Pro-inflammatory gene expression in solid glioblastoma microenvironment and in hypoxic stem cells from human glioblastoma

Tafani, Marco; Vito, Maura Di; Frati, Alessandro; Pellegrini, Laura; Santis, Elena De; Sette, Giovanni; Eramo, Adriana; Sale, Patrizio; Mari, Emanuela; Santoro, Antonio; Raco, Antonino; Salvati, Maurizio; Maria, Ruggero De; Russo, Matteo Antonio

doi:10.1186/1742-2094-8-32

Cited by 111 publications

(103 citation statements)

References 33 publications

(43 reference statements)

Supporting

Mentioning

100

Contrasting

Unclassified

Order By: Relevance

“…The microenvironment of glioblastoma tumors is characterized by the infiltration of hyperactivated immune cells, which aggravate disease progression. Thus, it can be hypothesized that inhibition of lipid metabolism can also reduce inflammation at tumor sites [88][89][90]. However, the potential side effects of pyrrolidine-2 deter its use in vivo.…”

Section: Discussionmentioning

confidence: 99%

Pharmacological inhibition of lipid droplet formation enhances the effectiveness of curcumin in glioblastoma

Zhang

Cui

Amiri

et al. 2016

European Journal of Pharmaceutics and Biopharmaceutics

View full text Add to dashboard Cite

a b s t r a c tIncreased lipid droplet number and fatty acid synthesis allow glioblastoma multiforme, the most common and aggressive type of brain cancer, to withstand accelerated metabolic rates and resist therapeutic treatments. Lipid droplets are postulated to sequester hydrophobic therapeutic agents, thereby reducing drug effectiveness. We hypothesized that the inhibition of lipid droplet accumulation in glioblastoma cells using pyrrolidine-2, a cytoplasmic phospholipase A2 alpha inhibitor, can sensitize cancer cells to the killing effect of curcumin, a promising anticancer agent isolated from the turmeric spice. We observed that curcumin localized in the lipid droplets of human U251N glioblastoma cells. Reduction of lipid droplet number using pyrrolidine-2 drastically enhanced the therapeutic effect of curcumin in both 2D and 3D glioblastoma cell models. The mode of cell death involved was found to be mediated by caspase-3. Comparatively, the current clinical chemotherapeutic standard, temozolomide, was significantly less effective in inducing glioblastoma cell death. Together, our results suggest that the inhibition of lipid droplet accumulation is an effective way to enhance the chemotherapeutic effect of curcumin against glioblastoma multiforme.

show abstract

Section: Discussionmentioning

confidence: 99%

Pharmacological inhibition of lipid droplet formation enhances the effectiveness of curcumin in glioblastoma

Zhang

Cui

Amiri

et al. 2016

European Journal of Pharmaceutics and Biopharmaceutics

View full text Add to dashboard Cite

show abstract

“…Different studies tried to generate a model of GBM and they hypothesized that the GBM tumor mass was a multilayer and the every tumor layer showed distinct characteristic. Pistollato et al [10] describe GSCs distribution according to tissue hypoxic gradient, Piccirilla et al [11] found a different behavior of GSCs derived from distinct tumor areas and Tafani et al [12] demonstrated that the different pro-inflammatory gene expression of diverse tumor areas. The tumor cells are hypoxic, showed high activation of NF-kB and the expression of pro-inflammatory genes were high, the peri-tumor area showed the high activation of NFkB and the pro-inflammatory genes expressions were low, the core region of the tumor was high proliferation capacity and clonogenic ability, the expression of differentiation markers were low and the genetic abnormalities not shared with the tumor periphery.…”

Section: Review Articlementioning

confidence: 99%

Therapeutic Potential of Glioblastoma Stem Cells

Kalkan¹

2015

MOJCSR

View full text Add to dashboard Cite

Primary and the secondary GBM, these are the two distinct disease entity. The genetic and the epigenetic background of these tumors are highly variable and the treatment procedure of these tumors is not curable because of the cellular heterogeneity and intrinsic ability of the tumor cells to invading healthy tissues. The fatal outcomes of these tumors promote the researchers to find out new markers associated with prognosis and treatment planning. Here we summarized the roles of glioblastoma stem cells in tumor progression and malignant behaviors of GBMs with attention to signaling pathways and molecular regulator involved in maintaining the glioblastoma stem cell phenotype. A better understanding of these stem-like cells is necessary for designing new effective treatments and developing novel molecular strategies to targeting glioblastoma stem cells treatment for these patients.

show abstract

“…In response, tumor cells proliferate (ᛏ Ki67) and migrate; and resting stem cells undergo activation and enter the cell cycle. These stem cells are vulnerable to malignant transformation instead of differentiation (156).…”

Section: Tumor Cell Colonies Generated In the Inflammasomesmentioning

confidence: 99%

Molecular biology of oncogenic inflammatory processes. I. Non-oncogenic and oncogenic pathogens, intrinsic inflammatory reactions without pathogens, and microRNA/DNA interactions (Review)

Sinkovics

2011

Int J Oncol

View full text Add to dashboard Cite

Abstract. In some inflammasomes tumor cells are generated. The internal environment of the inflammasome is conducive to the induction of malignant transformation. Epigenetic changes initiate this process. The subverted stromal connective tissue cells act to promote and sustain the process of malignant trans formation. In its early stages, the premalignant cells depend on paracrine circuitries for the reception of growth factors. The ligands are derived from the connective tissue, and the receptors are expressed on the recipient premalignant cells. The initial events are not a direct attack on the protooncogenes, and thus it may be entirely reversible. Epigenetic processes of hypermethylation of the genes at the promoters of tumor suppressor genes (to silence them), and deacetylation of the histones aimed at the promoters of protooncogenes (to activate them) are ongoing. A large number of short RNA sequences (interfering, micro, short hairpin, noncoding RNAs) silence tumor suppressor genes, by neutralizing their mRNAs. In a serial sequence oncogenes undergo amplifications, pointmutations, translocations and fusions. In its earliest stage, the process is reversible by demethylation of the silenced suppressor gene promoters (to reactivate them), or reacetylation of the histones of the oncogene promoters, thus deactivating them. The external administration of histone deacetylase inhibitors usually leads to the restoration of histone acetylation. In time, the uncorrected processes solidify into constitutive and irreversible gene mutations. Some of the pathogens inducing inflammations with consquential malignant transformation contain oncogenic gene sequences (papilloma viruses, EpsteinBarr virus, Kaposi's sarcomaassociated herpesvirus, hepatitis B and C viruses, Merkel cell polyoma virus, Helicobacter pylori, enterotoxigenic Bacteroides fragilis). These induced malignancies may be multifocal. Other pathogens are devoid of any known oncogenic genomic sequences (mycoplasma vavcarcinogenesis, chlamydia MALTlymphoma genesis). In these cases the host's inflammatory reactions induce the malignant transformation in serial sequences of gene alterations initiated by hypoxia and reactive oxygen and nitrogen species generation. Carcinogenic intrinsic inflammatory processes endogenously initiated without a pathogen are recognized. Chronic inflammatory processes signal the RNA/DNA complex. In response, the DNA may revert into its ancient primordial 'immortal' format, which the clinics recognize as 'oncogenesis'. The DNA remains the ultimate master of bioengineering in order to sustain life. A discussion on the most versatile and resistant primordial RNA/ DNA complex and the pre, proto, and unicellular world in which they coexisted is included. Contents1. Pathogens without oncogenic genomic sequences activating cellular oncogenes 2. The inflammasome 3. Tumor cell colonies generated in the inflammasomes 4. Pathogens with potentially oncogenic genomic sequences 5. Mechanisms of inflammatory carcinogenesis Pathogens without oncogenic...

show abstract

Pro-inflammatory gene expression in solid glioblastoma microenvironment and in hypoxic stem cells from human glioblastoma

Cited by 111 publications

References 33 publications

Pharmacological inhibition of lipid droplet formation enhances the effectiveness of curcumin in glioblastoma

Pharmacological inhibition of lipid droplet formation enhances the effectiveness of curcumin in glioblastoma

Therapeutic Potential of Glioblastoma Stem Cells

Molecular biology of oncogenic inflammatory processes. I. Non-oncogenic and oncogenic pathogens, intrinsic inflammatory reactions without pathogens, and microRNA/DNA interactions (Review)

Contact Info

Product

Resources

About