An Interplay between Senescence, Apoptosis and Autophagy in Glioblastoma Multiforme—Role in Pathogenesis and Therapeutic Perspective

Pawłowska, Elżbieta; Szczepańska, Joanna; Szatkowska, Magdalena; Błasiak, Janusz

doi:10.3390/ijms19030889

Cited by 74 publications

(60 citation statements)

References 120 publications

(134 reference statements)

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“…LN229 was used as model for aggressive, autophagy‐prone malignant GBM, whereas MCF‐7 was selected for consistency with our previous studies . We aimed at supporting the observations made from in vitro colorimetric assays, concerning the effects of the conjugation with a quinoline residue of the ruthenacarborane fragment on proliferation, survival and death mechanisms of the selected cell lines.…”

Section: Resultsmentioning

confidence: 96%

“…Thus, 4 acts in vitro as a hybrid molecule against malignant glioblastoma cells (LN229), inhibiting cellular division and, in parallel, cytoprotective autophagy, which supports the rational drug design idea of this work. It is obvious from the recent literature that modulation of autophagy is an attractive therapeutic approach for treatment of GBM, for inducing (re)sensitization to cytotoxic or cytostatic drugs . It needs to be said that a full elucidation of the cause‐effect relationship between autophagy and cancer cells survival or death would be a very ambitious scope at this point.…”

Section: Resultsmentioning

confidence: 99%

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Quinoline‐Conjugated Ruthenacarboranes: Toward Hybrid Drugs with a Dual Mode of Action

et al. 2019

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The role of autophagy in cancer is often complex, ranging from tumor-promoting to -suppressing effects. In this study, two novel hybrid molecules were designed, containing a ruthenacarborane fragment conjugated with a known modulator of autophagy, namely a quinoline derivative. The complex closo-[3-(η 6 -p-cymene)-1-(quinolin-8-yl-acetate)-3,1,2-RuC 2 B 9 H 10 ](4) showed a dual mode of action against the LN229 (human glioblastoma) cell line, where it inhibited tumor-promoting autophagy, and strongly inhibited cell proliferation, de facto blocking cellular division. These results, together with the tendency to spontaneously form nanoparticles in aqueous solution, make complex 4 a very promising drug candidate for further studies in vivo, for the treatment of autophagy-prone glioblastomas. [a] Dr. . Results from flow cytometric and fluorescence microscopy analysis, and wound healing assay of MCF-7 cells incubated (72 h) with 3 and 4 at 20 μM. (A) CFSE staining (left panel) and wound healing assay (right panel); (B) AnnV/PI double staining; (C) DAPI-stained cells observed under fluorescence microscope (magnification X200). Arrows indicate apoptotic cells; (D) ApoStat staining; (E) AO staining. Experiments were run in triplicate. One representative example per each experiment is shown. For each staining protocol, the respective control (untreated cells) is also shown. (FL1, green channel; FL2, orange channel; FL3, dark red channel).

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Section: Resultsmentioning

confidence: 96%

Section: Resultsmentioning

confidence: 99%

Quinoline‐Conjugated Ruthenacarboranes: Toward Hybrid Drugs with a Dual Mode of Action

et al. 2019

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“…Several studies demonstrate the efficacy of resveratrol in lowering tumorigenesis and preventing metastasis [23,89,90]. Resveratrol has a powerful capability of down-regulating the self-renewal and tumor-initiating capability of glioma stem cells obtained from GBM patients by inducing the p53/ p21 pathway [91].…”

Section: Resveratrol Effects On Central Nervous System Cancersmentioning

confidence: 99%

Bioactive Phenolic Compounds in the Modulation of Central and Peripheral Nervous System Cancers: Facts and Misdeeds

Perrone

Sampaolo

Melone

2020

Cancers

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Efficacious therapies are not available for the cure of both gliomas and glioneuronal tumors, which represent the most numerous and heterogeneous primary cancers of the central nervous system (CNS), and for neoplasms of the peripheral nervous system (PNS), which can be divided into benign tumors, mainly represented by schwannomas and neurofibromas, and malignant tumors of the peripheral nerve sheath (MPNST). Increased cellular oxidative stress and other metabolic aspects have been reported as potential etiologies in the nervous system tumors. Thus polyphenols have been tested as effective natural compounds likely useful for the prevention and therapy of this group of neoplasms, because of their antioxidant and anti-inflammatory activity. However, polyphenols show poor intestinal absorption due to individual intestinal microbiota content, poor bioavailability, and difficulty in passing the blood–brain barrier (BBB). Recently, polymeric nanoparticle-based polyphenol delivery improved their gastrointestinal absorption, their bioavailability, and entry into defined target organs. Herein, we summarize recent findings about the primary polyphenols employed for nervous system tumor prevention and treatment. We describe the limitations of their application in clinical practice and the new strategies aimed at enhancing their bioavailability and targeted delivery.

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“…DNA-PK CS inhibition increased cell death in glioblastoma cells by the disruption of NHEJ and the sensitization of exposed cells to telomerase inhibitors (103). Strikingly, the inhibition of DNA-PK CS sensitized glioma cells to irradiation by inhibiting autophagy, supporting the theory of autophagy-mediated irradiation resistance and the dependence of HGG cells on autophagy (104,105).…”

Section: The Dna Damage Responsementioning

confidence: 65%

Modulating autophagy as a therapeutic strategy for the treatment of paediatric high‐grade glioma

et al. 2019

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Paediatric high‐grade gliomas (pHGG) represent a therapeutically challenging group of tumors. Despite decades of research, there has been minimal improvement in treatment and the clinical prognosis remains poor. Autophagy, a highly conserved process for recycling metabolic substrates is upregulated in pHGG, promoting tumor progression and evading cell death. There is significant crosstalk between autophagy and a plethora of critical cellular pathways, many of which are dysregulated in pHGG. The following article will discuss our current understanding of autophagy signaling in pHGG and the potential modulation of this network as a therapeutic target.

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An Interplay between Senescence, Apoptosis and Autophagy in Glioblastoma Multiforme—Role in Pathogenesis and Therapeutic Perspective

Cited by 74 publications

References 120 publications

Quinoline‐Conjugated Ruthenacarboranes: Toward Hybrid Drugs with a Dual Mode of Action

Quinoline‐Conjugated Ruthenacarboranes: Toward Hybrid Drugs with a Dual Mode of Action

Bioactive Phenolic Compounds in the Modulation of Central and Peripheral Nervous System Cancers: Facts and Misdeeds

Modulating autophagy as a therapeutic strategy for the treatment of paediatric high‐grade glioma

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