Project description:Glioblastoma (GBM) is the most aggressive brain tumor and resistant to current available therapeutics, such as radiation. To improve the clinical efficacy, it is important to understand the cellular mechanisms underlying tumor responses to radiation. Here, we investigated long-term cellular responses of human GBM cells to ionizing radiation. Comparing to the initial response within 12 hours, gene expression modulation at 7 days after radiation is markedly different. While genes related to cell cycle arrest and DNA damage responses are mostly modulated at the initial stage; immune-related genes are specifically affected as the long-term effect. This later response is associated with increased cellular senescence and inhibition of transcriptional coactivator with PDZ-binding motif (TAZ). Mechanistically, TAZ inhibition does not depend on the canonical Hippo pathway, but relies on enhanced degradation mediated by the β-catenin destruction complex in the Wnt pathway. We further showed that depletion of TAZ by RNAi promotes radiation-induced senescence and growth arrest. Pharmacological activation of the β-catenin destruction complex is able to promote radiation-induced TAZ inhibition and growth arrest in these tumor cells. The correlation between senescence and reduced expression of YAP as well as β-catenin also occurs in human gliomas treated by radiation. Collectively, these findings suggested that inhibition of TAZ is involved in radiation-induced senescence and might benefit GBM radiotherapy.

Project description:Recently, senescence has been suggested as a defense mechanism to block sporadic induction of cancer cells. Radiation treatment induces proliferating cancer cells to turn into non-proliferating senescent cells in vitro. To characterize transcriptional reprogramming after radiation treatment, we measured the gene expression profiles of MCF7 at different time points after treatment. In these experiments, we found that IR induced premature senescence in MCF7 cells, and IR treatment resulted in significant changes in the expression of 305 marker genes (less than 1% FDR), which were strongly correlated (|r|>0.9) with IR treatment in a time-dependent manner. Functional analysis of these markers indicated that the dynamics of cytoskeletal structure and lysosomal activity gradually increased. The expression of marker genes for modulator proteins, that were responsible for the dynamics of actin stress fibers and focal adhesion, displayed a particularly strong positive correlation with senescence-associated (SA) morphological changes through time. We also observed a strong induction of genes related to lysosomal metabolic activity, which was accompanied by an increase in the number of SA-beta-Gal positive cells. However, the expression of genes for the cell cycle progression, the post-transcription and the translation activities gradually decreased after radiation treatment. Especially, we observed clear cell cycle arrest specifically at the S and G2/M phases with consistent down-regulation of genes for microtubule assembly/disassembly or spindle biogenesis. Gene expression profiles were obtained from human MCF7 cells after ionizing radiation (6 Gy) at day 0 (no ionizing radiation), day 1 (after ionizing radiation), day 2, day 3, and day 4.

Project description:ObjectiveIonizing radiation (IR) causes cardiac senescence, which eventually manifests as radiation-induced heart damage (RIHD). This study is aimed at exploring the mechanisms underlying IR-induced senescence using acetylation proteomics.MethodsIrradiated mouse hearts and H9C2 cells were harvested for senescence detection. Acetylation proteomics was used to investigate alterations in lysine acetylation. Atp5f1c acetylation after IR was verified using coimmunoprecipitation (Co-IP). Atp5f1c lysine 55 site acetylation (Atp5f1c K55-Ac) point mutation plasmids were used to evaluate the influence of Atp5f1c K55-Ac on energy metabolism and cellular senescence. Deacetylation inhibitors, plasmids, and siRNA transfection were used to determine the mechanism of Atp5f1c K55-Ac regulation.ResultsThe mice showed cardiomyocyte and cardiac aging phenotypes after IR. We identified 90 lysine acetylation sites from 70 protein alterations in the heart in response to IR. Hyperacetylated proteins are primarily involved in energy metabolism. Among them, Atp5f1c was hyperacetylated, as confirmed by Co-IP. Atp5f1c K55-Ac decreased ATP enzyme activity and synthesis. Atp5f1c K55 acetylation induced cardiomyocyte senescence, and Sirt4 and Sirt5 regulated Atp5f1c K55 deacetylation.ConclusionOur findings reveal a mechanism of RIHD through which Atp5f1c K55-Ac leads to cardiac aging and Sirt4 or Sirt5 modulates Atp5f1c acetylation. Therefore, the regulation of Atp5f1c K55-Ac might be a potential target for the treatment of RIHD.

Project description:Stress-induced cell senescence plays a crucial role in maintaining cardiac function after AMI, but the specific mechanism remains unclear. The objective of this study was to investigate the regulatory role of myocyte enhancer factor 2A (MEF2A) in cardiomyocyte senescence and its impact on cardiac function following AMI. Cardiomyocyte-specific MEF2A knockout mice (MEF2A-MyH6-CreErt2(f/f,+)) were generated, and their anterior descending branches were ligated to establish an AMI model. Ultrasound assessment of cardiac function 30 days post-AMI revealed that the specific knockout of MEF2A in cardiomyocytes worsened cardiac dysfunction and fibrosis, increased biomarkers of myocardial necrosis, and led to senescence in cardiomyocytes. Through high-throughput sequencing analysis of mRNA and protein in myocardial tissue from both MEF2A-MyH6-Creert2 (f/f,+) and wild-type mice, it was discovered that there was a decrease in expression levels for the enzymes of the cyclooxygenase (COX) family after MEF2A knockout. Additionally, KEGG analysis showed that differentially expressed genes were linked to cellular senescence processes . This suggests that MEF2A plays a regulatory role in cellular senescence through its interaction with the cox family. Meanwhile, COX inhibitors were found to weaken the beneficial effects of MEF2A overexpression on cardiomyocyte senescence in H9C2 cells. Our observations showed that knocking out MEF2A led to a decrease in H3K4me3 methylation levels and an increase in H3K4me3 antibody binding to specific cox family promoters when overexpressed. The use of MM102, a methylation inhibitor, nearly eliminated the positive effects of MEF2A overexpression on cell senescence, providing evidence that regulation of methylation is how MEF2A influences COX family expression changes. After screening, it was found that MEF2A can affect the methyltransferase activity partly by regulating the transcription level of SET1A subunit.

Project description:Ultraviolet B (UVB) radiation is a major contributor to skin photo-ageing. Although mainly absorbed by the epidermis, UVB photons managing to penetrate the upper dermis affect human dermal fibroblasts (HDFs), leading, among others, to the accumulation of senescent cells. In vitro studies have shown that repeated exposures to subcytotoxic UVB radiation doses provoke HDFs’ premature senescence shortly after the end of the treatment period. Here, we found that repetitive exposures to non-cytotoxic UVB radiation doses after several days lead to mixed cultures, containing both senescent cells and fibroblasts resisting senescence. “Resistant” fibroblasts were more resilient to a novel intense UVB radiation stimulus. RNA-seq analysis revealed that ERCC6, encoding Cockayne syndrome group B (CSB) protein, is upregulated in resistant HDFs compared to young and senescent cells, also confirmed at the protein level. CSB was found to be a key molecule conferring protection towards UVB cytotoxicity, as siRNA-mediated CSB loss-of-expression rendered HDFs significantly more susceptible to a high UVB radiation dose. In accordance, cells from a CSB-deficient patient were found to be dramatically more photosensitive. UVB-resistant HDFs remained normal (able to undergo replicative senescence) and non-tumorigenic. Even though they formed a distinct population in-between young and senescent cells, resistant HDFs retained numerous tissue-impairing characteristics of the senescence-associated secretory phenotype, including increased matrix metalloprotease activity and promotion of epidermoid tumor xenografts in immunodeficient mice. Collectively, here we describe a novel subpopulation of HDFs showing increased resistance to UVB-mediated premature senescence, as well as undesirable traits that may negatively affect skin homeostasis.

Project description:Stress-induced cell senescence plays a crucial role in maintaining cardiac function after AMI, but the specific mechanism remains unclear. The objective of this study was to investigate the regulatory role of myocyte enhancer factor 2A (MEF2A) in cardiomyocyte senescence and its impact on cardiac function following AMI. Cardiomyocyte-specific MEF2A knockout mice (MEF2A-MyH6-CreErt2(f/f,+)) were generated, and their anterior descending branches were ligated to establish an AMI model. Ultrasound assessment of cardiac function 30 days post-AMI revealed that the specific knockout of MEF2A in cardiomyocytes worsened cardiac dysfunction and fibrosis, increased biomarkers of myocardial necrosis, and led to senescence in cardiomyocytes. Through high-throughput sequencing analysis of mRNA and protein in myocardial tissue from both MEF2A-MyH6-Creert2 (f/f,+) and wild-type mice, it was discovered that there was a decrease in expression levels for the enzymes of the cyclooxygenase (COX) family after MEF2A knockout. Additionally, KEGG analysis showed that differentially expressed genes were linked to cellular senescence processes . This suggests that MEF2A plays a regulatory role in cellular senescence through its interaction with the cox family. Meanwhile, COX inhibitors were found to weaken the beneficial effects of MEF2A overexpression on cardiomyocyte senescence in H9C2 cells. Our observations showed that knocking out MEF2A led to a decrease in H3K4me3 methylation levels and an increase in H3K4me3 antibody binding to specific cox family promoters when overexpressed. The use of MM102, a methylation inhibitor, nearly eliminated the positive effects of MEF2A overexpression on cell senescence, providing evidence that regulation of methylation is how MEF2A influences COX family expression changes. After screening, it was found that MEF2A can affect the methyltransferase activity  partly by regulating the transcription level of SET1A subunit.

Project description:Noncompaction cardiomyopathy is a common congenital cardiomyopathy associated with a deficiency of ventricular cardiomyocytes and impaired pump function. The genetic basis and underlying mechanisms of this disorder remain elusive. Polyploidization is an intrinsic feature of mammalian cardiomyocytes, which occurs shortly after birth and is accompanied by cardiomyocyte cell cycle arrest. We show that genetic deletion of the RNA binding protein with multiple splicing (Rbpms) in mice results in premature onset of cardiomyocyte polyploidization (binucleation) and consequent noncompaction cardiomyopathy. A similar blockade to cytokinesis occurs in human iPSC-derived cardiomyocytes with RBPMS gene deletion. Paired-end RNA sequencing analysis revealed that Rbpms plays an essential role in RNA splicing and mediates isoform switching from the short to the long form of Pdlim5, a heart-specific LIM domain protein that connects the sarcomere with various signaling proteins during heart development. The loss of Rbpms leads to abnormal accumulation of short Pdlim5 isoforms that disrupt cardiomyocyte cytokinesis. Our results link premature cardiomyocyte binucleation to noncompaction cardiomyopathy and highlight the central role of Rbpms in this process.

Project description:We generated cardiomyocyte-specific Aars2 knockout mice using Myh6-Cre, and observed progressive cardiac function decline starting at postnatal day (P) 28, with severe chamber dilation, and phenotypes reminance of mitochondrial cardiomyopathy. All homozygous mutant mice died before reaching P70. We sought to identify the transcriptome changes by Aars2-deficiency at P14 and P21 in adult, prior to the onset of the cardiomyopathy.

Project description:Recently, senescence has been suggested as a defense mechanism to block sporadic induction of cancer cells. Radiation treatment induces proliferating cancer cells to turn into non-proliferating senescent cells in vitro. To characterize transcriptional reprogramming after radiation treatment, we measured the gene expression profiles of MCF7 at different time points after treatment. In these experiments, we found that IR induced premature senescence in MCF7 cells, and IR treatment resulted in significant changes in the expression of 305 marker genes (less than 1% FDR), which were strongly correlated (|r|>0.9) with IR treatment in a time-dependent manner. Functional analysis of these markers indicated that the dynamics of cytoskeletal structure and lysosomal activity gradually increased. The expression of marker genes for modulator proteins, that were responsible for the dynamics of actin stress fibers and focal adhesion, displayed a particularly strong positive correlation with senescence-associated (SA) morphological changes through time. We also observed a strong induction of genes related to lysosomal metabolic activity, which was accompanied by an increase in the number of SA-beta-Gal positive cells. However, the expression of genes for the cell cycle progression, the post-transcription and the translation activities gradually decreased after radiation treatment. Especially, we observed clear cell cycle arrest specifically at the S and G2/M phases with consistent down-regulation of genes for microtubule assembly/disassembly or spindle biogenesis.

Project description:Radiation lung injury is characterized by early inflammation and late fibrosis. The causes underlying the chronic, progressive nature of radiation injury are poorly understood. Here, we report that the gene expression of irradiated lung tissue correlates with that observed in the lungs in aged animals. We demonstrate that NOX4 expression and superoxide elaboration is increased in irradiated lungs and pneumocytes in a dose dependent fashion. We used microarrays to detail the global programme of gene expression and report that irradiated lung tissue correlates with that observed in the lungs in aged animals. Female C57Bl/Ncr mice, aged 10 weeks were treated with/ without radiation to the thorax with a X-RAD 320 x-ray irradiator at a dose rate of 2.61 Gy/minute. An age-matched cohort of mice received no IR while additional cohorts received 5 Gy in a single dose, 17.5 Gy in a single dose. RNA was extracted and hybridization done on Affymetrix Mouse430_2 microarrays.