Combined EGFR and Autophagy Modulation Impairs Cell Migration and Enhances Radiosensitivity in Human Glioblastoma Cells

Palumbo, Silvia; Tini, Paolo; Toscano, Marzia; Allavena, Giulia; Angeletti, Francesca; Manai, Federico; Miracco, Clelia; Comincini, Sergio; Pirtoli, Luigi

doi:10.1002/jcp.24640

Cited by 44 publications

(38 citation statements)

References 45 publications

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“…Autophagy is a double-edged sword in tumour progression and treatment: it can either facilitate cancer survival under metabolic stress or induce autophagic tumour cell death [35,36]. Mounting evidence accumulated in recent years suggests that inhibition of autophagy can reduce the treatment resistance of chemotherapy and radiotherapy in various types of cancers [37,38], which is also the case in GBM treatment [39,40]. To clarify the role of autophagy in peiminine therapy for GBM, LN229 and U251 cells were observed under TEM after peiminine treatment (Fig.…”

Section: Discussionmentioning

confidence: 99%

Peiminine Inhibits Glioblastoma in Vitro and in Vivo Through Cell Cycle Arrest and Autophagic Flux Blocking

Zhao¹,

Shen²,

Zheng³

et al. 2018

Cell Physiol Biochem

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Background/Aims: Glioblastoma multiforme (GBM) is the most devastating and widespread primary central nervous system tumour in adults, with poor survival rate and high mortality rates. Existing treatments do not provide substantial benefits to patients; therefore, novel treatment strategies are required. Peiminine, a natural bioactive compound extracted from the traditional Chinese medicine Fritillaria thunbergii, has many pharmacological effects, especially anticancer activities. However, its anticancer effects on GBM and the underlying mechanism have not been demonstrated. This study was conducted to investigate the potential antitumour effects of peiminine in human GBM cells and to explore the related molecular signalling mechanisms in vitro and in vivo Methods: Cell viability and proliferation were detected with MTT and colony formation assays. Morphological changes associated with autophagy were assessed by transmission electron microscopy (TEM). The cell cycle rate was measured by flow cytometry. To detect changes in related genes and signalling pathways in vitro and in vivo, RNA-seq, Western blotting and immunohistochemical analyses were employed. Results: Peiminine significantly inhibited the proliferation and colony formation of GBM cells and resulted in changes in many tumour-related genes and transcriptional products. The potential anti-GBM role of peiminine might involve cell cycle arrest and autophagic flux blocking via changes in expression of the cyclin D1/CDK network, p62 and LC3. Changes in Changes in flow cytometry results and TEM findings were also observed. Molecular alterations included downregulation of the expression of not only phospho-Akt and phospho-GSK3β but also phospho-AMPK and phospho-ULK1. Furthermore, overexpression of AKT and inhibition of AKT reversed and augmented peiminine-induced cell cycle arrest in GBM cells, respectively. The cellular activation of AMPK reversed the changes in the levels of protein markers of autophagic flux. These results demonstrated that peiminine mediates cell cycle arrest by suppressing AktGSk3β signalling and blocks autophagic flux by depressing AMPK-ULK1 signalling in GBM cells. Finally, peiminine inhibited the growth of U251 gliomas in vivo. Conclusion: Peiminine inhibits glioblastoma in vitro and in vivo via arresting the cell cycle and blocking autophagic flux, suggesting new avenues for GBM therapy.

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Section: Discussionmentioning

confidence: 99%

Peiminine Inhibits Glioblastoma in Vitro and in Vivo Through Cell Cycle Arrest and Autophagic Flux Blocking

Zhao¹,

Shen²,

Zheng³

et al. 2018

Cell Physiol Biochem

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“…Indeed, autophagy can positively or negatively regulate both GBM invasion and resistance to therapy, the two hallmarks of GBM aggressiveness. 85 Concerning invasion and cell motility, whereas Catalano et al 86 reported an impairment of migration and invasion of GBM cells after autophagy induction, Palumbo et al 87 noticed this impairment after autophagy inhibition, especially when EGFR was coinhibited, thus highlighting the importance of growth factor signaling.…”

Section: Autophagy and Gbmmentioning

confidence: 99%

Glioblastoma, hypoxia and autophagy: a survival-prone ‘ménage-à-trois’

2016

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Glioblastoma multiforme is the most common and the most aggressive primary brain tumor. It is characterized by a high degree of hypoxia and also by a remarkable resistance to therapy because of its adaptation capabilities that include autophagy. This degradation process allows the recycling of cellular components, leading to the formation of metabolic precursors and production of adenosine triphosphate. Hypoxia can induce autophagy through the activation of several autophagy-related proteins such as BNIP3, AMPK, REDD1, PML, and the unfolded protein response-related transcription factors ATF4 and CHOP. This review summarizes the most recent data about induction of autophagy under hypoxic condition and the role of autophagy in glioblastoma.

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“…A study by Lomonaco et al 33 provided evidence that inhibition of autophagy enhanced CD133+ glioblastoma stem cell sensitivity to ionizing radiation after bafilomycin treatment or Atg5 silencing. Notably, Palumbo et al 30 found that Atg7 silencing resulted in reduced T98 cell sensitivity to radiation and to a combination of radiation with anti-EGFR therapy 34 , indicating a complex role of different Atgs in radiation response. …”

Section: Discussionmentioning

confidence: 99%

Autophagic flux response and glioblastoma sensitivity to radiation

Mitrakas¹,

Kalamida²,

Giatromanolaki

et al. 2018

Cancer Biology & Medicine

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Objective:Glioblastoma is the most common primary brain tumor in adults and one of the most lethal human tumors. It constitutes a unique non-metastasizing human tumor model with high resistance to radiotherapy and chemotherapy. The current study investigates the association between autophagic flux and glioblastoma cell resistance.Methods:The expression kinetics of autophagy- and lysosome-related proteins following exposure of two glioblastoma cell lines (T98 and U87) to clinically relevant radiation doses was examined. Then, the response of cells resistant to radiotherapy and chemotherapy was investigated after silencing of LC3A, LC3B, and TFEB genes in vitro and in vivo. Results:Following irradiation with 4 Gy, the relatively radioresistant T98 cells exhibited enhanced autophagic flux. The more radiosensitive U87 cell line suffered a blockage of autophagic flux. Silencing of LC3A, LC3B, and TFEB genes in vitro, significantly sensitized cells to radiotherapy and temozolomide (U87: P < 0.01 and < 0.05, respectively; T98: P < 0.01 and < 0.01, respectively). Silencing of the LC3A gene sensitized mouse xenografts to radiation. Conclusions:Autophagy in cancer cells may be a key factor of radio-resistance and chemo-resistance in glioblastoma cells. Blocking autophagy may improve the efficacy of radiochemotherapy for glioblastoma patients.

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Combined EGFR and Autophagy Modulation Impairs Cell Migration and Enhances Radiosensitivity in Human Glioblastoma Cells

Cited by 44 publications

References 45 publications

Peiminine Inhibits Glioblastoma in Vitro and in Vivo Through Cell Cycle Arrest and Autophagic Flux Blocking

Peiminine Inhibits Glioblastoma in Vitro and in Vivo Through Cell Cycle Arrest and Autophagic Flux Blocking

Glioblastoma, hypoxia and autophagy: a survival-prone ‘ménage-à-trois’

Autophagic flux response and glioblastoma sensitivity to radiation

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