Your search keyword '"Cell-cycle"' showing total 27 results

1. HMGA1 Regulates the Expression of Replication-Dependent Histone Genes and Cell-Cycle in Breast Cancer Cells.

Author

Petrosino, Sara, Pacor, Sabrina, Pegoraro, Silvia, Gazziero, Virginia Anna, Canarutto, Giulia, Piazza, Silvano, Manfioletti, Guidalberto, and Sgarra, Riccardo

Subjects

*BRCA genes, *GENE expression, *TRIPLE-negative breast cancer, *BREAST cancer, *CANCER cells, *BREAST

Abstract

Breast cancer (BC) is the primary cause of cancer mortality in women and the triple-negative breast cancer (TNBC) is the most aggressive subtype characterized by poor differentiation and high proliferative properties. High mobility group A1 (HMGA1) is an oncogenic factor involved in the onset and progression of the neoplastic transformation in BC. Here, we unraveled that the replication-dependent-histone (RD-HIST) gene expression is enriched in BC tissues and correlates with HMGA1 expression. We explored the role of HMGA1 in modulating the RD-HIST genes expression in TNBC cells and show that MDA-MB-231 cells, depleted of HMGA1, express low levels of core histones. We show that HMGA1 participates in the activation of the HIST1H4H promoter and that it interacts with the nuclear protein of the ataxia-telangiectasia mutated locus (NPAT), the coordinator of the transcription of the RD-HIST genes. Moreover, we demonstrate that HMGA1 silencing increases the percentage of cells in G0/G1 phase both in TNBC and epirubicin resistant TNBC cells. Moreover, HMGA1 silencing causes an increase in epirubicin IC50 both in parental and epirubicin resistant cells thus suggesting that targeting HMGA1 could affect the efficacy of epirubicin treatment. [ABSTRACT FROM AUTHOR]

Published

2023

2. iPLA2β-Null Mice Show HCC Protection by an Induction of Cell-Cycle Arrest after Diethylnitrosamine Treatment.

Author

Andrade, Adriana, Poth, Tanja, Brobeil, Alexander, Merle, Uta, and Chamulitrat, Walee

Subjects

*NON-alcoholic fatty liver disease, *PHOSPHOLIPID antibodies, *PHOSPHOLIPASES, *PHOSPHOLIPASE A2, *BLOOD lactate, *MICE

Abstract

Group VIA phospholipase A2 (iPLA2β) play diverse biological functions in epithelial cells and macrophages. Global deletion in iPLA2β-null (KO) mice leads to protection against hepatic steatosis in non-alcoholic fatty liver disease, in part, due to the replenishment of the loss of hepatocellular phospholipids. As the loss of phospholipids also occurs in hepatocellular carcinoma (HCC), we hypothesized that global deletion in KO mice may lead to protection against HCC. Here, HCC induced by diethylnitrosamine (DEN) was chosen because DEN causes direct injury to the hepatocytes. Male wild-type (WT) and KO mice at 3–5 weeks of age (12–13 mice/group) were subjected to a single intraperitoneal treatment with 10 mg/kg DEN, and mice were killed 12 months later. Analyses of histology, plasma cytokines, and gene expression were performed. Due to the low-dose DEN used, we observed a liver nodule in 3 of 13 WT and 2 of 12 KO mice. Only one DEN-treated WT mouse was confirmed to have HCC. DEN-treated KO mice did not show any HCC but showed suppressed hepatic expression of cell-cycle cyclinD2 and BCL2 as well as inflammatory markers IL-1β, IL-10, and VCAM-1. Notably, DEN-treated KO mice showed increased hepatic necrosis and elevated levels of plasma lactate dehydrogenase suggesting an exacerbation of liver injury. Thus, global iPLA2β deficiency in DEN-treated mice rendered HCC protection by an induction of cell-cycle arrest. Our results suggest the role of iPLA2β inhibition in HCC treatment. [ABSTRACT FROM AUTHOR]

Published

2022

3. From Double-Strand Break Recognition to Cell-Cycle Checkpoint Activation: High Content and Resolution Image Cytometry Unmasks 53BP1 Multiple Roles in DNA Damage Response and p53 Action.

Author

Furia, Laura, Pelicci, Simone, Scanarini, Mirco, Pelicci, Pier Giuseppe, and Faretta, Mario

Subjects

*DNA repair, *HIGH resolution imaging, *DNA damage, *DOUBLE-strand DNA breaks, *DOSE-response relationship (Radiation), *CYTOMETRY, *MOLECULAR interactions

Abstract

53BP1 protein has been isolated in-vitro as a putative p53 interactor. From the discovery of its engagement in the DNA-Damage Response (DDR), its role in sustaining the activity of the p53-regulated transcriptional program has been frequently under-evaluated, even in the case of a specific response to numerous DNA Double-Strand Breaks (DSBs), i.e., exposure to ionizing radiation. The localization of 53BP1 protein constitutes a key to decipher the network of activities exerted in response to stress. We present here an automated-microscopy for image cytometry protocol to analyze the evolution of the DDR, and to demonstrate how 53BP1 moved from damaged sites, where the well-known interaction with the DSB marker γH2A.X takes place, to nucleoplasm, interacting with p53, and enhancing the transcriptional regulation of the guardian of the genome protein. Molecular interactions have been quantitatively described and spatiotemporally localized at the highest spatial resolution by a simultaneous analysis of the impairment of the cell-cycle progression. Thanks to the high statistical sampling of the presented protocol, we provide a detailed quantitative description of the molecular events following the DSBs formation. Single-Molecule Localization Microscopy (SMLM) Analysis finally confirmed the p53–53BP1 interaction on the tens of nanometers scale during the distinct phases of the response. [ABSTRACT FROM AUTHOR]

Published

2022

4. Loss of p16: A Bouncer of the Immunological Surveillance?

Author

Katherine M. Aird, Raquel Buj, Naveen Kumar Tangudu, and Kelly E. Leon

Subjects

Senescence, Chemokine, chemotherapy resistance, senescence, Regulator, Review, Biology, General Biochemistry, Genetics and Molecular Biology, law.invention, Downregulation and upregulation, law, Transcriptional regulation, melanoma, pancreatic adenocarcinoma, lcsh:Science, Ecology, Evolution, Behavior and Systematics, Paleontology, senescence-associated secretory phenotype (SASP), Cell cycle, Phenotype, cell-cycle, Space and Planetary Science, tumor infiltration, biology.protein, Cancer research, Suppressor, lcsh:Q

Abstract

p16INK4A (hereafter called p16) is an important tumor suppressor protein frequently suppressed in human cancer and highly upregulated in many types of senescence. Although its role as a cell cycle regulator is very well delineated, little is known about its other non-cell cycle-related roles. Importantly, recent correlative studies suggest that p16 may be a regulator of tissue immunological surveillance through the transcriptional regulation of different chemokines, interleukins and other factors secreted as part of the senescence-associated secretory phenotype (SASP). Here, we summarize the current evidence supporting the hypothesis that p16 is a regulator of tumor immunity.

Published

2021

5. Genotoxic Effects of Cylindrospermopsin, Microcystin-LR and Their Binary Mixture in Human Hepatocellular Carcinoma (HepG2) Cell Line

Author

Universidad de Sevilla. Departamento de Nutrición y Bromatología, Toxicología y Medicina Legal, Ministerio de Economía y Competitividad (MINECO). España, Ministerio de Ciencia, Innovación y Universidades (MICINN). España, European Cooperation in Science and Technology (COST), Díez-Quijada Jiménez, Leticia, Hercog, Klara, Štampar, Martina, Filipič, Metka, Cameán Fernández, Ana María, Jos Gallego, Ángeles Mencía, Žegura, Bojana, Universidad de Sevilla. Departamento de Nutrición y Bromatología, Toxicología y Medicina Legal, Ministerio de Economía y Competitividad (MINECO). España, Ministerio de Ciencia, Innovación y Universidades (MICINN). España, European Cooperation in Science and Technology (COST), Díez-Quijada Jiménez, Leticia, Hercog, Klara, Štampar, Martina, Filipič, Metka, Cameán Fernández, Ana María, Jos Gallego, Ángeles Mencía, and Žegura, Bojana

Abstract

Simultaneous occurrence of cylindrospermopsin (CYN) and microcystin-LR (MCLR) has been reported in the aquatic environment and thus human exposure to such mixtures is possible. As data on the combined effects of CYN/MCLR are scarce, we aimed to investigate the adverse effects related to genotoxic activities induced by CYN (0.125, 0.25 and 0.5 µg/mL) and MCLR (1 µg/mL) as single compounds and their combinations in HepG2 cells after 24 and 72 h exposure. CYN and CYN/MCLR induced DNA double-strand breaks after 72 h exposure, while cell cycle analysis revealed that CYN and CYN/MCLR arrested HepG2 cells in G0/G1 phase. Moreover, CYN and the combination with MCLR upregulated CYP1A1 and target genes involved in DNA-damage response (CDKN1A, GADD45A). Altogether, the results showed that after 72 h exposure genotoxic activity of CYN/MCLR mixture was comparable to the one of pure CYN. On the contrary, MCLR (1 µg/mL) had no effect on the viability of cells and had no influence on cell division. It did not induce DNA damage and did not deregulate studied genes after prolonged exposure. The outcomes of the study confirm the importance of investigating the combined effects of several toxins as the effects can differ from those induced by single compounds.

Published

2020

6. HMGA1 Regulates the Expression of Replication-Dependent Histone Genes and Cell-Cycle in Breast Cancer Cells.

Author

Petrosino S, Pacor S, Pegoraro S, Gazziero VA, Canarutto G, Piazza S, Manfioletti G, and Sgarra R

Subjects

Female, Humans, Cell Cycle, Cell Line, Tumor, Epirubicin, Histones metabolism, HMGA1a Protein genetics, HMGA1a Protein metabolism, Triple Negative Breast Neoplasms genetics, Triple Negative Breast Neoplasms metabolism

Abstract

Breast cancer (BC) is the primary cause of cancer mortality in women and the triple-negative breast cancer (TNBC) is the most aggressive subtype characterized by poor differentiation and high proliferative properties. High mobility group A1 (HMGA1) is an oncogenic factor involved in the onset and progression of the neoplastic transformation in BC. Here, we unraveled that the replication-dependent-histone (RD-HIST) gene expression is enriched in BC tissues and correlates with HMGA1 expression. We explored the role of HMGA1 in modulating the RD-HIST genes expression in TNBC cells and show that MDA-MB-231 cells, depleted of HMGA1, express low levels of core histones. We show that HMGA1 participates in the activation of the HIST1H4H promoter and that it interacts with the nuclear protein of the ataxia-telangiectasia mutated locus (NPAT), the coordinator of the transcription of the RD-HIST genes. Moreover, we demonstrate that HMGA1 silencing increases the percentage of cells in G0/G1 phase both in TNBC and epirubicin resistant TNBC cells. Moreover, HMGA1 silencing causes an increase in epirubicin IC 50 both in parental and epirubicin resistant cells thus suggesting that targeting HMGA1 could affect the efficacy of epirubicin treatment.

Published

2022

7. Chromochloris zofingiensis (Chlorophyceae) Divides by Consecutive Multiple Fission Cell-Cycle under Batch and Continuous Cultivation

Author

Idan Koren, Aliza Zarka, Inna Khozin-Goldberg, and Sammy Boussiba

Subjects

0106 biological sciences, 0301 basic medicine, Cell division, Fission, Chlorophyceae, Context (language use), Biology, 01 natural sciences, General Biochemistry, Genetics and Molecular Biology, Article, 03 medical and health sciences, chemistry.chemical_compound, Astaxanthin, 010608 biotechnology, multiple fission, lcsh:QH301-705.5, General Immunology and Microbiology, Phototroph, microalgae, Cell cycle, biology.organism_classification, astaxanthin, 030104 developmental biology, chemistry, lcsh:Biology (General), cell-cycle, Green algae, General Agricultural and Biological Sciences, Biological system, Chromochloris zofingiensis

Abstract

Several green algae can divide by multiple fission and spontaneously synchronize their cell cycle with the available light regime. The yields that can be obtained from a microalgal culture are directly affected by cell cycle events. Chromochloris zofingiensis is considered as one of the most promising microalgae for biotechnological applications due to its fast growth and the flexible trophic capabilities. It is intensively investigated in the context of bio-commodities production (carotenoids, storage lipids), however, the pattern of cell-cycle events under common cultivation strategies was not yet characterized for C. zofingiensis. In this study, we have employed fluorescence microscopy to characterize the basic cell-cycle dynamics under batch and continuous modes of phototrophic C. zofingiensis cultivation. Staining with SYBR green—applied in DMSO solution—enabled, for the first time, the clear and simple visualization of polynuclear stages in this microalga. Accordingly, we concluded that C. zofingiensis divides by a consecutive pattern of multiple fission, whereby it spontaneously synchronizes growth and cell division according to the available illumination regime. In high-light continuous culture or low-light batch culture, C. zofingiensis cell-cycle was completed within several light-dark (L/D) cycles (14 h/10 h), however, cell divisions were synchronized with the dark periods only in the high-light continuous culture. In both modes of cultivation, daughter cell release was mainly facilitated by division of 8 and 16-polynuclear cells. The results of this study are of both fundamental and applied science significance and are also important for the development of an efficient nuclear transformation system for C. zofingiensis.

Published

2021

8. Unravelling the Potential Cytotoxic Effects of Metal Oxide Nanoparticles and Metal(Loid) Mixtures on A549 Human Cell Line

Author

Fernanda Rosário, Ana Teresa Reis, Maria João Bessa, Carla Costa, Cláudia B. Lopes, Ana C. Estrada, Fátima Brandão, Daniela S. Tavares, João Paulo Teixeira, and Instituto de Saúde Pública da Universidade do Porto

Subjects

mercury, General Chemical Engineering, Cell, 02 engineering and technology, 010501 environmental sciences, Pharmacology, 01 natural sciences, Article, Flow cytometry, lcsh:Chemistry, A549, medicine, General Materials Science, Clonogenic assay, Cytotoxicity, 0105 earth and related environmental sciences, A549 cell, medicine.diagnostic_test, Cell growth, Chemistry, co-exposure, arsenic, cerium oxide nanoparticles, Cell cycle, 021001 nanoscience & nanotechnology, medicine.anatomical_structure, mixtures, lcsh:QD1-999, cell-cycle, Toxicity, cytotoxicity, clonogenic assay, Genotoxicidade Ambiental, 0210 nano-technology, titanium dioxide nanoparticles

Abstract

Humans are typically exposed to environmental contaminants&rsquo, mixtures that result in different toxicity than exposure to the individual counterparts. Yet, the toxicology of chemical mixtures has been overlooked. This work aims at assessing and comparing viability and cell cycle of A549 cells after exposure to single and binary mixtures of: titanium dioxide nanoparticles (TiO2NP) 0.75&ndash, 75 mg/L, cerium oxide nanoparticles (CeO2NP) 0.0.75&ndash, 10 &mu, g/L, arsenic (As) 0.75&ndash, 2.5 mg/L, and mercury (Hg) 5&ndash, 100 mg/L. Viability was assessed through water-soluble tetrazolium (WST-1) and thiazolyl blue tetrazolium bromide (MTT) (24 h exposure) and clonogenic (seven-day exposure) assays. Cell cycle alterations were explored by flow cytometry. Viability was affected in a dose- and time-dependent manner. Prolonged exposure caused inhibition of cell proliferation even at low concentrations. Cell-cycle progression was affected by TiO2NP 75 mg/L, and As 0.75 and 2.5 &mu, g/L, increasing the cell proportion at G0/G1 phase. Combined exposure of TiO2NP or CeO2NP mitigated As adverse effects, increasing the cell surviving factor, but cell cycle alterations were still observed. Only CeO2NP co-exposure reduced Hg toxicity, translated in a decrease of cells in Sub-G1. Toxicity was diminished for both NPs co-exposure compared to its toxicity alone, but a marked toxicity for the highest concentrations was observed for longer exposures. These findings prove that joint toxicity of contaminants must not be disregarded.

Published

2020

9. Genotoxic Effects of Cylindrospermopsin, Microcystin-LR and Their Binary Mixture in Human Hepatocellular Carcinoma (HepG2) Cell Line

Author

Metka Filipič, Leticia Díez-Quijada, Ángeles Jos, Bojana Žegura, Klara Hercog, Ana M. Cameán, Martina Štampar, Universidad de Sevilla. Departamento de Nutrición y Bromatología, Toxicología y Medicina Legal, Ministerio de Economía y Competitividad (MINECO). España, Ministerio de Ciencia, Innovación y Universidades (MICINN). España, and European Cooperation in Science and Technology (COST)

Subjects

Carcinoma, Hepatocellular, Cell division, Microcystins, DNA damage, Health, Toxicology and Mutagenesis, lcsh:Medicine, Microcystin-LR, 010501 environmental sciences, Toxicology, 01 natural sciences, Article, 03 medical and health sciences, chemistry.chemical_compound, Alkaloids, Downregulation and upregulation, polycyclic compounds, cylindrospermopsin, Humans, DNA double-strand breaks, Enzyme Inhibitors, HepG2 cells, 030304 developmental biology, 0105 earth and related environmental sciences, 0303 health sciences, Cyanobacteria Toxins, Dose-Response Relationship, Drug, microcystin-LR, lcsh:R, Liver Neoplasms, mRNA expression, Hep G2 Cells, Cell cycle, Molecular biology, mixture, chemistry, cell-cycle, Marine Toxins, Cylindrospermopsin, GADD45A, DNA, DNA Damage

Abstract

Simultaneous occurrence of cylindrospermopsin (CYN) and microcystin-LR (MCLR) has been reported in the aquatic environment and thus human exposure to such mixtures is possible. As data on the combined effects of CYN/MCLR are scarce, we aimed to investigate the adverse effects related to genotoxic activities induced by CYN (0.125, 0.25 and 0.5 &micro, g/mL) and MCLR (1 &micro, g/mL) as single compounds and their combinations in HepG2 cells after 24 and 72 h exposure. CYN and CYN/MCLR induced DNA double-strand breaks after 72 h exposure, while cell cycle analysis revealed that CYN and CYN/MCLR arrested HepG2 cells in G0/G1 phase. Moreover, CYN and the combination with MCLR upregulated CYP1A1 and target genes involved in DNA-damage response (CDKN1A, GADD45A). Altogether, the results showed that after 72 h exposure genotoxic activity of CYN/MCLR mixture was comparable to the one of pure CYN. On the contrary, MCLR (1 &micro, g/mL) had no effect on the viability of cells and had no influence on cell division. It did not induce DNA damage and did not deregulate studied genes after prolonged exposure. The outcomes of the study confirm the importance of investigating the combined effects of several toxins as the effects can differ from those induced by single compounds.

Published

2020

10. In Vitro Hepatotoxic and Neurotoxic Effects of Titanium and Cerium Dioxide Nanoparticles, Arsenic and Mercury Co-Exposure.

Author

Rosário, Fernanda, Costa, Carla, Lopes, Cláudia B., Estrada, Ana C., Tavares, Daniela S., Pereira, Eduarda, Teixeira, João Paulo, and Reis, Ana Teresa

Subjects

*TITANIUM dioxide nanoparticles, *ARSENIC, *CERIUM oxides, *CELL cycle, *POLLUTANTS, *BINARY mixtures, *CELL proliferation

Abstract

Considering the increasing emergence of new contaminants, such as nanomaterials, mixing with legacy contaminants, including metal(loid)s, it becomes imperative to understand the toxic profile resulting from these interactions. This work aimed at assessing and comparing the individual and combined hepatotoxic and neurotoxic potential of titanium dioxide nanoparticles (TiO2NPs 0.75–75 mg/L), cerium oxide nanoparticles (CeO2NPs 0.075–10 μg/L), arsenic (As 0.01–2.5 mg/L), and mercury (Hg 0.5–100 mg/L) on human hepatoma (HepG2) and neuroblastoma (SH-SY5Y) cells. Viability was assessed through WST-1 (24 h) and clonogenic (7 days) assays and it was affected in a dose-, time- and cell-dependent manner. Higher concentrations caused greater toxicity, while prolonged exposure caused inhibition of cell proliferation, even at low concentrations, for both cell lines. Cell cycle progression, explored by flow cytometry 24 h post-exposure, revealed that TiO2NPs, As and Hg but not CeO2NPs, changed the profiles of SH-SY5Y and HepG2 cells in a dose-dependent manner, and that the cell cycle was, overall, more affected by exposure to mixtures. Exposure to binary mixtures revealed either potentiation or antagonistic effects depending on the composition, cell type and time of exposure. These findings prove that joint toxicity of contaminants cannot be disregarded and must be further explored. [ABSTRACT FROM AUTHOR]

Published

2022

11. Double Strand Breaks and Cell-Cycle Arrest Induced by the Cyanobacterial Toxin Cylindrospermopsin in HepG2 Cells.

Author

Štraser, Alja, Filipič, Metka, Novak, Matjaž, and Žegura, Bojana

Abstract

The newly emerging cyanobacterial cytotoxin cylindrospermopsin (CYN) is increasingly found in surface freshwaters, worldwide. It poses a potential threat to humans after chronic exposure as it was shown to be genotoxic in a range of test systems and is potentially carcinogenic. However, the mechanisms of CYN toxicity and genotoxicity are not well understood. In the present study CYN induced formation of DNA double strand breaks (DSBs), after prolonged exposure (72 h), in human hepatoma cells, HepG2. CYN (0.1-0.5 µg/mL, 24-96 h) induced morphological changes and reduced cell viability in a dose and time dependent manner. No significant increase in lactate dehydrogenase (LDH) leakage could be observed after CYN exposure, indicating that the reduction in cell number was due to decreased cell proliferation and not due to cytotoxicity. This was confirmed by imunocytochemical analysis of the cell-proliferation marker Ki67. Analysis of the cell-cycle using flow-cytometry showed that CYN has an impact on the cell cycle, indicating G0/G1 arrest after 24 h and S-phase arrest after longer exposure (72 and 96 h). Our results provide new evidence that CYN is a direct acting genotoxin, causing DSBs, and these facts need to be considered in the human health risk assessment. [ABSTRACT FROM AUTHOR]

Published

2013

12. mDrop-Seq: Massively Parallel Single-Cell RNA-Seq of Saccharomyces cerevisiae and Candida albicans.

Author

Dohn, Ryan, Xie, Bingqing, Back, Rebecca, Selewa, Alan, Eckart, Heather, Rao, Reeta Prusty, and Basu, Anindita

Subjects

CANDIDA albicans, SACCHAROMYCES cerevisiae, SACCHAROMYCES, DEVIATORIC stress (Engineering), RNA sequencing, CANDIDA, GENETIC variation

Abstract

Advances in high-throughput single-cell RNA sequencing (scRNA-seq) have been limited by technical challenges such as tough cell walls and low RNA quantity that prevent transcriptomic profiling of microbial species at throughput. We present microbial Drop-seq or mDrop-seq, a high-throughput scRNA-seq technique that is demonstrated on two yeast species, Saccharomyces cerevisiae, a popular model organism, and Candida albicans, a common opportunistic pathogen. We benchmarked mDrop-seq for sensitivity and specificity and used it to profile 35,109 S. cerevisiae cells to detect variation in mRNA levels between them. As a proof of concept, we quantified expression differences in heat shock S. cerevisiae using mDrop-seq. We detected differential activation of stress response genes within a seemingly homogenous population of S. cerevisiae under heat shock. We also applied mDrop-seq to C. albicans cells, a polymorphic and clinically relevant species of yeast with a thicker cell wall compared to S. cerevisiae. Single-cell transcriptomes in 39,705 C. albicans cells were characterized using mDrop-seq under different conditions, including exposure to fluconazole, a common anti-fungal drug. We noted differential regulation in stress response and drug target pathways between C. albicans cells, changes in cell cycle patterns and marked increases in histone activity when treated with fluconazole. We demonstrate mDrop-seq to be an affordable and scalable technique that can quantify the variability in gene expression in different yeast species. We hope that mDrop-seq will lead to a better understanding of genetic variation in pathogens in response to stimuli and find immediate applications in investigating drug resistance, infection outcome and developing new drugs and treatment strategies. [ABSTRACT FROM AUTHOR]

Published

2022

13. Betulinic Acid Decorated with Polar Groups and Blue Emitting BODIPY Dye: Synthesis, Cytotoxicity, Cell-Cycle Analysis and Anti-HIV Profiling.

Author

Kodr, David, Stanková, Jarmila, Rumlová, Michaela, Džubák, Petr, Řehulka, Jiří, Zimmermann, Tomáš, Křížová, Ivana, Gurská, Soňa, Hajdúch, Marián, Drašar, Pavel B., and Jurášek, Michal

Subjects

BETULINIC acid, STAINS & staining (Microscopy), BIOSYNTHESIS, FLUORESCENCE microscopy, ENDOPLASMIC reticulum

Abstract

Betulinic acid (BA) is a potent triterpene, which has shown promising potential in cancer and HIV-1 treatment. Here, we report a synthesis and biological evaluation of 17 new compounds, including BODIPY labelled analogues derived from BA. The analogues terminated by amino moiety showed increased cytotoxicity (e.g., BA had on CCRF-CEM IC50 > 50 μM, amine 3 IC50 0.21 and amine 14 IC50 0.29). The cell-cycle arrest was evaluated and did not show general features for all the tested compounds. A fluorescence microscopy study of six derivatives revealed that only 4 and 6 were detected in living cells. These compounds were colocalized with the endoplasmic reticulum and mitochondria, indicating possible targets in these organelles. The study of anti-HIV-1 activity showed that 8, 10, 16, 17 and 18 have had IC50i > 10 μM. Only completely processed p24 CA was identified in the viruses formed in the presence of compounds 4 and 12. In the cases of 2, 8, 9, 10, 16, 17 and 18, we identified not fully processed p24 CA and p25 CA-SP1 protein. This observation suggests a similar mechanism of inhibition as described for bevirimat. [ABSTRACT FROM AUTHOR]

Published

2021

14. Anti-Atherosclerotic Effect of Gossypetin on Abnormal Vascular Smooth Muscle Cell Proliferation and Migration.

Author

Lin, Hui-Hsuan, Hsieh, Ming-Chang, Wang, Chi-Ping, Yu, Pei-Rong, Lee, Ming-Shih, and Chen, Jing-Hsien

Subjects

VASCULAR smooth muscle, MUSCLE cells, CELL migration, PROTEIN kinase B, MATRIX metalloproteinases, HYDROXYCHOLESTEROLS

Abstract

Gossypetin (GTIN), known as 3,5,7,8,3′,4′-hexahydroxyflavone, has been demonstrated to exert anti-atherosclerotic potential against apoptotic injury in oxidized low-density lipoprotein-incubated endothelial cells, and atherosclerotic lesions of cholesterol-fed rabbits. However, the effect and underlying mechanism of GTIN on abnormal vascular smooth muscle cells (VSMCs) proliferation and migration, a major event in the pathogenesis of atherosclerosis, is still unknown. In this study, non-cytotoxic doses of GTIN abolished the VSMCs A7r5 proliferation and cell-cycle S phase distribution. The GTIN-arrested G0/G1 phase might be performed by increasing the expressions of phosphorylated p53 and its downstream molecules that inhibit the activation of cyclin E/cyclin-dependent kinase (cdk)-2, blocking retinoblastoma protein (Rb) phosphorylation and the subsequent dissociation of Rb/transcription factor E2F1 complex. In addition, the results indicated that GTIN inhibited VSMCs wound-healing and migratory abilities through reducing matrix metalloproteinase (MMP)-9 activity and expression, as well as down-regulating protein kinase B (PKB)/nuclear factor-kappaB (NF-κB) signaling. GTIN also revealed potential in diminishing reactive oxygen species (ROS) generation. These findings suggested the inhibitory effects of GTIN on VSMCs dysfunction could likely lead to the containment of atherosclerosis and other cardiovascular illness. [ABSTRACT FROM AUTHOR]

Published

2021

15. Loss of p16: A Bouncer of the Immunological Surveillance?

Author

Leon, Kelly E., Tangudu, Naveen Kumar, Aird, Katherine M., and Buj, Raquel

Subjects

*TUMOR suppressor proteins, *CHEMOKINES, *P16 gene, *PHENOTYPES, *CELL cycle, *INTERLEUKINS

Abstract

p16INK4A (hereafter called p16) is an important tumor suppressor protein frequently suppressed in human cancer and highly upregulated in many types of senescence. Although its role as a cell cycle regulator is very well delineated, little is known about its other non-cell cycle-related roles. Importantly, recent correlative studies suggest that p16 may be a regulator of tissue immunological surveillance through the transcriptional regulation of different chemokines, interleukins and other factors secreted as part of the senescence-associated secretory phenotype (SASP). Here, we summarize the current evidence supporting the hypothesis that p16 is a regulator of tumor immunity. [ABSTRACT FROM AUTHOR]

Published

2021

16. Chromochloris zofingiensis (Chlorophyceae) Divides by Consecutive Multiple Fission Cell-Cycle under Batch and Continuous Cultivation.

Author

Koren, Idan, Boussiba, Sammy, Khozin-Goldberg, Inna, Zarka, Aliza, and Devaux, Pierre

Subjects

*GREEN algae, *APPLIED sciences, *CARBON dioxide in water, *NUCLEAR reactions, *DNA synthesis, *CAROTENOIDS, *DUNALIELLA

Abstract

Simple Summary: Microalgae are plant-like micro-organisms naturally found in fresh and marine water environments, inhabiting a vast range of ecosystems. They capture light energy through photosynthesis and convert low energy inorganic compounds (carbon dioxide and water) into high energy complex organic compounds, such as carbohydrates and fats. Chromochloris zofingiensis is a unicellular microalga currently under intensive research, due to its ability to produce high value pharmaceutical and nutritional pigments. Understanding its growth characteristics is crucial for the establishment of an efficient commercial production of those pigments from this alga. Thus, we have developed a method to stain the nucleus of the alga which enabled us to follow the division pattern under commonly used cultivation methods. We found that C. zofingiensis cells conduct consecutive DNA synthesis and divisions of the nucleus to produce 8 or 16 nuclei before it divides into 8 or 16 daughter cells, respectively. Under high light illumination, the whole process lasts several days, through which cells grow during the light period and divide during the dark period. These findings can be assimilated for the development of the biotechnology process for high pigment productivity. Several green algae can divide by multiple fission and spontaneously synchronize their cell cycle with the available light regime. The yields that can be obtained from a microalgal culture are directly affected by cell cycle events. Chromochloris zofingiensis is considered as one of the most promising microalgae for biotechnological applications due to its fast growth and the flexible trophic capabilities. It is intensively investigated in the context of bio-commodities production (carotenoids, storage lipids); however, the pattern of cell-cycle events under common cultivation strategies was not yet characterized for C. zofingiensis. In this study, we have employed fluorescence microscopy to characterize the basic cell-cycle dynamics under batch and continuous modes of phototrophic C. zofingiensis cultivation. Staining with SYBR green—applied in DMSO solution—enabled, for the first time, the clear and simple visualization of polynuclear stages in this microalga. Accordingly, we concluded that C. zofingiensis divides by a consecutive pattern of multiple fission, whereby it spontaneously synchronizes growth and cell division according to the available illumination regime. In high-light continuous culture or low-light batch culture, C. zofingiensis cell-cycle was completed within several light-dark (L/D) cycles (14 h/10 h); however, cell divisions were synchronized with the dark periods only in the high-light continuous culture. In both modes of cultivation, daughter cell release was mainly facilitated by division of 8 and 16-polynuclear cells. The results of this study are of both fundamental and applied science significance and are also important for the development of an efficient nuclear transformation system for C. zofingiensis. [ABSTRACT FROM AUTHOR]

Published

2021

17. Investigation of DNA Damage and Cell-Cycle Distribution in Human Peripheral Blood Lymphocytes under Exposure to High Doses of Proton Radiotherapy.

Author

Miszczyk, Justyna and Iturri, Jagoba

Subjects

*EXPOSURE dose, *PROTONS, *LYMPHOCYTES, *RADIATION exposure, *DNA damage, *PROTON therapy, *MITOSIS

Abstract

Simple Summary: Radiotherapy is a cornerstone care therapy for many tumors. Despite permanent advances in ra-diation dose delivery, there are unmet needs for further improvement. In principle, proton therapy offers a substantial clinical advantage over conventional modalities using photons in uniform-dose delivery of radiation to tumors, along with significant reductions in the harmful effects on normal tissue. However, the effect and mechanisms of a single high-dose delivery remain unclear. The study aimed to systematically observe and compare the biological effects of DNA damage and cell-cycle phase distribution in the human peripheral blood lymphocytes ex vivo irradiation model of normal tissue after proton versus conventional radiotherapy (X-rays). The effects induced at a single high-dose radiation exposure at a dose range of 8.00–20.00 Gy were studied. The results in-dicate a different distribution of DNA damage following high doses of irradiation with protons versus photons between donors, types of radiation, and doses. The results illuminate the cellular and molecular mechanisms that underlie differences in the distribution of DNA damage and cell-cycle phases. An understanding of the mechanisms in the distinct pathways induced by radiation can facilitate the development of more efficient radiotherapies with beneficial immunological conse-quences. This study systematically investigates how a single high-dose therapeutic proton beam versus X-rays influences cell-cycle phase distribution and DNA damage in human peripheral blood lymphocytes (HPBLs). Blood samples from ten volunteers (both male and female) were irradiated with doses of 8.00, 13.64, 15.00, and 20.00 Gy of 250 kV X-rays or 60 MeV protons. The dose–effect relations were calculated and distributed by plotting the frequencies of DNA damage of excess Premature Chromosome Condensation (PCC) fragments and rings in the G2/M phase, obtained via chemical induction with calyculin A. The Papworth's u test was used to evaluate the distribution of DNA damage. The study shows that high doses of protons induce HPBL DNA damage in the G2/M phase differently than X-rays do. The results indicate a different distribution of DNA damage following high doses of irradiation with protons versus photons between donors, types of radiation, and doses. The proliferation index confirms the impact of high doses of mitosis and the influence of radiotherapy type on the different HPBL response. The results illuminate the cellular and molecular mechanisms that underlie differences in the distribution of DNA damage and cell-cycle phases; these findings may yield an improvement in the efficacy of the radiotherapies used. [ABSTRACT FROM AUTHOR]

Published

2021

18. Pan-Cancer Molecular Patterns and Biological Implications Associated with a Tumor-Specific Molecular Signature.

Author

Rocha, Darío, García, Iris A., González Montoro, Aldana, Llera, Andrea, Prato, Laura, Girotti, María R., Soria, Gastón, and Fernández, Elmer A.

Subjects

*BREAST cancer, *GENE amplification, *GENE expression, *UNCERTAINTY, *GENES, *DNA damage

Abstract

Studying tissue-independent components of cancer and defining pan-cancer subtypes could be addressed using tissue-specific molecular signatures if classification errors are controlled. Since PAM50 is a well-known, United States Food and Drug Administration (FDA)-approved and commercially available breast cancer signature, we applied it with uncertainty assessment to classify tumor samples from over 33 cancer types, discarded unassigned samples, and studied the emerging tumor-agnostic molecular patterns. The percentage of unassigned samples ranged between 55.5% and 86.9% in non-breast tissues, and gene set analysis suggested that the remaining samples could be grouped into two classes (named C1 and C2) regardless of the tissue. The C2 class was more dedifferentiated, more proliferative, with higher centrosome amplification, and potentially more TP53 and RB1 mutations. We identified 28 gene sets and 95 genes mainly associated with cell-cycle progression, cell-cycle checkpoints, and DNA damage that were consistently exacerbated in the C2 class. In some cancer types, the C1/C2 classification was associated with survival and drug sensitivity, and modulated the prognostic meaning of the immune infiltrate. Our results suggest that PAM50 could be repurposed for a pan-cancer context when paired with uncertainty assessment, resulting in two classes with molecular, biological, and clinical implications. [ABSTRACT FROM AUTHOR]

Published

2021

19. Genotoxic Effects of Cylindrospermopsin, Microcystin-LR and Their Binary Mixture in Human Hepatocellular Carcinoma (HepG2) Cell Line.

Author

Díez-Quijada, Leticia, Hercog, Klara, Štampar, Martina, Filipič, Metka, Cameán, Ana M., Jos, Ángeles, and Žegura, Bojana

Subjects

*BINARY mixtures, *DOUBLE-strand DNA breaks, *HEPATOCELLULAR carcinoma, *CELL lines, *GENETIC toxicology, *CELL analysis

Abstract

Simultaneous occurrence of cylindrospermopsin (CYN) and microcystin-LR (MCLR) has been reported in the aquatic environment and thus human exposure to such mixtures is possible. As data on the combined effects of CYN/MCLR are scarce, we aimed to investigate the adverse effects related to genotoxic activities induced by CYN (0.125, 0.25 and 0.5 µg/mL) and MCLR (1 µg/mL) as single compounds and their combinations in HepG2 cells after 24 and 72 h exposure. CYN and CYN/MCLR induced DNA double-strand breaks after 72 h exposure, while cell cycle analysis revealed that CYN and CYN/MCLR arrested HepG2 cells in G0/G1 phase. Moreover, CYN and the combination with MCLR upregulated CYP1A1 and target genes involved in DNA-damage response (CDKN1A, GADD45A). Altogether, the results showed that after 72 h exposure genotoxic activity of CYN/MCLR mixture was comparable to the one of pure CYN. On the contrary, MCLR (1 µg/mL) had no effect on the viability of cells and had no influence on cell division. It did not induce DNA damage and did not deregulate studied genes after prolonged exposure. The outcomes of the study confirm the importance of investigating the combined effects of several toxins as the effects can differ from those induced by single compounds. [ABSTRACT FROM AUTHOR]

Published

2020

20. Regulation of Replication Fork Advance and Stability by Nucleosome Assembly

Author

Prado, Felix, Maya, Douglas, [Prado, Felix] CSIC, Dept Genome Biol, Andalusian Mol Biol & Regenerat Med Ctr CABIMER, Seville 41092, Spain, [Maya, Douglas] CSIC, Dept Genome Biol, Andalusian Mol Biol & Regenerat Med Ctr CABIMER, Seville 41092, Spain, Andalusian government, and Spanish government

Subjects

S-phase checkpoint, Dna-polymerase-epsilon, Loop binding-protein, Newly synthesized histones, homologous recombination, DNA replication, H3 lysine-56 acetylation, Chromatin-remodeling complex, Cell-cycle, replication fork stability, Ubiquitin ligase, Mms22l-nfkbil2 complex, chromatin assembly, DNA damage tolerance

Abstract

The advance of replication forks to duplicate chromosomes in dividing cells requires the disassembly of nucleosomes ahead of the fork and the rapid assembly of parental and de novo histones at the newly synthesized strands behind the fork. Replication-coupled chromatin assembly provides a unique opportunity to regulate fork advance and stability. Through post-translational histone modifications and tightly regulated physical and genetic interactions between chromatin assembly factors and replisome components, chromatin assembly: (1) controls the rate of DNA synthesis and adjusts it to histone availability; (2) provides a mechanism to protect the integrity of the advancing fork; and (3) regulates the mechanisms of DNA damage tolerance in response to replication-blocking lesions. Uncoupling DNA synthesis from nucleosome assembly has deleterious effects on genome integrity and cell cycle progression and is linked to genetic diseases, cancer, and aging.

Published

2017

21. Ribosomal Protein uL11 as a Regulator of Metabolic Circuits Related to Aging and Cell Cycle.

Author

Mołoń, Mateusz, Molestak, Eliza, Kula-Maximenko, Monika, Grela, Przemysław, and Tchórzewski, Marek

Subjects

*CELLULAR aging, *RIBOSOMAL proteins, *PHENOMENOLOGICAL biology, *CELL cycle, *PROTEIN synthesis, *LONGEVITY

Abstract

Aging is a biological phenomenon common to all living organisms. It is thought that the rate of aging is influenced by diverse factors, in many cases related to the control of energy metabolism, i.e., the so-called pro-longevity effects of starvation. Translation, regarded as the main energy consumption process, lies at the center of interest, as it has a significant impact on the longevity phenomenon. It has been shown that perturbations in the translational apparatus may lead to a lower rate of aging. Therefore, the main aim of this study was to investigate aging in relation to the protein biosynthesis circuit, taking into account the uL11 ribosomal protein as a vital ribosomal element. To this end, we used set of yeast mutants with deleted single uL11A or uL11B genes and a double disruptant uL11AB mutant. We applied an integrated approach analyzing a broad range of biological parameters of yeast mutant cells, especially the longevity phenomenon, supplemented with biochemical and high throughput transcriptomic and metobolomic approaches. The analysis showed that the longevity phenomenon is not fully related to the commonly considered energy restriction effect, thus the slow-down of translation does not represent the sole source of aging. Additionally, we showed that uL11 can be classified as a moonlighting protein with extra-ribosomal function having cell-cycle regulatory potential. [ABSTRACT FROM AUTHOR]

Published

2020

22. DNA Damage: From Threat to Treatment.

Author

Carusillo, Antonio and Mussolino, Claudio

Subjects

*DNA repair, *DNA damage, *GENOME editing, *DNA, *TIMING circuits

Abstract

DNA is the source of genetic information, and preserving its integrity is essential in order to sustain life. The genome is continuously threatened by different types of DNA lesions, such as abasic sites, mismatches, interstrand crosslinks, or single-stranded and double-stranded breaks. As a consequence, cells have evolved specialized DNA damage response (DDR) mechanisms to sustain genome integrity. By orchestrating multilayer signaling cascades specific for the type of lesion that occurred, the DDR ensures that genetic information is preserved overtime. In the last decades, DNA repair mechanisms have been thoroughly investigated to untangle these complex networks of pathways and processes. As a result, key factors have been identified that control and coordinate DDR circuits in time and space. In the first part of this review, we describe the critical processes encompassing DNA damage sensing and resolution. In the second part, we illustrate the consequences of partial or complete failure of the DNA repair machinery. Lastly, we will report examples in which this knowledge has been instrumental to develop novel therapies based on genome editing technologies, such as CRISPR-Cas. [ABSTRACT FROM AUTHOR]

Published

2020

23. MSX1—A Potential Marker for Uterus-Preserving Therapy of Endometrial Carcinomas.

Author

Eppich, Simon, Kuhn, Christina, Schmoeckel, Elisa, Mayr, Doris, Mahner, Sven, Jeschke, Udo, Gallwas, Julia, and Heidegger, Helene Hildegard

Subjects

*RENAL cell carcinoma, *STEROID receptors, *CARCINOMA, *ENDOMETRIAL cancer, *WNT proteins

Abstract

Prognostic factors are of great interest in patients with endometrial cancer. One potential factor could be the protein MSX1, a transcription repressor, that has an inhibitory effect on the cell cycle. For this study, endometrioid endometrial carcinomas (n = 53), clear cell endometrial carcinomas (n = 6), endometrioid ovarian carcinomas (n = 19), and clear cell ovarian carcinomas (n = 11) were immunochemically stained for the protein MSX1 and evaluated using the immunoreactive score (IRS). A significant stronger expression of MSX1 was found in endometrioid endometrial carcinomas (p < 0.001), in grading 2 (moderate differentiation) (p = 0.001), and in tumor material of patients with no involvement of lymph nodes (p = 0.031). Correlations were found between MSX1 expression and the expression of β-Catenin, p21, p53, and the steroid receptors ERα, ERβ, PRα, and PRβ. A significant (p = 0.023) better survival for patients with an MSX1 expression in more than 10% of the tumor cells was observed for endometrioid endometrial carcinomas (21.3 years median survival (MSX1-positive) versus 17.3 years (MSX1-negative)). Although there is evidence that MSX1 expression correlates with improved long-term survival, further studies are necessary to evaluate if MSX1 can be used as a prognostic marker. [ABSTRACT FROM AUTHOR]

Published

2020

24. Perinuclear Lamin A and Nucleoplasmic Lamin B2 Characterize Two Types of Hippocampal Neurons through Alzheimer's Disease Progression.

Author

Gil, Laura, Niño, Sandra A., Chi-Ahumada, Erika, Rodríguez-Leyva, Ildelfonso, Guerrero, Carmen, Rebolledo, Ana Belén, Arias, José A., and Jiménez-Capdeville, María E.

Subjects

*ALZHEIMER'S disease, *DISEASE progression, *NUCLEAR reactions, *NEURONS, *CELL cycle, *NEUROFIBRILLARY tangles

Abstract

Background. Recent reports point to a nuclear origin of Alzheimer's disease (AD). Aged postmitotic neurons try to repair their damaged DNA by entering the cell cycle. This aberrant cell cycle re-entry involves chromatin modifications where nuclear Tau and the nuclear lamin are involved. The purpose of this work was to elucidate their participation in the nuclear pathological transformation of neurons at early AD. Methodology. The study was performed in hippocampal paraffin embedded sections of adult, senile, and AD brains at I-VI Braak stages. We analyzed phospho-Tau, lamins A, B1, B2, and C, nucleophosmin (B23) and the epigenetic marker H4K20me3 by immunohistochemistry. Results. Two neuronal populations were found across AD stages, one is characterized by a significant increase of Lamin A expression, reinforced perinuclear Lamin B2, elevated expression of H4K20me3 and nuclear Tau loss, while neurons with nucleoplasmic Lamin B2 constitute a second population. Conclusions. The abnormal cell cycle reentry in early AD implies a fundamental neuronal transformation. This implies the reorganization of the nucleo-cytoskeleton through the expression of the highly regulated Lamin A, heterochromatin repression and building of toxic neuronal tangles. This work demonstrates that nuclear Tau and lamin modifications in hippocampal neurons are crucial events in age-related neurodegeneration. [ABSTRACT FROM AUTHOR]

Published

2020

25. Unravelling the Potential Cytotoxic Effects of Metal Oxide Nanoparticles and Metal(Loid) Mixtures on A549 Human Cell Line.

Author

Rosário, Fernanda, Bessa, Maria João, Brandão, Fátima, Costa, Carla, Lopes, Cláudia B., Estrada, Ana C., Tavares, Daniela S., Teixeira, João Paulo, and Reis, Ana Teresa

Subjects

*METAL nanoparticles, *METALLIC oxides, *TITANIUM dioxide nanoparticles, *POLLUTANTS, *MERCURY vapor, *MERCURY, *CERIUM oxides, *CELL lines

Abstract

Humans are typically exposed to environmental contaminants' mixtures that result in different toxicity than exposure to the individual counterparts. Yet, the toxicology of chemical mixtures has been overlooked. This work aims at assessing and comparing viability and cell cycle of A549 cells after exposure to single and binary mixtures of: titanium dioxide nanoparticles (TiO2NP) 0.75–75 mg/L; cerium oxide nanoparticles (CeO2NP) 0.75–10 μg/L; arsenic (As) 0.75–2.5 mg/L; and mercury (Hg) 5–100 mg/L. Viability was assessed through water-soluble tetrazolium (WST-1) and thiazolyl blue tetrazolium bromide (MTT) (24 h exposure) and clonogenic (seven-day exposure) assays. Cell cycle alterations were explored by flow cytometry. Viability was affected in a dose- and time-dependent manner. Prolonged exposure caused inhibition of cell proliferation even at low concentrations. Cell-cycle progression was affected by TiO2NP 75 mg/L, and As 0.75 and 2.5 μg/L, increasing the cell proportion at G0/G1 phase. Combined exposure of TiO2NP or CeO2NP mitigated As adverse effects, increasing the cell surviving factor, but cell cycle alterations were still observed. Only CeO2NP co-exposure reduced Hg toxicity, translated in a decrease of cells in Sub-G1. Toxicity was diminished for both NPs co-exposure compared to its toxicity alone, but a marked toxicity for the highest concentrations was observed for longer exposures. These findings prove that joint toxicity of contaminants must not be disregarded. [ABSTRACT FROM AUTHOR]

Published

2020

26. Double Strand Breaks and Cell-Cycle Arrest Induced by the Cyanobacterial Toxin Cylindrospermopsin in HepG2 Cells

Author

Metka Filipič, Matjaž Novak, Bojana Žegura, and Štraser Alja

Subjects

Cell cycle checkpoint, cell-proliferation, Time Factors, Cell Survival, cylindrospermopsin, cell-cycle, double-strand breaks, HepG2 cells, Bacterial Toxins, Pharmaceutical Science, Biology, medicine.disease_cause, Resting Phase, Cell Cycle, Article, chemistry.chemical_compound, Alkaloids, Drug Discovery, medicine, Humans, DNA Breaks, Double-Stranded, Viability assay, Cytotoxicity, Uracil, Pharmacology, Toxicology and Pharmaceutics (miscellaneous), lcsh:QH301-705.5, Carcinogen, Cell Proliferation, Genetics, Cyanobacteria Toxins, Dose-Response Relationship, Drug, Cell growth, Hep G2 Cells, Cell cycle, Flow Cytometry, Molecular biology, G1 Phase Cell Cycle Checkpoints, chemistry, lcsh:Biology (General), S Phase Cell Cycle Checkpoints, Cylindrospermopsin, Genotoxicity

Abstract

The newly emerging cyanobacterial cytotoxin cylindrospermopsin (CYN) is increasingly found in surface freshwaters, worldwide. It poses a potential threat to humans after chronic exposure as it was shown to be genotoxic in a range of test systems and is potentially carcinogenic. However, the mechanisms of CYN toxicity and genotoxicity are not well understood. In the present study CYN induced formation of DNA double strand breaks (DSBs), after prolonged exposure (72 h), in human hepatoma cells, HepG2. CYN (0.1–0.5 µg/mL, 24–96 h) induced morphological changes and reduced cell viability in a dose and time dependent manner. No significant increase in lactate dehydrogenase (LDH) leakage could be observed after CYN exposure, indicating that the reduction in cell number was due to decreased cell proliferation and not due to cytotoxicity. This was confirmed by imunocytochemical analysis of the cell-proliferation marker Ki67. Analysis of the cell-cycle using flow-cytometry showed that CYN has an impact on the cell cycle, indicating G0/G1 arrest after 24 h and S-phase arrest after longer exposure (72 and 96 h). Our results provide new evidence that CYN is a direct acting genotoxin, causing DSBs, and these facts need to be considered in the human health risk assessment.

Published

2013

27. Pan-Cancer Molecular Patterns and Biological Implications Associated with a Tumor-Specific Molecular Signature.

Author

Rocha D, García IA, González Montoro A, Llera A, Prato L, Girotti MR, Soria G, and Fernández EA

Subjects

Algorithms, Biomarkers, Tumor genetics, Breast Neoplasms genetics, Breast Neoplasms metabolism, Cell Differentiation drug effects, Cell Line, Tumor, Cell Proliferation drug effects, Cell Proliferation genetics, Centrosome metabolism, Cohort Studies, Databases, Genetic, Gene Expression Profiling, Humans, Inhibitory Concentration 50, Membrane Proteins genetics, Membrane Proteins metabolism, Mutation, Neoplasms genetics, Neoplasms mortality, Prognosis, Proportional Hazards Models, Receptor, ErbB-2 genetics, Receptor, ErbB-2 metabolism, Retinoblastoma Binding Proteins genetics, Tumor Suppressor Protein p53 genetics, Ubiquitin-Protein Ligases genetics, Biomarkers, Tumor metabolism, Cell Cycle Checkpoints genetics, Cell Differentiation genetics, DNA Damage genetics, Embryonic Stem Cells metabolism, Gene Expression Regulation, Neoplastic genetics, Neoplasms classification, Neoplasms metabolism

Abstract

Studying tissue-independent components of cancer and defining pan-cancer subtypes could be addressed using tissue-specific molecular signatures if classification errors are controlled. Since PAM50 is a well-known, United States Food and Drug Administration (FDA)-approved and commercially available breast cancer signature, we applied it with uncertainty assessment to classify tumor samples from over 33 cancer types, discarded unassigned samples, and studied the emerging tumor-agnostic molecular patterns. The percentage of unassigned samples ranged between 55.5% and 86.9% in non-breast tissues, and gene set analysis suggested that the remaining samples could be grouped into two classes (named C1 and C2) regardless of the tissue. The C2 class was more dedifferentiated, more proliferative, with higher centrosome amplification, and potentially more TP53 and RB1 mutations. We identified 28 gene sets and 95 genes mainly associated with cell-cycle progression, cell-cycle checkpoints, and DNA damage that were consistently exacerbated in the C2 class. In some cancer types, the C1/C2 classification was associated with survival and drug sensitivity, and modulated the prognostic meaning of the immune infiltrate. Our results suggest that PAM50 could be repurposed for a pan-cancer context when paired with uncertainty assessment, resulting in two classes with molecular, biological, and clinical implications.

Published

2020