevalonate pathway inhibitors in cancers with p53 mutations.

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Section: Wee1 Inhibitorsmentioning

confidence: 97%

Section: Mutant P53 and Mevalonate Pathwaymentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Recent Advances of WEE1 Inhibitors and Statins in Cancers With p53 Mutations

et al. 2021

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“…An important observation of great importance for cancer therapy is that statins have an apoptotic effect mainly in the case of neoplastic cells. This means that statins are not destructive in normal cells, as is the case with most drugs used to treat cancer [23][24][25].…”

Section: Introductionmentioning

confidence: 96%

Mevastatin in colon cancer by spectroscopic and microscopic methods - Raman imaging and AFM studies

Beton

Wysocki

Brożek-Płuska

2021

Preprint

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One of the most important areas of medical science is oncology, which is responsible for both the diagnostics and treatment of cancer diseases. Simultaneously one of the main challenges of oncology is the development of modern drugs effective in the fight against cancer. Statins are a group of biologically active compounds with the activity of 3-hydroxy-3-methyl glutaryl-CoA reductase inhibitors, an enzyme catalyzing the reduction of 3-hydroxy-3-methyl-glutaryl-CoA (HMG-CoA) to mevalonic acid. By acting on this enzyme, statins inhibit the endogenous cholesterol synthesis which in turn causes the reduction of its systemic concentrations. However, in vitro and in vivo studies confirm also the cytostatic and cytotoxic effects of statins against various types of cancer cells including colon cancer. In the presented studies the influence of mevastatin on cancerous colon cells CaCo-2 by Raman spectroscopy and imaging is discussed and compared with biochemistry characteristic for normal colon cells CCD-18Co. Based on vibrational features of colon cells: normal cells CCD-18Co, cancerous cells CaCo-2 and cancerous cells CaCo-2 treated by mevastatin in different concentrations and incubation times we have confirm the influence of this statin on biochemistry composition of cancerous human colon cells. Moreover, the spectroscopic results for colon normal cells and cancerous cells based on data typical for nucleic acids, proteins, lipids have been compared. The cytotoxisity of mevastatin was determined by using XTT tests.

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Targeting ferroptosis for improved radiotherapy outcomes in HPV‐negative head and neck squamous cell carcinoma

Noh,

Lee,

Lee

et al. 2024

Molecular Oncology

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To enhance the efficacy of radiotherapy (RT) in human papillomavirus (HPV)‐negative head and neck squamous cell carcinoma (HNSCC), we explored targeting ferroptosis, a regulated cell death process. We developed a gene signature associated with ferroptosis using Cox proportional hazard modeling in HPV‐negative HNSCC patients who underwent RT. This ferroptosis‐related gene signature (FRGS) was a significant predictor of overall survival and recurrence‐free survival in HPV‐negative HNSCC patients who received RT. Subtype B of the FRGS, characterized by decreased expression of ferroptosis inducers [nuclear receptor coactivator 4 (NCOA4) and natural resistance‐associated macrophage protein 2 homolog/divalent metal transporter 1 (NRAMP2/DMT1)] and increased expression of suppressors [phospholipid hydroperoxide glutathione peroxidase (GPX4) and ferritin heavy chain (FTH1)], was associated with poorer prognosis, potentially indicating the inhibition of ferroptosis. Furthermore, our in vitro and in vivo studies demonstrated that treatment with statins, such as atorvastatin and simvastatin, induced ferroptosis and sensitized radioresistant HNSCC cells to irradiation, improving radiosensitivity and potentially enhancing the response to RT. Additionally, in xenograft models, the combination of statins and RT led to a significant reduction in tumor initiation. These findings provide valuable insights for enhancing treatment and improving prognosis in HPV‐negative HNSCC by targeting ferroptosis and utilizing statins to sensitize tumors to RT‐induced cell death.

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Statins: a repurposed drug to fight cancer

Cited by 200 publications

References 313 publications

Recent Advances of WEE1 Inhibitors and Statins in Cancers With p53 Mutations

Recent Advances of WEE1 Inhibitors and Statins in Cancers With p53 Mutations

Mevastatin in colon cancer by spectroscopic and microscopic methods - Raman imaging and AFM studies

Targeting ferroptosis for improved radiotherapy outcomes in HPV‐negative head and neck squamous cell carcinoma

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