348 research outputs found
Correlated fragile site expression allows the identification of candidate fragile genes involved in immunity and associated with carcinogenesis
Background: Common fragile sites (cfs) are specific regions in the human genome that are particularly prone to genomic instability under conditions of replicative stress. Several investigations support the view that common fragile sites play a role in carcinogenesis. We discuss a genome-wide approach based on graph theory and Gene Ontology vocabulary for the functional characterization of common fragile sites and for the identification of genes that contribute to tumour cell biology.
Results: Common fragile sites were assembled in a network based on a simple measure of correlation among common fragile site patterns of expression. By applying robust measurements to capture in quantitative terms the non triviality of the network, we identified several topological features clearly indicating departure from the Erdos-Renyi random graph model. The most important outcome was the presence of an unexpected large connected component far below the percolation threshold. Most of the best characterized common fragile sites belonged to this connected component. By filtering this connected component with Gene Ontology, statistically significant shared functional features were detected. Common fragile sites were found to be enriched for genes associated to the immune response and to mechanisms involved in tumour progression such as extracellular space remodeling and angiogenesis. Moreover we showed how the internal organization of the graph in communities and even in very simple subgraphs can be a starting point for the identification of new factors of instability at common fragile sites.
Conclusion: We developed a computational method addressing the fundamental issue of studying the functional content of common fragile sites. Our analysis integrated two different approaches. First, data on common fragile site expression were analyzed in a complex networks framework. Second, outcomes of the network statistical description served as sources for the functional annotation of genes at common fragile sites by means of the Gene Ontology vocabulary. Our results support the hypothesis that fragile sites serve a function; we propose that fragility is linked to a coordinated regulation of fragile genes expression
Correlated fragile site expression allows the identification of candidate fragile genes involved in immunity and associated with carcinogenesis
Common fragile sites (cfs) are specific regions in the human genome that are
particularly prone to genomic instability under conditions of replicative
stress. Several investigations support the view that common fragile sites play
a role in carcinogenesis. We discuss a genome-wide approach based on graph
theory and Gene Ontology vocabulary for the functional characterization of
common fragile sites and for the identification of genes that contribute to
tumour cell biology. CFS were assembled in a network based on a simple measure
of correlation among common fragile site patterns of expression. By applying
robust measurements to capture in quantitative terms the non triviality of the
network, we identified several topological features clearly indicating
departure from the Erdos-Renyi random graph model. The most important outcome
was the presence of an unexpected large connected component far below the
percolation threshold. Most of the best characterized common fragile sites
belonged to this connected component. By filtering this connected component
with Gene Ontology, statistically significant shared functional features were
detected. Common fragile sites were found to be enriched for genes associated
to the immune response and to mechanisms involved in tumour progression such as
extracellular space remodeling and angiogenesis. Our results support the
hypothesis that fragile sites serve a function; we propose that fragility is
linked to a coordinated regulation of fragile genes expression.Comment: 18 pages, accepted for publication in BMC Bioinformatic
Ecological implications beyond the ecotoxicity of plastic debris on marine phytoplankton assemblage structure and functioning
none7noPlastic pollution is a global issue posing a threat to marine biota with ecological implications on ecosystem
functioning. Micro and nanoplastic impact on phytoplankton autotrophic species (e.g., cell growth inhibition,
decrease in chlorophyll a and photosynthetic efficiency and hetero-aggregates formation) have been largely
documented. However, the heterogeneity of data makes rather difficult a comparison based on size (i.e. micro vs
nano). In addition, knowledge gaps on the ecological impact on phytoplankton assemblage structure and
functioning are evident. A new virtual meta-analysis on cause-effect relationships of micro and nanoplastics on
phytoplankton species revealed the significant effect posed by polymer type on reducing cell density for tested
PVC, PS and PE plastics. Linked with autotrophic phytoplankton role in atmospheric CO2 fixation, a potential
impact of plastics on marine carbon pump is discussed. The understanding of the effects of microplastics and
nanoplastics on the phytoplankton functioning is fundamental to raise awareness on the overall impact on the
first level of marine food web. Interactions between micro and nanoplastics and phytoplankton assemblages have
been quite documented by in vitro examinations; but, further studies considering natural plankton assemblages
and/or large mesocosm experiments should be performed to evaluate and try predicting ecological impacts on
primary producers.openCasabianca Silvia, Bellingeri Arianna, Capellacci Samuela, Sbrana Alice, Russo Tommaso, Corsi Ilaria, Penna AntonellaCasabianca, Silvia; Bellingeri, Arianna; Capellacci, Samuela; Sbrana, Alice; Russo, Tommaso; Corsi, Ilaria; Penna, Antonell
The “discard problem” in Mediterranean fisheries, in the face of the European Union landing obligation: the case of bottom trawl fishery and implications for management
Since the first introduction of the landing obligation (a.k.a. Discard ban) in 2015, the EU Mediterranean fisheries are facing some unforeseen challenges. The demersal bottom trawl fisheries, being the most significant contributors to the so-called 'discard problem', are confronted with the greatest challenges. Data from the Italian and the Greek fleet, spanning over two decades (1995–2015), were analysed with the intention of revealing the diversity and heterogeneity of the discard problem, especially for regulated species. Species composition of discards, as well as discarding rates, were shown to be irregular, fluctuating among areas, depth strata, seasons and years. Although fish dominated the discarded gross catch in weight, benthic invertebrates (other than commercial cephalopods and crustaceans) were the taxa discarded almost exclusively. The established minimum conservation reference size was largely ignored by fishers. From a management point of view, the present investigation suggests that the recently established Discard Management Plans lack scientific evidence (given the high intrinsic variability of the parameters and confusion regarding the rules) and provide exemptions from the landing obligation that will in practice allow the average Mediterranean bottom trawl vessel to continue business as usual. Moreover, detecting if these rules are actually respected is an almost impossible task for the Mediterranean control and enforcement authorities. Incentivizing the adoption of fishing technologies and practices that reduce pre-harvest mortality and post-harvest discards, while avoiding damage to sensitive marine species and habitats, seems the only way to move forward, rather than dealing with the problem after it has occurred
Synthesis of CdS and CdSe nanocrystallites using a novel single-molecule precursors approach
The synthesis of CdS and CdSe nanocrystallites using the thermolysis of several dithioor
diselenocarbamato complexes of cadmium in trioctylphosphine oxide (TOPO) is reported.
The nanodispersed materials obtained show quantum size effects in their optical spectra
and exhibit near band-edge luminescence. The influence of experimental parameters on
the properties of the nanocrystallites is discussed. HRTEM images of these materials show
well-defined, crystalline nanosized particles. Standard size fractionation procedures can
be performed in order to narrow the size dispersion of the samples. The TOPO-capped CdS
and CdSe nanocrystallites and simple organic bridging ligands, such as 2,2¢-bipyrimidine,
are used as the starting materials for the preparation of novel nanocomposites. The optical
properties shown by these new nanocomposites are compared with those of the starting
nanodispersed materials
Global Mapping of DNA Conformational Flexibility on Saccharomyces cerevisiae
In this study we provide the first comprehensive map of DNA conformational flexibility in Saccharomyces cerevisiae complete genome. Flexibility plays a key role in DNA supercoiling and DNA/protein binding, regulating DNA transcription, replication or repair. Specific interest in flexibility analysis concerns its relationship with human genome instability. Enrichment in flexible sequences has been detected in unstable regions of human genome defined fragile sites, where genes map and carry frequent deletions and rearrangements in cancer. Flexible sequences have been suggested to be the determinants of fragile gene proneness to breakage; however, their actual role and properties remain elusive. Our in silico analysis carried out genome-wide via the StabFlex algorithm, shows the conserved presence of highly flexible regions in budding yeast genome as well as in genomes of other Saccharomyces sensu stricto species. Flexibile peaks in S. cerevisiae identify 175 ORFs mapping on their 3’UTR, a region affecting mRNA translation, localization and stability. (TA)n repeats of different extension shape the central structure of peaks and co-localize with polyadenylation efficiency element (EE) signals. ORFs with flexible peaks share common features. Transcripts are characterized by decreased half-life: this is considered peculiar of genes involved in regulatory systems with high turnover; consistently, their function affects biological processes such as cell cycle regulation or stress response. Our findings support the functional importance of flexibility peaks, suggesting that the flexible sequence may be derived by an expansion of canonical TAYRTA polyadenylation efficiency element. The flexible (TA)n repeat amplification could be the outcome of an evolutionary neofunctionalization leading to a differential 3’-end processing and expression regulation in genes with peculiar function. Our study provides a new support to the functional role of flexibility in genomes and a strategy for its characterization inside human fragile sites
Identification of COVID-19 patients at risk of hospital admission and mortality: a European multicentre retrospective analysis of mid-regional pro-adrenomedullin
Background: Mid-Regional pro-Adrenomedullin (MR-proADM) is an inflammatory biomarker that improves the prognostic assessment of patients with sepsis, septic shock and organ failure. Previous studies of MR-proADM have primarily focussed on bacterial infections. A limited number of small and monocentric studies have examined MR-proADM as a prognostic factor in patients infected with SARS-CoV-2, however there is need for multicenter validation. An evaluation of its utility in predicting need for hospitalisation in viral infections was also performed. Methods: An observational retrospective analysis of 1861 patients, with SARS-CoV-2 confirmed by RT-qPCR, from 10 hospitals across Europe was performed. Biomarkers, taken upon presentation to Emergency Departments (ED), clinical scores, patient demographics and outcomes were collected. Multiclass random forest classifier models were generated as well as calculation of area under the curve analysis. The primary endpoint was hospital admission with and without death. Results: Patients suitable for safe discharge from Emergency Departments could be identified through an MR-proADM value of ≤ 1.02 nmol/L in combination with a CRP (C-Reactive Protein) of ≤ 20.2 mg/L and age ≤ 64, or in combination with a SOFA (Sequential Organ Failure Assessment) score < 2 if MR-proADM was ≤ 0.83 nmol/L regardless of age. Those at an increased risk of mortality could be identified upon presentation to secondary care with an MR-proADM value of > 0.85 nmol/L, in combination with a SOFA score ≥ 2 and LDH > 720 U/L, or in combination with a CRP > 29.26 mg/L and age ≤ 64, when MR-proADM was > 1.02 nmol/L. Conclusions: This international study suggests that for patients presenting to the ED with confirmed SARS-CoV-2 infection, MR-proADM in combination with age and CRP or with the patient’s SOFA score could identify patients at low risk where outpatient treatment may be safe
In vitro mycorrhization of micropropagated plants: studies on Castanea sativa Mill.
In vitro mycorrhization can be made by several axenic and nonaxenic
techniques but criticism exists about their artificiality and inability to
reproduce under natural conditions. However, artificial mycorrhization under
controlled conditions can provide important information about the physiology
of symbiosis. Micropropagated Castanea sativa plants were inoculated with
the mycorrhizal fungus Pisolithus tinctorius after in vitro rooting. The
mycorrhizal process was monitored at regular intervals in order to evaluate the
mantle and hartig net formation, and the growth rates of mycorrhizal and
nonmycorrhizal plants. Plant roots show fungal hyphae adhesion at the surface
after 24 hours of mycorrhizal induction. After 20 days a mantle can be
observed and a hartig net is forming although the morphology of the epidermal
cells remains unaltered. At 30 days of root–fungus contact the hartig net is
well developed and the epidermal cells are already enlarged. After 50 days of
mycorrhizal induction, growth was higher for mycorrhizal plants than for
nonmycorrhizal ones. The length of the major roots was lower in mycorrhizal
plants after 40 days. Fresh and dry weights were higher in mycorrhizal plants
after 30 days. The growth rates of chestnut mycorrhizal plants are in agreement
with the morphological development of the mycorrhizal structures observed at
each mycorrhizal time. The assessment of symbiotic establishment takes into
account the formation of a mantle and a hartig net that were already developed
at 30 days, when differences between fresh and dry weights of mycorrhizal and
nonmycorrhizal plants can be quantified. In vitro conditions, mycorrhization
influences plant physiology after 20 days of root–fungus contact, namely in
terms of growth rates. Fresh and dry weights, heights, stem diameter and
growth rates increased while major root growth rate decreased in mycorrhizal
plants.Springe
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