Your search keyword '"Feldmesser, Ester"' showing total 30 results

1. miR‐4734 conditionally suppresses ER stress‐associated proinflammatory responses.

Author

Michael, Dan, Feldmesser, Ester, Gonen, Chagay, Furth, Noa, Maman, Alexander, Heyman, Ori, Argoetti, Amir, Tofield, Adin, Baichman‐Kass, Amichai, Ben‐Dov, Aviyah, Benbenisti, Dan, Hen, Nadav, Rotkopf, Ron, Ganci, Federica, Blandino, Giovanni, Ulitsky, Igor, and Oren, Moshe

Subjects

*GENE expression, *ENDOPLASMIC reticulum, *GENETIC overexpression, *GENES, *FIBROBLASTS

Abstract

Prolonged metabolic stress can lead to severe pathologies. In metabolically challenged primary fibroblasts, we assigned a novel role for the poorly characterized miR‐4734 in restricting ATF4 and IRE1‐mediated upregulation of a set of proinflammatory cytokines and endoplasmic reticulum stress‐associated genes. Conversely, inhibition of this miRNA augmented the expression of those genes. Mechanistically, miR‐4734 was found to restrict the expression of the transcriptional activator NF‐kappa‐B inhibitor zeta (NFKBIZ), which is required for optimal expression of the proinflammatory genes and whose mRNA is targeted directly by miR‐4734. Concordantly, overexpression of NFKBIZ compromised the effects of miR‐4734, underscoring the importance of this direct targeting. As the effects of miR‐4734 were evident under stress but not under basal conditions, it may possess therapeutic utility towards alleviating stress‐induced pathologies. [ABSTRACT FROM AUTHOR]

Published

2023

2. An Emiliania huxleyi pan-transcriptome reveals basal strain specificity in gene expression patterns.

Author

Feldmesser, Ester, Ben-Dor, Shifra, and Vardi, Assaf

Subjects

*COCCOLITHUS huxleyi, *GENE expression, *VIRUS diseases, *SULFUR cycle, *CARBON cycle, *MICROBIAL communities, *BIOGEOCHEMICAL cycles

Abstract

Emiliania huxleyi is a cosmopolitan coccolithophore widespread in temperate oceans. This unicellular photoautotroph forms massive recurring blooms that play an important role in large biogeochemical cycles of carbon and sulfur, which play a role in climate change. The mechanism of bloom formation and demise, controlled by giant viruses that routinely infect these blooms, is poorly understood. We generated a pan-transcriptome of E. huxleyi, derived from three strains with different susceptibility to viral infection. Expression profiling of E. huxleyi sensitive and resistant strains showed major basal differences, including many genes that are induced upon viral infection. This suggests that basal gene expression can affect the host metabolic state and the susceptibility of E. huxleyi to viruses. Due to its ecological importance, the pan-transcriptome and its protein translation, applicable to many E. huxleyi strains, is a powerful resource for investigation of eukaryotic microbial communities. [ABSTRACT FROM AUTHOR]

Published

2021

3. The molecular mechanisms that determine different degrees of polyphagy in the Bemisia tabaci species complex.

Author

Malka, Osnat, Feldmesser, Ester, Brunschot, Sharon, Santos‐Garcia, Diego, Han, Wen‐Hao, Seal, Susan, Colvin, John, and Morin, Shai

Subjects

*SWEETPOTATO whitefly, *CASSAVA, *SPECIES, *GENES, *BIOLOGICAL transport, *CELLULAR signal transduction

Abstract

The whitefly Bemisia tabaci is a closely related group of >35 cryptic species that feed on the phloem sap of a broad range of host plants. Species in the complex differ in their host‐range breadth, but the mechanisms involved remain poorly understood. We investigated, therefore, how six different B. tabaci species cope with the environmental unpredictability presented by a set of four common and novel host plants. Behavioral studies indicated large differences in performances on the four hosts and putative specialization of one of the species to cassava plants. Transcriptomic analyses revealed two main insights. First, a large set of genes involved in metabolism (>85%) showed differences in expression between the six species, and each species could be characterized by its own unique expression pattern of metabolic genes. However, within species, these genes were constitutively expressed, with a low level of environmental responsiveness (i.e., to host change). Second, within each species, sets of genes mainly associated with the super‐pathways "environmental information processing" and "organismal systems" responded to the host switching events. These included genes encoding for proteins involved in sugar homeostasis, signal transduction, membrane transport, and immune, endocrine, sensory and digestive responses. Our findings suggested that the six B. tabaci species can be divided into four performance/transcriptomic "Types" and that polyphagy can be achieved in multiple ways. However, polyphagy level is determined by the specific identity of the metabolic genes/pathways that are enriched and overexpressed in each species (the species' individual metabolic "tool kit"). [ABSTRACT FROM AUTHOR]

Published

2021

4. Using Synthetic Mouse Spike-In Transcripts to Evaluate RNA-Seq Analysis Tools.

Author

Leshkowitz, Dena, Feldmesser, Ester, Friedlander, Gilgi, Jona, Ghil, Ainbinder, Elena, Parmet, Yisrael, and Horn-Saban, Shirley

Subjects

*RNA sequencing, *GENETIC transcription, *NUCLEOTIDE sequencing, *ALTERNATIVE RNA splicing, *GENE expression, *LABORATORY mice

Abstract

One of the key applications of next-generation sequencing (NGS) technologies is RNA-Seq for transcriptome genome-wide analysis. Although multiple studies have evaluated and benchmarked RNA-Seq tools dedicated to gene level analysis, few studies have assessed their effectiveness on the transcript-isoform level. Alternative splicing is a naturally occurring phenomenon in , significantly increasing the of proteins that can be encoded by the genome. The aim of this study was to assess and compare the ability of the bioinformatics approaches and tools to assemble, quantify and detect differentially expressed transcripts using RNA-Seq data, in a controlled experiment. To this end, in vitro synthesized mouse spike-in control transcripts were added to the total RNA of differentiating mouse embryonic bodies, and their expression patterns were measured. This novel approach was used to assess the accuracy of the tools, as established by comparing the observed results versus the results expected of the mouse controlled spiked-in transcripts. We found that detection of differential expression at the gene level is adequate, yet on the transcript-isoform level, all tools tested lacked . [ABSTRACT FROM AUTHOR]

Published

2016

5. Improving transcriptome construction in non-model organisms: integrating manual and automated gene definition in Emiliania huxleyi.

Author

Feldmesser, Ester, Rosenwasser, Shilo, Vardi, Assaf, and Ben-Dor, Shifra

Subjects

*COCCOLITHUS huxleyi, *GENETIC transcription, *NUCLEOTIDE sequence, *MARINE biotechnology, *GENOMES

Abstract

Background The advent of Next Generation Sequencing technologies and corresponding bioinformatics tools allows the definition of transcriptomes in non-model organisms. Non-model organisms are of great ecological and biotechnological significance, and consequently the understanding of their unique metabolic pathways is essential. Several methods that integrate de novo assembly with genome-based assembly have been proposed. Yet, there are many open challenges in defining genes, particularly where genomes are not available or incomplete. Despite the large numbers of transcriptome assemblies that have been performed, quality control of the transcript building process, particularly on the protein level, is rarely performed if ever. To test and improve the quality of the automated transcriptome reconstruction, we used manually defined and curated genes, several of them experimentally validated. Results Several approaches to transcript construction were utilized, based on the available data: a draft genome, high quality RNAseq reads, and ESTs. In order to maximize the contribution of the various data, we integrated methods including de novo and genome based assembly, as well as EST clustering. After each step a set of manually curated genes was used for quality assessment of the transcripts. The interplay between the automated pipeline and the quality control indicated which additional processes were required to improve the transcriptome reconstruction. We discovered that E. huxleyi has a very high percentage of non-canonical splice junctions, and relatively high rates of intron retention, which caused unique issues with the currently available tools. While individual tools missed genes and artificially joined overlapping transcripts, combining the results of several tools improved the completeness and quality considerably. The final collection, created from the integration of several quality control and improvement rounds, was compared to the manually defined set both on the DNA and protein levels, and resulted in an improvement of 20% versus any of the read-based approaches alone. Conclusions To the best of our knowledge, this is the first time that an automated transcript definition is subjected to quality control using manually defined and curated genes and thereafter the process is improved. We recommend using a set of manually curated genes to troubleshoot transcriptome reconstruction. [ABSTRACT FROM AUTHOR]

Published

2014

6. Mutations in Olfactory Signal Transduction Genes Are Not a Major Cause of Human Congenital General Anosmia.

Author

Feldmesser, Ester, Bercovich, Dani, Avidan, Nili, Halbertal, Shmuel, Haim, Liora, Gross-Isseroff, Ruth, Goshen, Sivan, and Lancet, Doron

Subjects

*ANOSMIA, *QUALITY of life, *ADENOSINE monophosphate, *OLFACTORY receptors, *CARRIER proteins

Abstract

Anosmia affects the western world population, mostly the elderly, reaching to 5% in subjects over the age of 45 years and strongly lowering their quality of life. A smaller minority (about 0.01%) is born without a sense of smell, afflicted with congenital general anosmia (CGA). No causative genes for human CGA have been identified yet, except for some syndromic cases such as Kallman syndrome. In mice, however, deletion of any of the 3 main olfactory transduction components (guanidine triphosphate binding protein, adenylyl cyclase, and the cyclic adenosine monophosphate–gated channel) causes profound reduction of physiological responses to odorants. In an attempt to identify human CGA-related mutations, we performed whole-genome linkage analysis in affected families, but no significant linkage signals were observed, probably due to the small size of families analyzed. We further carried out direct mutation screening in the 3 main olfactory transduction genes in 64 unrelated anosmic individuals. No potentially causative mutations were identified, indicating that transduction gene variations underlie human CGA rarely and that mutations in other genes have to be identified. The screened genes were found to be under purifying selection, suggesting that they play a crucial functional role not only in olfaction but also potentially in additional pathways. [ABSTRACT FROM AUTHOR]

Published

2007

7. Gene Expression in 1-Methylcyclopropene (1-MCP) Treated Tomatoes during Pre-Climacteric Ripening Suggests Shared Regulation of Methionine Biosynthesis, Ethylene Production and Respiration.

Author

Gamrasni, Dan, Feldmesser, Ester, Ben-Arie, Ruth, Raz, Amir, Tabatznik Asiag, Amit, Glikman, Michal, Aharoni, Asaph, and Goldway, Martin

Subjects

*FRUIT ripening, *ETHYLENE, *1-Methylcyclopropene, *GENE expression, *METHIONINE, *RESPIRATION

Abstract

The physiology of fruit ripening is defined as either 'climacteric' or 'non-climacteric'. In climacteric fruit respiration during ripening increases until it reaches a peak, which is accompanied by an increase in autocatalytic ethylene production, whereas the respiration of non-climacteric fruit does not increase and they have no requirement for ethylene to complete their ripening. In an attempt to gain further insight into the involvement of autocatalytic ethylene production with the climacteric rise in respiration, tomato fruit were harvested at three defined stages of maturity prior to the climacteric peak (mature green, breaker, and early orange) and immediately exposed to the gaseous molecule 1-methylcyclopropene (1-MCP). The gene expression profile at each of these stages was monitored after 24 h, using an Affymetrix tomato microarray chip. This approach enabled us to identify ethylene responsive genes that are commonly regulated at early stages of ripening, as well as new candidate genes. In addition, 1-MCP treatment affected the levels of metabolites related to methionine biosynthesis. Methionine feeds climacteric ethylene production and we found that promotors of the genes of enzymes that catalyze the production of homoserine and homocysteine (aspartokinase/homoserine dehydrogenases and cystathionine beta lyase, respectively), precursors in the methionine pathway, contain the AtSR1 binding motif. This binding motif is recognized by ethylene activated transcription factors, hence indicating a role for ethylene in methionine synthesis during early ripening, explaining the autocatalytic ethylene production during subsequent ripening stages. [ABSTRACT FROM AUTHOR]

Published

2020

8. Rapid starch degradation in the wood of olive trees under heat and drought is permitted by three stress‐specific beta amylases.

Author

Tsamir‐Rimon, Mor, Ben‐Dor, Shifra, Feldmesser, Ester, Oppenhimer‐Shaanan, Yaara, David‐Schwartz, Rakefet, Samach, Alon, and Klein, Tamir

Subjects

*OLIVE, *STARCH, *STARCH metabolism, *METABOLIC regulation, *GENE families, *AMYLASES

Abstract

Summary: Carbon reserve use is a major drought response in trees, enabling tree survival in conditions prohibiting photosynthesis. However, regulation of starch metabolism under drought at the whole‐tree scale is still poorly understood.To this end, we combined measurements of nonstructural carbohydrates (NSCs), tree physiology and gene expression. The experiment was conducted outside on olive trees in pots under 90 d of seasonal spring to summer warming. Half of the trees were also subjected to limited water conditions for 28 d.Photosynthesis decreased in dehydrating trees from 19 to 0.5 µmol m−2 s−1 during the drought period. Starch degradation and mannitol production were a major drought response, with mannitol increasing to 71% and 41% out of total NSCs in shoots and roots, respectively. We identified the gene family members potentially relevant either to long‐term or stress‐induced carbon storage. Partitioning of expression patterns among β amylase and starch synthase family members was observed, with three β amylases possibly facilitating the rapid starch degradation under heat and drought.Our results suggest a group of stress‐related, starch metabolism genes, correlated with NSC fluctuations during drought and recovery. The daily starch metabolism gene expression was different from the stress‐mode starch metabolism pattern, where some genes are uniquely expressed during the stress‐mode response. [ABSTRACT FROM AUTHOR]

Published

2021

9. Major differences in microRNA quantification are platform and sequence dependent.

Author

Feldmesser, Ester, Leshkowitz, Dena, Parmet, Yisrael, and Horn-Saban, Shirley

Subjects

*MICRORNA

Abstract

An abstract of the conference paper "Major differences in microRNA quantification are platform and sequence dependent," by Ester Feldmesser and colleagues is presented.

Published

2012

10. Species‐complex diversification and host‐plant associations in Bemisia tabaci: A plant‐defence, detoxification perspective revealed by RNA‐Seq analyses.

Author

Malka, Osnat, Santos‐Garcia, Diego, Feldmesser, Ester, Sharon, Elad, Krause‐Sakate, Renate, Delatte, Hélène, Brunschot, Sharon, Patel, Mitulkumar, Visendi, Paul, Mugerwa, Habibu, Seal, Susan, Colvin, John, and Morin, Shai

Subjects

*SWEETPOTATO whitefly, *SPECIES diversity, *PLANT species, *GENE expression, *RNA sequencing, *PHYLOGENY

Abstract

Insect–plant associations and their role in diversification are mostly studied in specialists. Here, we aimed to identify macroevolution patterns in the relationships between generalists and their host plants that have the potential to promote diversification. We focused on the Bemisia tabaci species complex containing more than 35 cryptic species. Mechanisms for explaining this impressive diversification have focused so far on allopatric forces that assume a common, broad, host range. We conducted a literature survey which indicated that species in the complex differ in their host range, with only few showing a truly broad one. We then selected six species, representing different phylogenetic groups and documented host ranges. We tested whether differences in the species expression profiles of detoxification genes are shaped more by their phylogenetic relationships or by their ability to successfully utilize multiple hosts, including novel ones. Performance assays divided the six species into two groups of three, one showing higher performance on various hosts than the other (the lower performance group). The same grouping pattern appeared when the species were clustered according to their expression profiles. Only species placed in the lower performance group showed a tendency to lower the expression of multiple genes. Taken together, these findings bring evidence for the existence of a common detoxification "machinery," shared between species that can perform well on multiple hosts. We raise the possibility that this "machinery" might have played a passive role in the diversification of the complex, by allowing successful migration to new/novel environments, leading, in some cases, to fragmentation and speciation. [ABSTRACT FROM AUTHOR]

Published

2018

11. VSV-ΔG-Spike Candidate Vaccine Induces Protective Immunity and Protects K18-hACE2 Mice against SARS-CoV-2 Variants.

Author

Yahalom-Ronen, Yfat, Tamir, Hadas, Melamed, Sharon, Politi, Boaz, Achdout, Hagit, Erez, Noam, Israeli, Ofir, Cohen-Gihon, Inbar, Chery Mimran, Lilach, Barlev-Gross, Moria, Mandelboim, Michal, Orr, Irit, Feldmesser, Ester, Weiss, Shay, Beth-Din, Adi, Paran, Nir, and Israely, Tomer

Subjects

*SARS-CoV-2, *MICE, *VIRAL load, *VACCINES, *IMMUNITY, *IMMUNE response

Abstract

Since the emergence of the original SARS-CoV-2, several variants were described, raising questions as to the ability of recently developed vaccine platforms to induce immunity and provide protection against these variants. Here, we utilized the K18-hACE2 mouse model to show that VSV-ΔG-spike vaccination provides protection against several SARS-CoV-2 variants: alpha, beta, gamma, and delta. We show an overall robust immune response, regardless of variant identity, leading to reduction in viral load in target organs, prevention of morbidity and mortality, as well as prevention of severe brain immune response, which follows infection with various variants. Additionally, we provide a comprehensive comparison of the brain transcriptomic profile in response to infection with different variants of SARS-CoV-2 and show how vaccination prevents these disease manifestations. Taken together, these results highlight the robust VSV-ΔG-spike protective response against diverse SARS-CoV-2 variants, as well as its promising potential against newly arising variants. [ABSTRACT FROM AUTHOR]

Published

2023

12. Identification of the algal dimethyl sulfide--releasing enzyme: A missing link in the marine sulfur cycle.

Author

Alcolombri, Uria, Ben-Dor, Shifra, Feldmesser, Ester, Levin, Yishai, Tawfik, Dan S., and Vardi, Assaf

Subjects

*DIMETHYLPROPIOTHETIN, *SULFUR cycle, *DIMETHYL sulfide, *LYASES, *COCCOLITHUS huxleyi, *MARINE food chain, *SEQUENCE alignment

Abstract

The article discusses research on the identification of the dimethylsulfoniopropionate (DMSP) lyase Alma1 from the bloom-forming algae Emiliania huxleyi which releases dimethyl sulfide (DMS) into the atmosphere. Topics include the role of DMSP in marine food webs and the marine sulfur cycle, the use of sequence homology to determine that Alma1 is present a wide array of phytoplankton and marine organisms, and the impact of DMS on cloud formation.

Published

2015

13. Effects of ethylene degreening on the transcriptome of mandarin flesh

Author

Mayuoni, Lina, Sharabi-Schwager, Michal, Feldmesser, Ester, and Porat, Ron

Subjects

*ETHYLENE, *CITRUS fruit coloring, *TRANSCRIPTION factors, *GENE expression, *HIGH temperatures, *FRUIT quality, *METABOLISM, *FOOD of animal origin, *MOLECULAR structure

Abstract

Abstract: The commercial practice of degreening citrus fruit by exposure to ethylene was developed to accelerate peel color development, but little is yet known about its putative effects on the edible flesh. To improve our understanding of the molecular mechanisms involved in the responses of mandarin flesh to ethylene degreening, we performed genome-wide transcriptional profiling analysis with the Affymetrix Citrus GeneChip®. Overall, out of 30,171 probe sets representing citrus transcripts on the microarray, we found that expression of 734 probe sets was significantly (q ≤0.01) altered by factors of at least 3 by exposure to air or 4μLL−1 ethylene for 48h at 20°C. One-way ANOVA pair-wise comparisons revealed 163 probe sets that were affected by exposure both to air and to ethylene, 498 sets that were affected only by ethylene, and 73 that were affected only by air. Overall, keeping the fruit at 20°C for 48h without ethylene led to an arrest of general cellular and metabolic activity. In contrast, exposure to ethylene stimulated adaptation processes that involved induction of gene expression related to carbohydrate, amino acid, secondary and hormone metabolism, stress and defense, and activation of regulatory processes, including transcription regulation and protein posttranslational modifications. In light of these observations, we propose that ethylene degreening simultaneously stimulates two independent processes in mandarin flesh: on the one hand, storing the fruit at a relatively high temperature of 20°C resulted in suppression of gene expression and overall metabolic arrest whereas, on the other hand, exposure to ethylene activated gene expression and stimulated various adaptation and metabolic processes, which might impact on fruit internal and nutritional quality. [Copyright &y& Elsevier]

Published

2011

14. Combined presentation and immunogenicity analysis reveals a recurrent RAS.Q61K neoantigen in melanoma.

Author

Peri, Aviyah, Greenstein, Erez, Alon, Michal, Pai, Joy A., Dingjan, Tamir, Reich-Zeliger, Shlomit, Barnea, Eilon, Barbolin, Chaya, Levy, Ronen, Arnedo-Pac, Claudia, Kalaora, Shelly, Dassa, Bareket, Feldmesser, Ester, Shang, Ping, Greenberg, Polina, Levin, Yishai, Benedek, Gil, Levesque, Mitchell P., Adams, David J., and Lotem, Michal

Subjects

*IMMUNE response, *T cell receptors, *TUMOR-infiltrating immune cells, *PEPTIDES, *T cells

Abstract

Neoantigens are now recognized drivers of the antitumor immune response. Recurrent neoantigens, shared among groups of patients, have thus become increasingly coveted therapeutic targets. Here, we report on the data-driven identification of a robustly presented, immunogenic neoantigen that is derived from the combination of HLA-A*01:01 and RAS.Q61K. Analysis of large patient cohorts indicated that this combination applies to 3% of patients with melanoma. Using HLA peptidomics, we were able to demonstrate robust endogenous presentation of the neoantigen in 10 tumor samples. We detected specific reactivity to the mutated peptide within tumor-infiltrating lymphocytes (TILs) from 2 unrelated patients, thus confirming its natural immunogenicity. We further investigated the neoantigen-specific clones and their T cell receptors (TCRs) via a combination of TCR sequencing, TCR overexpression, functional assays, and single-cell transcriptomics. Our analysis revealed a diverse repertoire of neoantigen-specific clones with both intra- and interpatient TCR similarities. Moreover, 1 dominant clone proved to cross-react with the highly prevalent RAS.Q61R variant. Transcriptome analysis revealed a high association of TCR clones with specific T cell phenotypes in response to cognate melanoma, with neoantigen-specific cells showing an activated and dysfunctional phenotype. Identification of recurrent neoantigens and their reactive TCRs can promote “off-theshelf” precision immunotherapies, alleviating limitations of personalized treatments. [ABSTRACT FROM AUTHOR]

Published

2021

15. Activation and detoxification of cassava cyanogenic glucosides by the whitefly Bemisia tabaci.

Author

Easson, Michael L. A. E., Malka, Osnat, Paetz, Christian, Hojná, Anna, Reichelt, Michael, Stein, Beate, van Brunschot, Sharon, Feldmesser, Ester, Campbell, Lahcen, Colvin, John, Winter, Stephan, Morin, Shai, Gershenzon, Jonathan, and Vassão, Daniel G.

Subjects

*CASSAVA, *GLUCOSIDES, *SWEETPOTATO whitefly, *PLANT defenses, *HERBIVORES

Abstract

Two-component plant defenses such as cyanogenic glucosides are produced by many plant species, but phloem-feeding herbivores have long been thought not to activate these defenses due to their mode of feeding, which causes only minimal tissue damage. Here, however, we report that cyanogenic glycoside defenses from cassava (Manihot esculenta), a major staple crop in Africa, are activated during feeding by a pest insect, the whitefly Bemisia tabaci, and the resulting hydrogen cyanide is detoxified by conversion to beta-cyanoalanine. Additionally, B. tabaci was found to utilize two metabolic mechanisms to detoxify cyanogenic glucosides by conversion to non-activatable derivatives. First, the cyanogenic glycoside linamarin was glucosylated 1–4 times in succession in a reaction catalyzed by two B. tabaci glycoside hydrolase family 13 enzymes in vitro utilizing sucrose as a co-substrate. Second, both linamarin and the glucosylated linamarin derivatives were phosphorylated. Both phosphorylation and glucosidation of linamarin render this plant pro-toxin inert to the activating plant enzyme linamarase, and thus these metabolic transformations can be considered pre-emptive detoxification strategies to avoid cyanogenesis. [ABSTRACT FROM AUTHOR]

Published

2021

16. UTAP: User-friendly Transcriptome Analysis Pipeline.

Author

Kohen, Refael, Barlev, Jonathan, Hornung, Gil, Stelzer, Gil, Feldmesser, Ester, Kogan, Kiril, Safran, Marilyn, and Leshkowitz, Dena

Subjects

*RNA sequencing, *GENE expression, *BIOINFORMATICS, *MEDICAL research, *TRANSCRIPTOMES

Abstract

Background: RNA-Seq technology is routinely used to characterize the transcriptome, and to detect gene expression differences among cell types, genotypes and conditions. Advances in short-read sequencing instruments such as Illumina Next-Seq have yielded easy-to-operate machines, with high throughput, at a lower price per base. However, processing this data requires bioinformatics expertise to tailor and execute specific solutions for each type of library preparation. Results: In order to enable fast and user-friendly data analysis, we developed an intuitive and scalable transcriptome pipeline that executes the full process, starting from cDNA sequences derived by RNA-Seq [Nat Rev Genet 10:57-63, 2009] and bulk MARS-Seq [Science 343:776-779, 2014] and ending with sets of differentially expressed genes. Output files are placed in structured folders, and results summaries are provided in rich and comprehensive reports, containing dozens of plots, tables and links. Conclusion: Our User-friendly Transcriptome Analysis Pipeline (UTAP) is an open source, web-based intuitive platform available to the biomedical research community, enabling researchers to efficiently and accurately analyse transcriptome sequence data. [ABSTRACT FROM AUTHOR]

Published

2019

17. An ensemble of regulatory elements controls Runx3 spatiotemporal expression in subsets of dorsal root ganglia proprioceptive neurons.

Author

Appel, Elena, Weissmann, Sarit, Salzberg, Yehuda, Orlovsky, Kira, Negreanu, Varda, Tsoory, Michael, Raanan, Calanit, Feldmesser, Ester, Bernstein, Yael, Wolstein, Orit, Levanon, Ditsa, and Groner, Yoram

Subjects

*RUNX proteins, *GENE expression, *DORSAL root ganglia, *NEURONS, *SPATIOTEMPORAL processes

Abstract

The Runx3 transcription factor is essential for development and diversification of the dorsal root ganglia (DRGs) TrkC sensory neurons. In Runx3-deficient mice, developing TrkC neurons fail to extend central and peripheral afferents, leading to cell death and disruption of the stretch reflex circuit, resulting in severe limb ataxia. Despite its central role, the mechanisms underlying the spatiotemporal expression specificities of Runx3 in TrkC neurons were largely unknown. Here we first defined the genomic transcription unit encompassing regulatory elements (REs) that mediate the tissue-specific expression of Runx3. Using transgenic mice expressing BAC reporters spanning the Runx3 locus, we discovered three REs--dubbed R1, R2, and R3--that cross-talk with promoter-2 (P2) to drive TrkC neuron-specific Runx3 transcription. Deletion of single or multiple elements either in the BAC transgenics or by CRISPR/Cas9-mediated endogenous ablation established the REs' ability to promote and/or repress Runx3 expression in developing sensory neurons. Our analysis reveals that an intricate combinatorial interplay among the three REs governs Runx3 expression in distinct subtypes of TrkC neurons while concomitantly extinguishing its expression in non-TrkC neurons. These findings provide insights into the mechanism regulating cell type-specific expression and subtype diversification of TrkC neurons in developing DRGs. [ABSTRACT FROM AUTHOR]

Published

2016

18. Cap-independent translation by DAP5 controls cell fate decisions in human embryonic stem cells.

Author

Yoffe, Yael, David, Maya, Kalaora, Rinat, Povodovski, Lital, Bialik, Shani, Kimchi, Adi, Friedlander, Gilgi, Feldmesser, Ester, Ainbinder, Elena, and Saada, Ann

Subjects

*HUMAN embryonic stem cells, *PLURIPOTENT stem cells, *PROTEIN synthesis, *MESSENGER RNA, *GENETIC translation, *HUMAN chromatin

Abstract

Multiple transcriptional and epigenetic changes drive differentiation of embryonic stem cells (ESCs). This study unveils an additional level of gene expression regulation involving noncanonical, cap-independent translation of a select group of mRNAs. This is driven by deathassociated protein 5 (DAP5/eIF4G2/NAT1), a translation initiation factor mediating IRES-dependent translation. We found that the DAP5 knockdown from human ESCs (hESCs) resulted in persistence of pluripotent gene expression, delayed induction of differentiation-associated genes in different cell lineages, and defective embryoid body formation. The latter involved improper cellular organization, lack of cavitation, and enhanced mislocalized apoptosis. RNA sequencing of polysome-associated mRNAs identified candidates with reduced translation efficiency in DAP5- depleted hESCs. These were enriched in mitochondrial proteins involved in oxidative respiration, a pathway essential for differentiation, the significance of which was confirmed by the aberrant mitochondrial morphology and decreased oxidative respiratory activity in DAP5 knockdown cells. Further analysis identified the chromatin modifier HMGN3 as a cap-independent DAP5 translation target whose knockdown resulted in defective differentiation. Thus, DAP5-mediated translation of a specific set of proteins is critical for the transition from pluripotency to differentiation, highlighting the importance of cap-independent translation in stem cell fate decisions. [ABSTRACT FROM AUTHOR]

Published

2016

19. Runx1 Transcription Factor Is Required for Myoblasts Proliferation during Muscle Regeneration.

Author

Umansky, Kfir Baruch, Gruenbaum-Cohen, Yael, Tsoory, Michael, Feldmesser, Ester, Goldenberg, Dalia, Brenner, Ori, and Groner, Yoram

Subjects

*TRANSCRIPTION factors, *MYOBLASTS, *CELL proliferation, *CELL differentiation, *REGENERATION (Biology), *HISTONE genetics

Abstract

Following myonecrosis, muscle satellite cells proliferate, differentiate and fuse, creating new myofibers. The Runx1 transcription factor is not expressed in naïve developing muscle or in adult muscle tissue. However, it is highly expressed in muscles exposed to myopathic damage yet, the role of Runx1 in muscle regeneration is completely unknown. Our study of Runx1 function in the muscle’s response to myonecrosis reveals that this transcription factor is activated and cooperates with the MyoD and AP-1/c-Jun transcription factors to drive the transcription program of muscle regeneration. Mice lacking dystrophin and muscle Runx1 (mdx-/Runx1f/f), exhibit impaired muscle regeneration leading to age-dependent muscle waste, gradual decrease in motor capabilities and a shortened lifespan. Runx1-deficient primary myoblasts are arrested at cell cycle G1 and consequently differentiate. Such premature differentiation disrupts the myoblasts’ normal proliferation/differentiation balance, reduces the number and size of regenerating myofibers and impairs muscle regeneration. Our combined Runx1-dependent gene expression, ChIP-seq, ATAC-seq and histone H3K4me1/H3K27ac modification analyses revealed a subset of Runx1-regulated genes that are co-occupied by MyoD and c-Jun in mdx-/Runx1f/f muscle. The data provide unique insights into the transcriptional program driving muscle regeneration and implicate Runx1 as an important participant in the pathology of muscle wasting diseases. [ABSTRACT FROM AUTHOR]

Published

2015

20. Rewiring Host Lipid Metabolism by Large Viruses Determines the Fate of Emiliania huxleyi, a Bloom-Forming Alga in the Ocean.

Author

Rosenwasser, Shilo, Mausz, Michaela A., Schatz, Daniella, Sheyn, Uri, Malitsky, Sergey, Aharoni, Asaph, Weinstock, Eyal, Tzfadia, Oren, Ben-Dor, Shifra, Feldmesser, Ester, Pohnert, Georg, and Vardi, Assaf

Subjects

*LIPID metabolism, *COCCOLITHUS huxleyi, *LIFE cycles (Biology), *OCEAN, *ARMS race, *ALGAE

Abstract

Marine viruses are major ecological and evolutionary drivers of microbial food webs regulating the fate of carbon in the ocean. We combined transcriptomic and metabolomic analyses to explore the cellular pathways mediating the interaction between the bloom-forming coccolithophore Emiliania huxleyi and its specific coccolithoviruses (E. huxleyi virus [ EhV ]). We show that EhV induces profound transcriptome remodeling targeted toward fatty acid synthesis to support viral assembly. A metabolic shift toward production of viral-derived sphingolipids was detected during infection and coincided with downregulation of host de novo sphingolipid genes and induction of the viral-encoded homologous pathway. The depletion of host-specific sterols during lytic infection and their detection in purified virions revealed their novel role in viral life cycle. We identify an essential function of the mevalonate-isoprenoid branch of sterol biosynthesis during infection and propose its downregulation as an antiviral mechanism. We demonstrate how viral replication depends on the hijacking of host lipid metabolism during the chemical "arms race" in the ocean. [ABSTRACT FROM AUTHOR]

Published

2014

21. Mapping the diatom redox-sensitive proteome provides insight into response to nitrogen stress in the marine environment.

Author

Rosenwasser, Shilo, van Creveld, Shiri Graff, Schatz, Daniella, Malitsky, Sergey, Tzfadia, Oren, Aharoni, Asaph, Levin, Yishai, Gabashvili, Alexandra, Feldmesser, Ester, and Vardi, Assaf

Subjects

*PHYTOPLANKTON, *EUKARYOTES, *DIATOMS, *MASS spectrometry, *PHOTOBIOLOGY

Abstract

Diatoms are ubiquitous marine photosynthetic eukaryotes responsible for approximately 20% of global photosynthesis. Little is known about the redox-based mechanisms that mediate diatom sensing and acclimation to environmental stress. Here we used a quantitative mass spectrometry-based approach to elucidate the redox-sensitive signaling network (redoxome) mediating the response of diatoms to oxidative stress. We quantified the degree of oxidation of 3,845 cysteines in the Phaeodactylum tricornutum proteome and identified approximately 300 redox-sensitive proteins. Intriguingly, we found redox-sensitive thiols in numerous enzymes composing the nitrogen assimilation pathway and the recently discovered diatom urea cycle. In agreement with this finding, the flux from nitrate into glutamine and glutamate, measured by the incorporation of 15N, was strongly inhibited under oxidative stress conditions. Furthermore, by targeting the redox-sensitive GFP sensor to various subcellular localizations, we mapped organelle-specific oxidation patterns in response to variations in nitrogen quota and quality. We propose that redox regulation of nitrogen metabolism allows rapid metabolic plasticity to ensure cellular homeostasis, and thus is essential for the ecological success of diatoms in the marine ecosystem. [ABSTRACT FROM AUTHOR]

Published

2014

22. Overexpression of AtSHN1/WIN1 Provokes Unique Defense Responses.

Author

Sela, Dikla, Buxdorf, Kobi, Shi, Jian Xin, Feldmesser, Ester, Schreiber, Lukas, Aharoni, Asaph, and Levy, Maggie

Subjects

*PLANT cells & tissues, *PLANT defenses, *GENE expression in plants, *PLANT injuries, *PLANT lipids, *CELL death, *GENETIC transformation, *PREVENTION, *PLANTS

Abstract

The plant cell cuticle serves as the first barrier protecting plants from mechanical injury and invading pathogens. The cuticle can be breached by cutinase-producing pathogens and the degradation products may activate pathogenesis signals in the invading pathogens. Cuticle degradation products may also trigger the plant’s defense responses. Botrytis cinerea is an important plant pathogen, capable of attacking and causing disease in a wide range of plant species. Arabidopsis thaliana shn1-1D is a gain-of-function mutant, which has a modified cuticular lipid composition. We used this mutant to examine the effect of altering the whole-cuticle metabolic pathway on plant responses to B. cinerea attack. Following infection with B. cinerea, the shn1-1D mutant discolored more quickly, accumulated more H2O2, and showed accelerated cell death relative to wild-type (WT) plants. Whole transcriptome analysis of B. cinerea-inoculated shn1-1D vs. WT plants revealed marked upregulation of genes associated with senescence, oxidative stress and defense responses on the one hand, and genes involved in the magnitude of defense-response control on the other. We propose that altered cutin monomer content and composition of shn1-1D plants triggers excessive reactive oxygen species accumulation and release which leads to a strong, unique and uncontrollable defense response, resulting in plant sensitivity and death. [ABSTRACT FROM AUTHOR]

Published

2013

23. Mononuclear phagocyte miRNome analysis identifies miR-142 as critical regulator of murine dendritic cell homeostasis.

Author

Mildner, Alexander, Chapnik, Elik, Manor, Ohad, Yona, Simon, Ki-Wook Kim, Aychek, Tegest, Varol, Diana, Beck, Gilad, Itzhaki, Zohar Barnett, Feldmesser, Ester, Amit, Ido, Hornstein, Eran, and Jung, Steffen

Subjects

*PHAGOCYTES, *DENDRITIC cells, *NATURAL immunity, *STEM cells, *TRANSCRIPTION factors, *GENE expression, *MYELOID leukemia

Abstract

The mononuclear phagocyte system comprises cells as diverse as monocytes, macrophages, and dendritic cells (DCs), which collectively play key roles in innate immune responses and the triggering of adaptive immunity. Recent studies have highlighted the role of growth and transcription factors in defining developmental pathways and lineage relations within this cellular compartment. However, contributions of miRNAs to the development of mononuclear phagocytes remain largely unknown. In the present study, we report a comprehensive map of miRNA expression profiles for distinct myeloid populations, including BM-resident progenitors, monocytes, and mature splenic DCs. Each of the analyzed cell populations displayed a distinctive miRNA profile, suggesting a role for miRNAs in defining myeloid cell identities. Focusing on DC development, we found miR-142 to be highly expressed in classic FLT3-L-dependent CD4+ DCs, whereas reduced expression was observed in closely related CD8a+ or CD4-CD8α-DCs. Moreover, mice deficient for miR-142 displayed an impairment of CD4+ DC homeostasis both in vitro and in vivo. Furthermore, loss of miR-142-de pen dent CD4+ DCs was accompanied by a severe and specific defect in the priming of CD4+ T cells. The results of our study establish a novel role for miRNAs in myeloid cell specification and define miR-142 as a pivotal genetic component in the maintenance of CD4+ DCs. [ABSTRACT FROM AUTHOR]

Published

2013

24. Expression Profiling and Biochemical Analysis Suggest Stress Response as a Potential Mechanism Inhibiting Proliferation of Polyamine-depleted Cells.

Author

Landau, Guy, Ran, Avichai, Bercovich, Zippi, Feldmesser, Ester, Horn-Saban, Shirley, Korkotian, Eduard, Jacob-Hirsh, Jasmine, Rechavi, Gideon, Ron, David, and Kahana, Chaim

Subjects

*POLYAMINES, *CELL proliferation, *GENE expression, *RETICULUM (Ruminants), *CELL growth

Abstract

Polyamines are small organic polycations that are absolutely required for cell growth and proliferation; yet the basis for this requirement is mostly unknown. Here, we combined a genomewide expression profiling with biochemical analysis to reveal the molecular basis for inhibited proliferation of polyamine-depleted cells. Transcriptional responses accompanying growth arrest establishment in polyamine-depleted cells or growth resumption following polyamine replenishment were monitored and compared. Changes in the expression of genes related to various fundamental cellular processes were established. Analysis of mirrorsymmetric expression patterns around the G1-arrest point identified a set of genes representing a stress-response signature. Indeed, complementary biochemical analysis demonstrated activation of the PKR-like endoplasmic reticulum kinase arm of the unfolded protein response and of the stress-induced p38 MAPK. These changes were accompanied by induction of key growth-inhibitory factors such as p21 and Gadd45a and reduced expression of various cyclins, most profoundly cyclin D1, setting the basis for the halted proliferation. However, although the induced stress response could arrest growth, polyamine depletion also inhibited proliferation of PKR-like endoplasmic reticulum kinase and p38α- deficient cells and of cells harboring a nonphosphorylatable mutant eIF2α (S51A), suggesting that additional yet unidentified mechanisms might inhibit proliferation of polyamine-depleted cells. Despite lengthy persistence of the stress and activation of apoptotic signaling, polyamine-depleted cells remained viable, apparently due to induced expression of protective genes and development of autophagy. [ABSTRACT FROM AUTHOR]

Published

2012

25. RNF20 and USP44 Regulate Stem Cell Differentiation by Modulating H2B Monoubiquitylation

Author

Fuchs, Gilad, Shema, Efrat, Vesterman, Rita, Kotler, Eran, Wolchinsky, Zohar, Wilder, Sylvia, Golomb, Lior, Pribluda, Ariel, Zhang, Feng, Haj-Yahya, Mahmood, Feldmesser, Ester, Brik, Ashraf, Yu, Xiaochun, Hanna, Jacob, Aberdam, Daniel, Domany, Eytan, and Oren, Moshe

Subjects

*EMBRYONIC stem cells, *UBIQUITINATION, *HISTONES, *GENETIC transcription, *CELL differentiation, *LIGASES, *GENETIC regulation

Abstract

Summary: Embryonic stem cells (ESCs) maintain high genomic plasticity, which is essential for their capacity to enter diverse differentiation pathways. Posttranscriptional modifications of chromatin histones play a pivotal role in maintaining this plasticity. We now report that one such modification, monoubiquitylation of histone H2B on lysine 120 (H2Bub1), catalyzed by the E3 ligase RNF20, increases during ESC differentiation and is required for efficient execution of this process. This increase is particularly important for the transcriptional induction of relatively long genes during ESC differentiation. Furthermore, we identify the deubiquitinase USP44 as a negative regulator of H2B ubiquitylation, whose downregulation during ESC differentiation contributes to the increase in H2Bub1. Our findings suggest that optimal ESC differentiation requires dynamic changes in H2B ubiquitylation patterns, which must occur in a timely and well-coordinated manner. [ABSTRACT FROM AUTHOR]

Published

2012

26. Insights into the transcriptomics of polyphagy: Bemisia tabaci adaptability to phenylpropanoids involves coordinated expression of defense and metabolic genes

Author

Alon, Michal, Elbaz, Moshe, Ben-Zvi, Michal Moyal, Feldmesser, Ester, Vainstein, Alexander, and Morin, Shai

Subjects

*GENETIC transcription, *SWEETPOTATO whitefly, *PHENYLPROPANOIDS, *GENE expression, *AGRICULTURAL pests, *HORTICULTURAL crops, *DNA microarrays, *PLANT defenses, *PLANT metabolism

Abstract

Abstract: The whitefly Bemisia tabaci is a major generalist agricultural pest of field and horticultural crops world-wide. Despite its importance, the molecular bases of defense mechanisms in B. tabaci against major plant secondary defense compounds, such as the phenylpropanoids, remain unknown. Our experimental system utilized transgenic Nicotiana tabacum plants constitutively expressing the PAP1/AtMYB75 transcription factor which activates relatively specifically the phenylpropanoid/flavonoids biosynthetic pathway. Our study used suppression subtractive hybridization (SSH) and cDNA microarray approaches to compare gene expression between B. tabaci adults subjected to wild-type or transgenic plants for 6 h. A total of 2880 clones from the SSH libraries were sequenced. Both the SSH and cDNA microarray analyses indicated a complex interaction between B. tabaci and secondary defense metabolites produced by the phenylproapnoids/flavonoids pathway, involving enhanced expression of detoxification, immunity, oxidative stress and general stress related genes as well as general metabolism and ribosomal genes. Quantitative real-time PCR revealed significant changes in the expression of several of these genes in response to feeding on artificial diet containing the flavonoids quercetin. The elevated transcriptional activity was not accompanied by reduced reproductive performance, indicating high adaptability of B. tabaci to this large group of plant secondary defense metabolites. [Copyright &y& Elsevier]

Published

2012

27. Equivalent Mutations in the Eight Subunits of the Chaperonin CCT Produce Dramatically Different Cellular and Gene Expression Phenotypes

Author

Amit, Maya, Weisberg, Sarah J., Nadler-Holly, Michal, McCormack, Elizabeth A., Feldmesser, Ester, Kaganovich, Daniel, Willison, Keith R., and Horovitz, Amnon

Subjects

*MOLECULAR chaperones, *GENETIC mutation, *GENE expression, *EUKARYOTIC cells, *PROTEIN folding, *ADENOSINE triphosphate, *HYDROLYSIS, *SACCHAROMYCES cerevisiae, *YEAST fungi

Abstract

Abstract: The eukaryotic cytoplasmic chaperonin-containing TCP-1 (CCT) is a complex formed by two back-to-back stacked hetero-octameric rings that assists the folding of actins, tubulins, and other proteins in an ATP-dependent manner. Here, we tested the significance of the hetero-oligomeric nature of CCT in its function by introducing, in each of the eight subunits in turn, an identical mutation at a position that is conserved in all the subunits and is involved in ATP hydrolysis, in order to establish the extent of ‘individuality’ of the various subunits. Our results show that these identical mutations lead to dramatically different phenotypes. For example, Saccharomyces cerevisiae yeast cells with the mutation in subunit CCT2 display heat sensitivity and cold sensitivity for growth, have an excess of actin patches, and are the only strain here generated that is pseudo-diploid. By contrast, cells with the mutation in subunit CCT7 are the only ones to accumulate juxtanuclear protein aggregates that may reflect an impaired stress response in this strain. System-level analysis of the strains using RNA microarrays reveals connections between CCT and several cellular networks, including ribosome biogenesis and TOR2, that help to explain the phenotypic variability observed. [ABSTRACT FROM AUTHOR]

Published

2010

28. A Critical Role for Ceramide Synthase 2 in Liver Homeostasis.

Author

Pewzner-Jung, Yael, Brenner, Ori, Braun, Svantje, Laviad, Elad L., Ben-Dor, Shifra, Feldmesser, Ester, Horn-Saban, Shirley, Amann-Zalcenstein, Daniela, Raanan, Calanit, Berkutzki, Tamara, Erez-Roman, Racheli, Ben-David, Oshrit, Levy, Michal, Holzman, Dorin, Hyejung Park, Nyska, Abraham, Merrill Jr., Alfred H., and Futerman, Anthony H.

Subjects

*CERAMIDES, *HOMEOSTASIS, *LIVER, *MICE, *GLYCOSPHINGOLIPIDS

Abstract

We have generated a mouse that cannot synthesize very long acyl chain (C22-C24) ceramides (Pewzner-Jung, Y., Park, H., Laviad, E. L., Silva, L. C., Lahiri, S., Stiban, J., Erez-Roman, R., Brugger, B., Sachsenheimer, T., Wieland, F. T., Prieto, M., Merrill, A. H., and Futerman, A. H. (2010) J. Biol. Chem. 285, 10902-10910) due to ablation of ceramide synthase 2 (CerS2). As a result, significant changes were observed in the sphingolipid profile of livers from these mice, including elevated C16-ceramide and sphinganine levels. We now examine the functional consequences of these changes. CerS2 null mice develop severe nonzonal hepatopathy from about 30 days of age, the age at which CerS2 expression peaks in wild type mice, and display increased rates of hepatocyte apoptosis and proliferation. In older mice there is extensive and pronounced hepatocellular anisocytosis with widespread formation of nodules of regenerative hepatocellular hyperplasia. Progressive hepatomegaly and noninvasive hepatocellular carcinoma are also seen from ~10 months of age. Even though CerS2 is found at equally high mRNA levels in kidney and liver, there are no changes in renal function and no pathological changes in the kidney. High throughput analysis of RNA expression in liver revealed up-regulation of genes associated with cell cycle regulation, protein transport, cell-cell interactions and apoptosis, and down-regulation of genes associated with intermediary metabolism, such as lipid and steroid metabolism, adipocyte signaling, and amino acid metabolism. In addition, levels of the cell cycle regulator, the cyclin dependent-kinase inhibitor p21WAF1/CIP1, were highly elevated, which occurs by at least two mechanisms, one of which may involve p53. We propose a functional rationale for the synthesis of sphingolipids with very long acyl chains in liver homeostasis and in cell physiology. [ABSTRACT FROM AUTHOR]

Published

2010

29. Reduced Lamin A/C Does Not Facilitate Cancer Cell Transendothelial Migration but Compromises Lung Metastasis.

Author

Roncato, Francesco, Regev, Ofer, Feigelson, Sara W., Yadav, Sandeep Kumar, Kaczmarczyk, Lukasz, Levi, Nehora, Drago-Garcia, Diana, Ovadia, Samuel, Kizner, Marina, Addadi, Yoseph, Sabino, João C., Ovadya, Yossi, de Almeida, Sérgio F., Feldmesser, Ester, Gerlitz, Gabi, Alon, Ronen, and Roccaro, Aldo M.

Subjects

*PROTEIN metabolism, *ENDOTHELIAL cells, *IN vitro studies, *IN vivo studies, *LUNGS, *CAPILLARIES, *ANIMAL experimentation, *LUNG tumors, *METASTASIS, *CELL physiology, *CELL nuclei, *CELL motility, *CELL survival, *CELL lines, *MICE, *EPIGENOMICS

Abstract

Simple Summary: The nucleus is the largest and stiffest organelle of tumor cells. Cancer metastasis depends on the ability of cancer cells circulating in the blood to exit blood vessels and survive in target organs. The roles of the shell (lamina) of the nucleus in cancer cell migration and survival in distinct organs of metastasis are still unclear. A-type lamins are key lamina components that increase nuclear stiffness and reduce squeezing capacity through highly rigid barriers. We addressed how reduced expression of A-lamins (lamin A/C) affects cancer cell survival and crossing of endothelial barriers and lung capillaries and found that reduced lamin A/C expression impairs cancer growth in spheroids and restricts cancer metastasis to lungs without improving cancer cell squeezing and extravasation from lung vessels, the key platform for cancer entry into lungs. The mechanisms by which the nuclear lamina of tumor cells influences tumor growth and migration are highly disputed. Lamin A and its variant lamin C are key lamina proteins that control nucleus stiffness and chromatin conformation. Downregulation of lamin A/C in two prototypic metastatic lines, B16F10 melanoma and E0771 breast carcinoma, facilitated cell squeezing through rigid pores, and reduced heterochromatin content. Surprisingly, both lamin A/C knockdown cells grew poorly in 3D spheroids within soft agar, and lamin A/C deficient cells derived from spheroids transcribed lower levels of the growth regulator Yap1. Unexpectedly, the transendothelial migration of both cancer cells in vitro and in vivo, through lung capillaries, was not elevated by lamin A/C knockdown and their metastasis in lungs was even dramatically reduced. Our results are the first indication that reduced lamin A/C content in distinct types of highly metastatic cancer cells does not elevate their transendothelial migration (TEM) capacity and diapedesis through lung vessels but can compromise lung metastasis at a post extravasation level. [ABSTRACT FROM AUTHOR]

Published

2021

30. RNF20 and USP44 Regulate Stem Cell Differentiation by Modulating H2B Monoubiquitylation.

Author

Fuchs, Gilad, Shema, Efrat, Vesterman, Rita, Kotler, Eran, Wolchinsky, Zohar, Wilder, Sylvia, Golomb, Lior, Pribluda, Ariel, Zhang, Feng, Haj-Yahya, Mahmood, Feldmesser, Ester, Brik, Ashraf, Yu, Xiaochun, Hanna, Jacob, Aberdam, Daniel, Domany, Eytan, and Oren, Moshe

Subjects

*STEM cells, *CELL differentiation, *UBIQUITINATION, *SMALL interfering RNA, *PEPTIDASE

Published

2015