Combined low dose radio- and radioimmunotherapy of experimental HeLa Hep 2 tumours

Eriksson, David; Joniani, Homa Mirzaie; Sheikholvaezin, Ali; Löfroth, Per‐Olov; Johansson, Lennart; Riklund, Katrine; Stigbrand, Torgny

doi:10.1007/s00259-003-1177-2

Cited by 29 publications

(21 citation statements)

References 35 publications

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“…Furthermore, an enhancement of the fraction of cells with several nuclei as well as abnormally shaped multilobulated nuclei could be identified in irradiated cells. This pronounced polymorphism in nuclear appearance has earlier been observed in experimental tumors following radioimmunotherapy (28). The fraction of cells containing >4N DNA, classified as polyploid cells, indicates an amplification of this subpopulation of cells, especially in the treatment group receiving the highest dose of radiation.…”

Section: Discussionsupporting

confidence: 61%

Cell Cycle Disturbances and Mitotic Catastrophes in HeLa Hep2 Cells following 2.5 to 10 Gy of Ionizing Radiation

Eriksson

Löfroth²,

Johansson³

et al. 2007

Clinical Cancer Research

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Purpose: Experimental radioimmunotherapy delivering absorbed doses of 2.5 to 10 Gy has been shown to cause growth retardation of tumors. The purpose of this study was to elucidate the sequential molecular and cellular events occurring in HeLa Hep2 cells exposed to such doses. Methods: Dose-response curves, activation of cell cycle checkpoints, and mitotic behavior were investigated in HeLa Hep2 cells following 2.5- to 10-Gy irradiation by carrying out 3-(4,5-dimethylthiazol-2-yl)-2,5-diphenyltetrazolium bromide assays, Western blots, fluorescence-activated cell sorting analysis, and immunofluorescence stainings. Terminal deoxyribonucleotidyl transferase–mediated dUTP nick end labeling staining was used to detect apoptosis. Results: A G2-M arrest was shown by fluorescence-activated cell sorting analysis. p53 and p21 were found to be up-regulated but were not immediately related to the arrest. The G2-M arrest was transient and the cells reentered the cell cycle still containing unrepaired cellular damage. This premature entry caused an increase of anaphase bridges, lagging chromosomal material, and multipolar mitotic spindles as visualized by propidium iodide staining and immunofluorescence staining with α-tubulin and γ-tubulin antibodies. Furthermore, a dose-dependent significant increase in centrosome numbers from 12.6 ± 6.6% to 67 ± 5.3% was identified as well as a dose-dependent increase of polyploid cells from 2.8 ± 1.3% to 17.6 ± 2.1% with the highest absorbed dose of 10 Gy. These disturbances caused the cells to progress into mitotic catastrophe and a fraction of these dying cells showed apoptotic features as displayed by terminal deoxyribonucleotidyl transferase–mediated dUTP nick end labeling staining 5 to 7 days after irradiation. Conclusion: An absorbed dose of 2.5 to 10 Gy was shown to force HeLa Hep2 cells into mitotic catastrophe and delayed apoptosis. These might be important cell death mechanisms involved in tumor growth retardation following radioimmunotherapy of solid tumors.

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Section: Discussionsupporting

confidence: 61%

Cell Cycle Disturbances and Mitotic Catastrophes in HeLa Hep2 Cells following 2.5 to 10 Gy of Ionizing Radiation

Eriksson

Löfroth²,

Johansson³

et al. 2007

Clinical Cancer Research

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“…The mitotic catastrophe is generally considered a consequence of premature or improper entry of a cell into mitosis and can be induced by a multitude of DNA-damaging agents including radiation. The mitotic catastrophe is executed by most non-hematopoietic tumor cells in response to ionizing radiation [68] and is frequently observed in experimental tumors following radiotherapy and radioimmunotherapy [69][70][71][72][73]. Mitotic catastrophe is today considered to be the major cell death mechanism by which solid tumors respond to clinical radiotherapy.…”

Section: Radiation-induced Mitotic Catastrophementioning

confidence: 99%

Radiation-induced cell death mechanisms

2010

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The main goal when treating malignancies with radiation therapy is to deprive tumor cells of their reproductive potential. One approach to achieve this is by inducing tumor cell apoptosis. Accumulating evidences suggest that induction of apoptosis alone is insufficient to account for the therapeutic effect of radiotherapy. It has become obvious in the last few years that inhibition of the proliferative capacity of malignant cells following irradiation, especially with solid tumors, can occur via alternative cell death modalities or permanent cell cycle arrests, i.e., senescence. In this review, apoptosis and mitotic catastrophe, the two major cell deaths induced by radiation, are described and dissected in terms of activating mechanisms. Furthermore, treatment-induced senescence and its relevance for the outcome of radiotherapy of cancer will be discussed. The importance of p53 for the induction and execution of these different types of cell deaths is highlighted. The efficiency of radiotherapy and radioimmunotherapy has much to gain by understanding the cell death mechanisms that are induced in tumor cells following irradiation. Strategies to use specific inhibitors that will manipulate key molecules in these pathways in combination with radiation might potentiate therapy and enhance tumor cell kill.

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“…RIT was tested for combined administration with radio(chemo)therapy in patients with liver metastases from colorectal cancer, 116 recurrent lymphomas, 117 as well as in pre-clinical models of head and neck cancer 118 and colon cancer. 119,120 Although RIT alone is not a curative treatment, combined chemo-RIT in patients with recurrent GBM and chemoradiation-RIT in patients with newly diagnosed GBM seems to be a promising treatment strategy.…”

Section: Particle Therapymentioning

confidence: 99%

Glioblastoma multiforme: emerging treatments and stratification markers beyond new drugs

Neubeck¹,

Seidlitz²,

Kitzler³

et al. 2015

BJR

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Glioblastoma multiforme (GBM) is the most common primary brain tumour in adults. The standard therapy for GBM is maximal surgical resection followed by radiotherapy with concurrent and adjuvant temozolomide (TMZ). In spite of the extensive treatment, the disease is associated with poor clinical outcome. Further intensification of the standard treatment is limited by the infiltrating growth of the GBM in normal brain areas, the expected neurological toxicities with radiation doses .60 Gy and the dose-limiting toxicities induced by systemic therapy. To improve the outcome of patients with GBM, alternative treatment modalities which add low or no additional toxicities to the standard treatment are needed. Many Phase II trials on new chemotherapeutics or targeted drugs have indicated potential efficacy but failed to improve the overall or progression-free survival in Phase III clinical trials. In this review, we will discuss contemporary issues related to recent technical developments and new metabolic strategies for patients with GBM including MR (spectroscopy) imaging, (amino acid) positron emission tomography (PET), amino acid PET, surgery, radiogenomics, particle therapy, radioimmunotherapy and diets.

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Combined low dose radio- and radioimmunotherapy of experimental HeLa Hep 2 tumours

Cited by 29 publications

References 35 publications

Cell Cycle Disturbances and Mitotic Catastrophes in HeLa Hep2 Cells following 2.5 to 10 Gy of Ionizing Radiation

Cell Cycle Disturbances and Mitotic Catastrophes in HeLa Hep2 Cells following 2.5 to 10 Gy of Ionizing Radiation

Radiation-induced cell death mechanisms

Glioblastoma multiforme: emerging treatments and stratification markers beyond new drugs

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