909 research outputs found
The RNA helicase database
RNA helicases are ubiquitous and essential enzymes that function in nearly all aspects of RNA metabolism. The RNA helicase database (www.rnahelicase.org) integrates the wealth of accumulating information on RNA helicases in a readily accessible format. The database is a portal that allows straightforward retrieval of comprehensive information on sequence, structure and on biochemical and cellular functions of all RNA helicases from the most widely used model organisms Escherichia coli, Saccharomyces cerevisiae, Caenorhabditis elegans, Drosophila melanogaster, mouse and human. Also included are RNA helicases from other organisms that are subject to specific investigation. The database is structured according to the most recent helicase classification into helicase superfamilies (SFs) and families, and thus emphasizes phyologenetic relations between RNA helicases as well. Information on individual RNA helicases can be accessed through various browsing routes or through text-based searches of the database
TARGET: A Digitizing And Trigger ASIC For The Cherenkov Telescope Array
The future ground-based gamma-ray observatory Cherenkov Telescope Array (CTA)
will feature multiple types of imaging atmospheric Cherenkov telescopes, each
with thousands of pixels. To be affordable, camera concepts for these
telescopes have to feature low cost per channel and at the same time meet the
requirements for CTA in order to achieve the desired scientific goals. We
present the concept of the TeV Array Readout Electronics with GSa/s sampling
and Event Trigger (TARGET) Application Specific Circuit (ASIC), envisaged to be
used in the cameras of various CTA telescopes, e.g. the Gamma-ray Cherenkov
Telescope (GCT), a proposed 2-Mirror Small-Sized Telescope, and the
Schwarzschild-Couder Telescope (SCT), a proposed Medium-Sized Telescope. In the
latest version of this readout concept the sampling and trigger parts are split
into dedicated ASICs, TARGET C and T5TEA, both providing 16 parallel input
channels. TARGET C features a tunable sampling rate (usually 1 GSa/s), a 16k
sample deep buffer for each channel and on-demand digitization and transmission
of waveforms with typical spans of ~100 ns. The trigger ASIC, T5TEA, provides 4
low voltage differential signal (LVDS) trigger outputs and can generate a
pedestal voltage independently for each channel. Trigger signals are generated
by T5TEA based on the analog sum of the input in four independent groups of
four adjacent channels and compared to a threshold set by the user. Thus, T5TEA
generates four LVDS trigger outputs, as well as 16 pedestal voltages fed to
TARGET C independently for each channel. We show preliminary results of the
characterization and testing of TARGET C and T5TEA.Comment: 6 pages, 8 figures, Proceedings of the 6th International Symposium on
High-Energy Gamma-Ray Astronomy (Gamma2016
Rodent Aβ Modulates the Solubility and Distribution of Amyloid Deposits in Transgenic Mice
The amino acid sequence of amyloid precursor protein (APP) is highly conserved, and age-related Abeta aggregates have been described in a variety of vertebrate animals, with the notable exception of mice and rats. Three amino acid substitutions distinguish mouse and human Abeta that might contribute to their differing properties in vivo. To examine the amyloidogenic potential of mouse Abeta, we studied several lines of transgenic mice overexpressing wild-type mouse amyloid precursor protein (moAPP) either alone or in conjunction with mutant PS1 (PS1dE9). Neither overexpression of moAPP alone nor co-expression with PS1dE9 caused mice to develop Alzheimer-type amyloid pathology by 24 months of age. We further tested whether mouse Abeta could accelerate the deposition of human Abeta by crossing the moAPP transgenic mice to a bigenic line expressing human APPswe with PS1dE9. The triple transgenic animals (moAPP x APPswe/PS1dE9) produced 20% more Abeta but formed amyloid deposits no faster and to no greater extent than APPswe/PS1dE9 siblings. Instead, the additional mouse Abeta increased the detergent solubility of accumulated amyloid and exacerbated amyloid deposition in the vasculature. These findings suggest that, although mouse Abeta does not influence the rate of amyloid formation, the incorporation of Abeta peptides with differing sequences alters the solubility and localization of the resulting aggregates
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The helicase Ded1p controls use of near-cognate translation initiation codons in 5' UTRs.
The conserved and essential DEAD-box RNA helicase Ded1p from yeast and its mammalian orthologue DDX3 are critical for the initiation of translation1. Mutations in DDX3 are linked to tumorigenesis2-4 and intellectual disability5, and the enzyme is targeted by a range of viruses6. How Ded1p and its orthologues engage RNAs during the initiation of translation is unknown. Here we show, by integrating transcriptome-wide analyses of translation, RNA structure and Ded1p-RNA binding, that the effects of Ded1p on the initiation of translation are connected to near-cognate initiation codons in 5' untranslated regions. Ded1p associates with the translation pre-initiation complex at the mRNA entry channel and repressing the activity of Ded1p leads to the accumulation of RNA structure in 5' untranslated regions, the initiation of translation from near-cognate start codons immediately upstream of these structures and decreased protein synthesis from the corresponding main open reading frames. The data reveal a program for the regulation of translation that links Ded1p, the activation of near-cognate start codons and mRNA structure. This program has a role in meiosis, in which a marked decrease in the levels of Ded1p is accompanied by the activation of the alternative translation initiation sites that are seen when the activity of Ded1p is repressed. Our observations indicate that Ded1p affects translation initiation by controlling the use of near-cognate initiation codons that are proximal to mRNA structure in 5' untranslated regions
Principais usos da madeira de reflorestamento.
O plantio de espécies florestais de rápido crescimento em propriedades rurais traz uma série de benefÃcios indiretos,tais como a ocupação de solos não agricultáveis,proteção de nascentes e cursos d'água,recuperação do solo,entre outros.Contudo,a cultura da floresta é também uma atividade econômica,tal como uma cultura agrÃcola tradicional
Dynamic Regulation of Alternative Splicing by Silencers that Modulate 5′ Splice Site Competition
SummaryAlternative splicing makes a major contribution to proteomic diversity in higher eukaryotes with ∼70% of genes encoding two or more isoforms. In most cases, the molecular mechanisms responsible for splice site choice remain poorly understood. Here, we used a randomization-selection approach in vitro to identify sequence elements that could silence a proximal strong 5′ splice site located downstream of a weakened 5′ splice site. We recovered two exonic and four intronic motifs that effectively silenced the proximal 5′ splice site both in vitro and in vivo. Surprisingly, silencing was only observed in the presence of the competing upstream 5′ splice site. Biochemical evidence strongly suggests that the silencing motifs function by altering the U1 snRNP/5′ splice site complex in a manner that impairs commitment to specific splice site pairing. The data indicate that perturbations of non-rate-limiting step(s) in splicing can lead to dramatic shifts in splice site choice
Target of Opportunity observations of flaring blazars with H.E.S.S.
Blazars are the most common class of TeV extragalactic emitters. In the
framework of the AGN unified model, they are understood as AGNs with a
relativistic jet pointing close the line of sight. They are characterized by
extreme variability, observed to be as fast as minutes. These flares are
usually observed at multiple wavelengths and their study require fast reaction
and coordination among multiwavelength observatories. An important part of
blazars observations with the H.E.S.S. array of Cherenkov telescopes is thus in
the form of Target of Opportunity (ToO) observations. In this contribution the
H.E.S.S. blazar ToO program is presented, with a focus on recent results.Comment: to appear in the proceedings of the ICRC 2023 Conferenc
The helicase HAGE prevents interferon-a-induced PML expression in ABCB5+ malignant melanoma-initiating cells by promoting the expression of SOCS1
The tumour suppressor PML (promyelocytic leukaemia protein) regulates several cellular pathways involving cell growth, apoptosis, differentiation and senescence. PML also has an important role in the regulation of stem cell proliferation and differentiation. Here, we show the involvement of the helicase HAGE in the transcriptional repression of PML expression in ABCB5 + malignant melanoma-initiating cells (ABCB5 + MMICs), a population of cancer stem cells which are responsible for melanoma growth, progression and resistance to drug-based therapy. HAGE prevents PML gene expression by inhibiting the activation of the JAK-STAT (janus kinase-signal transducers and activators of transcription) pathway in a mechanism which implicates the suppressor of cytokine signalling 1 (SOCS1). Knockdown of HAGE led to a significant decrease in SOCS1 protein expression, activation of the JAK-STAT signalling cascade and a consequent increase of PML expression. To confirm that the reduction in SOCS1 expression was dependent on the HAGE helicase activity, we showed that SOCS1, effectively silenced by small interfering RNA, could be rescued by re-introduction of HAGE into cells lacking HAGE. Furthermore, we provide a mechanism by which HAGE promotes SOCS1 mRNA unwinding and protein expression in vitro
Genetic modulation of soluble Aβ rescues cognitive and synaptic impairment in a mouse model of Alzheimer\u27s disease
An unresolved debate in Alzheimer's disease (AD) is whether amyloid plaques are pathogenic, causing overt physical disruption of neural circuits, or protective, sequestering soluble forms of amyloid-β (Aβ) that initiate synaptic damage and cognitive decline. Few animal models of AD have been capable of isolating the relative contribution made by soluble and insoluble forms of Aβ to the behavioral symptoms and biochemical consequences of the disease. Here we use a controllable transgenic mouse model expressing a mutant form of amyloid precursor protein (APP) to distinguish the impact of soluble Aβ from that of deposited amyloid on cognitive function and synaptic structure. Rapid inhibition of transgenic APP modulated the production of Aβ without affecting pre-existing amyloid deposits and restored cognitive performance to the level of healthy controls in Morris water maze, radial arm water maze, and fear conditioning. Selective reduction of Aβ with a γ-secretase inhibitor provided similar improvement, suggesting that transgene suppression restored cognition, at least in part by lowering Aβ. Cognitive improvement coincided with reduced levels of synaptotoxic Aβ oligomers, greater synaptic density surrounding amyloid plaques, and increased expression of presynaptic and postsynaptic markers. Together these findings indicate that transient Aβ species underlie much of the cognitive and synaptic deficits observed in this model and demonstrate that significant functional and structural recovery can be attained without removing deposited amyloid
The NuSTAR view of the non-thermal emission from PSR J0437-4715
We present a hard X-ray Nuclear Spectroscopic Telescope Array (NuSTAR) observation of PSR J0437−4715, the nearest millisecond pulsar. The known pulsations at the apparent pulse period ∼5.76ms are observed with a significance of 3.7σ, at energies up to 20 keV above which the NuSTAR background dominates. We measure a photon index Γ = 1.50 ± 0.25 (90 per cent confidence) for the power-law fit to the non-thermal emission. It had been shown that spectral models with two or three thermal components fit the XMM–Newton spectrum of PSR J0437−4715, depending on the slope of the power-law component, and the amount of absorption of soft X-rays. The new constraint on the high-energy emission provided by NuSTAR removes ambiguities regarding the thermal components of the emission below 3keV. We performed a simultaneous spectral analysis of the XMM–Newton and NuSTAR data to confirm that three thermal components and a power law are required to fit the 0.3–20 keV emission of PSR J0437−4715. Adding a ROSAT-PSPC spectrum further confirmed this result and allowed us to better constrain the temperatures of the three thermal components. A phase-resolved analysis of the NuSTAR data revealed no significant change in the photon index of the high-energy emission. This NuSTAR observation provides further impetus for future observations with the NICER mission (Neutron Star Interior Composition Explorer) whose sensitivity will provide much stricter constraints on the equation of state of nuclear matter by combining model fits to the pulsar's phase-folded light curve with the pulsar's well-defined mass and distance from radio timing observations
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